- Gull, Nicole;
- Jones, Michelle R;
- Peng, Pei-Chen;
- Coetzee, Simon G;
- Silva, Tiago C;
- Plummer, Jasmine T;
- Reyes, Alberto Luiz P;
- Davis, Brian D;
- Chen, Stephanie S;
- Lawrenson, Kate;
- Lester, Jenny;
- Walsh, Christine;
- Rimel, Bobbie J;
- Li, Andrew J;
- Cass, Ilana;
- Berg, Yonatan;
- Govindavari, John-Paul B;
- Rutgers, Joanna KL;
- Berman, Benjamin P;
- Karlan, Beth Y;
- Gayther, Simon A
Background
Little is known about the role of global DNA methylation in recurrence and chemoresistance of high grade serous ovarian cancer (HGSOC).Methods
We performed whole genome bisulfite sequencing and transcriptome sequencing in 62 primary and recurrent tumors from 28 patients with stage III/IV HGSOC, of which 11 patients carried germline, pathogenic BRCA1 and/or BRCA2 mutations.Results
Landscapes of genome-wide methylation (on average 24.2 million CpGs per tumor) and transcriptomes in primary and recurrent tumors showed extensive heterogeneity between patients but were highly preserved in tumors from the same patient. We identified significant differences in the burden of differentially methylated regions (DMRs) in tumors from BRCA1/2 compared to non-BRCA1/2 carriers (mean 659 DMRs and 388 DMRs in paired comparisons respectively). We identified overexpression of immune pathways in BRCA1/2 carriers compared to non-carriers, implicating an increased immune response in improved survival (P = 0.006) in these BRCA1/2 carriers.Conclusion
These findings indicate methylome and gene expression programs established in the primary tumor are conserved throughout disease progression, even after extensive chemotherapy treatment, and that changes in methylation and gene expression are unlikely to serve as drivers for chemoresistance in HGSOC.