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49 results on '"Rohlmann, Astrid"'

6. Protein mutated in paroxysmal dyskinesia interacts with the active zone protein RIM and suppresses synaptic vesicle exocytosis.

Author

Shen, Yiguo, Ge, Woo-Ping, Li, Yulong, Hirano, Arisa, Lee, Hsien-Yang, Rohlmann, Astrid, Missler, Markus, Tsien, Richard, Ptáček, Louis, Fu, Ying-hui, and Jan, Lily

Subjects
exocytosis, neurological disease, paroxysmal dyskinesia, ATP-Binding Cassette Transporters, Animals, Chorea, Exocytosis, Mice, Mice, Knockout, Muscle Proteins, Protein Binding, Synaptic Vesicles
Abstract

Paroxysmal nonkinesigenic dyskinesia (PNKD) is an autosomal dominant episodic movement disorder precipitated by coffee, alcohol, and stress. We previously identified the causative gene but the function of the encoded protein remains unknown. We also generated a PNKD mouse model that revealed dysregulated dopamine signaling in vivo. Here, we show that PNKD interacts with synaptic active zone proteins Rab3-interacting molecule (RIM)1 and RIM2, localizes to synapses, and modulates neurotransmitter release. Overexpressed PNKD protein suppresses release, and mutant PNKD protein is less effective than wild-type at inhibiting exocytosis. In PNKD KO mice, RIM1/2 protein levels are reduced and synaptic strength is impaired. Thus, PNKD is a novel synaptic protein with a regulatory role in neurotransmitter release.

Published
2015

15. An extracellular vesicle-related gene expression signature identifies high-risk patients in medulloblastoma

Author

Albert, Thomas K, primary, Interlandi, Marta, additional, Sill, Martin, additional, Graf, Monika, additional, Moreno, Natalia, additional, Menck, Kerstin, additional, Rohlmann, Astrid, additional, Melcher, Viktoria, additional, Korbanka, Sonja, additional, Meyer zu Hörste, Gerd, additional, Lautwein, Tobias, additional, Frühwald, Michael C, additional, Krebs, Christian F, additional, Holdhof, Dörthe, additional, Schoof, Melanie, additional, Bleckmann, Annalen, additional, Missler, Markus, additional, Dugas, Martin, additional, Schüller, Ulrich, additional, Jäger, Natalie, additional, Pfister, Stefan M, additional, and Kerl, Kornelius, additional

Published
2020
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16. α-Neurexins couple Ca2+ channels to synaptic vesicle exocytosis

Author

Missler, Markus, Zhang, Weiqi, Rohlmann, Astrid, Kattenstroth, Gunnar, Hammer, Robert E., Gottmann, Kurt, and Sudhof, Thomas C.

Subjects
Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Author(s): Markus Missler (corresponding author) [1, 2, 3]; Weiqi Zhang [3]; Astrid Rohlmann [3]; Gunnar Kattenstroth [4]; Robert E. Hammer [2, 5]; Kurt Gottmann [4]; Thomas C. Südhof (corresponding author) [...]

Published
2003
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17. Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development

Author

Bikbaev, Arthur, primary, Ciuraszkiewicz-Wojciech, Anna, additional, Heck, Jennifer, additional, Klatt, Oliver, additional, Freund, Romy, additional, Mitlöhner, Jessica, additional, Enrile Lacalle, Sara, additional, Sun, Miao, additional, Repetto, Daniele, additional, Frischknecht, Renato, additional, Ablinger, Cornelia, additional, Rohlmann, Astrid, additional, Missler, Markus, additional, Obermair, Gerald J., additional, Di Biase, Valentina, additional, and Heine, Martin, additional

Published
2020
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20. An extracellular vesicle-related gene expression signature identifies high-risk patients in medulloblastoma.

Author

Albert, Thomas K, Interlandi, Marta, Sill, Martin, Graf, Monika, Moreno, Natalia, Menck, Kerstin, Rohlmann, Astrid, Melcher, Viktoria, Korbanka, Sonja, Hörste, Gerd Meyer zu, Lautwein, Tobias, Frühwald, Michael C, Krebs, Christian F, Holdhof, Dörthe, Schoof, Melanie, Bleckmann, Annalen, Missler, Markus, Dugas, Martin, Schüller, Ulrich, and Jäger, Natalie

Published
2021
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22. Human CCR5high effector memory cells perform CNS parenchymal immune surveillance via GZMK-mediated transendothelial diapedesis

