Mita Shin-ichiro, Kobayashi Naohiko, Yoshida Kohtaro, Nakano Shigefumi, Matsuoka Hiroaki
Department of Hypertension and Cardiorenal Medicine, Dokkyo University School of Medicine, Mibu, Tochigi, 321-0293, Japan.
J Hypertens. 2005 Jan;23(1):87-96. doi: 10.1097/00004872-200501000-00017.
Rho-kinase plays a crucial role in various cellular functions. To elucidate molecular mechanisms of Rho-kinase-mediated cardiovascular remodeling in vivo, we evaluated whether a signaling pathway through Rho is involved, and whether Y-27632, a specific Rho-kinase inhibitor, stimulates endothelial nitric oxide synthase (eNOS) and suppresses the oxidative stress and lectin-like oxidized low-density lipoprotein receptor-1 (LOX-1) pathway in the left ventricle of Dahl salt-sensitive hypertensive (DS) rats.
Y-27632 (3 mg/kg per day) or vehicle were given for 5 weeks, from age 6 weeks to a stage of left ventricular hypertrophy (11 weeks). Age-matched Dahl salt-resistant (DR) rats fed the same diet served as a control group.
Increased left ventricular weight in the hypertrophy stage was significantly ameliorated by Y-27632. Upregulated RhoA protein, Rho-kinase gene expression and myosin light-chain phosphorylation in the hypertrophy stage were suppressed by Y-27632. Increased expression of NAD(P)H oxidase p22phox, p47phox, gp91phox and LOX-1 in DS rats were inhibited by Y-27632. Upregulated protein kinase Cepsilon and p65 nuclear factor-kappaB phosphorylation in DS rats was reduced by Y-27632. In contrast, downregulated eNOS expression in hypertrophy stage was upregulated by Y-27632. Y-27632 effectively inhibited vascular lesion formation, such as medial thickness and perivascular fibrosis, and suppressed transforming growth factor-beta1, type I and III collagen, and fibronectin gene expression.
Inhibiting the Rho-kinase pathway may play a key role in the cardioprotective effect on cardiovascular remodeling associated with eNOS and the oxidative stress-LOX-1 pathway in DS rats, and may be at least a potential therapeutic strategy for hypertension with cardiac hypertrophy.
Rho激酶在多种细胞功能中发挥关键作用。为阐明Rho激酶介导的体内心血管重塑的分子机制,我们评估了是否涉及通过Rho的信号通路,以及特异性Rho激酶抑制剂Y-27632是否能刺激内皮型一氧化氮合酶(eNOS),并抑制 Dahl 盐敏感型高血压(DS)大鼠左心室的氧化应激和凝集素样氧化低密度脂蛋白受体-1(LOX-1)通路。
从6周龄至左心室肥厚阶段(11周龄),给予Y-27632(每天3mg/kg)或赋形剂,持续5周。给予相同饮食的年龄匹配的Dahl盐抵抗(DR)大鼠作为对照组。
Y-27632显著改善了肥厚阶段左心室重量的增加。Y-27632抑制了肥厚阶段RhoA蛋白上调、Rho激酶基因表达和肌球蛋白轻链磷酸化。Y-27632抑制了DS大鼠中烟酰胺腺嘌呤二核苷酸磷酸(NAD(P)H)氧化酶p22phox、p47phox、gp91phox和LOX-1表达的增加。Y-27632降低了DS大鼠中蛋白激酶Cε和p65核因子-κB磷酸化的上调。相反,Y-27632上调了肥厚阶段下调的eNOS表达。Y-27632有效抑制了血管病变形成,如中层厚度和血管周围纤维化,并抑制了转化生长因子-β1、I型和III型胶原蛋白以及纤连蛋白基因表达。
抑制Rho激酶通路可能在对与eNOS和氧化应激-LOX-1通路相关的DS大鼠心血管重塑的心脏保护作用中起关键作用,并且可能至少是高血压伴心脏肥厚的一种潜在治疗策略。
