[{"author":[{"full_name":"Lieb, Élliott H","first_name":"Élliott","last_name":"Lieb"},{"full_name":"Robert Seiringer","orcid":"0000-0002-6781-0521","last_name":"Seiringer","first_name":"Robert","id":"4AFD0470-F248-11E8-B48F-1D18A9856A87"},{"last_name":"Solovej","first_name":"Jan","full_name":"Solovej, Jan P"}],"month":"05","citation":{"chicago":"Lieb, Élliott, Robert Seiringer, and Jan Solovej. “Ground State Energy of the Low Density Fermi Gas.” Physical Review A - Atomic, Molecular, and Optical Physics. American Physical Society, 2005. https://doi.org/10.1103/PhysRevA.71.053605.","ieee":"É. Lieb, R. Seiringer, and J. Solovej, “Ground state energy of the low density Fermi gas,” Physical Review A - Atomic, Molecular, and Optical Physics, vol. 71, no. 5. American Physical Society, 2005.","short":"É. Lieb, R. Seiringer, J. Solovej, Physical Review A - Atomic, Molecular, and Optical Physics 71 (2005).","mla":"Lieb, Élliott, et al. “Ground State Energy of the Low Density Fermi Gas.” Physical Review A - Atomic, Molecular, and Optical Physics, vol. 71, no. 5, American Physical Society, 2005, doi:10.1103/PhysRevA.71.053605.","ama":"Lieb É, Seiringer R, Solovej J. Ground state energy of the low density Fermi gas. Physical Review A - Atomic, Molecular, and Optical Physics. 2005;71(5). doi:10.1103/PhysRevA.71.053605","ista":"Lieb É, Seiringer R, Solovej J. 2005. Ground state energy of the low density Fermi gas. Physical Review A - Atomic, Molecular, and Optical Physics. 71(5).","apa":"Lieb, É., Seiringer, R., & Solovej, J. (2005). Ground state energy of the low density Fermi gas. Physical Review A - Atomic, Molecular, and Optical Physics. American Physical Society. https://doi.org/10.1103/PhysRevA.71.053605"},"date_created":"2018-12-11T11:57:13Z","extern":1,"publist_id":"4565","issue":"5","publication":"Physical Review A - Atomic, Molecular, and Optical Physics","date_published":"2005-05-01T00:00:00Z","status":"public","abstract":[{"text":"Recent developments in the physics of low-density trapped gases make it worthwhile to verify old, well-known results that, while plausible, were based on perturbation theory and assumptions about pseudopotentials. We use and extend recently developed techniques to give a rigorous derivation of the asymptotic formula for the ground-state energy of a dilute gas of N fermions interacting with a short-range, positive potential of scattering length a. For spin-12 fermions, this is E∼E0+(22m)2πNa, where E0 is the energy of the noninteracting system and is the density. A similar formula holds in two dimensions (2D), with a replaced by ln(a2). Obviously this 2D energy is not the expectation value of a density-independent pseudopotential.","lang":"eng"}],"_id":"2362","intvolume":" 71","quality_controlled":0,"doi":"10.1103/PhysRevA.71.053605","title":"Ground state energy of the low density Fermi gas","date_updated":"2021-01-12T06:57:01Z","publisher":"American Physical Society","day":"01","publication_status":"published","main_file_link":[{"url":"http://arxiv.org/abs/math-ph/0412080","open_access":"1"}],"year":"2005","oa":1,"type":"journal_article","volume":71},{"publisher":"Springer","date_updated":"2021-01-12T06:57:25Z","publication_status":"published","day":"01","quality_controlled":0,"title":"The Clique problem in intersection graphs of ellipses and triangles","doi":"10.1007/s00224-005-1141-6","volume":38,"type":"journal_article","year":"2005","citation":{"ama":"Ambühl C, Wagner U. The Clique problem in intersection graphs of ellipses and triangles. Theory of Computing Systems. 2005;38(3):279-292. doi:10.1007/s00224-005-1141-6","apa":"Ambühl, C., & Wagner, U. (2005). The Clique problem in intersection graphs of ellipses and triangles. Theory of Computing Systems. Springer. https://doi.org/10.1007/s00224-005-1141-6","ista":"Ambühl C, Wagner U. 2005. The Clique problem in intersection graphs of ellipses and triangles. Theory of Computing Systems. 38(3), 279–292.","ieee":"C. Ambühl and U. Wagner, “The Clique problem in intersection graphs of ellipses and triangles,” Theory of Computing Systems, vol. 38, no. 3. Springer, pp. 279–292, 2005.","chicago":"Ambühl, Christoph, and Uli Wagner. “The Clique Problem in Intersection Graphs of Ellipses and Triangles.” Theory of Computing Systems. Springer, 2005. https://doi.org/10.1007/s00224-005-1141-6.","short":"C. Ambühl, U. Wagner, Theory of Computing Systems 38 (2005) 279–292.","mla":"Ambühl, Christoph, and Uli Wagner. “The Clique Problem in Intersection Graphs of Ellipses and Triangles.” Theory of Computing Systems, vol. 38, no. 3, Springer, 2005, pp. 279–92, doi:10.1007/s00224-005-1141-6."},"date_created":"2018-12-11T11:57:36Z","extern":1,"month":"05","author":[{"full_name":"Ambühl, Christoph","last_name":"Ambühl","first_name":"Christoph"},{"orcid":"0000-0002-1494-0568","full_name":"Uli Wagner","first_name":"Uli","last_name":"Wagner","id":"36690CA2-F248-11E8-B48F-1D18A9856A87"}],"_id":"2427","intvolume":" 38","status":"public","date_published":"2005-05-01T00:00:00Z","publist_id":"4497","publication":"Theory of Computing Systems","issue":"3","abstract":[{"text":"Intersection graphs of disks and of line segments, respectively, have been well studied, because of both practical applications and theoretically interesting properties of these graphs. Despite partial results, the complexity status of the Clique problem for these two graph classes is still open. Here, we consider the Clique problem for intersection graphs of ellipses, which, in a sense, interpolate between disks and line segments, and show that the problem is APX-hard in that case. Moreover, this holds even if for all ellipses, the ratio of the larger over the smaller radius is some prescribed number. Furthermore, the reduction immediately carries over to intersection graphs of triangles. To our knowledge, this is the first hardness result for the Clique problem in intersection graphs of convex objects with finite description complexity. We also describe a simple approximation algorithm for the case of ellipses for which the ratio of radii is bounded.","lang":"eng"}],"page":"279 - 292"},{"type":"conference","conference":{"name":"SODA: Symposium on Discrete Algorithms"},"year":"2005","day":"01","publication_status":"published","date_updated":"2021-01-12T06:57:25Z","publisher":"SIAM","doi":"10.1137/S0097539704446682","title":"Online conflict-free coloring for intervals","quality_controlled":0,"_id":"2428","page":"545 - 554","abstract":[{"text":"We consider an online version of the conflict-free coloring of a set of points on the line, where each newly inserted point must be assigned a color upon insertion, and at all times the coloring has to be conflict-free, in the sense that in every interval I there is a color that appears exactly once in I. We present several deterministic and randomized algorithms for achieving this goal, and analyze their performance, that is, the maximum number of colors that they need to use, as a function of the number n of inserted points. We first show that a natural and simple (deterministic) approach may perform rather poorly, requiring Ω(√n) colors in the worst case. We then modify this approach, to obtain an efficient deterministic algorithm that uses a maximum of Θ(log 2 n) colors. Next, we present two randomized solutions. The first algorithm requires an expected number of at most O(log 2 n) colors, and produces a coloring which is valid with high probability, and the second one, which is a variant of our efficient deterministic algorithm, requires an expected number of at most O(log n log log n) colors but always produces a valid coloring. We also analyze the performance of the simplest proposed algorithm when the points are inserted in a random order, and present an incomplete analysis that indicates that, with high probability, it uses only O(log n) colors. Finally, we show that in the extension of this problem to two dimensions, where the relevant ranges are disks, n colors may be required in the worst case. The average-case behavior for disks, and cases involving other planar ranges, are still open.","lang":"eng"}],"publist_id":"4496","status":"public","date_published":"2005-01-01T00:00:00Z","extern":1,"date_created":"2018-12-11T11:57:36Z","citation":{"ista":"Fiat A, Levy M, Matoušek J, Pach E, Sharir M, Smorodinsky S, Wagner U, Welzl E. 2005. Online conflict-free coloring for intervals. SODA: Symposium on Discrete Algorithms, 545–554.","apa":"Fiat, A., Levy, M., Matoušek, J., Pach, E., Sharir, M., Smorodinsky, S., … Welzl, E. (2005). Online conflict-free coloring for intervals (pp. 545–554). Presented at the SODA: Symposium on Discrete Algorithms, SIAM. https://doi.org/10.1137/S0097539704446682","ama":"Fiat A, Levy M, Matoušek J, et al. Online conflict-free coloring for intervals. In: SIAM; 2005:545-554. doi:10.1137/S0097539704446682","mla":"Fiat, Amos, et al. Online Conflict-Free Coloring for Intervals. SIAM, 2005, pp. 545–54, doi:10.1137/S0097539704446682.","short":"A. Fiat, M. Levy, J. Matoušek, E. Pach, M. Sharir, S. Smorodinsky, U. Wagner, E. Welzl, in:, SIAM, 2005, pp. 545–554.","chicago":"Fiat, Amos, Meital Levy, Jiří Matoušek, Elchanan Pach, Micha Sharir, Shakhar Smorodinsky, Uli Wagner, and Emo Welzl. “Online Conflict-Free Coloring for Intervals,” 545–54. SIAM, 2005. https://doi.org/10.1137/S0097539704446682.","ieee":"A. Fiat et al., “Online conflict-free coloring for intervals,” presented at the SODA: Symposium on Discrete Algorithms, 2005, pp. 545–554."