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Papazian Lab Homepage Electrical excitability in the brain: voltage-gated ion Home channels, cell & circuit function, neural control of behavior, relationship between spike activity and neuronal viability. Electrical activity underlies most aspects of brain function. Our research focuses on the voltage-gated ion channels that confer electrical excitability on neurons and the consequences of changes in channel activity for neuronal firing, circuit function, behavior, and neuronal viability during development and aging. People Projects Publications Work in our lab spans many levels of analysis, from the molecular to the behavioral. We are studying how voltage controls the activity of K+ channels, how changes in channel function or expression affect the firing patterns of neurons and the emergent properties of neuronal circuits, and how altering neuronal excitability affects behavior. We are also investigating the relationship between excitability and neuronal survival at different stages of life. We use a wide variety of experimental approaches to address these issues, including electrophysiology, imaging, biochemistry, molecular biology, genetics, and behavioral analysis. In the past few years, we have adopted the zebrafish, Danio rerio, as our main model system for integrative analysis. We also use Xenopus oocytes to investigate channel function and primary cultures of rodent neurons to explore the relationship between channel activity and neuronal function and viability. Contact Positions Map & Directions We are always looking for bright, hard-working individuals who want to work in a collaborative environment focusing on mechanistic, quantitative approaches to key questions in neuroscience. Links Electrical activity underlies most aspects of brain function. Our research focuses on the voltage-gated ion channels that confer electrical excitability on neurons and the consequences of changes in channel activity for neuronal firing, circuit function, behavior, and neuronal viability during development and aging. Work in our lab spans many levels of analysis, from the molecular to the behavioral. We are studying how voltage controls the activity of K+ channels, how changes in channel function or expression affect the firing patterns of neurons and the emergent properties of neuronal circuits, and how altering neuronal excitability affects behavior. We are also investigating the relationship between excitability and neuronal survival at different stages of life. We use a wide variety of experimental approaches to address these issues, including electrophysiology, imaging, biochemistry, molecular biology, genetics, and behavioral analysis. In the past few years, we have adopted the zebrafish, Danio rerio, as our main model system for integrative analysis. We also use Xenopus oocytes to investigate channel function and primary cultures of rodent neurons to explore the relationship between channel activity and neuronal function and viability. We are always looking for bright, hard-working individuals who want to work in a collaborative environment focusing on mechanistic, quantitative approaches to key questions in neuroscience. People Home Projects Publications Diane M Papazian PhD Professor Department of Physiology UCLA Current Lab Members Jie Yi (Ray) Hsieh Fadi (Pete) Issa Contact Meng-chin Lin Natali Minassian Positions Allan Mock Liz Vuong Map & Directions Links Lab Photos Former Lab Members Chih-Yung Tang, National Taiwan University Seema Tiwari-Woodruff, UCLA Lucia Santacruz-Toloza, Duke University Christine Schulteis, Immusol Will Silverman, University of Miami Muriel Lainé, University of Chicago John Bannister, University of Tennessee Chris Mazzochi Jessica Richardson, UC Davis School of Law Myong-chul Koag Mike Myers, Cal State Long Beach Raj Khanna, Indiana University Naomi Nagaya, University of Michigan Yu Huang, Chinese University of Hong Kong Scott John, UCLA Max Shao, UCLA Sang-Ah Seoh Miriam Pillos Diane M Papazian