GPVI受体介导血小板活化变异性的理论解释

A. A. Martyanov, M. G. Stepanyan, A. N. Sveshnikova
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引用次数: 0

摘要

血小板是负责防止血管受损时失血的非核细胞,其表面的关键受体之一是细胞外基质蛋白胶原糖蛋白VI (GPVI)的受体。GPVI触发血小板中的酪氨酸激酶信号,同时通过磷脂酶c - γ - 2 (plc - γ - 2)启动钙信号和通过磷酸肌醇-3-激酶(PI3K)启动磷酸肌醇信号。之前,我们的研究小组证明,在健康的供体中,通过GPVI受体激活的钙反应有两倍以上的变异性。本文提出了一个通过GPVI受体激活血小板的计算机模型来解释这一现象。该模型是一个用LSODA方法集成的常微分方程组。模型方程来源于我们之前发表的通过CLEC-2受体激活血小板的模型。利用所建立的模型,预测血小板活化程度对GPVI受体数量的单调依赖性。对模型参数的敏感性分析表明,血小板对GPVI活化的反应由GPVI受体的数量以及酪氨酸激酶的催化参数决定,而受体数量的两倍变化足以解释所观察到的现象。因此,理论上可以预测,健康供者血小板表面GPVI受体数量的变化可以决定血小板对GPVI受体刺激的钙反应的变异性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Theoretical Explanation for the Variability in Platelet Activation through the GPVI Receptor

One of the key receptors on the surface of platelets, non-nuclear cells responsible for preventing blood loss when blood vessels are damaged, is the receptor for the extracellular matrix protein collagen, glycoprotein VI (GPVI). GPVI triggers tyrosine kinase signaling in platelets, simultaneously initiating calcium signaling via phospholipase Cγ2 (PLCγ2) and phosphoinositide signaling via phosphoinositide-3-kinase (PI3K). Previously, our group demonstrated that among healthy donors there is more than a twofold variability in calcium response to activation through the GPVI receptor. Here, a computer model of platelet activation through the GPVI receptor is proposed to explain this phenomenon. This model is a system of ordinary differential equations integrated with the LSODA method. The model equations were derived from our previously published model of platelet activation via the CLEC-2 receptor. Using the developed model, a monotonic dependence of the degree of platelet activation on the number of GPVI receptors was predicted. An analysis of the sensitivity of the model to its parameters showed that the platelet response to activation through GPVI is determined by the number of GPVI receptors, as well as the catalytic parameters of tyrosine kinases, while a twofold change in the number of receptors is sufficient to explain the observed phenomenon. Thus, it was theoretically predicted that the variability of calcium responses of platelets to their stimulation through the GPVI receptor could be determined by the variability in the number of GPVI receptors on the platelet surface of healthy donors.

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来源期刊
CiteScore
1.40
自引率
0.00%
发文量
28
期刊介绍: Biochemistry (Moscow), Supplement Series A: Membrane and Cell Biology   is an international peer reviewed journal that publishes original articles on physical, chemical, and molecular mechanisms that underlie basic properties of biological membranes and mediate membrane-related cellular functions. The primary topics of the journal are membrane structure, mechanisms of membrane transport, bioenergetics and photobiology, intracellular signaling as well as membrane aspects of cell biology, immunology, and medicine. The journal is multidisciplinary and gives preference to those articles that employ a variety of experimental approaches, basically in biophysics but also in biochemistry, cytology, and molecular biology. The journal publishes articles that strive for unveiling membrane and cellular functions through innovative theoretical models and computer simulations.
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