Glucagon-Like Peptide Receptor Agonist Inhibits Angiotensin II-Induced Proliferation and Migration in Vascular Smooth Muscle Cells and Ameliorates Phosphate-Induced Vascular Smooth Muscle Cells Calcification.

IF 6.8 2区医学 Q1 ENDOCRINOLOGY & METABOLISM Diabetes & Metabolism Journal Pub Date : 2024-01-01 Epub Date: 2024-01-03 DOI:10.4093/dmj.2022.0363

Jinmi Lee, Seok-Woo Hong, Min-Jeong Kim, Sun Joon Moon, Hyemi Kwon, Se Eun Park, Eun-Jung Rhee, Won-Young Lee

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Abstract

Backgruound: Glucagon-like peptide-1 receptor agonist (GLP-1RA), which is a therapeutic agent for the treatment of type 2 diabetes mellitus, has a beneficial effect on the cardiovascular system.

Methods: To examine the protective effects of GLP-1RAs on proliferation and migration of vascular smooth muscle cells (VSMCs), A-10 cells exposed to angiotensin II (Ang II) were treated with either exendin-4, liraglutide, or dulaglutide. To examine the effects of GLP-1RAs on vascular calcification, cells exposed to high concentration of inorganic phosphate (Pi) were treated with exendin-4, liraglutide, or dulaglutide.

Results: Ang II increased proliferation and migration of VSMCs, gene expression levels of Ang II receptors AT1 and AT2, proliferation marker of proliferation Ki-67 (Mki-67), proliferating cell nuclear antigen (Pcna), and cyclin D1 (Ccnd1), and the protein expression levels of phospho-extracellular signal-regulated kinase (p-Erk), phospho-c-JUN N-terminal kinase (p-JNK), and phospho-phosphatidylinositol 3-kinase (p-Pi3k). Exendin-4, liraglutide, and dulaglutide significantly decreased the proliferation and migration of VSMCs, the gene expression levels of Pcna, and the protein expression levels of p-Erk and p-JNK in the Ang II-treated VSMCs. Erk inhibitor PD98059 and JNK inhibitor SP600125 decreased the protein expression levels of Pcna and Ccnd1 and proliferation of VSMCs. Inhibition of GLP-1R by siRNA reversed the reduction of the protein expression levels of p-Erk and p-JNK by exendin-4, liraglutide, and dulaglutide in the Ang II-treated VSMCs. Moreover, GLP-1 (9-36) amide also decreased the proliferation and migration of the Ang II-treated VSMCs. In addition, these GLP-1RAs decreased calcium deposition by inhibiting activating transcription factor 4 (Atf4) in Pi-treated VSMCs.

Conclusion: These data show that GLP-1RAs ameliorate aberrant proliferation and migration in VSMCs through both GLP-1Rdependent and independent pathways and inhibit Pi-induced vascular calcification.

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胰高血糖素样肽受体激动剂抑制血管紧张素 II 诱导的血管平滑肌细胞增殖和迁移，并改善磷酸盐诱导的血管平滑肌细胞钙化。

背景：胰高血糖素样肽-1受体激动剂（GLP-1RA）是一种治疗2型糖尿病的药物，对心血管系统具有有益作用：为了研究 GLP-1RA 对血管平滑肌细胞（VSMC）增殖和迁移的保护作用，用依那西汀-4、利拉鲁肽或度拉鲁肽处理暴露于血管紧张素 II（Ang II）的 A-10 细胞。为了研究 GLP-1RAs 对血管钙化的影响，暴露在高浓度无机磷酸盐（Pi）中的细胞分别接受了艾森丁-4、利拉鲁肽或度拉鲁肽的治疗：结果：Ang II 增加了血管内皮细胞的增殖和迁移，Ang II 受体 AT1 和 AT2、增殖标志物 Ki-67 (Mki-67)、增殖细胞核抗原 (Pcna)、细胞周期蛋白 D1 (Ccc) 和细胞周期蛋白 D1 (Ccc) 的基因表达水平也增加了、和细胞周期蛋白 D1（Ccnd1）的基因表达水平，以及磷酸胞外信号调节激酶（p-Erk）、磷酸-c-JUN N-末端激酶（p-JNK）和磷酸磷脂酰肌醇 3-激酶（p-Pi3k）的蛋白表达水平。艾森丁-4、利拉鲁肽和杜拉鲁肽能显著减少 Ang II 处理的 VSMC 的增殖和迁移、Pcna 的基因表达水平以及 p-Erk 和 p-JNK 的蛋白表达水平。Erk抑制剂PD98059和JNK抑制剂SP600125降低了Pcna和Ccnd1的蛋白表达水平以及VSMCs的增殖。通过 siRNA 抑制 GLP-1R 可逆转依生丁-4、利拉鲁肽和度拉鲁肽对 Ang II 处理的 VSMCs 中 p-Erk 和 p-JNK 蛋白表达水平的降低。此外，GLP-1（9-36）酰胺还能减少 Ang II 处理的 VSMC 的增殖和迁移。此外，这些 GLP-1RA 还能通过抑制 Pi 处理的 VSMC 中的活化转录因子 4（Atf4）来减少钙沉积：这些数据表明，GLP-1RAs 可通过 GLP-1R 依赖性和独立途径改善 VSMC 的异常增殖和迁移，并抑制 Pi 诱导的血管钙化。

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来源期刊

Diabetes & Metabolism Journal Medicine-Endocrinology, Diabetes and Metabolism

CiteScore

10.40

自引率

6.80%

发文量

审稿时长

52 weeks

期刊介绍： The aims of the Diabetes & Metabolism Journal are to contribute to the cure of and education about diabetes mellitus, and the advancement of diabetology through the sharing of scientific information on the latest developments in diabetology among members of the Korean Diabetes Association and other international societies. The Journal publishes articles on basic and clinical studies, focusing on areas such as metabolism, epidemiology, pathogenesis, complications, and treatments relevant to diabetes mellitus. It also publishes articles covering obesity and cardiovascular disease. Articles on translational research and timely issues including ubiquitous care or new technology in the management of diabetes and metabolic disorders are welcome. In addition, genome research, meta-analysis, and randomized controlled studies are welcome for publication. The editorial board invites articles from international research or clinical study groups. Publication is determined by the editors and peer reviewers, who are experts in their specific fields of diabetology.