Biology-driven therapy advances in high-grade serous ovarian cancer
Yinu Wang, … , Mazhar Adli, Daniela Matei
Yinu Wang, … , Mazhar Adli, Daniela Matei
Published January 2, 2024
Citation Information: J Clin Invest. 2024;134(1):e174013. https://doi.org/10.1172/JCI174013.
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Review

Biology-driven therapy advances in high-grade serous ovarian cancer

Abstract

Following a period of slow progress, the completion of genome sequencing and the paradigm shift relative to the cell of origin for high grade serous ovarian cancer (HGSOC) led to a new perspective on the biology and therapeutic solutions for this deadly cancer. Experimental models were revisited to address old questions, and improved tools were generated. Additional pathways emerging as drivers of ovarian tumorigenesis and key dependencies for therapeutic targeting, in particular, VEGF-driven angiogenesis and homologous recombination deficiency, were discovered. Molecular profiling of histological subtypes of ovarian cancer defined distinct genetic events for each entity, enabling the first attempts toward personalized treatment. Armed with this knowledge, HGSOC treatment was revised to include new agents. Among them, PARP inhibitors (PARPis) were shown to induce unprecedented improvement in clinical benefit for selected subsets of patients. Research on mechanisms of resistance to PARPis is beginning to discover vulnerabilities and point to new treatment possibilities. This Review highlights these advances, the remaining challenges, and unsolved problems in the field.

Authors

Yinu Wang, Alexander James Duval, Mazhar Adli, Daniela Matei

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Figure 2

Key mechanisms implicated in emergence of platinum resistance.

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Key mechanisms implicated in emergence of platinum resistance. OC cells ...
OC cells develop chemoresistance due to diverse mechanisms, including paracrine release of cytokines from stromal elements in the TME, upregulation of cell membrane ABC transporters to enhance drug efflux, increased cellular antioxidant defense to reduce ROS, promotion of antiapoptotic signaling through increased expression of antiapoptotic proteins and decreased expression of death ligand receptors, metabolic reprogramming, an increase in chromatin packing, genetic and epigenetic inactivation of tumor suppressor and DNA repair genes, modulation of superenhancers that induce transcriptional reprogramming, and acquisition of mutations, including reverting BRCA 1 and 2 mutations. ABCB1, also known as P-glycoprotein (PgP) and multidrug resistance protein 1 (MDR1); ABCC1, multidrug resistance-associated protein 1 (also known as MRP1); ABCG2, breast cancer resistance protein (also known as BCRP); TRAILR1, TNF-related apoptosis-inducing ligand receptor 1; TRAILR2, TNF-related apoptosis-inducing ligand receptor 2; FAS, Fas cell surface death receptor; MADD, MAPK-activating death domain; c-FLIP, cellular FLICE-like inhibitory protein; GPX4, glutathione peroxidase 4; NRF2, nuclear factor erythroid-2 related factor; ALDH1, aldehyde dehydrogenase 1; BRCA1, breast cancer gene 1; EMT, epithelial-mesenchymal transition; RB1, retinoblastoma 1; NF1, neurofibromatosis 1; RAD51B, RAD51 paralog B.