首页> 美国卫生研究院文献>Biochemical Journal >The integrin alpha IIb beta 3 contains distinct and interacting binding sites for snake-venom RGD (Arg-Gly-Asp) proteins. Evidence that the receptor-binding characteristics of snake-venom RGD proteins are related to the amino acid environment flanking the sequence RGD.

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The integrin alpha IIb beta 3 contains distinct and interacting binding sites for snake-venom RGD (Arg-Gly-Asp) proteins. Evidence that the receptor-binding characteristics of snake-venom RGD proteins are related to the amino acid environment flanking the sequence RGD.

机译：整联蛋白alpha IIb beta 3包含蛇毒RGD（Arg-Gly-Asp）蛋白的独特且相互作用的结合位点。蛇毒RGD蛋白的受体结合特性与序列RGD两侧的氨基酸环境有关的证据。

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We have previously demonstrated [Lu, Williams, Deadman, Salmon, Kakkar, Wilkinson, Baruch, Authi and Rahman (1994) Biochem. J. 304, 929-936] the preferential antagonism of the interactions of the integrin alpha IIb beta 3 on activated platelets with three immobilized glycoprotein ligands (fibrinogen, fibronectin and von Willebrand factor) by a selected panel of snake-venom RGD (Arg-Gly-Asp)-containing proteins including the disintegrins kistrin and elegantin, and the neurotoxin variant dendroaspin. Kistrin and dendroaspin, although structurally unrelated, contain similar amino acids flanking the tripeptide RGD and behaved as identical antagonists preferentially inhibiting platelet adhesion to immobilized fibrinogen as opposed to fibronectin. In contrast, elegantin, which shares extensive sequence similarity with kistrin but has different amino acids around the tripeptide RGD, preferentially inhibited platelet adhesion to immobilized fibronectin as opposed to fibrinogen. To develop further insights into the mechanisms underlying the preferential antagonism shown by the venom proteins in the adhesion studies, we, in the present study, sought to determine the binding properties of kistrin, elegantin and dendroaspin to the alpha IIb beta 3 complex by radioligand kinetic and competition studies. In direct binding experiments, both kistrin and dendroaspin were observed to bind to a single class of binding site on ADP-activated platelets with apparent equilibrium dissociation constant (Kdapp) values of 42 +/- 2 nM and 21 +/- 6 nM respectively. In competition studies, dendroaspin blocked the binding of 125I-labelled kistrin to ADP-activated platelets in a simple competitive manner, with an apparent equilibrium inhibition constant (Kiapp) of 143 +/- 14 nM, from which an indirect Kdapp = 22 nM for dendroaspin was determined. This result suggests that kistrin and dendroaspin bind to the same site on the integrin alpha IIb beta 3 consistent with their similar inhibitory properties. In contrast, elegantin recognized two classes of binding sites on the alpha IIb beta 3 complex with Kdapp values of 10.5 +/- 0.8 nM and 175 +/- 10 nM, and, unlike dendroaspin, did not inhibit the binding of 125I-labelled kistrin to ADP-activated platelets. However, in reciprocal experiments both kistrin and dendroaspin inhibited the binding of 125I-elegantin to ADP-activated platelets in a non-competitive manner, with Kiapp values of 34 +/- 3 nM and 21 +/- 2 nM respectively. Thus elegantin appears to interact with distinct but interacting sites on the alpha IIb beta 3 complex from the binding site of kistrin and dendroaspin, consistent with its distinctive inhibitory preferences as shown in platelet adhesion studies.(ABSTRACT TRUNCATED AT 400 WORDS)

机译：我们以前曾证明过[Lu，Williams，Deadman，Salmon，Kakkar，Wilkinson，Baruch，Authi和Rahman（1994）Biochem。 J. 304，929-936]通过选定的一组蛇毒RGD（Arg--）对整合素αIIb beta 3在活化的血小板上与三种固定的糖蛋白配体（纤维蛋白原，纤连蛋白和von Willebrand因子）的相互作用的优先拮抗作用。含有Gly-Asp）的蛋白质，包括整联蛋白，麒麟蛋白和莱曼汀，以及神经毒素变体树状毒素。尽管在结构上不相关，但Kistrin和dendroaspin含有相似的氨基酸，位于三肽RGD的侧翼，并且作为相同的拮抗剂，与纤连蛋白相对，优先抑制血小板粘附于固定的纤维蛋白原。相反，与纤连蛋白具有广泛的序列相似性但在三肽RGD周围具有不同氨基酸的莱曼汀则优先抑制血小板与固定的纤连蛋白的粘附，而不是与纤维蛋白原的粘附。为了进一步研究粘着研究中毒蛋白显示的优先拮抗作用的潜在机制，我们在本研究中试图通过放射性配体动力学确定Kistrin，Eleginin和Dendrosaspin与αIIb beta 3复合物的结合特性。和竞争研究。在直接结合实验中，观察到麒麟蛋白和树突蛋白都与ADP活化血小板上的一类结合位点结合，其表观平衡解离常数（Kdapp）值分别为42 +/- 2 nM和21 +/- 6 nM。在竞争研究中，树状毒菌素以一种简单的竞争方式阻止了125I标记的麒麟菜蛋白与ADP活化的血小板的结合，其表观平衡抑制常数（Kiapp）为143 +/- 14 nM，由此间接Kdapp = 22 nM。确定树突状毒素。该结果表明，麒麟蛋白和树突蛋白结合至整联蛋白αIIb beta 3上的相同位点，这与它们相似的抑制特性一致。相比之下，bealyin可以识别Kdapp值为10.5 +/- 0.8 nM和175 +/- 10 nM的alpha IIb beta 3复合体上的两类结合位点，并且与树突孢菌素不同，它不抑制125I标记的麒麟菜蛋白的结合ADP激活的血小板。然而，在对等实验中，麒麟蛋白和树突蛋白都以非竞争性方式抑制125 I-elegantin与ADP活化血小板的结合，Kiapp值分别为34 +/- 3 nM和21 +/- 2 nM。因此，lamanstin似乎与来自纤连蛋白和树突状毒素的结合位点的alpha IIb beta 3复合物上独特但相互作用的位点相互作用，这与血小板粘附研究中显示的其独特的抑制性偏好相吻合（摘要截短了400字）。

