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首页> 外文期刊>British Journal of Haematology >Activation of caspases-9, -3 and -8 in human platelets triggered by BH3-only mimetic ABT-737 and calcium ionophore A23187: Caspase-8 is activated via bypass of the death receptors
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Activation of caspases-9, -3 and -8 in human platelets triggered by BH3-only mimetic ABT-737 and calcium ionophore A23187: Caspase-8 is activated via bypass of the death receptors

机译:仅BH3模拟物ABT-737和钙离子载体A23187触发的人血小板中caspases-9,-3和-8的激活:通过绕过死亡受体来激活caspase-8。

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摘要

Platelet apoptosis and activation have been studied in human platelets treated with BH3-only mimetic ABT-737 and calcium ionophore A23187, agents triggering apoptosis through the intrinsic mitochondrial pathway. Platelet apoptosis was determined as activation of crucial apoptosis-associated caspases, initiator caspase-9 of intrinsic apoptosis pathway, executioner caspase-3 and initiator caspase-8 of extrinsic death receptor pathway, and platelet activation was detected by P-selectin (CD62) exposure on the platelet surface. We found that ABT-737 predominantly induced activation of caspases-9, -3 and -8 rather than CD62 exposure, whereas A23187 induces both caspases activation and CD62 exposure. Caspase-8 activation was stimulated independently of the extrinsic apoptosis pathway via mitochondrial membrane permeabilization and depolarization. These data suggest that (i) caspase-8 activation is triggered in ABT-737- and A23187-treated anucleate platelets through the mitochondria-initiated caspase activation cascade bypassing the death receptors, and (ii) ABT-737-treated platelets are a useful experimental tool for discerning the role of platelet apoptosis in platelet function and survival.
机译:在仅用BH3模拟的ABT-737和钙离子载体A23187(通过内在的线粒体途径触发细胞凋亡的药物)治疗的人类血小板中,已经研究了血小板的细胞凋亡和活化。血小板凋亡被确定为关键的凋亡相关胱天蛋白酶,内在凋亡途径的启动子caspase-9,外源性死亡受体途径的execution子手caspase-3和启动子caspase-8的激活,并且通过P-选择素(CD62)暴露检测到血小板激活在血小板表面。我们发现,ABT-737主要诱导caspases-9,-3和-8的活化而不是CD62的活化,而A23187诱导caspases活化和CD62的活化。通过线粒体膜通透性和去极化作用独立于外在凋亡途径刺激Caspase-8激活。这些数据表明(i)通过线粒体引发的caspase激活级联绕过死亡受体,从而在ABT-737和A23187处理的无核血小板中触发caspase-8激活,并且(ii)ABT-737处理的血小板是有用的识别血小板凋亡在血小板功能和存活中的作用的实验工具。

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