},"author":[{"full_name":"Fiat, Amos","last_name":"Fiat","first_name":"Amos"},{"last_name":"Levy","first_name":"Meital","full_name":"Levy, Meital B"},{"last_name":"Matoušek","first_name":"Jiří","full_name":"Matoušek, Jiří"},{"last_name":"Pach","first_name":"Elchanan","full_name":"Pach, Elchanan M"},{"full_name":"Sharir, Micha","last_name":"Sharir","first_name":"Micha"},{"last_name":"Smorodinsky","first_name":"Shakhar","full_name":"Smorodinsky, Shakhar"},{"orcid":"0000-0002-1494-0568","full_name":"Uli Wagner","id":"36690CA2-F248-11E8-B48F-1D18A9856A87","last_name":"Wagner","first_name":"Uli"},{"last_name":"Welzl","first_name":"Emo","full_name":"Welzl, Emo"}],"month":"01"},{"year":"2005","volume":433,"type":"journal_article","quality_controlled":0,"title":"The PIN auxin efflux facilitator network controls growth and patterning in Arabidopsis roots","doi":"10.1038/nature03184","publisher":"Nature Publishing Group","date_updated":"2021-01-12T06:57:35Z","publication_status":"published","day":"01","status":"public","date_published":"2005-01-01T00:00:00Z","issue":"7021","publication":"Nature","publist_id":"4448","abstract":[{"text":"Local accumulation of the plant growth regulator auxin mediates pattern formation in Arabidopsis roots and influences outgrowth and development of lateral root- and shoot-derived primordia. However, it has remained unclear how auxin can simultaneously regulate patterning and organ outgrowth and how its distribution is stabilized in a primordium-specif ic manner. Here we show that five PIN genes collectively control auxin distribution to regulate cell division and cell expansion in the primary root. Furthermore, the joint action of these genes has an important role in pattern formation by focusing the auxin maximum and restricting the expression domain of PLETHORA (PLT) genes, major determinants for root stem cell specification. In turn, PLT genes are required for PIN gene transcription to stabilize the auxin maximum at the distal root tip. Our data reveal an interaction network of auxin transport facilitators and root fate determinants that control patterning and growth of the root primordium.","lang":"eng"}],"page":"39 - 44","_id":"2455","intvolume":" 433","month":"01","author":[{"full_name":"Billou, Ikram","first_name":"Ikram","last_name":"Billou"},{"full_name":"Xu, Jian","first_name":"Jian","last_name":"Xu"},{"full_name":"Wildwater, Marjolein","first_name":"Marjolein","last_name":"Wildwater"},{"full_name":"Willemsen, Viola","first_name":"Viola","last_name":"Willemsen"},{"first_name":"Ivan","last_name":"Paponov","full_name":"Paponov, Ivan A"},{"id":"4159519E-F248-11E8-B48F-1D18A9856A87","first_name":"Jirí","last_name":"Friml","orcid":"0000-0002-8302-7596","full_name":"Jirí Friml"},{"last_name":"Heldstra","first_name":"Renze","full_name":"Heldstra, Renze"},{"last_name":"Aida","first_name":"Mitsuhiro","full_name":"Aida, Mitsuhiro"},{"full_name":"Palme, Klaus J","first_name":"Klaus","last_name":"Palme"},{"full_name":"Scheres, Ben","last_name":"Scheres","first_name":"Ben"}],"citation":{"short":"I. Billou, J. Xu, M. Wildwater, V. Willemsen, I. Paponov, J. Friml, R. Heldstra, M. Aida, K. Palme, B. Scheres, Nature 433 (2005) 39–44.","mla":"Billou, Ikram, et al. “The PIN Auxin Efflux Facilitator Network Controls Growth and Patterning in Arabidopsis Roots.” Nature, vol. 433, no. 7021, Nature Publishing Group, 2005, pp. 39–44, doi:10.1038/nature03184.","ieee":"I. Billou et al., “The PIN auxin efflux facilitator network controls growth and patterning in Arabidopsis roots,” Nature, vol. 433, no. 7021. Nature Publishing Group, pp. 39–44, 2005.","chicago":"Billou, Ikram, Jian Xu, Marjolein Wildwater, Viola Willemsen, Ivan Paponov, Jiří Friml, Renze Heldstra, Mitsuhiro Aida, Klaus Palme, and Ben Scheres. “The PIN Auxin Efflux Facilitator Network Controls Growth and Patterning in Arabidopsis Roots.” Nature. Nature Publishing Group, 2005. https://doi.org/10.1038/nature03184.","apa":"Billou, I., Xu, J., Wildwater, M., Willemsen, V., Paponov, I., Friml, J., … Scheres, B. (2005). The PIN auxin efflux facilitator network controls growth and patterning in Arabidopsis roots. Nature. Nature Publishing Group. https://doi.org/10.1038/nature03184","ista":"Billou I, Xu J, Wildwater M, Willemsen V, Paponov I, Friml J, Heldstra R, Aida M, Palme K, Scheres B. 2005. The PIN auxin efflux facilitator network controls growth and patterning in Arabidopsis roots. Nature. 433(7021), 39–44.","ama":"Billou I, Xu J, Wildwater M, et al. The PIN auxin efflux facilitator network controls growth and patterning in Arabidopsis roots. Nature. 2005;433(7021):39-44. doi:10.1038/nature03184"},"date_created":"2018-12-11T11:57:46Z","extern":1},{"date_created":"2018-12-11T11:57:48Z","citation":{"ama":"Dubová J, Hejátko J, Friml J. Reproduction, plants. In: Meyers R, ed. Encyclopedia of Molecular Cell Biology and Molecular Medicine. Vol 12. Wiley-Blackwell; 2005:249-295. doi:10.1002/3527600906","apa":"Dubová, J., Hejátko, J., & Friml, J. (2005). Reproduction, plants. In R. Meyers (Ed.), Encyclopedia of Molecular Cell Biology and Molecular Medicine (Vol. 12, pp. 249–295). Wiley-Blackwell. https://doi.org/10.1002/3527600906","ista":"Dubová J, Hejátko J, Friml J. 2005.Reproduction, plants. In: Encyclopedia of Molecular Cell Biology and Molecular Medicine. vol. 12, 249–295.","ieee":"J. Dubová, J. Hejátko, and J. Friml, “Reproduction, plants,” in Encyclopedia of Molecular Cell Biology and Molecular Medicine, vol. 12, R. Meyers, Ed. Wiley-Blackwell, 2005, pp. 249–295.","chicago":"Dubová, J, Jan Hejátko, and Jiří Friml. “Reproduction, Plants.” In Encyclopedia of Molecular Cell Biology and Molecular Medicine, edited by Robert Meyers, 12:249–95. Wiley-Blackwell, 2005. https://doi.org/10.1002/3527600906.","short":"J. Dubová, J. Hejátko, J. Friml, in:, R. Meyers (Ed.), Encyclopedia of Molecular Cell Biology and Molecular Medicine, Wiley-Blackwell, 2005, pp. 249–295.","mla":"Dubová, J., et al. “Reproduction, Plants.” Encyclopedia of Molecular Cell Biology and Molecular Medicine, edited by Robert Meyers, vol. 12, Wiley-Blackwell, 2005, pp. 249–95, doi:10.1002/3527600906."},"extern":1,"month":"10","author":[{"full_name":"Dubová, J","first_name":"J","last_name":"Dubová"},{"full_name":"Hejátko, Jan","last_name":"Hejátko","first_name":"Jan"},{"first_name":"Jirí","last_name":"Friml","id":"4159519E-F248-11E8-B48F-1D18A9856A87","orcid":"0000-0002-8302-7596","full_name":"Jirí Friml"}],"intvolume":" 12","_id":"2463","status":"public","date_published":"2005-10-28T00:00:00Z","publist_id":"4440","publication":"Encyclopedia of Molecular Cell Biology and Molecular Medicine","page":"249 - 295","publisher":"Wiley-Blackwell","date_updated":"2021-01-12T06:57:38Z","publication_status":"published","day":"28","quality_controlled":0,"title":"Reproduction, plants","doi":"10.1002/3527600906","editor":[{"full_name":"Meyers, Robert A","first_name":"Robert","last_name":"Meyers"}],"volume":12,"type":"book_chapter","year":"2005"},{"_id":"2464","intvolume":" 16","publication":"Intercellular Communication in Plants","publist_id":"4439","date_published":"2005-01-13T00:00:00Z","status":"public","extern":1,"alternative_title":["Annual Plant Reviews"],"date_created":"2018-12-11T11:57:49Z","citation":{"ama":"Friml J, Wiśniewska J. Auxin as an intercellular signal. In: Fleming A, ed. Intercellular Communication in Plants. Vol 16. Wiley-Blackwell; 2005.","ista":"Friml J, Wiśniewska J. 2005.Auxin as an intercellular signal. In: Intercellular Communication in Plants. Annual Plant Reviews, vol. 16.","apa":"Friml, J., & Wiśniewska, J. (2005). Auxin as an intercellular signal. In A. Fleming (Ed.), Intercellular Communication in Plants (Vol. 16). Wiley-Blackwell.","chicago":"Friml, Jiří, and Justyna Wiśniewska. “Auxin as an Intercellular Signal.” In Intercellular Communication in Plants, edited by Andrew Fleming, Vol. 16. Wiley-Blackwell, 2005.","ieee":"J. Friml and J. Wiśniewska, “Auxin as an intercellular signal,” in Intercellular Communication in Plants, vol. 16, A. Fleming, Ed. Wiley-Blackwell, 2005.","short":"J. Friml, J. Wiśniewska, in:, A. Fleming (Ed.), Intercellular Communication in Plants, Wiley-Blackwell, 2005.","mla":"Friml, Jiří, and Justyna Wiśniewska. “Auxin as an Intercellular Signal.” Intercellular Communication in Plants, edited by Andrew Fleming, vol. 16, Wiley-Blackwell, 2005."},"author":[{"orcid":"0000-0002-8302-7596","full_name":"Jirí Friml","id":"4159519E-F248-11E8-B48F-1D18A9856A87","last_name":"Friml","first_name":"Jirí"},{"full_name":"Wiśniewska, Justyna","last_name":"Wiśniewska","first_name":"Justyna"}],"month":"01","type":"book_chapter","volume":16,"year":"2005","day":"13","publication_status":"published","date_updated":"2021-01-12T06:57:38Z","publisher":"Wiley-Blackwell","editor":[{"full_name":"Fleming, Andrew J.","first_name":"Andrew","last_name":"Fleming"}],"title":"Auxin as an intercellular signal","quality_controlled":0},{"quality_controlled":0,"title":"Glutamate and GABA receptor signalling in the developing brain","doi":"10.1016/j.neuroscience.2004.09.042","publisher":"Elsevier","date_updated":"2020-07-14T12:45:44Z","publication_status":"published","day":"01","year":"2005","volume":130,"type":"review","month":"01","author":[{"first_name":"Rafael","last_name":"Luján","full_name":"Luján, Rafael"},{"id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","last_name":"Shigemoto","first_name":"Ryuichi","full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444"},{"last_name":"López Bendito","first_name":"Guillermina","full_name":"López-Bendito, Guillermina"}],"citation":{"chicago":"Luján, Rafael, Ryuichi Shigemoto, and Guillermina López Bendito. “Glutamate and GABA Receptor Signalling in the Developing Brain.” Neuroscience. Elsevier, 2005. https://doi.org/10.1016/j.neuroscience.2004.09.042.","ieee":"R. Luján, R. Shigemoto, and G. López Bendito, “Glutamate and GABA receptor signalling in the developing brain,” Neuroscience, vol. 130, no. 3. Elsevier, pp. 567–580, 2005.","mla":"Luján, Rafael, et al. “Glutamate and GABA Receptor Signalling in the Developing Brain.” Neuroscience, vol. 130, no. 3, Elsevier, 2005, pp. 567–80, doi:10.1016/j.neuroscience.2004.09.042.","short":"R. Luján, R. Shigemoto, G. López Bendito, Neuroscience 130 (2005) 567–580.","ama":"Luján R, Shigemoto R, López Bendito G. Glutamate and GABA receptor signalling in the developing brain. Neuroscience. 