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中国中医科学院 中药研究所,北京 100700
张依,在读博士,从事中药药理学研究,E-mail:dr_zhangyi@126.com
张彦琼,博士,研究员,博士生导师,从事中药药理学研究,E-mail:yqzhang@icmm.ac.cn
收稿日期:2021-12-10,
网络出版日期:2022-03-25,
纸质出版日期:2023-03-05
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张依,王晓月,丁子禾等.中药配伍雷公藤制剂治疗类风湿关节炎的安全性系统评价及其增效减毒网络调控机制[J].中国实验方剂学杂志,2023,29(05):1-8.
ZHANG Yi,WANG Xiaoyue,DING Zihe,et al.Systematic Review on Safety of Chinese Medicines Combined with Tripterygium wilfordii Preparations in Treatment of Rheumatoid Arthritis and Exploration on Underlying Network Regulatory Mechanisms of Enhancing Efficacy and Reducing Toxicity[J].Chinese Journal of Experimental Traditional Medical Formulae,2023,29(05):1-8.
张依,王晓月,丁子禾等.中药配伍雷公藤制剂治疗类风湿关节炎的安全性系统评价及其增效减毒网络调控机制[J].中国实验方剂学杂志,2023,29(05):1-8. DOI: 10.13422/j.cnki.syfjx.20220943.
ZHANG Yi,WANG Xiaoyue,DING Zihe,et al.Systematic Review on Safety of Chinese Medicines Combined with Tripterygium wilfordii Preparations in Treatment of Rheumatoid Arthritis and Exploration on Underlying Network Regulatory Mechanisms of Enhancing Efficacy and Reducing Toxicity[J].Chinese Journal of Experimental Traditional Medical Formulae,2023,29(05):1-8. DOI: 10.13422/j.cnki.syfjx.20220943.
目的
2
系统评价中药配伍雷公藤多苷(甙)片/雷公藤片(TWPT/TWT)治疗类风湿关节炎(RA)的安全性,并初步探索常用配伍方案增效减毒的网络调控机制。
方法
2
检索中文数据库(中国知网、万方数据库、维普数据库)和英文数据库(PubMed、Cochrane Library、EMbase)自建库至2021年7月TWPT/TWT治疗RA出现相关不良反应的研究,应用风险评价工具对研究进行质量评价,提取数据并采用Stata 15.0软件进行分析。进一步,运用中药整合药理学网络计算平台2.0(TCMIP v2.0,
http://www.tcmip.cn/
http://www.tcmip.cn/
),构建“药物靶标-效毒症状基因”相互作用网络,探析雷公藤常用配伍方案增效减毒的分子机制。
结果
2
共检索到2 132篇文献,最终纳入包含中药配伍TWPT/TWT治疗RA的临床研究文献18篇。系统评价结果显示,TWPT/TWT治疗RA的不良反应主要表现为消化系统、血液系统、生殖系统病变,其中以消化系统损害的发生率最高,而中药配伍可以有效改善TWPT/TWT所导致的不良反应[RR(95% CI)=0.45(0.30,0.66),
P
<
0.01]。进而,亚组分析结果显示,RA患者的年龄、病程、配伍用药方案、用药剂量和疗程均会影响TWPT/TWT不良反应的发生。临床研究结果提示,白芍总苷(TGP)配伍TWPT/TWT应用最为广泛,且TGP减轻TWPT/TWT肝毒性的作用较其他中药更为显著,因此,本研究以该配伍方案为范例,进一步探索其缓解RA的“效-毒”关联机制。“药物靶标-效毒症状基因”相互作用网络挖掘结果显示,TGP-TWPT/TWT配伍的核心网络靶标主要通过调节机体免疫应答、减轻炎症反应、矫正代谢紊乱和改善细胞功能,来实现增效减毒作用。其中,参与“免疫-炎症”功能模块的白细胞介素-4(IL-4)和白细胞介素-13(IL-13)是两药配伍增效和减毒的共同靶点;“机体代谢”功能模块中的内源性甾醇、胆汁酸和胆汁盐、胰岛素分泌等代谢途径与TWPT/TWT致肝毒和TGP减肝毒机制密切相关;而细胞功能调节通路,如干细胞因子(SCF)/酪氨酸激酶受体(KIT)信号通路、磷脂酰肌醇3-激酶(PI3K)/蛋白激酶B(Akt)信号通路等,则共同参与了TWPT/TWT缓解RA和致肝毒的作用机制。
结论
2
临床采用合适的中药配伍TWPT/TWT治疗RA可有效增加其风湿病情改善作用且减轻其不良反应,其中,TGP-TWPT/TWT配伍方案的减毒作用最为显著。进一步的生物网络挖掘结果表明,TGP-TWPT/TWT配伍的减毒机制可能与两药靶标对白细胞介素信号通路和胆汁酸代谢途径的调节相关,二者配伍的协同增效机制可能通过作用于白细胞介素信号通路及细胞功能调节通路而实现。
Objective
2
To systematically evaluate the safety of Chinese medicines combined with
Tripterygium wilfordii
polyglycoside tablets/
Tripterygium wilfordii
tablets (TWPT/TWT) in the treatment of rheumatoid arthritis (RA), and to explore the network regulatory mechanisms of enhancing efficacy and reducing toxicity of commonly used combination regimes.
