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PPP2R1A mutations cause ATR inhibitor sensitivity in ovarian clear cell carcinoma
in
Cancer research
/ Chemotherapy
/ CRISPR
/ Genes
/ Genomes
/ Genomic instability
/ Genomics
/ Kinases
/ Lethality
/ Medical research
/ Mutagenesis
/ Mutants
/ Mutation
/ Ovarian cancer
/ Ovarian carcinoma
/ Phosphatase
/ Phosphoprotein phosphatase
/ Protein phosphatase
/ Proteins
/ S phase
2025
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PPP2R1A mutations cause ATR inhibitor sensitivity in ovarian clear cell carcinoma
by
in
Cancer research
/ Chemotherapy
/ CRISPR
/ Genes
/ Genomes
/ Genomic instability
/ Genomics
/ Kinases
/ Lethality
/ Medical research
/ Mutagenesis
/ Mutants
/ Mutation
/ Ovarian cancer
/ Ovarian carcinoma
/ Phosphatase
/ Phosphoprotein phosphatase
/ Protein phosphatase
/ Proteins
/ S phase
2025
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
PPP2R1A mutations cause ATR inhibitor sensitivity in ovarian clear cell carcinoma
in
Cancer research
/ Chemotherapy
/ CRISPR
/ Genes
/ Genomes
/ Genomic instability
/ Genomics
/ Kinases
/ Lethality
/ Medical research
/ Mutagenesis
/ Mutants
/ Mutation
/ Ovarian cancer
/ Ovarian carcinoma
/ Phosphatase
/ Phosphoprotein phosphatase
/ Protein phosphatase
/ Proteins
/ S phase
2025
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PPP2R1A mutations cause ATR inhibitor sensitivity in ovarian clear cell carcinoma
Journal Article
PPP2R1A mutations cause ATR inhibitor sensitivity in ovarian clear cell carcinoma
2025
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Overview
Identification of ARID1A/ATR synthetic lethality led to ATR inhibitor phase II trials in ovarian clear cell carcinoma (OCCC), a cancer of unmet need. Using multiple CRISPR-Cas9 mutagenesis and interference screens, we show that inactivation of protein phosphatase 2A (PP2A) subunits, including PPP2R1A, enhance ATRi sensitivity in ARID1A mutant OCCC. Analysis of a new OCCC cohort indicates that 52% possess oncogenic PPP2R1A p.R183 mutations and of these, one half possessed both ARID1A as well as PPP2R1A mutations. Using CRISPR-prime editing to generate new isogenic models of PPP2R1A mutant OCCC, we found that PPP2R1A p.R183W and p.R183P mutations cause ATRi-induced S phase stress, premature mitotic entry, genomic instability and ATRi sensitivity in OCCC tumour cells. p.R183 mutation also enhanced both in vitro and in vivo ATRi sensitivity in preclinical models of ARID1A mutant OCCC. These results argue for the assessment of PPP2R1A mutations as a biomarker of ATRi sensitivity.
Publisher
Nature Publishing Group
Subject
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