首页> 外文OA文献 >Aggretin, a heterodimeric C-type lectin from Calloselasma rhodostoma (malayan pit viper), stimulates platelets by binding to alpha 2beta 1 integrin and glycoprotein Ib, activating Syk and phospholipase Cgamma 2, but does not involve the glycoprotein VI/Fc receptor gamma chain collagen receptor
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Aggretin, a heterodimeric C-type lectin from Calloselasma rhodostoma (malayan pit viper), stimulates platelets by binding to alpha 2beta 1 integrin and glycoprotein Ib, activating Syk and phospholipase Cgamma 2, but does not involve the glycoprotein VI/Fc receptor gamma chain collagen receptor

机译:Aggretin,一种来自Calloselasma rhodostoma(马来亚蛇毒蛇)的异二聚体C型凝集素,通过与α2beta 1整联蛋白和糖蛋白Ib结合,激活Syk和磷脂酶Cgamma 2来刺激血小板,但不涉及糖蛋白VI / Fc受体γ链胶原蛋白受体

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摘要

Aggretin, a potent platelet activator, was isolated from Calloselasma rhodostoma venom, and 30-amino acid N-terminal sequences of both subunits were determined. Aggretin belongs to the heterodimeric snake C-type lectin family and is thought to activate platelets by binding to platelet glycoprotein alpha(2)beta(1). We now show that binding to glycoprotein (GP) Ib is also required. Aggretin-induced platelet activation was inhibited by a monoclonal antibody to GPIb as well as by antibodies to alpha(2)beta(1). Binding of both of these platelet receptors to aggretin was confirmed by affinity chromatography. No binding of other major platelet membrane glycoproteins, in particular GPVI, to aggretin was detected. Aggretin also activates platelets from Fc receptor gamma chain (Fcgamma)-deficient mice to a greater extent than those from normal control mice, showing that it does not use the GPVI/Fcgamma pathway. Platelets from Fcgamma-deficient mice expressed fibrinogen receptors normally in response to collagen, although they did not aggregate, indicating that these platelets may partly compensate via other receptors including alpha(2)beta(1) or GPIb for the lack of the Fcgamma pathway. Signaling by aggretin involves a dose-dependent lag phase followed by rapid tyrosine phosphorylation of a number of proteins. Among these are p72(SYK), p125(FAK), and PLCgamma2, whereas, in comparison with collagen and convulxin, the Fcgamma subunit neither is phosphorylated nor coprecipitates with p72(SYK). This supports an independent, GPIb- and integrin-based pathway for activation of p72(SYK) not involving the Fcgamma receptor.
机译:从强直性疟原虫蛇毒瘤毒液中分离了一种有效的血小板活化剂Aggretin,测定了两个亚基的30个氨基酸的N端序列。 Aggretin属于异二聚体蛇C型凝集素家族,被认为通过与血小板糖蛋白alpha(2)beta(1)结合来激活血小板。我们现在显示还需要与糖蛋白(GP)Ib结合。 Aggretin诱导的血小板活化受到针对GPIb的单克隆抗体以及针对alpha(2)beta(1)的抗体的抑制。通过亲和色谱法证实了这两种血小板受体与聚集素的结合。没有检测到其他主要的血小板膜糖蛋白,特别是GPVI与凝集素的结合。 Aggretin还比正常对照小鼠更大程度地活化了来自Fc受体γ链(Fcgamma)缺陷小鼠的血小板,这表明它不使用GPVI / Fcgamma途径。来自Fcgamma缺陷型小鼠的血小板正常表达胶原蛋白时会产生纤维蛋白原受体,尽管它们没有聚集,表明这些血小板可能会通过其他受体(包括alpha(2)beta(1)或GPIb)部分补偿缺乏Fcgamma途径。聚集蛋白的信号转导涉及剂量依赖性的迟滞期,随后是许多蛋白质的酪氨酸快速磷酸化。其中有p72(SYK),p125(FAK)和PLCgamma2,而与胶原蛋白和惊厥毒素相比,Fcgamma亚基既不被磷酸化也不与p72(SYK)共沉淀。这支持了一个独立的,基于GPIb和整联蛋白的途径来激活不涉及Fcγ受体的p72(SYK)。

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