Dolutegravir potentiates platelet activation by a calcium-dependent, ionophore-like mechanism.

IF 2.4 4区 医学 Q3 TOXICOLOGY
Morris Madzime, Annette J Theron, Ronald Anderson, Gregory R Tintinger, Helen C Steel, Pieter W A Meyer, Jan G Nel, Charles Feldman, Theresa M Rossouw
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引用次数: 1

Abstract

Dolutegravir is a highly potent HIV integrase strand transfer inhibitor that is recommended for first-line anti-retroviral treatment in all major treatment guidelines. A recent study has shown that people taking this class of anti-retroviral treatment have a substantially higher risk of early-onset cardiovascular disease, a condition shown previously to be associated with increased platelet reactivity. To date, few studies have explored the effects of dolutegravir on platelet activation. Accordingly, the current study was undertaken with the primary objective of investigating the effects of dolutegravir on the reactivity of human platelets in vitro. Platelet-rich plasma, isolated platelets, or buffy coat cell suspensions prepared from the blood of healthy adults were treated with dolutegravir (2.5-10 µg/ml), followed by activation with adenosine 5'-diphosphate (ADP), thrombin, or a thromboxane A2 receptor agonist U46619. Expression of platelet CD62P (P-selectin), formation of heterotypic neutrophil:platelet aggregates, and calcium (Ca2+) fluxes were measured using flow cytometry and fluorescence spectrometry, respectively. Dolutegravir caused dose-related potentiation of ADP-, thrombin- and U46619-activated expression of CD62P by platelets, as well as a significant increases in formation of neutrophil:platelet aggregates. These effects were paralleled by a spontaneous, receptor-independent elevation in cytosolic Ca2+ that appears to underpin the mechanism by which the antiretroviral agent augments the responsiveness of these cells to ADP, thrombin and U46619. The most likely mechanism of dolutegravir-mediated increases in platelet cytosolic Ca2+ relates to a combination of lipophilicity and divalent/trivalent metal-binding and/or chelating properties of the anti-retroviral agent. These properties are likely to confer ionophore-type activities on dolutegravir that would promote movement of Ca2+ across the plasma membrane, delivering the cation to the cytosol where it would augment Ca2+-dependent intracellular signaling mechanisms. These effects of dolutegravir may lead to hyper-activation of platelets which, if operative in vivo, may contribute to an increased risk for cardiometabolic co-morbidities.

多来替韦通过钙依赖的离子载体样机制增强血小板活化。
Dolutegravir是一种高效的HIV整合酶链转移抑制剂,在所有主要治疗指南中推荐用于一线抗逆转录病毒治疗。最近的一项研究表明,接受这类抗逆转录病毒治疗的人患早发性心血管疾病的风险要高得多,而早发性心血管疾病先前被证明与血小板反应性增加有关。迄今为止,很少有研究探讨多替重力韦对血小板活化的影响。因此,本研究的主要目的是研究多替格拉韦对体外人血小板反应性的影响。用多替重力韦(2.5-10µg/ml)处理从健康成人血液中制备的富血小板血浆、分离血小板或黄皮细胞悬浮液,然后用5'-二磷酸腺苷(ADP)、凝血酶或血栓素A2受体激动剂U46619激活。分别用流式细胞术和荧光光谱法测定血小板CD62P (p -选择素)的表达、异型中性粒细胞的形成、血小板聚集体和钙(Ca2+)通量。Dolutegravir引起ADP-、凝血酶-和u46619的剂量相关增强,激活血小板CD62P的表达,并显著增加中性粒细胞血小板聚集体的形成。这些效应与细胞内自发的、不依赖受体的Ca2+升高相平行,这似乎支持了抗逆转录病毒药物增强这些细胞对ADP、凝血酶和U46619的反应性的机制。dolutegravvir介导的血小板胞浆Ca2+增加最可能的机制与亲脂性和抗逆转录病毒药物的二价/三价金属结合和/或螯合特性的结合有关。这些特性可能赋予dolutegravir离子载体类型的活性,从而促进Ca2+在质膜上的运动,将阳离子传递到细胞质中,从而增强Ca2+依赖的细胞内信号传导机制。多替格拉韦的这些作用可能导致血小板过度活化,如果在体内手术,可能会增加心脏代谢合并症的风险。
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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来源期刊
Journal of Immunotoxicology
Journal of Immunotoxicology 医学-毒理学
CiteScore
6.70
自引率
3.00%
发文量
26
审稿时长
1 months
期刊介绍: The Journal of Immunotoxicology is an open access, peer-reviewed journal that provides a needed singular forum for the international community of immunotoxicologists, immunologists, and toxicologists working in academia, government, consulting, and industry to both publish their original research and be made aware of the research findings of their colleagues in a timely manner. Research from many subdisciplines are presented in the journal, including the areas of molecular, developmental, pulmonary, regulatory, nutritional, mechanistic, wildlife, and environmental immunotoxicology, immunology, and toxicology. Original research articles as well as timely comprehensive reviews are published.
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