2005;130(3):567-580. doi:10.1016/j.neuroscience.2004.09.042","ista":"Luján R, Shigemoto R, López Bendito G. 2005. Glutamate and GABA receptor signalling in the developing brain. Neuroscience. 130(3), 567–580.","apa":"Luján, R., Shigemoto, R., & López Bendito, G. (2005). Glutamate and GABA receptor signalling in the developing brain. Neuroscience. Elsevier. https://doi.org/10.1016/j.neuroscience.2004.09.042"},"date_created":"2018-12-11T11:58:51Z","extern":1,"date_published":"2005-01-01T00:00:00Z","status":"public","publication":"Neuroscience","issue":"3","publist_id":"4250","abstract":[{"lang":"eng","text":"Our understanding of the role played by neurotransmitter receptors in the developing brain has advanced in recent years. The major excitatory and inhibitory neurotransmitters in the brain, glutamate and GABA, activate both ionotropic (ligand-gated ion channels) and metabotropic (G protein-coupled) receptors, and are generally associated with neuronal communication in the mature brain. However, before the emergence of their role in neurotransmission in adulthood, they also act to influence earlier developmental events, some of which occur prior to synapse formation: such as proliferation, migration, differentiation or survival processes during neural development. To fulfill these actions in the constructing of the nervous system, different types of glutamate and GABA receptors need to be expressed both at the right time and at the right place. The identification by molecular cloning of 16 ionotropic glutamate receptor subunits, eight metabotropic glutamate receptor subtypes, 21 ionotropic and two metabotropic GABA receptor subunits, some of which exist in alternatively splice variants, has enriched our appreciation of how molecular diversity leads to functional diversity in the brain. It now appears that many different types of glutamate and GABA receptor subunits have prominent expression in the embryonic and/or postnatal brain, whereas others are mainly present in the adult brain. Although the significance of this differential expression of subunits is not fully understood, it appears that the change in subunit composition is essential for normal development in particular brain regions. This review focuses on emerging information relating to the expression and role of glutamatergic and GABAergic neurotransmitter receptors during prenatal and postnatal development."}],"page":"567 - 580","intvolume":" 130","_id":"2647"},{"citation":{"apa":"Luján, R., Albasanz, J., Shigemoto, R., & Juíz, J. (2005). Preferential localization of the hyperpolarization-activated cyclic nucleotide-gated cation channel subunit HCN1 in basket cell terminals of the rat cerebellum. European Journal of Neuroscience. Wiley-Blackwell. https://doi.org/10.1111/j.1460-9568.2005.04043.x","ista":"Luján R, Albasanz J, Shigemoto R, Juíz J. 2005. Preferential localization of the hyperpolarization-activated cyclic nucleotide-gated cation channel subunit HCN1 in basket cell terminals of the rat cerebellum. European Journal of Neuroscience. 21(8), 2073–2082.","ama":"Luján R, Albasanz J, Shigemoto R, Juíz J. Preferential localization of the hyperpolarization-activated cyclic nucleotide-gated cation channel subunit HCN1 in basket cell terminals of the rat cerebellum. European Journal of Neuroscience. 2005;21(8):2073-2082. doi:10.1111/j.1460-9568.2005.04043.x","short":"R. Luján, J. Albasanz, R. Shigemoto, J. Juíz, European Journal of Neuroscience 21 (2005) 2073–2082.","mla":"Luján, Rafael, et al. “Preferential Localization of the Hyperpolarization-Activated Cyclic Nucleotide-Gated Cation Channel Subunit HCN1 in Basket Cell Terminals of the Rat Cerebellum.” European Journal of Neuroscience, vol. 21, no. 8, Wiley-Blackwell, 2005, pp. 2073–82, doi:10.1111/j.1460-9568.2005.04043.x.","ieee":"R. Luján, J. Albasanz, R. Shigemoto, and J. Juíz, “Preferential localization of the hyperpolarization-activated cyclic nucleotide-gated cation channel subunit HCN1 in basket cell terminals of the rat cerebellum,” European Journal of Neuroscience, vol. 21, no. 8. Wiley-Blackwell, pp. 2073–2082, 2005.","chicago":"Luján, Rafael, José Albasanz, Ryuichi Shigemoto, and José Juíz. “Preferential Localization of the Hyperpolarization-Activated Cyclic Nucleotide-Gated Cation Channel Subunit HCN1 in Basket Cell Terminals of the Rat Cerebellum.” European Journal of Neuroscience. Wiley-Blackwell, 2005. https://doi.org/10.1111/j.1460-9568.2005.04043.x."},"date_created":"2018-12-11T11:58:52Z","extern":1,"author":[{"full_name":"Luján, Rafael","last_name":"Luján","first_name":"Rafael"},{"full_name":"Albasanz, José L","first_name":"José","last_name":"Albasanz"},{"orcid":"0000-0001-8761-9444","full_name":"Ryuichi Shigemoto","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","last_name":"Shigemoto","first_name":"Ryuichi"},{"full_name":"Juíz, José M","first_name":"José","last_name":"Juíz"}],"month":"04","intvolume":" 21","_id":"2648","publication":"European Journal of Neuroscience","issue":"8","publist_id":"4248","date_published":"2005-04-01T00:00:00Z","status":"public","page":"2073 - 2082","abstract":[{"lang":"eng","text":"Hyperpolarization-activated and cyclic nucleotide-gated (HCN) channels are involved in the control of neuronal excitability and plasticity. In this study, we used immunoblotting and immunohistochemical techniques to reveal the developmental expression and subcellular distribution of the HCN1 subunit in the cerebellar cortex. During postnatal development, the spatio-temporal expression of HCN1 correlated well with the morphological events occurring during the ontogenesis of cerebellar interneurons. Using immunoblotting techniques, HCN1 was weakly detected during the first postnatal week and continued to increase throughout postnatal development, peaking at postnatal day (P)15. At the light-microscopic level, HCN1 immunoreactivity was very weak until P7 whereas from P10-12 to adulthood it was strongly detected in the lower third of the molecular layer and in the Purkinje cell layer. HCN1 was present in axons running through the molecular layer and in the pericellular basket around Purkinje cells at P12, but in the periaxonal plexus (the pinceau) surrounding their initial segment only after P15. Using immunofluorescence, HCN1 colocalized with GAD65 and synaptophysin, demonstrating that the subunit was present in inhibitory axons and axon terminals. At the electron-microscopic level, in adulthood, HCN1 immunoparticles were detected at postsynaptic sites in basket and Purkinje cells but most immunoparticles were found at presynaptic sites in basket cell axons and in terminals. In the axon terminals, the distribution of HCN1 was relatively uniform along the extrasynaptic plasma membrane; this was confirmed using quantitative techniques. The present findings suggest that HCN1 channels may provide a significant route for modulating co-ordinated cerebellar synaptic transmission through basket cells."}],"date_updated":"2021-01-12T06:58:48Z","publisher":"Wiley-Blackwell","day":"01","publication_status":"published","quality_controlled":0,"doi":"10.1111/j.1460-9568.2005.04043.x","title":"Preferential localization of the hyperpolarization-activated cyclic nucleotide-gated cation channel subunit HCN1 in basket cell terminals of the rat cerebellum","type":"journal_article","volume":21,"year":"2005"},{"publist_id":"4249","publication":"Journal of Neuroscience","issue":"4","date_published":"2005-01-26T00:00:00Z","status":"public","page":"799 - 807","abstract":[{"text":"The number of ionotropic receptors in synapses is an essential factor for determining the efficacy of fast transmission. We estimated the number of functional AMPA receptors at single postsynaptic sites by a combination of two-photon uncaging of glutamate and the nonstationary fluctuation analysis in immature rat Purkinje cells (PCs), which receive a single type of excitatory input from climbing fibers. Areas of postsynaptic membrane specialization at the recorded synapses were measured by reconstruction of serial ultrathin sections. The number of functional AMPA receptors was proportional to the synaptic area with a density of ∼ 1280 receptors/μm 2. Moreover, highly sensitive freeze-fracture replica labeling revealed a homogeneous density of immunogold particles for AMPA receptors in synaptic sites (910 ± 36 particles/μm 2) and much lower density in extrasynaptic sites (19 ± 2 particles/μm 2) in the immature PCs. Our results indicate that in this developing synapse, the efficacy of transmission is determined by the synaptic area.","lang":"eng"}],"_id":"2649","intvolume":" 25","author":[{"full_name":"Tanaka, Junichi","first_name":"Junichi","last_name":"Tanaka"},{"full_name":"Matsuzaki, Masanori","first_name":"Masanori","last_name":"Matsuzaki"},{"first_name":"Etsuko","last_name":"Tarusawa","full_name":"Tarusawa, Etsuko"},{"full_name":"Momiyama, Akiko","last_name":"Momiyama","first_name":"Akiko"},{"first_name":"Elek","last_name":"Molnár","full_name":"Molnár, Elek"},{"last_name":"Kasai","first_name":"Haruo","full_name":"Kasai, Haruo"},{"orcid":"0000-0001-8761-9444","full_name":"Ryuichi Shigemoto","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","last_name":"Shigemoto","first_name":"Ryuichi"}],"month":"01","date_created":"2018-12-11T11:58:52Z","citation":{"ieee":"J. Tanaka et al., “Number and density of AMPA receptors in single synapses in immature cerebellum,” Journal of Neuroscience, vol. 25, no. 4. Society for Neuroscience, pp. 799–807, 2005.","chicago":"Tanaka, Junichi, Masanori Matsuzaki, Etsuko Tarusawa, Akiko Momiyama, Elek Molnár, Haruo Kasai, and Ryuichi Shigemoto. “Number and Density of AMPA Receptors in Single Synapses in Immature Cerebellum.” Journal of Neuroscience. Society for Neuroscience, 2005. https://doi.org/10.1523/JNEUROSCI.4256-04.2005.","short":"J. Tanaka, M. Matsuzaki, E. Tarusawa, A. Momiyama, E. Molnár, H. Kasai, R. Shigemoto, Journal of Neuroscience 25 (2005) 799–807.","mla":"Tanaka, Junichi, et al. “Number and Density of AMPA Receptors in Single Synapses in Immature Cerebellum.” Journal of Neuroscience, vol. 25, no. 4, Society for Neuroscience, 2005, pp. 799–807, doi:10.1523/JNEUROSCI.4256-04.2005.","ama":"Tanaka J, Matsuzaki M, Tarusawa E, et al. Number and density of AMPA receptors in single synapses in immature cerebellum. Journal of Neuroscience. 