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海胆精子鞭毛动力蛋白ATP酶β重链上光解和胰蛋白酶裂解位点的图谱。

A map of photolytic and tryptic cleavage sites on the beta heavy chain of dynein ATPase from sea urchin sperm flagella.

作者信息

Mocz G, Tang W J, Gibbons I R

机构信息

Pacific Biomedical Research Center, University of Hawaii, Honolulu 96822.

出版信息

J Cell Biol. 1988 May;106(5):1607-14. doi: 10.1083/jcb.106.5.1607.

Abstract

NH2-terminal analysis of the alpha and beta heavy chain polypeptides (Mr greater than 400,000) from the outer arm dynein of sea urchin sperm flagella, compared with that of the 230,000- and 200,000-Mr peptides formed upon photocleavage of dynein by irradiation at 365 nm in the presence of vanadate and ATP, shows that the NH2 termini of the intact chains are acetylated and that the 230,000- and 200,000 Mr peptides constitute the amino- and carboxy-terminal portions of the heavy chains, respectively. Tryptic digestion of the beta heavy chain is known to separate it into two particles, termed fragments A and B, that sediment at 12S and 6S (Ow, R. A., W.-J. Y. Tang, G. Mocz, and I. R. Gibbons, 1987. J. Biol. Chem. 262:3409-3414). Immunoblots against monoclonal antibodies specific for epitopes on the beta heavy chain, used in conjunction with photoaffinity labeling, show that the ATPase-containing fragment A is derived from the amino-terminal region of the beta chain, with the two photolytic sites thought to be associated with the purine-binding and the gamma-phosphate-binding areas of the ATP-binding site spanning an approximately 100,000 Mr region near the middle of the intact beta chain. Fragment B is derived from the complementary carboxy-terminal region of the beta chain.

摘要

对海胆精子鞭毛外臂动力蛋白的α和β重链多肽(分子量大于400,000)进行氨基末端分析,并与在钒酸盐和ATP存在下于365nm照射使动力蛋白光裂解后形成的分子量为230,000和200,000的肽段进行比较,结果表明完整链的氨基末端被乙酰化,且分子量为230,000和200,000的肽段分别构成重链的氨基末端和羧基末端部分。已知对β重链进行胰蛋白酶消化可将其分离成两个颗粒,称为片段A和B,它们分别在12S和6S沉降(Ow,R. A.,W.-J. Y. Tang,G. Mocz和I. R. Gibbons,1987. J. Biol. Chem. 262:3409 - 3414)。结合光亲和标记,针对β重链上特定表位的单克隆抗体进行免疫印迹分析表明,含ATP酶的片段A源自β链的氨基末端区域,两个光解位点被认为与ATP结合位点的嘌呤结合区和γ磷酸结合区相关,跨越完整β链中部附近约100,000分子量的区域。片段B源自β链互补的羧基末端区域。

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