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IBSP a potential recurrence biomarker promotes the progression of colorectal cancer via Fyn/β‐catenin signaling pathway

机译:IBSP是一种潜在的复发生物标志物通过Fyn /β-catenin信号通路促进结肠直肠癌的进展

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摘要

Colorectal cancer (CRC) is a frequently occurring digestive system cancer and postoperative tumor metastasis and recurrence are the main reasons for the failure of CRC treatment. The aim of this study was to identifying and validating key genes associated with metastatic recurrence of CRC. RNA expression of three datasets ({"type":"entrez-geo","attrs":{"text":"GSE17538","term_id":"17538"}}GSE17538, {"type":"entrez-geo","attrs":{"text":"GSE32323","term_id":"32323"}}GSE32323, and {"type":"entrez-geo","attrs":{"text":"GSE29623","term_id":"29623"}}GSE29623) was used for biomarker discovery. We identified integrin‐binding sialoprotein (IBSP) as a candidate biomarker which was validated in three clinical cohorts ({"type":"entrez-geo","attrs":{"text":"GSE41258","term_id":"41258"}}GSE41258, {"type":"entrez-geo","attrs":{"text":"GSE21510","term_id":"21510"}}GSE21510, and {"type":"entrez-geo","attrs":{"text":"GSE39582","term_id":"39582"}}GSE39582) and our clinical specimens. The results suggested that IBSP expression significantly increased at mRNA and protein levels among CRC cases, which was associated with metastatic recurrence, metastasis, high risk of recurrence, and poor survival in CRC. Consistent results were obtained in CRC cells. The relative level of serum IBSP evidently increased among CRC patients relative to normal controls, and downregulated after operation. As suggested by gene set enrichment analysis (GSEA), the IBSP level was associated with cell‐matrix adhesion in CRC. Functional experiments in vitro showed that IBSP promoted the growth and aggressiveness of CRC, and the potential mechanism by which IBSP promoted carcinogenesis of CRC was the abnormal activation of Fyn/β‐catenin signaling pathway. To sum up, findings in the present work indicate that IBSP can serve as the candidate biomarker for the diagnosis, treatment, and prognosis of CRC.
机译:结肠直肠癌(CRC)是一个频繁出现消化系统癌症及术后肿瘤转移和复发是用于CRC治疗失败的主要原因。本研究的目的是为了识别和验证与CRC的转移性复发有关的关键基因。的三个数据集RNA表达({ “类型”: “的Entrez-缘”, “ATTRS”:{ “文本”: “GSE17538”, “term_id”: “17538”}} GSE17538,{ “类型”:“的Entrez-地理”, “ATTRS”:{ “文本”: “GSE32323”, “term_id”: “32323”}} GSE32323,和{ “类型”: “的Entrez-缘”, “ATTRS”:{ “文本”: “GSE29623”用于生物标记发现 “29623”}} GSE29623): “term_id”。我们确定了整联蛋白结合唾液蛋白(IBSP),其在三个临床同伙验证的候选生物标志物({“类型”:“Entrez的-地理”,“ATTRS”:{“文”:“GSE41258”,“term_id”:” 41258 “}} GSE41258,{” 类型 “:” 的Entrez-缘 “ ”ATTRS“:{ ”文本“: ”GSE21510“, ”term_id“: ”21510“}} GSE21510,和{ ”类型“:” entrez-地理”, “ATTRS”:{ “文”: “GSE39582”, “term_id”: “39582”}} GSE39582)和我们的临床标本。结果表明,IBSP表达显著CRC的情况下,这是转移性复发,转移,复发的高风险和生存差CRC相关当中的mRNA和蛋白水平增加。一致的结果,在CRC细胞获得。血清IBSP的相对水平的CRC患者相对于正常对照组中显着增加,和运算后下调。如通过基因组富集分析(GSEA)所建议的,IBSP水平与在CRC细胞 - 基质粘附相关联。体外功能实验表明,IBSP促进CRC的生长和侵略性,并且通过该IBSP促进CRC的致癌的潜在机制是的Fyn的异常激活/β连环蛋白信号传导途径。综上所述,在目前的工作中发现表明,国际基础科学计划可以作为候选生物标记物用于诊断,治疗和CRC的预后。

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