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糖化白蛋白修饰血小板黏附和聚集反应。

Glycated albumin modifies platelet adhesion and aggregation responses.

机构信息

a Department of Biomedical Engineering , Stony Brook University , Stony Brook , NY , USA.

出版信息

Platelets. 2017 Nov;28(7):682-690. doi: 10.1080/09537104.2016.1260703. Epub 2017 Jan 9.

DOI:10.1080/09537104.2016.1260703
PMID:28067098
Abstract

A diabetic vasculature is detrimental to cardiovascular health through the actions of advanced glycation end products (AGEs) on endothelial cells and platelets. Platelets activated by AGEs agonize endothelial responses promoting cardiovascular disease (CVD) development. While it has been established that AGEs can alter platelet functions, little is known about the specific platelet pathways that AGEs modify. Therefore, we evaluated the effects of AGEs on specific salient platelet pathways related to CVDs and whether the effects that AGEs elicit are dependent on glycation extent. To accomplish our objective, platelets were incubated with reversibly or irreversibly glycated albumin. A time course for adhesion and aggregation agonist receptor expression was assessed. Optical platelet aggregometry was used to confirm the functional activity of platelets after AGE exposure. In general, platelets subjected to glycated albumin had a significantly enhanced adhesion and aggregation potential. Furthermore, we observed an enhancement in dense body secretion and intracellular calcium concentration. This was especially prevalent for platelets exposed to irreversibly glycated albumin. Additionally, functional aggregation correlated well with receptor expression, suggesting that AGE-induced altered receptor sensitivity translated to altered platelet functions. Our findings indicate that under diabetic vascular conditions platelets become more susceptible to activation and aggregation due to an overall enhanced receptor expression, which may act to promote CVD development.

摘要

糖尿病血管对心血管健康有害,这是通过糖基化终产物 (AGEs) 对内皮细胞和血小板的作用实现的。AGEs 激活的血小板通过激动内皮细胞反应促进心血管疾病 (CVD) 的发展。虽然已经确定 AGEs 可以改变血小板功能,但对于 AGEs 修饰的特定血小板途径知之甚少。因此,我们评估了 AGEs 对与 CVD 相关的特定显著血小板途径的影响,以及 AGEs 引起的作用是否依赖于糖化程度。为了实现我们的目标,我们将血小板与可还原或不可还原的糖化白蛋白孵育。评估了粘附和聚集激动剂受体表达的时间过程。使用光学血小板聚集仪来确认 AGE 暴露后血小板的功能活性。一般来说,糖化白蛋白处理的血小板具有明显增强的粘附和聚集潜力。此外,我们观察到致密体分泌和细胞内钙离子浓度增加。这在暴露于不可还原糖化白蛋白的血小板中尤为明显。此外,功能聚集与受体表达很好地相关,这表明 AGE 诱导的改变的受体敏感性转化为改变的血小板功能。我们的研究结果表明,在糖尿病血管条件下,由于整体增强的受体表达,血小板更容易被激活和聚集,这可能会促进 CVD 的发展。

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