---
_id: '14834'
abstract:
- lang: eng
  text: Bacteria divide by binary fission. The protein machine responsible for this
    process is the divisome, a transient assembly of more than 30 proteins in and
    on the surface of the cytoplasmic membrane. Together, they constrict the cell
    envelope and remodel the peptidoglycan layer to eventually split the cell into
    two. For Escherichia coli, most molecular players involved in this process have
    probably been identified, but obtaining the quantitative information needed for
    a mechanistic understanding can often not be achieved from experiments in vivo
    alone. Since the discovery of the Z-ring more than 30 years ago, in vitro reconstitution
    experiments have been crucial to shed light on molecular processes normally hidden
    in the complex environment of the living cell. In this review, we summarize how
    rebuilding the divisome from purified components – or at least parts of it - have
    been instrumental to obtain the detailed mechanistic understanding of the bacterial
    cell division machinery that we have today.
acknowledgement: We acknowledge members of the Loose laboratory at ISTA for helpful
  discussions—in particular M. Kojic for his insightful comments. This work was supported
  by the Austrian Science Fund (FWF P34607) to M.L.
article_number: '151380'
article_processing_charge: Yes
article_type: review
author:
- first_name: Philipp
  full_name: Radler, Philipp
  id: 40136C2A-F248-11E8-B48F-1D18A9856A87
  last_name: Radler
  orcid: '0000-0001-9198-2182 '
- first_name: Martin
  full_name: Loose, Martin
  id: 462D4284-F248-11E8-B48F-1D18A9856A87
  last_name: Loose
  orcid: 0000-0001-7309-9724
citation:
  ama: 'Radler P, Loose M. A dynamic duo: Understanding the roles of FtsZ and FtsA
    for Escherichia coli cell division through in vitro approaches. <i>European Journal
    of Cell Biology</i>. 2024;103(1). doi:<a href="https://doi.org/10.1016/j.ejcb.2023.151380">10.1016/j.ejcb.2023.151380</a>'
  apa: 'Radler, P., &#38; Loose, M. (2024). A dynamic duo: Understanding the roles
    of FtsZ and FtsA for Escherichia coli cell division through in vitro approaches.
    <i>European Journal of Cell Biology</i>. Elsevier. <a href="https://doi.org/10.1016/j.ejcb.2023.151380">https://doi.org/10.1016/j.ejcb.2023.151380</a>'
  chicago: 'Radler, Philipp, and Martin Loose. “A Dynamic Duo: Understanding the Roles
    of FtsZ and FtsA for Escherichia Coli Cell Division through in Vitro Approaches.”
    <i>European Journal of Cell Biology</i>. Elsevier, 2024. <a href="https://doi.org/10.1016/j.ejcb.2023.151380">https://doi.org/10.1016/j.ejcb.2023.151380</a>.'
  ieee: 'P. Radler and M. Loose, “A dynamic duo: Understanding the roles of FtsZ and
    FtsA for Escherichia coli cell division through in vitro approaches,” <i>European
    Journal of Cell Biology</i>, vol. 103, no. 1. Elsevier, 2024.'
  ista: 'Radler P, Loose M. 2024. A dynamic duo: Understanding the roles of FtsZ and
    FtsA for Escherichia coli cell division through in vitro approaches. European
    Journal of Cell Biology. 103(1), 151380.'
  mla: 'Radler, Philipp, and Martin Loose. “A Dynamic Duo: Understanding the Roles
    of FtsZ and FtsA for Escherichia Coli Cell Division through in Vitro Approaches.”
    <i>European Journal of Cell Biology</i>, vol. 103, no. 1, 151380, Elsevier, 2024,
    doi:<a href="https://doi.org/10.1016/j.ejcb.2023.151380">10.1016/j.ejcb.2023.151380</a>.'
  short: P. Radler, M. Loose, European Journal of Cell Biology 103 (2024).
date_created: 2024-01-18T08:16:43Z
date_published: 2024-01-12T00:00:00Z
date_updated: 2024-01-23T08:37:13Z
day: '12'
ddc:
- '570'
department:
- _id: MaLo
doi: 10.1016/j.ejcb.2023.151380
external_id:
  pmid:
  - '38218128'
has_accepted_license: '1'
intvolume: '       103'
issue: '1'
keyword:
- Cell Biology
- General Medicine
- Histology
- Pathology and Forensic Medicine
language:
- iso: eng
main_file_link:
- open_access: '1'
  url: https://doi.org/10.1016/j.ejcb.2023.151380
month: '01'
oa: 1
oa_version: Published Version
pmid: 1
project:
- _id: fc38323b-9c52-11eb-aca3-ff8afb4a011d
  grant_number: P34607
  name: "Understanding bacterial cell division by in vitro\r\nreconstitution"
publication: European Journal of Cell Biology
publication_identifier:
  issn:
  - 0171-9335
publication_status: epub_ahead
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: 'A dynamic duo: Understanding the roles of FtsZ and FtsA for Escherichia coli
  cell division through in vitro approaches'
tmp:
  image: /images/cc_by.png
  legal_code_url: https://creativecommons.org/licenses/by/4.0/legalcode
  name: Creative Commons Attribution 4.0 International Public License (CC-BY 4.0)
  short: CC BY (4.0)
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 103
year: '2024'
...
---
_id: '14726'
abstract:
- lang: eng
  text: Autocrine signaling pathways regulated by RAPID ALKALINIZATION FACTORs (RALFs)
    control cell wall integrity during pollen tube germination and growth in Arabidopsis
    (Arabidopsis thaliana). To investigate the role of pollen-specific RALFs in another
    plant species, we combined gene expression data with phylogenetic and biochemical
    studies to identify candidate orthologs in maize (Zea mays). We show that Clade
    IB ZmRALF2/3 mutations, but not Clade III ZmRALF1/5 mutations, cause cell wall
    instability in the sub-apical region of the growing pollen tube. ZmRALF2/3 are
    mainly located in the cell wall and are partially able to complement the pollen
    germination defect of their Arabidopsis orthologs AtRALF4/19. Mutations in ZmRALF2/3
    compromise pectin distribution patterns leading to altered cell wall organization
    and thickness culminating in pollen tube burst. Clade IB, but not Clade III ZmRALFs,
    strongly interact as ligands with the pollen-specific Catharanthus roseus RLK1-like
    (CrRLK1L) receptor kinases Zea mays FERONIA-like (ZmFERL) 4/7/9, LORELEI-like
    glycosylphosphatidylinositol-anchor (LLG) proteins Zea mays LLG 1 and 2 (ZmLLG1/2)
    and Zea mays pollen extension-like (PEX) cell wall proteins ZmPEX2/4. Notably,
    ZmFERL4 outcompetes ZmLLG2 and ZmPEX2 outcompetes ZmFERL4 for ZmRALF2 binding.
    Based on these data, we suggest that Clade IB RALFs act in a dual role as cell
    wall components and extracellular sensors to regulate cell wall integrity and
    thickness during pollen tube growth in maize and probably other plants.
article_number: koad324
article_processing_charge: No
article_type: original
author:
- first_name: Liang-Zi
  full_name: Zhou, Liang-Zi
  last_name: Zhou
- first_name: Lele
  full_name: Wang, Lele
  last_name: Wang
- first_name: Xia
  full_name: Chen, Xia
  last_name: Chen
- first_name: Zengxiang
  full_name: Ge, Zengxiang
  id: f43371a3-09ff-11eb-8013-bd0c6a2f6de8
  last_name: Ge
  orcid: 0000-0001-9381-3577
- first_name: Julia
  full_name: Mergner, Julia
  last_name: Mergner
- first_name: Xingli
  full_name: Li, Xingli
  last_name: Li
- first_name: Bernhard
  full_name: Küster, Bernhard
  last_name: Küster
- first_name: Gernot
  full_name: Längst, Gernot
  last_name: Längst
- first_name: Li-Jia
  full_name: Qu, Li-Jia
  last_name: Qu
- first_name: Thomas
  full_name: Dresselhaus, Thomas
  last_name: Dresselhaus
citation:
  ama: Zhou L-Z, Wang L, Chen X, et al. The RALF signaling pathway regulates cell
    wall integrity during pollen tube growth in maize. <i>The Plant Cell</i>. 2023.
    doi:<a href="https://doi.org/10.1093/plcell/koad324">10.1093/plcell/koad324</a>
  apa: Zhou, L.-Z., Wang, L., Chen, X., Ge, Z., Mergner, J., Li, X., … Dresselhaus,
    T. (2023). The RALF signaling pathway regulates cell wall integrity during pollen
    tube growth in maize. <i>The Plant Cell</i>. Oxford University Press. <a href="https://doi.org/10.1093/plcell/koad324">https://doi.org/10.1093/plcell/koad324</a>
  chicago: Zhou, Liang-Zi, Lele Wang, Xia Chen, Zengxiang Ge, Julia Mergner, Xingli
    Li, Bernhard Küster, Gernot Längst, Li-Jia Qu, and Thomas Dresselhaus. “The RALF
    Signaling Pathway Regulates Cell Wall Integrity during Pollen Tube Growth in Maize.”
    <i>The Plant Cell</i>. Oxford University Press, 2023. <a href="https://doi.org/10.1093/plcell/koad324">https://doi.org/10.1093/plcell/koad324</a>.
  ieee: L.-Z. Zhou <i>et al.</i>, “The RALF signaling pathway regulates cell wall
    integrity during pollen tube growth in maize,” <i>The Plant Cell</i>. Oxford University
    Press, 2023.
  ista: Zhou L-Z, Wang L, Chen X, Ge Z, Mergner J, Li X, Küster B, Längst G, Qu L-J,
    Dresselhaus T. 2023. The RALF signaling pathway regulates cell wall integrity
    during pollen tube growth in maize. The Plant Cell., koad324.
  mla: Zhou, Liang-Zi, et al. “The RALF Signaling Pathway Regulates Cell Wall Integrity
    during Pollen Tube Growth in Maize.” <i>The Plant Cell</i>, koad324, Oxford University
    Press, 2023, doi:<a href="https://doi.org/10.1093/plcell/koad324">10.1093/plcell/koad324</a>.
  short: L.-Z. Zhou, L. Wang, X. Chen, Z. Ge, J. Mergner, X. Li, B. Küster, G. Längst,
    L.-J. Qu, T. Dresselhaus, The Plant Cell (2023).
date_created: 2024-01-02T11:19:37Z
date_published: 2023-12-23T00:00:00Z
date_updated: 2024-01-03T12:43:41Z
day: '23'
ddc:
- '580'
doi: 10.1093/plcell/koad324
extern: '1'
has_accepted_license: '1'
keyword:
- Cell Biology
- Plant Science
language:
- iso: eng
main_file_link:
- open_access: '1'
  url: https://doi.org/10.1093/plcell/koad324
month: '12'
oa: 1
oa_version: Published Version
publication: The Plant Cell
publication_identifier:
  eissn:
  - 1532-298X
  issn:
  - 1040-4651
publication_status: epub_ahead
publisher: Oxford University Press
quality_controlled: '1'
status: public
title: The RALF signaling pathway regulates cell wall integrity during pollen tube
  growth in maize
tmp:
  image: /images/cc_by_nc_nd.png
  legal_code_url: https://creativecommons.org/licenses/by-nc-nd/4.0/legalcode
  name: Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International
    (CC BY-NC-ND 4.0)
  short: CC BY-NC-ND (4.0)
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
year: '2023'
...
---
_id: '14770'
abstract:
- lang: eng
  text: We developed LIONESS, a technology that leverages improvements to optical
    super-resolution microscopy and prior information on sample structure via machine
    learning to overcome the limitations (in 3D-resolution, signal-to-noise ratio
    and light exposure) of optical microscopy of living biological specimens. LIONESS
    enables dense reconstruction of living brain tissue and morphodynamics visualization
    at the nanoscale.
article_processing_charge: No
article_type: letter_note
author:
- first_name: Johann G
  full_name: Danzl, Johann G
  id: 42EFD3B6-F248-11E8-B48F-1D18A9856A87
  last_name: Danzl
  orcid: 0000-0001-8559-3973
- first_name: Philipp
  full_name: Velicky, Philipp
  id: 39BDC62C-F248-11E8-B48F-1D18A9856A87
  last_name: Velicky
  orcid: 0000-0002-2340-7431
citation:
  ama: Danzl JG, Velicky P. LIONESS enables 4D nanoscale reconstruction of living
    brain tissue. <i>Nature Methods</i>. 2023;20(8):1141-1142. doi:<a href="https://doi.org/10.1038/s41592-023-01937-5">10.1038/s41592-023-01937-5</a>
  apa: Danzl, J. G., &#38; Velicky, P. (2023). LIONESS enables 4D nanoscale reconstruction
    of living brain tissue. <i>Nature Methods</i>. Springer Nature. <a href="https://doi.org/10.1038/s41592-023-01937-5">https://doi.org/10.1038/s41592-023-01937-5</a>
  chicago: Danzl, Johann G, and Philipp Velicky. “LIONESS Enables 4D Nanoscale Reconstruction
    of Living Brain Tissue.” <i>Nature Methods</i>. Springer Nature, 2023. <a href="https://doi.org/10.1038/s41592-023-01937-5">https://doi.org/10.1038/s41592-023-01937-5</a>.
  ieee: J. G. Danzl and P. Velicky, “LIONESS enables 4D nanoscale reconstruction of
    living brain tissue,” <i>Nature Methods</i>, vol. 20, no. 8. Springer Nature,
    pp. 1141–1142, 2023.
  ista: Danzl JG, Velicky P. 2023. LIONESS enables 4D nanoscale reconstruction of
    living brain tissue. Nature Methods. 20(8), 1141–1142.
  mla: Danzl, Johann G., and Philipp Velicky. “LIONESS Enables 4D Nanoscale Reconstruction
    of Living Brain Tissue.” <i>Nature Methods</i>, vol. 20, no. 8, Springer Nature,
    2023, pp. 1141–42, doi:<a href="https://doi.org/10.1038/s41592-023-01937-5">10.1038/s41592-023-01937-5</a>.
  short: J.G. Danzl, P. Velicky, Nature Methods 20 (2023) 1141–1142.
date_created: 2024-01-10T08:07:15Z
date_published: 2023-08-01T00:00:00Z
date_updated: 2024-01-10T08:37:48Z
day: '01'
department:
- _id: JoDa
doi: 10.1038/s41592-023-01937-5
external_id:
  isi:
  - '001025621500002'
intvolume: '        20'
isi: 1
issue: '8'
keyword:
- Cell Biology
- Molecular Biology
- Biochemistry
- Biotechnology
language:
- iso: eng
month: '08'
oa_version: None
page: 1141-1142
publication: Nature Methods
publication_identifier:
  eissn:
  - 1548-7105
  issn:
  - 1548-7091
publication_status: published
publisher: Springer Nature
quality_controlled: '1'
related_material:
  record:
  - id: '13267'
    relation: extended_version
    status: public
scopus_import: '1'
status: public
title: LIONESS enables 4D nanoscale reconstruction of living brain tissue
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 20
year: '2023'
...
---
_id: '14781'
abstract:
- lang: eng
  text: Germ granules, condensates of phase-separated RNA and protein, are organelles
    that are essential for germline development in different organisms. The patterning
    of the granules and their relevance for germ cell fate are not fully understood.
    Combining three-dimensional in vivo structural and functional analyses, we study
    the dynamic spatial organization of molecules within zebrafish germ granules.
    We find that the localization of RNA molecules to the periphery of the granules,
    where ribosomes are localized, depends on translational activity at this location.
