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一种分析抗体基因家族多样性的数学方法。

A mathematical approach to the analysis of diversity in antibody gene families.

作者信息

Hood J M, Loh E Y, Hood L

出版信息

Biochem Genet. 1976 Jun;14(5-6):467-79. doi: 10.1007/BF00486127.

Abstract

In this article, we develop a mathematical approach for the analysis of diversity in antibody gene families. This approach is arrived at by examing two general questions about protein populations: (1) What is a relative measure of the diversity exhibited by one protein family when compared with a second? (2) What is the probability that two protein populations were derived from a single common population? These quantitative approaches permit a variety of precise evolutionary, genetic, and developmental questions to be asked of antibody gene families. Using this methodology, we demonstrate that the diversity in mouse K-immunoglobulin chains is considerably greater than in their human K counterparts. We also show that the variable (Vl) regions of light chains associated with IgG and IgA immunoglobulins in the mouse appear to have been derived from a common population of Vl genes. This approach also can be used to analyse sequence data from other informational multigene families.

摘要

在本文中,我们开发了一种数学方法来分析抗体基因家族的多样性。这种方法是通过研究关于蛋白质群体的两个一般性问题得出的:(1)与第二个蛋白质家族相比,一个蛋白质家族所展现的多样性的相对度量是什么?(2)两个蛋白质群体源自单个共同群体的概率是多少?这些定量方法使得针对抗体基因家族能够提出各种精确的进化、遗传和发育问题。使用这种方法,我们证明小鼠K免疫球蛋白链的多样性远大于其人类K对应物。我们还表明,小鼠中与IgG和IgA免疫球蛋白相关的轻链可变(Vl)区域似乎源自Vl基因的一个共同群体。这种方法也可用于分析来自其他信息多基因家族的序列数据。

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