Mechanism of Dahuang Mudantang in Improving Pancreatic Injury in Rats with Acute Pancreatitis of Dampness-heat in Large Intestine Syndrome Based on Network Pharmacology and Experimental Verification

WANG Qiong; WANG Yongfeng; ZHANG Yanying; SONG Bing; GUO Chao; LIU Xinhong; BAI Min; WANG Zhandong; WEN Linlin; ZHAO Hongzhang

doi:10.13422/j.cnki.syfjx.20231036

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Mechanism of Dahuang Mudantang in Improving Pancreatic Injury in Rats with Acute Pancreatitis of Dampness-heat in Large Intestine Syndrome Based on Network Pharmacology and Experimental Verification

更新时间：2023-09-21

- Mechanism of Dahuang Mudantang in Improving Pancreatic Injury in Rats with Acute Pancreatitis of Dampness-heat in Large Intestine Syndrome Based on Network Pharmacology and Experimental Verification
  增强出版
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 29, Issue 20, Pages: 61-68(2023)
- 作者机构：
  
  1.甘肃中医药大学，兰州 730000
  2.甘肃省实验动物行业技术中心，兰州 730000
  3.甘肃农业大学，兰州 730000
- 作者简介：
- 基金信息：
- DOI：10.13422/j.cnki.syfjx.20231036
  CLC： R2-0;R33;R318.14;R576;R365.4
- Published：20 October 2023，
  
  Published Online：04 August 2023，
  
  Received：14 April 2023，
- 稿件说明：
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王琼,汪永锋,张延英等.基于网络药理学和实验验证探讨大黄牡丹汤改善大肠湿热型急性胰腺炎大鼠胰腺损伤的机制[J].中国实验方剂学杂志,2023,29(20):61-68.

WANG Qiong,WANG Yongfeng,ZHANG Yanying,et al.Mechanism of Dahuang Mudantang in Improving Pancreatic Injury in Rats with Acute Pancreatitis of Dampness-heat in Large Intestine Syndrome Based on Network Pharmacology and Experimental Verification[J].Chinese Journal of Experimental Traditional Medical Formulae,2023,29(20):61-68.
王琼,汪永锋,张延英等.基于网络药理学和实验验证探讨大黄牡丹汤改善大肠湿热型急性胰腺炎大鼠胰腺损伤的机制[J].中国实验方剂学杂志,2023,29(20):61-68. DOI： 10.13422/j.cnki.syfjx.20231036.

WANG Qiong,WANG Yongfeng,ZHANG Yanying,et al.Mechanism of Dahuang Mudantang in Improving Pancreatic Injury in Rats with Acute Pancreatitis of Dampness-heat in Large Intestine Syndrome Based on Network Pharmacology and Experimental Verification[J].Chinese Journal of Experimental Traditional Medical Formulae,2023,29(20):61-68. DOI： 10.13422/j.cnki.syfjx.20231036.

摘要

目的

揭示大黄牡丹汤对大肠湿热型急性胰腺炎大鼠胰腺损伤的干预作用，并结合网络药理学探讨其可能机制。

方法

随机将96只SPF级Wistar大鼠分为6组，空白组、模型组、大黄牡丹汤低、中、高剂量组（3.5、7、14 g·kg

-1

）、清胰利胆颗粒组（3 g·kg

-1

）每组16只。除空白组外，其余各组大鼠采用“高温高湿环境+高糖高脂饮食+5%牛磺胆酸钠逆行胰胆管注射法”建立大肠湿热型急性胰腺炎（AP）大鼠模型。空白组、模型组大鼠给予等体积蒸馏水灌胃，治疗组于造模前1 h、造模后12、24 h分别给药，末次给药1 h后采集样本。观察大鼠一般情况；评价大肠湿热型模型；采用生化法检测血清淀粉酶（AMS）、C反应蛋白（CRP）含量情况；苏木素-伊红（HE）染色观察胰腺组织病理形态；采用网络药理学预测大黄牡丹汤干预急性胰腺炎的可能靶点，并采用分子生物学技术验证相关靶点。

结果

与空白组比较，模型组大鼠精神萎靡、毛发杂乱且无光泽、粪便软黏、黄而恶臭、肛温升高并伴有弓背扭体反应，血清中AMS、CRP含量明显升高（

0.05），光镜下可见胰管走形异常、小叶间隙紊乱及炎症细胞浸润，腺泡细胞水肿、充血、坏死等病理改变；与模型组比较，各治疗组大鼠一般生存状况有不同程度改善、扭体反应减轻、粪便软黏、黄而恶臭明显改善，胰腺组织水肿、坏死程度减轻，血清中AMS、CRP含量降低（

