首页> 外文期刊>European journal of cancer: official journal for European Organization for Research and Treatment of Cancer (EORTC) [and] European Association for Cancer Research (EACR) >Hepatitis A virus cellular receptor 1/kidney injury molecule-1 is a susceptibility gene for clear cell renal cell carcinoma and hepatitis A virus cellular receptor/kidney injury molecule-1 ectodomain shedding a predictive biomarker of tumour progression
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Hepatitis A virus cellular receptor 1/kidney injury molecule-1 is a susceptibility gene for clear cell renal cell carcinoma and hepatitis A virus cellular receptor/kidney injury molecule-1 ectodomain shedding a predictive biomarker of tumour progression

机译:甲型肝炎病毒细胞受体1 /肾损伤分子-1是透明细胞肾细胞癌的易感基因,甲型肝炎病毒细胞受体/肾损伤分子-1胞外域脱落了肿瘤进展的预测生物标志物

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Aim of the study: To correlate hepatitis A virus cellular receptor (HAVCR)/kidney injury molecule-1 (KIM-1) expression in clear cell renal cell carcinoma (ccRCC) tumours with patient outcome and study the consequences of HAVCR/KIM-1 ectodomain shedding. Methods: HAVCR/KIM-1 expression in ccRCC, oncocytomes, papillary carcinomas and unaffected tissue counterparts was evaluated. Minimal change disease and pre-clamping normal and ccRCC tissue biopsies were included. Tissue microarrays from 98 ccRCC tumours were analysed. Tumour registry data and patient outcome were retrospectivelly collected. Deletions in HAVCR/KIM-1 ectodomain and lentiviral infection of 786-O cells with HAVCR/KIM-1 mutated constructs to determine their subcellular distribution and invasive capacity were performed. Results: HAVCR/KIM-1 was expressed in ccRCC, papillary tumours and in tubule cells of adjacent and distal unaffected counterparts of ccRCC tumours. The latest was not related to ischemic or tumour-related paracrine effects since pre-clamping normal biopsies were positive for HAVCR/KIM-1 and unaffected counterparts of papillary tumours were negative. HAVCR/KIM-1 analyses in patients and the invasive capacity of HAVCR/KIM-1 shedding mutants in cell lines demonstrated that: (i) relative low HAVCR/KIM-1 membrane levels correlate with activated shedding in ccRCC patients and mutant cell lines; (ii) augmented shedding directly correlates with higher invasiveness and tumour malignancy. Concluding statements: Constitutive expression of HAVCR/KIM-1 in kidney might constitute a susceptibility trait for ccRCC tumour development. Enhanced HAVCR/KIM-1 ectodomain shedding promotes invasive phenotype in vitro and more aggressive tumours in vivo.
机译:研究目的:将透明细胞肾细胞癌(ccRCC)肿瘤中的甲型肝炎病毒细胞受体(HAVCR)/肾损伤分子1(KIM-1)表达与患者预后相关,并研究HAVCR / KIM-1的后果胞外域脱落。方法:评估HAVCR / KIM-1在ccRCC,肿瘤细胞,乳头状癌和未受影响的组织对应物中的表达。包括最小变化疾病以及钳夹前的正常和ccRCC组织活检。分析了来自98 ccRCC肿瘤的组织芯片。回顾性收集肿瘤登记数据和患者预后。进行HAVCR / KIM-1胞外域的缺失和用HAVCR / KIM-1突变构建体对786-O细胞的慢病毒感染,以确定其亚细胞分布和侵袭能力。结果:HAVCR / KIM-1在ccRCC,乳头状瘤以及与ccRCC肿瘤相邻和未受影响的远端对应小管细胞中表达。最新的结果与缺血性或肿瘤相关的旁分泌作用无关,因为钳夹前的正常活检对HAVCR / KIM-1呈阳性,而未受影响的乳头状肿瘤对应物则为阴性。对患者的HAVCR / KIM-1分析以及HAVCR / KIM-1脱落突变株在细胞系中的侵袭能力表明:(i)相对较低的HAVCR / KIM-1膜水平与ccRCC患者和突变细胞系中的活化脱落有关; (ii)脱落增加与更高的浸润性和肿瘤恶性直接相关。结论:肾脏中HAVCR / KIM-1的组成型表达可能构成ccRCC肿瘤发展的易感性状。增强的HAVCR / KIM-1胞外域脱落促进体外侵袭性表型和体内更具侵袭性的肿瘤。

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