一种新的Ubc9依赖通路调节SIRT1- ER-α轴和brca1相关的TNBC肺转移。

Jingyao Xu, Collin Shumate, Yulong Qin, V. Reddy, Yonte Burnam, V. López, J. Okoli, E. P. Reddy, Veena N Rao
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引用次数: 5

摘要

三阴性乳腺癌(TNBC)是一种异质性疾病,具有较高的复发率和远处转移率。与其他人群相比,非裔美国女性(AA) BRCA1突变和TNBC的频率更高。基底样肿瘤比其他TNBC亚型有更高的脑、肺和远端淋巴结转移率,导致更高的死亡率。我们之前的研究表明,SUMO e2偶联酶Ubc9可诱导brca1功能不全的TNBC细胞和TNBC细胞系的增殖和迁移,这些细胞系是由TNBC女性胸膜积液转移建立的。为了了解参与远处转移的下游信号轴,我们使用了临床相关的BRCA1突变体和肺转移性TNBC细胞系,我们的结果显示,通过免疫荧光分析,与正常乳腺上皮细胞相比,这些细胞中caveolin-1、VEGF和SIRT1的表达不受调节。我们观察到SIRT1是由野生型BRCA1a和BRCA1a I26A突变体诱导的,与TNBC细胞中疾病相关的Ubc9结合突变体不同。敲低Ubc9可诱导TNBC中SIRT1的表达和乳腺癌细胞中ER-α的表达。这是首次报道Ubc9在BRCA1相关TNBC细胞中抑制SIRT1和ER-α表达的作用。这也表明,诱导SIRT1表达可能不需要bard依赖的E3泛素连接酶和BRCA1的HR(同源重组)活性。我们的研究结果首次表明,在BRCA1突变体TNBC中,ubc9介导的VEGF诱导、caveolin-1、SIRT1和ER-α表达的抑制是TNBC EMT(上皮间质转化)导致肺转移伴胸腔积液的一种新的分子机制。靶向Ubc9诱导SIRT1和ER-α的药物或使用SIRT1激动剂联合化疗可作为治疗基底样转移性brca1相关TNBC的有希望的靶向治疗方法,从而降低TNBC患者的死亡率。
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A novel Ubc9 -dependent pathway regulates SIRT1- ER-α Axis and BRCA1-associated TNBC lung metastasis.
Triple negative breast cancer (TNBC) is a heterogeneous disease and has a higher rate of recurrence and distant metastasis. African-American (AA) women have a higher frequency of BRCA1 mutations and TNBC compared to other populations. Basal-like tumors have a higher rate of brain, lung and distant nodal metastasis more than other TNBC subtypes, contributing to higher mortality rate. Our previous work suggested Ubc9, a SUMO E2-conjugating enzyme to induce proliferation and migration of BRCA1-incompetent TNBC cells and TNBC cell lines established from the pleural effusion metastasis of a woman with TNBC. To understand the downstream signaling axis involved in distant metastasis we have used clinically relevant BRCA1 mutant and lung metastatic TNBC cell lines and our results show deregulated expression of caveolin-1, VEGF and SIRT1 in these cells compared to normal mammary epithelial cells by immunofluorescence analysis. We observed SIRT1 to be induced by wild type BRCA1a and BRCA1a I26A mutant unlike the disease associated Ubc9 binding mutants in TNBC cells. Knock down of Ubc9 induced SIRT1 expression in TNBC and ER-α expression in breast cancer cells. This is the first report demonstrating a role for Ubc9 in repressing both SIRT1 and ER-α expression in BRCA1 associated TNBC cells. It also suggests that the BARD-dependent E3 Ubiquitin ligase and HR (homologous recombination) activity of BRCA1 may not be required for inducing SIRT1 expression. Our results suggest for the first time that in BRCA1 mutant TNBC Ubc9-mediated induction of VEGF, inhibition of caveolin-1, SIRT1 and ER-α expression as a novel molecular mechanism underlying TNBC EMT (epithelial mesenchymal transition) leading to lung metastasis with pleural effusion. Drugs that target Ubc9 to both induce SIRT1 and ER-α or using SIRT1 agonists in combination with chemotherapy can be used as a promising targeted therapeutic approach for treating basal-like metastatic BRCA1-linked TNBC thus reducing the mortality in patients with TNBC.
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