The evolving role of thrombospondin-1 in hemostasis and vascular biology

被引：78

作者：

Bonnefoy, A. ^{[2
,3
]}

Moura, R. ^{[1
]}

Hoylaerts, M. F. ^{[1
]}

机构：

[1] Katholieke Univ Leuven, Ctr Mol & Vasc Biol, B-3000 Louvain, Belgium

[2] Univ Montreal St Luc, INSERM, Ctr Hosp, Ctr Rech,U743, Montreal, PQ H2X 1P1, Canada

[3] Inst Cardiol Montreal, Ctr Rech, Montreal, PQ H1T 1C8, Canada

来源：

CELLULAR AND MOLECULAR LIFE SCIENCES | 2008年 / 65卷 / 05期

关键词：

matricellular proteins; cell adhesion; platelet; wound healing; ADAMTS-13; CD47; CD36;

D O I：

10.1007/s00018-007-7487-y

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Thrombospondin-1 (TSP1) is a multi-domain, multi-functional glycoprotein synthesized by many cells. Matricellular TSP1 modulates cell adhesion and proliferation. TSP1 is involved in angiogenesis, inflammation, wound healing and cancer. As a major platelet protein, for a long time it was postulated to control hemostasis via platelet aggregate stabilization. However, these in vitro findings have been questioned in the absence of corroborating clinical data and of obvious hemostatic defects in TSP1 gene-deficient mice.Yet, the past few years have provided indices to implicate TSP1 in hemostasis. In clinical studies, a correlation exists between a welldefined TSP1 polymorphism and a significant risk of myocardial infarction.At the same time, recent in vivo animal model data imply TSP1 in the multimer size control of von Willebrand factor, in smooth muscle cell regulation and in vascular perfusion. These findings shed new light on the role of TSP1 in hemostasis and prothrombotic vascular pathologies.

引用

页码：713 / 727

页数：15

共 152 条

[1]

Adams J, 2004, INT J BIOCHEM CELL B, V36, P960, DOI 10.1016/j.biocel.2004.02.009

[2]

AGAM G, 1984, P SOC EXP BIOL MED, V177, P482

[3] THROMBOSPONDIN PLATELET INTERACTIONS - ROLE OF DIVALENT-CATIONS, WALL SHEAR RATE, AND PLATELET MEMBRANE-GLYCOPROTEINS [J].

AGBANYO, FR ;

SIXMA, JJ ;

DEGROOT, PG ;

LANGUINO, LR ;

PLOW, EF .

JOURNAL OF CLINICAL INVESTIGATION, 1993, 92 (01) :288-296

[4] MECHANISMS FOR EXPRESSION OF THROMBOSPONDIN ON THE PLATELET CELL-SURFACE [J].

AIKEN, ML ;

GINSBERG, MH ;

PLOW, EF .

SEMINARS IN THROMBOSIS AND HEMOSTASIS, 1987, 13 (03) :307-316

[5] CD47 ligation selectively downregulates human interleukin 12 production [J].

Armant, M ;

Avice, MN ;

Hermann, P ;

Rubio, M ;

Kiniwa, M ;

Delespesse, G ;

Sarfati, M .

JOURNAL OF EXPERIMENTAL MEDICINE, 1999, 190 (08) :1175-1181

[6]

ASCH AS, 1989, PROG HEMOST THROMB, V9, P157

[7] THROMBOSPONDIN SEQUENCE MOTIF (CSVTCG) IS RESPONSIBLE FOR CD36-BINDING [J].

ASCH, AS ;

SILBIGER, S ;

HEIMER, E ;

NACHMAN, RL .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1992, 182 (03) :1208-1217

[8] ISOLATION OF THE THROMBOSPONDIN MEMBRANE-RECEPTOR [J].

ASCH, AS ;

BARNWELL, J ;

SILVERSTEIN, RL ;

NACHMAN, RL .

JOURNAL OF CLINICAL INVESTIGATION, 1987, 79 (04) :1054-1061

[9] ANALYSIS OF CD36 BINDING DOMAINS - LIGAND SPECIFICITY CONTROLLED BY DEPHOSPHORYLATION OF AN ECTODOMAIN [J].

ASCH, AS ;

LIU, I ;

BRICCETTI, FM ;

BARNWELL, JW ;

KWAKYEBERKO, F ;

DOKUN, A ;

GOLDBERGER, J ;

PERNAMBUCO, M .

SCIENCE, 1993, 262 (5138) :1436-1440

[10]

ASCH AS, 1985, BLOOD, V66, P926

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