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MiR-320a inhibits gastric carcinoma by targeting activity in the FoxM1-P27KIP1 axis.


ABSTRACT: MicroRNAs (miRNAs) regulate tumorigenesis by inhibiting gene expression. In this study, we showed that miR-320a expression is decreased in human gastric cancer tissues and correlates inversely with expression of FoxM1, a key cell cycle regulator involved in gastric carcinoma. By contrast, the expression of P27KIP1, a downstream effector of FoxM1, correlates positively with miR-320a levels. Luciferase assays indicate that miR-320a suppresses FoxM1 expression, and in vitro recovery tests using FoxM1 siRNA indicate miR-320a inhibits gastric cancer cell proliferation by suppressing activity in the FoxM1-P27KIP1 axis. In vivo, nude mice injected with BGC-823 gastric cancer cells expressing a miR-320a inhibitor exhibit faster tumor growth than mice injected with control cells. Analysis of FoxM1 and P27KIP1 expression in tumor tissues indicates that miR-320a suppression increases the tumor growth by enhancing FoxM1-P27KIP1 signaling. These results thus reveal the crucial role played by miR-320a in limiting gastric carcinoma by directly targeting FoxM1- P27KIP1 axis.

SUBMITTER: Wang Y 

PROVIDER: S-EPMC5045395 | biostudies-literature | 2016 May

REPOSITORIES: biostudies-literature

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MiR-320a inhibits gastric carcinoma by targeting activity in the FoxM1-P27KIP1 axis.

Wang Yangyang Y   Zeng Jiping J   Pan Jianyong J   Geng Xue X   Li Lupeng L   Wu Jing J   Song Ping P   Wang Ying Y   Liu Jilan J   Wang Lixiang L  

Oncotarget 20160501 20


MicroRNAs (miRNAs) regulate tumorigenesis by inhibiting gene expression. In this study, we showed that miR-320a expression is decreased in human gastric cancer tissues and correlates inversely with expression of FoxM1, a key cell cycle regulator involved in gastric carcinoma. By contrast, the expression of P27KIP1, a downstream effector of FoxM1, correlates positively with miR-320a levels. Luciferase assays indicate that miR-320a suppresses FoxM1 expression, and in vitro recovery tests using Fox  ...[more]

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