PhD Professor Department of Physiology UCLA Education: 1973-1977 B.S. (Chemistry), with high distinction University of Michigan Ann Arbor, Michigan 1977-1983 Ph.D. (Biological Chemistry) Harvard University Cambridge, Massachusetts Professional Positions: 1983-1989 Postdoctoral Fellow Laboratory of Lily and Yuh Nung Jan University of California, San Francisco 1989-1994 Assistant Professor, Department of Physiology UCLA School of Medicine 1994-2000 Associate Professor, Department of Physiology UCLA School of Medicine 1999-2005 Executive Vice Chair, Department of Physiology UCLA David Geffen School of Medicine 2000-now Professor, Department of Physiology UCLA David Geffen School of Medicine Honors: Fellow of the Biophysical Society, 2009 H. W. Magoun Distinguished Lecturer, UCLA Brain Research Institute, 2008 Contributing Member, Faculty of 1000, 2004-2007 Councilor, Biophysical Society, 2004-2006 Fellow, American Association for the Advancement of Science, 1999 Grass Foundation Traveling Scientist, Society for Neuroscience, 1997 Pew Scholar in the Biomedical Sciences, 1991-1995 Klingenstein Fellow in the Neurosciences, 1989-1992 Home Back to People Jie Yi (Ray) Hsieh Home Back to People Fadi (Pete) Issa PhD Home Back to People Meng-chin A Lin PhD Home Back to People Natali A Minassian Home Back to People Allan Mock Home Back to People Papazian Lab Photos Home Back to People Projects Home People Gating of voltage-dependent K+ channels (more . . .) We are investigating the mechanism of voltage-dependent activation in K+ channels. K+ channels are tetramers with a central K+-selective pore and 4 voltage sensor domains, one per subunit. Upon membrane depolarization, the voltage sensor domains undergo conformational changes that result in pore opening. Our current goals are to identify experimental constraints that make it possible to model the structure of the closed channel and to determine the pathway taken by the S4 segment, the main moving element in the voltage sensor, during activation. Neuronal Excitability and Spinocerebellar Ataxia Type 13 (more . . .) Publications Contact Positions Spinocerebellar Ataxia Type 13 is an autosomal dominant genetic disease in humans caused by mutations in KCNC3, which encodes Kv3.3, a voltage-gated K+ channel. The two original SCA13 mutations are associated with distinct clinical manifestations. A mutation in the voltage sensor domain leads to progressive adult onset ataxia accompanied by degeneration of cerebellar neurons. This mutant subunit has a strong dominant negative effect on Kv3 expression. In contrast, a mutation in the pore domain causes a form of SCA13 that emerges in infancy, characterized by a severely shrunken and malformed cerebellum and non-progressive motor deficits. This mutation affects gating, shifting the voltage dependence of activation in the negative direction and dramatically slowing channel closing. We are testing the hypothesis that changes in Kv3.3 channel function alter the excitability of cerebellar neurons, with detrimental consequences for motor behavior and neuronal survival during brain development or aging. We are working to determine how changes in excitability decrease the viability of neurons and why different mutations affect neuronal survival at different stages of life. Zebrafish Model of Human Ataxia (more . . .) We are expressing SCA13 mutant subunits in zebrafish to determine the consequences for neuronal function, development, viability, and locomotor behavior. Currently, we are focusing on the spinal cord. Map & Directions Endogenous Kv3.3 is expressed in primary motor neurons, which control the fastest and largest amplitude movements in zebrafish, including the startle (escape) response. Expression of a dominant negative SCA13 subunit dramatically affects the escape response, reducing the precision and amplitude of the C start and impairing the execution of subsequent steps in the motor program. These features strongly resemble human ataxia. Links Selected Recent Publications Home People Projects Silverman, W.R., Roux, B., and Papazian, D.M. (2003) Structural basis of two-stage voltage-dependent activation in K+ channels. Proc. Natl. Acad. Sci. USA 100, 2935-2940. Contact Positions Lainé, M., Lin, M.A., Bannister, J.P.A., Silverman, W.R., Mock, A.F., Roux, B., and Papazian, D.M. (2003) Atomic proximity between S4 segment and pore domain in Shaker potassium channels. Neuron 39, 467-481. Tiwari-Woodruff, S.K.