2005;25(4):799-807. doi:10.1523/JNEUROSCI.4256-04.2005","apa":"Tanaka, J., Matsuzaki, M., Tarusawa, E., Momiyama, A., Molnár, E., Kasai, H., & Shigemoto, R. (2005). Number and density of AMPA receptors in single synapses in immature cerebellum. Journal of Neuroscience. Society for Neuroscience. https://doi.org/10.1523/JNEUROSCI.4256-04.2005","ista":"Tanaka J, Matsuzaki M, Tarusawa E, Momiyama A, Molnár E, Kasai H, Shigemoto R. 2005. Number and density of AMPA receptors in single synapses in immature cerebellum. Journal of Neuroscience. 25(4), 799–807."},"extern":1,"year":"2005","type":"journal_article","volume":25,"quality_controlled":0,"doi":"10.1523/JNEUROSCI.4256-04.2005","title":"Number and density of AMPA receptors in single synapses in immature cerebellum","date_updated":"2021-01-12T06:58:48Z","publisher":"Society for Neuroscience","day":"26","publication_status":"published"},{"volume":21,"type":"journal_article","year":"2005","publication_status":"published","day":"01","publisher":"Wiley-Blackwell","date_updated":"2021-01-12T06:58:49Z","title":"GABAB and CB1 cannabinoid receptor expression identifies two types of septal cholinergic neurons","doi":"10.1111/j.1460-9568.2005.04146.x","quality_controlled":0,"_id":"2650","intvolume":" 21","abstract":[{"lang":"eng","text":"Septohippocampal cholinergic neurons play key roles in learning and memory processes, and in the generation of hippocampal theta rhythm. The range of receptors for endogenous modulators expressed on these neurons is unclear. Here we describe GABAB 1a/b receptor (GABABR) and type 1 cannabinoid receptor (CB1R) expression in rat septal cholinergic [i.e. choline acetyltransferase (ChAT)-positive] cells. Using double immunofluorescent staining, we found that almost two-thirds of the cholinergic cells in the rat medial septum were GABABR positive, and that these cells had significantly larger somata than did GABABR-negative cholinergic neurons. We detected CB1R labelling in somata after axonal protein transport was blocked by colchicine. In these animals about one-third of the cholinergic cells were CB1R positive. These cells again had larger somata than CB1R-negative cholinergic neurons. The analyses confirmed that the size of GABABR-positive and CB 1R-positive cholinergic cells were alike, and all CB 1R-positive cholinergic cells were GABABR positive as well. CB1R-positive cells were invariably ChAT positive. All retrogradely labelled septohippocampal cholinergic cells were positive for GABABR and at least half of them also for CB1R. These data shed light on the existence of at least two cholinergic cell types in the medial septum: one expresses GABABR and CB1R, has large somata and projects to the hippocampus, whereas the other is negative for GABABR and CB1R and has smaller somata. The results also suggest that cholinergic transmission in the hippocampus is fine-tuned by endocannabinoid signalling."}],"page":"3034 - 3042","date_published":"2005-06-01T00:00:00Z","status":"public","publist_id":"4247","issue":"11","publication":"European Journal of Neuroscience","extern":1,"date_created":"2018-12-11T11:58:52Z","citation":{"ama":"Nyíri G, Szabadits E, Cserép C, Mackie K, Shigemoto R, Freund T. GABAB and CB1 cannabinoid receptor expression identifies two types of septal cholinergic neurons. European Journal of Neuroscience. 2005;21(11):3034-3042. doi:10.1111/j.1460-9568.2005.04146.x","ista":"Nyíri G, Szabadits E, Cserép C, Mackie K, Shigemoto R, Freund T. 2005. GABAB and CB1 cannabinoid receptor expression identifies two types of septal cholinergic neurons. European Journal of Neuroscience. 21(11), 3034–3042.","apa":"Nyíri, G., Szabadits, E., Cserép, C., Mackie, K., Shigemoto, R., & Freund, T. (2005). GABAB and CB1 cannabinoid receptor expression identifies two types of septal cholinergic neurons. European Journal of Neuroscience. Wiley-Blackwell. https://doi.org/10.1111/j.1460-9568.2005.04146.x","chicago":"Nyíri, Gábor, Eszter Szabadits, Csaba Cserép, Ken Mackie, Ryuichi Shigemoto, and Tamás Freund. “GABAB and CB1 Cannabinoid Receptor Expression Identifies Two Types of Septal Cholinergic Neurons.” European Journal of Neuroscience. Wiley-Blackwell, 2005. https://doi.org/10.1111/j.1460-9568.2005.04146.x.","ieee":"G. Nyíri, E. Szabadits, C. Cserép, K. Mackie, R. Shigemoto, and T. Freund, “GABAB and CB1 cannabinoid receptor expression identifies two types of septal cholinergic neurons,” European Journal of Neuroscience, vol. 21, no. 11. Wiley-Blackwell, pp. 3034–3042, 2005.","mla":"Nyíri, Gábor, et al. “GABAB and CB1 Cannabinoid Receptor Expression Identifies Two Types of Septal Cholinergic Neurons.” European Journal of Neuroscience, vol. 21, no. 11, Wiley-Blackwell, 2005, pp. 3034–42, doi:10.1111/j.1460-9568.2005.04146.x.","short":"G. Nyíri, E. Szabadits, C. Cserép, K. Mackie, R. Shigemoto, T. Freund, European Journal of Neuroscience 21 (2005) 3034–3042."},"month":"06","author":[{"first_name":"Gábor","last_name":"Nyíri","full_name":"Nyíri, Gábor"},{"first_name":"Eszter","last_name":"Szabadits","full_name":"Szabadits, Eszter"},{"first_name":"Csaba","last_name":"Cserép","full_name":"Cserép, Csaba"},{"last_name":"Mackie","first_name":"Ken","full_name":"Mackie, Ken P"},{"id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","last_name":"Shigemoto","first_name":"Ryuichi","orcid":"0000-0001-8761-9444","full_name":"Ryuichi Shigemoto"},{"full_name":"Freund, Tamás F","first_name":"Tamás","last_name":"Freund"}]},{"day":"01","publication_status":"published","date_updated":"2021-01-12T06:58:50Z","publisher":"American Society of Andrology","doi":"10.2164/jandrol.04185","title":"Cellular localization of GABA and GABAB receptor subunit proteins during spermiogenesis in rat testis","quality_controlled":0,"type":"journal_article","volume":26,"year":"2005","extern":1,"date_created":"2018-12-11T11:58:52Z","citation":{"apa":"Kanbara, K., Okamoto, K., Nomura, S., Kaneko, T., Shigemoto, R., Azuma, H., … Watanabe, M. (2005). Cellular localization of GABA and GABAB receptor subunit proteins during spermiogenesis in rat testis. Journal of Andrology. American Society of Andrology. https://doi.org/10.2164/jandrol.04185","ista":"Kanbara K, Okamoto K, Nomura S, Kaneko T, Shigemoto R, Azuma H, Katsuoka Y, Watanabe M. 2005. Cellular localization of GABA and GABAB receptor subunit proteins during spermiogenesis in rat testis. Journal of Andrology. 26(4), 485–493.","ama":"Kanbara K, Okamoto K, Nomura S, et al. Cellular localization of GABA and GABAB receptor subunit proteins during spermiogenesis in rat testis. Journal of Andrology. 2005;26(4):485-493. doi:10.2164/jandrol.04185","mla":"Kanbara, Kiyoto, et al. “Cellular Localization of GABA and GABAB Receptor Subunit Proteins during Spermiogenesis in Rat Testis.” Journal of Andrology, vol. 26, no. 4, American Society of Andrology, 2005, pp. 485–93, doi:10.2164/jandrol.04185.","short":"K. Kanbara, K. Okamoto, S. Nomura, T. Kaneko, R. Shigemoto, H. Azuma, Y. Katsuoka, M. Watanabe, Journal of Andrology 26 (2005) 485–493.","ieee":"K. Kanbara et al., “Cellular localization of GABA and GABAB receptor subunit proteins during spermiogenesis in rat testis,” Journal of Andrology, vol. 26, no. 4. American Society of Andrology, pp. 485–493, 2005.","chicago":"Kanbara, Kiyoto, Keiko Okamoto, Sakashi Nomura, Takeshi Kaneko, Ryuichi Shigemoto, Haruhito Azuma, Yoji Katsuoka, and Masahiko Watanabe. “Cellular Localization of GABA and GABAB Receptor Subunit Proteins during Spermiogenesis in Rat Testis.” Journal of Andrology. American Society of Andrology, 2005. https://doi.org/10.2164/jandrol.04185."