Molecular Mechanism Linking BRCA1 Dysfunction to High Grade Serous Epithelial Ovarian Cancers with Peritoneal Permeability and Ascites.

A. Desai, J. Xu, K. Aysola, O. Akinbobuyi, M. White, V. Reddy, J. Okoli, C. Clark, E. Partridge, E. Childs, D. Beech, M. Rice, E. Reddy, V. Rao
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引用次数: 6

Abstract

Ovarian cancer constitutes the second most common gynecological cancer with a five-year survival rate of 40%. Among the various histotypes associated with hereditary ovarian cancer, high-grade serous epithelial ovarian carcinoma (HGSEOC) is the most predominant and women with inherited mutations in BRCA1 have a lifetime risk of 40-60%. HGSEOC is a challenge for clinical oncologists, due to late presentation of patient, diagnosis and high rate of relapse. Ovarian tumors have a wide range of clinical presentations including development of ascites as a result of deregulated endothelial function thereby causing increased vascular permeability of peritoneal vessels. The molecular mechanisms remain elusive. Studies have shown that fallopian tube cancers develop in women with BRCA1 gene mutations more often than previously suspected. Recent studies suggest that many primary peritoneal cancers and some high-grade serous epithelial ovarian carcinomas actually start in the fallopian tubes. In this article we have addressed the molecular pathway of a recently identified potential biomarker Ubc9 whose deregulated expression due to BRCA1 dysfunction can result in HGSEOC with peritoneal permeability and formation of ascites. We also discuss the role of downstream targets Caveolin-1 and Vascular Endothelial Growth Factor (VEGF) in the pathogenesis of ascites in ovarian carcinomas. Finally we hypothesize a signaling axis between Ubc9 over expression, loss of Caveolin-1 and induction of VEGF in BRCA1 mutant HGSEOC cells. We suggest that Ubc9-mediated stimulation of VEGF as a novel mechanism underlying ovarian cancer aggressiveness and ascites formation. Agents that target Ubc9 and VEGF signaling may represent a novel therapeutic strategy to impede peritoneal growth and spread of HGSEOC.
BRCA1功能障碍与高级别浆液性上皮性卵巢癌伴腹膜通透性和腹水的分子机制
卵巢癌是第二大常见妇科癌症,5年生存率为40%。在与遗传性卵巢癌相关的各种组织类型中,高级别浆液上皮性卵巢癌(HGSEOC)是最主要的,BRCA1遗传突变的女性的终生风险为40-60%。由于患者出现较晚,诊断较晚,复发率高,对临床肿瘤学家来说是一个挑战。卵巢肿瘤具有广泛的临床表现,包括由于内皮功能失调而导致腹水的发展,从而导致腹膜血管通透性增加。分子机制仍然难以捉摸。研究表明,携带BRCA1基因突变的女性患输卵管癌的几率比之前猜测的要高。最近的研究表明,许多原发性腹膜癌和一些高级浆液上皮性卵巢癌实际上起源于输卵管。在这篇文章中,我们讨论了最近发现的潜在生物标志物Ubc9的分子途径,Ubc9由于BRCA1功能障碍而表达失调,可导致HGSEOC伴腹膜通透性和腹水形成。我们还讨论了下游靶点Caveolin-1和血管内皮生长因子(VEGF)在卵巢癌腹水发病机制中的作用。最后,我们假设在BRCA1突变体HGSEOC细胞中存在Ubc9过表达、Caveolin-1缺失和VEGF诱导之间的信号轴。我们认为ubc9介导的VEGF刺激是卵巢癌侵袭性和腹水形成的新机制。靶向Ubc9和VEGF信号的药物可能是一种新的治疗策略,可以阻止HGSEOC在腹膜的生长和扩散。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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