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通过具有凝血酶依赖性(U87MG)和二磷酸腺苷依赖性(SKNMC)血小板激活机制的人肿瘤细胞系的微泡对血栓形成进行形态计量学评估。

Morphometric evaluation of thrombogenesis by microvesicles from human tumor cell lines with thrombin-dependent (U87MG) and adenosine diphosphate-dependent (SKNMC) platelet-activating mechanisms.

作者信息

Bastida E, Escolar G, Ordinas A, Jamieson G A

出版信息

J Lab Clin Med. 1986 Dec;108(6):622-7.

PMID:3783031
Abstract

The Baumgartner perfusion apparatus has been used for quantitative comparison of the interaction of platelets with subendothelium in the presence of microvesicles derived from SKNMC (human neuroblastoma) cells, which aggregate platelets by an adenosine diphosphate (ADP)-dependent mechanism, and U87MG (human glioblastoma) cells, which function by a thrombin-dependent mechanism. The derived microvesicles from each line were as effective as the intact cells in inducing thrombogenesis on both undigested and alpha-chymotrypsin-digested subendothelium. Thrombus size on digested vessels was greater than on undigested vessels by fivefold for SKNMC cells and microvesicles and by 20-fold for U87MG cells and sevenfold for U87MG microvesicles. The results show that microvesicles from both cell lines initiate interactions between platelets and subendothelium identical to those caused by intact tumor cells. The results also demonstrate that intact tumor cells in the circulation may not be necessary for the thromboembolic complications of malignancy.

摘要

鲍姆加特纳灌注装置已用于定量比较血小板与内皮下层在存在源自SKNMC(人神经母细胞瘤)细胞的微泡和U87MG(人胶质母细胞瘤)细胞情况下的相互作用。SKNMC细胞通过二磷酸腺苷(ADP)依赖性机制聚集血小板,U87MG细胞则通过凝血酶依赖性机制发挥作用。来自每个细胞系的微泡在未消化和经α-糜蛋白酶消化的内皮下层上诱导血栓形成方面与完整细胞一样有效。对于SKNMC细胞和微泡,消化血管上的血栓大小比未消化血管上的大五倍;对于U87MG细胞,大20倍;对于U87MG微泡,大七倍。结果表明,来自两种细胞系的微泡引发的血小板与内皮下层之间的相互作用与完整肿瘤细胞引起的相互作用相同。结果还表明,循环中的完整肿瘤细胞对于恶性肿瘤的血栓栓塞并发症可能并非必需。

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