We analyzed genomic data from the prostate cancer of African- and European American
men to identify differences contributing to racial disparity of outcome. We also performed
FISH-based studies of Chromodomain helicase DNA-binding protein 1 (CHD1) loss on prostate
cancer tissue microarrays. We created CHD1-deficient prostate cancer cell lines for
genomic, drug sensitivity and functional homologous recombination (HR) activity analysis.
Subclonal deletion of CHD1 was nearly three times as frequent in prostate tumors of
African American than in European American men and it associates with rapid disease
progression. CHD1 deletion was not associated with HR deficiency associated mutational
signatures or HR deficiency as detected by RAD51 foci formation. This was consistent
with the moderate increase of olaparib and talazoparib sensitivity with several CHD1
deficient cell lines showing talazoparib sensitivity in the clinically relevant concentration
range. CHD1 loss may contribute to worse disease outcome in African American men.
