miR-223 通过靶向 FoxO3a 调节胰腺癌对顺铂的耐药性。
MiR-223 regulates CDDP resistance in pancreatic cancer via targeting FoxO3a.
机构信息
Center for Clinical Laboratory, People's Hospital of Xinjiang Uygur Autonomous Region, Urumqi, Xinjiang Uygur Autonomous Region, China.
出版信息
Eur Rev Med Pharmacol Sci. 2019 Sep;23(18):7892-7898. doi: 10.26355/eurrev_201909_19000.
OBJECTIVE
FoxO3a is a well-defined tumor suppressor gene in the forkhead transcription factor O subfamily (FoxO), and its reduction is related to the occurrence of various tumors. It was found that miR-223 expression is abnormally elevated in pancreatic cancer tissues. Bioinformatics analysis revealed a targeted complementary binding relationship between miR-223 and FoxO3a. This study explored whether miR-155 regulates the expression of FoxO3a and affects the proliferation, apoptosis, and cisplatin (CDDP) resistance of oral cancer cells.
MATERIALS AND METHODS
Dual-Luciferase reporter gene assay validated the targeted relationship between miR-223 and FoxO3a. The CDDP-resistant pancreatic cancer cell line BXPC3/CDDP was established, and the expressions of miR-223 and FoxO3a were compared. BXPC3/CDDP cells were divided into miR-NC group and miR-223 inhibitor group. QRT-PCR was adopted to test miR-223 and FoxO3a mRNA expressions. Western blot was performed to determine FoxO3a protein expression. Cell apoptosis was detected by flow cytometry and cell proliferation was detected by EdU staining.
RESULTS
There was a targeted regulatory relationship between miR-223 and FoxO3a mRNA. The expression of miR-223 was significantly higher, while the expression of FoxO3a mRNA and protein was significantly lower in BXPC3/CDDP cells than that in BXPC3 cells. Cell Counting Kit-8 (CCK-8) experiments showed that the same concentration of CDDP exhibited significantly lower proliferation inhibition in BXPC3/CDDP cells than BXPC3 cells. Compared with miR-NC group, transfection of miR-223 inhibitor significantly increased the expression of FoxO3a in BXPC3/CDDP cells, which significantly attenuated cell proliferation and enhanced apoptosis in CDDP-treated cells.
CONCLUSIONS
Increased expression of miR-233 was associated with CDDP resistance in pancreatic cancer cells. Inhibition of miR-223 expression upregulated FoxO3a expression, restrained pancreatic cancer cell proliferation, promoted cell apoptosis, and enhanced CDDP sensitivity in pancreatic cancer cells.
目的
FoxO3a 是叉头转录因子 O 亚家族(FoxO)中明确的肿瘤抑制基因,其减少与各种肿瘤的发生有关。研究发现 miR-223 在胰腺癌组织中的表达异常升高。生物信息学分析显示 miR-223 与 FoxO3a 之间存在靶向互补结合关系。本研究探讨了 miR-155 是否调节 FoxO3a 的表达并影响口腔癌细胞的增殖、凋亡和顺铂(CDDP)耐药性。
材料与方法
双荧光素酶报告基因实验验证了 miR-223 与 FoxO3a 的靶向关系。建立了耐 CDDP 的胰腺癌细胞系 BXPC3/CDDP,并比较了 miR-223 和 FoxO3a 的表达。将 BXPC3/CDDP 细胞分为 miR-NC 组和 miR-223 抑制剂组。采用 QRT-PCR 检测 miR-223 和 FoxO3a mRNA 的表达。Western blot 检测 FoxO3a 蛋白的表达。通过流式细胞术检测细胞凋亡,通过 EdU 染色检测细胞增殖。
结果
miR-223 与 FoxO3a mRNA 存在靶向调控关系。与 BXPC3 细胞相比,BXPC3/CDDP 细胞中 miR-223 的表达明显升高,而 FoxO3a mRNA 和蛋白的表达明显降低。细胞计数试剂盒-8(CCK-8)实验显示,相同浓度的 CDDP 对 BXPC3/CDDP 细胞的增殖抑制作用明显低于 BXPC3 细胞。与 miR-NC 组相比,转染 miR-223 抑制剂后,BXPC3/CDDP 细胞中 FoxO3a 的表达明显增加,CDDP 处理细胞的增殖明显受到抑制,凋亡明显增加。
结论
miR-223 的表达增加与胰腺癌细胞对 CDDP 的耐药性有关。抑制 miR-223 的表达上调 FoxO3a 的表达,抑制胰腺癌细胞增殖,促进细胞凋亡,并增强胰腺癌细胞对 CDDP 的敏感性。
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