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幽门螺杆菌进化过程中多个基因的获得与丢失。

Gain and loss of multiple genes during the evolution of Helicobacter pylori.

作者信息

Gressmann Helga, Linz Bodo, Ghai Rohit, Pleissner Klaus-Peter, Schlapbach Ralph, Yamaoka Yoshio, Kraft Christian, Suerbaum Sebastian, Meyer Thomas F, Achtman Mark

机构信息

Department of Molecular Biology, Max-Planck-Institut für Infektionsbiologie, Berlin, Germany.

出版信息

PLoS Genet. 2005 Oct;1(4):e43. doi: 10.1371/journal.pgen.0010043.

Abstract

Sequence diversity and gene content distinguish most isolates of Helicobacter pylori. Even greater sequence differences differentiate distinct populations of H. pylori from different continents, but it was not clear whether these populations also differ in gene content. To address this question, we tested 56 globally representative strains of H. pylori and four strains of Helicobacter acinonychis with whole genome microarrays. Of the weighted average of 1,531 genes present in the two sequenced genomes, 25% are absent in at least one strain of H. pylori and 21% were absent or variable in H. acinonychis. We extrapolate that the core genome present in all isolates of H. pylori contains 1,111 genes. Variable genes tend to be small and possess unusual GC content; many of them have probably been imported by horizontal gene transfer. Phylogenetic trees based on the microarray data differ from those based on sequences of seven genes from the core genome. These discrepancies are due to homoplasies resulting from independent gene loss by deletion or recombination in multiple strains, which distort phylogenetic patterns. The patterns of these discrepancies versus population structure allow a reconstruction of the timing of the acquisition of variable genes within this species. Variable genes that are located within the cag pathogenicity island were apparently first acquired en bloc after speciation. In contrast, most other variable genes are of unknown function or encode restriction/modification enzymes, transposases, or outer membrane proteins. These seem to have been acquired prior to speciation of H. pylori and were subsequently lost by convergent evolution within individual strains. Thus, the use of microarrays can reveal patterns of gene gain or loss when examined within a phylogenetic context that is based on sequences of core genes.

摘要

序列多样性和基因含量可区分大多数幽门螺杆菌分离株。不同大陆的幽门螺杆菌不同种群之间存在更大的序列差异,但尚不清楚这些种群在基因含量上是否也存在差异。为解决这个问题,我们使用全基因组微阵列检测了56株具有全球代表性的幽门螺杆菌菌株和4株犬幽门螺杆菌菌株。在两个已测序基因组中存在的1531个基因的加权平均值中,至少有25%在至少一株幽门螺杆菌中缺失,21%在犬幽门螺杆菌中缺失或可变。我们推断所有幽门螺杆菌分离株中存在的核心基因组包含1111个基因。可变基因往往较小且具有不寻常的GC含量;其中许多可能是通过水平基因转移导入的。基于微阵列数据的系统发育树与基于核心基因组七个基因序列的系统发育树不同。这些差异是由于多个菌株中通过缺失或重组导致的独立基因丢失所产生的平行进化,这扭曲了系统发育模式。这些差异模式与种群结构允许重建该物种内可变基因获得的时间。位于cag致病岛中的可变基因显然是在物种形成后首先作为一个整体获得的。相比之下,大多数其他可变基因功能未知或编码限制/修饰酶、转座酶或外膜蛋白。这些似乎是在幽门螺杆菌物种形成之前获得的,随后在各个菌株中通过趋同进化而丢失。因此,在基于核心基因序列的系统发育背景下进行检测时,使用微阵列可以揭示基因获得或丢失的模式。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6902/1270003/d1b582ef1db1/pgen.0010043.g001.jpg

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