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[益气养阴化瘀通络中药及其拆方对糖尿病模型大鼠nephrin的影响]

[Effects of Chinese materia medica of qi benefiting, yin nourishing, stasis removing, and collaterals dredging and their dissembled recipes on nephrin of diabetes mellitus model rats].

作者信息

Li Li-Li, Chen Zhi-Qiang, Wang Yue-Hua

机构信息

Institute of Integrated Traditional and Western Medicine, Hebei Medical University, Shijiazhuang.

出版信息

Zhongguo Zhong Xi Yi Jie He Za Zhi. 2012 Jul;32(7):960-4.

Abstract

OBJECTIVE

To observe the effects of Chinese materia medica (CMM) of qi benefiting, yin nourishing, stasis removing, and collaterals dredging (QBYNSRCD) and their dissembled recipes on nephrin of diabetes mellitus (DM) model rats.

METHODS

The DM model was induced by high fat diet combined with low dose STZ. Rats in the normal control group (abbreviated as Group N) and the model group (abbreviated as Group M) were administered with ultrapure water at corresponding volume by gastrogavage. Rats in the CMM of QBYNSRCD treatment group (abbreviated as Group YHT) were administered with CMM of QBYNSRCD, composed of milkvetch root, rehmannia root, danshen root, chuanxiong (2 packages each), solomonseal, earth worm, leech, and scorpion (1 package each), which was administered at 1.0 g/kg. Rats in the CMM of qi benefiting, yin nourishing, and stasis removing (QBYNSR) treatment group (abbreviated as Group YT) were administered with CMM of QBYNSR, composed of milkvetch root, rehmannia root, danshen root, chuanxiong (2 packages each), and solomonseal (1 package each), which was administered at 0. 92 g/kg. Rats in the CMM of qi benefiting, yin nourishing, and collaterals dredging (QBYNCD) treatment group (abbreviated as Group YT) were administered with CMM of QBYNCD, composed of milkvetch root, rehmannia root (2 packages each), solomonseal, earth worm, leech, and scorpion (1 package each), which was administered at 0.79 g/kg. The volume was set to 1 mL/100 g, once daily by gastrogavage, for total 32 weeks. Rats' body weight was measured. By the end of medication, urinary creatinine (UCr), 24-h urinary albumin (U-alb), and urinary nephrin (U-nephrin), fasting blood glucose (FBG), glycosylated hemoglobin (HbA1c), serum creatinine (SCr), and nephrin of kidney tissues homogenate (K-nephrin) were detected. The renal tissue sections were stained with Masson. The pathomorphological changes were observed.

RESULTS

The body weight of rats in Group N increased gradually. After modeling, the body weight of rats in Group M and all medicated groups obviously decreased. Compared with Group M, the decreased body weight was not obvious in all medicated groups, still showing statistical difference (P < 0.01). Compared with Group N, U-alb and U-nephrin in Group M significantly increased (P < 0.01) in a positive linear correlation (r = 0.941, P = 0.017). K-nephrin significantly decreased, and K-nephrin had a negative linear correlation with U-alb (r = -0. 987, P = 0.002). FBG, CCr, and HbA1c significantly increased (P < 0.01). Glomeruli were obviously enlarged under light microscope, with obviously increased extracellular matrix accumulation. Compared with Group M, corresponding indices were obviously improved ( P < 0.01) except FBG and HbA1c in Group YT. As for inter-group comparison among all medicated groups, the improvement of CCr was the best in Group YHT with statistical difference shown (P < 0.01). There was no statistical difference for the rest indices (P > 0.05). When compared with Group M, the hypertrophy of glomerulus was not so obvious in all medicated groups. Neither was extracellular matrix accumulation.

CONCLUSIONS

CMM of QBYNSRCD and dissembled recipes showed renal protection on DM model rats. One of its action pathways might be reducing the loss of nephrin, thus reducing U-alb.

摘要

目的

观察益气养阴、祛瘀通络中药及其拆方对糖尿病(DM)模型大鼠肾素的影响。

方法

采用高脂饮食联合低剂量链脲佐菌素诱导建立DM模型。正常对照组(简称N组)和模型组(简称M组)大鼠分别给予相应体积的超纯水灌胃。益气养阴、祛瘀通络中药治疗组(简称YHT组)大鼠给予益气养阴、祛瘀通络中药,其组成为黄芪、生地黄、丹参、川芎各2包,黄精、地龙、水蛭、全蝎各1包,按1.0 g/kg灌胃。益气养阴、祛瘀中药治疗组(简称YT组)大鼠给予益气养阴、祛瘀中药,其组成为黄芪、生地黄、丹参、川芎各2包,黄精1包,按0.92 g/kg灌胃。益气养阴、通络中药治疗组(简称YNCD组)大鼠给予益气养阴、通络中药,其组成为黄芪、生地黄各2包,黄精、地龙、水蛭、全蝎各1包,按0.79 g/kg灌胃。给药体积设定为1 mL/100 g,每日1次灌胃,共32周。测量大鼠体重。给药结束时,检测尿肌酐(UCr)、24小时尿白蛋白(U-alb)、尿肾素(U-nephrin)、空腹血糖(FBG)、糖化血红蛋白(HbA1c)、血清肌酐(SCr)及肾组织匀浆肾素(K-nephrin)。肾组织切片进行Masson染色,观察病理形态学变化。

结果

N组大鼠体重逐渐增加。造模后,M组及各用药组大鼠体重明显下降。与M组比较,各用药组大鼠体重下降不明显,但仍有统计学差异(P<0.01)。与N组比较,M组U-alb和U-nephrin显著升高(P<0.01),呈正线性相关(r=0.941,P=0.017)。K-nephrin显著降低,K-nephrin与U-alb呈负线性相关(r=-0.987,P=0.002)。FBG、CCr和HbA1c显著升高(P<0.01)。光镜下肾小球明显增大,细胞外基质积聚明显增加。与M组比较,除YT组FBG和HbA1c外,各用药组相应指标均明显改善(P<0.01)。各用药组间比较,YHT组CCr改善最佳,有统计学差异(P<0.01)。其余指标无统计学差异(P>0.05)。与M组比较,各用药组肾小球肥大不明显,细胞外基质积聚也不明显。

结论

益气养阴、祛瘀通络中药及其拆方对DM模型大鼠具有肾脏保护作用。其作用途径之一可能是减少肾素丢失,从而降低U-alb。

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