Mycoplasma DnaK expression increases cancer development in vivo upon DNA damage

基因组不稳定性 体内 DNA损伤 DNA修复 癌症 生物 支原体 离体 DNA 癌变 遗传学 癌症研究 分子生物学 细胞生物学
作者
Francesca Benedetti,Giovannino Silvestri,Frank Denaro,Giovanni Finesso,Rafael Contreras-Galindo,Arshi Munawwar,Sumiko Williams,Harry Davis,Joseph Bryant,Yin Wang,Enrico Radaelli,Chozha Vendan Rathinam,Robert C. Gallo,Davide Zella
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:121 (10) 被引量:1
标识
DOI:10.1073/pnas.2320859121
摘要

Well-controlled repair mechanisms are involved in the maintenance of genomic stability, and their failure can precipitate DNA abnormalities and elevate tumor risk. In addition, the tumor microenvironment, enriched with factors inducing oxidative stress and affecting cell cycle checkpoints, intensifies DNA damage when repair pathways falter. Recent research has unveiled associations between certain bacteria, including Mycoplasmas , and various cancers, and the causative mechanism(s) are under active investigation. We previously showed that Mycoplasma fermentans DnaK, an HSP70 family chaperone protein, hampers the activity of proteins like PARP1 and p53, crucial for genomic integrity. Moreover, our analysis of its interactome in human cancer cell lines revealed DnaK’s engagement with several components of DNA-repair machinery. Finally, in vivo experiments performed in our laboratory using a DnaK knock-in mouse model generated by our group demonstrated that DnaK exposure led to increased DNA copy number variants, indicative of genomic instability. We present here evidence that expression of DnaK is linked to increased i) incidence of tumors in vivo upon exposure to urethane, a DNA damaging agent; ii) spontaneous DNA damage ex vivo; and iii) expression of proinflammatory cytokines ex vivo, variations in reactive oxygen species levels, and increased β-galactosidase activity across tissues. Moreover, DnaK was associated with increased centromeric instability. Overall, these findings highlight the significance of Mycoplasma DnaK in the etiology of cancer and other genetic disorders providing a promising target for prevention, diagnostics, and therapeutics.
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