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血浆蛋白酶、凝血酶和纤溶酶在体外可降解兔主动脉段的蛋白聚糖:一项超微结构与生化综合研究。

The plasma proteases, thrombin and plasmin, degrade the proteoglycan of rabbit aorta segments in vitro: an integrated ultrastructural and biochemical study.

作者信息

Richardson M, Hatton M W, Moore S

机构信息

Department of Pathology, McMaster University Medical Centre, Hamilton, Ontario.

出版信息

Clin Invest Med. 1988 Apr;11(2):139-50.

PMID:2969314
Abstract

The effects of plasmin and thrombin on the proteoglycan component of uninjured and deendothelialized rabbit thoracic aorta were examined in vitro. Aortas labelled with 35S in vivo, were exposed to each protease and the 35S-products released from the vessel were analysed. Aortas exposed to the same enzymes were examined by transmission electron microscopy of ruthenium red-stained sections, and the proteoglycan content evaluated by morphometric analysis. In uninjured vessels with endothelium intact, there was no evidence of release of proteoglycan by either enzyme unless very high concentrations were used. High concentrations of both plasmin and thrombin induced vacuolation of endothelial cells, and changes in the fine structure of smooth muscle cells. In contrast exposure of de-endothelialized vessels to smaller concentrations of plasmin or thrombin resulted in a significant loss of proteoglycan, and less marked changes in the morphology of the smooth muscle cells. Thrombin treatment released 35S-labelled products containing chondroitin-, dermatan- and heparan-sulphates whereas plasmin released products containing only chondroitin- and dermatan-sulphates together with other, unknown 35S-labelled products. These observations indicate the potential of non-specific, plasma-derived proteases to degrade arterial connective tissue.

摘要

在体外研究了纤溶酶和凝血酶对未损伤及去内皮兔胸主动脉蛋白聚糖成分的影响。将体内用35S标记的主动脉暴露于每种蛋白酶,并分析从血管中释放的35S产物。通过对钌红染色切片进行透射电子显微镜检查,对暴露于相同酶的主动脉进行检查,并通过形态计量分析评估蛋白聚糖含量。在未损伤且内皮完整的血管中,除非使用非常高的浓度,否则没有证据表明这两种酶会释放蛋白聚糖。高浓度的纤溶酶和凝血酶均可诱导内皮细胞空泡化以及平滑肌细胞精细结构的改变。相比之下,将去内皮的血管暴露于较低浓度的纤溶酶或凝血酶会导致蛋白聚糖显著丢失,且平滑肌细胞形态变化不太明显。凝血酶处理释放出含有硫酸软骨素、硫酸皮肤素和硫酸乙酰肝素的35S标记产物,而纤溶酶释放出仅含有硫酸软骨素和硫酸皮肤素的产物以及其他未知的35S标记产物。这些观察结果表明血浆来源的非特异性蛋白酶具有降解动脉结缔组织的可能性。

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