},"author":[{"last_name":"Kanbara","first_name":"Kiyoto","full_name":"Kanbara, Kiyoto"},{"full_name":"Okamoto, Keiko","last_name":"Okamoto","first_name":"Keiko"},{"first_name":"Sakashi","last_name":"Nomura","full_name":"Nomura, Sakashi"},{"first_name":"Takeshi","last_name":"Kaneko","full_name":"Kaneko, Takeshi"},{"full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444","last_name":"Shigemoto","first_name":"Ryuichi","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87"},{"last_name":"Azuma","first_name":"Haruhito","full_name":"Azuma, Haruhito"},{"full_name":"Katsuoka, Yoji","first_name":"Yoji","last_name":"Katsuoka"},{"first_name":"Masahiko","last_name":"Watanabe","full_name":"Watanabe, Masahiko"}],"month":"07","intvolume":" 26","_id":"2651","page":"485 - 493","abstract":[{"lang":"eng","text":"The GABAergic system, a major inhibitory regulator in the central nervous system, may also play important roles in peripheral nonneuronal tissues and cells. Recent studies showed that GABAB receptor is expressed in testis and sperm. To understand the role of the GABAergic system in spermiogenesis, we examined cellular localization of GABA and GABAB receptor subunits in rat spermatids by immunocytochemistry. Immunoreactivity for GABA was detected around acrosomal granules of spermatids during the Golgi and cap phases. GABAB(1) immunoreactivity was observed in the acrosomal vesicle of spermatids in Golgi phase, and during cap phase, this reactivity expanded to the entire region of the acrosome covering the nuclear membrane. The level of reactivity decreased gradually with maturation of spermatids. In contrast, GABAB(2) immunoreactivity was not observed in spermatids during Golgi phase but was detected in the equatorial region during cap phase. Both GABA immunoreactivity and GABAB(2) immunoreactivity were transferred to the residual cytoplasm during the release of spermatozoa. Electron microscopic immunocytochemistry revealed that, during cap phase, GABA and GABAB(1) were distributed within the whole acrosomal vesicle but not in the acrosomal granule. GABAB(2) immunoreactivity was observed in the narrow space between the inner acrosomal and nuclear membrane and was limited to the equatorial region of the spermatid head. These results indicate that the GABAergic system might be involved in regulation of spermiogenesis."}],"publication":"Journal of Andrology","issue":"4","publist_id":"4246","date_published":"2005-07-01T00:00:00Z","status":"public"},{"year":"2005","type":"journal_article","volume":25,"quality_controlled":0,"doi":"10.1523/JNEUROSCI.1135-05.2005","title":"Neurogliaform neurons form a novel inhibitory network in the hippocampal CA1 area","date_updated":"2021-01-12T06:58:50Z","publisher":"Society for Neuroscience","day":"20","publication_status":"published","issue":"29","publist_id":"4245","publication":"Journal of Neuroscience","date_published":"2005-07-20T00:00:00Z","status":"public","page":"6775 - 6786","abstract":[{"text":"We studied neurogliaform neurons in the stratum lacunosum moleculare of the CA1 hippocampal area. These interneurons have short stellate dendrites and an extensive axonal arbor mainly located in the stratum lacunosum moleculare. Single-cell reverse transcription-PCR showed that these neurons were GABAergic and that the majority expressed mRNA for neuropeptide Y. Most neurogliaform neurons tested were immunoreactive for α-actinin-2, and many stratum lacunosum moleculare interneurons coexpressed α-actinin-2 and neuropeptide Y. Neurogliaform neurons received monosynaptic, DNQX-sensitive excitatory input from the perforant path, and 40 Hz stimulation of this input evoked EPSCs displaying either depression or initial facilitation, followed by depression. Paired recordings performed between neurogliaform neurons showed that 85% of pairs were electrically connected and 70% were also connected via GABAergic synapses. Injection of sine waveforms into neurons during paired recordings resulted in transmission of the waveforms through the electrical synapse. Unitary IPSCs recorded from neurogliaform pairs readily fatigued, had a slow decay, and had a strong depression of the synaptic response at a 5 Hz stimulation frequency that was antagonized by the GABA B antagonist (2S)-3-[[(1S)-1-(3,4-dichlorophenyl)ethyl]amino-2-hydroxypropyl](phenylmethyl) phosphinic acid (CGP55845). The amplitude of the first IPSC during the 5 Hz stimulation was also increased by CGP55845, suggesting a tonic inhibition of synaptic transmission. A small unitary GABA B-mediated IPSC could also be detected, providing the first evidence for such a component between GABAergic interneurons. Electron microscopic localization of the GABA B1 subunit at neurogliaform synapses revealed the protein in both presynaptic and postsynaptic membranes. Our data disclose a novel interneuronal network well suited for modulating the flow of information between the entorhinal cortex and CA1 hippocampus.","lang":"eng"}],"intvolume":" 25","_id":"2652","author":[{"full_name":"Price, Christopher J","last_name":"Price","first_name":"Christopher"},{"last_name":"Cauli","first_name":"Bruno","full_name":"Cauli, Bruno"},{"last_name":"Kovács","first_name":"Endre","full_name":"Kovács, Endre R"},{"full_name":"Kulik, Ákos","first_name":"Ákos","last_name":"Kulik"},{"full_name":"Lambolez, Bertrand","first_name":"Bertrand","last_name":"Lambolez"},{"full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444","first_name":"Ryuichi","last_name":"Shigemoto","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87"},{"full_name":"Capogna,Marco","first_name":"Marco","last_name":"Capogna"}],"month":"07","citation":{"ieee":"C. Price et al., “Neurogliaform neurons form a novel inhibitory network in the hippocampal CA1 area,” Journal of Neuroscience, vol. 25, no. 29. Society for Neuroscience, pp. 6775–6786, 2005.","chicago":"Price, Christopher, Bruno Cauli, Endre Kovács, Ákos Kulik, Bertrand Lambolez, Ryuichi Shigemoto, and Marco Capogna. “Neurogliaform Neurons Form a Novel Inhibitory Network in the Hippocampal CA1 Area.” Journal of Neuroscience. Society for Neuroscience, 2005. https://doi.org/10.1523/JNEUROSCI.1135-05.2005.","short":"C. Price, B. Cauli, E. Kovács, Á. Kulik, B. Lambolez, R. Shigemoto, M. Capogna, Journal of Neuroscience 25 (2005) 6775–6786.","mla":"Price, Christopher, et al. “Neurogliaform Neurons Form a Novel Inhibitory Network in the Hippocampal CA1 Area.” Journal of Neuroscience, vol. 25, no. 29, Society for Neuroscience, 2005, pp. 6775–86, doi:10.1523/JNEUROSCI.1135-05.2005.","ama":"Price C, Cauli B, Kovács E, et al. Neurogliaform neurons form a novel inhibitory network in the hippocampal CA1 area. Journal of Neuroscience. 2005;25(29):6775-6786. doi:10.1523/JNEUROSCI.1135-05.2005","apa":"Price, C., Cauli, B., Kovács, E., Kulik, Á., Lambolez, B., Shigemoto, R., & Capogna, M. (2005). Neurogliaform neurons form a novel inhibitory network in the hippocampal CA1 area. Journal of Neuroscience. Society for Neuroscience. https://doi.org/10.1523/JNEUROSCI.1135-05.2005","ista":"Price C, Cauli B, Kovács E, Kulik Á, Lambolez B, Shigemoto R, Capogna M. 2005. Neurogliaform neurons form a novel inhibitory network in the hippocampal CA1 area. Journal of Neuroscience. 25(29), 6775–6786."},"date_created":"2018-12-11T11:58:53Z","extern":1},{"author":[{"last_name":"Hagiwara","first_name":"Akari","full_name":"Hagiwara, Akari"},{"full_name":"Fukazawa, Yugo","first_name":"Yugo","last_name":"Fukazawa"},{"first_name":"Maki","last_name":"Deguchi Tawarada","full_name":"Deguchi-Tawarada, Maki"},{"last_name":"Ohtsuka","first_name":"Toshihisa","full_name":"Ohtsuka, Toshihisa"},{"full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","last_name":"Shigemoto","first_name":"Ryuichi"}],"month":"08","extern":1,"citation":{"mla":"Hagiwara, Akari, et al. “Differential Distribution of Release-Related Proteins in the Hippocampal CA3 Area as Revealed by Freeze-Fracture Replica Labeling.” Journal of Comparative Neurology, vol. 489, no. 2, Wiley-Blackwell, 2005, pp. 195–216, doi:10.1002/cne.20633.","short":"A. Hagiwara, Y. Fukazawa, M. Deguchi Tawarada, T. Ohtsuka, R. Shigemoto, Journal of Comparative Neurology 489 (2005) 195–216.","chicago":"Hagiwara, Akari, Yugo Fukazawa, Maki Deguchi Tawarada, Toshihisa Ohtsuka, and Ryuichi Shigemoto. “Differential Distribution of Release-Related Proteins in the Hippocampal CA3 Area as Revealed by Freeze-Fracture Replica Labeling.” Journal of Comparative Neurology. Wiley-Blackwell, 2005. https://doi.org/10.1002/cne.20633.","ieee":"A. Hagiwara, Y. Fukazawa, M. Deguchi Tawarada, T. Ohtsuka, and R. Shigemoto, “Differential distribution of release-related proteins in the hippocampal CA3 area as revealed by freeze-fracture replica labeling,” Journal of Comparative Neurology, vol. 489, no. 2. Wiley-Blackwell, pp. 195–216, 2005.","ista":"Hagiwara A, Fukazawa Y, Deguchi Tawarada M, Ohtsuka T, Shigemoto R. 2005. Differential distribution of release-related proteins in the hippocampal CA3 area as revealed by freeze-fracture replica labeling. Journal of Comparative Neurology. 489(2), 195–216.","apa":"Hagiwara, A., Fukazawa, Y., Deguchi Tawarada, M., Ohtsuka, T., & Shigemoto, R. (2005). Differential distribution of release-related proteins in the hippocampal CA3 area as revealed by freeze-fracture replica labeling. Journal of Comparative Neurology. Wiley-Blackwell. https://doi.org/10.1002/cne.20633","ama":"Hagiwara A, Fukazawa Y, Deguchi Tawarada M, Ohtsuka T, Shigemoto R. Differential distribution of release-related proteins in the hippocampal CA3 area as revealed by freeze-fracture replica labeling. Journal of Comparative Neurology. 2005;489(2):195-216. doi:10.1002/cne.20633"},"date_created":"2018-12-11T11:58:53Z","page":"195 - 216","abstract":[{"lang":"eng","text":"Synaptic vesicle release occurs at a specialized membrane domain known as the presynaptic active zone (AZ). Several membrane proteins are involved in the vesicle release processes such as docking, priming, and exocytotic fusion. Cytomatrix at the active zone (CAZ) proteins are structural components of the AZ and are highly concentrated in it. Localization of other release-related proteins including target soluble N-ethylmaleimide-sensitive-factor attachment protein receptor (t-SNARE) proteins, however, has not been well demonstrated in the AZ. Here, we used sodium dodecyl sulfate-digested freeze-fracture replica labeling (SDS-FRL) to analyze quantitatively the distribution of CAZ and t-SNARE proteins in the hippocampal CA3 area. The AZ in replicated membrane was identified by immunolabeling for CAZ proteins (CAZ-associated structural protein [CAST] and Bassoon). Clusters of immunogold particles for these proteins were found on the P-face of presynaptic terminals of the mossy fiber and associational/commissural (AJC) fiber. Co-labeling with CAST revealed distribution of the t-SNARE proteins syntaxin and synaptosomal-associated protein of 25 kDa (SNAP-25) in the AZ as well as in the extrasynaptic membrane surrounding the AZ (SZ). Quantitative analysis demonstrated that the density of immunoparticles for CAST in the AZ was more than 100 times higher than in the SZ, whereas that for syntaxin and SNAP-25 was not significantly different between the AZ and SZ in both the A/C and mossy fiber terminals. These results support the involvement of the t-SNARE proteins in exocytotic fusion in the AZ and the role of CAST in specialization of the membrane domain for the AZ."