*, Lin, M.A.*, Schulteis, C.T., and Papazian, D.M. (2000) Voltage-dependent structural interactions in the Shaker K+ channel. J. Gen. Physiol. 115, 123-138. (Cover article) (*co-first authors) Silverman, W.R., Tang, C.-Y., Mock, A.F., Huh, K.-B., and Papazian, D.M. (2000) Mg2+ modulates voltage-dependent activation in ether-à-go-go potassium channels by binding between transmembrane segments S2 and S3. J. Gen. Physiol. 116, 663-677. Map & Directions Links Tang, C.-Y., Bezanilla, F., and Papazian, D.M. (2000) Extracellular Mg2+ modulates slow gating transitions and the opening of Drosophila ether-à-go-go potassium channels. J. Gen. Physiol. 115, 319-337. Full Publication List (PubMed) Lin, M.A., Abramson, J., and Papazian, D.M. (2009) Transfer of ion binding site from ether-à-go-go to Shaker: Mg2+ binds to resting state to modulate channel opening. Submitted for publication. Figueroa, K.P.*, Minassian, N.A.*, Stevanin G., Waters, M., Garibyan, V., Bürk, K., Brice, A., Dürr, A., Papazian, D.M., and Pulst, S.M. (2009) SCA13: KCNC3 mutations and genotype/phenotype correlations in 260 familial ataxia patients. Hum. Mutat., in press. (*cofirst authors) Koag, M.C. and Papazian, D.M. (2009) Voltage-dependent conformational changes of KvAP S4 segment in bacterial membrane environment. Channels 3, epub ahead of print (PMID 19713752). Lin, M.A. and Papazian, D.M. (2007) Differences between ion binding to eag and HERG voltage sensors contribute to differential regulation of activation and deactivation gating. Channels 1, 429-437. Waters, M.F., Minassian, N.A., Stevanin, G., Figueroa, K.P., Bannister, J.P.A., Nolte, D., Mock, A.F., Evidente, V.G., Fee, D., Müller, U., Dürr, A., Brice, A., Papazian, D.M., and Pulst, S.M. (2006) Mutations in the voltage-gated potassium channel KCNC3 cause degenerative and developmental CNS phenotypes. Nat. Genet. 38, 447-451. Bannister, J.P.A., Chanda, B., Bezanilla, F., and Papazian, D.M. (2005) Optical detection of rate-determining, ion-modulated conformational changes of the ether-à-go-go K+ channel voltage sensor. Proc. Natl. Acad. Sci. USA 102, 18718-18723. Silverman, W.R., Roux, B., and Papazian, D.M. (2003) Structural basis of two-stage voltage-dependent activation in K+ channels. Proc. Natl. Acad. Sci. USA 100, 2935-2940. Lainé, M., Lin, M.A., Bannister, J.P.A., Silverman, W.R., Mock, A.F., Roux, B., and Papazian, D.M. (2003) Atomic proximity between S4 segment and pore domain in Shaker potassium channels. Neuron 39, 467-481. Tiwari-Woodruff, S.K.*, Lin, M.A.*, Schulteis, C.T., and Papazian, D.M. (2000) Voltage-dependent structural interactions in the Shaker K+ channel. J. Gen. Physiol. 115, 123-138. (Cover article) (*co-first authors) Silverman, W.R., Tang, C.-Y., Mock, A.F., Huh, K.-B., and Papazian, D.M. (2000) Mg2+ modulates voltage-dependent activation in ether-à-go-go potassium channels by binding between transmembrane segments S2 and S3. J. Gen. Physiol. 116, 663-677. Tang, C.-Y., Bezanilla, F., and Papazian, D.M. (2000) Extracellular Mg2+ modulates slow gating transitions and the opening of Drosophila ether-à-go-go potassium channels. J. Gen. Physiol. 115, 319-337. Figueroa, K.P.*, Minassian, N.A.