N-乙酰丝氨酰-天冬氨酰-赖氨酰-脯氨酸对醛固酮盐性高血压大鼠心脏和肾脏的抗纤维化作用
Antifibrotic effects of N-acetyl-seryl-aspartyl-Lysyl-proline on the heart and kidney in aldosterone-salt hypertensive rats.
作者信息
Peng H, Carretero O A, Raij L, Yang F, Kapke A, Rhaleb N E
机构信息
Hypertension and Vascular Research Division, Department of Biostatistics and Research Epidemiology, Henry Ford Hospital, Detroit, Michigan, USA.
出版信息
Hypertension. 2001 Feb;37(2 Pt 2):794-800. doi: 10.1161/01.hyp.37.2.794.
N-acetyl-seryl-aspartyl-lysyl-proline (Ac-SDKP) inhibits not only hematopoietic cell proliferation but also fibroblast proliferation and collagen synthesis in vitro. Ac-SDKP also prevents collagen deposition and cell proliferation in the left ventricle (LV) in rats with renovascular hypertension (renin dependent). However, it is not clear whether Ac-SDKP has similar effects in a model of renin-independent hypertension (aldosterone-salt). Using a hypertensive rat model of cardiac and renal fibrosis created by chronic elevation of circulating aldosterone (ALDO) levels, we examined the effect of Ac-SDKP on blood pressure, cardiac and renal fibrosis and hypertrophy, and proliferating cell nuclear antigen (PCNA) expression in the LV and left kidney. Uninephrectomized rats were divided into 4 groups: (1) controls that received tap water, (2) rats that received ALDO (0.75 microgram/h SC) and 1% NaCl/0.2% KCl in drinking water (ALDO-salt), (3) rats that received ALDO-salt plus Ac-SDKP 400 microgram. kg(-1). day(-1) SC, and (4) rats that received ALDO-salt plus Ac-SDKP 800 microgram. kg(-1). d(-1) SC. After 6 weeks of treatment, the ALDO-salt group was found to have significantly increased blood pressure with decreased body weight and plasma renin concentration (P<0.05), LV and renal hypertrophy as well as renal injury, significantly increased collagen content in both ventricles and kidney as well as increased collagen volume fraction in the LV (P<0.0001), and significantly increased interstitial and perivascular PCNA-positive cells in the LV and kidney (P<0.0001). Ac-SDKP at 800 microgram. kg(-1). d(-1) markedly prevented cardiac and renal fibrosis (P<0.005) without affecting blood pressure or organ hypertrophy. It also suppressed PCNA expression in the LV and kidney in a dose-dependent manner. We concluded that Ac-SDKP prevents increased collagen deposition and cell proliferation in the heart and kidney in ALDO-salt hypertensive rats. Because ACE inhibitors increase plasma and tissue Ac-SDKP and decrease cardiac and renal fibrosis, we speculate that Ac-SDKP may participate in the antifibrotic effect of ACE inhibitors.
N-乙酰丝氨酰-天冬氨酰-赖氨酰-脯氨酸(Ac-SDKP)不仅在体外能抑制造血细胞增殖,还能抑制成纤维细胞增殖及胶原蛋白合成。Ac-SDKP还可防止肾血管性高血压(肾素依赖性)大鼠左心室(LV)的胶原蛋白沉积和细胞增殖。然而,尚不清楚Ac-SDKP在肾素非依赖性高血压(醛固酮-盐)模型中是否具有类似作用。利用通过循环醛固酮(ALDO)水平长期升高建立的心脏和肾脏纤维化高血压大鼠模型,我们研究了Ac-SDKP对血压、心脏和肾脏纤维化及肥大,以及左心室和左肾中增殖细胞核抗原(PCNA)表达的影响。单侧肾切除的大鼠分为4组:(1)饮用自来水的对照组;(2)接受ALDO(0.75微克/小时,皮下注射)并饮用含1% NaCl/0.2% KCl水的大鼠(ALDO-盐组);(3)接受ALDO-盐加400微克·kg⁻¹·天⁻¹皮下注射Ac-SDKP的大鼠;(4)接受ALDO-盐加800微克·kg⁻¹·天⁻¹皮下注射Ac-SDKP的大鼠。治疗6周后,发现ALDO-盐组血压显著升高,体重和血浆肾素浓度降低(P<0.05),左心室和肾脏肥大以及肾损伤,两个心室和肾脏中的胶原蛋白含量显著增加,左心室中的胶原体积分数增加(P<0.0001),左心室和肾脏中间质和血管周围PCNA阳性细胞显著增加(P<0.0001)。800微克·kg⁻¹·天⁻¹的Ac-SDKP显著预防了心脏和肾脏纤维化(P<0.005),而不影响血压或器官肥大。它还以剂量依赖性方式抑制左心室和肾脏中PCNA的表达。我们得出结论,Ac-SDKP可防止ALDO-盐高血压大鼠心脏和肾脏中胶原蛋白沉积增加和细胞增殖。由于血管紧张素转换酶抑制剂可增加血浆和组织中的Ac-SDKP并减少心脏和肾脏纤维化,我们推测Ac-SDKP可能参与了血管紧张素转换酶抑制剂的抗纤维化作用。
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