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首页> 外文期刊>Pathology >The secondary Mullerian system, field effect, BRCA, and tubal fimbria: our evolving understanding of the origin of tubo-ovarian high-grade serous carcinoma and why assignment of primary site matters
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The secondary Mullerian system, field effect, BRCA, and tubal fimbria: our evolving understanding of the origin of tubo-ovarian high-grade serous carcinoma and why assignment of primary site matters

机译:次生穆勒系统,场效应,BRCA和输卵管纤维膜:我们对输卵管卵巢高级浆液性癌的起源以及为什么分配主要部位的认识不断发展

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It has long been held that most epithelial ovarian carcinomas arise from the ovarian surface epithelium. Theories on origin were based on the assumption that there was a common cell of origin for all ovarian carcinoma histotypes, and that these histotypes were closely related and frequently admixed. It is now recognised that the histotypes are distinct diseases. Recent studies on early, organ-confined, non-uterine high-grade serous carcinoma (HGSC) have led to a change in our understanding of their anatomical site of origin. These studies were initially on patients at high risk of developing HGSC but more recently have been extended to cases without family history or genetic markers of increased risk. These have shown that incidental HGSC, when detected before dissemination, is most commonly identified in the tubal fimbria. As a result, we have had to revisit theories on the cell and site of origin of HGSC. This progress in our understanding has necessitated a change in how we handle cases in clinical practice, as it impacts on primary site assignment, which in turn has implications for staging. In this review we will discuss the evolution of our understanding of the cell of origin of HGSC, the evidence for the tubal fimbria as the anatomical site of origin of most non-uterine HGSC, and the clinical implications of these recent developments.
机译:长期以来一直认为,大多数上皮性卵巢癌源自卵巢表面上皮。关于起源的理论是基于以下假设:所有卵巢癌组织学类型都有一个共同的起源细胞,并且这些组织学类型密切相关并且经常混合。现在已经认识到,组织型是不同的疾病。对早期,器官受限,非子宫高级浆液性癌(HGSC)的最新研究已导致我们对它们的解剖起源部位的理解发生了变化。这些研究最初针对的是发生HGSC的高风险患者,但最近已扩展到没有家族史或遗传风险增加的病例。这些表明,偶然的HGSC,在传播前被检测出,最常见于输卵管菌毛。结果,我们不得不重新审视关于HGSC的细胞和起源部位的理论。我们理解的这一进步需要改变我们在临床实践中处理病例的方式,因为这会影响主要部位的分配,进而影响分期。在这篇综述中,我们将讨论我们对HGSC起源细胞的理解的演变,输卵管纤维膜作为大多数非子宫HGSC起源的解剖部位的证据,以及这些最新进展的临床意义。

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