*, Stevanin G., Waters, M., Garibyan, V., Bürk, K., Brice, A., Dürr, A., Papazian, D.M., and Pulst, S.M. (2009) SCA13: KCNC3 mutations and genotype/phenotype correlations in 260 familial ataxia patients. Submitted for publication. (*co-first authors) Lin, M.A., Abramson, J., and Papazian, D.M. (2009) Transfer of ion binding site from ether-à-go-go to Shaker: Mg2+ binds to resting state to modulate channel opening. Submitted for publication. Koag, M.C. and Papazian, D.M. (2009) Voltage-dependent conformational changes of KvAP S4 segment in bacterial membrane environment. Channels 3, epub ahead of print (PMID 19713752). Lin, M.A. and Papazian, D.M. (2007) Differences between ion binding to eag and HERG voltage sensors contribute to differential regulation of activation and deactivation gating. Channels 1, 429-437. Waters, M.F., Minassian, N.A., Stevanin, G., Figueroa, K.P., Bannister, J.P.A., Nolte, D., Mock, A.F., Evidente, V.G., Fee, D., Müller, U., Dürr, A., Brice, A., Papazian, D.M., and Pulst, S.M. (2006) Mutations in the voltage-gated potassium channel KCNC3 cause degenerative and developmental CNS phenotypes. Nat. Genet. 38, 447-451. Bannister, J.P.A., Chanda, B., Bezanilla, F., and Papazian, D.M. (2005) Optical detection of rate-determining, ion-modulated conformational changes of the ether-à-go-go K+ channel voltage sensor. Proc. Natl. Acad. Sci. USA 102, 18718-18723. Silverman, W.R., Roux, B., and Papazian, D.M. (2003) Structural basis of two-stage voltage-dependent activation in K+ channels. Proc. Natl. Acad. Sci. USA 100, 2935-2940. Lainé, M., Lin, M.A., Bannister, J.P.A., Silverman, W.R., Mock, A.F., Roux, B., and Papazian, D.M. (2003) Atomic proximity between S4 segment and pore domain in Shaker potassium channels. Neuron 39, 467-481. Tiwari-Woodruff, S.K.*, Lin, M.A.*, Schulteis, C.T., and Papazian, D.M. (2000) Voltage-dependent structural interactions in the Shaker K+ channel. J. Gen. Physiol. 115, 123-138. (Cover article) (*co-first authors) Silverman, W.R., Tang, C.-Y., Mock, A.F., Huh, K.-B., and Papazian, D.M. (2000) Mg2+ modulates voltage-dependent activation in ether-à-go-go potassium channels by binding between transmembrane segments S2 and S3. J. Gen. Physiol. 116, 663-677. Tang, C.-Y., Bezanilla, F., and Papazian, D.M. (2000) Extracellular Mg2+ modulates slow gating transitions and the opening of Drosophila ether-à-gogo potassium channels. J. Gen. Physiol. 115, 319-337. Figueroa, K.P.*, Minassian, N.A.*, Stevanin G., Waters, M., Garibyan, V., Bürk, K., Brice, A., Dürr, A., Papazian, D.M., and Pulst, S.M. (2009) SCA13: KCNC3 mutations and genotype/phenotype correlations in 260 familial ataxia patients. Submitted for publication. (*co-first authors) Lin, M.A., Abramson, J., and Papazian, D.M. (2009) Transfer of ion binding site from ether-à-go-go to Shaker: Mg2+ binds to resting state to modulate channel opening. Submitted for publication. Koag, M.C. and Papazian, D.M. (2009) Voltage-dependent conformational changes of KvAP S4 segment in bacterial membrane environment. Channels 3, epub ahead of print (PMID 19713752). Lin, M.A. and Papazian, D.M. (2007) Differences between ion binding to eag and HERG voltage sensors contribute to differential regulation of activation and deactivation gating. Channels 1, 429-437. Waters, M.F., Minassian, N.A., Stevanin, G., Figueroa, K.P., Bannister, J.P.A., Nolte, D., Mock, A.F., Evidente, V.G., Fee, D., Müller, U., Dürr, A., Brice, A., Papazian, D.M., and Pulst, S.M. (2006) Mutations in the voltage-gated potassium channel KCNC3 cause degenerative and developmental CNS phenotypes. Nat. Genet. 38, 447-451. Bannister, J.P.A., Chanda, B., Bezanilla, F., and Papazian, D.M. (2005) Optical detection of rate-determining, ion-modulated conformational changes of the ether-à-go-go K+ channel voltage sensor. Proc. Natl. Acad. Sci. USA 102, 18718-18723. Figueroa, K.P.*, Minassian, N.A.*, Stevanin G., Waters, M., Garibyan, V., Bürk, K., Brice, A., Dürr, A., Papazian, D.M., and Pulst, S.M. (2009) SCA13: KCNC3 mutations and genotype/phenotype correlations in 260 familial ataxia patients. Submitted for publication. (*co-first authors) Lin, M.A., Abramson, J., and Papazian, D.M. (2009) Transfer of ion binding site from ether-à-go-go to Shaker: Mg2+ binds to resting state to modulate channel opening. Submitted for publication. Koag, M.C. and Papazian, D.M. (2009) Voltage-dependent conformational changes of KvAP S4 segment in bacterial membrane environment. Channels 3, epub ahead of print (PMID 19713752). Lin, M.A. and Papazian, D.M. (2007) Differences between ion binding to eag and HERG voltage sensors contribute to differential regulation of activation and deactivation gating. Channels 1, 429-437. Waters, M.F., Minassian, N.A., Stevanin, G., Figueroa, K.P., Bannister, J.P.A., Nolte, D., Mock, A.F., Evidente, V.G., Fee, D., Müller, U., Dürr, A., Brice, A., Papazian, D.M., and Pulst, S.M. (2006) Mutations in the voltage-gated potassium channel KCNC3 cause degenerative and developmental CNS phenotypes. Nat. Genet. 