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首页> 外文期刊>The biochemical journal >Human platelet glycoprotein IIIb binds to thrombospondin fragments bearing the C-terminal region, and/or the type I repeats (CSVTCG motif), but not to the N-terminal heparin-binding region
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Human platelet glycoprotein IIIb binds to thrombospondin fragments bearing the C-terminal region, and/or the type I repeats (CSVTCG motif), but not to the N-terminal heparin-binding region

机译:人血小板糖蛋白IIIb与带有C末端区域的血小板反应蛋白片段结合,和/或I型重复序列(CSVTCG基序),但不与N末端肝素结合区域结合

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pMajor blood membrane platelet glycoprotein IIIb (GPIIIb), also termed GPIV or CD365, has been identified as a receptor for thrombospondin (TSP), collagen and Plasmodium falciparum-infected erythrocytes. The aim of the present study was to identify region(s) of TSP involved in binding of GPIIIb. Proteolytic fragments of TSP (M(r) 140 kDa, 120-18 kDa and 27 kDa on SDS/PAGE under reducing conditions) were purified by f.p.l.c. and identified by N-terminal gas-phase sequencing, e.l.i.s.a. and Western blots using monoclonal antibodies directed against defined domains of TSP. The 140 kDa and 120-18 kDa fragments (C-terminal region), but not the 27 kDa fragment (N-terminal region), were shown to bind to GPIIIb by using e.l.i.s.a. and affinity-chromatography systems. TSP binding to a GPIIIb-affinity column was Ca(2+)-dependent and reduced by 45% in the presence of EDTA. Moreover, TSP was only partially eluted with EDTA from a Ca(2+)-equilibrated GPIIIb column. A fragment of 68 kDa, obtained by further digestion of the 140 kDa fragment, bound to the GPIIIb-Sepharose affinity column. This fragment, or stalk-like region, bears the TSP type I repeats that show sequence similarity to regions on properdin, Plasmodium falciparum proteins and antistasin. Peptides (CSVTCG or SVTCGGGV) representing these repeats bound isolated GPIIIb in a Ca(2+)-independent way, but did not completely inhibit the GPIIIb and TSP interaction. These studies indicate that GPIIIb binds to the TSP via the C-terminal region and/or the CSVTCG motif, but not to the N-terminal region. Interaction between GPIIIb and the TSP C-terminal region or the CSVTCG motif is respectively Ca(2+)-dependent and -independent./p
机译:>主要膜血小板糖蛋白IIIb(GPIIIb),也称为GPIV或CD365,已被确定为血小板反应蛋白(TSP),胶原蛋白和恶性疟原虫感染的红细胞的受体。本研究的目的是鉴定参与GPIIIb结合的TSP区域。通过f.p.l.c纯化TSP的蛋白水解片段(在还原条件下在SDS / PAGE上的M(r)140kDa,120-18kDa和27kDa)。并通过N端气相测序法(e.l.i.s.a.和针对TSP定义域的单克隆抗体进行Western印迹分析。通过使用e.i.s.a.显示140 kDa和120-18 kDa片段(C末端区域)而不是27 kDa片段(N末端区域)与GPIIIb结合。和亲和层析系统。 TSP绑定到GPIIIb亲和柱是Ca(2+)依赖性的,并且在EDTA存在下降低了45%。此外,TSP仅用EDTA从Ca(2+)平衡的GPIIIb柱中部分洗脱。通过进一步消化140 kDa片段获得的68 kDa片段与GPIIIb-Sepharose亲和柱结合。该片段或茎状区域带有I型TSP重复序列,该序列与备解素,恶性疟原虫蛋白和抗stasstin上的区域显示出序列相似性。代表这些重复的肽(CSVTCG或SVTCGGGV)以独立于Ca(2+)的方式结合分离的GPIIIb,但没有完全抑制GPIIIb和TSP的相互作用。这些研究表明GPIIIb通过C末端区域和/或CSVTCG基序与TSP结合,但不与N末端区域结合。 GPIIIb与TSP C末端区域或CSVTCG基序之间的相互作用分别是Ca(2+)依赖性和-In依赖性。

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