0.05），以大黄牡丹汤高剂量组效果最明显（

0.05）。网络药理学预测结果表明常春藤皂苷元、

-谷甾醇、槲皮素是与疾病靶点连接最为广泛的活性化合物，而蛋白质-蛋白质相互作用（PPI）发现蛋白激酶B（Akt）、肿瘤蛋白P53（TP53）、肿瘤坏死因子（TNF）、白细胞介素-6（IL-6）、转录激活因子（JUN）、血管内皮生长因子

（VEGF

）、白细胞介素-1

（IL-1

）、血管内皮细胞黏附分子1（VCAM1）是“药物-疾病”中较为关键靶点，京都基因与基因组百科全书（KEGG）富集发现丝裂原活化蛋白激酶（MAPK）信号通路的响应可能是大黄牡丹汤干预急性胰腺炎的核心机制。分子生物学检测表明与空白组比较，模型组小鼠胰腺组织中TNF-

、IL-6、VCAM-1含量明显上升（

0.05），丝裂原活化蛋白激酶p38（p38 MAPK）、蛋白激酶2（MK2）、人组织抗原R（HUR）基因蛋白表达水平明显升高（

0.05）；与模型组比较，各治疗组大鼠胰腺组织中TNF-

、IL-6、VCAM-1含量下降（

0.05），p38 MAPK、MK2、HUR基因蛋白表达水平均降低，以大黄牡丹汤高剂量组效果最明显（

0.05）。

结论

大黄牡丹汤激活并调控p38 MAPK/MK2/HUR信号通路进而抑制炎症因子释放，最终改善胰腺损伤。

Abstract

Objective

To reveal the intervention effect of Dahuang Mudantang on pancreatic injury in rats with acute pancreatitis （AP） of dampness-heat in large intestine syndrome and explore its possible mechanism based on network pharmacology.

Method

Ninety-six SPF-grade Wistar rats were randomly divided into the following six groups： a blank group， a model group， low-， medium-， and high-dose Dahuang Mudantang groups （3.5， 7， and 14 g·kg

-1

）， and a Qingyi Lidan granules group （3 g·kg

-1

）， with 16 rats in each group. The AP model of dampness-heat in large intestine syndrome was induced in rats except for those in the blank group by "high-temperature and high-humidity environment + high-sugar and high-fat diet + retrograde injection of 5% sodium taurocholate into the pancreaticobiliary duct". The blank and model groups received equal volumes of distilled water by gavage， while the treatment groups were administered Dahuang Mudantang or Qingyi Lidan granules 1 hour before modeling， and 12 and 24 hours after modeling. Samples were collected 1 hour after the last administration. The general conditions of the rats were observed. The AP model of dampness-heat in large intestine syndrome was evaluated. Serum amylase （AMS） and C-reactive protein （CRP） levels were determined using biochemical methods. Pancreatic tissue morphology was observed using hematoxylin-eosin （HE） staining. Network pharmacology was employed to predict potential targets of Dahuang Mudantang in the intervention in AP， and molecular biology technique was used to verify relevant targets.

Result

Compared with the blank group， the model group exhibited lethargy， unkempt fur， loose and foul-smelling stools， elevated anal temperature with arching and twisting reactions， significantly increased serum levels of AMS and CRP （

0.05）， abnormal pancreatic ductules， disordered interlobular spaces， and inflammatory cell infiltration in histopathological examination， as well as pathological changes including pancreatic acinar cell swelling， congestion， and necrosis. Compared with the model group， the treatment groups showed varying degrees of improvement in general survival conditions， reduced twisting reactions， visibly improved stool characteristics， reduced pancreatic tissue edema and necrosis， decreased serum AMS and CRP levels （

0.05）， with the high-dose Dahuang Mudantang group showing the most pronounced effects （

0.05）. Network pharmacology prediction indicated that hederagenin，

-sitosterol， and quercetin were the most widely connected active compounds with disease targets. Protein-protein interaction （PPI） network analysis revealed that protein kinase B （Akt）， tumor protein P53 （TP53）， tumor necrosis factor （TNF）， interleukin-6 （IL-6）， transcription factor （JUN）， vascular endothelial growth factor

