Department of Cardiovascular Medicine, Graduate School of Medical Sciences, Kyoto Prefectural University of Medicine, Kyoto 602-8566, Japan.
Department of Pathology and Cell Regulation, Graduate School of Medical Sciences, Kyoto Prefectural University of Medicine, Kyoto 602-8566, Japan.
Cardiovasc Res. 2024 Nov 5;120(13):1562-1576. doi: 10.1093/cvr/cvae130.
Specific cavins and caveolins, known as caveola-related proteins, have been implicated in cardiac hypertrophy and myocardial injury. Cavin-2 forms complexes with other caveola-related proteins, but the role of Cavin-2 in cardiomyocytes (CMs) is poorly understood. Here, we investigated an unknown function of Cavin-2 in CMs.
Under cardiac stress-free conditions, systemic Cavin-2 knockout (KO) induced mild and significant CM hypertrophy. Cavin-2 KO suppressed phosphatase and tensin homologue (PTEN) associated with Akt signalling, whereas there was no difference in Akt activity between the hearts of the wild-type and the Cavin-2 KO mice under cardiac stress-free conditions. However, after swim training, CM hypertrophy was more facilitated with enhanced phosphoinositide 3-kinase (PI3K)-Akt activity in the hearts of Cavin-2 KO mice. Cavin-2 knockdown neonatal rat CMs (NRCMs) using adenovirus expressing Cavin-2 short hairpin RNA were hypertrophied and resistant to hypoxia and H2O2-induced apoptosis. Cavin-2 knockdown increased Akt phosphorylation in NRCMs, and an Akt inhibitor inhibited Cavin-2 knockdown-induced anti-apoptotic responses in a dose-dependent manner. Cavin-2 knockdown increased phosphatidylinositol-3,4,5-triphosphate production and attenuated PTEN at the membrane fraction of NRCMs. Immunostaining and immunoprecipitation showed that Cavin-2 was associated with PTEN at the plasma membrane of NRCMs. A protein stability assay showed that Cavin-2 knockdown promoted PTEN destabilization in NRCMs. In an Angiotensin II (2-week continuous infusion)-induced pathological cardiac hypertrophy model, CM hypertrophy and CM apoptosis were suppressed in CM-specific Cavin-2 conditional KO (Cavin-2 cKO) mice. Because Cavin-2 cKO mouse hearts showed increased Akt activity but not decreased extracellular signal-regulated kinase activity, suppression of pathological hypertrophy by Cavin-2 loss may be due to increased survival of healthy CMs.
Cavin-2 plays a negative regulator in the PI3K-Akt signalling in CMs through interaction with PTEN. Loss of Cavin-2 enhances Akt activity by promoting PTEN destabilization, which promotes physiological CM hypertrophy and may enhance Akt-mediated cardioprotective effects against pathological CM hypertrophy.
已知称为小窝相关蛋白的特定小窝蛋白和小窝蛋白在心肌肥厚和心肌损伤中起作用。Cavin-2 与其他小窝相关蛋白形成复合物,但 Cavin-2 在心肌细胞 (CM) 中的作用知之甚少。在这里,我们研究了 Cavin-2 在 CM 中的未知功能。
在心脏无应激条件下,全身性 Cavin-2 敲除 (KO) 诱导轻度但显着的 CM 肥大。Cavin-2 KO 抑制了与 Akt 信号相关的磷酸酶和张力蛋白同源物 (PTEN),而在心脏无应激条件下,野生型和 Cavin-2 KO 小鼠心脏中的 Akt 活性没有差异。然而,游泳训练后,Cavin-2 KO 小鼠心脏中的磷酸肌醇 3-激酶 (PI3K)-Akt 活性增强,CM 肥大程度更高。用表达 Cavin-2 短发夹 RNA 的腺病毒使新生大鼠心肌细胞 (NRCM) 中的 Cavin-2 敲低,导致心肌细胞肥大,并对缺氧和 H2O2 诱导的细胞凋亡具有抗性。Cavin-2 敲低增加了 NRCM 中的 Akt 磷酸化,并且 Akt 抑制剂以剂量依赖性方式抑制了 Cavin-2 敲低诱导的抗凋亡反应。Cavin-2 敲低增加了磷脂酰肌醇-3,4,5-三磷酸的产生,并减少了 NRCM 质膜上的 PTEN。免疫染色和免疫沉淀显示 Cavin-2 与 NRCM 质膜上的 PTEN 相关。蛋白质稳定性测定表明 Cavin-2 敲低促进了 NRCM 中 PTEN 的不稳定。在血管紧张素 II (2 周连续输注) 诱导的病理性心肌肥厚模型中,CM 肥大和 CM 凋亡在 CM 特异性 Cavin-2 条件性 KO (Cavin-2 cKO) 小鼠中受到抑制。由于 Cavin-2 cKO 小鼠心脏表现出 Akt 活性增加而细胞外信号调节激酶活性降低,因此 Cavin-2 缺失对病理性肥大的抑制可能是由于健康 CM 的存活增加所致。
Cavin-2 通过与 PTEN 相互作用在 CM 中的 PI3K-Akt 信号中起负调节作用。Cavin-2 的缺失通过促进 PTEN 失稳来增强 Akt 活性,从而促进生理性 CM 肥大,并可能增强 Akt 介导的对病理性 CM 肥大的心脏保护作用。
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