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Publication : Increased genomic instability and reshaping of tissue microenvironment underlie oncogenic properties of Arid1a mutations.

First Author  D'Ambrosio A Year  2024
Journal  Sci Adv Volume  10
Issue  11 Pages  eadh4435
PubMed ID  38489371 Mgi Jnum  J:346086
Mgi Id  MGI:7613446 Doi  10.1126/sciadv.adh4435
Citation  D'Ambrosio A, et al. (2024) Increased genomic instability and reshaping of tissue microenvironment underlie oncogenic properties of Arid1a mutations. Sci Adv 10(11):eadh4435
abstractText  Oncogenic mutations accumulating in many chromatin-associated proteins have been identified in different tumor types. With a mutation rate from 10 to 57%, ARID1A has been widely considered a tumor suppressor gene. However, whether this role is mainly due to its transcriptional-related activities or its ability to preserve genome integrity is still a matter of intense debate. Here, we show that ARID1A is largely dispensable for preserving enhancer-dependent transcriptional regulation, being ARID1B sufficient and required to compensate for ARID1A loss. We provide in vivo evidence that ARID1A is mainly required to preserve genomic integrity in adult tissues. ARID1A loss primarily results in DNA damage accumulation, interferon type I response activation, and chronic inflammation leading to tumor formation. Our data suggest that in healthy tissues, the increased genomic instability that follows ARID1A mutations and the selective pressure imposed by the microenvironment might result in the emergence of aggressive, possibly immune-resistant, tumors.
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