Author

Herich, Sebastian, primary, Schneider-Hohendorf, Tilman, additional, Rohlmann, Astrid, additional, Khaleghi Ghadiri, Maryam, additional, Schulte-Mecklenbeck, Andreas, additional, Zondler, Lisa, additional, Janoschka, Claudia, additional, Ostkamp, Patrick, additional, Richter, Jannis, additional, Breuer, Johanna, additional, Dimitrov, Stoyan, additional, Rammensee, Hans-Georg, additional, Grauer, Oliver M, additional, Klotz, Luisa, additional, Gross, Catharina C, additional, Stummer, Walter, additional, Missler, Markus, additional, Zarbock, Alexander, additional, Vestweber, Dietmar, additional, Wiendl, Heinz, additional, and Schwab, Nicholas, additional

Published
2019
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25. Differential response to endothelial epithelial sodium channel inhibition ex vivo correlates with arterial stiffness in humans

Author

Lenders, Malte, primary, Hofschröer, Verena, additional, Schmitz, Boris, additional, Kasprzak, Bernd, additional, Rohlmann, Astrid, additional, Missler, Markus, additional, Pavenstädt, Hermann, additional, Oberleithner, Hans, additional, Brand, Stefan-Martin, additional, Kusche-Vihrog, Kristina, additional, and Brand, Eva, additional

Published
2015
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28. Dendritic spine formation and synaptic function require neurobeachin

Author

Niesmann, Katharina, Breuer, Dorothee, Brockhaus, Johannes, Born, Gesche, Wolff, Ilka, Reissner, Carsten, Kilimann, Manfred W., Rohlmann, Astrid, Missler, Markus, Niesmann, Katharina, Breuer, Dorothee, Brockhaus, Johannes, Born, Gesche, Wolff, Ilka, Reissner, Carsten, Kilimann, Manfred W., Rohlmann, Astrid, and Missler, Markus

Abstract

A challenge in neuroscience is to understand the mechanisms underlying synapse formation. Most excitatory synapses in the brain are built on spines, which are actin-rich protrusions from dendrites. Spines are a major substrate of brain plasticity, and spine pathologies are observed in various mental illnesses. Here we investigate the role of neurobeachin (Nbea), a multidomain protein previously linked to cases of autism, in synaptogenesis. We show that deletion of Nbea leads to reduced numbers of spinous synapses in cultured neurons from complete knockouts and in cortical tissue from heterozygous mice, accompanied by altered miniature postsynaptic currents. In addition, excitatory synapses terminate mostly at dendritic shafts instead of spine heads in Nbea mutants, and actin becomes less enriched synaptically. As actin and synaptopodin, a spine-associated protein with actin-bundling activity, accumulate ectopically near the Golgi apparatus of mutant neurons, a role emerges for Nbea in trafficking important cargo to pre- and postsynaptic compartments.

Published
2011
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31. Protein mutated in paroxysmal dyskinesia interacts with the active zone protein RIM and suppresses synaptic vesicle exocytosis.

Author

Yiguo Shen, Woo-Ping Ge, Yulong Li, Hirano, Arisa, Hsien-Yang Lee, Rohlmann, Astrid, Missler, Markus, Tsien, Richard W., Lily Yeh Jan, Ying-Hui Fu, and Ptáček, Louis J.

Subjects
DYSKINESIAS, EXOCYTOSIS, CELL physiology, COFFEE, BEVERAGES
Abstract

Paroxysmal nonkinesigenic dyskinesia (PNKD) is an autosomal dominant episodic movement disorder precipitated by coffee, alcohol, and stress. We previously identified the causative gene but the function of the encoded protein remains unknown. We also generated a PNKD mouse model that revealed dysregulated dopamine signaling in vivo. Here, we show that PNKD interacts with synaptic active zone proteins Rab3-interacting molecule (RIM)1 and RIM2, localizes to synapses, and modulates neurotransmitter release. Overexpressed PNKD protein suppresses release, and mutant PNKD protein is less effective than wild-type at inhibiting exocytosis. In PNKD KO mice, RIM1/2 protein levels are reduced and synaptic strength is impaired. Thus, PNKD is a novel synaptic protein with a regulatory role in neurotransmitter release. [ABSTRACT FROM AUTHOR]

Published
2015
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43. Extracellular Domains of α-Neurexins Participate in Regulating Synaptic Transmission by Selectively Affecting N-and P/Q-Type Ca2+ Channels.

