Abstract
BackgroundCisplatin based chemotherapy cures over 80% of metastatic testicular germ cell tumours (TGCT). In contrast, almost all other solid cancers in adults are incurable once they have spread beyond the primary site. Cell lines derived from TGCTs are hypersensitive to cisplatin reflecting the clinical response. Earlier findings suggested that a reduced repair capacity might contribute to the cisplatin hypersensitivity of testis tumour cells (TTC), but the critical DNA damage has not been defined. This study was aimed at investigating the formation and repair of intrastrand and interstrand crosslinks (ICLs) induced by cisplatin in TTC and their contribution to TTC hypersensitivity.ResultsWe observed that repair of intrastrand crosslinks is similar in cisplatin sensitive TTC and resistant bladder cancer cells, whereas repair of ICLs was significantly reduced in TTC. γH2AX formation, which serves as a marker of DNA breaks formed in response to ICLs, persisted in cisplatin-treated TTC and correlated with sustained phosphorylation of Chk2 and enhanced PARP-1 cleavage. Expression of the nucleotide excision repair factor ERCC1-XPF, which is implicated in the processing of ICLs, is reduced in TTC. To analyse the causal role of ERCC1-XPF for ICL repair and cisplatin sensitivity, we over-expressed ERCC1-XPF in TTC by transient transfection. Over-expression increased ICL repair and rendered TTC more resistant to cisplatin, which suggests that ERCC1-XPF is rate-limiting for repair of ICLs resulting in the observed cisplatin hypersensitivity of TTC.ConclusionOur data indicate for the first time that the exceptional sensitivity of TTC and, therefore, very likely the curability of TGCT rests on their limited ICL repair due to low level of expression of ERCC1-XPF.
Highlights
Intrastrand crosslinks are repaired by nucleotide excision repair (NER), whereas interstrand crosslinks (ICLs) are removed by ICL repair, a process less well understood than NER [6]
A survey of repair proteins revealed that the expression level of the ERCC1-XPF endonuclease, which is involved in repair of both intrastrand crosslinks and ICLs, is low in testis tumour cell lines compared to other tumour lines [7] suggesting that ERCC1-XPF might contribute to the observed cisplatin sensitivity
To investigate whether repair of cisplatin-induced intrastrand crosslinks is impaired in testis tumour cells (TTC), experiments were performed to measure their removal from genomic DNA
Summary
Cisplatin based chemotherapy cures over 80% of metastatic testicular germ cell tumours (TGCT). This study was aimed at investigating the formation and repair of intrastrand and interstrand crosslinks (ICLs) induced by cisplatin in TTC and their contribution to TTC hypersensitivity. Over 80% of patients with metastatic testicular germ cell tumours (TGCT) can be cured using cisplatin-based chemotherapy [1]. Interstrand crosslinks (ICLs) between the two DNA strands are minor lesions, accounting for less than 5% of all cisplatin lesions [5]. A survey of repair proteins revealed that the expression level of the ERCC1-XPF endonuclease, which is involved in repair of both intrastrand crosslinks and ICLs, is low in testis tumour cell lines compared to other tumour lines [7] suggesting that ERCC1-XPF might contribute to the observed cisplatin sensitivity
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