}],"publication":"Journal of Comparative Neurology","issue":"2","publist_id":"4244","date_published":"2005-08-22T00:00:00Z","status":"public","_id":"2653","intvolume":" 489","doi":"10.1002/cne.20633","title":"Differential distribution of release-related proteins in the hippocampal CA3 area as revealed by freeze-fracture replica labeling","quality_controlled":0,"day":"22","publication_status":"published","date_updated":"2021-01-12T06:58:50Z","publisher":"Wiley-Blackwell","year":"2005","type":"journal_article","volume":489},{"intvolume":" 25","_id":"2654","abstract":[{"lang":"eng","text":"Presynaptic metabotropic glutamate receptors (mGluRs) show a highly selective expression and subcellular location in nerve terminals modulating neurotransmitter release. We have demonstrated that alternatively spliced variants of mGluR8, mGluR8a and mGluR8b, have an overlapping distribution in the hippocampus, and besides perforant path terminals, they are expressed in the presynaptic active zone of boutons making synapses selectively with several types of GABAergic interneurons, primarily in the stratum oriens. Boutons labeled for mGluR8 formed either type I or type II synapses, and the latter were GABAergic. Some mGluR8-positive boutons also expressed mGluR7 or vasoactive intestinal polypeptide. Interneurons strongly immunopositive for the muscarinic M2 or the mGlu1 receptors were the primary targets of mGluR8-containing terminals in the stratum oriens, but only neurochemically distinct subsets were innervated by mGluR8-enriched terminals. The majority of M2-positive neurons were mGluR8 innervated, but a minority, which expresses somatostatin, was not. Rare neurons coexpressing calretinin and M2 were consistently targeted by mGluR8-positive boutons. In vivo recording and labeling of an mGluR8-decorated and strongly M2-positive interneuron revealed a trilaminar cell with complex spike bursts during theta oscillations and strong discharge during sharp wave/ripple events. The trilaminar cell had a large projection from the CA1 area to the subiculum and a preferential innervation of interneurons in the CA1 area in addition to pyramidal cell somata and dendrites. The postsynaptic interneuron type-specific expression of the high-efficacy presynaptic mGluR8 in both putative glutamatergic and in identified GABAergic terminals predicts a role in adjusting the activity of interneurons depending on the level of network activity."}],"page":"10520 - 10536","status":"public","date_published":"2005-11-09T00:00:00Z","publication":"Journal of Neuroscience","publist_id":"4242","issue":"45","extern":1,"citation":{"ista":"Ferraguti F, Klausberger T, Cobden P, Baude A, Roberts J, Szűcs P, Kinoshita A, Shigemoto R, Somogyi P, Dalezios Y. 2005. Metabotropic glutamate receptor 8-expressing nerve terminals target subsets of GABAergic neurons in the hippocampus. Journal of Neuroscience. 25(45), 10520–10536.","apa":"Ferraguti, F., Klausberger, T., Cobden, P., Baude, A., Roberts, J., Szűcs, P., … Dalezios, Y. (2005). Metabotropic glutamate receptor 8-expressing nerve terminals target subsets of GABAergic neurons in the hippocampus. Journal of Neuroscience. Society for Neuroscience. https://doi.org/10.1523/JNEUROSCI.2547-05.2005","ama":"Ferraguti F, Klausberger T, Cobden P, et al. Metabotropic glutamate receptor 8-expressing nerve terminals target subsets of GABAergic neurons in the hippocampus. Journal of Neuroscience. 2005;25(45):10520-10536. doi:10.1523/JNEUROSCI.2547-05.2005","short":"F. Ferraguti, T. Klausberger, P. Cobden, A. Baude, J. Roberts, P. Szűcs, A. Kinoshita, R. Shigemoto, P. Somogyi, Y. Dalezios, Journal of Neuroscience 25 (2005) 10520–10536.","mla":"Ferraguti, Francesco, et al. “ Metabotropic Glutamate Receptor 8-Expressing Nerve Terminals Target Subsets of GABAergic Neurons in the Hippocampus.” Journal of Neuroscience, vol. 25, no. 45, Society for Neuroscience, 2005, pp. 10520–36, doi:10.1523/JNEUROSCI.2547-05.2005.","chicago":"Ferraguti, Francesco, Thomas Klausberger, Philip Cobden, Agnès Baude, John Roberts, Péter Szűcs, Ayae Kinoshita, Ryuichi Shigemoto, Péter Somogyi, and Yannis Dalezios. “ Metabotropic Glutamate Receptor 8-Expressing Nerve Terminals Target Subsets of GABAergic Neurons in the Hippocampus.” Journal of Neuroscience. Society for Neuroscience, 2005. https://doi.org/10.1523/JNEUROSCI.2547-05.2005.","ieee":"F. Ferraguti et al., “ Metabotropic glutamate receptor 8-expressing nerve terminals target subsets of GABAergic neurons in the hippocampus,” Journal of Neuroscience, vol. 25, no. 45. Society for Neuroscience, pp. 10520–10536, 2005."},"date_created":"2018-12-11T11:58:53Z","month":"11","author":[{"full_name":"Ferraguti, Francesco","first_name":"Francesco","last_name":"Ferraguti"},{"full_name":"Klausberger,Thomas","first_name":"Thomas","last_name":"Klausberger"},{"first_name":"Philip","last_name":"Cobden","full_name":"Cobden, Philip M"},{"last_name":"Baude","first_name":"Agnès","full_name":"Baude, Agnès"},{"first_name":"John","last_name":"Roberts","full_name":"Roberts, John D"},{"full_name":"Szűcs, Péter","last_name":"Szűcs","first_name":"Péter"},{"last_name":"Kinoshita","first_name":"Ayae","full_name":"Kinoshita, Ayae"},{"id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","first_name":"Ryuichi","last_name":"Shigemoto","orcid":"0000-0001-8761-9444","full_name":"Ryuichi Shigemoto"},{"full_name":"Somogyi, Péter","last_name":"Somogyi","first_name":"Péter"},{"full_name":"Dalezios, Yannis","first_name":"Yannis","last_name":"Dalezios"}],"volume":25,"type":"journal_article","year":"2005","publication_status":"published","day":"09","publisher":"Society for Neuroscience","date_updated":"2021-01-12T06:58:51Z","title":" Metabotropic glutamate receptor 8-expressing nerve terminals target subsets of GABAergic neurons in the hippocampus","doi":"10.1523/JNEUROSCI.2547-05.2005","quality_controlled":0},{"type":"journal_article","volume":25,"year":"2005","date_updated":"2021-01-12T06:58:51Z","publisher":"Society for Neuroscience","day":"05","publication_status":"published","quality_controlled":0,"doi":"10.1523/JNEUROSCI.2134-05.2005","title":"Target-cell-specific left-right asymmetry of NMDA receptor content in Schaffer collateral synapses in ε1/NR2A knock-out mice","_id":"2655","intvolume":" 25","issue":"40","publication":"Journal of Neuroscience","publist_id":"4243","status":"public","date_published":"2005-10-05T00:00:00Z","page":"9213 - 9226","abstract":[{"lang":"eng","text":"Input-dependent left-right asymmetry of NMDA receptor ε2 (NR2B) subunit allocation was discovered in hippocampal Schaffer collateral (Sch) and commissural fiber pyramidal cell synapses (Kawakami et al., 2003). To investigate whether this asymmetrical ε2 allocation is also related to the types of the postsynaptic cells, we compared postembedding immunogold labeling for ε2 in left and right Sch synapses on pyramidal cells and interneurons. To facilitate the detection of ε2 density difference, we used ε1 (NR2A) knock-out (KO) mice, which have a simplified NMDA receptor subunit composition. The labeling density for ε2 but not ζ1 (NR1) and subtype 2/3 glutamate receptor (GluR2/3) in Sch-CA1 pyramidal cell synapses was significantly different between the left and right hippocampus with opposite directions in strata oriens and radiatum; the left to right ratio of ε2 labeling density was 1:1.50 in stratum oriens and 1.44:1 in stratum radiatum. No significant difference, however, was detected in CA1 stratum radiatum between the left and right Sch-GluR4-positive (mostly parvalbumin-positive) and Sch-GluR4-negative interneuron synapses. Consistent with the anatomical asymmetry, the amplitude ratio of NMDA EPSCs to non-NMDA EPSCs in pyramidal cells was approximately two times larger in right than left stratum radiatum and vice versa in stratum oriens of ε1 KO mice. Moreover, the amplitude of long-term potentiation in the Sch-CA1 synapses of left stratum radiatum was significantly larger than that in the right corresponding synapses. These results indicate that the asymmetry of ε2 distribution is target cell specific, resulting in the left-right difference in NMDA receptor content and plasticity in Sch-CA1 pyramidal cell synapses in ε1 KO mice."}],"citation":{"mla":"Wu, Yue, et al. “Target-Cell-Specific Left-Right Asymmetry of NMDA Receptor Content in Schaffer Collateral Synapses in Ε1/NR2A Knock-out Mice.” Journal of Neuroscience, vol. 25, no. 40, Society for Neuroscience, 2005, pp. 9213–26, doi:10.1523/JNEUROSCI.2134-05.2005.","short":"Y. Wu, R. Kawakami, Y. Shinohara, M. Fukaya, K. Sakimura, M. Mishina, M. Watanabe, I. Ito, R. Shigemoto, Journal of Neuroscience 25 (2005) 9213–9226.","chicago":"Wu, Yue, Ryosuke Kawakami, Yoshiaki Shinohara, Masahiro Fukaya, Kenji Sakimura, Masayoshi Mishina, Masahiko Watanabe, Isao Ito, and Ryuichi Shigemoto. “Target-Cell-Specific Left-Right Asymmetry of NMDA Receptor Content in Schaffer Collateral Synapses in Ε1/NR2A Knock-out Mice.” Journal of Neuroscience. Society for Neuroscience, 2005. https://doi.org/10.1523/JNEUROSCI.2134-05.2005.","ieee":"Y. Wu et al., “Target-cell-specific left-right asymmetry of NMDA receptor content in Schaffer collateral synapses in ε1/NR2A knock-out mice,” Journal of Neuroscience, vol. 25, no. 40. Society for Neuroscience, pp. 9213–9226, 2005.","ista":"Wu Y, Kawakami R, Shinohara Y, Fukaya M, Sakimura K, Mishina M, Watanabe M, Ito I, Shigemoto R. 2005. Target-cell-specific left-right asymmetry of NMDA receptor content in Schaffer collateral synapses in ε1/NR2A knock-out mice. Journal of Neuroscience. 