Author

Zhang, Weiqi, Rohlmann, Astrid, Sargsyan, Vardanush, Aramuni, Gayane, Hammer, Robert E., Südhof, Thomas C., and Missler, Markus

Subjects
*TRANSGENIC mice, *CALCIUM channels, *SYNAPSES, *CELL adhesion, *BRAIN stem, *NEURAL transmission
Abstract

Neurexins constitute a large family of highly variable cell-surface molecules that may function in synaptic transmission and/or synapse formation. Each of the three known neurexin genes encodes two major neurexin variants, α- and β-neurexins, that are composed of distinct extracellular domains linked to identical intracellular sequences. Deletions of one, two, or all three α-neurexins in mice recently demonstrated their essential role at synapses. In multiple α-neurexin knock-outs, neurotransmitter release from excitatory and inhibitory synapses was severely reduced, primarily probably because voltage-dependent Ca2+ channels were impaired. It remained unclear, however, which neurexin variants actually influence exocytosis and Ca2+ channels, which domain of neurexins is required for this function, and which Ca2+-channel subtypes are regulated. Here, we show by electrophysiological recordings that transgenic neurexin 1α rescues the release and Ca2+-current phenotypes, whereas transgenic neurexin 1β has no effect, indicating the importance of the extracellular sequences for the function of neurexins. Because neurexin 1α rescued the knock-out phenotype independent of the α-neurexin gene deleted, these data are consistent with a redundant function among different α-neurexins. In both knock-out and transgenically rescued mice, α-neurexins selectively affected the component of neurotransmitter release that depended on activation of N- and P/Q-type Ca2+ channels, but left L-type Ca2+ channels unscathed. Our findings indicate that α-neurexins represent organizer molecules in neurotransmission that regulate N- and P/Q-type Ca2+ channels, constituting an essential role at synapses that critically involves the extracellular domains of neurexins. [ABSTRACT FROM AUTHOR]

Published
2005
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44. a-Neurexins couple Ca2+ channels to synaptic vesicle exocytosis.

Author

Missler, Markus, Zhang, Weiqi, Rohlmann, Astrid, Kattenstroth, Gunnar, Hammer, Robert E., Gottmann, Kurt, and Sudhof, Thomas C.

Subjects
SYNAPSES, NEUROTRANSMITTERS, CELL adhesion molecules, MICE, RESEARCH
Abstract

Synapses are specialized intercellular junctions in which cell adhesion molecules connect the presynaptic machinery for neurotransmitter release to the postsynaptic machinery for receptor signalling. Neurotransmitter release requires the presynaptic co-assembly of Ca2+ channels with the secretory apparatus, but little is known about how synaptic components are organized. a-Neurexins, a family of >1,000 presynaptic cell-surface proteins encoded by three genes, link the pre- and postsynaptic compartments of synapses by binding extracellularly to postsynaptic cell adhesion molecules and intracellularly to presynaptic PDZ domain proteins. Using triple-knockout mice, we show that a-neurexins are not required for synapse formation, but are essential for Ca2+-triggered neurotransmitter release. Neurotransmitter release is impaired because synaptic Ca2+ channel function is markedly reduced, although the number of cell-surface Ca2+ channels appears normal. These data suggest that a-neurexins organize presynaptic terminals by functionally coupling Ca2+ channels to the presynaptic machinery. [ABSTRACT FROM AUTHOR]

Published
2003
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45. Cellular uptake of saposin (SAP) precursor and lysosomal delivery by the low density lipoprotein receptor-related protein (LRP).

Author

Hiesberger, Thomas, Hüttler, Silke, Rohlmann, Astrid, Schneider, Wolfgang, Sandhoff, Konrad, and Herz, Joachim

Subjects
SPHINGOLIPIDS, SCIENTIFIC experimentation, PROTEOLYTIC enzymes, METABOLISM, CELLS, LYSOSOMES, MACROPHAGES
Abstract

Sphingolipid activator proteins SAP-A, -B, -C and -D (also called saposins) are generated by proteolytic processing from a 73 kDa precursor and function as obligatory activators of lysosomal enzymes involved in glycosphingolipid metabolism. Although the SAP precursor can be recognized by the mannose-6-phosphate (M-6-P) receptor and shuttled directly from the secretory pathway to the lysosome, a substantial fraction of newly synthesized precursor is secreted from the cell where it may participate in sphingolipid transport and signaling events. Re-uptake of the secreted precursor is mediated by high-affinity cell surface receptors that are apparently distinct from the M-6-P receptor. We found that the low density lipoprotein receptor-related protein (LRP), a multifunctional endocytic receptor that is expressed on most cells, can mediate cellular uptake and lysosomal delivery of SAP precursor. Additional in vivo experiments in mice revealed that the mannose receptor system on macrophages also participates in precursor internalization. We conclude that SAP precursor gains entry into cells by at least three independent receptor mechanisms including the M-6-P receptor, the mannose receptor and LRP. [ABSTRACT FROM AUTHOR]

