Inhibition of Increased Invasiveness of Breast Cancer Cells With Acquired Tamoxifen Resistance by Suppression of CYR61.

IF 2.6 4区医学 Q2 GENETICS & HEREDITY

Cancer Genomics & Proteomics Pub Date : 2023-11-01 DOI:10.21873/cgp.20403

Gerd Bauerschmitz, Silke Hüchel, Julia Gallwas, Carsten Gründker

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Abstract

Background/aim: Hormone sensitivity-targeted therapy with selective estrogen receptor modulators (SERMs), such as 4-hydroxytamoxifen (4-OHT), is the mainstay of treatment for breast cancers (BCs) that express estrogen receptor α (ERα). However, development of resistance limits this therapy approach. The question arises whether changes associated with 4-OHT resistance could be exploited therapeutically.

Materials and methods: First, 4-OHT-resistant sublines of ERα-positive breast carcinoma cell lines MCF-7 and T47D were generated. Viability was assessed by the Alamar Blue assay. Cell invasion was quantified in modified Boyden chambers with Matrigel. Changes in expression of CYR61, S100A4, and ERα were examined by RT-qPCR. Expression of CYR61 was suppressed by transient gene silencing using siRNA. Successful suppression was verified by western blot. Efficacy of 4-OHT treatment was analyzed by quantification of viability using Alamar Blue assay. Correlation of CYR61 levels in patients with luminal A BC to distant metastases-free survival was determined by Kaplan-Meier analysis.

Results: ERα-positive MCF-7 and T47D BC cells exhibit an extremely weak invasion rate. Acquired tamoxifen resistance significantly increased the invasive behavior of both tamoxifen-resistant MCF-7-TR and T47D-TR sublines. In addition, expression of CYR61 and S100A4 showed significantly increased levels, whereas expression of ERα was decreased. Suppression of CYR61 expression resulted in a significant decreased invasion rate. In addition, expression of S100A4 was reduced, whereas expression of ERα was increased. Furthermore, suppression of CYR61 resulted in re-sensitization to 4-OHT. High CYR61 levels in patients with luminal A BC resulted in reduced distant metastases-free survival.

Conclusion: The prometastatic factor CYR61 appears to play an important role in the increased invasiveness of tamoxifen-resistant ERα-positive BC cells. Its suppression leads to a lower invasion rate. Given the few therapeutic options available for tamoxifen-resistant BC, therapy that reduces CYR61 may improve its treatability in future.

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通过抑制CYR61抑制具有获得性三苯氧胺耐药性的乳腺癌症细胞侵袭性增加。

背景/目的：选择性雌激素受体调节剂（SERM），如4-羟基他莫昔芬（4-OHT）的激素敏感性靶向治疗是治疗表达雌激素受体α（ERα）的乳腺癌（BCs）的主要方法。然而，耐药性的发展限制了这种治疗方法。产生的问题是，与4-OHT耐药性相关的变化是否可以用于治疗。材料与方法：首先，从ERα阳性乳腺癌细胞系MCF-7和T47D中筛选出抗4-OHT亚系。通过Alamar Blue测定法评估可行性。用Matrigel在改良的Boyden室中定量细胞侵袭。通过RT-qPCR检测CYR61、S100A4和ERα的表达变化。通过使用siRNA的瞬时基因沉默来抑制CYR61的表达。通过蛋白质印迹验证了成功的抑制。4-OHT治疗的疗效通过使用Alamar蓝测定法定量生存能力来分析。通过Kaplan-Meier分析确定管腔A BC患者的CYR61水平与无远处转移生存率的相关性。结果：ERα阳性的MCF-7和T47D-BC细胞侵袭率极低。获得性三苯氧胺耐药性显著增加了三苯氧碱耐药性MCF-7-TR和T47D-TR亚系的侵袭行为。此外，CYR61和S100A4的表达水平显著升高，而ERα的表达降低。CYR61表达的抑制导致侵袭率显著降低。此外，S100A4的表达减少，而ERα的表达增加。此外，对CYR61的抑制导致对4-OHT的再致敏。管腔A BC患者的高CYR61水平导致无远处转移生存率降低。结论：促增殖因子CYR61在三苯氧胺耐药ERα阳性BC细胞侵袭性增强中起重要作用。它的抑制导致较低的入侵率。鉴于三苯氧胺耐药BC的治疗选择很少，减少CYR61的治疗可能会提高其未来的可治疗性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cancer Genomics & Proteomics ONCOLOGY-GENETICS & HEREDITY

CiteScore

5.00

自引率

8.00%

发文量

期刊介绍： Cancer Genomics & Proteomics (CGP) is an international peer-reviewed journal designed to publish rapidly high quality articles and reviews on the application of genomic and proteomic technology to basic, experimental and clinical cancer research. In this site you may find information concerning the editorial board, editorial policy, issue contents, subscriptions, submission of manuscripts and advertising. The first issue of CGP circulated in January 2004. Cancer Genomics & Proteomics is a journal of the International Institute of Anticancer Research. From January 2013 CGP is converted to an online-only open access journal. Cancer Genomics & Proteomics supports (a) the aims and the research projects of the INTERNATIONAL INSTITUTE OF ANTICANCER RESEARCH and (b) the organization of the INTERNATIONAL CONFERENCES OF ANTICANCER RESEARCH.