25(40), 9213–9226.","apa":"Wu, Y., Kawakami, R., Shinohara, Y., Fukaya, M., Sakimura, K., Mishina, M., … Shigemoto, R. (2005). Target-cell-specific left-right asymmetry of NMDA receptor content in Schaffer collateral synapses in ε1/NR2A knock-out mice. Journal of Neuroscience. Society for Neuroscience. https://doi.org/10.1523/JNEUROSCI.2134-05.2005","ama":"Wu Y, Kawakami R, Shinohara Y, et al. Target-cell-specific left-right asymmetry of NMDA receptor content in Schaffer collateral synapses in ε1/NR2A knock-out mice. Journal of Neuroscience. 2005;25(40):9213-9226. doi:10.1523/JNEUROSCI.2134-05.2005"},"date_created":"2018-12-11T11:58:54Z","extern":1,"author":[{"first_name":"Yue","last_name":"Wu","full_name":"Wu, Yue"},{"last_name":"Kawakami","first_name":"Ryosuke","full_name":"Kawakami, Ryosuke"},{"full_name":"Shinohara, Yoshiaki","first_name":"Yoshiaki","last_name":"Shinohara"},{"first_name":"Masahiro","last_name":"Fukaya","full_name":"Fukaya, Masahiro"},{"full_name":"Sakimura, Kenji","last_name":"Sakimura","first_name":"Kenji"},{"last_name":"Mishina","first_name":"Masayoshi","full_name":"Mishina, Masayoshi"},{"full_name":"Watanabe, Masahiko","last_name":"Watanabe","first_name":"Masahiko"},{"first_name":"Isao","last_name":"Ito","full_name":"Ito, Isao"},{"full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","first_name":"Ryuichi","last_name":"Shigemoto"}],"month":"10"},{"author":[{"full_name":"Feng, Yu-Peng","last_name":"Feng","first_name":"Yu"},{"full_name":"Li, Yun-Qing","last_name":"Li","first_name":"Yun"},{"full_name":"Wang, Wen","last_name":"Wang","first_name":"Wen"},{"full_name":"Wu, Sheng-Xi","first_name":"Sheng","last_name":"Wu"},{"full_name":"Chen, Tao","last_name":"Chen","first_name":"Tao"},{"full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444","id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","first_name":"Ryuichi","last_name":"Shigemoto"},{"last_name":"Mizuno","first_name":"Noboru","full_name":"Mizuno, Noboru"}],"month":"11","extern":1,"citation":{"short":"Y. Feng, Y. Li, W. Wang, S. Wu, T. Chen, R. Shigemoto, N. Mizuno, Neuroscience Letters 388 (2005) 144–148.","mla":"Feng, Yu, et al. “Morphological Evidence for GABA/Glycine-Cocontaining Terminals in Synaptic Contact with Neurokinin-1 Receptor-Expressing Neurons in the Sacral Dorsal Commissural Nucleus of the Rat.” Neuroscience Letters, vol. 388, no. 3, Elsevier, 2005, pp. 144–48, doi:10.1016/j.neulet.2005.06.068.","ieee":"Y. Feng et al., “Morphological evidence for GABA/glycine-cocontaining terminals in synaptic contact with neurokinin-1 receptor-expressing neurons in the sacral dorsal commissural nucleus of the rat,” Neuroscience Letters, vol. 388, no. 3. Elsevier, pp. 144–148, 2005.","chicago":"Feng, Yu, Yun Li, Wen Wang, Sheng Wu, Tao Chen, Ryuichi Shigemoto, and Noboru Mizuno. “Morphological Evidence for GABA/Glycine-Cocontaining Terminals in Synaptic Contact with Neurokinin-1 Receptor-Expressing Neurons in the Sacral Dorsal Commissural Nucleus of the Rat.” Neuroscience Letters. Elsevier, 2005. https://doi.org/10.1016/j.neulet.2005.06.068.","apa":"Feng, Y., Li, Y., Wang, W., Wu, S., Chen, T., Shigemoto, R., & Mizuno, N. (2005). Morphological evidence for GABA/glycine-cocontaining terminals in synaptic contact with neurokinin-1 receptor-expressing neurons in the sacral dorsal commissural nucleus of the rat. Neuroscience Letters. Elsevier. https://doi.org/10.1016/j.neulet.2005.06.068","ista":"Feng Y, Li Y, Wang W, Wu S, Chen T, Shigemoto R, Mizuno N. 2005. Morphological evidence for GABA/glycine-cocontaining terminals in synaptic contact with neurokinin-1 receptor-expressing neurons in the sacral dorsal commissural nucleus of the rat. Neuroscience Letters. 388(3), 144–148.","ama":"Feng Y, Li Y, Wang W, et al. Morphological evidence for GABA/glycine-cocontaining terminals in synaptic contact with neurokinin-1 receptor-expressing neurons in the sacral dorsal commissural nucleus of the rat. Neuroscience Letters. 2005;388(3):144-148. doi:10.1016/j.neulet.2005.06.068"},"date_created":"2018-12-11T11:58:54Z","page":"144 - 148","abstract":[{"text":"Previous studies have shown that neurons in the sacral dorsal commissural nucleus (SDCN) express neurokinin-1 receptor (NK1R) and can be modulated by the co-release of GABA and glycine (Gly) from single presynaptic terminal. These results raise the possibility that GABA/Gly-cocontaining terminals might make synaptic contacts with NK1R-expressing neurons in the SDCN. In order to provide morphological evidence for this hypothesis, the triple-immunohistochemical studies were performed in the SDCN. Triple-immunofluorescence histochemical study showed that some axon terminals in close association with NK1R-immunopositive (NK1R-ip) neurons in the SDCN were immunopositive for both glutamic acid decarboxylase (GAD) and glycine transporter 2 (GlyT2). In electron microscopic dual- and triple-immunohistochemistry for GAD/GlyT2, GAD/NK1R, GlyT2/NK1R, or GAD/GlyT2/NK1R also revealed dually labeled (GAD/GlyT2-ip) synaptic terminals upon SDCN neurons, as well as GAD- and/or GlyT2-ip axon terminals in synaptic contact with NK1R-ip SDCN neurons. These results suggested that some synaptic terminals upon NK1R-expressing SDCN neurons co-released both GABA and Gly.","lang":"eng"}],"publist_id":"4241","issue":"3","publication":"Neuroscience Letters","status":"public","date_published":"2005-11-18T00:00:00Z","_id":"2656","intvolume":" 388","doi":"10.1016/j.neulet.2005.06.068","title":"Morphological evidence for GABA/glycine-cocontaining terminals in synaptic contact with neurokinin-1 receptor-expressing neurons in the sacral dorsal commissural nucleus of the rat","quality_controlled":0,"day":"18","publication_status":"published","date_updated":"2021-01-12T06:58:51Z","publisher":"Elsevier","year":"2005","type":"journal_article","volume":388},{"publication":"European Journal of Neuroscience","publist_id":"4240","issue":"12","status":"public","date_published":"2005-12-01T00:00:00Z","page":"3241 - 3254","abstract":[{"lang":"eng","text":"Enhanced glutamatergic neurotransmission via the subthalamopallidal or subthalamonigral projection seems crucial for developing parkinsonian motor signs. In the present study, the possible changes in the expression of metabotropic glutamate receptors (mGluRs) were examined in the basal ganglia of a primate model for Parkinson's disease. When the patterns of immunohistochemical localization of mGluRs in monkeys administered systemically with 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) were analysed in comparison with normal controls, we found that expression of mGluR1α, but not of other subtypes, was significantly reduced in the internal and external segments of the globus pallidus and the substantia nigra pars reticulata. To elucidate the functional role of mGluR1 in the control of pallidal neuron activity, extracellular unit recordings combined with intrapallidal microinjections of mGluR1-related agents were then performed in normal and parkinsonian monkeys. In normal awake conditions, the spontaneous firing rates of neurons in the pallidal complex were increased by DHPG, a selective agonist of group I mGluRs, whereas they were decreased by AIDA, a selective antagonist of group I mGluRs, or LY367385, a selective antagonist of mGluR1. These electrophysiological data strongly indicate that the excitatory mechanism of pallidal neurons by glutamate is mediated at least partly through mGluR1. The effects of the mGluR1-related agents on neuronal firing in the internal pallidal segment became rather obscure after MPTP treatment. Our results suggest that the specific down-regulation of pallidal and nigral mGluR1 ot in the parkinsonian state may exert a compensatory action to reverse the overactivity of the subthalamic nucleus-derived glutamatergic input that is generated in the disease."}],"intvolume":" 22","_id":"2658","author":[{"first_name":"Katsuyuki","last_name":"Kaneda","full_name":"Kaneda, Katsuyuki"},{"last_name":"Tachibana","first_name":"Yoshihisa","full_name":"Tachibana, Yoshihisa"},{"first_name":"Michiko","last_name":"Imanishi","full_name":"Imanishi, Michiko"},{"first_name":"Hitoshi","last_name":"Kita","full_name":"Kita, Hitoshi"},{"id":"499F3ABC-F248-11E8-B48F-1D18A9856A87","last_name":"Shigemoto","first_name":"Ryuichi","full_name":"Ryuichi Shigemoto","orcid":"0000-0001-8761-9444"},{"full_name":"Nambu, Atsushi","first_name":"Atsushi","last_name":"Nambu"},{"last_name":"Takada","first_name":"Masahiko","full_name":"Takada, Masahiko"}],"month":"12","date_created":"2018-12-11T11:58:55Z","citation":{"apa":"Kaneda, K., Tachibana, Y., Imanishi, M., Kita, H., Shigemoto, R., Nambu, A., & Takada, M. (2005). Down-regulation of metabotropic glutamate receptor 1α in globus pallidus and substantia nigra of parkinsonian monkeys. European Journal of Neuroscience. Wiley-Blackwell. https://doi.org/10.1111/j.1460-9568.2005.04488.x","ista":"Kaneda K, Tachibana Y, Imanishi M, Kita H, Shigemoto R, Nambu A, Takada M. 2005. Down-regulation of metabotropic glutamate receptor 1α in globus pallidus and substantia nigra of parkinsonian monkeys. European Journal of Neuroscience. 