The Hypertension Related Gene G-Protein Coupled Receptor Kinase 4 Contributes to Breast Cancer Proliferation.

IF 1.8 Q3 ONCOLOGY
Breast Cancer : Basic and Clinical Research Pub Date : 2021-05-20 eCollection Date: 2021-01-01 DOI:10.1177/11782234211015753
Wei Yue, Hanh T Tran, Ji-Ping Wang, Katherine Schiermeyer, John J Gildea, Peng Xu, Robin A Felder
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引用次数: 0

Abstract

Purpose: Clinical studies have shown that breast cancer risk is increased in hypertensive women. The underlying molecular mechanism remains undetermined. The current study tests our hypothesis that G protein coupled receptor kinase 4 (GRK4) is a molecule that links hypertension and breast cancer. GRK4 plays an important role in regulation of renal sodium excretion. Sustained activation of GRK4 as in the circumstances of single nucleotide polymorphism (SNPs) causes hypertension. Expression of GRK4 in the kidney is regulated by cMyc, an oncogene that is amplified in breast cancer.

Methods: Western analysis was used to evaluate GRK4 protein expression in seven breast cancer cell lines. GRK4 gene single nucleotide polymorphism in breast cancer cell lines and in breast cancer cDNA arrays were determined using TaqMan Genotyping qPRC. The function of GRK4 was evaluated in MCF-7 cells with cMyc knock-down and GRK4 re-expression and in MDA-MB-468 cells expressing inducible GRK4 shRNA lentivirus constructs. Nuclei counting and 5-Bromo-2'-deoxy-uridine (BrdU) labeling were used to evaluate cell growth and proliferation.

Results: Genotyping of GRK4 SNPs in breast cancer cDNA arrays (n = 94) revealed that the frequency of carrying two hypertension related SNPs A142 V or R65 L is threefold higher in breast cancer patients than in healthy people (P = 7.53E-11). GRK4 protein is expressed in seven breast cancer cell lines but not the benign mammary epithelial cell line, MCF-10A. Three hypertension related SNPs in the GRK4 gene were identified in the breast cancer cell lines. Except for BT20, all other breast cancer lines have 1-3 GRK4 SNPs of which A142 V occurs in all 6 lines. MDA-MB-468 cells contain homozygous A142 V and R65 L SNPs. Knocking down cMyc in MCF-7 cells significantly reduced the growth rate, which was rescued by re-expression of GRK4. We then generated three stable GRK4 knock-down MDA-MB-468 lines using inducible lentiviral shRNA vectors. Doxycycline (Dox) induced GRK4 silencing significantly reduced GRK4 mRNA and protein levels, growth rates, and proliferation. As a marker of cell proliferation, the percentage of BrdU-labeled cells decreased from 45 ± 3% in the cells without Dox to 32 ± 5% in the cells treated with 0.1 µg/mL Dox.

Conclusions: GRK4 acts as an independent proliferation promotor in breast cancer. Our results suggest that targeted inhibition of GRK4 could be a new therapy for both hypertension and breast cancer.

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高血压相关基因 G 蛋白偶联受体激酶 4 促进乳腺癌增殖
目的:临床研究表明,高血压妇女患乳腺癌的风险增加。其潜在的分子机制仍未确定。目前的研究验证了我们的假设,即 G 蛋白偶联受体激酶 4(GRK4)是连接高血压和乳腺癌的分子。GRK4 在调节肾脏钠排泄方面发挥着重要作用。在单核苷酸多态性(SNPs)的情况下,GRK4的持续激活会导致高血压。GRK4 在肾脏中的表达受 cMyc 的调控,cMyc 是一种在乳腺癌中扩增的癌基因:方法:采用 Western 分析法评估 GRK4 蛋白在七种乳腺癌细胞系中的表达。使用 TaqMan 基因分型 qPRC 测定乳腺癌细胞系和乳腺癌 cDNA 阵列中 GRK4 基因的单核苷酸多态性。在敲除 cMyc 和重新表达 GRK4 的 MCF-7 细胞以及表达诱导性 GRK4 shRNA 慢病毒构建体的 MDA-MB-468 细胞中评估了 GRK4 的功能。细胞核计数和5-溴-2'-脱氧尿苷(BrdU)标记用于评估细胞的生长和增殖:乳腺癌 cDNA 阵列中 GRK4 SNPs 的基因分型(n = 94)显示,乳腺癌患者携带两个高血压相关 SNPs A142 V 或 R65 L 的频率是健康人的三倍(P = 7.53E-11)。GRK4 蛋白在七种乳腺癌细胞系中表达,但在良性乳腺上皮细胞系 MCF-10A 中不表达。在乳腺癌细胞系中发现了 GRK4 基因中三个与高血压相关的 SNPs。除 BT20 外,其他所有乳腺癌细胞系都有 1-3 个 GRK4 SNPs,其中 A142 V 在所有 6 个细胞系中都有出现。MDA-MB-468 细胞含有同源的 A142 V 和 R65 L SNPs。在MCF-7细胞中敲除cMyc会显著降低生长速度,而重新表达GRK4则可挽救生长速度。然后,我们利用诱导慢病毒 shRNA 载体生成了三个稳定的 GRK4 基因敲除 MDA-MB-468 株系。多西环素(Dox)诱导的 GRK4 沉默显著降低了 GRK4 mRNA 和蛋白水平、生长率和增殖。作为细胞增殖的标志物,BrdU标记细胞的百分比从未用过Dox的细胞的45 ± 3%下降到用0.1 µg/mL Dox处理的细胞的32 ± 5%:结论:GRK4是乳腺癌的独立增殖促进因子。我们的研究结果表明,靶向抑制 GRK4 可能是治疗高血压和乳腺癌的一种新疗法。
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来源期刊
CiteScore
5.10
自引率
3.40%
发文量
22
审稿时长
8 weeks
期刊介绍: Breast Cancer: Basic and Clinical Research is an international, open access, peer-reviewed, journal which considers manuscripts on all areas of breast cancer research and treatment. We welcome original research, short notes, case studies and review articles related to breast cancer-related research. Specific areas of interest include, but are not limited to, breast cancer sub types, pathobiology, metastasis, genetics and epigenetics, mammary gland biology, breast cancer models, prevention, detection, therapy and clinical interventions, and epidemiology and population genetics.
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