    In addition, we find that the vertebrate-specific Dead end (Dnd1) protein is essential
    for nanos3 RNA localization at the condensates’ periphery. Accordingly, in the
    absence of Dnd1, or when translation is inhibited, nanos3 RNA translocates into
    the granule interior, away from the ribosomes, a process that is correlated with
    the loss of germ cell fate. These findings highlight the relevance of sub-granule
    compartmentalization for post-transcriptional control and its importance for preserving
    germ cell totipotency.
acknowledgement: We thank Celeste Brennecka for editing and Michal Reichman-Fried
  for critical comments on the manuscript. We thank Ursula Jordan, Esther Messerschmidt,
  and Ines Sandbote for technical assistance. This work was supported by funding from
  the University of Münster (K.J.W., K.T., E.R., A.G., T.G.-T., J.S., and M.G.), the
  Max Planck Institute for Molecular Biomedicine (D.Z.), the German Research Foundation
  grant CRU 326 (P2) RA863/12-2 (E.R.), Baylor University (K.H. and D.R.), and the
  National Institutes of Health grant R35 GM 134910 (D.R.). We thank the referees
  for insightful comments that helped improve the manuscript.
article_processing_charge: No
article_type: original
author:
- first_name: Kim Joana
  full_name: Westerich, Kim Joana
  last_name: Westerich
- first_name: Katsiaryna
  full_name: Tarbashevich, Katsiaryna
  last_name: Tarbashevich
- first_name: Jan
  full_name: Schick, Jan
  last_name: Schick
- first_name: Antra
  full_name: Gupta, Antra
  last_name: Gupta
- first_name: Mingzhao
  full_name: Zhu, Mingzhao
  last_name: Zhu
- first_name: Kenneth
  full_name: Hull, Kenneth
  last_name: Hull
- first_name: Daniel
  full_name: Romo, Daniel
  last_name: Romo
- first_name: Dagmar
  full_name: Zeuschner, Dagmar
  last_name: Zeuschner
- first_name: Mohammad
  full_name: Goudarzi, Mohammad
  id: 3384113A-F248-11E8-B48F-1D18A9856A87
  last_name: Goudarzi
- first_name: Theresa
  full_name: Gross-Thebing, Theresa
  last_name: Gross-Thebing
- first_name: Erez
  full_name: Raz, Erez
  last_name: Raz
citation:
  ama: Westerich KJ, Tarbashevich K, Schick J, et al. Spatial organization and function
    of RNA molecules within phase-separated condensates in zebrafish are controlled
    by Dnd1. <i>Developmental Cell</i>. 2023;58(17):1578-1592.e5. doi:<a href="https://doi.org/10.1016/j.devcel.2023.06.009">10.1016/j.devcel.2023.06.009</a>
  apa: Westerich, K. J., Tarbashevich, K., Schick, J., Gupta, A., Zhu, M., Hull, K.,
    … Raz, E. (2023). Spatial organization and function of RNA molecules within phase-separated
    condensates in zebrafish are controlled by Dnd1. <i>Developmental Cell</i>. Elsevier.
    <a href="https://doi.org/10.1016/j.devcel.2023.06.009">https://doi.org/10.1016/j.devcel.2023.06.009</a>
  chicago: Westerich, Kim Joana, Katsiaryna Tarbashevich, Jan Schick, Antra Gupta,
    Mingzhao Zhu, Kenneth Hull, Daniel Romo, et al. “Spatial Organization and Function
    of RNA Molecules within Phase-Separated Condensates in Zebrafish Are Controlled
    by Dnd1.” <i>Developmental Cell</i>. Elsevier, 2023. <a href="https://doi.org/10.1016/j.devcel.2023.06.009">https://doi.org/10.1016/j.devcel.2023.06.009</a>.
  ieee: K. J. Westerich <i>et al.</i>, “Spatial organization and function of RNA molecules
    within phase-separated condensates in zebrafish are controlled by Dnd1,” <i>Developmental
    Cell</i>, vol. 58, no. 17. Elsevier, p. 1578–1592.e5, 2023.
  ista: Westerich KJ, Tarbashevich K, Schick J, Gupta A, Zhu M, Hull K, Romo D, Zeuschner
    D, Goudarzi M, Gross-Thebing T, Raz E. 2023. Spatial organization and function
    of RNA molecules within phase-separated condensates in zebrafish are controlled
    by Dnd1. Developmental Cell. 58(17), 1578–1592.e5.
  mla: Westerich, Kim Joana, et al. “Spatial Organization and Function of RNA Molecules
    within Phase-Separated Condensates in Zebrafish Are Controlled by Dnd1.” <i>Developmental
    Cell</i>, vol. 58, no. 17, Elsevier, 2023, p. 1578–1592.e5, doi:<a href="https://doi.org/10.1016/j.devcel.2023.06.009">10.1016/j.devcel.2023.06.009</a>.
  short: K.J. Westerich, K. Tarbashevich, J. Schick, A. Gupta, M. Zhu, K. Hull, D.
    Romo, D. Zeuschner, M. Goudarzi, T. Gross-Thebing, E. Raz, Developmental Cell
    58 (2023) 1578–1592.e5.
date_created: 2024-01-10T09:41:21Z
date_published: 2023-09-11T00:00:00Z
date_updated: 2024-01-16T08:56:36Z
day: '11'
department:
- _id: Bio
doi: 10.1016/j.devcel.2023.06.009
external_id:
  pmid:
  - '37463577'
intvolume: '        58'
issue: '17'
keyword:
- Developmental Biology
- Cell Biology
- General Biochemistry
- Genetics and Molecular Biology
- Molecular Biology
language:
- iso: eng
main_file_link:
- open_access: '1'
  url: https://www.biorxiv.org/content/10.1101/2023.07.09.548244
month: '09'
oa: 1
oa_version: Preprint
page: 1578-1592.e5
pmid: 1
publication: Developmental Cell
publication_identifier:
  issn:
  - 1534-5807
publication_status: published
publisher: Elsevier
quality_controlled: '1'
status: public
title: Spatial organization and function of RNA molecules within phase-separated condensates
  in zebrafish are controlled by Dnd1
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 58
year: '2023'
...
---
_id: '14788'
abstract:
- lang: eng
  text: "Eukaryotic cells use clathrin-mediated endocytosis to take up a large range
    of extracellular cargo. During endocytosis, a clathrin coat forms on the plasma
    membrane, but it remains controversial when and how it is remodeled into a spherical
    vesicle.\r\nHere, we use 3D superresolution microscopy to determine the precise
    geometry of the clathrin coat at large numbers of endocytic sites. Through pseudo-temporal
    sorting, we determine the average trajectory of clathrin remodeling during endocytosis.
    We find that clathrin coats assemble first on flat membranes to 50% of the coat
    area before they become rapidly and continuously bent, and this mechanism is confirmed
    in three cell lines. We introduce the cooperative curvature model, which is based
    on positive feedback for curvature generation. It accurately describes the measured
    shapes and dynamics of the clathrin coat and could represent a general mechanism
    for clathrin coat remodeling on the plasma membrane."
acknowledgement: We thank the entire Ries and Kaksonen labs for fruitful discussions
  and support. This work was supported by the European Research Council (ERC CoG-724489
  to J. Ries), the National Institutes of Health Common Fund 4D Nucleome Program (Grant
  U01 to J. Ries), the Human Frontier Science Program (RGY0065/2017 to J. Ries), the
  EMBL Interdisciplinary Postdoc Programme (EIPOD) under Marie Curie Actions COFUND
  (Grant 229597 to O. Avinoam), the European Molecular Biology Laboratory (M. Mund,
  A. Tschanz, Y.-L. Wu and J. Ries), and the Swiss National Science Foundation (grant
  310030B_182825 and NCCR Chemical Biology to M. Kaksonen). O. Avinoam is an incumbent
  of the Miriam Berman Presidential Development Chair.
article_number: e202206038
article_processing_charge: No
article_type: original
author:
- first_name: Markus
  full_name: Mund, Markus
  last_name: Mund
- first_name: Aline
  full_name: Tschanz, Aline
  last_name: Tschanz
- first_name: Yu-Le
  full_name: Wu, Yu-Le
  last_name: Wu
- first_name: Felix F
  full_name: Frey, Felix F
  id: a0270b37-8f1a-11ec-95c7-8e710c59a4f3
  last_name: Frey
  orcid: 0000-0001-8501-6017
- first_name: Johanna L.
  full_name: Mehl, Johanna L.
  last_name: Mehl
- first_name: Marko
  full_name: Kaksonen, Marko
  last_name: Kaksonen
- first_name: Ori
  full_name: Avinoam, Ori
  last_name: Avinoam
- first_name: Ulrich S.
  full_name: Schwarz, Ulrich S.
  last_name: Schwarz
- first_name: Jonas
  full_name: Ries, Jonas
  last_name: Ries
citation:
  ama: Mund M, Tschanz A, Wu Y-L, et al. Clathrin coats partially preassemble and
    subsequently bend during endocytosis. <i>Journal of Cell Biology</i>. 2023;222(3).
    doi:<a href="https://doi.org/10.1083/jcb.202206038">10.1083/jcb.202206038</a>
  apa: Mund, M., Tschanz, A., Wu, Y.-L., Frey, F. F., Mehl, J. L., Kaksonen, M., …
    Ries, J. (2023). Clathrin coats partially preassemble and subsequently bend during
    endocytosis. <i>Journal of Cell Biology</i>. Rockefeller University Press. <a
    href="https://doi.org/10.1083/jcb.202206038">https://doi.org/10.1083/jcb.202206038</a>
  chicago: Mund, Markus, Aline Tschanz, Yu-Le Wu, Felix F Frey, Johanna L. Mehl, Marko
    Kaksonen, Ori Avinoam, Ulrich S. Schwarz, and Jonas Ries. “Clathrin Coats Partially
    Preassemble and Subsequently Bend during Endocytosis.” <i>Journal of Cell Biology</i>.
    Rockefeller University Press, 2023. <a href="https://doi.org/10.1083/jcb.202206038">https://doi.org/10.1083/jcb.202206038</a>.
  ieee: M. Mund <i>et al.</i>, “Clathrin coats partially preassemble and subsequently
    bend during endocytosis,” <i>Journal of Cell Biology</i>, vol. 222, no. 3. Rockefeller
    University Press, 2023.
  ista: Mund M, Tschanz A, Wu Y-L, Frey FF, Mehl JL, Kaksonen M, Avinoam O, Schwarz
    US, Ries J. 2023. Clathrin coats partially preassemble and subsequently bend during
    endocytosis. Journal of Cell Biology. 222(3), e202206038.
  mla: Mund, Markus, et al. “Clathrin Coats Partially Preassemble and Subsequently
    Bend during Endocytosis.” <i>Journal of Cell Biology</i>, vol. 222, no. 3, e202206038,
    Rockefeller University Press, 2023, doi:<a href="https://doi.org/10.1083/jcb.202206038">10.1083/jcb.202206038</a>.
  short: M. Mund, A. Tschanz, Y.-L. Wu, F.F. Frey, J.L. Mehl, M. Kaksonen, O. Avinoam,
    U.S. Schwarz, J. Ries, Journal of Cell Biology 222 (2023).
date_created: 2024-01-10T10:45:55Z
date_published: 2023-02-03T00:00:00Z
date_updated: 2024-01-16T10:17:05Z
day: '03'
ddc:
- '570'
department:
- _id: AnSa
doi: 10.1083/jcb.202206038
external_id:
  isi:
  - '000978065000001'
  pmid:
  - '36734980'
file:
- access_level: open_access
  checksum: 505d5cac36c14b073b68c7fed1a92bd3
  content_type: application/pdf
  creator: dernst
  date_created: 2024-01-16T10:15:09Z
  date_updated: 2024-01-16T10:15:09Z
  file_id: '14811'
  file_name: 2023_JCB_Mund.pdf
  file_size: 5678069
  relation: main_file
  success: 1
file_date_updated: 2024-01-16T10:15:09Z
has_accepted_license: '1'
intvolume: '       222'
isi: 1
issue: '3'
keyword:
- Cell Biology
language:
- iso: eng
month: '02'
oa: 1
oa_version: Published Version
pmid: 1
publication: Journal of Cell Biology
publication_identifier:
  eissn:
  - 1540-8140
  issn:
  - 0021-9525
publication_status: published
publisher: Rockefeller University Press
quality_controlled: '1'
status: public
title: Clathrin coats partially preassemble and subsequently bend during endocytosis
tmp:
  image: /images/cc_by.png
  legal_code_url: https://creativecommons.org/licenses/by/4.0/legalcode
  name: Creative Commons Attribution 4.0 International Public License (CC-BY 4.0)
  short: CC BY (4.0)
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 222
year: '2023'
...
---
_id: '14827'
abstract:
- lang: eng
  text: Understanding complex living systems, which are fundamentally constrained
    by physical phenomena, requires combining experimental data with theoretical physical
    and mathematical models. To develop such models, collaborations between experimental
    cell biologists and theoreticians are increasingly important but these two groups
    often face challenges achieving mutual understanding. To help navigate these challenges,
    this Perspective discusses different modelling approaches, including bottom-up
    hypothesis-driven and top-down data-driven models, and highlights their strengths
    and applications. Using cell mechanics as an example, we explore the integration
    of specific physical models with experimental data from the molecular, cellular
    and tissue level up to multiscale input. We also emphasize the importance of constraining
    model complexity and outline strategies for crosstalk between experimental design
    and model development. Furthermore, we highlight how physical models can provide
    conceptual insights and produce unifying and generalizable frameworks for biological
    phenomena. Overall, this Perspective aims to promote fruitful collaborations that
    advance our understanding of complex biological systems.
acknowledgement: "We thank Prisca Liberali and Edouard Hannezo for many inspiring
  discussions; Mehmet Can Uçar, Nicoletta I Petridou and Qiutan Yang for a critical
  reading of the manuscript, and Claudia Flandoli for the artwork in Figs 2 and 3.
  We would also like to thank The Company of Biologists for the opportunity to attend
  the 2023 workshop on Collective Cell Migration, and all workshop participants for
  discussions.\r\nC.S. was supported by a European Molecular Biology Organization
  (EMBO) Postdoctoral Fellowship (ALTF 660-2020) and Human Frontier Science Program
  (HFSP) Postdoctoral fellowship (LT000746/2021-L). D.B.B. was supported by the NOMIS
  Foundation as a NOMIS Fellow and by an EMBO Postdoctoral Fellowship (ALTF 343-2022)."
article_number: jcs.261515
article_processing_charge: No
article_type: original
author:
- first_name: Cornelia
  full_name: Schwayer, Cornelia
  id: 3436488C-F248-11E8-B48F-1D18A9856A87
  last_name: Schwayer
  orcid: 0000-0001-5130-2226
- first_name: David
  full_name: Brückner, David
  id: e1e86031-6537-11eb-953a-f7ab92be508d
  last_name: Brückner
  orcid: 0000-0001-7205-2975
citation:
  ama: Schwayer C, Brückner D. Connecting theory and experiment in cell and tissue
    mechanics. <i>Journal of Cell Science</i>. 2023;136(24). doi:<a href="https://doi.org/10.1242/jcs.261515">10.1242/jcs.261515</a>
  apa: Schwayer, C., &#38; Brückner, D. (2023). Connecting theory and experiment in
    cell and tissue mechanics. <i>Journal of Cell Science</i>. The Company of Biologists.
    <a href="https://doi.org/10.1242/jcs.261515">https://doi.org/10.1242/jcs.261515</a>
  chicago: Schwayer, Cornelia, and David Brückner. “Connecting Theory and Experiment
    in Cell and Tissue Mechanics.” <i>Journal of Cell Science</i>. The Company of
    Biologists, 2023. <a href="https://doi.org/10.1242/jcs.261515">https://doi.org/10.1242/jcs.261515</a>.
  ieee: C. Schwayer and D. Brückner, “Connecting theory and experiment in cell and
    tissue mechanics,” <i>Journal of Cell Science</i>, vol. 136, no. 24. The Company
    of Biologists, 2023.
  ista: Schwayer C, Brückner D. 2023. Connecting theory and experiment in cell and
    tissue mechanics. Journal of Cell Science. 136(24), jcs. 261515.
  mla: Schwayer, Cornelia, and David Brückner. “Connecting Theory and Experiment in
    Cell and Tissue Mechanics.” <i>Journal of Cell Science</i>, vol. 136, no. 24,
    jcs. 261515, The Company of Biologists, 2023, doi:<a href="https://doi.org/10.1242/jcs.261515">10.1242/jcs.261515</a>.
  short: C. Schwayer, D. Brückner, Journal of Cell Science 136 (2023).
date_created: 2024-01-17T12:46:55Z
date_published: 2023-12-27T00:00:00Z
date_updated: 2024-01-22T13:35:48Z
day: '27'
department:
- _id: EdHa
- _id: CaHe
doi: 10.1242/jcs.261515
external_id:
  pmid:
  - '38149871'
intvolume: '       136'
issue: '24'
keyword:
- Cell Biology
language:
- iso: eng
month: '12'
oa_version: None
pmid: 1
project:
- _id: 34e2a5b5-11ca-11ed-8bc3-b2265616ef0b
  grant_number: 343-2022
  name: A mechano-chemical theory for stem cell fate decisions in organoid development
publication: Journal of Cell Science
publication_identifier:
  eissn:
  - 1477-9137
  issn:
  - 0021-9533
publication_status: published
publisher: The Company of Biologists
quality_controlled: '1'
scopus_import: '1'
status: public
title: Connecting theory and experiment in cell and tissue mechanics
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 136
year: '2023'
...
