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Genomics of ovarian cancer progression reveals diverse metastatic trajectories including intraepithelial metastasis to the fallopian tube

机译:卵巢癌进展的基因组学揭示了多种转移轨迹包括上皮内转移至输卵管

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摘要

Accumulating evidence has supported the fallopian tube rather than the ovary as the origin for high grade serous ovarian cancer (HGSOC). To understand the relationship between putative precursor lesions and metastatic tumors, we performed whole exome sequencing on specimens from eight HGSOC patient progression series consisting of serous tubal intraepithelial carcinomas (STIC), invasive fallopian tube lesions, invasive ovarian lesions, and omental metastases. Integration of copy number and somatic mutations revealed patient-specific patterns with similar mutational signatures and copy number variation profiles across all anatomic sites, suggesting that genomic instability is an early event in HGSOC. Phylogenetic analyses supported STIC as precursor lesions in half of our patient cohort, but also identified STIC as metastases in two patients. Ex vivo assays revealed that HGSOC spheroids can implant in the fallopian tube epithelium and mimic STIC lesions. That STIC may represent metastases calls into question the assumption that STIC are always indicative of primary fallopian tube cancers.
机译:越来越多的证据支持输卵管而不是卵巢是高度浆液性卵巢癌(HGSOC)的起源。为了了解假定的前体病变与转移性肿瘤之间的关系,我们对来自8个HGSOC患者进展系列的标本进行了全外显子组测序,该系列患者包括浆液性输卵管上皮内癌(STIC),输卵管输卵管病变,卵巢浸润性病变和网膜转移。拷贝数和体细胞突变的整合揭示了在所有解剖部位具有相似突变特征和拷贝数变异特征的患者特异性模式,这表明基因组不稳定是HGSOC的早期事件。系统发生学分析支持STIC作为我们患者队列中一半的前体病变,但也将STIC确定为两名患者的转移灶。离体测定显示,HGSOC球体可以植入输卵管上皮并模拟STIC病变。 STIC可能代表转移,这使人们怀疑STIC始终指示原发性输卵管癌。

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