雌二醇介导LINC01541与miR-429的相互作用以促进G1/G2期子宫内膜样腺癌的血管生成:一项初步研究。
Estradiol mediates the interaction of LINC01541 and miR-429 to promote angiogenesis of G1/G2 endometrioid adenocarcinoma : A pilot study.
作者信息
Qiao Dan, Qin Xiaoduo, Yang Haiyan, Liu Xuantong, Liu Libing, Liu Sufen, Jia Zhongzhi
机构信息
Department of Gynecology, Dalian Medical University, Dalian, China.
Department of Gynecology, Changzhou No. 2 People's Hospital, Changzhou, China.
出版信息
Front Oncol. 2022 Aug 5;12:951573. doi: 10.3389/fonc.2022.951573. eCollection 2022.
BACKGROUND
Endometrioid adenocarcinoma (EAC) is the most common subtype of endometrial cancer (EC) and is an estrogen-related cancer. In this study, we sought to investigate the expressions and mechanism of action of 17β-estradiol (E2) and long noncoding RNA (lncRNA) LINC01541 in G1/G2 EAC samples.
METHODS
The expressions of estrogen receptor β (ESR2), LINC01541, miR-200s, and VEGFA were evaluated using real-time PCR in human EAC tissues (n = 8) and adjacent normal tissues (n = 8). Two EC cell lines (Ishikawa and RL95-2) were selected for validation . Bioinformatics analyses and luciferase reporter analyses were performed to verify potential binding sites. qRT-PCR, Western blot, and CCK-8 were used to identify the regulatory mechanisms of related genes in cell biological behavior.
RESULTS
Compared with adjacent normal tissues, LINC01541 and miR-200s family (except miR-200c) were highly expressed in EAC tissues (n=8), while ESR2 and VEGFA were lowly expressed in EAC tissues (* < 0.05; ** < 0.01). : E2 inhibited the expression of LINC01541 and miR-429 in both cell lines, and estrogen antagonist (PHTPP) could reverse this effect, in addition, PHTPP could promote the proliferation of these two cancer cells, cell transfection LINC01541 also had this effect after overexpression of plasmid and miR-429 mimic. E2 promotes the expression of VEGFA in both cell lines, and PHTPP can also reverse this effect. LINC01541 interacts with miR-429 to promote the expression of each other, and both inhibit the synthesis of VEGFA in EAC cells after overexpression. Through the double validation of bioinformatics analysis and dual fluorescein reporter gene, it was confirmed that miR-429 targets the regulation of VEGFA expression (* < 0.05; ** < 0.01).
CONCLUSION
E2 promotes the synthesis of VEGFA by altering the expression levels of LINC01541 and miR-429 in EAC, thereby affecting the angiogenesis process of EAC. Also, E2-mediated LINC01541/miR-429 expression may affect cell migration in EAC. In addition, we identified a reciprocal promotion between LINC01541 and miR-429.
背景
子宫内膜样腺癌(EAC)是子宫内膜癌(EC)最常见的亚型,是一种与雌激素相关的癌症。在本研究中,我们试图研究17β-雌二醇(E2)和长链非编码RNA(lncRNA)LINC01541在G1/G2期EAC样本中的表达及作用机制。
方法
采用实时定量PCR检测人EAC组织(n = 8)和相邻正常组织(n = 8)中雌激素受体β(ESR2)、LINC01541、miR-200s和VEGFA的表达。选择两种EC细胞系(Ishikawa和RL95-2)进行验证。进行生物信息学分析和荧光素酶报告基因分析以验证潜在的结合位点。采用qRT-PCR、蛋白质免疫印迹法和CCK-8法鉴定相关基因在细胞生物学行为中的调控机制。
结果
与相邻正常组织相比,LINC01541和miR-200s家族(miR-200c除外)在EAC组织(n = 8)中高表达,而ESR2和VEGFA在EAC组织中低表达(*P < 0.05;**P < 0.01)。E2抑制两种细胞系中LINC01541和miR-429的表达,雌激素拮抗剂(PHTPP)可逆转这种作用,此外,PHTPP可促进这两种癌细胞的增殖,转染LINC01541质粒过表达和miR-429模拟物后也有此作用。E2促进两种细胞系中VEGFA的表达,PHTPP也可逆转这种作用。LINC01541与miR-429相互作用促进彼此表达,过表达后二者均抑制EAC细胞中VEGFA的合成。通过生物信息学分析和双荧光素报告基因的双重验证,证实miR-429靶向调控VEGFA的表达(*P < 0.05;**P < 0.01)。
结论
E2通过改变EAC中LINC01541和miR-429的表达水平促进VEGFA的合成,从而影响EAC的血管生成过程。此外,E2介导的LINC01541/miR-429表达可能影响EAC中的细胞迁移。另外,我们发现LINC01541和miR-429之间存在相互促进作用。
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