（VEGF

）， interleukin-1

（IL-1

）， and vascular cell adhesion molecule-1 （VCAM1） were key targets in the "drug-disease" interaction. KEGG enrichment analysis suggested that the response of the mitogen activated protein kinase （MAPK） signaling pathway might be a core mechanism for DHMDT in the intervention in AP. Molecular biology analysis showed that compared with the blank group， the model group had significantly increased levels of TNF-

， IL-6， and VCAM-1 in pancreatic tissue （

0.05）， as well as significantly elevated expression levels of p38 mitogen-activated protein kinase （p38 MAPK）， mitogen-activated protein kinase-activated protein kinase 2 （MK2）， and human antigen R （HUR） genes and proteins （

0.05）. Compared with the model group， the treatment groups exhibited decreased levels of TNF-

， IL-6， and VCAM-1 in pancreatic tissue （

0.05）， reduced expression levels of p38 MAPK， MK2， and HUR genes and proteins， with the high-dose Dahuang Mudantang group showing the most pronounced effects （

0.05）.

Conclusion

Dahuang Mudantang activates and regulates the p38 MAPK/MK2/HUR signaling pathway to suppress the release of inflammatory factors， thereby improving pancreatic injury.

关键词

急性胰腺炎大肠湿热型大黄牡丹汤丝裂原活化蛋白激酶p38蛋白激酶-2人组织抗原R

Keywords

acute pancreatitisdampness-heat in large intestine syndromeDahuang Mudantangp38 mitogen-activated protein kinaseprotein kinase-2human tissue antigen

references

IANNUZZI J P，KING J A，LEONG J H，et al.Global incidence of acute pancreatitis is increasing over time： A systematic review and Meta-analysis［J］.Gastroenterology，2022，162（1）：122-134.

GREENBERG J A，HSU J，BAWAZEER M，et al.Clinical practice guideline：Management of acute pancreatitis［J］.Can J Surg，2016，59（2）：128-140.

卓玉珍，崔立华，李彩霞，等.中药复方治疗急性胰腺炎作用机制研究进展［J］.中国中西医结合外科杂志，2019，25（3）：394-398.

庞克斌，刘军昌，李晓光.大黄牡丹汤灌肠对重症急性胰腺炎患者炎症反应及微循环的影响［J］.贵州医药，2019，43（4）：605-607.

宋冰，辜吉秀，汪永锋，等.大黄牡丹汤调控HMGB1/RAGE/NF-κB信号通路干预急性胰腺炎模型大鼠的机制［J］.畜牧兽医学报，2021，52（11）：3260-3269.

WANG C， HOCKERMAN S， JACOBSEN E J， et al. Selective inhibition of the p38 MAPK-MK2 axis inhibits inflammatory cues including inflammasome priming signals［J］.J Exp Med，2018，215（5）：1315-1325.

宋冰，汪永锋，余四九，等.基于TLR4/MyD88信号通路探讨大黄牡丹汤对急性胰腺炎大鼠模型的保护作用［J］.中国实验动物学报，2021，29（1）：17-26.

郑凤萍，罗巨利，王爱华.清热燥湿方保留灌肠对大肠湿热型溃疡性结肠炎大鼠模型Th1/Th2的影响［J］.中外医学研究，2019，17（27）：181-182.

陈阳，崔波，范燕豪，等.葛根芩连汤中各成分在正常与大肠湿热证模型大鼠的肠吸收差异研究［J］.中国中药杂志，2020，45（1）：169-178.

文林林，汪永锋，白敏，等.基于HMGB1/RAGE/NF-κB信号通路探讨大黄牡丹汤对急性胰腺炎肠损伤大鼠的干预作用及机制［J］.中国实验方剂学杂志，2023，29（19）：1-8.

孙银凤，杨丹，白敏，等.大黄牡丹汤对急性胰腺炎大鼠肝损伤的保护作用［J］.中国实验动物学报，2022，30（2）：169-176.

国家中医药管理局.中医病证诊断疗效标准［M］.南京：南京大学出版社，1994：67.

曹思齐，王凤仪，汤胜男，等.芍药汤对大肠湿热型溃疡性结肠炎大鼠结肠组织中CD14，FADD，Caspase-8表达的影响［J］.中国实验方剂学杂志，2021，27（5）：1-7.

