ISSN: 1165-158X

Клеточная и молекулярная биология

Открытый доступ

Наша группа организует более 3000 глобальных конференций Ежегодные мероприятия в США, Европе и США. Азия при поддержке еще 1000 научных обществ и публикует более 700 Открытого доступа Журналы, в которых представлены более 50 000 выдающихся деятелей, авторитетных учёных, входящих в редколлегии.

 

Журналы открытого доступа набирают больше читателей и цитируемости
700 журналов и 15 000 000 читателей Каждый журнал получает более 25 000 читателей

Абстрактный

ARHGAP11A Promotes Lung Adenocarcinoma Proliferation and Invasion through ROCK-LIMK-Cofilin Pathway

Jian Zhang and De-Yan Cao

Background: We aimed to investigate the clinical significance and biological roles of ARHGAP11A in lung adenocarcinoma (LUAD). Methods: We firstly analyzed the expression level of ARHGAP11A in LUAD based on TCGA. Next, quantitative reverse transcription PCR (qRT-PCR) was performed to examine the expression level of ARHGAP11A in LUAD cell lines (A549, and Calu-3). After ARHGAP11A knockdown in A549 cells, cell counting kit-8 (CCK-8) and trans well assays were used to measure the proliferation and migration ability of A549 cells with or without ARHGAP11A silence. Western blotting was utilized to identify the underlying pathway through which ARHGAP11A silencing mediates biological roles in LUAD. Results: ARHGAP11A was significantly over-expressed in LUAD tissues. Patients in the high ARHGAP11A expression subgroup experienced worse overall survival compared to the low expression subgroup. Univariate and multivariate analysis exhibited that ARHGAP11A was an independent prognostic predictor for LUAD. After ARHGAP11A silencing in A549 cells, cell proliferation rate, invasive and migratory capacity were observed to be inhibited. Remarkably, western blot results exhibited that reduction of ARHGAP11A remarkably inhibited the expression of ROCK, pLIMK2, and pCofilin in A549 cells. Conclusion: Increased ARHGAP11A expression could regulate LUAD cell proliferation and metastasis, and identified it as a poor prognostic biomarker in LUAD.

Отказ от ответственности: Этот реферат был переведен с помощью инструментов искусственного интеллекта и еще не прошел проверку или верификацию.