Mutational signatures among young-onset testicular cancers.

Nicole E Mealey Dylan E O'Sullivan Cheryl E Peters Daniel Y C HengDarren R Brenner

Published in: BMC medical genomics (2021)

Signature contributions differ by age with signatures 1, 8 and 29 were more common among younger-onset tumors. While these signatures are connected with endogenous deamination of 5-methylcytosine, late replication errors and chewing tobacco, respectively, additional research is needed to further elucidate the etiology of young-onset testicular cancer. Large studies of mutational signatures among young-onset patients are required to understand epidemiologic trends as well as inform targeted prevention and treatment strategies.

Keyphrases

genome wide
end stage renal disease
middle aged
ejection fraction
newly diagnosed
peritoneal dialysis
germ cell
papillary thyroid
emergency department
prognostic factors
gene expression
squamous cell carcinoma
squamous cell
adverse drug
electronic health record