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期刊名称 Biochemical Journal
作者
S Rahman; X Lu; V V Kakkar; K S Authi;
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年(卷),期 1995(312),Pt 1
年度 1995
页码 223–232
总页数 10
原文格式 PDF
正文语种
中图分类分子生物学;
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专利

1. 华丽蛇毒素RGD序列上游点突变对结构和功能的影响分析 [J] . 徐存拴, 辛泽华, 等发育与生殖生物学报：英文版 . 2002,第004期
2. The integrin αIIbβ3 contains distinct and interacting binding sites for snake-venom RGD (Arg-Gly-Asp) proteins. Evidence that the receptor-binding characteristics of snake-venom RGD proteins are related to the amino acid environment flanking the sequence RGD [J] . K S Authi, S Rahman, V V Kakkar, The biochemical journal . 1995,第1期

机译：整联蛋白αIIbβ3包含蛇毒RGD（Arg-Gly-Asp）蛋白的独特且相互作用的结合位点。蛇毒RGD蛋白的受体结合特性与RGD序列侧翼的氨基酸环境有关的证据
3. THE INTEGRIN ALPHA(IIB)BETA(3) CONTAINS DISTINCT AND INTERACTING BINDING SITES FOR SNAKE-VENOM RGD (ARG-GLY-ASP) PROTEINS - EVIDENCE THAT THE RECEPTOR-BINDING CHARACTERISTICS OF SNAKE-VENOM RGD PROTEINS ARE RELATED TO THE AMINO ACID ENVIRONMENT FLANK [J] . Rahman S., Kakkar VV., Authi KS., The Biochemical Journal . 1995,第0期

机译：蛇毒RGD（ARG-GLY-ASP）蛋白质的整合和相互作用部位的整合素α（IIB）BETA（3）-证据表明与蛇毒RGD蛋白质的受体结合特性有关侧翼
4. Preferential antagonism of the interactions of the integrin αIIb β3 with immobilized glycoprotein ligands by snake-venom RGD (Arg-Gly-Asp) proteins. Evidence supporting a functional role for the amino acid residues flanking the tripeptide RGD in determining the inhibitory properties of snake-venom RGD proteins [J] . D Baruch, G P Salmon, J A Williams, The biochemical journal . 1994,第3期

机译：蛇毒RGD（Arg-Gly-Asp）蛋白对整合素αIIbβ3与固定的糖蛋白配体相互作用的优先拮抗作用。支持三肽RGD侧翼的氨基酸残基在确定蛇毒RGD蛋白抑制特性中的功能性作用的证据
5. Preferential antagonism of the interactions of the integrin alpha IIb beta 3 with immobilized glycoprotein ligands by snake-venom RGD (Arg-Gly-Asp) proteins. Evidence supporting a functional role for the amino acid residues flanking the tripeptide RGD in determining the inhibitory properties of snake-venom RGD proteins. [O] . X Lu, J A Williams, J J Deadman, 1994

机译：蛇毒RGD（Arg-Gly-Asp）蛋白对整合素αIIb beta 3与固定的糖蛋白配体相互作用的优先拮抗作用。支持三肽RGD侧翼的氨基酸残基在确定蛇毒RGD蛋白抑制特性方面发挥功能性作用的证据。
6. The integrin αIIbβ3 contains distinct and interacting binding sites for snake-venom RGD (Arg-Gly-Asp) proteins. Evidence that the receptor-binding characteristics of snake-venom RGD proteins are related to the amino acid environment flanking the sequence RGD [O] . S Rahman, X Lu, V V Kakkar, 1995

机译：整联蛋白αIIBβ3含有蛇毒液RGD（Arg-Gly-ASP）蛋白的不同和相互作用的结合位点。蛇 - 毒液RGD蛋白的受体结合特性与序列RGD序列的氨基酸环境有关

The integrin alpha IIb beta 3 contains distinct and interacting binding sites for snake-venom RGD (Arg-Gly-Asp) proteins. Evidence that the receptor-binding characteristics of snake-venom RGD proteins are related to the amino acid environment flanking the sequence RGD.

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