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Gut Pathogens  2011 

Positive selection on a bacterial oncoprotein associated with gastric cancer

DOI: 10.1186/1757-4749-3-18

Keywords: gastric cancer, oncogene, positive selection, Helicobacter pylori, cagA

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Abstract:

Here, we reveal that the cagA gene displays strong signatures of positive selection in bacteria isolated from amerindian populations, using the Ka/Ks ratio. Weaker signatures are also detected in the gene from bacteria isolated from asian populations, using the Ka/Ks ratio and the more sensitive branches-sites model of the PAML package. When the cagA gene isolated from amerindian populations was examined in more detail it was found that the region under positive selection contains the EPIYA domains, which are known to modulate the carcinogenicity of the gene. This means that the carcinogenicity modulating region of the gene is undergoing adaptation. The results are discussed in relation to the high incidences of stomach cancer in some latin american and asian populations.Positive selection on cagA indicates antagonistic coevolution between host and bacteria, which appears paradoxical given that cagA is detrimental to the human host upon which the bacteria depends. This suggests several non-exclusive possibilities; that gastric cancer has not been a major selective pressure on human populations, that cagA has an undetermined benefit to the human host, or that horizontal transmission of H.pylori between hosts has been more important in the evolution of H.pylori than previously recognized, reducing the selective pressure to lower the pathogenicity of the bacteria. The different patterns of adaptation of the gene in different human populations indicates that there are population specific differences in the human gut environment - due either to differences in host genetics or diet and other lifestyle features.Helicobacter pylori is a Gram negative bacterium that lives in the human stomach as part of the normal gastric microbiome [1], and is generally present in the majority of the adult population [2]. The bacterium has co-evolved with human populations [3] and is well adapted and largely specific to the human host. The ancestor of H.pylori was intestinal and during its

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