摘要
目的观察单用及联用吡哆胺、替米沙坦对自发性高血压大鼠(SHR)肾脏损害的影响。方法 20周龄雄性SHR随机分为4组(每组12只):高血压组(蒸馏水)、替米沙坦组[6mg/(kg·d)]、吡哆胺组[200mg/(kg·d)]、联合组[替米沙坦6mg/(kg·d)+吡哆胺200mg/(kg·d)],连续灌胃给药。WKY大鼠为正常对照组,蒸馏水2mL/d灌胃。实验干预16周,测量干预前后的尾动脉收缩压,测定干预后24h尿微量白蛋白含量(免疫散射比浊法)及血清晚期糖基化终末产物(AGE)浓度(ELISA法),观察肾组织光镜下(HE、Masson染色)和透射电镜下的形态学改变,Westernblot法检测肾皮质转化生长因子β(TGF-β)水平。结果与正常对照组比较,高血压组血清AGE[(6.7±0.4)比(5.5±0.4)mg/L]、24h尿微量白蛋白[(404.9±91.8)比(20.2±3.1)mg]、肾皮质TGF-β含量[(1.6±0.2)比(0.8±0.3)]较高(均P<0.01);与高血压组比较,替米沙坦组、吡哆胺组、联合组24h尿微量白蛋白、血清AGE、肾皮质TGF-β较低(均P<0.01);与替米沙坦组比较,吡哆胺组、联合组的血清AGE[(5.6±0.9)、(5.2±0.6)比(6.0±0.5)mg/L]较低(P<0.05);与吡哆胺组比较,替米沙坦组、联合组干预后16周收缩压[(99.8±11.7)、(97.0±10.3)比(195.4±20.7)mmHg]较低(P<0.01)。高血压组肾小球基底膜不规则增厚,足突融合,毛细血管管腔狭窄,肾间质纤维性物质明显增多。结论吡哆胺和替米沙坦均可改善高血压大鼠早期肾损害,减少尿微量白蛋白,改善肾组织超微结构变化。吡哆胺对肾损害的改善作用可能与抑制体内AGE生成有关。
Objective To investigate the effects of pyridoxamine and telmisartan on the renal damages in of spontaneously hypertensive rats (SHR). Methods SHR(male, 20 weeks of age) were randomly divided into 4 groups (n= 12) : hypertension control group(given distilled water), telmisartan group ( given 6 mg/kg telmisartan), pyridoxamine group(given 200 mg/kg pyridoxamine) and combined group(given 6 mg/kg telmisartan and 200 mg/kg pyridoxamine). Thirteen Wistar rats were served as controls, which were givengastric lavage with 2 mL of distilled water. This experiment was continued for 16 weeks. Tail systolic blood pressure (SBP) was measured be- fore and after the treatment. The levels of 24 h urinary albumin and serum advanced glycation end products(AGE) were determined by nephelometry and ELISA seperately. The kidney morphological changes were observed under light (H&E or Masson's trichrome) and transmission electron microscopy. Expression of transforming growth factor-13 (TGF-13} in the renal cortex was determined by Western blot. Results Compared with control group, the levels of serum AGE [(6.74±0.4) vs (5.5±0.4) mg/L], 24 h urinary albumin [(404. 9±91.8) vs (20.2±3.1)mg] and the expression of TGF-13 in renal cortex [(1.6 ± 0.2) vs (0.8± 0.3)] were significantly increased in hypertension control group (P〈0.01 ). And the levels of serum AGE, 24 h urinary albumin and the expression of TGF-13 in renal cortex were lower in telmisartan group, pyridoxamine group and combined group than in hypertension control group. Also the levels of serum AGE in pyridoxamine group (5.6±0.9) and combined group (5.2 ±0.6) were lower than those of telmisartan group (6.0±0.5)mg/L (P〈0.05). After 16 weeks, SBP in telmisartan group (99.8±11.7) mm Hg and combined group (97.0± 10.3)mm Hg were lower than that of pyridoxamine group (195.4± 20.7)ram Hg (P〈0.01). Histopathology showed irregular thickness of glomerulus, lumen occl
出处
《中华高血压杂志》
CAS
CSCD
北大核心
2013年第4期365-370,共6页
Chinese Journal of Hypertension
基金
福建省自然科学基金项目(2010J01127)
关键词
晚期糖基化终末产物
自发性高血压大鼠
肾损害
吡哆胺
Advanced glycation end-products
Spontaneously hypertensive rats
Renal damage
Pyridoxamine
