mir-3168 targeted inhibition of TP53 promotes malignant transformation and cisplatin resistance of AGS and AGS/DDP gastric cancer cells

WEI Wu-jun; WANG Chun-fang; JIANG Qi; XU Gui-dan; HUANG Jing-jing; LIN Cheng; HU Ren-tong; CHANG Zheng-yi

首页> 中文期刊> 《海南医科大学学报(英文版)》 >mir-3168 targeted inhibition of TP53 promotes malignant transformation and cisplatin resistance of AGS and AGS/DDP gastric cancer cells

mir-3168 targeted inhibition of TP53 promotes malignant transformation and cisplatin resistance of AGS and AGS/DDP gastric cancer cells

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Objective:To investigate the effect of mir-3168 on the malignant transformation and cisplatin resistance of AGS and AGS/DDP gastric cancer cells,and to verify its target gene.Methods:The expression of mir-3168 in AGS and AGS/DDP gastric cancer cells was detected by qPCR,and mir-3168 mimic,inhibitor and negative control were synthesized.They were transfected into AGS and AGS/DDP gastric cancer cells,respectively.The expression of mir-3168 and TP53 mRNA was detected by qPCR.Cell viability was detected by CCK8 under gradient cisplatin treatment and non treatment,apoptosis was detected by flow cytometry,cell invasion was detected by Transwell,and TP53 protein expression was detected by western blot,The database predicted the binding sites of mir-3168 and TP53.According to the binding sites,the double luciferase experiment was used to verify the binding of mir-3168 and TP53.Results:Compared with cisplatin sensitive gastric cancer cell AGS,mir-3168 was significantly overexpressed in cisplatin resistant gastric cancer cell AGS/DDP;mir-3168 mimic promotes cisplatin resistance,proliferation and invasion of AGS and AGS/DDP gastric cancer cells,and inhibits apoptosis of AGS and AGS/DDP gastric cancer cells;mir-3168 inhibitor inhibits cisplatin resistance,proliferation and invasion of AGS and AGS/DDP gastric cancer cells,and promotes apoptosis of AGS and AGS/DDP gastric cancer cells;mir-3168 mimic inhibits the expression of TP53 mRNA and protein,and mir-3168 inhibitor promotes the expression of TP53 mRNA and protein;Targetscan database predicted that there was a binding point between mir-3168 and TP53,and the double luciferase experiment suggested that mir-3168 was bound to TP53 through the predicted binding site.Conclusion:mir-3168 may promote the malignant transformation of AGS and AGS/DDP gastric cancer cells and cisplatin resistance by targeting TP53.

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《海南医科大学学报(英文版)》 |2023年第6期|8-14|共7页
作者
WEI Wu-jun; WANG Chun-fang; JIANG Qi; XU Gui-dan; HUANG Jing-jing; LIN Cheng; HU Ren-tong; CHANG Zheng-yi;
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作者单位

The Medical Laboratory Department of the Affiliated Hospital of Youjiang Medical College for Nationalities 533000;

The Clinical Medical Research Center for Hepatobiliary Diseases 533000;

The Department of Gastroenterology Affiliated Hospital of Youjiang Medical College for Nationalities 533000;

The Health Department of Baise Maternal and Child Health Hospital 533000;

The Cancer Department Affiliated Hospital of Youjiang Medical College for Nationalities 533000;

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原文格式 PDF
正文语种 chi
中图分类肿瘤学;
关键词
Gastric cancer; Malignant transformation; Cisplatin resistance; mir-3168; TP53;

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mir-3168 targeted inhibition of TP53 promotes malignant transformation and cisplatin resistance of AGS and AGS/DDP gastric cancer cells

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