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Aegyptin 对胶原蛋白中 von Willebrand 因子结合位点(RGQOGVMGF)具有高亲和力,并在体内抑制颈总动脉血栓形成。

Aegyptin displays high-affinity for the von Willebrand factor binding site (RGQOGVMGF) in collagen and inhibits carotid thrombus formation in vivo.

机构信息

Section of Vector Biology, Laboratory of Malaria and Vector Research, National Institute of Allergy and Infectious Diseases/NIH, Bethesda, MD 20852, USA.

出版信息

FEBS J. 2010 Jan;277(2):413-27. doi: 10.1111/j.1742-4658.2009.07494.x. Epub 2009 Dec 15.

Abstract

Aegyptin is a 30 kDa mosquito salivary gland protein that binds to collagen and inhibits platelet aggregation. We have studied the biophysical properties of aegyptin and its mechanism of action. Light-scattering plot showed that aegyptin has an elongated monomeric form, which explains the apparent molecular mass of 110 kDa estimated by gel-filtration chromatography. Surface plasmon resonance identified the sequence RGQOGVMGF (where O is hydroxyproline) that mediates collagen interaction with von Willebrand factor (vWF) as a high-affinity binding site for aegyptin, with a K(D) of approximately 5 nM. Additionally, aegyptin interacts with the linear peptide RGQPGVMGF and heat-denatured collagen, indicating that the triple helix and hydroxyproline are not a prerequisite for binding. However, aegyptin does not interact with scrambled RGQPGVMGF peptide. Aegyptin also recognizes the peptides (GPO)(10) and GFOGER with low affinity (microM range), which respectively represent glycoprotein VI and integrin alpha2beta1 binding sites in collagen. Truncated forms of aegyptin were engineered, and the C-terminus fragment was shown to interact with collagen and to attenuate platelet aggregation. In addition, aegyptin prevents laser-induced carotid thrombus formation in the presence of Rose Bengal in vivo, without significant bleeding in rats. In conclusion, aegyptin interacts with distinct binding sites in collagen, and is useful tool to inhibit platelet-collagen interaction in vitro and in vivo.

摘要

埃及伊蚊唾液腺蛋白 30kDa 是一种与胶原蛋白结合并抑制血小板聚集的蛋白。我们研究了埃及伊蚊唾液腺蛋白的生物物理特性及其作用机制。光散射图谱表明,埃及伊蚊唾液腺蛋白呈长形单体形式,这解释了凝胶过滤色谱法估计的 110kDa 的表观分子量。表面等离子体共振鉴定出与 von Willebrand 因子(vWF)介导胶原蛋白相互作用的序列 RGQOGVMGF(其中 O 是羟脯氨酸)是埃及伊蚊唾液腺蛋白的高亲和力结合位点,K(D)约为 5nM。此外,埃及伊蚊唾液腺蛋白还与线性肽 RGQPGVMGF 和热变性胶原蛋白相互作用,表明三螺旋和羟脯氨酸不是结合的必要条件。然而,埃及伊蚊唾液腺蛋白与 scrambled RGQPGVMGF 肽没有相互作用。埃及伊蚊唾液腺蛋白还识别低亲和力(微摩尔范围)的肽(GPO)(10)和 GFOGER,它们分别代表胶原蛋白中糖蛋白 VI 和整合素 alpha2beta1 的结合位点。设计了埃及伊蚊唾液腺蛋白的截断形式,结果表明 C 端片段与胶原蛋白相互作用并抑制血小板聚集。此外,埃及伊蚊唾液腺蛋白在体内存在 Rose Bengal 的情况下可防止激光诱导的颈动脉血栓形成,而在大鼠中没有明显出血。总之,埃及伊蚊唾液腺蛋白与胶原蛋白中的不同结合位点相互作用,是体外和体内抑制血小板-胶原蛋白相互作用的有用工具。

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