---
_id: '12162'
abstract:
- lang: eng
  text: Homeostatic balance in the intestinal epithelium relies on a fast cellular
    turnover, which is coordinated by an intricate interplay between biochemical signalling,
    mechanical forces and organ geometry. We review recent modelling approaches that
    have been developed to understand different facets of this remarkable homeostatic
    equilibrium. Existing models offer different, albeit complementary, perspectives
    on the problem. First, biomechanical models aim to explain the local and global
    mechanical stresses driving cell renewal as well as tissue shape maintenance.
    Second, compartmental models provide insights into the conditions necessary to
    keep a constant flow of cells with well-defined ratios of cell types, and how
    perturbations can lead to an unbalance of relative compartment sizes. A third
    family of models address, at the cellular level, the nature and regulation of
    stem fate choices that are necessary to fuel cellular turnover. We also review
    how these different approaches are starting to be integrated together across scales,
    to provide quantitative predictions and new conceptual frameworks to think about
    the dynamics of cell renewal in complex tissues.
acknowledgement: "This work received funding from the ERC under the European Union’s
  Horizon 2020 research and innovation programme (grant agreement No. 851288 to E.H.).\r\nB.
  C-M wants to acknowledge the support of the field of excellence Complexity of Life,
  in Basic Research and Innovation of the University of Graz."
article_processing_charge: Yes (via OA deal)
article_type: review
author:
- first_name: Bernat
  full_name: Corominas-Murtra, Bernat
  id: 43BE2298-F248-11E8-B48F-1D18A9856A87
  last_name: Corominas-Murtra
  orcid: 0000-0001-9806-5643
- first_name: Edouard B
  full_name: Hannezo, Edouard B
  id: 3A9DB764-F248-11E8-B48F-1D18A9856A87
  last_name: Hannezo
  orcid: 0000-0001-6005-1561
citation:
  ama: Corominas-Murtra B, Hannezo EB. Modelling the dynamics of mammalian gut homeostasis.
    <i>Seminars in Cell &#38; Developmental Biology</i>. 2023;150-151:58-65. doi:<a
    href="https://doi.org/10.1016/j.semcdb.2022.11.005">10.1016/j.semcdb.2022.11.005</a>
  apa: Corominas-Murtra, B., &#38; Hannezo, E. B. (2023). Modelling the dynamics of
    mammalian gut homeostasis. <i>Seminars in Cell &#38; Developmental Biology</i>.
    Elsevier. <a href="https://doi.org/10.1016/j.semcdb.2022.11.005">https://doi.org/10.1016/j.semcdb.2022.11.005</a>
  chicago: Corominas-Murtra, Bernat, and Edouard B Hannezo. “Modelling the Dynamics
    of Mammalian Gut Homeostasis.” <i>Seminars in Cell &#38; Developmental Biology</i>.
    Elsevier, 2023. <a href="https://doi.org/10.1016/j.semcdb.2022.11.005">https://doi.org/10.1016/j.semcdb.2022.11.005</a>.
  ieee: B. Corominas-Murtra and E. B. Hannezo, “Modelling the dynamics of mammalian
    gut homeostasis,” <i>Seminars in Cell &#38; Developmental Biology</i>, vol. 150–151.
    Elsevier, pp. 58–65, 2023.
  ista: Corominas-Murtra B, Hannezo EB. 2023. Modelling the dynamics of mammalian
    gut homeostasis. Seminars in Cell &#38; Developmental Biology. 150–151, 58–65.
  mla: Corominas-Murtra, Bernat, and Edouard B. Hannezo. “Modelling the Dynamics of
    Mammalian Gut Homeostasis.” <i>Seminars in Cell &#38; Developmental Biology</i>,
    vol. 150–151, Elsevier, 2023, pp. 58–65, doi:<a href="https://doi.org/10.1016/j.semcdb.2022.11.005">10.1016/j.semcdb.2022.11.005</a>.
  short: B. Corominas-Murtra, E.B. Hannezo, Seminars in Cell &#38; Developmental Biology
    150–151 (2023) 58–65.
date_created: 2023-01-12T12:09:47Z
date_published: 2023-12-02T00:00:00Z
date_updated: 2024-01-16T13:22:32Z
day: '02'
ddc:
- '570'
department:
- _id: EdHa
doi: 10.1016/j.semcdb.2022.11.005
ec_funded: 1
external_id:
  isi:
  - '001053522200001'
  pmid:
  - '36470715'
file:
- access_level: open_access
  checksum: c619887cf130f4649bf3035417186004
  content_type: application/pdf
  creator: dernst
  date_created: 2024-01-08T10:16:04Z
  date_updated: 2024-01-08T10:16:04Z
  file_id: '14741'
  file_name: 2023_SeminarsCellDevBiology_CorominasMurtra.pdf
  file_size: 1343750
  relation: main_file
  success: 1
file_date_updated: 2024-01-08T10:16:04Z
has_accepted_license: '1'
isi: 1
keyword:
- Cell Biology
- Developmental Biology
language:
- iso: eng
month: '12'
oa: 1
oa_version: Published Version
page: 58-65
pmid: 1
project:
- _id: 05943252-7A3F-11EA-A408-12923DDC885E
  call_identifier: H2020
  grant_number: '851288'
  name: Design Principles of Branching Morphogenesis
publication: Seminars in Cell & Developmental Biology
publication_identifier:
  issn:
  - 1084-9521
publication_status: published
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: Modelling the dynamics of mammalian gut homeostasis
tmp:
  image: /images/cc_by.png
  legal_code_url: https://creativecommons.org/licenses/by/4.0/legalcode
  name: Creative Commons Attribution 4.0 International Public License (CC-BY 4.0)
  short: CC BY (4.0)
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 150-151
year: '2023'
...
---
_id: '12163'
abstract:
- lang: eng
  text: Small GTPases play essential roles in the organization of eukaryotic cells.
    In recent years, it has become clear that their intracellular functions result
    from intricate biochemical networks of the GTPase and their regulators that dynamically
    bind to a membrane surface. Due to the inherent complexities of their interactions,
    however, revealing the underlying mechanisms of action is often difficult to achieve
    from in vivo studies. This review summarizes in vitro reconstitution approaches
    developed to obtain a better mechanistic understanding of how small GTPase activities
    are regulated in space and time.
acknowledgement: The authors acknowledge support from IST Austria and helpful comments
  from the anonymous reviewers that helped to improve this manuscript. We apologize
  to the authors of primary literature and outstanding research not cited here due
  to space restraints.
article_processing_charge: Yes (via OA deal)
article_type: review
author:
- first_name: Martin
  full_name: Loose, Martin
  id: 462D4284-F248-11E8-B48F-1D18A9856A87
  last_name: Loose
  orcid: 0000-0001-7309-9724
- first_name: Albert
  full_name: Auer, Albert
  id: 3018E8C2-F248-11E8-B48F-1D18A9856A87
  last_name: Auer
  orcid: 0000-0002-3580-2906
- first_name: Gabriel
  full_name: Brognara, Gabriel
  id: D96FFDA0-A884-11E9-9968-DC26E6697425
  last_name: Brognara
- first_name: Hanifatul R
  full_name: Budiman, Hanifatul R
  id: 55380f95-15b2-11ec-abd3-aff8e230696b
  last_name: Budiman
- first_name: Lukasz M
  full_name: Kowalski, Lukasz M
  id: e3a512e2-4bbe-11eb-a68a-e3857a7844c2
  last_name: Kowalski
- first_name: Ivana
  full_name: Matijevic, Ivana
  id: 83c17ce3-15b2-11ec-abd3-f486545870bd
  last_name: Matijevic
citation:
  ama: Loose M, Auer A, Brognara G, Budiman HR, Kowalski LM, Matijevic I. In vitro
    reconstitution of small GTPase regulation. <i>FEBS Letters</i>. 2023;597(6):762-777.
    doi:<a href="https://doi.org/10.1002/1873-3468.14540">10.1002/1873-3468.14540</a>
  apa: Loose, M., Auer, A., Brognara, G., Budiman, H. R., Kowalski, L. M., &#38; Matijevic,
    I. (2023). In vitro reconstitution of small GTPase regulation. <i>FEBS Letters</i>.
    Wiley. <a href="https://doi.org/10.1002/1873-3468.14540">https://doi.org/10.1002/1873-3468.14540</a>
  chicago: Loose, Martin, Albert Auer, Gabriel Brognara, Hanifatul R Budiman, Lukasz
    M Kowalski, and Ivana Matijevic. “In Vitro Reconstitution of Small GTPase Regulation.”
    <i>FEBS Letters</i>. Wiley, 2023. <a href="https://doi.org/10.1002/1873-3468.14540">https://doi.org/10.1002/1873-3468.14540</a>.
  ieee: M. Loose, A. Auer, G. Brognara, H. R. Budiman, L. M. Kowalski, and I. Matijevic,
    “In vitro reconstitution of small GTPase regulation,” <i>FEBS Letters</i>, vol.
    597, no. 6. Wiley, pp. 762–777, 2023.
  ista: Loose M, Auer A, Brognara G, Budiman HR, Kowalski LM, Matijevic I. 2023. In
    vitro reconstitution of small GTPase regulation. FEBS Letters. 597(6), 762–777.
  mla: Loose, Martin, et al. “In Vitro Reconstitution of Small GTPase Regulation.”
    <i>FEBS Letters</i>, vol. 597, no. 6, Wiley, 2023, pp. 762–77, doi:<a href="https://doi.org/10.1002/1873-3468.14540">10.1002/1873-3468.14540</a>.
  short: M. Loose, A. Auer, G. Brognara, H.R. Budiman, L.M. Kowalski, I. Matijevic,
    FEBS Letters 597 (2023) 762–777.
date_created: 2023-01-12T12:09:58Z
date_published: 2023-03-01T00:00:00Z
date_updated: 2023-08-16T08:32:29Z
day: '01'
ddc:
- '570'
department:
- _id: MaLo
doi: 10.1002/1873-3468.14540
external_id:
  isi:
  - '000891573000001'
  pmid:
  - '36448231'
file:
- access_level: open_access
  checksum: 7492244d3f9c5faa1347ef03f6e5bc84
  content_type: application/pdf
  creator: dernst
  date_created: 2023-08-16T08:31:04Z
  date_updated: 2023-08-16T08:31:04Z
  file_id: '14063'
  file_name: 2023_FEBSLetters_Loose.pdf
  file_size: 3148143
  relation: main_file
  success: 1
file_date_updated: 2023-08-16T08:31:04Z
has_accepted_license: '1'
intvolume: '       597'
isi: 1
issue: '6'
keyword:
- Cell Biology
- Genetics
- Molecular Biology
- Biochemistry
- Structural Biology
- Biophysics
language:
- iso: eng
month: '03'
oa: 1
oa_version: Published Version
page: 762-777
pmid: 1
publication: FEBS Letters
publication_identifier:
  eissn:
  - 1873-3468
  issn:
  - 0014-5793
publication_status: published
publisher: Wiley
quality_controlled: '1'
scopus_import: '1'
status: public
title: In vitro reconstitution of small GTPase regulation
tmp:
  image: /images/cc_by_nc_nd.png
  legal_code_url: https://creativecommons.org/licenses/by-nc-nd/4.0/legalcode
  name: Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International
    (CC BY-NC-ND 4.0)
  short: CC BY-NC-ND (4.0)
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 597
year: '2023'
...
---
_id: '12669'
abstract:
- lang: eng
  text: The study of RNAs has become one of the most influential research fields in
    contemporary biology and biomedicine. In the last few years, new sequencing technologies
    have produced an explosion of new and exciting discoveries in the field but have
    also given rise to many open questions. Defining these questions, together with
    old, long-standing gaps in our knowledge, is the spirit of this article. The breadth
    of topics within RNA biology research is vast, and every aspect of the biology
    of these molecules contains countless exciting open questions. Here, we asked
    12 groups to discuss their most compelling question among some plant RNA biology
    topics. The following vignettes cover RNA alternative splicing; RNA dynamics;
    RNA translation; RNA structures; R-loops; epitranscriptomics; long non-coding
    RNAs; small RNA production and their functions in crops; small RNAs during gametogenesis
    and in cross-kingdom RNA interference; and RNA-directed DNA methylation. In each
    section, we will present the current state-of-the-art in plant RNA biology research
    before asking the questions that will surely motivate future discoveries in the
    field. We hope this article will spark a debate about the future perspective on
    RNA biology and provoke novel reflections in the reader.
article_number: koac346
article_processing_charge: No
article_type: original
author:
- first_name: Pablo A
  full_name: Manavella, Pablo A
  last_name: Manavella
- first_name: Micaela A
  full_name: Godoy Herz, Micaela A
  last_name: Godoy Herz
- first_name: Alberto R
  full_name: Kornblihtt, Alberto R
  last_name: Kornblihtt
- first_name: Reed
  full_name: Sorenson, Reed
  last_name: Sorenson
- first_name: Leslie E
  full_name: Sieburth, Leslie E
  last_name: Sieburth
- first_name: Kentaro
  full_name: Nakaminami, Kentaro
  last_name: Nakaminami
- first_name: Motoaki
  full_name: Seki, Motoaki
  last_name: Seki
- first_name: Yiliang
  full_name: Ding, Yiliang
  last_name: Ding
- first_name: Qianwen
  full_name: Sun, Qianwen
  last_name: Sun
- first_name: Hunseung
  full_name: Kang, Hunseung
  last_name: Kang
- first_name: Federico D
  full_name: Ariel, Federico D
  last_name: Ariel
- first_name: Martin
  full_name: Crespi, Martin
  last_name: Crespi
- first_name: Axel J
  full_name: Giudicatti, Axel J
  last_name: Giudicatti
- first_name: Qiang
  full_name: Cai, Qiang
  last_name: Cai
- first_name: Hailing
  full_name: Jin, Hailing
  last_name: Jin
- first_name: Xiaoqi
  full_name: Feng, Xiaoqi
  id: e0164712-22ee-11ed-b12a-d80fcdf35958
  last_name: Feng
  orcid: 0000-0002-4008-1234
- first_name: Yijun
  full_name: Qi, Yijun
  last_name: Qi
- first_name: Craig S
  full_name: Pikaard, Craig S
  last_name: Pikaard
citation:
  ama: 'Manavella PA, Godoy Herz MA, Kornblihtt AR, et al. Beyond transcription: compelling
    open questions in plant RNA biology. <i>The Plant Cell</i>. 2023;35(6). doi:<a
    href="https://doi.org/10.1093/plcell/koac346">10.1093/plcell/koac346</a>'
  apa: 'Manavella, P. A., Godoy Herz, M. A., Kornblihtt, A. R., Sorenson, R., Sieburth,
    L. E., Nakaminami, K., … Pikaard, C. S. (2023). Beyond transcription: compelling
    open questions in plant RNA biology. <i>The Plant Cell</i>. Oxford University
    Press. <a href="https://doi.org/10.1093/plcell/koac346">https://doi.org/10.1093/plcell/koac346</a>'
  chicago: 'Manavella, Pablo A, Micaela A Godoy Herz, Alberto R Kornblihtt, Reed Sorenson,
    Leslie E Sieburth, Kentaro Nakaminami, Motoaki Seki, et al. “Beyond Transcription:
    Compelling Open Questions in Plant RNA Biology.” <i>The Plant Cell</i>. Oxford
    University Press, 2023. <a href="https://doi.org/10.1093/plcell/koac346">https://doi.org/10.1093/plcell/koac346</a>.'
