Impact of the Helicobacter pylori Oncoprotein CagA in Gastric Carcinogenesis.

Masanori Hatakeyama
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Abstract

Helicobacter pylori CagA is the first and only bacterial oncoprotein etiologically associated with human cancer. Upon delivery into gastric epithelial cells via bacterial type IV secretion, CagA acts as a pathogenic/pro-oncogenic scaffold that interacts with and functionally perturbs multiple host proteins such as pro-oncogenic SHP2 phosphatase and polarity-regulating kinase PAR1b/MARK2. Although H. pylori infection is established during early childhood, gastric cancer generally develops in elderly individuals, indicating that oncogenic CagA activity is effectively counteracted at a younger age. Moreover, the eradication of cagA-positive H. pylori cannot cure established gastric cancer, indicating that H. pylori CagA-triggered gastric carcinogenesis proceeds via a hit-and-run mechanism. In addition to its direct oncogenic action, CagA induces BRCAness, a cellular status characterized by replication fork destabilization and loss of error-free homologous recombination-mediated DNA double-strand breaks (DSBs) by inhibiting cytoplasmic-to-nuclear localization of the BRCA1 tumor suppressor. This causes genomic instability that leads to the accumulation of excess mutations in the host cell genome, which may underlie hit-and-run gastric carcinogenesis. The close connection between CagA and BRCAness was corroborated by a recent large-scale case-control study that revealed that the risk of gastric cancer in individuals carrying pathogenic variants of genes that induce BRCAness (such as BRCA1 and BRCA2) dramatically increases upon infection with cagA-positive H. pylori. Accordingly, CagA-mediated BRCAness plays a crucial role in the development of gastric cancer in conjunction with the direct oncogenic action of CagA.

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幽门螺杆菌肿瘤蛋白 CagA 对胃癌发病的影响
幽门螺杆菌 CagA 是第一个也是唯一一个与人类癌症病因相关的细菌肿瘤蛋白。通过细菌 IV 型分泌物进入胃上皮细胞后,CagA 成为致病/致癌支架,与多种宿主蛋白(如促致癌的 SHP2 磷酸酶和极性调节激酶 PAR1b/MARK2)相互作用并在功能上扰乱它们。虽然幽门螺杆菌在儿童早期就已感染,但胃癌一般发生在老年人身上,这表明致癌的 CagA 活性在较年轻时就能被有效抵消。此外,根除 cagA 阳性幽门螺杆菌并不能治愈已确诊的胃癌,这表明幽门螺杆菌 CagA 引发的胃癌是通过 "打了就跑 "的机制发生的。除了直接致癌作用外,CagA 还通过抑制 BRCA1 肿瘤抑制因子从胞质到核的定位,诱导 BRCAness(一种以复制叉不稳定和无差错同源重组介导的 DNA 双链断裂(DSB)丧失为特征的细胞状态)。这就造成了基因组的不稳定性,导致宿主细胞基因组中过量突变的积累,这可能是 "打了就跑 "的胃癌发生的根本原因。最近的一项大规模病例对照研究证实了 CagA 与 BRCAness 之间的密切联系,该研究显示,携带诱导 BRCAness 基因(如 BRCA1 和 BRCA2)致病变体的个体在感染 cagA 阳性幽门螺杆菌后患胃癌的风险急剧增加。因此,CagA 介导的 BRCAness 与 CagA 的直接致癌作用一起,在胃癌的发展中起着至关重要的作用。
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来源期刊
CiteScore
5.60
自引率
0.00%
发文量
26
审稿时长
>12 weeks
期刊介绍: The review series Current Topics in Microbiology and Immunology provides a synthesis of the latest research findings in the areas of molecular immunology, bacteriology and virology. Each timely volume contains a wealth of information on the featured subject. This review series is designed to provide access to up-to-date, often previously unpublished information.
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