Department of Endoscopy, Cho Ray Hospital, Ho Chi Minh, Vietnam.
Department of Environmental and Preventive Medicine, Oita University Faculty of Medicine, Oita, Japan.
Microb Genom. 2021 Nov;7(11). doi: 10.1099/mgen.0.000680.
Genome-wide association studies (GWASs) can reveal genetic variations associated with a phenotype in the absence of any hypothesis of candidate genes. The problem of false-positive sites linked with the responsible site might be bypassed in bacteria with a high homologous recombination rate, such as , which causes gastric cancer. We conducted a small-sample GWAS (125 gastric cancer cases and 115 controls) followed by prediction of gastric cancer and control (duodenal ulcer) strains. We identified 11 single nucleotide polymorphisms (eight amino acid changes) and three DNA motifs that, combined, allowed effective disease discrimination. They were often informative of the underlying molecular mechanisms, such as electric charge alteration at the ligand-binding pocket, alteration in subunit interaction, and mode-switching of DNA methylation. We also identified three novel virulence factors/oncoprotein candidates. These results provide both defined targets for further informatic and experimental analyses to gain insights into gastric cancer pathogenesis and a basis for identifying a set of biomarkers for distinguishing these -related diseases.
全基因组关联研究(GWAS)可以在没有候选基因假设的情况下揭示与表型相关的遗传变异。在同源重组率高的细菌中,如导致胃癌的细菌,与负责的位点相关的假阳性位点的问题可能会被绕过。我们进行了一项小样本 GWAS(125 例胃癌病例和 115 例对照),随后预测了胃癌和对照(十二指肠溃疡)菌株。我们鉴定了 11 个单核苷酸多态性(8 个氨基酸变化)和 3 个 DNA 基序,它们结合在一起可以有效地进行疾病区分。它们通常可以提供有关潜在分子机制的信息,例如配体结合口袋的电荷改变、亚基相互作用的改变以及 DNA 甲基化模式的转换。我们还鉴定了三个新的毒力因子/癌蛋白候选物。这些结果不仅为进一步的信息学和实验分析提供了明确的目标,以深入了解胃癌的发病机制,还为鉴定一组区分这些相关疾病的生物标志物提供了基础。
