Current data and future perspectives on DNA methylation in ovarian cancer (Review)

Fu, Mengyu; Deng, Fengying; Chen, Jie; Fu, Li; Lei, Jiahui; Xu, Ting; Chen, Youguo; Zhou, Jinhua; Gao, Qinqin; Ding, Hongmei

doi:10.3892/ijo.2024.5650

Int J Oncol

2024

DOI: 10.3892/ijo.2024.5650

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Current data and future perspectives on DNA methylation in ovarian cancer (Review)

Mengyu Fu,

Fengying Deng,

Jie Chen

et al.

Abstract: Ovarian cancer (OC) represents the most prevalent malignancy of the female reproductive system. Its distinguishing features include a high aggressiveness, substantial morbidity and mortality, and a lack of apparent symptoms, which collectively pose significant challenges for early detection. Given that aberrant DNA methylation events leading to altered gene expression are characteristic of numerous tumor types, there has been extensive research into epigenetic mechanisms, particularly DNA methylation, in human… Show more

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References 185 publications

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Clinical validation of a DNA methylation biomarker to predict overall survival of relapsed ovarian cancer patients

Habiburrahman,

Masrour,

Patel

et al. 2024

Preprint

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Background: About 70% of ovarian cancer (OC) patients relapse after initial chemotherapy, making it crucial to predict survival before second-line treatment. Our previous work discovered a blood-based DNA methylation prognostic signature (PLAT-M8) that uses 8 CpG sites related to chemoresistance. We aim to validate this biomarker and its correlation with clinicopathological features and treatment profiles in additional cohorts. Methods: Extracted DNA from whole blood was provided from the BriTROC-1 (n=47) and OV04 cohorts (n=57) upon the first relapse. Additional samples from Hammersmith Hospital (n=100) were collected during first-line chemotherapy (cycles 3-4 and 6). Bisulphite pyrosequencing was used to quantify DNA methylation at the previously identified 8 CpG sites. The methylation data obtained were combined with previous data from ScoTROC-1D and 1V (n=141) and OCTIPS (n=46). Cox regression was used to assess overall survival (OS) after relapse concerning clinicopathological characteristics. The DNA methylation Class (Class 1 vs 2) was determined by consensus clustering. Findings: Blood DNA methylation at relapse predicts better clinical outcomes. Methylation Class shows no association with outcome during first-line chemotherapy treatment. Methylation Class 1 is associated with shorter survival, as indicated by a meta-analysis of five cohorts (OS: HR 2.54, 1.67-3.85). Class 2 patients on carboplatin monotherapy have the best prognosis, while Class 1 patients on the same treatment have the poorest prognosis (OS: aHR 9.69, 2.38-39.47). Class 1 is linked to older patients (>75 years) with advanced-stage, platinum-resistant cases, correlating with residual disease, and shorter progression-free survival. In contrast, Class 2 of PLAT-M8 is linked to platinum-sensitive patients, and higher complete response rates by RECIST criteria, but shows no correlation with CA-125. These findings emphasise the potential of PLAT-M8 in guiding second-line chemotherapy decisions. Interpretation: PLAT-M8 methylation biomarker is associated with survival in OC patients with relapse and hypothetically may predict platinum treatment response at second-line chemotherapy.

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Clinical validation of a DNA methylation biomarker to predict overall survival of relapsed ovarian cancer patients

Habiburrahman,

Masrour,

Patel

et al. 2024

Preprint

View full text Add to dashboard Cite

show abstract

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Current data and future perspectives on DNA methylation in ovarian cancer (Review)

Cited by 1 publication

References 185 publications

Clinical validation of a DNA methylation biomarker to predict overall survival of relapsed ovarian cancer patients

Clinical validation of a DNA methylation biomarker to predict overall survival of relapsed ovarian cancer patients

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