THE IMPACT OF ALCOHOL ON PRO-METASTATIC N-GLYCOSYLATION IN PROSTATE CANCER.

A V Kubyshkin, I I Fomochkina, A M Petrosyan
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引用次数: 0

Abstract

Chronic alcohol abuse and alcoholism are considered risk factors for prostate cancer (PCa) progression, but the mechanism is unknown. Previously, we found that: (1) fragmentation of the Golgi complex correlates with the progression of PCa; (2) ethanol (EtOH) induces Golgi disorganization, which, in turn, alters intra-Golgi localization of some Golgi proteins. Also, progression of the prostate tumor is associated with activation of N-acetylglucosaminyltransferase-V (MGAT5)-mediated N-glycosylation of pro-metastatic proteins, including matriptase and integrins, followed by their enhanced retention at the cell surface. Here, using high-resolution microscopy, we found that alcohol effect on Golgi in low passage androgen-responsive LNCaP cells mimic the fragmented Golgi phenotype of androgen-refractory high passage LNCaP and PC-3 cells. Next, we detected that transition to androgen unresponsiveness is accompanied by downregulation of N-acetylglucosaminyltransferase-III (MGAT3), the enzyme that competes with MGAT5 for anti-metastatic N-glycan branching. Moreover, in low passage LNCaP cells, alcohol-induced Golgi fragmentation induced translocation of MGAT3 from the Golgi to the cytoplasm, while intra-Golgi localization of MGAT5 appeared unaffected. Then, the relationship between Golgi morphology, MGAT3 intracellular position, and clinicopathologic features was assessed in human PCa patient specimens with and without a history of alcohol dependence. We revealed that within the same clinical stage, the level of Golgi disorganization and the cytoplasmic shift of MGAT3 was more prominent in patients consuming alcohol. In vitro studies suggest that EtOH-induced downregulation of MGAT3 correlates with activation of MGAT5-mediated glycosylation and overexpression of both matriptase and integrins. In sum, we provide a novel insight into the alcohol-mediated tumor promotion.

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酒精对前列腺癌中促转移性n -糖基化的影响
慢性酒精滥用和酒精中毒被认为是前列腺癌(PCa)进展的危险因素,但其机制尚不清楚。先前,我们发现:(1)高尔基复合体的断裂与PCa的进展相关;(2)乙醇(EtOH)诱导高尔基分解,进而改变一些高尔基蛋白的高尔基内定位。此外,前列腺肿瘤的进展与n -乙酰氨基葡萄糖转移酶v (MGAT5)介导的前转移蛋白(包括基质酶和整合素)的n -糖基化激活有关,随后它们在细胞表面的保留增强。在这里,使用高分辨率显微镜,我们发现酒精对低传代雄激素应答的LNCaP细胞高尔基体的影响类似于雄激素难应答的高传代LNCaP和PC-3细胞的碎片化高尔基体表型。接下来,我们发现向雄激素无反应性的转变伴随着n -乙酰氨基葡萄糖转移酶iii (MGAT3)的下调,该酶与MGAT5竞争抗转移性n -聚糖分支。此外,在低传代LNCaP细胞中,酒精诱导的高尔基体断裂诱导MGAT3从高尔基体转移到细胞质,而MGAT5在高尔基体内的定位并未受到影响。然后,在有和没有酒精依赖史的人类PCa患者标本中评估高尔基形态、MGAT3细胞内位置与临床病理特征之间的关系。我们发现,在相同的临床阶段,高尔基体解体水平和MGAT3的细胞质移位在饮酒患者中更为突出。体外研究表明,etoh诱导的MGAT3下调与mgat5介导的糖基化激活以及基质酶和整合素的过表达相关。总之,我们为酒精介导的肿瘤促进提供了新的见解。
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