CGRP单克隆抗体预防性治疗偏头痛疗效和安全性的贝叶斯网状Meta分析
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篇名: CGRP单克隆抗体预防性治疗偏头痛疗效和安全性的贝叶斯网状Meta分析
TITLE: Efficacy and Safety of Calcitonin Gene-related Peptide Monoclonal Antibodies in the Preventive Treatment of Migraine:A Bayesian Network Meta-analysis
摘要: 目的:系统评价4种降钙素基因相关肽(CGRP)单克隆抗体预防性治疗偏头痛的疗效和安全性,为临床治疗提供循证参考。方法:计算机检索Cochrane图书馆、PubMed、Embase、中国期刊全文数据库、维普网和万方数据等,收集4种CGRP单克隆抗体(试验组)对比安慰剂(对照组)预防性治疗偏头痛的随机对照试验(RCT)。筛选文献并提取资料后,采用Cochrane系统评价员手册5.1.0提供的偏倚风险评估工具对纳入文献质量进行评价,采用GeMTC0.14.3软件和Stata16.0软件进行贝叶斯网状Meta分析。结果:共纳入19项RCT,共计11392例患者,涉及Erenumab70、140mg/月,Fremanezumab675mg/3月、225mg/月,Galcane-zumab120、240、300mg/月,Eptinezumab100、300mg/3月和安慰剂等10种干预措施。Meta分析结果显示,与对照组比较,4种GGRP单克隆抗体均可显著减少患者每月平均偏头痛天数较基线的变化(MMD)(P<0.05);各试验组之间,与Galcanezumab300mg/月[MD=-1.30,95%CI(-2.59,-0.05),P<0.05]、Eptinezumab100mg/3月[MD=-1.18,95%CI(-2.26,-0.03),P<0.05]比较,Fremanezumab225mg/月可显著减少患者MMD;网状Meta排序结果为Fremanezumab225mg/月>Fremanezumab675mg/3月>Galcanezumab120mg/月>Erenumab140mg/月>Galcanezumab240mg/月>Eptinezumab300mg/3月>Erenumab70mg/月>Eptinezumab100mg/3月>Galcanezumab300mg/月>安慰剂。与对照组比较,4种GGRP单克隆抗体均可显著增加每月平均偏头痛天数较基线减少≥50%的患者比例(MMD50)(P<0.05);各试验组之间,与Eptinezumab100mg/3月组比较,Fremane-zumab675mg/3月[OR=1.51,95%CI(1.02,2.31),P<0.05]、Fremanezumab225mg/月[OR=1.58,95%CI(1.05,2.44),P<0.05]组的MMD50均显著升高;网状Meta排序结果为Fremanezumab225mg/月>Fremanezumab675mg/3月>Erenumab140mg/月>Galcanezumab120mg/月>Eptinezumab300mg/3月>Galcanezumab240mg/月>Erenumab70mg/月>Galcanezumab300mg/月>Eptinezumab100mg/3月>安慰剂。安全性方面,Fremanezumab675mg/3月[OR=1.31,95%CI(1.05,1.64),P<0.05]、Galcane-zumab240mg/月[OR=1.39,95%CI(1.09,1.74),P<0.05]组患者的总不良反应发生率(AE)均显著高于对照组;各试验组之间,与Galcanezumab240mg/月组比较,Erenumab70mg/月[OR=0.67,95%CI(0.50,0.93),P<0.05]、140mg/月[OR=0.70,95%CI(0.51,0.98),P<0.05]组患者的AE均显著降低;与Fremanezumab675mg/3月组比较,Erenumab70mg/月[OR=0.72,95%CI(0.52,0.98),P<0.05]组患者的AE显著降低;网状Meta排序结果为Galcanezumab240mg/月>Fremanezumab675mg/3月>Galcane-zumab120mg/月>Galcanezumab300mg/月>Eptinezumab300mg/3月>Fremanezumab225mg/月>Eptinezumab100mg/3月>安慰剂>Erenumab140mg/月>Erenumab70mg/月。结论:4种CGRP单克隆抗体均能预防性治疗偏头痛,其中Fremanezumab225mg/月的疗效可能最佳,Erenumab70mg/月的安全性可能最高。
ABSTRACT: OBJECTIVE:To systematically evaluate th e efficacy and safety of 4 kinds of calcitonin gene-related peptide (CGRP)monoclonal antibodies in the preventive treatment of migraine ,and to provide evidence-based reference for the clinical treatment of migraine. METHODS :Retrieved from the Cochrane Library ,PubMed,Embase,CJFD,VIP and Wanfang database , RCTs about 4 kinds of CGRP monoclonal antibodies (trial Δ 基金项目 :四川省科技厅重点研发 (重大科技专项 )项目 group) versus placebo (control group ) in the preventive (No.2019YFS0180) *硕士研究生 。研究方向 :临床药学 、循证药学 。电话:0830- treatment of migraine were collected. After literature screening 3165787。