尿路上皮癌相关1基因通过竞争性抑制miR-18a增强乳腺癌细胞的他莫昔芬治疗耐药

doi:10.3969/j.issn.1671-167X.2017.02.020

摘要/Abstract

摘要：

目的：探讨尿路上皮癌相关1（urothelial carcinoma-associated 1，UCA1）基因及miR-18a在雌激素受体（estrogen receptor, ER）阳性的乳腺癌细胞他莫昔芬耐药中的作用和调控机制。方法：通过反转录实时定量PCR测定乳腺癌细胞中UCA1和miR-18a的表达，用双荧光素酶报告实验验证miR-18a和UCA1 3′UTR区域结合。在他莫昔芬敏感的MCF-7细胞中过表达UCA1或敲减miR-18a，在他莫昔芬耐药的LCC9和BT474细胞中敲减UCA1或过表达miR-18a，CCK-8方法测定细胞活力，软琼脂克隆形成实验测定细胞克隆形成能力，流式细胞术测定细胞周期。结果：他莫昔芬耐药的LCC2、LCC9和BT474细胞中，UCA1表达量显著高于他莫昔芬敏感的MCF-7细胞。MCF-7细胞在0.1 μmol/L 他莫昔芬处理后，UCA1的表达水平显著升高。UCA1过表达提高了MCF-7细胞在他莫昔芬处理后的活力，而UCA1 siRNA则显著降低了LCC9和BT474细胞在他莫昔芬处理后的活力。在MCF-7细胞中，相对于质粒对照+他莫昔芬组，UCA1+他莫昔芬组的克隆数目多19.0%，克隆平均大小增加29.0%，G1期细胞比例减少7.3%，S期细胞增加6.7%。在BT474细胞中，相对于siRNA对照+他莫昔芬组，si-UCA1+他莫昔芬组的克隆数目少54.0%，克隆平均大小减少42.0%，G1期细胞比例增加9.0%，S期细胞减少6.2%。UCA1有一个miR-18a结合位点，敲减miR-18a提高了MCF-7细胞在他莫昔芬处理后的活力，过表达miR-18a则显著降低了BT474细胞在他莫昔芬处理后的活力。在MCF-7细胞中，相对于对照+他莫昔芬组，miR-18a抑制+他莫昔芬组的克隆数目多15.0%，克隆平均大小增加33.0%，G1期细胞比例减少8.8%，S期细胞增加5.3%。在BT474细胞中，相对于对照+他莫昔芬组，miR-18a过表达+他莫昔芬组的克隆数目少47.0%，克隆平均大小减少25.0%，G1期细胞比例增加13.3%，S期细胞减少7.9%。结论： UCA1可以通过竞争性抑制miR-18a增强乳腺癌细胞的他莫昔芬治疗耐药。

关键词: 受体, 雌激素, 乳腺肿瘤, 尿路上皮癌相关1基因, 他莫昔芬

Abstract:

Objective： To investigate how urothelial carcinoma-associated 1 (UCA1) and miR-18a modulates acquired tamoxifen resistance and the relevant mechanisms in estrogen receptor (ER) positive cancer cells. Methods: qRT-PCR was performed to detect UCA1 and miR-18a expression in breast cancer cells. Dual luciferase assay was performed to detect the binding between miR-18a and UCA1 3′UTR. Tamoxifen sensitive MCF-7 cells were transfected with UCA1 expression vector or miR-18a inhi-bitors. Tamoxifen resistant LCC9 and BT474 cells were transfected with UCA1 siRNA or miR-18a mi-mics. CCK-8 assay was performed to detect cell viability. Soft agar assay was performed to assess cell colony formation. Flow cytometric analysis was performed to check cell cycle distribution. Results: UCA1 was significantly upregulated in tamoxifen resistant LCC2, LCC9, and BT474 cells than in tamoxifen sensitive MCF-7 cells. UCA1 expression was significantly upregulated in MCF-7 cells after treatment with 0.1 μmol/L tamoxifen. UCA1 overexpression enhanced cell viability of MCF-7 cells after tamoxifen treatment, while UCA1 siRNA significantly suppressed viability of LCC9 and BT474 cells after tamoxifen treatment. In MCF-7 cells, compared with vector control+tamoxifen group, the average cell colony number and colony size of the UCA1+tamoxifen group was 19.0% more and 29.0% larger respectively, while the proportions of the cells in G1 phase and in S phase were 7.3% lower and 6.7% higher respectively. In BT474 cells, compared with siRNA control+tamoxifen group, the average cell colony number and colony size of the si-UCA1+tamoxifen group were 54.0% less and 42.0% smaller respectively, while the proportions of the cells in G1 phase and in S phase were 9.0% higher and 6.2% lower respectively. UCA1 directly interacted with miR18a and reduced its expression in ER positive breast cancer cells. Knockdown of miR-18a increased viability of MCF-7 cells after tamoxifen treatment, while miR-18a overexpression significantly reduced viability of BT474 cells after tamoxifen treatment. In MCF-7 cells, compared with miRNA inhibitor control+tamoxifen group, the average cell colony number and colony size of the miR-18a inhibitor+tamoxifen group were 15.0% more and 33.0% larger respectively, while the proportions of the cells in G1 phase and in S phase were 8.8% lower and 5.3% higher respectively. In BT474 cells, compared with miRNA control+tamoxifen group, the average cell colony number and colony size of the miR-18a mimics+tamoxifen group were 47.0% less and 25.0% smaller respectively, while the proportions of the cells in G1 phase and in S phase were 13.3% higher and 7.9% lower respectively. Conclusion: UCA1 can increase tamoxifen resistance of ER positive breast cancer cells via competitively inhibiting of miR18a.

Key words: Receptors, estrogen, Breast neoplasms, UCA1, Tamoxifen

中图分类号:

R737.9

李秀楠，刘爱蕙，唐欣，任宇. 尿路上皮癌相关1基因通过竞争性抑制miR-18a增强乳腺癌细胞的他莫昔芬治疗耐药[J]. 北京大学学报(医学版), 2017, 49(2): 295-302.

LI Xiu-nan, LIU Ai-hui, TANG Xin, REN Yu. Urothelial carcinoma-associated 1 enhances tamoxifen resistance in breast cancer cells through competitively inhibiting miR-18a[J]. Journal of Peking University(Health Sciences), 2017, 49(2): 295-302.

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