Abstract

Integrins are heterodimeric receptors which mediate vital cell-cell and cell-matrix interactions such as those taking place during morphogenesis, growth and differentiation, angiogenesis, hemostasis, inflammation and gene expression. Integrins bind in a divalent cation dependent manner to diverse ligands including certain plasma proteins, and extracellular matrix and membrane proteins. Despite the diversity of integrin ligands, an acidic residue is an essential feature of their integrin binding motif. In contrast to other receptors where binding to ligand is often intrinsic, integrin binding to many physiologic ligands is not constitutive but rather inducible, and is associated with conformational changes in integrins that extend to their ligand binding regions. The activation-dependent interaction of integrins with ligands plays a crucial role in regulating cell-cell and cell-matrix adhesion and in avoiding serious damage to host tissues. The overall goal of this proposal is to elucidate the structural basis of integrin-ligand interactions and to define in molecular terms the nature of integrin activation. During the previous funding period, we have identified a major ligand binding site within a conserved 200 amino acid domain (A-or I-domain) in the extracellular region of the alpha (CD11b) subunit of integrin CD11b/CD18. This domain contains a novel metal binding site which is required for the interaction of the domain as well as the holoreceptor with several ligands. We also solved the 3-dimensional crystal structure of this domain. A glutamate residue from another molecule completes the coordination of the solvent-exposed metal ion in the structure. We proposed that this arrangement may be a mimic of the interaction of an integrin with ligands, and may explain the indispensable role of acidic residues in integrin binding motifs. Hydropathy plot analysis of a highly conserved metal- and ligand binding region in all integrin beta subunits revealed a striking similarity to the alpha subunit A-domain, and we suggested that an A-like domain is also present in all integrin beta subunits. We also found that the A- domain exists in two conformations, and we proposed based on indirect structural comparisons with G proteins that the two conformations may represent active and inactive states of the domain. The presence of binding sites for several ligands in the A-domain also suggested the feasibility of targeting this domain to generate novel antagonists. In this application, we therefore propose three specific aims: 1) to derive the 3-D structure of the CD11b A-domain in complex with a ligand- derived peptide and evaluate the functional status of the two A-domain conformations. 2) to solve the 3-D structure of the A-like domain in integrin beta subunits. 3) To generate specific antagonists of the CD11b/CD18 receptor using a genetic approach. Biochemical, structural-, cell- and molecular biology techniques will be used. The derived information will be invaluable in developing a structure-based understanding of integrin ligand binding and activation. Given the potential role of CD11b/CD18 in inflammation and injury, derivation of specific antagonists of this receptor could have therapeutic benefits.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK048549-16
Application #
6380923
Study Section
Pathobiochemistry Study Section (PBC)
Program Officer
Badman, David G
Project Start
1989-04-01
Project End
2002-03-31
Budget Start
2001-04-01
Budget End
2002-03-31
Support Year
16
Fiscal Year
2001
Total Cost
$305,825
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Dehnadi, Abbas; Benedict Cosimi, A; Neal Smith, Rex et al. (2017) Prophylactic orthosteric inhibition of leukocyte integrin CD11b/CD18 prevents long-term fibrotic kidney failure in cynomolgus monkeys. Nat Commun 8:13899
Camarata, Troy D; Weaver, Grant C; Vasilyev, Alexandr et al. (2015) Negative Regulation of TGF? Signaling by Stem Cell Antigen-1 Protects against Ischemic Acute Kidney Injury. PLoS One 10:e0129561
Wu, Qing; Zhang, Jiaojiao; Koh, Wonshill et al. (2015) Talin1 is required for cardiac Z-disk stabilization and endothelial integrity in zebrafish. FASEB J 29:4989-5005
Zhang, Jiaojiao; Yuan, Shipeng; Vasilyev, Aleksandr et al. (2015) The transcriptional coactivator Taz regulates proximodistal patterning of the pronephric tubule in zebrafish. Mech Dev 138 Pt 3:328-35
Adair, Brian D; Altintas, Mehmet M; Möller, Clemens C et al. (2014) Structure of the kidney slit diaphragm adapter protein CD2-associated protein as determined with electron microscopy. J Am Soc Nephrol 25:1465-73
Palmyre, Aurélien; Lee, Jeongeun; Ryklin, Gennadiy et al. (2014) Collective epithelial migration drives kidney repair after acute injury. PLoS One 9:e101304
Van Agthoven, Johannes F; Xiong, Jian-Ping; Alonso, José Luis et al. (2014) Structural basis for pure antagonism of integrin ?V?3 by a high-affinity form of fibronectin. Nat Struct Mol Biol 21:383-8
Yu, Chih-Chuan; Fornoni, Alessia; Weins, Astrid et al. (2013) Abatacept in B7-1-positive proteinuric kidney disease. N Engl J Med 369:2416-23
Frohlich, Else M; Alonso, José Luis; Borenstein, Jeffrey T et al. (2013) Topographically-patterned porous membranes in a microfluidic device as an in vitro model of renal reabsorptive barriers. Lab Chip 13:2311-9
Adair, Brian D; Xiong, Jian-Ping; Alonso, José Luis et al. (2013) EM structure of the ectodomain of integrin CD11b/CD18 and localization of its ligand-binding site relative to the plasma membrane. PLoS One 8:e57951

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