BRCA1 Mutation Leads to Deregulated Ubc9 Levels which Triggers Proliferation and Migration of Patient-Derived High Grade Serous Ovarian Cancer and Triple Negative Breast Cancer Cells

Jingyao Xu, A. Footman, Yunlong Qin, K. Aysola, S. Black, V. Reddy, Karan P. Singh, William E. Grizzle, S. You, D. Moellering, E. Reddy, Y. Fu, Veena Rao
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引用次数: 10

Abstract

Women who carry a germline mutation in BRCA1 gene typically develop triple negative breast cancers (TNBC) and high grade serous ovarian cancers (HGSOC). Previously, we reported that wild type BRCA1 proteins, unlike the disease-associated mutant BRCA1 proteins to bind the sole sumo E2-conjugating enzyme Ubc9. In this study, we have used clinically relevant cell lines with known BRCA1 mutations and report the in-vivo association of BRCA1 and Ubc9 in normal mammary epithelial cells but not in BRCA1 mutant HGSOC and TNBC cells by immunofluorescence analysis. BRCA1-mutant HGSOC/TNBC cells and ovarian tumor tissues showed increased expression of Ubc9 compared to BRCA1 reconstituted HGSOC, normal mammary epithelial cells and matched normal ovarian tissues. Knockdown of Ubc9 expression resulted in decreased proliferation and migration of BRCA1 mutant TNBC and HGSOC cells. This is the first study demonstrating the functional link between BRCA1 mutation, high Ubc9 expression and increased migration of HGSOC and TNBC cells. High Ubc9 expression due to BRCA1 mutation may trigger an early growth and transformation advantage to normal breast and ovarian epithelial cells resulting in aggressive cancers. Future work will focus on studying whether Ubc9 expression could show a positive correlation with BRCA1 linked HGSOC and basal like TNBC phenotype.
BRCA1突变导致Ubc9水平失调,引发患者源性高级别浆液性卵巢癌和三阴性乳腺癌细胞的增殖和迁移
携带BRCA1基因种系突变的女性通常会发展为三阴性乳腺癌(TNBC)和高级别浆液性卵巢癌(HGSOC)。之前,我们报道了野生型BRCA1蛋白,与疾病相关突变型BRCA1蛋白不同,可以结合唯一的相扑e2偶联酶Ubc9。在这项研究中,我们使用了已知BRCA1突变的临床相关细胞系,并通过免疫荧光分析报告了BRCA1和Ubc9在正常乳腺上皮细胞中的体内关联,而在BRCA1突变的HGSOC和TNBC细胞中没有关联。与BRCA1重组的HGSOC、正常乳腺上皮细胞和匹配的正常卵巢组织相比,BRCA1突变的HGSOC/TNBC细胞和卵巢肿瘤组织中Ubc9的表达增加。敲低Ubc9表达导致BRCA1突变体TNBC和HGSOC细胞增殖和迁移减少。这是第一个证明BRCA1突变、Ubc9高表达与HGSOC和TNBC细胞迁移增加之间存在功能联系的研究。BRCA1突变导致的Ubc9高表达可能触发正常乳腺和卵巢上皮细胞的早期生长和转化优势,从而导致侵袭性癌症。未来的工作将重点研究Ubc9表达是否与BRCA1相关的HGSOC和基底样TNBC表型呈正相关。
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