  ieee: 'P. A. Manavella <i>et al.</i>, “Beyond transcription: compelling open questions
    in plant RNA biology,” <i>The Plant Cell</i>, vol. 35, no. 6. Oxford University
    Press, 2023.'
  ista: 'Manavella PA, Godoy Herz MA, Kornblihtt AR, Sorenson R, Sieburth LE, Nakaminami
    K, Seki M, Ding Y, Sun Q, Kang H, Ariel FD, Crespi M, Giudicatti AJ, Cai Q, Jin
    H, Feng X, Qi Y, Pikaard CS. 2023. Beyond transcription: compelling open questions
    in plant RNA biology. The Plant Cell. 35(6), koac346.'
  mla: 'Manavella, Pablo A., et al. “Beyond Transcription: Compelling Open Questions
    in Plant RNA Biology.” <i>The Plant Cell</i>, vol. 35, no. 6, koac346, Oxford
    University Press, 2023, doi:<a href="https://doi.org/10.1093/plcell/koac346">10.1093/plcell/koac346</a>.'
  short: P.A. Manavella, M.A. Godoy Herz, A.R. Kornblihtt, R. Sorenson, L.E. Sieburth,
    K. Nakaminami, M. Seki, Y. Ding, Q. Sun, H. Kang, F.D. Ariel, M. Crespi, A.J.
    Giudicatti, Q. Cai, H. Jin, X. Feng, Y. Qi, C.S. Pikaard, The Plant Cell 35 (2023).
date_created: 2023-02-23T09:14:59Z
date_published: 2023-06-01T00:00:00Z
date_updated: 2023-10-04T09:48:43Z
day: '01'
department:
- _id: XiFe
doi: 10.1093/plcell/koac346
extern: '1'
external_id:
  pmid:
  - '36477566'
intvolume: '        35'
issue: '6'
keyword:
- Cell Biology
- Plant Science
language:
- iso: eng
main_file_link:
- open_access: '1'
  url: https://doi.org/10.1093/plcell/koac346
month: '06'
oa: 1
oa_version: Published Version
pmid: 1
publication: The Plant Cell
publication_identifier:
  eissn:
  - 1532-298X
  issn:
  - 1040-4651
publication_status: published
publisher: Oxford University Press
quality_controlled: '1'
scopus_import: '1'
status: public
title: 'Beyond transcription: compelling open questions in plant RNA biology'
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 35
year: '2023'
...
---
_id: '12747'
abstract:
- lang: eng
  text: Muscle degeneration is the most prevalent cause for frailty and dependency
    in inherited diseases and ageing. Elucidation of pathophysiological mechanisms,
    as well as effective treatments for muscle diseases, represents an important goal
    in improving human health. Here, we show that the lipid synthesis enzyme phosphatidylethanolamine
    cytidyltransferase (PCYT2/ECT) is critical to muscle health. Human deficiency
    in PCYT2 causes a severe disease with failure to thrive and progressive weakness.
    pcyt2-mutant zebrafish and muscle-specific Pcyt2-knockout mice recapitulate the
    participant phenotypes, with failure to thrive, progressive muscle weakness and
    accelerated ageing. Mechanistically, muscle Pcyt2 deficiency affects cellular
    bioenergetics and membrane lipid bilayer structure and stability. PCYT2 activity
    declines in ageing muscles of mice and humans, and adeno-associated virus-based
    delivery of PCYT2 ameliorates muscle weakness in Pcyt2-knockout and old mice,
    offering a therapy for individuals with a rare disease and muscle ageing. Thus,
    PCYT2 plays a fundamental and conserved role in vertebrate muscle health, linking
    PCYT2 and PCYT2-synthesized lipids to severe muscle dystrophy and ageing.
acknowledgement: 'The authors thank the participants and their families for participating
  in the study. We thank all members of our laboratories for helpful discussions.
  We are grateful to Vienna BioCenter Core Facilities: Mouse Phenotyping Unit, Histopathology
  Unit, Bioinformatics Unit, BioOptics Unit, Electron Microscopy Unit and Comparative
  Medicine Unit. We are grateful to the Lipidomics Facility, and K. Klavins and T.
  Hannich at the CeMM Research Center for Molecular Medicine of the Austrian Academy
  of Sciences for assistance with lipidomics analysis. We also thank T. Huan and A.
  Hui (UBC Vancouver) for mouse tissue and mitochondria lipidomics analysis. We thank
  A. Klymchenko (Laboratoire de Bioimagerie et Pathologies Université de Strasbourg,
  Strasbourg, France) for providing the NR12S probe. We are thankful to the Sen. Paul
  D. Wellstone Muscular Dystrophy Cooperative Specialized Research Center Viral Vector
  Core Facility for AAV6 production. We also thank K. P. Campbell and M. E. Anderson
  (University of Iowa, Carver College of Medicine) for advice on muscle tissue handling.
  We thank A. Al-Qassabi from the Sultan Qaboos University for the clinical assessment
  of the participants. D.C. and J.M.P. are supported by the Austrian Federal Ministry
  of Education, Science and Research, the Austrian Academy of Sciences, and the City
  of Vienna, and grants from the Austrian Science Fund (FWF) Wittgenstein award (Z
  271-B19), the T. von Zastrow Foundation, and a Canada 150 Research Chairs Program
  (F18-01336). J.S.C. is supported by grants RO1AR44533 and P50AR065139 from the US
  National Institutes of Health. C.K. is supported by a grant from the Agence Nationale
  de la Recherche (ANR-18-CE14-0007-01). A.V.K. is supported by European Union’s Horizon
  2020 research and innovation programme under the Marie Skłodowska-Curie grant agreement
  no. 67544, and an Austrian Science Fund (FWF; no P-33799). A.W. is supported by
  Austrian Research Promotion Agency (FFG) project no 867674. E.S. is supported by
  a SciLifeLab fellowship and Karolinska Institutet Foundation Grants. Work in the
  laboratory of G.S.-F. is supported by the Austrian Academy of Sciences, the European
  Research Council (ERC AdG 695214 GameofGates) and the Innovative Medicines Initiative
  2 Joint Undertaking (grant agreement no. 777372, ReSOLUTE). S.B., M.L. and R.Y.
  acknowledge the support of the Spastic Paraplegia Foundation.'
article_processing_charge: No
article_type: original
author:
- first_name: Domagoj
  full_name: Cikes, Domagoj
  last_name: Cikes
- first_name: Kareem
  full_name: Elsayad, Kareem
  last_name: Elsayad
- first_name: Erdinc
  full_name: Sezgin, Erdinc
  last_name: Sezgin
- first_name: Erika
  full_name: Koitai, Erika
  last_name: Koitai
- first_name: Torma
  full_name: Ferenc, Torma
  last_name: Ferenc
- first_name: Michael
  full_name: Orthofer, Michael
  last_name: Orthofer
- first_name: Rebecca
  full_name: Yarwood, Rebecca
  last_name: Yarwood
- first_name: Leonhard X.
  full_name: Heinz, Leonhard X.
  last_name: Heinz
- first_name: Vitaly
  full_name: Sedlyarov, Vitaly
  last_name: Sedlyarov
- first_name: Nasser
  full_name: Darwish-Miranda, Nasser
  id: 39CD9926-F248-11E8-B48F-1D18A9856A87
  last_name: Darwish-Miranda
  orcid: 0000-0002-8821-8236
- first_name: Adrian
  full_name: Taylor, Adrian
  last_name: Taylor
- first_name: Sophie
  full_name: Grapentine, Sophie
  last_name: Grapentine
- first_name: Fathiya
  full_name: al-Murshedi, Fathiya
  last_name: al-Murshedi
- first_name: Anne
  full_name: Abot, Anne
  last_name: Abot
- first_name: Adelheid
  full_name: Weidinger, Adelheid
  last_name: Weidinger
- first_name: Candice
  full_name: Kutchukian, Candice
  last_name: Kutchukian
- first_name: Colline
  full_name: Sanchez, Colline
  last_name: Sanchez
- first_name: Shane J. F.
  full_name: Cronin, Shane J. F.
  last_name: Cronin
- first_name: Maria
  full_name: Novatchkova, Maria
  last_name: Novatchkova
- first_name: Anoop
  full_name: Kavirayani, Anoop
  last_name: Kavirayani
- first_name: Thomas
  full_name: Schuetz, Thomas
  last_name: Schuetz
- first_name: Bernhard
  full_name: Haubner, Bernhard
  last_name: Haubner
- first_name: Lisa
  full_name: Haas, Lisa
  last_name: Haas
- first_name: Astrid
  full_name: Hagelkruys, Astrid
  last_name: Hagelkruys
- first_name: Suzanne
  full_name: Jackowski, Suzanne
  last_name: Jackowski
- first_name: Andrey
  full_name: Kozlov, Andrey
  last_name: Kozlov
- first_name: Vincent
  full_name: Jacquemond, Vincent
  last_name: Jacquemond
- first_name: Claude
  full_name: Knauf, Claude
  last_name: Knauf
- first_name: Giulio
  full_name: Superti-Furga, Giulio
  last_name: Superti-Furga
- first_name: Eric
  full_name: Rullman, Eric
  last_name: Rullman
- first_name: Thomas
  full_name: Gustafsson, Thomas
  last_name: Gustafsson
- first_name: John
  full_name: McDermot, John
  last_name: McDermot
- first_name: Martin
  full_name: Lowe, Martin
  last_name: Lowe
- first_name: Zsolt
  full_name: Radak, Zsolt
  last_name: Radak
- first_name: Jeffrey S.
  full_name: Chamberlain, Jeffrey S.
  last_name: Chamberlain
- first_name: Marica
  full_name: Bakovic, Marica
  last_name: Bakovic
- first_name: Siddharth
  full_name: Banka, Siddharth
  last_name: Banka
- first_name: Josef M.
  full_name: Penninger, Josef M.
  last_name: Penninger
citation:
  ama: Cikes D, Elsayad K, Sezgin E, et al. PCYT2-regulated lipid biosynthesis is
    critical to muscle health and ageing. <i>Nature Metabolism</i>. 2023;5:495-515.
    doi:<a href="https://doi.org/10.1038/s42255-023-00766-2">10.1038/s42255-023-00766-2</a>
  apa: Cikes, D., Elsayad, K., Sezgin, E., Koitai, E., Ferenc, T., Orthofer, M., …
    Penninger, J. M. (2023). PCYT2-regulated lipid biosynthesis is critical to muscle
    health and ageing. <i>Nature Metabolism</i>. Springer Nature. <a href="https://doi.org/10.1038/s42255-023-00766-2">https://doi.org/10.1038/s42255-023-00766-2</a>
  chicago: Cikes, Domagoj, Kareem Elsayad, Erdinc Sezgin, Erika Koitai, Torma Ferenc,
    Michael Orthofer, Rebecca Yarwood, et al. “PCYT2-Regulated Lipid Biosynthesis
    Is Critical to Muscle Health and Ageing.” <i>Nature Metabolism</i>. Springer Nature,
    2023. <a href="https://doi.org/10.1038/s42255-023-00766-2">https://doi.org/10.1038/s42255-023-00766-2</a>.
  ieee: D. Cikes <i>et al.</i>, “PCYT2-regulated lipid biosynthesis is critical to
    muscle health and ageing,” <i>Nature Metabolism</i>, vol. 5. Springer Nature,
    pp. 495–515, 2023.
  ista: Cikes D, Elsayad K, Sezgin E, Koitai E, Ferenc T, Orthofer M, Yarwood R, Heinz
    LX, Sedlyarov V, Darwish-Miranda N, Taylor A, Grapentine S, al-Murshedi F, Abot
    A, Weidinger A, Kutchukian C, Sanchez C, Cronin SJF, Novatchkova M, Kavirayani
    A, Schuetz T, Haubner B, Haas L, Hagelkruys A, Jackowski S, Kozlov A, Jacquemond
    V, Knauf C, Superti-Furga G, Rullman E, Gustafsson T, McDermot J, Lowe M, Radak
    Z, Chamberlain JS, Bakovic M, Banka S, Penninger JM. 2023. PCYT2-regulated lipid
    biosynthesis is critical to muscle health and ageing. Nature Metabolism. 5, 495–515.
  mla: Cikes, Domagoj, et al. “PCYT2-Regulated Lipid Biosynthesis Is Critical to Muscle
    Health and Ageing.” <i>Nature Metabolism</i>, vol. 5, Springer Nature, 2023, pp.
    495–515, doi:<a href="https://doi.org/10.1038/s42255-023-00766-2">10.1038/s42255-023-00766-2</a>.
  short: D. Cikes, K. Elsayad, E. Sezgin, E. Koitai, T. Ferenc, M. Orthofer, R. Yarwood,
    L.X. Heinz, V. Sedlyarov, N. Darwish-Miranda, A. Taylor, S. Grapentine, F. al-Murshedi,
    A. Abot, A. Weidinger, C. Kutchukian, C. Sanchez, S.J.F. Cronin, M. Novatchkova,
    A. Kavirayani, T. Schuetz, B. Haubner, L. Haas, A. Hagelkruys, S. Jackowski, A.
    Kozlov, V. Jacquemond, C. Knauf, G. Superti-Furga, E. Rullman, T. Gustafsson,
    J. McDermot, M. Lowe, Z. Radak, J.S. Chamberlain, M. Bakovic, S. Banka, J.M. Penninger,
    Nature Metabolism 5 (2023) 495–515.
date_created: 2023-03-23T12:58:43Z
date_published: 2023-03-20T00:00:00Z
date_updated: 2023-11-28T07:31:33Z
day: '20'
department:
- _id: Bio
doi: 10.1038/s42255-023-00766-2
external_id:
  isi:
  - '000992064000002'
  pmid:
  - '36941451'
intvolume: '         5'
isi: 1
keyword:
- Cell Biology
- Physiology (medical)
- Endocrinology
- Diabetes and Metabolism
- Internal Medicine
language:
- iso: eng
main_file_link:
- open_access: '1'
  url: https://doi.org/10.1101/2022.03.02.482658
month: '03'
oa: 1
oa_version: Preprint
page: 495-515
pmid: 1
publication: Nature Metabolism
publication_identifier:
  issn:
  - 2522-5812
publication_status: published
publisher: Springer Nature
quality_controlled: '1'
related_material:
  link:
  - relation: erratum
    url: https://doi.org/10.1038/s42255-023-00791-1
scopus_import: '1'
status: public
title: PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 5
year: '2023'
...
---
_id: '11051'
abstract:
- lang: eng
  text: Nuclear pore complexes (NPCs) bridge the nucleus and the cytoplasm and are
    indispensable for crucial cellular activities, such as bidirectional molecular
    trafficking and gene transcription regulation. The discovery of long-lived proteins
    (LLPs) in NPCs from postmitotic cells raises the exciting possibility that the
    maintenance of NPC integrity might play an inherent role in lifelong cell function.
    Age-dependent deterioration of NPCs and loss of nuclear integrity have been linked
    to age-related decline in postmitotic cell function and degenerative diseases.
