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一种经验与机制相结合的密码子模型。

A combined empirical and mechanistic codon model.

作者信息

Doron-Faigenboim Adi, Pupko Tal

机构信息

Department of Cell Research and Immunology, George S. Wise Faculty of Life Sciences, Tel Aviv University, Tel Aviv, 69978, Israel.

出版信息

Mol Biol Evol. 2007 Feb;24(2):388-97. doi: 10.1093/molbev/msl175. Epub 2006 Nov 16.

Abstract

The evolutionary selection forces acting on a protein are commonly inferred using evolutionary codon models by contrasting the rate of synonymous to nonsynonymous substitutions. Most widely used models are based on theoretical assumptions and ignore the empirical observation that distinct amino acids differ in their replacement rates. In this paper, we develop a general method that allows assimilation of empirical amino acid replacement probabilities into a codon-substitution matrix. In this way, the resulting codon model takes into account not only the transition-transversion bias and the nonsynonymous/synonymous ratio, but also the different amino acid replacement probabilities as specified in empirical amino acid matrices. Different empirical amino acid replacement matrices, such as secondary structure-specific matrices or organelle-specific matrices (e.g., mitochondria and chloroplasts), can be incorporated into the model, making it context dependent. Using a diverse set of coding DNA sequences, we show that the novel model better fits biological data as compared with either mechanistic or empirical codon models. Using the suggested model, we further analyze human immunodeficiency virus type 1 protease sequences obtained from drug-treated patients and reveal positive selection in sites that are known to confer drug resistance to the virus.

摘要

通常通过对比同义替换率和非同义替换率,利用进化密码子模型来推断作用于蛋白质的进化选择力。最常用的模型基于理论假设,忽略了不同氨基酸替换率不同这一实证观察结果。在本文中,我们开发了一种通用方法,可将实证氨基酸替换概率纳入密码子替换矩阵。通过这种方式,所得的密码子模型不仅考虑了转换 - 颠换偏差和非同义/同义比率,还考虑了实证氨基酸矩阵中指定的不同氨基酸替换概率。不同的实证氨基酸替换矩阵,如二级结构特异性矩阵或细胞器特异性矩阵(如线粒体和叶绿体),可纳入该模型,使其具有上下文依赖性。使用一系列不同的编码DNA序列,我们表明,与机械或实证密码子模型相比,新模型能更好地拟合生物学数据。使用所建议的模型,我们进一步分析了从接受药物治疗的患者中获得的人类免疫缺陷病毒1型蛋白酶序列,并揭示了已知赋予病毒耐药性的位点存在正选择。

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