Abstract

allb-beta3 and aVbeta3 integrins mediate adhesion of platelets and other cells to matrix ligands at sites of vascular injury. Ligand binding is regulated by activating or """"""""inside-out"""""""" signals that modulate integrin affinity through conformational changes and integrin avidity through microclustering. Recently, integrin conformational changes have been characterized structurally and talin has been identified as a key regulator of these changes by binding to the beta3 cytoplasmic tail. Here, three major unresolved questions will be asked concerning the molecular basis of inside-out signaling. First, what is the relationship between talin and two other proteins, Rap1b and ADAP, recently implicated as positive regulators of beta3 integrin affinity? The role of Rap1b or ADAP in talin-dependent beta3 integrin activation will be assessed in primary mouse megakaryocytes, platelets and an improved CHO cell model system in which beta3 integrins are sensitive to inside-out signals. Over-expression and knockdown approaches will be used to investigate the inter-dependency of these mediators and their relative effects on beta3 integrin affinity and microclustering. Then, Rap1b and ADAP effectors that regulate beta3 integrins will be identified and their actions characterized. Second, are there regulators of beta3 integrin affinity still to be discovered? Here, the effects on allb-beta3 affinity of PTB domain- containing proteins other than talin will be determined, focusing particular attention on moesin and Dok-2, platelet proteins implicated in cytoskeletal regulation. In a complementary approach, affinity regulation of beta3 integrins will be characterized in zebrafish to evaluate mechanistic similarities and differences with the regulatory process in mammals. Third, what are the mechanisms and consequences of beta3 integrin activation in neoplastic cells? Over-expression and knockdown approaches will investigate whether Rap1b or talin are required for constitutive aVbeta3 activation in certain tumor cells and whether this integrin activation promotes a metastatic phenotype. The potential for oncogenic activation of allb-beta3 in chronic myeloproliferative diseases will be evaluated in mouse megakaryocytes and platelets by over-expressing constitutively-active JAK2 (V617F), a common mutation in these bleeding- and thrombosis-prone diseases. Together, these studies will provide insights into how beta3 integrin activation is regulated, how the activation mechanism is co-opted in clinical disorders, and how it may be harnessed to develop better anti-platelet drugs. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL056595-13
Application #
7447331
Study Section
Hemostasis and Thrombosis Study Section (HT)
Program Officer
Link, Rebecca P
Project Start
1996-07-01
Project End
2011-06-30
Budget Start
2008-07-01
Budget End
2009-06-30
Support Year
13
Fiscal Year
2008
Total Cost
$375,049
Indirect Cost

  Institution

Name
University of California San Diego
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
804355790
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Lagarrigue, Frederic; Gingras, Alexandre R; Paul, David S et al. (2018) Rap1 binding to the talin 1 F0 domain makes a minimal contribution to murine platelet GPIIb-IIIa activation. Blood Adv 2:2358-2368
Liao, Zhongji; Kasirer-Friede, Ana; Shattil, Sanford J (2017) Optogenetic interrogation of integrin ?V?3 function in endothelial cells. J Cell Sci 130:3532-3541
Ley, Klaus; Rivera-Nieves, Jesus; Sandborn, William J et al. (2016) Integrin-based therapeutics: biological basis, clinical use and new drugs. Nat Rev Drug Discov 15:173-83
Liao, Zhongji; Kato, Hisashi; Pandey, Manjula et al. (2015) Interaction of kindlin-2 with integrin ?3 promotes outside-in signaling responses by the ?V?3 vitronectin receptor. Blood 125:1995-2004
Desgrosellier, Jay S; Lesperance, Jacqueline; Seguin, Laetitia et al. (2014) Integrin ?v?3 drives slug activation and stemness in the pregnant and neoplastic mammary gland. Dev Cell 30:295-308
van Sorge, Nina M; Cole, Jason N; Kuipers, Kirsten et al. (2014) The classical lancefield antigen of group a Streptococcus is a virulence determinant with implications for vaccine design. Cell Host Microbe 15:729-740
Kasirer-Friede, Ana; Kang, Jian; Kahner, Bryan et al. (2014) ADAP interactions with talin and kindlin promote platelet integrin ?IIb?3 activation and stable fibrinogen binding. Blood 123:3156-65
Casar, B; Rimann, I; Kato, H et al. (2014) In vivo cleaved CDCP1 promotes early tumor dissemination via complexing with activated ?1 integrin and induction of FAK/PI3K/Akt motility signaling. Oncogene 33:255-68
Ye, Feng; Petrich, Brian G; Anekal, Praju et al. (2013) The mechanism of kindlin-mediated activation of integrin ?IIb?3. Curr Biol 23:2288-2295
Kato, Hisashi; Liao, Zhongji; Mitsios, John V et al. (2012) The primacy of ?1 integrin activation in the metastatic cascade. PLoS One 7:e46576

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