- Nyhet
G Protein Coupled Receptors
Structure
Del 520 i serien Methods in Enzymology
2 177 kr
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Beskrivning
This new volume of Methods in Enzymology continues the legacy of this premier serial by containing quality chapters authored by leaders in the field. This volume covers G protein coupled receptors and includes chapters on such topics as post-translation modification of GPCR in relationship to biased agonism, structure-based virtual screening, and GPCR oligomerization in the brain.
- Continues the legacy of this premier serial with quality chapters authored by leaders in the field
- Covers G protein coupled receptors
- Contains chapters on such topics as post-translation modification of GPCR in relationship to biased agonism, structure-based virtual screening, and GPCR oligomerization in the brain
Produktinformation
- Utgivningsdatum:2013-03-15
- Mått:152 x 229 x undefined mm
- Vikt:720 g
- Format:Inbunden
- Språk:Engelska
- Serie:Methods in Enzymology
- Antal sidor:440
- Förlag:Elsevier Science
- Medarbetare:P.Michael Conn
- ISBN:9780123918611
Mer om författaren
P. Michael Conn is the Senior Vice President for Research and Associate Provost, Texas Tech Health Sciences Center. He is The Robert C. Kimbrough, Professor of Internal Medicine and Cell Biology/Biochemistry. He was previously Director of Research Advocacy and Professor of Physiology and Pharmacology, Cell Biology and Development and Obstetrics and Gynecology at Oregon Health and Science University and Senior Scientist of the Oregon National Primate Research Center (ONPRC). He served for twelve years as Special Assistant to the President and Associate Director of the ONPRC. After receiving a B.S. degree and teaching certification from the University of Michigan (1971), a M.S. from North Carolina State University (1973), and a Ph.D. degree from Baylor College of Medicine (1976), Conn did a fellowship at the NIH, then joined the faculty in the Department of Pharmacology, Duke University Medical Center where he was promoted to Associate Professor in 1982. In 1984, he became Professor and Head of Pharmacology at the University of Iowa College of Medicine, a position he held for eleven years. Conn is known for his research in the area of the cellular and molecular basis of action of gonadotropin releasing hormone action in the pituitary and therapeutic approaches that restore misfolded proteins to function. His work has led to drugs that have benefitted humans and animals. Most recently, he has identified a new class of drugs, pharmacoperones, which act by regulating the intracellular trafficking of receptors, enzymes and ion channels. He has authored or co-authored over 350 publications in this area and written or edited over 200 books, including texts in neurosciences, molecular biology and endocrinology. Conn has served as the editor of many professional journals and book series (Endocrinology, Journal of Clinical Endocrinology and Metabolism, Endocrine, Methods, Progress in Molecular Biology and Translational Science and Contemporary Endocrinology). Conn served on the National Board of Medical Examiners, including two years as chairman of the reproduction and endocrinology committee. The work of his laboratory has been recognized with a MERIT award from the NIH, the J.J. Abel Award of the American Society for Pharmacology and Experimental Therapeutics, the Weitzman, Oppenheimer and Ingbar Awards of the Endocrine Society, the National Science Medal of Mexico (the Miguel Aleman Prize) and the Stevenson Award of Canada. He is the recipient of the Oregon State Award for Discovery, the Media Award of the American College of Neuropsychopharmacology and was named a distinguished Alumnus of Baylor College of Medicine in 2012. Conn is a previous member of Council for the American Society for Cell Biology and the Endocrine Society and is a prior President of the Endocrine Society, during which time he founded the Hormone Foundation and worked with political leadership to heighten the public’s awareness of diabetes. Conn’s students and fellows have gone on to become leaders in industry and academia. He is an elected member of the Mexican Institute of Medicine and a fellow of the American Association for the Advancement of Science. He is the co-author of The Animal Research War (2008) and many articles for the public and academic community on the value of animal research and the dangers posed by animal extremism. His op/eds have appeared in The Washington Post, The LA Times, The Wall Street Journal, the Des Moines Register, and elsewhere. Conn consults with organizations that are influenced by animal extremism and with universities and companies facing challenges from these groups.
Innehållsförteckning
- G Protein Coupled Receptors: Techniques for Probing StructureComformational Ensemble View of G Protein-Coupled Receptors and The Effect of Mutations and Ligand BindingStructural Evolution of G-Protein-Coupled Receptors: A Sequence Space ApproachDirected Evolution of G Protein-Coupled Receptors for High Functional Expression and Detergent StabilityThe Role of Hydrophobic Amino Acids in the Structure and Function of the Rhodopsin Family of G Protein-Coupled ReceptorsStructure of β-Adrenergic ReceptorsAdvances in Methods to Characterize Ligand-Induced Ionic Lock and Rotamer Toggle Molecular Switch in G-Protein Coupled ReceptorsCrystallogenesis of Adenosine A2A Receptor – T4 Lysozyme Fusion Protein: A Practical Route for the StructureProbing GPCR Structure: Adenosine and P2Y Nucleotide ReceptorsStrategies for Studying the Ligand Binding Site of GPCRs: Photoaffinity Labeling of the VPAC1 Receptor, a Prototype of Class B GPCRsExpression of Mammalian G Protein-Coupled Receptors in Caenorhabditis ElegansExpression, Purification and Structural Analysis of Intracellular C-Termini from Metabotropic Glutamate ReceptorsUnnatural Amino Acid Mutagenesis of GPCRs Using Amber Codon Suppression and Bioorthogonal LabelingMapping a Ligand Binding Site Using Genetically-Encoded Photoactivatable CrosslinkersAlternative mRNA Splicing of G Protein-Coulped ReceptorsFunctional Residues of the CB1 Cannabinoid Receptor
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