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MicroRNA expression patterns in adrenocortical carcinoma variants and clinical pathologic correlations

机译:肾上腺皮质癌变体中MicroRNA的表达模式及其临床病理相关性

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Several microRNAs (miRNAs) were shown to be deregulated in adrenocortical carcinoma (ACC) as compared with adenoma, but a detailed assessment of their expression in its histologic variants and correlation with clinicopathologic characteristics has not been performed, so far. Our aim was to assess the expression of 5 selected miRNAs (IGF2 gene-related miR-483-3p and 5p and hypoxia-induced miR-210, miR-195, and miR-1974) in a series of 51 ACCs (35 classical, 6 myxoid, and 10 oncocytic) as compared with clinical and pathologic features and immunohistochemical expression of prognostic markers, including steroidogenic factor 1, p53, β-catenin, and glucose transporter 1. Oncocytic carcinomas had a reduced expression of miR-483-3p (P =.0325), miR-483-5p (P =.0175), and miR-210 (P =.0366), as compared with other histotypes. Overexpression of miR-210 was associated with the presence of necrosis (P =.0035), high Ki-67 index (P =.0013), and high glucose transporter 1 expression (P =.0043), whereas an inverse correlation with mitotic rate was observed in cases with high miR-493-3p (P =.0191) and miR-1974 (P =.0017) expression. High miR-1974 was also associated with low Ki-67 (P =.0312) and European Network for the Study of Adrenal Tumors stage (P =.0082) and negative p53 (P =.0013). At univariate analysis myxoid/classic histotype (P =.026), high miR-210 (P =.0465), high steroidogenic factor 1 protein (P =.0017), high Ki-67 (P =.0066), and high mitotic index (P =.0006) were significantly associated the shorter overall survival, the latter being the sole independent prognostic factor at multivariate analysis (P =.017). In conclusion, (a) miR-483-3p, miR-483-5p, and miR-210 are differentially expressed in ACC variants, and (b) high miR-210 is associated with clinicopathologic parameters of aggressiveness and a poor prognosis.
机译:与腺瘤相比,肾上腺皮质癌(ACC)中有数种microRNA(miRNA)失控,但到目前为止,尚未对其组织学变体中的表达及其与临床病理特征的相关性进行详细评估。我们的目的是评估在一系列51种ACC(35种经典的ACC)中,选择的5种miRNA(IGF2基因相关的miR-483-3p和5p以及缺氧诱导的miR-210,miR-195和miR-1974)的表达。与类固醇形成因子1,p53,β-catenin和葡萄糖转运蛋白1等预后标志物的临床和病理特征以及免疫组化表达相比,粘液样蛋白的表达为6例,而粘液样蛋白的表达为10例。粘液样癌的miR-483-3p(与其他组织型相比,P = .0325),miR-483-5p(P = .0175)和miR-210(P = .0366)。 miR-210的过表达与坏死的存在(P = .0035),高的Ki-67指数(P = .0013)和高的葡萄糖转运蛋白1表达(P = .0043)相关,而与有丝分裂呈负相关在高表达miR-493-3p(P = .0191)和miR-1974(P = .0017)的情况下观察到高表达。高miR-1974也与低Ki-67(P = .0312)和欧洲肾上腺肿瘤研究阶段(P = .0082)和阴性p53(P = .0013)相关。在单变量分析中,类固醇/经典组织型(P = .026),高miR-210(P = .0465),高类固醇生成因子1蛋白(P = .0017),高Ki-67(P = .0066)和高有丝分裂指数(P = .0006)与总生存期较短显着相关,后者是多因素分析中唯一的独立预后因素(P = .017)。总之,(a)miR-483-3p,miR-483-5p和miR-210在ACC变体中差异表达,并且(b)高miR-210与侵略性和不良预后的临床病理参数有关。

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