22(12), 3241–3254.","ama":"Kaneda K, Tachibana Y, Imanishi M, et al. Down-regulation of metabotropic glutamate receptor 1α in globus pallidus and substantia nigra of parkinsonian monkeys. European Journal of Neuroscience. 2005;22(12):3241-3254. doi:10.1111/j.1460-9568.2005.04488.x","short":"K. Kaneda, Y. Tachibana, M. Imanishi, H. Kita, R. Shigemoto, A. Nambu, M. Takada, European Journal of Neuroscience 22 (2005) 3241–3254.","mla":"Kaneda, Katsuyuki, et al. “Down-Regulation of Metabotropic Glutamate Receptor 1α in Globus Pallidus and Substantia Nigra of Parkinsonian Monkeys.” European Journal of Neuroscience, vol. 22, no. 12, Wiley-Blackwell, 2005, pp. 3241–54, doi:10.1111/j.1460-9568.2005.04488.x.","ieee":"K. Kaneda et al., “Down-regulation of metabotropic glutamate receptor 1α in globus pallidus and substantia nigra of parkinsonian monkeys,” European Journal of Neuroscience, vol. 22, no. 12. Wiley-Blackwell, pp. 3241–3254, 2005.","chicago":"Kaneda, Katsuyuki, Yoshihisa Tachibana, Michiko Imanishi, Hitoshi Kita, Ryuichi Shigemoto, Atsushi Nambu, and Masahiko Takada. “Down-Regulation of Metabotropic Glutamate Receptor 1α in Globus Pallidus and Substantia Nigra of Parkinsonian Monkeys.” European Journal of Neuroscience. Wiley-Blackwell, 2005. https://doi.org/10.1111/j.1460-9568.2005.04488.x."},"extern":1,"year":"2005","type":"journal_article","volume":22,"quality_controlled":0,"doi":"10.1111/j.1460-9568.2005.04488.x","title":"Down-regulation of metabotropic glutamate receptor 1α in globus pallidus and substantia nigra of parkinsonian monkeys","date_updated":"2021-01-12T06:58:52Z","publisher":"Wiley-Blackwell","day":"01","publication_status":"published"},{"type":"journal_article","volume":6,"year":"2005","day":"01","publication_status":"published","date_updated":"2021-01-12T06:59:24Z","publisher":"Birkhäuser","doi":"10.1007/s00023-005-0205-0","title":"Existence of the D0-D4 bound state: A detailed proof","quality_controlled":0,"intvolume":" 6","_id":"2743","page":"247 - 267","abstract":[{"lang":"eng","text":"We consider the supersymmetric quantum mechanical system which is obtained by dimensionally reducing d = 6, N = 1 supersymmetric gauge theory with gauge group U(1) and a single charged hypermultiplet. Using the deformation method and ideas introduced by Porrati and Rozenberg [1], we present a detailed proof of the existence of a normalizable ground state for this system."}],"publication":"Annales Henri Poincare","issue":"2","publist_id":"4149","status":"public","date_published":"2005-04-01T00:00:00Z","extern":1,"citation":{"ista":"Erdös L, Hasler D, Solovej J. 2005. Existence of the D0-D4 bound state: A detailed proof. Annales Henri Poincare. 6(2), 247–267.","apa":"Erdös, L., Hasler, D., & Solovej, J. (2005). Existence of the D0-D4 bound state: A detailed proof. Annales Henri Poincare. Birkhäuser. https://doi.org/10.1007/s00023-005-0205-0","ama":"Erdös L, Hasler D, Solovej J. Existence of the D0-D4 bound state: A detailed proof. Annales Henri Poincare. 2005;6(2):247-267. doi:10.1007/s00023-005-0205-0","mla":"Erdös, László, et al. “Existence of the D0-D4 Bound State: A Detailed Proof.” Annales Henri Poincare, vol. 6, no. 2, Birkhäuser, 2005, pp. 247–67, doi:10.1007/s00023-005-0205-0.","short":"L. Erdös, D. Hasler, J. Solovej, Annales Henri Poincare 6 (2005) 247–267.","chicago":"Erdös, László, David Hasler, and Jan Solovej. “Existence of the D0-D4 Bound State: A Detailed Proof.” Annales Henri Poincare. Birkhäuser, 2005. https://doi.org/10.1007/s00023-005-0205-0.","ieee":"L. Erdös, D. Hasler, and J. Solovej, “Existence of the D0-D4 bound state: A detailed proof,” Annales Henri Poincare, vol. 6, no. 2. Birkhäuser, pp. 247–267, 2005."},"date_created":"2018-12-11T11:59:22Z","author":[{"full_name":"László Erdös","orcid":"0000-0001-5366-9603","first_name":"László","last_name":"Erdös","id":"4DBD5372-F248-11E8-B48F-1D18A9856A87"},{"full_name":"Hasler, David G","first_name":"David","last_name":"Hasler"},{"first_name":"Jan","last_name":"Solovej","full_name":"Solovej, Jan P"}],"month":"04"},{"publisher":"World Scientific Publishing","date_updated":"2021-01-12T06:59:25Z","publication_status":"published","day":"01","quality_controlled":0,"title":"The linear Boltzmann equation as the low density limit of a random Schrödinger equation","doi":"10.1142/S0129055X0500242X","volume":17,"type":"journal_article","year":"2005","date_created":"2018-12-11T11:59:22Z","citation":{"ama":"Eng D, Erdös L. The linear Boltzmann equation as the low density limit of a random Schrödinger equation. Reviews in Mathematical Physics. 2005;17(6):669-743. doi:10.1142/S0129055X0500242X","apa":"Eng, D., & Erdös, L. (2005). The linear Boltzmann equation as the low density limit of a random Schrödinger equation. Reviews in Mathematical Physics. World Scientific Publishing. https://doi.org/10.1142/S0129055X0500242X","ista":"Eng D, Erdös L. 2005. The linear Boltzmann equation as the low density limit of a random Schrödinger equation. Reviews in Mathematical Physics. 17(6), 669–743.","ieee":"D. Eng and L. Erdös, “The linear Boltzmann equation as the low density limit of a random Schrödinger equation,” Reviews in Mathematical Physics, vol. 17, no. 6. World Scientific Publishing, pp. 669–743, 2005.","chicago":"Eng, David, and László Erdös. “The Linear Boltzmann Equation as the Low Density Limit of a Random Schrödinger Equation.” Reviews in Mathematical Physics. World Scientific Publishing, 2005. https://doi.org/10.1142/S0129055X0500242X.","short":"D. Eng, L. Erdös, Reviews in Mathematical Physics 17 (2005) 669–743.","mla":"Eng, David, and László Erdös. “The Linear Boltzmann Equation as the Low Density Limit of a Random Schrödinger Equation.” Reviews in Mathematical Physics, vol. 17, no. 6, World Scientific Publishing, 2005, pp. 669–743, doi:10.1142/S0129055X0500242X."},"extern":1,"month":"07","author":[{"last_name":"Eng","first_name":"David","full_name":"Eng, David"},{"first_name":"László","last_name":"Erdös","id":"4DBD5372-F248-11E8-B48F-1D18A9856A87","full_name":"László Erdös","orcid":"0000-0001-5366-9603"}],"intvolume":" 17","_id":"2744","status":"public","date_published":"2005-07-01T00:00:00Z","publication":"Reviews in Mathematical Physics","issue":"6","publist_id":"4148","abstract":[{"lang":"eng","text":"We study the long time evolution of a quantum particle interacting with a random potential in the Boltzmann-Grad low density limit. We prove that the phase space density of the quantum evolution defined through the Husimi function converges weakly to a linear Boltzmann equation. The Boltzmann collision kernel is given by the full quantum scattering cross-section of the obstacle potential."}],"page":"669 - 743"},{"quality_controlled":0,"title":"Turbulence regeneration in pipe flow at moderate reynolds numbers","doi":"10.1103/PhysRevLett.95.214502","publisher":"American Physical Society","date_updated":"2021-01-12T06:59:43Z","publication_status":"published","day":"17","year":"2005","volume":95,"type":"journal_article","month":"11","author":[{"id":"3A374330-F248-11E8-B48F-1D18A9856A87","first_name":"Björn","last_name":"Hof","orcid":"0000-0003-2057-2754","full_name":"Björn Hof"},{"first_name":"Casimir","last_name":"Van Doorne","full_name":"van Doorne, Casimir W"},{"full_name":"Westerweel, Jerry","first_name":"Jerry","last_name":"Westerweel"},{"first_name":"Frans","last_name":"Nieuwstadt","full_name":"Nieuwstadt, Frans T"}],"citation":{"ama":"Hof B, Van Doorne C, Westerweel J, Nieuwstadt F. Turbulence regeneration in pipe flow at moderate reynolds numbers. Physical Review Letters. 2005;95(21). doi:10.1103/PhysRevLett.95.214502","apa":"Hof, B., Van Doorne, C., Westerweel, J., & Nieuwstadt, F. (2005). Turbulence regeneration in pipe flow at moderate reynolds numbers. Physical Review Letters. American Physical Society. https://doi.org/10.1103/PhysRevLett.95.214502","ista":"Hof B, Van Doorne C, Westerweel J, Nieuwstadt F. 2005. Turbulence regeneration in pipe flow at moderate reynolds numbers. Physical Review Letters. 95(21).","ieee":"B. Hof, C. Van Doorne, J. Westerweel, and F. Nieuwstadt, “Turbulence regeneration in pipe flow at moderate reynolds numbers,” Physical Review Letters, vol. 95, no. 21. American Physical Society, 2005.","chicago":"Hof, Björn, Casimir Van Doorne, Jerry Westerweel, and Frans Nieuwstadt. “Turbulence Regeneration in Pipe Flow at Moderate Reynolds Numbers.” Physical Review Letters. American Physical Society, 2005. https://doi.org/10.1103/PhysRevLett.95.214502.","mla":"Hof, Björn, et al. “Turbulence Regeneration in Pipe Flow at Moderate Reynolds Numbers.” Physical Review Letters, vol. 95, no. 21, American Physical Society, 2005, doi:10.1103/PhysRevLett.95.214502.","short":"B. Hof, C. Van Doorne, J. Westerweel, F. Nieuwstadt, Physical Review Letters 95 (2005)."},"date_created":"2018-12-11T11:59:36Z","extern":1,"date_published":"2005-11-17T00:00:00Z","status":"public","publication":"Physical Review Letters","issue":"21","publist_id":"4101","abstract":[{"lang":"eng","text":"We present the results of an experimental investigation into the nature and structure of turbulent pipe flow at moderate Reynolds numbers. A turbulence regeneration mechanism is identified which sustains a symmetric traveling wave within the flow. The periodicity of the mechanism allows comparison to the wavelength of numerically observed exact traveling wave solutions and close agreement is found. The advection speed of the upstream turbulence laminar interface in the experimental flow is observed to form a lower bound on the phase velocities of the exact traveling wave solutions. Overall our observations suggest that the dynamics of the turbulent flow at moderate Reynolds numbers are governed by unstable nonlinear traveling waves."}],"_id":"2788","intvolume":" 95"}]