王瑞琼，吴国泰，杨志军，等.郁金散对抗生素相关性大肠湿热证大鼠肠黏膜屏障损伤的修复作用［J］.中国现代应用药学，2018，35（4）：529-536.

李仪奎.中药药理实验方法学［M］. 上海：上海科学技术出版社， 2006： 1070-1075.

肖懿，冯志乔，张桂贤，等.血必净注射液调节线粒体N-甲酰肽/NLRP3炎症通路对重症急性胰腺炎大鼠模型的治疗机制［J］.中国实验方剂学杂志，2022，28（7）：88-94.

戚亚婷，张玉峰，张依，等. 急性胰腺炎中医治疗研究进展［J］. 中国中医药现代远程教育， 2020， 18（24）： 145-147.

杨丹，孙银凤，白敏，等.基于PI3K/Akt信号通路的大黄牡丹汤对急性胰腺炎大鼠肺组织细胞凋亡及炎症反应的影响［J］.中国中医药信息杂志，2022，29（7）：73-79.

朱素华，张曼，徐圣秋.槲皮素对糖尿病视网膜病变小鼠氧化应激损伤和炎症反应的影响［J］.药学与临床研究，2023，31（1）：48-52.

王林. 常春藤皂苷元通过调控NF-κB/NLRP3炎性小体缓解脂多糖诱导急性肺损伤的作用机制［D］.沈阳：中国医科大学， 2022.

刘馨璐. β-谷甾醇缓解奶牛乳腺上皮细胞炎症损伤和对乳脂乳蛋白合成相关基因表达影响的研究［D］.长春：吉林大学， 2022.

文林林，刘馨鸿，张延英，等.牛月黄胆酸钠诱导大鼠急性胰腺炎肺肠损伤模型制备方法的研究［J］.中国临床药理学杂志，2023，39（6）：873-877.

王迪迪，刘秋圆，胡翠，等.急性胰腺炎患者血浆内皮细胞微粒水平的改变及其形成机制［J］.临床肝胆病杂志，2022，38（9）：2099-2105.

PIAO X，ZOU Y，SUI X，et al.Hydrostatin-SN10 ameliorates pancreatitis-induced lung injury by affecting IL-6-induced JAK2/STAT3-associated inflammation and oxidative stress［J］.Oxid Med Cell Longev，2019，2019：9659757.

WANG T，TIAN J，JIN Y.VCAM1 expression in the myocardium is associated with the risk of heart failure and immune cell infiltration in myocardium［J］.Sci Rep，2021，11（1）：19488.

WANG J，XU Y，JING H，et al.RORγt inhibitor SR1001 alleviates acute pancreatitis by suppressing pancreatic IL-17-producing Th17 and γδ-T cells in mice with ceruletide-induced pancreatitis［J］.Basic Clin Pharmacol Toxicol，2021，129（5）：357-368.

HUANG H，WANG M，GUO Z，et al.Rutaecarpine alleviates acute pancreatitis in mice and AR42J cells by suppressing the MAPK and NF-κB signaling pathways via calcitonin gene-related peptide［J］.Phytother Res，2021，35（11）：6472-6485.

甘苡榕，桂雄斌，俞渊，等.大黄灵仙方调控TAK1与TRAF6相互作用及共定位对胆管细胞炎症反应的影响［J］.中国实验方剂学杂志，2022，28（6）：92-99.

MA N，TENG X，ZHENG Q，et al.The regulatory mechanism of p38/MAPK in the chondrogenic differentiation from bone marrow mesenchymal stem cells［J］.J Orthop Surg Res，2019，14（1）：434.

BEAMER E，CORRêA S.The p38（MAPK）-MK2 signaling axis as a critical link between inflammation and synaptic transmission［J］.Front Cell Dev Biol，2021，9：635636.

LIU X，WU T，CHI P.Inhibition of MK2 shows promise for preventing postoperative ileus in mice［J］.J Surg Res，2013，185（1）：102-112.

SRIKANTAN S，GOROSPE M.HuR function in disease［J］.Front Biosci （Landmark Ed），2012，17（1）：189-205.

LAI Y，TANG H，ZHANG X，et al.Trimethylamine-N-Oxide aggravates kidney injury via activation of p38/MAPK signaling and upregulation of HuR［J］.Kidney Blood Press Res，2022，47（1）：61-71.

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