Method
2
The literature involving the adverse reactions of TWPT/TWT in treating RA was searched and collected from three Chinese databases (CNKI, Wanfang Data, VIP) and three English databases (PubMed, Cochrane Library, Embase) from the inception of the databases to July 2021. All studies were assessed by the Cochrane risk of bias tool, and the data were extracted and analyzed by Stata 15.0. Furthermore, Integrative Pharmacology-based Research Platform of Traditional Chinese Medicine 2.0 (TCMIP v2.0,
http://www.tcmip.cn/
http://www.tcmip.cn/
) was used to construct a "drug target-symptom gene of efficacy and toxicity" interaction network, to explore the underlying network regulatory mechanisms of enhancing efficacy and reducing toxicity of common
T. wilfordii
preparation combinations.
Result
2
A total of 2 132 articles on Chinese medicines combined with TWPT/TWT in the treatment of RA were retrieved, and 18 of them were finally included. The systematic review showed that the adverse reactions of TWPT/TWT against RA mainly occurred in the digestive system, blood system, and reproductive system, of which digestive system had the highest incidence of damages. However, the combination with Chinese medicines effectively alleviated the adverse reactions caused by TWPT/TWT [RR (95% CI)=0.45 (0.30, 0.66),
P
<
0.01]. In addition, the subgroup analysis indicated that the age of RA patients, course of disease, combination regimen, medication dosage and duration of treatment all affected the occurrence of adverse reactions of TWPT/TWT. It was found in clinical studies that total glucosides of paeony (TGP) and TWPT/TWT was most widely combined, and the effect of TGP in reducing TWPT/TWT-induced hepatotoxicity was also more significant than that of other Chinese medicines. Moreover, taking this combination regime as an example, this paper explored the "efficacy-toxicity" association mechanisms of TGP-TWPT/TWT against RA. The "drug target-symptom gene of efficacy and toxicity" interaction network revealed that the core network targets of TGP-TWPT/TWT enhanced efficacy and reduced toxicity mainly through regulating immunity-inflammation-related pathways, metabolic pathways and cell signal transduction. Especially, interleukin-4 (IL-4) and interleukin-13 (IL-13), which were involved in the "immunity-inflammation" module, were the common targets of TGP-TWPT/TWT to enhance efficacy and reduce toxicity. The endogenous sterols, bile acids and bile salts, insulin secretion and other metabolic pathways in the "body metabolism" module were closely associated with the mechanisms of TWPT/TWT inducing hepatotoxicity and TGP reducing hepatotoxicity. While cell function regulation pathways, such as stem cell factor (SCF)/tyrosine kinase receptor (KIT) signaling pathway and phosphatidylinositol 3-kinase (PI3K)/protein kinase B (Akt)signaling pathway were involved in both anti-RA effects and hepatotoxicity of TWPT/TWT.
Conclusion
2
Clinical application of suitable Chinese medicines combined with TWPT/TWT in the treatment of RA can effectively improve the rheumatism and reduce the adverse reactions of TWPT/TWT, and TGP-TWPT/TWT has the most significant toxicity-reducing effect. Further biological network-based investigation indicates that the toxicity-reducing mechanism of TGP-TWPT/TWT may be related to the regulation of interleukin signaling pathway and bile acid metabolism pathway, and the synergistic efficacy-enhancing effect of the combination may be achieved by acting on interleukin signaling pathway and cell function regulation pathway.
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