MiR-202 promotes endometriosis by regulating SOX6 expression.

Dongli Zhang; Yanyun Li; Jun Tian; Hongxia Zhang; Shelian Wang

MiR-202 promotes endometriosis by regulating SOX6 expression.

Dongli Zhang, Yanyun Li, Jun Tian, Hongxia Zhang, Shelian Wang

International journal of clinical and experimental medicine · 2015 · vol. 8(10) , pp. 17757–64 · PMID:26770366 · W2416059550

article OA: green CC0 ⤵ 12 in-corpus citations

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⚙ AI-generated summary by claude@2026-06, 2026-06-07 ⓘ

MiR-202 is upregulated in endometriosis, promoting disease progression by targeting SOX6 and affecting downstream cell proliferation and migration proteins.

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Abstract

OBJECTIVES: This study is to investigate the role and mechanism of microRNA-202 (miR-202) in endometriosis. METHODS: Forty-five cases of ectopic endometrial tissues, 25 cases of eutopic endometrial tissues and 26 cases of normal endometrial tissues were collected. MiR-202 expression was detected by quantitative RT-PCR. The protein expressions of SOX6 (sex determining region Y-box 6) and its downstream proteins (p21, cyclin D1 and pRb (retinoblastoma protein)) were detected by immunochemistry and western blot. MTT and transwell assays were used to examine cell proliferation and cell migration. The dual luciferase assay was applied to validate whether miR-202 can directly target SOX6 gene. RESULTS: MiR-202 was highly expressed in eutopic and ectopic endometrial tissues than normal endometrial tissues (P < 0.05), and the expression was higher in tissues with III/IV stages than I/II stages (P < 0.05). The expression of SOX6 protein was lower in ectopic endometrial tissues than in normal endometrial tissues. In ectopic endometrial tissues, the expression of p21 was decreased while cyclin D1 and pRb was up-regulated than in normal endometrial tissues (P < 0.05). In cultured endometrial cells, miR-202 down-regulation induced up-regulation of SOX6 and p21 whereas down-regulation of cyclin D1 and pRb. MiR-202 promoted the proliferation and metastasis of endometrial cells. And, miR-202 could complementary bind to SOX6 3'UTR to regulate the expression of SOX6. CONCLUSION: MiR-202 was up-regulated in the endometriosis. Through targeting SOX6 and its downstream proteins (p21, cyclin D1 and pRb), miR-202 can promote the progression of endometriosis.

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endometriosis

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Cited by (12)

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License: CC0 · commercial use OK

[1] Anti-inflammatory, antiangiogenic, and apoptosis-inducing activity of DLBS1442, a bioactive fraction of Phaleria macrocarpa, in a RL95-2 cell line as&nbsp;a&nbsp;molecular model of endometriosis via openalex

[2] Current Strategies for Endometriosis Management via openalex

[3] Endometriosis Fertility Index via openalex

[4] Endometriosis, Leiomyoma and Adenomyosis: the Risk of Gynecologic Malignancy via openalex

[5] Enhanced miR-210 expression promotes the pathogenesis of endometriosis through activation of signal transducer and activator of transcription 3 via openalex

[6] Estrogen promotes the survival of human secretory phase endometrial stromal cells via CXCL12/CXCR4 up-regulation-mediated autophagy inhibition via openalex

[7] Expression of focal adhesion kinase in endometrial stromal cells of women with endometriosis was adjusted by ovarian steroid hormones. via openalex

[8] Functional MicroRNA Involved in Endometriosis via openalex

[9] MicroRNA expression profile in endometriosis: its relation to angiogenesis and fibrinolytic factors via openalex

[10] microRNAs and angiogenesis in endometriosis via openalex

[11] miR-142-3p is a novel regulator of cell viability and proinflammatory signalling in endometrial stroma cells via openalex

[12] miR-191 Modulates Malignant Transformation of Endometriosis Through Regulating TIMP3 via openalex

[13] Pathogenesis of endometriosis: The role of initial infection and subsequent sterile inflammation (Review) via openalex

[14] Potential role of aromatase inhibitors in the treatment of endometriosis via openalex

[15] [Study on microRNA expression in endometrium of luteal phase and its relationship with infertility of endometriosis]. via openalex

[16] The differential expression of microRNA-143,145 in endometriosis. via openalex

[17] The expression of microRNA-451 in human endometriotic lesions is inversely related to that of macrophage migration inhibitory factor (MIF) and regulates MIF expression and modulation of epithelial cell survival via openalex

[18] Uterine rupture before the onset of labor following extensive resection of deeply infiltrating endometriosis with myometrial invasion via openalex

[19] W2126413893 via openalex

[20] W1835881010 via openalex

[21] W1983074119 via openalex

[22] W1989078109 via openalex

[23] W2068603397 via openalex

[24] W231785437 via openalex

[25] W2128474430 via openalex

[26] W2128554075 via openalex

[27] W2142257207 via openalex

[28] W2151934245 via openalex