[1]胡顺金吴幽婉杨丽
王东高磊
金华曹媛茹
王.糖肾康对 DN模型大鼠血清 MCP-1和 ICAM-1水平的影响[J].陕西中医药大学学报,2018,(01):083-87.[doi:10.13424/j.cnki.jsctcm.2018.01.027]
Hu Shunjin,Wu Youwan,Yang Li,et al.The Effect of Tangshenkang on MCP - 1 and ICAM - 1 Levels
in the Serum of DN Rat Models[J].Journal of Shaanxi University of Traditional Chinese Medicine,2018,(01):083-87.[doi:10.13424/j.cnki.jsctcm.2018.01.027]
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糖肾康对 DN模型大鼠血清 MCP-1和 ICAM-1水平的影响()
《陕西中医药大学学报》[ISSN:2096-1340/CN:61-1501/R]
- 卷:
-
- 期数:
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2018年01期
- 页码:
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083-87
- 栏目:
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实验研究
- 出版日期:
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2018-01-10
文章信息/Info
- Title:
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The Effect of Tangshenkang on MCP - 1 and ICAM - 1 Levels
in the Serum of DN Rat Models
- 文章编号:
-
2096-1340(2018)01-0083-05
- 作者:
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胡顺金1吴幽婉2杨丽
2
王东1高磊
2
金华1曹媛茹
2
王
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1. 安徽中医药大学第一附属医院,安徽 合肥 230031; 2. 安徽中医药大学研究生院,安徽 合肥 230038
- Author(s):
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Hu Shunjin1; Wu Youwan2; Yang Li2; Wang Dong1; Gao Lei2; Jin Hua1; Cao Yuanru2; Wang Yiping1
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1. The First Affiliated Hospital of Anhui University of Chinese Medicine,Anhui 230031,China;
2. Postgraduate School of Anhui University of Chinese Medicine,Anhui 230038,China
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- 关键词:
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糖肾康; 糖尿病肾病; 单核细胞趋化性蛋白 - 1; 细胞间粘附分子 - 1
- Keywords:
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Tangshenkang; DN; MCP - 1; ICAM - 1
- 分类号:
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R285. 5
- DOI:
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10.13424/j.cnki.jsctcm.2018.01.027
- 文献标志码:
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A
- 摘要:
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观察糖肾康对糖尿病肾病( DN) 大鼠血清中单核细胞趋化性蛋白 - 1( monocytechemotaticpro-
tein - 1,MCP - 1) 、细胞间粘附分子 - 1 ( intercellularcelladhesionmolecule - 1,ICAM - 1) 的影响,探讨糖肾康防治
DN 模型大鼠的作用机制。方法 将 40 只 SD 大鼠随机分为正常组( n = 8) 和造模组( n = 32) 。以三联法( 手术 +
高糖高脂饮食 + 链脲佐菌素) 诱导产生 DN 大鼠模型,造模过程中死亡 5 只,余下 27 只模型大鼠随机分为模型
组( n = 9) 、贝那普利组( n = 9) 和糖肾康组( n = 9) 。糖肾康组按 0. 8g/100g·d 灌胃,贝那普利组按 0. 15mg/100g
·d 灌胃,正常组及模型组给予等量温水灌胃,连续灌胃给药 8 周。观察各组大鼠尿白蛋白/尿肌酐( ACR) 、肾
脏组织病理及血清 MCP - 1、ICAM - 1 水平变化。结果 糖肾康可消减 DN 模型大鼠的 ACR 水平( P < 0. 01) ,改
善肾脏病理形态损害。模型组、贝那普利组和糖肾康组血清 MCP - 1、ICAM - 1 水平均高于正常组( P < 0. 01) ;
与模型组比较,治疗后贝那普利组与糖肾康组血清 MCP - 1、ICAM - 1 水平明显降低( P < 0. 01) ,糖肾康组和贝
那普利组比较无显著性差异( P > 0. 05) 。结论 糖肾康可有效减少 DN 模型大鼠尿蛋白,减轻肾脏病理形态损
害,其机制可能与降低血清 MCP - 1、ICAM - 1 水平,抑制肾脏免疫炎症反应有关。
- Abstract:
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To observe the effect of Tangshenkang on MCP - 1 and ICAM - 1levels in the serum of DN
rat models,and study its prevention and treatment mechanism. Method: 40 SD rats were randomly divided into normal
group( n = 8) and model group( n = 32) . DN rat models were induced by triple therapy ( operation + high - glucose and
high - fat diet + streptozotocin) . Five rats died during the modeling,and the remaining 27 rats were randomly dividedinto model group ( n = 9) Benazepril group ( n = 9) and Tangshenkang group ( n = 9) . The rats in Tangshenkang
group were given gavage at a dosage of 0. 8g / 100g · d,the benazepril group was gavaged at 0. 15mg / 100g · d,the
rats in the normal group and the model group were given the same amount of warm water for gavage,all for 8 weeks. Uri-
nary albumin / urinary creatinine ( ACR) ,renal histopathology and changes of serum levels of MCP - 1 and ICAM - 1 in
rats were observed. Result: Tangshenkang can reduce the ACR level in DN rat models ( P < 0. 01) ,and improve renal
pathological damage. The levels of serum MCP - 1 and ICAM - 1 in model group,benazepril group and Tangshenkang
group were higher than those in normal group ( P < 0. 01) . Compared with model group,Serum levels of MCP - 1 and
ICAM - 1 in Tangshenkang group and Benazepril group were significantly decreased ( P < 0. 01) ,but there was no signif-
icant difference between the two groups ( P > 0. 05) . Conclusion: Tangshenkang can effectively reduce urinary protein in
DN rat models and reduce renal pathological damage,which may be related to the decrease of serum MCP - 1,ICAM - 1
levels and the inhibition of renal immune inflammation.
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备注/Memo
- 备注/Memo:
-
收稿日期: 2017 - 09 - 20 编辑:文颖娟
更新日期/Last Update:
2019-12-10