38, 447-451. Bannister, J.P.A., Chanda, B., Bezanilla, F., and Papazian, D.M. (2005) Optical detection of rate-determining, ion-modulated conformational changes of the ether-à-go-go K+ channel voltage sensor. Proc. Natl. Acad. Sci. USA 102, 18718-18723. Silverman, W.R., Roux, B., and Papazian, D.M. (2003) Structural basis of two-stage voltage-dependent activation in K+ channels. Proc. Natl. Acad. Sci. USA 100, 2935-2940. Lainé, M., Lin, M.A., Bannister, J.P.A., Silverman, W.R., Mock, A.F., Roux, B., and Papazian, D.M. (2003) Atomic proximity between S4 segment and pore domain in Shaker potassium channels. Neuron 39, 467-481. Tiwari-Woodruff, S.K.*, Lin, M.A.*, Schulteis, C.T., and Papazian, D.M. (2000) Voltage-dependent structural interactions in the Shaker K+ channel. J. Gen. Physiol. 115, 123-138. (Cover article) (*co-first authors) Silverman, W.R., Tang, C.-Y., Mock, A.F., Huh, K.-B., and Papazian, D.M. (2000) Mg2+ modulates voltage-dependent activation in ether-à-go-go potassium channels by binding between transmembrane segments S2 and S3. J. Gen. Physiol. 116, 663-677. Tang, C.-Y., Bezanilla, F., and Papazian, D.M. (2000) Extracellular Mg2+ modulates slow gating transitions and the opening of Drosophila ether-à-gogo potassium channels. J. Gen. Physiol. 115, 319-337. Home Contact Information Diane M Papazian PhD People Projects Publications Positions E-mail: [email protected] Phone: (310) 206-7043 Lab: (310) 825-5766 Fax: (310) 206-5661 U.S. Mailing Address: Shipping Address: Department of Physiology David Geffen School of Medicine at UCLA 650 Charles Young Drive South Box 915751, Room 53-231 CHS Los Angeles, CA 90095-1751 Medical Receiving UCLA Physiology 650 Charles Young Drive South Box 915751, Room 53-231 CHS Los Angeles, CA 90095-1751 Campus Address: Map & Directions Links Department of Physiology 53-159 CHS Mail code 175118 Home People Projects Publications Graduate Students Positions Prospective graduate students have the option of applying to UCLA Access or directly to the Indepartmental PhD Programs in Neuroscience or in Molecular, Cellular and Integrative Physiology. Postdoctoral Fellows Recent PhD recipients with training relevant to our research are invited to apply. Please send your CV and the names of three references to Diane Papazian. At this time, only postdoc candidates who have or can raise their own salary support are being considered. Staff Research Positions Contact We occasionally have open positions for Staff Research Associates. These jobs are posted at: (URL) Research Experiences for Undergraduates Map & Directions Links Motivated undergraduates who are interested in specific projects in the lab should contact Diane Papazian. Only undergraduates who will commit to spending a minimum of 15 hours per week at the bench will be considered. Home People Map & Directions From the 405, exit on Wilshire Blvd heading east. Turn left on Westwood Blvd and follow it onto campus. Turn right at Charles Young Dr. South. You can enter The Center for Health Sciences through the School of Public Health on the south side of the block ( ). We are on the 5th floor, 53-159 CHS. Projects Publications Contact Campus map Positions Links Westwood Links Home People Molecular, Cellular and Integrative Physiology PhD Program Neuroscience PhD Program Projects UCLA Access Department of Physiology Publications Brain Research Institute Molecular Biology Institute Contact Science Links News & Politics Positions Los Angeles California Map & Directions
