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纤维蛋白原纤溶酶消化早期阶段Aα链和Bβ链裂解产物的免疫学鉴定

Immunologic identification of the cleavage products from the A alpha- and B beta-chains in the early stages of plasmin digestion of fibrinogen.

作者信息

Liu C Y, Sobel J H, Weitz J I, Kaplan K L, Nossel H L

出版信息

Thromb Haemost. 1986 Aug 20;56(1):100-6.

PMID:2946092
Abstract

Fragment X components (Mr 225,000 to 333,000) were distinguished on sodium dodecyl sulfate polyacrylamide gels. Western blotting with monoclonal antibodies to A alpha-chain segments demonstrated that the A alpha-chains of fibrinogen and the largest fragment X components (Mr 285,000-340,000) contained both A alpha 259-276 and A alpha 540-554. Fragment X components of Mr 270,000-285,000 contained A alpha 259-276 but lacked A alpha 540-554, whereas the smallest fragment X components (Mr 225,000-270,000) contained neither A alpha 540-554 nor A alpha 259-276. Studies of the small peptides generated during fragment X formation complemented the studies of the large molecules, by demonstrating peptides containing both A alpha 259-276 and A alpha 540-554 (Mr 41,600-41,800 and Mr 38,700-38,900), peptides containing A alpha 540-554 but not A alpha 259-276 (Mr 20,500-21,000 and Mr 17,300-17,500) and peptides containing only A alpha 259-276 (Mr 23,600-24,000 and Mr 20,500-21,000). Cleavage of B beta 1-42 from the amino terminal ends of the B beta-chains, measured with a specific radioimmunoassay, was linear until 1.6 moles per mole of fibrinogen had been released, and coincided with loss of the central and carboxy terminal A alpha-chain regions, i. e. A alpha 259-276 and A alpha 540-554. Based on present and previously reported data, a model is proposed for the evolution of the heterogeneous group of fragment X derivatives from fibrinogen with the simultaneous release of small peptides.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在十二烷基硫酸钠聚丙烯酰胺凝胶上可区分出片段X组分(分子量225,000至333,000)。用抗Aα链片段的单克隆抗体进行蛋白质印迹分析表明,纤维蛋白原的Aα链和最大的片段X组分(分子量285,000 - 340,000)同时含有Aα259 - 276和Aα540 - 554。分子量270,000 - 285,000的片段X组分含有Aα259 - 276但缺乏Aα540 - 554,而最小的片段X组分(分子量225,000 - 270,000)既不含有Aα540 - 554也不含有Aα259 - 276。对片段X形成过程中产生的小肽的研究通过证明同时含有Aα259 - 276和Aα540 - 554的肽(分子量41,600 - 41,800和分子量38,700 - 38,900)、含有Aα540 - 554但不含有Aα259 - 276的肽(分子量20,500 - 21,000和分子量17,300 - 17,500)以及仅含有Aα259 - 276的肽(分子量23,600 - 24,000和分子量20,500 - 21,000)补充了对大分子的研究。用特异性放射免疫测定法测定,从Bβ链氨基末端切除Bβ1 - 42呈线性,直至每摩尔纤维蛋白原释放出1.6摩尔,且与中央和羧基末端Aα链区域(即Aα259 - 276和Aα540 - 554)的丢失同时发生。基于目前和先前报道的数据,提出了一个关于纤维蛋白原衍生的片段X异质组进化并同时释放小肽的模型。(摘要截短于250字)

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