ARID1A (the AT-rich interaction domain 1A, also known as BAF250a) is one of the most commonly mutated genes in cancer(1,2). The majority of ARID1A mutations are inactivating mutations and lead to loss of ARID1A expression(3), which makes ARID1A a poor therapeutic target. Therefore, it is of clinical importance to identify molecular consequences of ARID1A deficiency that create therapeutic vulnerabilities in ARID1A-mutant tumors. In a proteomic screen, we found that ARID1A interacts with mismatch repair (MMR) protein MSH2. ARID1A recruited MSH2 to chromatin during DNA replication and promoted MMR. Conversely, ARID1A inactivation compromised MMR and increased mutagenesis. ARID1A deficiency correlated with microsatellite instability genomic signature and a predominant C>T mutation pattern and increased mutation load across multiple human cancer types. Tumors formed by an ARID1A-deficient ovarian cancer cell line in syngeneic mice displayed increased mutation load, elevated numbers of tumor-infiltrating lymphocytes, and PD-L1 expression. Notably, treatment with anti-PD-L1 antibody reduced tumor burden and prolonged survival of mice bearing ARID1A-deficient but not ARID1A-wild-type ovarian tumors. Together, these results suggest ARID1A deficiency contributes to impaired MMR and mutator phenotype in cancer, and may cooperate with immune checkpoint blockade therapy.
基金:
NCI Cancer Center Support Grant [CA016672]; Department of Defense grant [OC140431]; NIH R01 grant [CA181663, GM093104]; Cancer Prevention and Research Institute of Texas grant [RP160242]; NIH P01 grant [CA092584]
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出版当年[2017]版:
大类|1 区医学
小类|1 区生化与分子生物学1 区细胞生物学1 区医学:研究与实验
最新[2025]版:
大类|1 区医学
小类|1 区生化与分子生物学1 区细胞生物学1 区医学:研究与实验
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出版当年[2016]版:
Q1CELL BIOLOGYQ1MEDICINE, RESEARCH & EXPERIMENTALQ1BIOCHEMISTRY & MOLECULAR BIOLOGY
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Q1BIOCHEMISTRY & MOLECULAR BIOLOGYQ1CELL BIOLOGYQ1MEDICINE, RESEARCH & EXPERIMENTAL
医学