    In this review, we discuss our current understanding of NPC maintenance in proliferating
    and postmitotic cells, and how malfunction of nucleoporins (Nups) might contribute
    to the pathogenesis of various neurodegenerative and cardiovascular diseases.
article_processing_charge: No
article_type: review
author:
- first_name: Jinqiang
  full_name: Liu, Jinqiang
  last_name: Liu
- first_name: Martin W
  full_name: HETZER, Martin W
  id: 86c0d31b-b4eb-11ec-ac5a-eae7b2e135ed
  last_name: HETZER
  orcid: 0000-0002-2111-992X
citation:
  ama: Liu J, Hetzer M. Nuclear pore complex maintenance and implications for age-related
    diseases. <i>Trends in Cell Biology</i>. 2022;32(3):P216-227. doi:<a href="https://doi.org/10.1016/j.tcb.2021.10.001">10.1016/j.tcb.2021.10.001</a>
  apa: Liu, J., &#38; Hetzer, M. (2022). Nuclear pore complex maintenance and implications
    for age-related diseases. <i>Trends in Cell Biology</i>. Elsevier. <a href="https://doi.org/10.1016/j.tcb.2021.10.001">https://doi.org/10.1016/j.tcb.2021.10.001</a>
  chicago: Liu, Jinqiang, and Martin Hetzer. “Nuclear Pore Complex Maintenance and
    Implications for Age-Related Diseases.” <i>Trends in Cell Biology</i>. Elsevier,
    2022. <a href="https://doi.org/10.1016/j.tcb.2021.10.001">https://doi.org/10.1016/j.tcb.2021.10.001</a>.
  ieee: J. Liu and M. Hetzer, “Nuclear pore complex maintenance and implications for
    age-related diseases,” <i>Trends in Cell Biology</i>, vol. 32, no. 3. Elsevier,
    pp. P216-227, 2022.
  ista: Liu J, Hetzer M. 2022. Nuclear pore complex maintenance and implications for
    age-related diseases. Trends in Cell Biology. 32(3), P216-227.
  mla: Liu, Jinqiang, and Martin Hetzer. “Nuclear Pore Complex Maintenance and Implications
    for Age-Related Diseases.” <i>Trends in Cell Biology</i>, vol. 32, no. 3, Elsevier,
    2022, pp. P216-227, doi:<a href="https://doi.org/10.1016/j.tcb.2021.10.001">10.1016/j.tcb.2021.10.001</a>.
  short: J. Liu, M. Hetzer, Trends in Cell Biology 32 (2022) P216-227.
date_created: 2022-04-07T07:43:01Z
date_published: 2022-03-01T00:00:00Z
date_updated: 2022-07-18T08:58:33Z
day: '01'
doi: 10.1016/j.tcb.2021.10.001
extern: '1'
external_id:
  pmid:
  - '34782239'
intvolume: '        32'
issue: '3'
keyword:
- Cell Biology
language:
- iso: eng
month: '03'
oa_version: None
page: P216-227
pmid: 1
publication: Trends in Cell Biology
publication_identifier:
  issn:
  - 0962-8924
publication_status: published
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: Nuclear pore complex maintenance and implications for age-related diseases
type: journal_article
user_id: 72615eeb-f1f3-11ec-aa25-d4573ddc34fd
volume: 32
year: '2022'
...
---
_id: '12120'
abstract:
- lang: eng
  text: Plant root architecture flexibly adapts to changing nitrate (NO3−) availability
    in the soil; however, the underlying molecular mechanism of this adaptive development
    remains under-studied. To explore the regulation of NO3−-mediated root growth,
    we screened for low-nitrate-resistant mutant (lonr) and identified mutants that
    were defective in the NAC transcription factor NAC075 (lonr1) as being less sensitive
    to low NO3− in terms of primary root growth. We show that NAC075 is a mobile transcription
    factor relocating from the root stele tissues to the endodermis based on NO3−
    availability. Under low-NO3− availability, the kinase CBL-interacting protein
    kinase 1 (CIPK1) is activated, and it phosphorylates NAC075, restricting its movement
    from the stele, which leads to the transcriptional regulation of downstream target
    WRKY53, consequently leading to adapted root architecture. Our work thus identifies
    an adaptive mechanism involving translocation of transcription factor based on
    nutrient availability and leading to cell-specific reprogramming of plant root
    growth.
acknowledgement: The authors are grateful to Jörg Kudla, Ying Miao, Yu Zheng, Gang
  Li, and Jun Zheng for providing published materials and to Wenkun Zhou and Caifu
  Jiang for helpful discussions. This work was supported by grants from the National
  Key Research and Development Program of China (2021YFF1000500), the National Natural
  Science Foundation of China (32170265 and 32022007), the Beijing Municipal Natural
  Science Foundation (5192011), and the Chinese Universities Scientific Fund (2022TC153).
article_processing_charge: No
article_type: original
author:
- first_name: Huixin
  full_name: Xiao, Huixin
  last_name: Xiao
- first_name: Yumei
  full_name: Hu, Yumei
  last_name: Hu
- first_name: Yaping
  full_name: Wang, Yaping
  last_name: Wang
- first_name: Jinkui
  full_name: Cheng, Jinkui
  last_name: Cheng
- first_name: Jinyi
  full_name: Wang, Jinyi
  last_name: Wang
- first_name: Guojingwei
  full_name: Chen, Guojingwei
  last_name: Chen
- first_name: Qian
  full_name: Li, Qian
  last_name: Li
- first_name: Shuwei
  full_name: Wang, Shuwei
  last_name: Wang
- first_name: Yalu
  full_name: Wang, Yalu
  last_name: Wang
- first_name: Shao-Shuai
  full_name: Wang, Shao-Shuai
  last_name: Wang
- first_name: Yi
  full_name: Wang, Yi
  last_name: Wang
- first_name: Wei
  full_name: Xuan, Wei
  last_name: Xuan
- first_name: Zhen
  full_name: Li, Zhen
  last_name: Li
- first_name: Yan
  full_name: Guo, Yan
  last_name: Guo
- first_name: Zhizhong
  full_name: Gong, Zhizhong
  last_name: Gong
- first_name: Jiří
  full_name: Friml, Jiří
  id: 4159519E-F248-11E8-B48F-1D18A9856A87
  last_name: Friml
  orcid: 0000-0002-8302-7596
- first_name: Jing
  full_name: Zhang, Jing
  last_name: Zhang
citation:
  ama: Xiao H, Hu Y, Wang Y, et al. Nitrate availability controls translocation of
    the transcription factor NAC075 for cell-type-specific reprogramming of root growth.
    <i>Developmental Cell</i>. 2022;57(23):2638-2651.e6. doi:<a href="https://doi.org/10.1016/j.devcel.2022.11.006">10.1016/j.devcel.2022.11.006</a>
  apa: Xiao, H., Hu, Y., Wang, Y., Cheng, J., Wang, J., Chen, G., … Zhang, J. (2022).
    Nitrate availability controls translocation of the transcription factor NAC075
    for cell-type-specific reprogramming of root growth. <i>Developmental Cell</i>.
    Elsevier. <a href="https://doi.org/10.1016/j.devcel.2022.11.006">https://doi.org/10.1016/j.devcel.2022.11.006</a>
  chicago: Xiao, Huixin, Yumei Hu, Yaping Wang, Jinkui Cheng, Jinyi Wang, Guojingwei
    Chen, Qian Li, et al. “Nitrate Availability Controls Translocation of the Transcription
    Factor NAC075 for Cell-Type-Specific Reprogramming of Root Growth.” <i>Developmental
    Cell</i>. Elsevier, 2022. <a href="https://doi.org/10.1016/j.devcel.2022.11.006">https://doi.org/10.1016/j.devcel.2022.11.006</a>.
  ieee: H. Xiao <i>et al.</i>, “Nitrate availability controls translocation of the
    transcription factor NAC075 for cell-type-specific reprogramming of root growth,”
    <i>Developmental Cell</i>, vol. 57, no. 23. Elsevier, p. 2638–2651.e6, 2022.
  ista: Xiao H, Hu Y, Wang Y, Cheng J, Wang J, Chen G, Li Q, Wang S, Wang Y, Wang
    S-S, Wang Y, Xuan W, Li Z, Guo Y, Gong Z, Friml J, Zhang J. 2022. Nitrate availability
    controls translocation of the transcription factor NAC075 for cell-type-specific
    reprogramming of root growth. Developmental Cell. 57(23), 2638–2651.e6.
  mla: Xiao, Huixin, et al. “Nitrate Availability Controls Translocation of the Transcription
    Factor NAC075 for Cell-Type-Specific Reprogramming of Root Growth.” <i>Developmental
    Cell</i>, vol. 57, no. 23, Elsevier, 2022, p. 2638–2651.e6, doi:<a href="https://doi.org/10.1016/j.devcel.2022.11.006">10.1016/j.devcel.2022.11.006</a>.
  short: H. Xiao, Y. Hu, Y. Wang, J. Cheng, J. Wang, G. Chen, Q. Li, S. Wang, Y. Wang,
    S.-S. Wang, Y. Wang, W. Xuan, Z. Li, Y. Guo, Z. Gong, J. Friml, J. Zhang, Developmental
    Cell 57 (2022) 2638–2651.e6.
date_created: 2023-01-12T11:57:00Z
date_published: 2022-12-05T00:00:00Z
date_updated: 2023-10-04T08:23:20Z
day: '05'
department:
- _id: JiFr
doi: 10.1016/j.devcel.2022.11.006
external_id:
  isi:
  - '000919603800005'
  pmid:
  - '36473460'
intvolume: '        57'
isi: 1
issue: '23'
keyword:
- Developmental Biology
- Cell Biology
- General Biochemistry
- Genetics and Molecular Biology
- Molecular Biology
language:
- iso: eng
month: '12'
oa_version: None
page: 2638-2651.e6
pmid: 1
publication: Developmental Cell
publication_identifier:
  issn:
  - 1534-5807
publication_status: published
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: Nitrate availability controls translocation of the transcription factor NAC075
  for cell-type-specific reprogramming of root growth
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 57
year: '2022'
...
---
_id: '12121'
abstract:
- lang: eng
  text: Autophagosomes are double-membraned vesicles that traffic harmful or unwanted
    cellular macromolecules to the vacuole for recycling. Although autophagosome biogenesis
    has been extensively studied, autophagosome maturation, i.e., delivery and fusion
    with the vacuole, remains largely unknown in plants. Here, we have identified
    an autophagy adaptor, CFS1, that directly interacts with the autophagosome marker
    ATG8 and localizes on both membranes of the autophagosome. Autophagosomes form
    normally in Arabidopsis thaliana cfs1 mutants, but their delivery to the vacuole
    is disrupted. CFS1’s function is evolutionarily conserved in plants, as it also
    localizes to the autophagosomes and plays a role in autophagic flux in the liverwort
    Marchantia polymorpha. CFS1 regulates autophagic flux by bridging autophagosomes
    with the multivesicular body-localized ESCRT-I component VPS23A, leading to the
    formation of amphisomes. Similar to CFS1-ATG8 interaction, disrupting the CFS1-VPS23A
    interaction blocks autophagic flux and renders plants sensitive to nitrogen starvation.
    Altogether, our results reveal a conserved vacuolar sorting hub that regulates
    autophagic flux in plants.
acknowledgement: "We thank Suayip Ustün, Karin Schumacher, Erika Isono, Gerd Juergens,
  Takashi Ueda, Daniel Hofius, and Liwen Jiang for sharing published materials.\r\nWe
  acknowledge funding from Austrian Academy of Sciences, Austrian Science Fund (FWF,
  P 32355, P 34944), Austrian Science Fund (FWF-SFB F79), Vienna Science and Technology\r\nFund
  (WWTF, LS17-047) to Y. Dagdas; Austrian Academy of Sciences DOC Fellowship to J.
  Zhao, Marie Curie VIP2 Fellowship to J.C. De La Concepcion and M. Clavel; Hong Kong
  Research Grant Council (GRF14121019, 14113921, AoE/M-05/12, C4002-17G) to B.-H.
  Kang. We thank Vienna Biocenter Core Facilities (VBCF) Protein Chemistry, Biooptics,
  Plant Sciences, Molecular Biology, and Protein Technologies. We thank J. Matthew
  Watson\r\nand members of the Dagdas lab for the critical reading and editing of
  the manuscript."
article_number: e202203139
article_processing_charge: No
article_type: original
author:
- first_name: Jierui
  full_name: Zhao, Jierui
  last_name: Zhao
- first_name: Mai Thu
  full_name: Bui, Mai Thu
  last_name: Bui
- first_name: Juncai
  full_name: Ma, Juncai
  last_name: Ma
- first_name: Fabian
  full_name: Künzl, Fabian
  last_name: Künzl
- first_name: Lorenzo
  full_name: Picchianti, Lorenzo
  last_name: Picchianti
- first_name: Juan Carlos
  full_name: De La Concepcion, Juan Carlos
  last_name: De La Concepcion
- first_name: Yixuan
  full_name: Chen, Yixuan
  last_name: Chen
- first_name: Sofia
  full_name: Petsangouraki, Sofia
  last_name: Petsangouraki
- first_name: Azadeh
  full_name: Mohseni, Azadeh
  last_name: Mohseni
- first_name: Marta
  full_name: García-Leon, Marta
  last_name: García-Leon
- first_name: Marta Salas
  full_name: Gomez, Marta Salas
  last_name: Gomez
- first_name: Caterina
  full_name: Giannini, Caterina
  id: e3fdddd5-f6e0-11ea-865d-ca99ee6367f4
  last_name: Giannini
- first_name: Dubois
  full_name: Gwennogan, Dubois
  last_name: Gwennogan
- first_name: Roksolana
  full_name: Kobylinska, Roksolana
  last_name: Kobylinska
- first_name: Marion
  full_name: Clavel, Marion
  last_name: Clavel
- first_name: Swen
  full_name: Schellmann, Swen
  last_name: Schellmann
- first_name: Yvon
  full_name: Jaillais, Yvon
  last_name: Jaillais
- first_name: Jiří
  full_name: Friml, Jiří
  id: 4159519E-F248-11E8-B48F-1D18A9856A87
  last_name: Friml
  orcid: 0000-0002-8302-7596
- first_name: Byung-Ho
  full_name: Kang, Byung-Ho
  last_name: Kang
- first_name: Yasin
  full_name: Dagdas, Yasin
  last_name: Dagdas
citation:
  ama: Zhao J, Bui MT, Ma J, et al. Plant autophagosomes mature into amphisomes prior
    to their delivery to the central vacuole. <i>Journal of Cell Biology</i>. 2022;221(12).
    doi:<a href="https://doi.org/10.1083/jcb.202203139">10.1083/jcb.202203139</a>
  apa: Zhao, J., Bui, M. T., Ma, J., Künzl, F., Picchianti, L., De La Concepcion,
    J. C., … Dagdas, Y. (2022). Plant autophagosomes mature into amphisomes prior
    to their delivery to the central vacuole. <i>Journal of Cell Biology</i>. Rockefeller
    University Press. <a href="https://doi.org/10.1083/jcb.202203139">https://doi.org/10.1083/jcb.202203139</a>
  chicago: Zhao, Jierui, Mai Thu Bui, Juncai Ma, Fabian Künzl, Lorenzo Picchianti,
    Juan Carlos De La Concepcion, Yixuan Chen, et al. “Plant Autophagosomes Mature
    into Amphisomes Prior to Their Delivery to the Central Vacuole.” <i>Journal of
    Cell Biology</i>. Rockefeller University Press, 2022. <a href="https://doi.org/10.1083/jcb.202203139">https://doi.org/10.1083/jcb.202203139</a>.
  ieee: J. Zhao <i>et al.</i>, “Plant autophagosomes mature into amphisomes prior
    to their delivery to the central vacuole,” <i>Journal of Cell Biology</i>, vol.
    221, no. 12. Rockefeller University Press, 2022.
  ista: Zhao J, Bui MT, Ma J, Künzl F, Picchianti L, De La Concepcion JC, Chen Y,
    Petsangouraki S, Mohseni A, García-Leon M, Gomez MS, Giannini C, Gwennogan D,
    Kobylinska R, Clavel M, Schellmann S, Jaillais Y, Friml J, Kang B-H, Dagdas Y.
