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血小板磷脂对各种磷脂酶的不同敏感性以及凝血酶诱导的修饰。脂质结构域重排的可能证据。

Different susceptibilities of platelet phospholipids to various phospholipases and modifications induced by thrombin. Possible evidence of rearrangement of lipid domains.

作者信息

Wang C T, Tsai W J, Chang S M, Shiao Y J, Yang C C

出版信息

Biochim Biophys Acta. 1987 May 29;899(2):205-12. doi: 10.1016/0005-2736(87)90401-9.

Abstract

On the membrane surface of the human platelet, phosphatidylcholine (PC) and phosphatidylethanolamine (PE) were hydrolyzed to different extents by the snake venom phospholipases A2 of varying pI values. The susceptibility of platelet phospholipids to basic phospholipase A2 of Naja nigricollis (pI 10.6) has been reported (Wang et al. (1986) Biochim. Biophys. Acta 856, 244-258). The susceptibilities of platelet phospholipids to acidic phospholipase A2 of Naja naja atra (pI 5.2) and to neutral phospholipase A2 of Hemachatus haemachatus (pI 7.3) were investigated in this study. In gel-filtered platelets, acidic phospholipase A2 hydrolyzed 35% PC and 10% PE, while neutral phospholipase A2 hydrolyzed 18% PC and 3% PE. In thrombin-induced shape-changed platelets, acidic phospholipase A2 hydrolyzed 20% PC and 10% PE, while neutral phospholipase A2 hydrolyzed 15% PC and 6% PE. In thrombin-activated platelets, acidic phospholipase A2 hydrolyzed 25% PC and 7% PE, while neutral phospholipase A2 hydrolyzed 25% PC and 10% PE. Sequential lipid hydrolysis experiments showed that basic phospholipase A2 of Naja nigricollis could hydrolyze the remaining PC and PE in the membrane previously treated with the neutral enzyme. The results may mean that: the PC and the PE domains exist on the platelet membrane surface; and the lipid domains on the membrane surface of resting platelets are rearranged by thrombin.

摘要

在人血小板的膜表面,不同pI值的蛇毒磷脂酶A2对磷脂酰胆碱(PC)和磷脂酰乙醇胺(PE)的水解程度不同。已有报道(Wang等人,(1986年)《生物化学与生物物理学学报》856卷,244 - 258页)关于血小板磷脂对眼镜蛇(pI 10.6)碱性磷脂酶A2的敏感性。本研究调查了血小板磷脂对眼镜蛇(pI 5.2)酸性磷脂酶A2和锯鳞蝰(pI 7.3)中性磷脂酶A2的敏感性。在凝胶过滤的血小板中,酸性磷脂酶A2水解35%的PC和10%的PE,而中性磷脂酶A2水解18%的PC和3%的PE。在凝血酶诱导形状改变的血小板中,酸性磷脂酶A2水解20%的PC和10%的PE,而中性磷脂酶A2水解15%的PC和6%的PE。在凝血酶激活的血小板中,酸性磷脂酶A2水解25%的PC和7%的PE,而中性磷脂酶A2水解25%的PC和10%的PE。连续脂质水解实验表明,眼镜蛇的碱性磷脂酶A2可以水解先前用中性酶处理过的膜中剩余的PC和PE。结果可能意味着:PC和PE结构域存在于血小板膜表面;静息血小板膜表面的脂质结构域被凝血酶重新排列。

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