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强烈的正选择和重组驱动人类病原体脑膜炎奈瑟菌PilE蛋白的抗原变异。

Strong positive selection and recombination drive the antigenic variation of the PilE protein of the human pathogen Neisseria meningitidis.

作者信息

Andrews T Daniel, Gojobori Takashi

机构信息

The Wellcome Trust Sanger Institute, Hinxton, Cambridgeshire, CB10 1SA, United Kingdom.

出版信息

Genetics. 2004 Jan;166(1):25-32. doi: 10.1534/genetics.166.1.25.

Abstract

The PilE protein is the major component of the Neisseria meningitidis pilus, which is encoded by the pilE/pilS locus that includes an expressed gene and eight homologous silent fragments. The silent gene fragments have been shown to recombine through gene conversion with the expressed gene and thereby provide a means by which novel antigenic variants of the PilE protein can be generated. We have analyzed the evolutionary rate of the pilE gene using the nucleotide sequence of two complete pilE/pilS loci. The very high rate of evolution displayed by the PilE protein appears driven by both recombination and positive selection. Within the semivariable region of the pilE and pilS genes, recombination appears to occur within multiple small sequence blocks that lie between conserved sequence elements. Within the hypervariable region, positive selection was identified from comparison of the silent and expressed genes. The unusual gene conversion mechanism that operates at the pilE/pilS locus is a strategy employed by N. meningitidis to enhance mutation of certain regions of the PilE protein. The silent copies of the gene effectively allow "parallelized" evolution of pilE, thus enabling the encoded protein to rapidly explore a large area of sequence space in an effort to find novel antigenic variants.

摘要

菌毛蛋白(PilE)是脑膜炎奈瑟菌菌毛的主要成分,由pilE/pilS基因座编码,该基因座包含一个表达基因和八个同源沉默片段。已表明沉默基因片段可通过基因转换与表达基因重组,从而提供一种产生PilE蛋白新抗原变体的方式。我们利用两个完整的pilE/pilS基因座的核苷酸序列分析了pilE基因的进化速率。PilE蛋白显示出的极高进化速率似乎是由重组和正选择共同驱动的。在pilE和pilS基因的半可变区内,重组似乎发生在保守序列元件之间的多个小序列块内。在高变区内,通过对沉默基因和表达基因的比较确定了正选择。在pilE/pilS基因座起作用的这种不寻常的基因转换机制是脑膜炎奈瑟菌采用的一种策略,以增强PilE蛋白某些区域的突变。该基因的沉默拷贝有效地允许pilE进行“并行化”进化,从而使编码的蛋白能够迅速探索大片序列空间,以努力找到新的抗原变体。

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