    2022. Plant autophagosomes mature into amphisomes prior to their delivery to the
    central vacuole. Journal of Cell Biology. 221(12), e202203139.
  mla: Zhao, Jierui, et al. “Plant Autophagosomes Mature into Amphisomes Prior to
    Their Delivery to the Central Vacuole.” <i>Journal of Cell Biology</i>, vol. 221,
    no. 12, e202203139, Rockefeller University Press, 2022, doi:<a href="https://doi.org/10.1083/jcb.202203139">10.1083/jcb.202203139</a>.
  short: J. Zhao, M.T. Bui, J. Ma, F. Künzl, L. Picchianti, J.C. De La Concepcion,
    Y. Chen, S. Petsangouraki, A. Mohseni, M. García-Leon, M.S. Gomez, C. Giannini,
    D. Gwennogan, R. Kobylinska, M. Clavel, S. Schellmann, Y. Jaillais, J. Friml,
    B.-H. Kang, Y. Dagdas, Journal of Cell Biology 221 (2022).
date_created: 2023-01-12T11:57:10Z
date_published: 2022-12-01T00:00:00Z
date_updated: 2023-08-03T14:20:15Z
day: '01'
ddc:
- '580'
department:
- _id: JiFr
doi: 10.1083/jcb.202203139
external_id:
  isi:
  - '000932958800001'
  pmid:
  - '36260289'
file:
- access_level: open_access
  checksum: 050b5cc4b25e6b94fe3e3cbfe0f5c06b
  content_type: application/pdf
  creator: dernst
  date_created: 2023-01-23T10:30:11Z
  date_updated: 2023-01-23T10:30:11Z
  file_id: '12342'
  file_name: 2022_JCB_Zhao.pdf
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  success: 1
file_date_updated: 2023-01-23T10:30:11Z
has_accepted_license: '1'
intvolume: '       221'
isi: 1
issue: '12'
keyword:
- Cell Biology
language:
- iso: eng
month: '12'
oa: 1
oa_version: Published Version
pmid: 1
publication: Journal of Cell Biology
publication_identifier:
  eissn:
  - 1540-8140
  issn:
  - 0021-9525
publication_status: published
publisher: Rockefeller University Press
quality_controlled: '1'
scopus_import: '1'
status: public
title: Plant autophagosomes mature into amphisomes prior to their delivery to the
  central vacuole
tmp:
  image: /images/cc_by.png
  legal_code_url: https://creativecommons.org/licenses/by/4.0/legalcode
  name: Creative Commons Attribution 4.0 International Public License (CC-BY 4.0)
  short: CC BY (4.0)
type: journal_article
user_id: 4359f0d1-fa6c-11eb-b949-802e58b17ae8
volume: 221
year: '2022'
...
---
_id: '12122'
abstract:
- lang: eng
  text: Centrosomes play a crucial role during immune cell interactions and initiation
    of the immune response. In proliferating cells, centrosome numbers are tightly
    controlled and generally limited to one in G1 and two prior to mitosis. Defects
    in regulating centrosome numbers have been associated with cell transformation
    and tumorigenesis. Here, we report the emergence of extra centrosomes in leukocytes
    during immune activation. Upon antigen encounter, dendritic cells pass through
    incomplete mitosis and arrest in the subsequent G1 phase leading to tetraploid
    cells with accumulated centrosomes. In addition, cell stimulation increases expression
    of polo-like kinase 2, resulting in diploid cells with two centrosomes in G1-arrested
    cells. During cell migration, centrosomes tightly cluster and act as functional
    microtubule-organizing centers allowing for increased persistent locomotion along
    gradients of chemotactic cues. Moreover, dendritic cells with extra centrosomes
    display enhanced secretion of inflammatory cytokines and optimized T cell responses.
    Together, these results demonstrate a previously unappreciated role of extra centrosomes
    for regular cell and tissue homeostasis.
acknowledgement: "We thank Markéta Dalecká and Irena Krejzová for their support with
  FIB-SEM imaging, the Imaging Methods Core Facility at BIOCEV supported by the Ministry
  of Education, Youth and Sports Czech Republic (Large RI Project LM2018129 Czech-BioImaging),
  and European Regional Development Fund (project No. CZ.02.1.01/0.0/0.0/18_046/0016045)
  for their support with obtaining imaging data presented in this paper. The authors
  further thank Andreas Villunger, Florian Gärtner, Frank Bradke, and Sarah Förster
  for helpful discussions; Andy Zielinski for help with statistics; and Björn Weiershausen
  for assisting with figure illustration.\r\n\r\nThis work was funded by a fellowship
  of the Ministry of Innovation, Science and Research of North-Rhine-Westphalia (AZ:
  421-8.03.03.02-137069) to E. Kiermaier and the Deutsche Forschungsgemeinschaft (German
  Research Foundation) under Germany’s Excellence Strategy – EXC 2151 – 390873048.
  R. Hauschild was funded by grant number 2020-225401 from the Chan Zuckerberg Initiative
  Donor-Advised Fund, an advised fund of Silicon Valley Community Foundation. M. Hons
  is supported by Czech Science Foundation GACR 20-24603Y and Charles University PRIMUS/20/MED/013."
article_number: e202107134
article_processing_charge: No
article_type: original
author:
- first_name: Ann-Kathrin
  full_name: Weier, Ann-Kathrin
  last_name: Weier
- first_name: Mirka
  full_name: Homrich, Mirka
  last_name: Homrich
- first_name: Stephanie
  full_name: Ebbinghaus, Stephanie
  last_name: Ebbinghaus
- first_name: Pavel
  full_name: Juda, Pavel
  last_name: Juda
- first_name: Eliška
  full_name: Miková, Eliška
  last_name: Miková
- first_name: Robert
  full_name: Hauschild, Robert
  id: 4E01D6B4-F248-11E8-B48F-1D18A9856A87
  last_name: Hauschild
  orcid: 0000-0001-9843-3522
- first_name: Lili
  full_name: Zhang, Lili
  last_name: Zhang
- first_name: Thomas
  full_name: Quast, Thomas
  last_name: Quast
- first_name: Elvira
  full_name: Mass, Elvira
  last_name: Mass
- first_name: Andreas
  full_name: Schlitzer, Andreas
  last_name: Schlitzer
- first_name: Waldemar
  full_name: Kolanus, Waldemar
  last_name: Kolanus
- first_name: Sven
  full_name: Burgdorf, Sven
  last_name: Burgdorf
- first_name: Oliver J.
  full_name: Gruß, Oliver J.
  last_name: Gruß
- first_name: Miroslav
  full_name: Hons, Miroslav
  last_name: Hons
- first_name: Stefan
  full_name: Wieser, Stefan
  last_name: Wieser
- first_name: Eva
  full_name: Kiermaier, Eva
  last_name: Kiermaier
citation:
  ama: Weier A-K, Homrich M, Ebbinghaus S, et al. Multiple centrosomes enhance migration
    and immune cell effector functions of mature dendritic cells. <i>Journal of Cell
    Biology</i>. 2022;221(12). doi:<a href="https://doi.org/10.1083/jcb.202107134">10.1083/jcb.202107134</a>
  apa: Weier, A.-K., Homrich, M., Ebbinghaus, S., Juda, P., Miková, E., Hauschild,
    R., … Kiermaier, E. (2022). Multiple centrosomes enhance migration and immune
    cell effector functions of mature dendritic cells. <i>Journal of Cell Biology</i>.
    Rockefeller University Press. <a href="https://doi.org/10.1083/jcb.202107134">https://doi.org/10.1083/jcb.202107134</a>
  chicago: Weier, Ann-Kathrin, Mirka Homrich, Stephanie Ebbinghaus, Pavel Juda, Eliška
    Miková, Robert Hauschild, Lili Zhang, et al. “Multiple Centrosomes Enhance Migration
    and Immune Cell Effector Functions of Mature Dendritic Cells.” <i>Journal of Cell
    Biology</i>. Rockefeller University Press, 2022. <a href="https://doi.org/10.1083/jcb.202107134">https://doi.org/10.1083/jcb.202107134</a>.
  ieee: A.-K. Weier <i>et al.</i>, “Multiple centrosomes enhance migration and immune
    cell effector functions of mature dendritic cells,” <i>Journal of Cell Biology</i>,
    vol. 221, no. 12. Rockefeller University Press, 2022.
  ista: Weier A-K, Homrich M, Ebbinghaus S, Juda P, Miková E, Hauschild R, Zhang L,
    Quast T, Mass E, Schlitzer A, Kolanus W, Burgdorf S, Gruß OJ, Hons M, Wieser S,
    Kiermaier E. 2022. Multiple centrosomes enhance migration and immune cell effector
    functions of mature dendritic cells. Journal of Cell Biology. 221(12), e202107134.
  mla: Weier, Ann-Kathrin, et al. “Multiple Centrosomes Enhance Migration and Immune
    Cell Effector Functions of Mature Dendritic Cells.” <i>Journal of Cell Biology</i>,
    vol. 221, no. 12, e202107134, Rockefeller University Press, 2022, doi:<a href="https://doi.org/10.1083/jcb.202107134">10.1083/jcb.202107134</a>.
  short: A.-K. Weier, M. Homrich, S. Ebbinghaus, P. Juda, E. Miková, R. Hauschild,
    L. Zhang, T. Quast, E. Mass, A. Schlitzer, W. Kolanus, S. Burgdorf, O.J. Gruß,
    M. Hons, S. Wieser, E. Kiermaier, Journal of Cell Biology 221 (2022).
date_created: 2023-01-12T12:01:09Z
date_published: 2022-12-05T00:00:00Z
date_updated: 2023-08-16T11:29:12Z
day: '05'
ddc:
- '570'
department:
- _id: Bio
doi: 10.1083/jcb.202107134
external_id:
  isi:
  - '000932941400001'
  pmid:
  - '36214847 '
file:
- access_level: open_access
  checksum: 0c9af38f82af30c6ce528f2caece4246
  content_type: application/pdf
  creator: dernst
  date_created: 2023-08-16T11:24:53Z
  date_updated: 2023-08-16T11:24:53Z
  file_id: '14065'
  file_name: 2023_JCB_Weier.pdf
  file_size: 11090179
  relation: main_file
  success: 1
file_date_updated: 2023-08-16T11:24:53Z
has_accepted_license: '1'
intvolume: '       221'
isi: 1
issue: '12'
keyword:
- Cell Biology
language:
- iso: eng
month: '12'
oa: 1
oa_version: Published Version
pmid: 1
project:
- _id: c08e9ad1-5a5b-11eb-8a69-9d1cf3b07473
  grant_number: CZI01
  name: Tools for automation and feedback microscopy
publication: Journal of Cell Biology
publication_identifier:
  eissn:
  - 1540-8140
  issn:
  - 0021-9525
publication_status: published
publisher: Rockefeller University Press
quality_controlled: '1'
scopus_import: '1'
status: public
title: Multiple centrosomes enhance migration and immune cell effector functions of
  mature dendritic cells
tmp:
  image: /images/cc_by_nc_sa.png
  legal_code_url: https://creativecommons.org/licenses/by-nc-sa/4.0/legalcode
  name: Creative Commons Attribution-NonCommercial-ShareAlike 4.0 International (CC
    BY-NC-SA 4.0)
  short: CC BY-NC-SA (4.0)
type: journal_article
user_id: 2DF688A6-F248-11E8-B48F-1D18A9856A87
volume: 221
year: '2022'
...
---
_id: '12143'
abstract:
- lang: eng
  text: MicroRNA (miRNA) and RNA interference (RNAi) pathways rely on small RNAs produced
    by Dicer endonucleases. Mammalian Dicer primarily supports the essential gene-regulating
    miRNA pathway, but how it is specifically adapted to miRNA biogenesis is unknown.
    We show that the adaptation entails a unique structural role of Dicer’s DExD/H
    helicase domain. Although mice tolerate loss of its putative ATPase function,
    the complete absence of the domain is lethal because it assures high-fidelity
    miRNA biogenesis. Structures of murine Dicer⋅miRNA precursor complexes revealed
    that the DExD/H domain has a helicase-unrelated structural function. It locks
    Dicer in a closed state, which facilitates miRNA precursor selection. Transition
    to a cleavage-competent open state is stimulated by Dicer-binding protein TARBP2.
    Absence of the DExD/H domain or its mutations unlocks the closed state, reduces
    substrate selectivity, and activates RNAi. Thus, the DExD/H domain structurally
    contributes to mammalian miRNA biogenesis and underlies mechanistical partitioning
    of miRNA and RNAi pathways.
acknowledged_ssus:
- _id: EM-Fac
acknowledgement: We thank Kristian Vlahovicek (University of Zagreb) for support of
  bioinformatics analyses and Vladimir Benes (EMBL Sequencing Facility) and Genomics
  and Bioinformatics Core Facility at the Institute of Molecular Genetics for help
  with RNA sequencing. The main funding was provided by the Czech Science Foundation
  (EXPRO grant 20-03950X to P.S. and 22-19896S to R. Stefl). Early stages of the work
  were supported by European Research Council grants under the European Union’s Horizon
  2020 Research and Innovation Programme (grants 647403 to P.S. and 649030 to R. Stefl).
  V.B., D.F.J., and F.H. were in part supported by PhD student fellowships from the
  Charles University; this work will be in part fulfilling requirements for a PhD
  degree as “school work.” Funding of D.Z. included the OP RDE project “Internal Grant
  Agency of Masaryk University” no. CZ.02.2.69/0.0/0.0/19_073/0016943. The Ministry
  of Education, Youth, and Sports of the Czech Republic (MEYS CR) provided institutional
  support for CEITEC 2020 project LQ1601. For technical support, we acknowledge EMBL
  Monterotondo’s genome engineering and transgenic core facilities, the Czech Centre
  for Phenogenomics at the Institute of Molecular Genetics (supported by RVO 68378050
  from the Czech Academy of Sciences and LM2018126 and CZ.02.1.01/0.0/0.0/18_046/0015861
  CCP Infrastructure Upgrade II from MEYS CR), the Cryo-EM and Proteomics Core Facilities
  (CEITEC, Masaryk University) supported by the CIISB research infrastructure (LM2018127
  from MEYS CR), and support from the Scientific Service Units of ISTA through resources
  from the Electron Microscopy Facility. Computational resources included e-Infrastruktura
  CZ (LM2018140) and ELIXIR-CZ (LM2018131) projects by MEYS CR and the Croatian National
  Centres of Research Excellence in Personalized Healthcare (#KK.01.1.1.01.0010) and
  Data Science and Advanced Cooperative Systems (#KK.01.1.1.01.0009) projects funded
  by the European Structural and Investment Funds grants.
article_processing_charge: No
article_type: original
author:
- first_name: David
  full_name: Zapletal, David
  last_name: Zapletal
- first_name: Eliska
  full_name: Taborska, Eliska
  last_name: Taborska
- first_name: Josef
  full_name: Pasulka, Josef
  last_name: Pasulka
- first_name: Radek
  full_name: Malik, Radek
  last_name: Malik
- first_name: Karel
  full_name: Kubicek, Karel
  last_name: Kubicek
- first_name: Martina
  full_name: Zanova, Martina
  last_name: Zanova
- first_name: Christian
  full_name: Much, Christian
  last_name: Much
- first_name: Marek
  full_name: Sebesta, Marek
  last_name: Sebesta
- first_name: Valeria
  full_name: Buccheri, Valeria
  last_name: Buccheri
- first_name: Filip
  full_name: Horvat, Filip
  last_name: Horvat
- first_name: Irena
  full_name: Jenickova, Irena
  last_name: Jenickova
- first_name: Michaela
  full_name: Prochazkova, Michaela
  last_name: Prochazkova
- first_name: Jan
  full_name: Prochazka, Jan
  last_name: Prochazka
- first_name: Matyas
  full_name: Pinkas, Matyas
  last_name: Pinkas
- first_name: Jiri
  full_name: Novacek, Jiri
  last_name: Novacek
- first_name: Diego F.
  full_name: Joseph, Diego F.
  last_name: Joseph
- first_name: Radislav
  full_name: Sedlacek, Radislav
  last_name: Sedlacek
- first_name: Carrie A
  full_name: Bernecky, Carrie A
  id: 2CB9DFE2-F248-11E8-B48F-1D18A9856A87
  last_name: Bernecky
  orcid: 0000-0003-0893-7036
- first_name: Dónal
  full_name: O’Carroll, Dónal
  last_name: O’Carroll
- first_name: Richard
  full_name: Stefl, Richard
  last_name: Stefl
- first_name: Petr
  full_name: Svoboda, Petr
  last_name: Svoboda
citation:
  ama: Zapletal D, Taborska E, Pasulka J, et al. Structural and functional basis of
    mammalian microRNA biogenesis by Dicer. <i>Molecular Cell</i>. 2022;82(21):4064-4079.e13.
    doi:<a href="https://doi.org/10.1016/j.molcel.2022.10.010">10.1016/j.molcel.2022.10.010</a>
  apa: Zapletal, D., Taborska, E., Pasulka, J., Malik, R., Kubicek, K., Zanova, M.,
    … Svoboda, P. (2022). Structural and functional basis of mammalian microRNA biogenesis
    by Dicer. <i>Molecular Cell</i>. Elsevier. <a href="https://doi.org/10.1016/j.molcel.2022.10.010">https://doi.org/10.1016/j.molcel.2022.10.010</a>
  chicago: Zapletal, David, Eliska Taborska, Josef Pasulka, Radek Malik, Karel Kubicek,
    Martina Zanova, Christian Much, et al. “Structural and Functional Basis of Mammalian
    MicroRNA Biogenesis by Dicer.” <i>Molecular Cell</i>. Elsevier, 2022. <a href="https://doi.org/10.1016/j.molcel.2022.10.010">https://doi.org/10.1016/j.molcel.2022.10.010</a>.
  ieee: D. Zapletal <i>et al.</i>, “Structural and functional basis of mammalian microRNA
    biogenesis by Dicer,” <i>Molecular Cell</i>, vol. 82, no. 21. Elsevier, p. 4064–4079.e13,
    2022.
  ista: Zapletal D, Taborska E, Pasulka J, Malik R, Kubicek K, Zanova M, Much C, Sebesta
    M, Buccheri V, Horvat F, Jenickova I, Prochazkova M, Prochazka J, Pinkas M, Novacek
    J, Joseph DF, Sedlacek R, Bernecky C, O’Carroll D, Stefl R, Svoboda P. 2022. Structural
    and functional basis of mammalian microRNA biogenesis by Dicer. Molecular Cell.
