Effects of Bicyclol on Expression of NF-B and PAI-1 in Rats with Uniliteral Ureteral Obstruction

LIU Yan-hong; HAN Zi-ming

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Effects of Bicyclol on Expression of NF-B and PAI-1 in Rats with Uniliteral Ureteral Obstruction

更新时间：2024-01-04

- Effects of Bicyclol on Expression of NF-B and PAI-1 in Rats with Uniliteral Ureteral Obstruction
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 17, Issue 3, Pages: 205-209(2011)
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- Published：2011
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LIU Yan-hong, HAN Zi-ming. Effects of Bicyclol on Expression of NF-B and PAI-1 in Rats with Uniliteral Ureteral Obstruction[J]. Chinese journal of experimental traditional medical formulae, 2011, 17(3): 205-209.
DOI：

LIU Yan-hong, HAN Zi-ming. Effects of Bicyclol on Expression of NF-B and PAI-1 in Rats with Uniliteral Ureteral Obstruction[J]. Chinese journal of experimental traditional medical formulae, 2011, 17(3): 205-209. DOI：

摘要

目的: 通过双环醇干预单侧输尿管梗阻(uniliteral ureteral obstruction

UUO)模型大鼠

动态观察核转录因子-κB(nuclear factor-κB

NF-κB)、纤溶酶原激活物抑制剂-1(plasminogen activator inhibitor-1

PAI-1)和PAI-1 mRNA在梗阻侧肾组织间质中的表达

探讨双环醇延缓肾间质纤维化的可能机制。方法: 采用UUO致肾间质纤维化大鼠模型

将81只大鼠随机分假手术组、模型组、治疗组。治疗组于术后第1天开始给予双环醇200 mg ·kg-1灌胃;假手术组和模型组给予等量生理盐水灌胃。在术后7

21d每组各取9只大鼠处死

取梗阻侧肾组织行HE及Masson染色

观察肾脏病理学变化。用免疫组化方法检测肾组织NF-κB

PAI-1蛋白的表达。RT-PCR法检测各组肾组织PAI-1 mRNA的表达水平。结果: 模型组7

21 d肾间质纤维化的相对面积分别为(13.03±0.66)%

(25.76±1.47)%

(53.16±2.45)%

治疗组分别为(9.63±0.58)%

(16.84±0.83)%

(33.59±1.61)%

治疗组较模型组肾间质纤维化的相对面积明显降低(P<0.05)。7

21 d模型组肾组织NF-κB的表达分别为(11.73±0.42)%

(22.56±0.69)%

(36.27±1.14)%

而治疗组分别为(5.67±0.42)%

(10.79±0.37)%

(26.62±0.23)%;模型组肾组织PAI-1蛋白的表达分别为(7.29±0.23)%

(12.32±0.20)%

(18.36±0.19)%

治疗组分别为(4.26±0.14)%

(7.69±0.13)%

(13.35±0.21)%;肾组织PAI-1 mRNA在模型组的表达分别为(1.17±0.10)

(2.29±0.07)

(3.33±0.10)

而治疗组的表达分别为(0.32±0.03)

(1.18±0.05)

(2.06±0.40)

治疗组肾组织NF-κB

PAI-1蛋白和mRNA的表达均较模型组减少(P均<0.05)。结论: 双环醇能够减轻UUO所致的肾间质损伤及纤维化的程度。其作用机制可能是通过下调NF-κB

PAI-1的表达

从而抑制肾间质纤维化。

Abstract

Objective: To observe the expression of nuclear factor-κB (NF-κB)and plasminogen activator inhibitor-1(PAI-1) of the renal interstitial in rat unilateral ureteral obstruction (UUO) model and the renoprotective effect of bicyclol

and then to explore the mechanisms. Method: Renal interstitial fibrosis rat model was produced by unilateral ureteral obstruction

eighty-one rats were randomly assigned to shame operation group

UUO model group and bicyclol-treated group. After operations rats in bicyclol-treated group were intregastric administration(ia) at bicyclol 200 mg ·kg-1 once a day until rats were killed. Rats in sham-operated group and UUO model group were intragastric administrated at identical voluminal normal saline. In each group

nine rats were chosen randomly to be killed at the 7

14 and 21 d after operation for histological examination of kidney tissue.Renal tissues were examined by HE and Masson stain. The expression of NF-κB and PAI-1 were detected by immunohistochemical staining

and the expression of PAI-1-mRNA in renal tissue was determined by reverse transcription-polymerase chain reaction (RT-PCR). Result: The relative area of renal interstitial fibrosis of UUO model group at 7

14 and 21 d was (13.03±0.66)%

(25.76±1.47)%

and (53.16±2.45)%respectively. And that of bicyclol-treated group was (9.63±0.58)%

(16.84±0.83)% and(33.59±1.61)% respectively. Compared with UUO model group

fibrotic area of bicyclol-treated group was decreased markedly(P<0.05

respectively). The protein expression of NF-κB of UUO model group at 7

14 and 21 d was (11.73±0.42)%

(22.56±0.69)% and(36.27±1.14)% respectively

but that of bicyclol-treated group was (5.67±0.42)%

(10.79±0.37)% and(26.62±0.23)% respectively. The protein expression of PAI-1 of UUO model group at 7

14 and 21 d was (7.29±0.23)%

(12.32±0.20)% and (18.36±0.19)% respectively

but that of bicyclol-treated group was (4.26±0.14)%

(7.69±0.13)% and (13.35±0.21)% respectively. The expression of PAI-1 mRNA of UUO model group at 7

14 and 21 d was (1.17±0.10)

(2.29±0.07) and (3.33±0.10) respectively

but that of bicyclol-treated group was (0.32±0.03)

(1.18±0.05)and(2.06±0.40) respectively. Compared with UUO model group

the expression of NF-κB

PAI-1 protein and PAI-1 mRNA of bicyclol-treated group was decreased markedly(P<0.05

respectively). Conclusion: Bicyclol can alleviate the degree of renal interstitial fibrosis and protect renal function

down-regulates the expression of PAI-1 and NF-κB

thus blocking the renal fibrosis.

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