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Molecular Pathways and Targeted Therapies for Malignant Ovarian Germ Cell Tumors and Sex Cord–Stromal Tumors: A Contemporary Review

机译:恶性卵巢生殖细胞肿瘤和性索-间质性肿瘤的分子途径和靶向治疗:当代回顾

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摘要

Non-epithelial ovarian tumors are heterogeneous and account for approximately 10% of ovarian malignancies. The most common subtypes of non-epithelial ovarian tumors arise from germ cells or sex cord and stromal cells of the gonads. These tumors are usually detected at an early stage, and management includes surgical staging and debulking. When indicated for advanced disease, most respond to chemotherapy; however, options for patients with refractory disease are limited, and regimens can be associated with significant toxicities, including permanent organ dysfunction, secondary malignancies, and death. Targeted therapies that potentially decrease chemotherapy-related adverse effects and improve outcomes for patients with chemotherapy-refractory disease are needed. Here, we review the molecular landscape of non-epithelial ovarian tumors for the purpose of informing rational clinical trial design. Recent genomic discoveries have uncovered recurring somatic alterations and germline mutations in subtypes of non-epithelial ovarian tumors. Though there is a paucity of efficacy data on targeted therapies, such as kinase inhibitors, antibody–drug conjugates, immunotherapy, and hormonal therapy, exceptional responses to some compounds have been reported. The rarity and complexity of non-epithelial ovarian tumors warrant collaboration and efficient clinical trial design, including high-quality molecular characterization, to guide future efforts.
机译:非上皮性卵巢肿瘤是异质性的,约占卵巢恶性肿瘤的10%。非上皮性卵巢肿瘤的最常见亚型来自性腺的生殖细胞或性索和基质细胞。这些肿瘤通常在早期发现,治疗包括手术分期和减瘤。当指示为晚期疾病时,大多数对化疗有反应;然而,对于难治性疾病患者的选择是有限的,并且治疗方案可能与明显的毒性相关,包括永久性器官功能障碍,继发性恶性肿瘤和死亡。需要有针对性的疗法,以减少与化疗有关的不良反应并改善化疗难治性疾病患者的预后。在这里,我们审查非上皮性卵巢肿瘤的分子格局,以告知合理的临床试验设计。最近的基因组发现已发现非上皮性卵巢肿瘤亚型中反复出现的体细胞变化和种系突变。尽管针对靶向疗法(如激酶抑制剂,抗体-药物偶联物,免疫疗法和激素疗法)的功效数据很少,但已报道了对某些化合物的异常反应。非上皮性卵巢肿瘤的稀有性和复杂性值得合作和有效的临床试验设计(包括高质量的分子表征)来指导未来的工作。

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