ARHGAP29 Is Involved in Increased Invasiveness of Tamoxifen-resistant Breast Cancer Cells and its Expression Levels Correlate With Clinical Tumor Parameters of Breast Cancer Patients.

IF 2.6 4区医学 Q2 GENETICS & HEREDITY

Cancer Genomics & Proteomics Pub Date : 2024-07-01 DOI:10.21873/cgp.20454

Maike Kansy, Katharina Wert, Katharina Kolb, Julia Gallwas, Carsten Gründker

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引用次数: 0

Abstract

Background/aim: Aggressive breast cancer (BC) cells show high expression of Rho GTPase activating protein 29 (ARHGAP29), a negative regulator of RhoA. In breast cancer cells in which mesenchymal transformation was induced, ARHGAP29 was the only one of 32 GTPase-activating enzymes whose expression increased significantly. Therefore, we investigated whether there is a correlation between expression of ARHGAP29 and tumor progression in BC. Since tamoxifen-resistant BC cells exhibit increased mesenchymal properties and invasiveness, we additionally investigated the relationship between ARHGAP29 and increased invasion rate in tamoxifen resistance. The question arises as to whether ARHGAP29 is a suitable prognostic marker for the progression of BC.

Materials and methods: Tissue microarrays were used to investigate expression of ARHGAP29 in BC and adjacent normal breast tissues. Knockdown experiments using siRNA were performed to investigate the influence of ARHGAP29 and the possible downstream actors RhoC and pAKT1 on invasive growth of tamoxifen-resistant BC spheroids in vitro.

Results: Expression of ARHGAP29 was frequently increased in BC tissues compared to adjacent normal breast tissues. In addition, there was evidence of a correlation between high ARHGAP29 expression and advanced clinical tumor stage. Tamoxifen-resistant BC cells show a significantly higher expression of ARHGAP29 compared to their parental wild-type cells. After knockdown of ARHGAP29 in tamoxifen-resistant BC cells, expression of RhoC was significantly reduced. Further, expression of pAKT1 decreased significantly. Invasive growth of three-dimensional tamoxifen-resistant BC spheroids was reduced after knockdown of ARHGAP29. This could be partially reversed by AKT1 activator SC79.

Conclusion: Expression of ARHGAP29 correlates with the clinical tumor parameters of BC patients. In addition, ARHGAP29 is involved in increased invasiveness of tamoxifen-resistant BC cells. ARHGAP29 alone or in combination with its downstream partners RhoC and pAKT1 could be suitable prognostic markers for BC progression.

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ARHGAP29参与了他莫昔芬耐药乳腺癌细胞侵袭性的增加，其表达水平与乳腺癌患者的临床肿瘤参数相关。

背景/目的：侵袭性乳腺癌（BC）细胞高表达 Rho GTPase 激活蛋白 29（ARHGAP29），它是 RhoA 的负调控因子。在诱导间质转化的乳腺癌细胞中，ARHGAP29 是 32 个 GTPase 激活酶中唯一一个表达量显著增加的酶。因此，我们研究了 ARHGAP29 的表达与 BC 肿瘤进展之间是否存在相关性。由于他莫昔芬耐药的BC细胞表现出更强的间质特性和侵袭性，我们还研究了他莫昔芬耐药时ARHGAP29与侵袭率增加之间的关系。由此产生的问题是，ARHGAP29 是否是 BC 病变进展的合适预后标志物：组织芯片用于研究ARHGAP29在BC和邻近正常乳腺组织中的表达。使用 siRNA 进行基因敲除实验，研究 ARHGAP29 及其可能的下游作用因子 RhoC 和 pAKT1 对他莫昔芬耐药 BC 球形体体外侵袭性生长的影响：结果：与邻近的正常乳腺组织相比，ARHGAP29在BC组织中的表达量经常增加。此外，有证据表明 ARHGAP29 的高表达与肿瘤的临床分期有关。与亲代野生型细胞相比，他莫昔芬抗性 BC 细胞的 ARHGAP29 表达明显升高。他莫昔芬耐药 BC 细胞敲除 ARHGAP29 后，RhoC 的表达明显降低。此外，pAKT1 的表达也明显减少。在敲除 ARHGAP29 后，他莫昔芬耐药 BC 三维球体的侵袭性生长减少。AKT1激活剂SC79可部分逆转这种情况：结论：ARHGAP29的表达与BC患者的临床肿瘤参数相关。结论：ARHGAP29的表达与BC患者的临床肿瘤参数相关，此外，ARHGAP29还参与了他莫昔芬耐药BC细胞侵袭性的增加。ARHGAP29单独或与其下游伙伴RhoC和pAKT1结合可成为BC进展的合适预后标志物。

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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.