趋化因子及其受体家族分子适应性进化分析

遗传 ›› 2007, Vol. 29 ›› Issue (12): 1519-1524.

趋化因子及其受体家族分子适应性进化分析

陶敏¹, 樊棠怀^2,3, 徐立中², 胡成钰¹

1. 南昌大学生命科学学院, 南昌 330031;
2. 河海大学计算机及信息工程学院, 南京 210098;
3. 南昌工程学院计算机科学与技术系, 南昌 330099

收稿日期:2007-07-25 修回日期:2007-08-16 出版日期:2007-12-10 发布日期:2007-12-10
通讯作者: 胡成钰

Adaptive evolution of chemokines and their receptors genes

TAO Min¹, FAN Tang-Huai^2,3, XU Li-Zhong², HU Cheng-Yu¹

1. College of Life Science, Nanchang University, Nanchang 330031, China;
2. College of Computer and Information Engineering, Hohai University, Nanjing 210098, China;
3. Nanchang Institute of Technology, Nanchang 330099, China

Received:2007-07-25 Revised:2007-08-16 Online:2007-12-10 Published:2007-12-10
Contact: Chengyu Hu

摘要/Abstract

摘要： Branch-Site模型是检测基因序列中单个密码子位点是否具有选择作用的统计学方法。该模型能有效地检测基因在进化历程中是否受到选择作用, 并预测出那些在进化过程中对功能分化有重要贡献的、受正选择作用的密码子位点。趋化因子是一类控制免疫细胞定向迁移的细胞因子, 其功能行使由趋化因子受体介导。该文用Branch-Site模型分析趋化因子及其受体基因家族的分子适应性, 发现只有少数种类基因受到正选择作用, 如RANTES、CCR5等。并预测出一些可能受到正选择作用的位点, 蛋白3D分析显示, 它们均位于趋化因子和相应受体相互作用的结构区域。

关键词: Branch-Site模型, 正选择, 趋化因子受体, 趋化因子

Abstract:

Branch-Site Model is a statistical method for detecting molecular adaptation at individual along specific lineages. Not only the model could indicate whether genes in phylogeny under the positive selection or not, but also could forecast positive selection sites in these genes. The sites promote divergence and polymorphism of genes. Chemokines are chemotactic cytokines that can induce immune cells migration, conducting their functions via chemokine receptors. In the test, the molecular adaptation of chemokines and chemokines receptors genes had been analyzed by Branch-Site model. The results showed that only a few of genes, such as RANTES and CCR5, are in the course of positive selection. Several CCR5 positive selection sites are located in a region that involved in binding to receptor and its chemokine.

陶敏，樊棠怀，徐立中，胡成钰. 趋化因子及其受体家族分子适应性进化分析[J]. 遗传, 2007, 29(12): 1519-1524.

TAO Min, FAN Tang-Huai, XU Li-Zhong, HU Cheng-Yu. Adaptive evolution of chemokines and their receptors genes[J]. HEREDITAS, 2007, 29(12): 1519-1524.

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