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卵巢癌的组织学、分子和细胞遗传学特征:对诊断和治疗的影响。

Histologic, molecular, and cytogenetic features of ovarian cancers: implications for diagnosis and treatment.

机构信息

Department of Radiology, University of Texas Health Science Center, 7703 Floyd Curl Dr, San Antonio, TX 78229, USA.

出版信息

Radiographics. 2011 May-Jun;31(3):625-46. doi: 10.1148/rg.313105066.

DOI:10.1148/rg.313105066
PMID:21571648
Abstract

Ovarian epithelial carcinoma (OEC), the most common ovarian malignancy, is a heterogeneous disease with several histologic subtypes that show characteristic cytogenetic features, molecular signatures, oncologic signaling pathways, and clinical-biologic behavior. Recent advances in histopathology and cytogenetics have provided insights into pathophysiologic features and natural history of OECs. Several studies have shown that high- or low-grade serous, endometrioid, and clear cell carcinomas are characterized by mutations involving the TP53, K-ras/BRAF, CTNNB1, and PIK3CA genes, respectively. High-grade serous carcinomas, the most common subtype, often manifest with early transcoelomic spread of disease beyond the ovaries, whereas low-grade serous and mucinous carcinomas commonly manifest with early-stage disease, with a resultant excellent prognosis. On the basis of pathogenetic mechanisms, recent findings suggest a dualistic model of ovarian carcinogenesis consisting of types I and II. Type I (low-grade serous, mucinous, and endometrioid) cancers commonly arise from well-described, genetically stable precursor lesions (usually borderline tumors); manifest as large adnexal masses with early-stage disease; and have a relatively indolent clinical course, with an overall good prognosis. In contrast, type II carcinomas (high-grade serous, endometrioid, mixed, and undifferentiated variants) originate de novo from the adnexal epithelia, often demonstrate chromosomal instability, and have aggressive biologic behavior. Better knowledge of hereditary ovarian cancer syndromes and associated cytogenetic abnormalities has led to increased interest in novel biomarkers and molecular therapeutics. Genetic changes, pathologic features, imaging findings, and natural histories of a variety of histologic subtypes of OEC are discussed in this article.

摘要

卵巢上皮性癌(OEC)是最常见的卵巢恶性肿瘤,是一种具有多种组织学亚型的异质性疾病,具有特征性的细胞遗传学特征、分子特征、肿瘤信号通路和临床生物学行为。组织病理学和细胞遗传学的最新进展为 OEC 的病理生理学特征和自然史提供了深入了解。几项研究表明,高级别浆液性、子宫内膜样和透明细胞癌分别以涉及 TP53、K-ras/BRAF、CTNNB1 和 PIK3CA 基因的突变为特征。高级别浆液性癌是最常见的亚型,通常表现为疾病早期穿过体腔在卵巢外广泛扩散,而低级别浆液性和黏液性癌通常表现为早期疾病,因此预后极好。基于发病机制,最近的发现表明卵巢癌发生的二元模型,包括 I 型和 II 型。I 型(低级别浆液性、黏液性和子宫内膜样)癌症通常起源于明确的、遗传稳定的前驱病变(通常是交界性肿瘤);表现为大型附件肿块,处于早期疾病阶段;具有相对惰性的临床过程,总体预后良好。相比之下,II 型(高级别浆液性、子宫内膜样、混合性和未分化变体)则从头发生于附件上皮,通常表现为染色体不稳定性,具有侵袭性的生物学行为。对遗传性卵巢癌综合征和相关细胞遗传学异常的更好认识,导致人们对新型生物标志物和分子治疗方法的兴趣增加。本文讨论了各种组织学亚型的 OEC 的遗传变化、病理特征、影像学表现和自然史。

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