    82(21), 4064–4079.e13.
  mla: Zapletal, David, et al. “Structural and Functional Basis of Mammalian MicroRNA
    Biogenesis by Dicer.” <i>Molecular Cell</i>, vol. 82, no. 21, Elsevier, 2022,
    p. 4064–4079.e13, doi:<a href="https://doi.org/10.1016/j.molcel.2022.10.010">10.1016/j.molcel.2022.10.010</a>.
  short: D. Zapletal, E. Taborska, J. Pasulka, R. Malik, K. Kubicek, M. Zanova, C.
    Much, M. Sebesta, V. Buccheri, F. Horvat, I. Jenickova, M. Prochazkova, J. Prochazka,
    M. Pinkas, J. Novacek, D.F. Joseph, R. Sedlacek, C. Bernecky, D. O’Carroll, R.
    Stefl, P. Svoboda, Molecular Cell 82 (2022) 4064–4079.e13.
date_created: 2023-01-12T12:05:36Z
date_published: 2022-11-03T00:00:00Z
date_updated: 2023-08-04T08:57:17Z
day: '03'
ddc:
- '570'
department:
- _id: CaBe
doi: 10.1016/j.molcel.2022.10.010
external_id:
  isi:
  - '000898565300011'
  pmid:
  - '36332606'
file:
- access_level: open_access
  checksum: 999e443b54e4fdaa2542ca5a97619731
  content_type: application/pdf
  creator: dernst
  date_created: 2023-01-24T09:29:02Z
  date_updated: 2023-01-24T09:29:02Z
  file_id: '12354'
  file_name: 2022_MolecularCell_Zapletal.pdf
  file_size: 7368534
  relation: main_file
  success: 1
file_date_updated: 2023-01-24T09:29:02Z
has_accepted_license: '1'
intvolume: '        82'
isi: 1
issue: '21'
keyword:
- Cell Biology
- Molecular Biology
language:
- iso: eng
month: '11'
oa: 1
oa_version: Published Version
page: 4064-4079.e13
pmid: 1
publication: Molecular Cell
publication_identifier:
  issn:
  - 1097-2765
publication_status: published
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: Structural and functional basis of mammalian microRNA biogenesis by Dicer
tmp:
  image: /images/cc_by.png
  legal_code_url: https://creativecommons.org/licenses/by/4.0/legalcode
  name: Creative Commons Attribution 4.0 International Public License (CC-BY 4.0)
  short: CC BY (4.0)
type: journal_article
user_id: 4359f0d1-fa6c-11eb-b949-802e58b17ae8
volume: 82
year: '2022'
...
---
_id: '12238'
abstract:
- lang: eng
  text: Upon the initiation of collective cell migration, the cells at the free edge
    are specified as leader cells; however, the mechanism underlying the leader cell
    specification remains elusive. Here, we show that lamellipodial extension after
    the release from mechanical confinement causes sustained extracellular signal-regulated
    kinase (ERK) activation and underlies the leader cell specification. Live-imaging
    of Madin-Darby canine kidney (MDCK) cells and mouse epidermis through the use
    of Förster resonance energy transfer (FRET)-based biosensors showed that leader
    cells exhibit sustained ERK activation in a hepatocyte growth factor (HGF)-dependent
    manner. Meanwhile, follower cells exhibit oscillatory ERK activation waves in
    an epidermal growth factor (EGF) signaling-dependent manner. Lamellipodial extension
    at the free edge increases the cellular sensitivity to HGF. The HGF-dependent
    ERK activation, in turn, promotes lamellipodial extension, thereby forming a positive
    feedback loop between cell extension and ERK activation and specifying the cells
    at the free edge as the leader cells. Our findings show that the integration of
    physical and biochemical cues underlies the leader cell specification during collective
    cell migration.
acknowledgement: We thank the members of the Matsuda Laboratory for their helpful
  discussion and encouragement, and we thank K. Hirano and K. Takakura for their technical
  assistance. This work was supported by the Kyoto University Live Imaging Center.
  Financial support was provided in the form of JSPS KAKENHI grants (nos. 17J02107
  and 20K22653 to N.H., and 20H05898 and 19H00993 to M.M.), a JST CREST grant (no.
  JPMJCR1654 to M.M.), a Moonshot R&D grant (no. JPMJPS2022-11 to M.M.), Generalitat
  de Catalunya and the CERCA Programme (no. SGR-2017-01602 to X.T.), MICCINN/FEDER
  (no. PGC2018-099645-B-I00 to X.T.), and European Research Council (no. Adv-883739
  to X.T.). IBEC is a recipient of a Severo Ochoa Award of Excellence from the MINECO.
  This work was partly supported by an Extramural Collaborative Research Grant of
  Cancer Research Institute, Kanazawa University.
article_processing_charge: No
article_type: original
author:
- first_name: Naoya
  full_name: Hino, Naoya
  id: 5299a9ce-7679-11eb-a7bc-d1e62b936307
  last_name: Hino
- first_name: Kimiya
  full_name: Matsuda, Kimiya
  last_name: Matsuda
- first_name: Yuya
  full_name: Jikko, Yuya
  last_name: Jikko
- first_name: Gembu
  full_name: Maryu, Gembu
  last_name: Maryu
- first_name: Katsuya
  full_name: Sakai, Katsuya
  last_name: Sakai
- first_name: Ryu
  full_name: Imamura, Ryu
  last_name: Imamura
- first_name: Shinya
  full_name: Tsukiji, Shinya
  last_name: Tsukiji
- first_name: Kazuhiro
  full_name: Aoki, Kazuhiro
  last_name: Aoki
- first_name: Kenta
  full_name: Terai, Kenta
  last_name: Terai
- first_name: Tsuyoshi
  full_name: Hirashima, Tsuyoshi
  last_name: Hirashima
- first_name: Xavier
  full_name: Trepat, Xavier
  last_name: Trepat
- first_name: Michiyuki
  full_name: Matsuda, Michiyuki
  last_name: Matsuda
citation:
  ama: Hino N, Matsuda K, Jikko Y, et al. A feedback loop between lamellipodial extension
    and HGF-ERK signaling specifies leader cells during collective cell migration.
    <i>Developmental Cell</i>. 2022;57(19):2290-2304.e7. doi:<a href="https://doi.org/10.1016/j.devcel.2022.09.003">10.1016/j.devcel.2022.09.003</a>
  apa: Hino, N., Matsuda, K., Jikko, Y., Maryu, G., Sakai, K., Imamura, R., … Matsuda,
    M. (2022). A feedback loop between lamellipodial extension and HGF-ERK signaling
    specifies leader cells during collective cell migration. <i>Developmental Cell</i>.
    Elsevier. <a href="https://doi.org/10.1016/j.devcel.2022.09.003">https://doi.org/10.1016/j.devcel.2022.09.003</a>
  chicago: Hino, Naoya, Kimiya Matsuda, Yuya Jikko, Gembu Maryu, Katsuya Sakai, Ryu
    Imamura, Shinya Tsukiji, et al. “A Feedback Loop between Lamellipodial Extension
    and HGF-ERK Signaling Specifies Leader Cells during Collective Cell Migration.”
    <i>Developmental Cell</i>. Elsevier, 2022. <a href="https://doi.org/10.1016/j.devcel.2022.09.003">https://doi.org/10.1016/j.devcel.2022.09.003</a>.
  ieee: N. Hino <i>et al.</i>, “A feedback loop between lamellipodial extension and
    HGF-ERK signaling specifies leader cells during collective cell migration,” <i>Developmental
    Cell</i>, vol. 57, no. 19. Elsevier, p. 2290–2304.e7, 2022.
  ista: Hino N, Matsuda K, Jikko Y, Maryu G, Sakai K, Imamura R, Tsukiji S, Aoki K,
    Terai K, Hirashima T, Trepat X, Matsuda M. 2022. A feedback loop between lamellipodial
    extension and HGF-ERK signaling specifies leader cells during collective cell
    migration. Developmental Cell. 57(19), 2290–2304.e7.
  mla: Hino, Naoya, et al. “A Feedback Loop between Lamellipodial Extension and HGF-ERK
    Signaling Specifies Leader Cells during Collective Cell Migration.” <i>Developmental
    Cell</i>, vol. 57, no. 19, Elsevier, 2022, p. 2290–2304.e7, doi:<a href="https://doi.org/10.1016/j.devcel.2022.09.003">10.1016/j.devcel.2022.09.003</a>.
  short: N. Hino, K. Matsuda, Y. Jikko, G. Maryu, K. Sakai, R. Imamura, S. Tsukiji,
    K. Aoki, K. Terai, T. Hirashima, X. Trepat, M. Matsuda, Developmental Cell 57
    (2022) 2290–2304.e7.
date_created: 2023-01-16T09:51:39Z
date_published: 2022-10-01T00:00:00Z
date_updated: 2023-08-04T09:38:53Z
day: '01'
department:
- _id: CaHe
doi: 10.1016/j.devcel.2022.09.003
external_id:
  isi:
  - '000898428700006'
  pmid:
  - '36174555'
intvolume: '        57'
isi: 1
issue: '19'
keyword:
- Developmental Biology
- Cell Biology
- General Biochemistry
- Genetics and Molecular Biology
- Molecular Biology
language:
- iso: eng
month: '10'
oa_version: None
page: 2290-2304.e7
pmid: 1
publication: Developmental Cell
publication_identifier:
  issn:
  - 1534-5807
publication_status: published
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: A feedback loop between lamellipodial extension and HGF-ERK signaling specifies
  leader cells during collective cell migration
type: journal_article
user_id: 4359f0d1-fa6c-11eb-b949-802e58b17ae8
volume: 57
year: '2022'
...
---
_id: '12272'
abstract:
- lang: eng
  text: Reading, interpreting and crawling along gradients of chemotactic cues is
    one of the most complex questions in cell biology. In this issue, Georgantzoglou
    et al. (2022. J. Cell. Biol.https://doi.org/10.1083/jcb.202103207) use in vivo
    models to map the temporal sequence of how neutrophils respond to an acutely arising
    gradient of chemoattractant.
article_number: e202206127
article_processing_charge: No
article_type: original
author:
- first_name: Julian A
  full_name: Stopp, Julian A
  id: 489E3F00-F248-11E8-B48F-1D18A9856A87
  last_name: Stopp
- first_name: Michael K
  full_name: Sixt, Michael K
  id: 41E9FBEA-F248-11E8-B48F-1D18A9856A87
  last_name: Sixt
  orcid: 0000-0002-6620-9179
citation:
  ama: 'Stopp JA, Sixt MK. Plan your trip before you leave: The neutrophils’ search-and-run
    journey. <i>Journal of Cell Biology</i>. 2022;221(8). doi:<a href="https://doi.org/10.1083/jcb.202206127">10.1083/jcb.202206127</a>'
  apa: 'Stopp, J. A., &#38; Sixt, M. K. (2022). Plan your trip before you leave: The
    neutrophils’ search-and-run journey. <i>Journal of Cell Biology</i>. Rockefeller
    University Press. <a href="https://doi.org/10.1083/jcb.202206127">https://doi.org/10.1083/jcb.202206127</a>'
  chicago: 'Stopp, Julian A, and Michael K Sixt. “Plan Your Trip before You Leave:
    The Neutrophils’ Search-and-Run Journey.” <i>Journal of Cell Biology</i>. Rockefeller
    University Press, 2022. <a href="https://doi.org/10.1083/jcb.202206127">https://doi.org/10.1083/jcb.202206127</a>.'
  ieee: 'J. A. Stopp and M. K. Sixt, “Plan your trip before you leave: The neutrophils’
    search-and-run journey,” <i>Journal of Cell Biology</i>, vol. 221, no. 8. Rockefeller
    University Press, 2022.'
  ista: 'Stopp JA, Sixt MK. 2022. Plan your trip before you leave: The neutrophils’
    search-and-run journey. Journal of Cell Biology. 221(8), e202206127.'
  mla: 'Stopp, Julian A., and Michael K. Sixt. “Plan Your Trip before You Leave: The
    Neutrophils’ Search-and-Run Journey.” <i>Journal of Cell Biology</i>, vol. 221,
    no. 8, e202206127, Rockefeller University Press, 2022, doi:<a href="https://doi.org/10.1083/jcb.202206127">10.1083/jcb.202206127</a>.'
  short: J.A. Stopp, M.K. Sixt, Journal of Cell Biology 221 (2022).
date_created: 2023-01-16T10:01:08Z
date_published: 2022-07-20T00:00:00Z
date_updated: 2023-12-21T14:30:01Z
day: '20'
ddc:
- '570'
department:
- _id: MiSi
doi: 10.1083/jcb.202206127
external_id:
  isi:
  - '000874717200001'
  pmid:
  - '35856919'
file:
- access_level: open_access
  checksum: 6b1620743669679b48b9389bb40f5a11
  content_type: application/pdf
  creator: dernst
  date_created: 2023-01-30T10:39:34Z
  date_updated: 2023-01-30T10:39:34Z
  file_id: '12451'
  file_name: 2022_JourCellBiology_Stopp.pdf
  file_size: 969969
  relation: main_file
  success: 1
file_date_updated: 2023-01-30T10:39:34Z
has_accepted_license: '1'
intvolume: '       221'
isi: 1
issue: '8'
keyword:
- Cell Biology
language:
- iso: eng
month: '07'
oa: 1
oa_version: Published Version
pmid: 1
publication: Journal of Cell Biology
publication_identifier:
  eissn:
  - 1540-8140
  issn:
  - 0021-9525
publication_status: published
publisher: Rockefeller University Press
quality_controlled: '1'
related_material:
  record:
  - id: '14697'
    relation: dissertation_contains
    status: public
scopus_import: '1'
status: public
title: 'Plan your trip before you leave: The neutrophils’ search-and-run journey'
tmp:
  image: /images/cc_by_nc_sa.png
  legal_code_url: https://creativecommons.org/licenses/by-nc-sa/4.0/legalcode
  name: Creative Commons Attribution-NonCommercial-ShareAlike 4.0 International (CC
    BY-NC-SA 4.0)
  short: CC BY-NC-SA (4.0)
type: journal_article
user_id: 4359f0d1-fa6c-11eb-b949-802e58b17ae8
volume: 221
year: '2022'
...