Published
1998
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46. Sustained somatic gene inactivation by viral transfer of Cre recombinase

Author

Rohlmann, Astrid, Gotthardt, Michael, Willnow, Thomas E., Hammer, Robert E., and Herz, Joachim

Abstract

Transgenic and knockout mice have proven invaluable tools for analyzing physiologically relevant functions of numerous genes. In some cases, however, pleiotropic effects that result from a variable requirement for a particular gene in different tissues, cell types, or stages of embryonic development may complicate the analysis due to a complex phenotype or embryonic lethality. The loxP/Cre-mediated recombination system, which allows tissue-specific gene targeting in the mouse, can be used to overcome these problems. A limitation of current methods is that a mouse carrying a loxP-tagged gene must be crossed with a transgenic mouse expressing the Cre recombinase in an appropriate tissue to obtain the desired gene rearrangement. We have used recombinant adenovirus carrying the Cre recombinase to induce virtually quantitative somatic cell gene disruption in the liver. The targeted gene was the multifunctional low-density lipoprotein receptor-related protein (LRP), a cell surface receptor for α2-macroglobulin and other ligands. Transient expression of Cre following adenoviral infection produced the predicted gene rearrangement, functionally inactivating LRP in the liver. Rearrangement occurred within 6 days after infection and remained stable for at least 28 days. The results demonstrate the suitability of adenoviral Cre gene transfer to induce long-term, quantitative, and temporally controlled gene disruption in the mouse.

Published
1996
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47. Deletion of alpha-neurexins does not cause a major impairment of axonal pathfinding or synapse formation.

Author

Dudanova I, Tabuchi K, Rohlmann A, Südhof TC, and Missler M

Subjects
Animals, Animals, Newborn, Axons ultrastructure, Mice, Mice, Inbred C57BL, Mice, Knockout, Nerve Tissue Proteins metabolism, Neurons cytology, Neurons metabolism, Neurons ultrastructure, Neuropil metabolism, Olfactory Bulb cytology, Olfactory Bulb physiology, Silver Staining methods, Synapses ultrastructure, Synaptic Transmission physiology, Axons physiology, Neurotoxins metabolism, Synapses metabolism, Synaptic Transmission drug effects
Abstract

Alpha-neurexins are synaptic cell-surface molecules that are required for Ca(2+)-triggered exocytosis. Mice lacking all three alpha-neurexins show drastically reduced neurotransmitter release at excitatory and inhibitory synapses and die early postnatally. Although previous histological analysis of newborn alpha-neurexin triple mutants revealed only a moderate reduction in the density of type II synapses in the brainstem, cell culture studies proposed that neurexins are prominently involved in synapse formation. To assess the contribution of alpha-neurexins to the formation and structural properties of synapses in vivo, we performed a detailed morphological analysis of the brains from surviving adult double knockout mice lacking two of the three alpha-neurexins. Despite their impaired neurotransmission, we did not observe any gross anatomical defects or changes in the distribution of synaptic proteins in adult mutants. Only mild structural alterations were found: a approximately 20% reduction of neuropil area in many brain regions, resulting predominantly from shortened distal dendritic branches and fewer spines, as demonstrated by Golgi impregnation of pyramidal neurons. Quantitative electron microscopy revealed ultrastructurally normal type I and II terminals and a approximately 30% decrease in the density of type II synapses in the neocortex. To exclude errors in pathfinding, we investigated axonal projections in the olfactory bulb of newborn knockouts and did not observe any changes. Therefore, alpha-neurexins are not essential for the formation of the vast majority of synapses in vivo but rather regulate the function of these synapses.

Published
2007
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48. Extracellular domains of alpha-neurexins participate in regulating synaptic transmission by selectively affecting N- and P/Q-type Ca2+ channels.

