Abstract

The overall rationale for this project is to understand the molecular mechanisms that control polymorphonuclearneutrophil(PMN) migration into lumenal spaces at mucosal surfaces. There is abundant evidence, generated from many laboratories, that PMN migration across the epithelium in both lung and gastrointestinaltract is an important component of host defense against bacterial invasion at these surfaces. At the same time, PMN migration into these tissues can cause damage to the organs themselves, as PMN are important in initiating and perpetuating chronic inflammation that eventually leads to epithelial damage, scarring and fibrosis at epithelial surfaces. Chronic inflammation by PMN also has been associated with increased risk of cancer. While progress in understandingPMN migration to sites of inflammation has been rapid over the past decade, important gaps in understanding remain. In particular, little is understood about the molecular mechanisms involved in initial PMN attachment to the basolateral epithelial surface after their exit from the blood or about the transepithelial migration process itself. There are clues to understanding both these processes. Antibodies to the leukocyte integrin Mac-1 (CD11b/CD18, also known as alpha-M beta-2) prevent PMN adhesion to the epithelium, and antibodies to the ubiquitously expressed membrane protein CD47 inhibit transmigration without affecting initial adhesion. We propose to exploit these observations, our expertise in integrin and CD47 biology, and several unique reagents, including CD47-deficient and CD18-deficient mice, to reveal the molecular mechanisms of the two processes of PMN attachment to and transmigration through epithelial barriers. Specifically, we will address three critical questions: 1. Is PMN CD47 or epithelialCD47, or both, important in transepithelialmigration? 2. Does CD47 regulate interepithelialjunctions? 3. What isthe Mac-1 ligand on the basolateralsurface of epithelia? Completion of these studies will lead to increased understanding of a process critical to both host defense and disease pathogenesis and ultimatelywill enhance our abilityto controlthese processes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
1P01AI053194-01
Application #
6588019
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2002-12-01
Project End
2007-11-30
Budget Start
Budget End
Support Year
1
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Datta, Anirban; Sandilands, Emma; Mostov, Keith E et al. (2017) Fibroblast-derived HGF drives acinar lung cancer cell polarization through integrin-dependent RhoA-ROCK1 inhibition. Cell Signal 40:91-98
Singer, Mark S; Phillips, Joanna J; Lemjabbar-Alaoui, Hassan et al. (2015) SULF2, a heparan sulfate endosulfatase, is present in the blood of healthy individuals and increases in cirrhosis. Clin Chim Acta 440:72-8
Plaks, Vicki; Boldajipour, Bijan; Linnemann, Jelena R et al. (2015) Adaptive Immune Regulation of Mammary Postnatal Organogenesis. Dev Cell 34:493-504
Casbon, Amy-Jo; Reynaud, Damien; Park, Chanhyuk et al. (2015) Invasive breast cancer reprograms early myeloid differentiation in the bone marrow to generate immunosuppressive neutrophils. Proc Natl Acad Sci U S A 112:E566-75
Bucior, Iwona; Tran, Cindy; Engel, Joanne (2014) Assessing Pseudomonas virulence using host cells. Methods Mol Biol 1149:741-55
Bonnans, Caroline; Lohela, Marja; Werb, Zena (2014) Real-time imaging of myeloid cells dynamics in ApcMin/+ intestinal tumors by spinning disk confocal microscopy. J Vis Exp :51916
Tran, Cindy S; Eran, Yoni; Ruch, Travis R et al. (2014) Host cell polarity proteins participate in innate immunity to Pseudomonas aeruginosa infection. Cell Host Microbe 15:636-43
Kwon, Sang-Ho; Liu, Kathleen D; Mostov, Keith E (2014) Intercellular transfer of GPRC5B via exosomes drives HGF-mediated outward growth. Curr Biol 24:199-204
Kim, J H; Chan, C; Elwell, C et al. (2013) Endosulfatases SULF1 and SULF2 limit Chlamydia muridarum infection. Cell Microbiol 15:1560-71
Maltseva, Inna; Chan, Matilda; Kalus, Ina et al. (2013) The SULFs, extracellular sulfatases for heparan sulfate, promote the migration of corneal epithelial cells during wound repair. PLoS One 8:e69642

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