Diabetes and Cardiovascular Center, University of Missouri School of Medicine, Columbia, MO, USA.
Division of Endocrinology and Metabolism, Department of Medicine, University of Missouri-Columbia School of Medicine, D110, DC043.0 One Hospital Dr, Columbia, MO, 65212, USA.
Cardiovasc Diabetol. 2021 Apr 21;20(1):80. doi: 10.1186/s12933-021-01270-1.
Cardiac diastolic dysfunction (DD) and arterial stiffness are early manifestations of obesity-associated prediabetes, and both serve as risk factors for the development of heart failure with preserved ejection fraction (HFpEF). Since the incidence of DD and arterial stiffness are increasing worldwide due to exponential growth in obesity, an effective treatment is urgently needed to blunt their development and progression. Here we investigated whether the combination of an inhibitor of neprilysin (sacubitril), a natriuretic peptide-degrading enzyme, and an angiotensin II type 1 receptor blocker (valsartan), suppresses DD and arterial stiffness in an animal model of prediabetes more effectively than valsartan monotherapy.
Sixteen-week-old male Zucker Obese rats (ZO; n = 64) were assigned randomly to 4 different groups: Group 1: saline control (ZOC); Group 2: sacubitril/valsartan (sac/val; 68 mg•kg•day; ZOSV); Group 3: valsartan (31 mg•kg•day; ZOV) and Group 4: hydralazine, an anti-hypertensive drug (30 mg•kg•day; ZOH). Six Zucker Lean (ZL) rats that received saline only (Group 5) served as lean controls (ZLC). Drugs were administered daily for 10 weeks by oral gavage.
Sac/val improved echocardiographic parameters of impaired left ventricular (LV) stiffness in untreated ZO rats, without altering the amount of food consumed or body weight gained. In addition to improving DD, sac/val decreased aortic stiffness and reversed impairment in nitric oxide-induced vascular relaxation in ZO rats. However, sac/val had no impact on LV hypertrophy. Notably, sac/val was more effective than val in ameliorating DD. Although, hydralazine was as effective as sac/val in improving these parameters, it adversely affected LV mass index. Further, cytokine array revealed distinct effects of sac/val, including marked suppression of Notch-1 by both valsartan and sac/val, suggesting that cardiovascular protection afforded by both share some common mechanisms; however, sac/val, but not val, increased IL-4, which is increasingly recognized for its cardiovascular protection, possibly contributing, in part, to more favorable effects of sac/val over val alone in improving obesity-associated DD.
These studies suggest that sac/val is superior to val in reversing obesity-associated DD. It is an effective drug combination to blunt progression of asymptomatic DD and vascular stiffness to HFpEF development in a preclinical model of obesity-associated prediabetes.
心脏舒张功能障碍(DD)和动脉僵硬是肥胖相关糖尿病前期的早期表现,两者都是射血分数保留型心力衰竭(HFpEF)发展的危险因素。由于肥胖的指数级增长,DD 和动脉僵硬的发病率在全球范围内不断上升,因此迫切需要有效的治疗方法来抑制其发展和进展。在这里,我们研究了一种抑制脑啡肽酶(奈普利肽)、利钠肽降解酶和血管紧张素 II 型 1 型受体阻滞剂(缬沙坦)的组合是否比缬沙坦单药治疗更有效地抑制糖尿病前期动物模型中的 DD 和动脉僵硬。
16 周龄雄性 Zucker 肥胖大鼠(ZO;n=64)随机分为 4 个不同组:第 1 组:生理盐水对照(ZOC);第 2 组:沙库比曲缬沙坦(sac/val;68mg·kg·day;ZOSV);第 3 组:缬沙坦(31mg·kg·day;ZOV)和第 4 组:肼屈嗪,一种抗高血压药物(30mg·kg·day;ZOH)。6 只仅接受生理盐水的 Zucker 瘦鼠(ZL)作为瘦鼠对照(ZLC)。通过口服灌胃每天给予药物治疗 10 周。
沙库比曲缬沙坦改善了未经治疗的 ZO 大鼠左心室(LV)僵硬度受损的超声心动图参数,而不改变食物摄入量或体重增加。除了改善 DD 外,沙库比曲缬沙坦还降低了主动脉僵硬度并逆转了 ZO 大鼠中一氧化氮诱导的血管舒张受损。然而,沙库比曲缬沙坦对 LV 肥大没有影响。值得注意的是,沙库比曲缬沙坦在改善 DD 方面比缬沙坦更有效。尽管肼屈嗪在改善这些参数方面与沙库比曲缬沙坦同样有效,但它对 LV 质量指数有不利影响。此外,细胞因子阵列显示沙库比曲缬沙坦具有独特的作用,包括缬沙坦和沙库比曲缬沙坦均显著抑制 Notch-1,表明两者提供的心血管保护具有一些共同的机制;然而,沙库比曲缬沙坦而非缬沙坦增加了 IL-4,IL-4 越来越被认为具有心血管保护作用,这可能部分导致沙库比曲缬沙坦在改善肥胖相关 DD 方面优于缬沙坦单药治疗。
这些研究表明,沙库比曲缬沙坦在逆转肥胖相关 DD 方面优于缬沙坦。它是一种有效的药物组合,可在肥胖相关糖尿病前期的临床前模型中抑制无症状 DD 和血管僵硬向 HFpEF 发展。
Zotero 插件
