| Literature DB >> 33989515 |
Satoshi Imai1, Takuya Ooki1, Naoko Murata-Kamiya2, Daisuke Komura3, Kamrunnesa Tahmina1, Weida Wu1, Atsushi Takahashi-Kanemitsu1, Christopher Takaya Knight1, Akiko Kunita4, Nobumi Suzuki5, Adriana A Del Valle1, Mayo Tsuboi5, Masahiro Hata5, Yoku Hayakawa5, Naomi Ohnishi6, Koji Ueda6, Masashi Fukayama4, Tetsuo Ushiku4, Shumpei Ishikawa3, Masanori Hatakeyama7.
Abstract
Infection with CagA-producing Helicobacter pylori plays a causative role in the development of gastric cancer. Upon delivery into gastric epithelial cells, CagA deregulates prooncogenic phosphatase SHP2 while inhibiting polarity-regulating kinase PAR1b through complex formation. Here, we show that CagA/PAR1b interaction subverts nuclear translocation of BRCA1 by inhibiting PAR1b-mediated BRCA1 phosphorylation. It hereby induces BRCAness that promotes DNA double-strand breaks (DSBs) while disabling error-free homologous recombination-mediated DNA repair. The CagA/PAR1b interaction also stimulates Hippo signaling that circumvents apoptosis of DNA-damaged cells, giving cells time to repair DSBs through error-prone mechanisms. The DSB-activated p53-p21Cip1 axis inhibits proliferation of CagA-delivered cells, but the inhibition can be overcome by p53 inactivation. Indeed, sequential pulses of CagA in TP53-mutant cells drove somatic mutation with BRCAness-associated genetic signatures. Expansion of CagA-delivered cells with BRCAness-mediated genome instability, from which CagA-independent cancer-predisposing cells arise, provides a plausible "hit-and-run mechanism" of H. pylori CagA for gastric carcinogenesis.Entities:
Keywords: BRCA1; BRCAness; CagA; DNA double-strand break; Helicobacter pylori; PAR1b; gastric cancer; genome instability; homologous recombination; replication fork instability
Year: 2021 PMID: 33989515 DOI: 10.1016/j.chom.2021.04.006
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023