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人纤溶酶原、凝血酶原、组织纤溶酶原激活物、尿激酶和凝血因子XII的kringle结构域之间的遗传关系。

The genetic relationships between the kringle domains of human plasminogen, prothrombin, tissue plasminogen activator, urokinase, and coagulation factor XII.

作者信息

Castellino F J, Beals J M

机构信息

Department of Chemistry, University of Notre Dame, Indiana 46556.

出版信息

J Mol Evol. 1987;26(4):358-69. doi: 10.1007/BF02101155.

Abstract

A computer-based statistical evaluation of the optimal alignments of the kringle domains of human plasminogen, human prothrombin, human tissue plasminogen activator, human urokinase, and human coagulation Factor XIIa, as well as the putative kringle of human haptoglobin, has been performed. A variety of different alignments has been examined and scores calculated in terms of the number of standard deviations (SD) of a given match from randomness. With the exception of human haptoglobin, it was found that very high alignment scores (8.9-23.0 SD from randomness) were obtained between each of the kringles, with the kringle 1 and kringle 5 regions of human plasminogen displaying the highest similarity, and the S kringle of human prothrombin and the human Factor XII kringle showing the least similarity. The relationships obtained were employed to construct an evolutionary tree for the kringles. The predicted alignments have also allowed nucleotide mutations in these regions to be evaluated more accurately. For those regions for which nucleotide sequences are known, we have employed the maximal alignments from the protein sequences to assess nucleotide sequence similarities. It was found that a range of approximately 40-55% of the nucleotide bases were placed at identical positions in the kringles, with the highest number found in the alignment of the two kringles of human tissue plasminogen activator and the lowest number in the alignment of the S kringle of prothrombin with the second kringle of tissue plasminogen activator. From both protein and nucleotide alignments, we conclude that haptoglobin is not statistically homologous to any other kringle. Secondary structural comparisons of the kringle regions have been predicted by a combination of the Burgess and Chou-Fasman methods. In general, the kringles display a very high number of beta-turns, and very low alpha-helical contents. From analysis of the predicted structures in relationship to the functional properties of these domains, it appears as though many of their functional differences can be related to possible conformational alterations resulting from amino acid substitutions in the kringles.

摘要

已对人纤溶酶原、人凝血酶原、人组织纤溶酶原激活剂、人尿激酶和人凝血因子XIIa的kringle结构域,以及人触珠蛋白的假定kringle结构域进行了基于计算机的最佳比对统计评估。已检查了各种不同的比对,并根据给定匹配与随机性的标准偏差(SD)数量计算得分。除人触珠蛋白外,发现每个kringle结构域之间都获得了非常高的比对分数(比随机性高8.9 - 23.0 SD),其中人纤溶酶原的kringle 1和kringle 5区域显示出最高的相似性,而人凝血酶原的S kringle结构域与人凝血因子XII的kringle结构域显示出最低的相似性。所获得的关系被用于构建kringle结构域的进化树。预测的比对也使得能够更准确地评估这些区域中的核苷酸突变。对于已知核苷酸序列的那些区域,我们利用蛋白质序列的最大比对来评估核苷酸序列的相似性。发现约40 - 55%的核苷酸碱基在kringle结构域中处于相同位置,在人组织纤溶酶原激活剂的两个kringle结构域的比对中发现的数量最高,而在凝血酶原的S kringle结构域与组织纤溶酶原激活剂的第二个kringle结构域的比对中发现的数量最低。从蛋白质和核苷酸比对中,我们得出结论,触珠蛋白在统计学上与任何其他kringle结构域都不同源。已通过Burgess方法和Chou - Fasman方法相结合预测了kringle区域的二级结构比较。一般来说,kringle结构域显示出非常高数量的β - 转角和非常低的α - 螺旋含量。通过分析预测结构与这些结构域的功能特性之间的关系,似乎它们的许多功能差异可能与kringle结构域中氨基酸取代导致的可能构象改变有关。

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