The Role of Tumor Biomarkers in Tailoring the Approach to Advanced Ovarian Cancer
- Authors: Tonti, Noemi; Golia D'Augè, Tullio; Cuccu, Ilaria; De Angelis, Emanuele; D'Oria, Ottavia; Perniola, Giorgia; Laganà , Antonio Simone; Etrusco, Andrea; Ferrari, Federico; Saponara, Stefania; Di Donato, Violante; Bogani, Giorgio; Giannini, Andrea
- Publication year: 2024
- Type: Review essay (rassegna critica)
- OA Link: http://hdl.handle.net/10447/665142
Abstract
Growing evidence has demonstrated the role of mutations of tumor biomarkers in diagnosing and treating epithelial ovarian cancer. This review aims to analyze recent literature on the correlation between tumor biomarkers and chemotherapy in nonmucinous ovarian cancer, providing suggestions for personalized treatment approaches. An extensive literature search was conducted to identify relevant studies and trials. BRCA1/2 mutations are central in homologous recombination repair deficiency (HRD) in ovarian cancer, but several other genetic mutations also contribute to varying cancer risks. While the role of MMR testing in ovarian cancer is debated, it is more commonly linked to non-serous ovarian cancer, often associated with Lynch syndrome. A significant proportion of ovarian cancer patients have HRD, affecting treatment decisions in both first-line (especially in advanced stages) and second-line therapy due to HRD’s connection with platinum-based therapy and PARP inhibitors’ response. However, validated genetic tests to identify HRD have not yet been universally implemented. There is no definitive therapeutic algorithm for advanced ovarian cancer, despite ongoing efforts and multiple proposed tools. Future research should focus on expanding the utility of biomarkers, reducing resistance, and increasing the actionable biomarker pool.