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TYMS promotes genomic instability and tumor progression in Ink4a/Arf null background

María V. Guijarro, Akbar Nawab, Peter Dib, Sandra Burkett, Xiaoping Luo, Michael Feely, Elham Nasri, Robert P. Seifert, Frederic J. Kaye, Maria Zajac‐Kaye

2023Oncogene26 citationsDOIOpen Access PDF

Abstract

Abstract We previously showed that elevated TYMS exhibits oncogenic properties and promotes tumorigenesis after a long latency, suggesting cooperation with sequential somatic mutations. Here we report the cooperation of ectopic expression of human TYMS with loss of Ink4a/Arf , one of the most commonly mutated somatic events in human cancer. Using an hTS/Ink4a/Arf −/− genetically engineered mouse model we showed that deregulated TYMS expression in Ink4a/Arf null background accelerates tumorigenesis and metastasis. In addition, tumors from TYMS-expressing mice were associated with a phenotype of genomic instability including enhanced double strand DNA damage, aneuploidy and loss of G1/S checkpoint. Downregulation of TYMS in vitro decreased cell proliferation and sensitized tumor cells to antimetabolite chemotherapy. In addition, depletion of TYMS in vivo by TYMS shRNA reduced tumor incidence, delayed tumor progression and prolonged survival in hTS/Ink4a/Arf −/− mice. Our data shows that activation of TYMS in Ink4a/Arf null background enhances uncontrolled cell proliferation and tumor growth, supporting the development of new agents and strategies targeting TYMS to delay tumorigenesis and prolong survival.

Topics & Concepts

BiologyGenome instabilityTumor progressionCarcinogenesisCancer researchGeneticsInstabilityInternal medicineCancerDNADNA damageMedicinePhysicsMechanicsOcular Oncology and TreatmentsCancer Genomics and DiagnosticsAdvanced biosensing and bioanalysis techniques
TYMS promotes genomic instability and tumor progression in Ink4a/Arf null background | Litcius