---
_id: '12283'
abstract:
- lang: eng
  text: Neurons extend axons to form the complex circuitry of the mature brain. This
    depends on the coordinated response and continuous remodelling of the microtubule
    and F-actin networks in the axonal growth cone. Growth cone architecture remains
    poorly understood at nanoscales. We therefore investigated mouse hippocampal neuron
    growth cones using cryo-electron tomography to directly visualise their three-dimensional
    subcellular architecture with molecular detail. Our data showed that the hexagonal
    arrays of actin bundles that form filopodia penetrate and terminate deep within
    the growth cone interior. We directly observed the modulation of these and other
    growth cone actin bundles by alteration of individual F-actin helical structures.
    Microtubules with blunt, slightly flared or gently curved ends predominated in
    the growth cone, frequently contained lumenal particles and exhibited lattice
    defects. Investigation of the effect of absence of doublecortin, a neurodevelopmental
    cytoskeleton regulator, on growth cone cytoskeleton showed no major anomalies
    in overall growth cone organisation or in F-actin subpopulations. However, our
    data suggested that microtubules sustained more structural defects, highlighting
    the importance of microtubule integrity during growth cone migration.
acknowledgement: "J.A. was supported by a grant from the Medical Research Council
  (MRC), UK (MR/R000352/1) to C.A.M. Cryo-EM data were collected on equipment funded
  by the Wellcome Trust, UK (079605/Z/06/Z) and the Biotechnology and Biological Sciences
  Research Council (BBSRC) UK (BB/L014211/1). F.F.’s salary and institute were supported
  by Inserm (Institut National de la Santé et de la Recherche Médicale), CNRS (Centre
  National de la Recherche Scientifique) and Sorbonne Université. F.F.’s group was
  particularly supported by Agence Nationale de la\r\nRecherche (ANR-16-CE16-0011-03)
  and Seventh Framework Programme (EUHEALTH-\r\n2013, DESIRE, N° 60253; also funding
  M.S.’s salary) and the European Cooperation in Science and Technology (COST Action
  CA16118). Open Access funding provided by Birkbeck College: Birkbeck University
  of London. Deposited in PMC for immediate release."
article_number: '259234'
article_processing_charge: No
article_type: original
author:
- first_name: Joseph
  full_name: Atherton, Joseph
  last_name: Atherton
- first_name: Melissa A
  full_name: Stouffer, Melissa A
  id: 4C9372C4-F248-11E8-B48F-1D18A9856A87
  last_name: Stouffer
- first_name: Fiona
  full_name: Francis, Fiona
  last_name: Francis
- first_name: Carolyn A.
  full_name: Moores, Carolyn A.
  last_name: Moores
citation:
  ama: Atherton J, Stouffer MA, Francis F, Moores CA. Visualising the cytoskeletal
    machinery in neuronal growth cones using cryo-electron tomography. <i>Journal
    of Cell Science</i>. 2022;135(7). doi:<a href="https://doi.org/10.1242/jcs.259234">10.1242/jcs.259234</a>
  apa: Atherton, J., Stouffer, M. A., Francis, F., &#38; Moores, C. A. (2022). Visualising
    the cytoskeletal machinery in neuronal growth cones using cryo-electron tomography.
    <i>Journal of Cell Science</i>. The Company of Biologists. <a href="https://doi.org/10.1242/jcs.259234">https://doi.org/10.1242/jcs.259234</a>
  chicago: Atherton, Joseph, Melissa A Stouffer, Fiona Francis, and Carolyn A. Moores.
    “Visualising the Cytoskeletal Machinery in Neuronal Growth Cones Using Cryo-Electron
    Tomography.” <i>Journal of Cell Science</i>. The Company of Biologists, 2022.
    <a href="https://doi.org/10.1242/jcs.259234">https://doi.org/10.1242/jcs.259234</a>.
  ieee: J. Atherton, M. A. Stouffer, F. Francis, and C. A. Moores, “Visualising the
    cytoskeletal machinery in neuronal growth cones using cryo-electron tomography,”
    <i>Journal of Cell Science</i>, vol. 135, no. 7. The Company of Biologists, 2022.
  ista: Atherton J, Stouffer MA, Francis F, Moores CA. 2022. Visualising the cytoskeletal
    machinery in neuronal growth cones using cryo-electron tomography. Journal of
    Cell Science. 135(7), 259234.
  mla: Atherton, Joseph, et al. “Visualising the Cytoskeletal Machinery in Neuronal
    Growth Cones Using Cryo-Electron Tomography.” <i>Journal of Cell Science</i>,
    vol. 135, no. 7, 259234, The Company of Biologists, 2022, doi:<a href="https://doi.org/10.1242/jcs.259234">10.1242/jcs.259234</a>.
  short: J. Atherton, M.A. Stouffer, F. Francis, C.A. Moores, Journal of Cell Science
    135 (2022).
date_created: 2023-01-16T10:03:24Z
date_published: 2022-04-01T00:00:00Z
date_updated: 2023-08-04T10:28:34Z
day: '01'
ddc:
- '570'
department:
- _id: SiHi
doi: 10.1242/jcs.259234
external_id:
  isi:
  - '000783840400010'
  pmid:
  - '35383828'
file:
- access_level: open_access
  checksum: 4346ed32cb7c89a8ca051c7da68a9a1c
  content_type: application/pdf
  creator: dernst
  date_created: 2023-01-30T11:41:01Z
  date_updated: 2023-01-30T11:41:01Z
  file_id: '12461'
  file_name: 2022_JourCellBiology_Atherton.pdf
  file_size: 13868733
  relation: main_file
  success: 1
file_date_updated: 2023-01-30T11:41:01Z
has_accepted_license: '1'
intvolume: '       135'
isi: 1
issue: '7'
keyword:
- Cell Biology
language:
- iso: eng
month: '04'
oa: 1
oa_version: Published Version
pmid: 1
publication: Journal of Cell Science
publication_identifier:
  eissn:
  - 1477-9137
  issn:
  - 0021-9533
publication_status: published
publisher: The Company of Biologists
quality_controlled: '1'
scopus_import: '1'
status: public
title: Visualising the cytoskeletal machinery in neuronal growth cones using cryo-electron
  tomography
tmp:
  image: /images/cc_by.png
  legal_code_url: https://creativecommons.org/licenses/by/4.0/legalcode
  name: Creative Commons Attribution 4.0 International Public License (CC-BY 4.0)
  short: CC BY (4.0)
type: journal_article
user_id: 4359f0d1-fa6c-11eb-b949-802e58b17ae8
volume: 135
year: '2022'
...
---
_id: '11052'
abstract:
- lang: eng
  text: In order to combat molecular damage, most cellular proteins undergo rapid
    turnover. We have previously identified large nuclear protein assemblies that
    can persist for years in post-mitotic tissues and are subject to age-related decline.
    Here, we report that mitochondria can be long lived in the mouse brain and reveal
    that specific mitochondrial proteins have half-lives longer than the average proteome.
    These mitochondrial long-lived proteins (mitoLLPs) are core components of the
    electron transport chain (ETC) and display increased longevity in respiratory
    supercomplexes. We find that COX7C, a mitoLLP that forms a stable contact site
    between complexes I and IV, is required for complex IV and supercomplex assembly.
    Remarkably, even upon depletion of COX7C transcripts, ETC function is maintained
    for days, effectively uncoupling mitochondrial function from ongoing transcription
    of its mitoLLPs. Our results suggest that modulating protein longevity within
    the ETC is critical for mitochondrial proteome maintenance and the robustness
    of mitochondrial function.
article_processing_charge: No
article_type: original
author:
- first_name: Shefali
  full_name: Krishna, Shefali
  last_name: Krishna
- first_name: Rafael
  full_name: Arrojo e Drigo, Rafael
  last_name: Arrojo e Drigo
- first_name: Juliana S.
  full_name: Capitanio, Juliana S.
  last_name: Capitanio
- first_name: Ranjan
  full_name: Ramachandra, Ranjan
  last_name: Ramachandra
- first_name: Mark
  full_name: Ellisman, Mark
  last_name: Ellisman
- first_name: Martin W
  full_name: HETZER, Martin W
  id: 86c0d31b-b4eb-11ec-ac5a-eae7b2e135ed
  last_name: HETZER
  orcid: 0000-0002-2111-992X
citation:
  ama: Krishna S, Arrojo e Drigo R, Capitanio JS, Ramachandra R, Ellisman M, Hetzer
    M. Identification of long-lived proteins in the mitochondria reveals increased
    stability of the electron transport chain. <i>Developmental Cell</i>. 2021;56(21):P2952-2965.e9.
    doi:<a href="https://doi.org/10.1016/j.devcel.2021.10.008">10.1016/j.devcel.2021.10.008</a>
  apa: Krishna, S., Arrojo e Drigo, R., Capitanio, J. S., Ramachandra, R., Ellisman,
    M., &#38; Hetzer, M. (2021). Identification of long-lived proteins in the mitochondria
    reveals increased stability of the electron transport chain. <i>Developmental
    Cell</i>. Elsevier. <a href="https://doi.org/10.1016/j.devcel.2021.10.008">https://doi.org/10.1016/j.devcel.2021.10.008</a>
  chicago: Krishna, Shefali, Rafael Arrojo e Drigo, Juliana S. Capitanio, Ranjan Ramachandra,
    Mark Ellisman, and Martin Hetzer. “Identification of Long-Lived Proteins in the
    Mitochondria Reveals Increased Stability of the Electron Transport Chain.” <i>Developmental
    Cell</i>. Elsevier, 2021. <a href="https://doi.org/10.1016/j.devcel.2021.10.008">https://doi.org/10.1016/j.devcel.2021.10.008</a>.
  ieee: S. Krishna, R. Arrojo e Drigo, J. S. Capitanio, R. Ramachandra, M. Ellisman,
    and M. Hetzer, “Identification of long-lived proteins in the mitochondria reveals
    increased stability of the electron transport chain,” <i>Developmental Cell</i>,
    vol. 56, no. 21. Elsevier, p. P2952–2965.e9, 2021.
  ista: Krishna S, Arrojo e Drigo R, Capitanio JS, Ramachandra R, Ellisman M, Hetzer
    M. 2021. Identification of long-lived proteins in the mitochondria reveals increased
    stability of the electron transport chain. Developmental Cell. 56(21), P2952–2965.e9.
  mla: Krishna, Shefali, et al. “Identification of Long-Lived Proteins in the Mitochondria
    Reveals Increased Stability of the Electron Transport Chain.” <i>Developmental
    Cell</i>, vol. 56, no. 21, Elsevier, 2021, p. P2952–2965.e9, doi:<a href="https://doi.org/10.1016/j.devcel.2021.10.008">10.1016/j.devcel.2021.10.008</a>.
  short: S. Krishna, R. Arrojo e Drigo, J.S. Capitanio, R. Ramachandra, M. Ellisman,
    M. Hetzer, Developmental Cell 56 (2021) P2952–2965.e9.
date_created: 2022-04-07T07:43:14Z
date_published: 2021-11-08T00:00:00Z
date_updated: 2022-07-18T08:26:38Z
day: '08'
doi: 10.1016/j.devcel.2021.10.008
extern: '1'
external_id:
  pmid:
  - '34715012'
intvolume: '        56'
issue: '21'
keyword:
- Developmental Biology
- Cell Biology
- General Biochemistry
- Genetics and Molecular Biology
- Molecular Biology
language:
- iso: eng
month: '11'
oa_version: None
page: P2952-2965.e9
pmid: 1
publication: Developmental Cell
publication_identifier:
  issn:
  - 1534-5807
publication_status: published
publisher: Elsevier
quality_controlled: '1'
scopus_import: '1'
status: public
title: Identification of long-lived proteins in the mitochondria reveals increased
  stability of the electron transport chain
type: journal_article
user_id: 72615eeb-f1f3-11ec-aa25-d4573ddc34fd
volume: 56
year: '2021'
...
---
_id: '8966'
abstract:
- lang: eng
  text: During development, a single cell is transformed into a highly complex organism
    through progressive cell division, specification and rearrangement. An important
    prerequisite for the emergence of patterns within the developing organism is to
    establish asymmetries at various scales, ranging from individual cells to the
    entire embryo, eventually giving rise to the different body structures. This becomes
    especially apparent during gastrulation, when the earliest major lineage restriction
    events lead to the formation of the different germ layers. Traditionally, the
    unfolding of the developmental program from symmetry breaking to germ layer formation
    has been studied by dissecting the contributions of different signaling pathways
    and cellular rearrangements in the in vivo context of intact embryos. Recent efforts,
    using the intrinsic capacity of embryonic stem cells to self-assemble and generate
    embryo-like structures de novo, have opened new avenues for understanding the
    many ways by which an embryo can be built and the influence of extrinsic factors
    therein. Here, we discuss and compare divergent and conserved strategies leading
    to germ layer formation in embryos as compared to in vitro systems, their upstream
    molecular cascades and the role of extrinsic factors in this process.
acknowledgement: We thank Nicoletta Petridou, Diana Pinheiro, Cornelia Schwayer and
  Stefania Tavano for feedback on the manuscript. Research in the Heisenberg lab is
  supported by an ERC Advanced Grant (MECSPEC 742573) to C.-P.H. A.S. is a recipient
  of a DOC Fellowship of the Austrian Academy of Science.
article_processing_charge: Yes (via OA deal)
article_type: original
author:
- first_name: Alexandra
  full_name: Schauer, Alexandra
  id: 30A536BA-F248-11E8-B48F-1D18A9856A87
  last_name: Schauer
  orcid: 0000-0001-7659-9142
- first_name: Carl-Philipp J
  full_name: Heisenberg, Carl-Philipp J
  id: 39427864-F248-11E8-B48F-1D18A9856A87
  last_name: Heisenberg
  orcid: 0000-0002-0912-4566
citation:
  ama: Schauer A, Heisenberg C-PJ. Reassembling gastrulation. <i>Developmental Biology</i>.
    2021;474:71-81. doi:<a href="https://doi.org/10.1016/j.ydbio.2020.12.014">10.1016/j.ydbio.2020.12.014</a>
  apa: Schauer, A., &#38; Heisenberg, C.-P. J. (2021). Reassembling gastrulation.
    <i>Developmental Biology</i>. Elsevier. <a href="https://doi.org/10.1016/j.ydbio.2020.12.014">https://doi.org/10.1016/j.ydbio.2020.12.014</a>
  chicago: Schauer, Alexandra, and Carl-Philipp J Heisenberg. “Reassembling Gastrulation.”
    <i>Developmental Biology</i>. Elsevier, 2021. <a href="https://doi.org/10.1016/j.ydbio.2020.12.014">https://doi.org/10.1016/j.ydbio.2020.12.014</a>.
  ieee: A. Schauer and C.-P. J. Heisenberg, “Reassembling gastrulation,” <i>Developmental
    Biology</i>, vol. 474. Elsevier, pp. 71–81, 2021.
  ista: Schauer A, Heisenberg C-PJ. 2021. Reassembling gastrulation. Developmental
    Biology. 474, 71–81.
  mla: Schauer, Alexandra, and Carl-Philipp J. Heisenberg. “Reassembling Gastrulation.”
    <i>Developmental Biology</i>, vol. 474, Elsevier, 2021, pp. 71–81, doi:<a href="https://doi.org/10.1016/j.ydbio.2020.12.014">10.1016/j.ydbio.2020.12.014</a>.
  short: A. Schauer, C.-P.J. Heisenberg, Developmental Biology 474 (2021) 71–81.
date_created: 2020-12-22T09:53:34Z
date_published: 2021-06-01T00:00:00Z
date_updated: 2023-08-07T13:30:01Z
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title: Reassembling gastrulation
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