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兔、猪和小鼠血管生成素的表征与测序:对功能重要残基和区域的识别

Characterization and sequencing of rabbit, pig and mouse angiogenins: discernment of functionally important residues and regions.

作者信息

Bond M D, Strydom D J, Vallee B L

机构信息

Center for Biochemical and Biophysical Sciences and Medicine, Harvard Medical School, Boston, MA 02115.

出版信息

Biochim Biophys Acta. 1993 Mar 5;1162(1-2):177-86. doi: 10.1016/0167-4838(93)90145-h.

Abstract

Rabbit, pig and mouse angiogenins have been purified from blood serum and characterized, and the rabbit and pig proteins have been sequenced fully. A partial sequence of the mouse protein is consistent with the sequence deduced from the genomic DNA (Bond, M.D. and Vallee, B.L. (1990) Biochem. Biophys. Res. Commun. 171, 988-995). All three angiogenins are homologous to the pancreatic RNases and contain the essential catalytic residues His-13, Lys-40 and His-114, and the 6 half-cystines of the human protein. Like human angiogenin they display extremely low ribonucleolytic activities toward wheat-germ RNA, yeast RNA, poly(C) and poly(U). The rabbit and pig proteins induce neovascularization in vivo and also inhibit protein synthesis in vitro. The interaction of rabbit, pig and bovine angiogenins with placental ribonuclease inhibitor, a potent inhibitor of angiogenin, was examined by fluorescence spectroscopy. Rate and equilibrium binding constants indicate that rabbit angiogenin binds to the inhibitor much like human angiogenin, whereas the pig and bovine proteins show significant differences. A comparison of the five angiogenin sequences now available points to specific residues that are highly conserved among them but differ from the corresponding residues in the RNases. These residues are clustered in particular regions of the three-dimensional structure, two of which contribute to the angiogenic, second-messenger and/or protein synthesis inhibition activities of human angiogenin.

摘要

兔、猪和小鼠的血管生成素已从血清中纯化并进行了特性鉴定,兔和猪的蛋白质已完成全序列测定。小鼠蛋白质的部分序列与从基因组DNA推导的序列一致(邦德,医学博士和瓦利,B.L.(1990年)《生物化学与生物物理学研究通讯》171卷,988 - 995页)。所有这三种血管生成素都与胰腺核糖核酸酶同源,并且含有必需的催化残基组氨酸-13、赖氨酸-40和组氨酸-114,以及人蛋白质中的6个半胱氨酸。与人血管生成素一样,它们对小麦胚芽RNA、酵母RNA、聚(C)和聚(U)显示出极低的核糖核酸酶活性。兔和猪的蛋白质在体内可诱导新血管形成,在体外也能抑制蛋白质合成。通过荧光光谱法研究了兔、猪和牛的血管生成素与胎盘核糖核酸酶抑制剂(一种血管生成素的强效抑制剂)的相互作用。速率和平衡结合常数表明,兔血管生成素与抑制剂的结合方式与人血管生成素非常相似,而猪和牛的蛋白质则显示出显著差异。对现有的五个血管生成素序列进行比较,发现了它们之间高度保守但与核糖核酸酶中相应残基不同的特定残基。这些残基聚集在三维结构的特定区域,其中两个区域对人血管生成素的血管生成、第二信使和/或蛋白质合成抑制活性有贡献。

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