Therapeutic Effect of Arnebiae Radix Oil Ointment on Rat Pressure Ulcer Model and Its Mechanism

LIU Yu-feng; LI Dan; HUANG Mei; NAN Li-hong; XIE Qing-qing

doi:10.13422/j.cnki.syfjx.2017230122

您当前的位置：

首页 >

文章列表页 >

Therapeutic Effect of Arnebiae Radix Oil Ointment on Rat Pressure Ulcer Model and Its Mechanism

更新时间：2024-01-04

- Therapeutic Effect of Arnebiae Radix Oil Ointment on Rat Pressure Ulcer Model and Its Mechanism
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 23, Issue 23, Pages: 122-128(2017)
- 作者机构：
- 作者简介：
- 基金信息：
- DOI：10.13422/j.cnki.syfjx.2017230122
  CLC： R-332;R285.5
- Published：2017
- 稿件说明：
移动端阅览
LIU Yu-feng, LI Dan, HUANG Mei, et al. Therapeutic Effect of Arnebiae Radix Oil Ointment on Rat Pressure Ulcer Model and Its Mechanism[J]. Chinese journal of experimental traditional medical formulae, 2017, 23(23): 122-128.
DOI：

LIU Yu-feng, LI Dan, HUANG Mei, et al. Therapeutic Effect of Arnebiae Radix Oil Ointment on Rat Pressure Ulcer Model and Its Mechanism[J]. Chinese journal of experimental traditional medical formulae, 2017, 23(23): 122-128. DOI： 10.13422/j.cnki.syfjx.2017230122.

摘要

目的：观察紫草油膏对褥疮模型大鼠的治疗作用及可能的作用机制，为其临床推广应用提供一定的实验依据。方法：采用皮下植入铁片加磁铁的方法复制大鼠褥疮模型。将造模成功的大鼠随机分为模型组、阳性（消炎生肌膏）组、紫草油膏中、高剂量组和碘剂组。另设空白组和假手术组。于造模成功后次日开始外涂给药，每日1次。连续给药3 d后，肉眼观察受压部位皮肤形态学和颜色变化；光镜下观察受压部位皮肤组织病理学变化；免疫组化法检测核转录因子-κB p65（nuclear transcription factor-κB，NF-κB p65）表达水平；水溶性四唑盐法及微板法检测大鼠血清中超氧化物歧化酶（superoxide dismutase，SOD），丙二醛（malondialdehyde，MDA）的含量；酶联免疫吸附法（enzyme linked immunosorbent assay，ELISA）测定大鼠血清中白细胞介素-lα（interleukin-lα，IL-1α），肿瘤坏死因子-α（tumour necrosis factorα-α，TNF-α）的含量。结果：与空白组及假手术组比较，模型组大鼠受压部位发红不改变；病理观察到细胞排列紊乱，细胞间隙增宽，炎症细胞浸润等现象；血清中MDA，TNF-α，IL-1α及皮肤组织细胞核中NF-κB p65的含量明显升高（P<0.05，P<0.01），而血清中SOD的含量显著降低（P<0.01）。紫草油膏治疗3 d后，与模型组比较，受压部位皮肤组织红肿消退，状态明显好转；病理状态明显得到改善，炎症程度和数量均明显减轻或减少。紫草油膏中、高剂量组大鼠血清中SOD的含量明显高于模型组，而MDA的含量明显低于模型组（P<0.05，P<0.01）；紫草油膏高剂量组较模型组血清中TNF-α，IL-1α的含量显著降低（P<0.05），细胞核中NF-κB p65蛋白表达显著降低（P<0.05）。结论：紫草油膏对褥疮模型大鼠具有一定治疗作用，其机制与抑制细胞核中NF-κB p65的表达、降低大鼠血清中IL-lα，TNF-α，MDA的含量及增加SOD含量有关。

