Journal
SCIENTIFIC REPORTS
Volume 3, Issue -, Pages -Publisher
NATURE PUBLISHING GROUP
DOI: 10.1038/srep03042
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Funding
- Dr. Tsai-fan Yu Cancer Research Fund
- NIH [R01CA178456]
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Cancer-associated protein tyrosine kinase (PTK) mutations usually are gain of function (GOF) mutations that drive tumor growth and metastasis. We have found 50 JAK1 truncating mutations in 36 of 635 gynecologic tumors in the Total Cancer CareH (TCCH) tumor bank. Among cancer cell lines containing JAK1 truncating mutations in the Cancer Cell Line Encyclopedia databank 68% are gynecologic cancer cells. Within JAK1 the K142 P430 and K860 frame shift mutations were identified as hot spot mutation sites. Sanger sequencing of cancer cell lines primary tumors and matched normal tissues confirmed the JAK1 mutations and showed that these mutations are somatic. JAK1 mediates interferon (IFN)-gamma-regulated tumor immune surveillance. Functional assays show that JAK1 deficient cancer cells are defective inIFN-gamma-induced LMP2 and TAP1 expression loss of which inhibits presentation of tumor antigens. These findings identify recurrent JAK1 truncating mutations that could contribute to tumor immune evasion in gynecologic cancers especially in endometrial cancer.
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