Abstract

This proposal examines the hypothesis that agonist-induced trafficking of G-protein coupled receptors (GPCRs) is required for the initiation and termination of signal transduction, and that defects result in uncontrolled stimulation and disease. The molecular mechanisms and physiological roles of substance P (SP)- induced trafficking of the neurokinin 1 receptor (NKIR) will be examined at the level of the cell and the whole animal. It is important to understand the mechanisms of NK1R signaling in view of the pathophysiological roles of this receptor in neurogenic inflammation, pain and intestinal motility. NK1R regulation will be studied in transfected cell lines, endothelial cells and enteric neurons in short-term culture, and in knockout and transgenic mice.
Aim 1 will define the molecular mechanism of SP-stimulated endocytosis and intracellular trafficking of the NK1R. The role of the clathrin adapter p-arrestin, and of dynamin and Rab GTPases in NK1R trafficking will be examined by expression of dominant negative mutants, and by studying neurons from p- arrestin knockout mice. The role of the cytoskeleton and of endosomal acidification and phosphatases will be examined using specific drugs Aim 2 will define the importance of NK1R trafficking for the initiation of signal transduction. The role of p-arrestins, Rabs and the cytoskeleton in NKlR-mediated MAP kinase activation will be determined using reagents developed in Aim 1. These studies will define the role of p-arrestins as molecular scaffolds that recruit and organize components of the MAPK cascade.
Aim 3 will define the importance of NK1R trafficking in desensitization and resensitization of signaling. The role of G-protein receptor kinases (GRKs) and p-arrestins in desensitization will be determined by expression of dominant negative mutants and by studying neurons from knockout mice. The importance of Rabs, the cytoskeleton and endosomal sorting for resensitization will be examined using reagents from Aim 1.
Aim 4 will determine whether defects in mechanisms of NK1R desensilization result in prolonged SP signaling and disease. SP signaling will be examined in mice deficient in GRKs or p-arrestins, or expressing a desensitization and internalization-defective mutant NK1R (NK1R8325, a naturally occurring NK1R variant). The effects of SP on intestinal motility and neurogenic inflammation will be examined, with the expectation that defects in desensitization will result in exaggerated motor and inflammatory responses. Together, the results of these experiments will provide new information about GPCR signaling, and will define how defects in signal transduction can cause disease. PERFORMANCE SFTEfS) (organization, city, state) University of California, San Francisco Harvard University KEY PERSONNEL. SeeInstructions on Page 11. Use continuationpagesasneededtoprovidetherequired Informationin theformat shown below. Name Organization Role on Project Nigel Bunnett, Ph.D. University of California, San Francisco Principal Investigator Eileen Grady, Ph.D. University of California, San Francisco Co-investigator Kimberley Kirkwood, M.D. University of California, San Francisco Co-investigator Fabien Schmidlin, Ph.D. University of California, San Francisco Post-doctoral fellow Norma Gerard, Ph.D. Harvard University Principal Investigator Shoji Okinaga, M.D., Ph. D. Harvard University Post-doctoral Fellow Craig Gerard, M.D. Harvard University Consultant Stephen Collins, M.D. McMaster University Consultant Helen Raybould, Ph.D. University of California, Los Angeles Consultant Jon Seidman, Ph.D. Harvard University Consultant PHS 398 (Rev. 4/98) Page 2 BB Number pages consecutively at the bottom throughout the application. Do not use suffixes such as 3a, 3b.. CC Principal Investigator/Program Director (Last, first, middle) Bunnett, Nigel W., Ph.D. Type the name of the principal investlgatoir/proaju^Tm) director at the top of each printed page and each ooaojftrauation page. (For type specifications, see Specific Instructions onpage 10.) RESEARCH GRANT TABLE OF CONTENTS PAGE NUMBERS Face page 1 Description,

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37DK039957-20
Application #
7255470
Study Section
Special Emphasis Panel (NSS)
Program Officer
May, Michael K
Project Start
1987-07-01
Project End
2010-06-30
Budget Start
2007-07-01
Budget End
2008-06-30
Support Year
20
Fiscal Year
2007
Total Cost
$336,257
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Surgery
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Poole, Daniel P; Lieu, TinaMarie; Pelayo, Juan Carlos et al. (2015) Inflammation-induced abnormalities in the subcellular localization and trafficking of the neurokinin 1 receptor in the enteric nervous system. Am J Physiol Gastrointest Liver Physiol 309:G248-59
Pelayo, Juan-Carlos; Veldhuis, Nicholas A; Eriksson, Emily M et al. (2014) Localisation and activation of the neurokinin 1 receptor in the enteric nervous system of the mouse distal colon. Cell Tissue Res 356:319-32
Alemi, Farzad; Kwon, Edwin; Poole, Daniel P et al. (2013) The TGR5 receptor mediates bile acid-induced itch and analgesia. J Clin Invest 123:1513-30
Cattaruzza, Fiore; Poole, Daniel P; Bunnett, Nigel W (2013) Arresting inflammation: contributions of plasma membrane and endosomal signalling to neuropeptide-driven inflammatory disease. Biochem Soc Trans 41:137-43
Rajagopal, Senthilkumar; Kumar, Divya P; Mahavadi, Sunila et al. (2013) Activation of G protein-coupled bile acid receptor, TGR5, induces smooth muscle relaxation via both Epac- and PKA-mediated inhibition of RhoA/Rho kinase pathway. Am J Physiol Gastrointest Liver Physiol 304:G527-35
Alemi, Farzad; Poole, Daniel P; Chiu, Jonathan et al. (2013) The receptor TGR5 mediates the prokinetic actions of intestinal bile acids and is required for normal defecation in mice. Gastroenterology 144:145-54
Veldhuis, Nicholas A; Lew, Michael J; Abogadie, Fe C et al. (2012) N-glycosylation determines ionic permeability and desensitization of the TRPV1 capsaicin receptor. J Biol Chem 287:21765-72
Law, Ivy Ka Man; Murphy, Jane E; Bakirtzi, Kyriaki et al. (2012) Neurotensin-induced proinflammatory signaling in human colonocytes is regulated by ?-arrestins and endothelin-converting enzyme-1-dependent endocytosis and resensitization of neurotensin receptor 1. J Biol Chem 287:15066-75
Hasdemir, Burcu; Mahajan, Shilpi; Bunnett, Nigel W et al. (2012) Endothelin-converting enzyme-1 actions determine differential trafficking and signaling of corticotropin-releasing factor receptor 1 at high agonist concentrations. Mol Endocrinol 26:681-95
Murphy, Jane E; Roosterman, Dirk; Cottrell, Graeme S et al. (2011) Protein phosphatase 2A mediates resensitization of the neurokinin 1 receptor. Am J Physiol Cell Physiol 301:C780-91

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