A novel germline EGFR variant p.R831H causes predisposition to familial CDK12-mutant prostate cancer with tandem duplicator phenotype.
Kaiyu QianGang WangLin-Gao JuJiyan LiuYongwen LuoYejinpeng WangTianchen PengFangjin ChenYi ZhangYu XiaoXing-Huan WangPublished in: Oncogene (2020)
5-10% of total prostate cancer (PCa) cases are hereditary. Particularly, immune checkpoint inhibitor-sensitive tandem duplicator phenotype (TDP) accounts for 6.9% of PCa cases, whereas genetic susceptibility genes remain completely unknown. We identified a Chinese family with two PCa patients, in which the PCa phenotype co-segregated with a rare germline variant EGFRR831H. Patient-derived conditionally reprogrammed cells (CRC) exhibited increased EGFR and AKT phosphorylation, and a sensitivity to EGFR antagonist Afatinib in migration assays, suggesting the EGFR allele was constitutively active. Both EGFRR831H-mutant tumours contained biallelic CDK12 inactivation, together with prominent tandem duplication across the genome. These somatic mutations could be detected in urine before surgery. Analysis of public databases showed a significant correlation between the mutation status of EGFR and CDK12. Taken together, our genetic and functional analyses identified a previously undescribed link between EGFR and PCa.
Keyphrases
- epidermal growth factor receptor
- small cell lung cancer
- prostate cancer
- tyrosine kinase
- genome wide
- advanced non small cell lung cancer
- healthcare
- end stage renal disease
- radical prostatectomy
- induced apoptosis
- newly diagnosed
- dna repair
- ejection fraction
- high throughput
- minimally invasive
- gene expression
- dna methylation
- autism spectrum disorder
- deep learning
- early onset
- prognostic factors
- big data
- coronary artery bypass
- endoplasmic reticulum stress
- coronary artery disease
- percutaneous coronary intervention