Author

Zhang W, Rohlmann A, Sargsyan V, Aramuni G, Hammer RE, Südhof TC, and Missler M

Subjects
6-Cyano-7-nitroquinoxaline-2,3-dione pharmacology, Animals, Animals, Newborn, Blotting, Western methods, Brain Stem cytology, Brain Stem growth & development, Brain Stem metabolism, Calcium metabolism, Calcium Channel Blockers pharmacology, Dose-Response Relationship, Radiation, Electric Stimulation methods, Excitatory Amino Acid Antagonists pharmacology, Excitatory Postsynaptic Potentials drug effects, Excitatory Postsynaptic Potentials physiology, Excitatory Postsynaptic Potentials radiation effects, Glycoproteins deficiency, Glycoproteins metabolism, Horseradish Peroxidase metabolism, Immunoprecipitation methods, Membrane Potentials drug effects, Membrane Potentials physiology, Membrane Potentials radiation effects, Mice, Mice, Transgenic, Nerve Tissue Proteins deficiency, Nerve Tissue Proteins metabolism, Neural Inhibition drug effects, Neural Inhibition physiology, Neural Inhibition radiation effects, Neurons drug effects, Neurons physiology, Neurons radiation effects, Neuropeptides deficiency, Neuropeptides metabolism, Patch-Clamp Techniques methods, Sodium Channel Blockers pharmacology, Synaptic Transmission drug effects, Tetrodotoxin pharmacology, Calcium Channels, N-Type physiology, Calcium Channels, P-Type physiology, Glycoproteins chemistry, Neuropeptides chemistry, Protein Structure, Tertiary physiology, Synaptic Transmission physiology
Abstract

Neurexins constitute a large family of highly variable cell-surface molecules that may function in synaptic transmission and/or synapse formation. Each of the three known neurexin genes encodes two major neurexin variants, alpha- and beta-neurexins, that are composed of distinct extracellular domains linked to identical intracellular sequences. Deletions of one, two, or all three alpha-neurexins in mice recently demonstrated their essential role at synapses. In multiple alpha-neurexin knock-outs, neurotransmitter release from excitatory and inhibitory synapses was severely reduced, primarily probably because voltage-dependent Ca2+ channels were impaired. It remained unclear, however, which neurexin variants actually influence exocytosis and Ca2+ channels, which domain of neurexins is required for this function, and which Ca2+-channel subtypes are regulated. Here, we show by electrophysiological recordings that transgenic neurexin 1alpha rescues the release and Ca2+-current phenotypes, whereas transgenic neurexin 1beta has no effect, indicating the importance of the extracellular sequences for the function of neurexins. Because neurexin 1alpha rescued the knock-out phenotype independent of the alpha-neurexin gene deleted, these data are consistent with a redundant function among different alpha-neurexins. In both knock-out and transgenically rescued mice, alpha-neurexins selectively affected the component of neurotransmitter release that depended on activation of N- and P/Q-type Ca2+ channels, but left L-type Ca2+ channels unscathed. Our findings indicate that alpha-neurexins represent organizer molecules in neurotransmission that regulate N- and P/Q-type Ca2+ channels, constituting an essential role at synapses that critically involves the extracellular domains of neurexins.

Published
2005
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49. Alpha-neurexins couple Ca2+ channels to synaptic vesicle exocytosis.

Author

Missler M, Zhang W, Rohlmann A, Kattenstroth G, Hammer RE, Gottmann K, and Südhof TC

Subjects
Animals, Brain Stem cytology, Brain Stem physiology, Calcium metabolism, Calcium Signaling, Cell Adhesion, Cell Adhesion Molecules, Neuronal physiology, Cells, Cultured, Evoked Potentials, Glycoproteins, In Vitro Techniques, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Neocortex cytology, Neocortex physiology, Nerve Tissue Proteins genetics, Neuropeptides, Neurotransmitter Agents metabolism, Recombinant Fusion Proteins metabolism, Synaptic Transmission, Calcium Channels physiology, Exocytosis physiology, Nerve Tissue Proteins physiology, Synapses physiology, Synaptic Vesicles physiology
Abstract

Synapses are specialized intercellular junctions in which cell adhesion molecules connect the presynaptic machinery for neurotransmitter release to the postsynaptic machinery for receptor signalling. Neurotransmitter release requires the presynaptic co-assembly of Ca2+ channels with the secretory apparatus, but little is known about how synaptic components are organized. Alpha-neurexins, a family of >1,000 presynaptic cell-surface proteins encoded by three genes, link the pre- and postsynaptic compartments of synapses by binding extracellularly to postsynaptic cell adhesion molecules and intracellularly to presynaptic PDZ domain proteins. Using triple-knockout mice, we show that alpha-neurexins are not required for synapse formation, but are essential for Ca2+-triggered neurotransmitter release. Neurotransmitter release is impaired because synaptic Ca2+ channel function is markedly reduced, although the number of cell-surface Ca2+ channels appears normal. These data suggest that alpha-neurexins organize presynaptic terminals by functionally coupling Ca2+ channels to the presynaptic machinery.

Published
2003
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