Abstract

Objective: To observe the therapeutic effect of Arnebiae Radix oil ointment (AROO) on a rat model of pressure ulcer (PU) and its possible mechanism

in order to provide the experimental evidence for clinical application. Method: Rats were randomly divided into seven groups

namely blank control group

sham group

model group

positive control group

middle-dose AROO group

high-dose AROO group and iodine group. The PU model was induced by applying magnets over irons that were implanted under the skin of rats except for blank control and sham group. AROO was applied the next day after modeling. Rats in blank control

sham group and model group were treated with normal saline

where as the other groups were given the corresponding medicines once a day. After three days of administration

the morphologic and color changes in skin were observed

and the histopathological changes in pressed skin tissues were observed under microscope. Nuclear transcription factor-κB p65(NF-κB p65) was detected by immunohistochemistry; WST-1 and microplate method were used to detect the superoxide dismutase (SOD) and malondialdehyde (MDA) in rat serum. And the levels of interleukin-lα (IL-lα) and tumor necrosis factorα-α (TNF-α) in rat serum were detected as well by enzyme linked immunosorbent assay (ELISA). Result: Compared with blank control and sham group

compressed skin parts of the rats in model group were red and swollen; and pathological observation showed that the cell lines were disordered

the cell gaps were widened

and the inflammatory cells were infiltrated. The levels of TNF-α

IL-1α and MDA in the serum and the expression of NF-κB p65 were significantly increased

while the level of SOD was reduced. After being treated with AROO for 3 days

the swelling in compressed tissues subsided

the pathological status was significantly improved

the inflammation was relieved

and the content of SOD in middle and high-dose groups was significantly higher than that of model group. However

the content of MDA was significantly lower than that of model group (P <0.05

P<0.01)

the levels of TNF-α and IL-1α in the serum of high-dose group were significantly lower than those in model group (P<0.05)

and the NF-κB p65 protein expression in high-dose group was significantly lower than model group (P<0.05). Conclusion: AROO has a therapeutic effect on rat PU model. Its mechanism is possibly related to the regulation of NF-κB p65 expression and the content of IL-1α

TNF-α

SOD and MDA in rat serum.

关键词

Keywords

references

Views

下载量

CSCD

Alert me when the article has been cited

提交

Tools

Publicity Resources

Anti-cerebral Ischemia/Reperfusion Mechanism of Baicalin in Rats

Exploring Mechanism of Kelong Capsules in Treatment of Benign Prostatic Hyperplasia Based on Nrf2 Pathway and Macrophage Activation

Zhenzhu Tiaozhi Capsules Reduce Renal Lipid Deposition and Inflammation in Mouse Model of Diabetic Kidney Disease via SCAP-SREBP-1c/NLRP3 Signaling Pathway

Multidimensional Analysis of Mechanisms of Nuciferine Against Cerebral Ischemia Based on Transcriptomic Data

Mechanism of Modified Danggui Shaoyaosan in Improving Inflammation and Apoptosis in Acne via Regulating JNK/p38 MAPK Pathway

Related Author

WANG Wen-juan

REN Huan-huan

HAN Ji-chun

WANG Bo

LI Peng

ZHENG Qiu-sheng

SONG Guanhui

FAN Danping

Related Institution

The First Clinical Medical College of Shaanxi University of Chinese Medicine

Experimental Research Center，China Academy of Chinese Medical Sciences

Beijing University of Chinese Medicine

Guangdong Metabolic Diseases Research Center of Integrated Chinese and Western Medicine， Guangdong Pharmaceutical University

Institute of Chinese Materia Medica，China Academy of Chinese Medical Sciences

AI问答

Postal code：100700
Tel：010-84076882 Email：syfjx_2010@188.com
Technical support is provided by Beijing Founder electronics co., LTD 京ICP备11006657号-10 京公网安备11010802024621
It is recommended to read the content of this site in Chrome&IE9+. Please switch to extreme mode in browser 360.
Cookies We use cookies to help provide and enhance our service and tailor content. By continuing, you agree to the use of cookies.

⁰