E-mail:lewxinn@outlook.com and data extraction , the quality evaluation of included # 通信作者:教授,硕士生导师,硕士。研究方向:临床药学、循证 literature was performed by using the bias risk assessment tool 药学。电话:0830-3165787。E-mail:hyl3160131@163.com provided by the Cochrane system evaluator manual 5.1.0. 中国药房 2020年第31卷第18期 China Pharmacy 2020Vol. 31 No. 18 ·2275· Bayesian network Meta-analysis was performed by using GeMTC 0.14.3 software and Stata 16.0 software. RESULTS :A total of 19 RCTs involving 11 392 patients were included ,involving 10 interventions,such as Erenumab 70,140 mg/month;Fremanezumab 675 mg/3 months,225 mg/month;Galcanezumab 120,240,300 mg/month;Eptinezumab 100 mg/3 months,300 mg/3 months and placebo. Results of Meta-analysis showed that compared with control group ,4 kinds of CGRP monoclonal antibodies significantly reduced the change of mean monthly migraine days (MMD)(P<0.05). Among trial groups ,compared with Galcanezumab 300 mg/month [MD =-1.30,95%CI(-2.59,-0.05),P<0.05] and Eptinezumab 100 mg/3 months [MD =-1.18, 95%CI(-2.26,-0.03),P<0.05],Fremanezumab 225 mg/month could significantly reduce MMD. Network Meta-analysis ranking showed that Fremanezumab 225 mg/month>Fremanezumab 675 mg/3 months>Galcanezumab 120 mg/month>Erenumab 140 mg/month>Galcanezumab 240 mg/month>Eptinezumab 300 mg/3 months>Erenumab 70 mg/month>Eptinezumab 100 mg/3 months>Galcanezumab 300 mg/month>placebo. Compared with control group ,4 kinds of CGRP monoclonal antibodies were significantly increased of the proportion of patients whose mean monthly migraine days reduction ≥50% compared with baseline (MMD 50)(P<0.05). Among trial groups ,compared with Eptinezumab 100 mg/3 months group ,MMD 50 of Fremanezumab 675 mg/3 months group [OR =1.51,95%CI(1.02,2.31),P<0.05],Fremanezumab 225 mg/month group [OR =1.58,95%CI (1.05,2.44),P<0.05] were increased significantly. Network Meta-analysis ranking showed that Fremanezumab 225 mg/month> Fremanezumab 675 mg/3 months>Erenumab 140 mg/month>Galcanezumab 120 mg/month>Eptinezumab 300 mg/3 months> Galcanezumab 240 mg/month>Erenumab 70 mg/month>Galcanezumab 300 mg/month>Eptinezumab 100 mg/3 months>placebo. In terms of safety ,incidence of total adverse events (AE)of trial groups receiving Fremanezumab 675 mg/3 months [OR =1.31, 95%CI(1.05,1.64),P<0.05],Galcanezumab 240 mg/month [OR =1.39,95%CI(1.09,1.74),P<0.05] were significantly higher than control group. Among trial groups ,compared with Galcanezumab 240 mg/month group ,AE of Erenumab 70 mg/month group [OR =0.67,95%CI(0.50,0.93),P<0.05],Erenumab 140 mg/month group [OR =0.70,95%CI(0.51,0.98),P<0.05] were decreased significantly. Compared with Fremanezumab 675 mg/3 months group ,AE of Erenumab 70 mg/month group [OR = 0.72,95%CI(0.52,0.98),P<0.05] were decreased significantly. Network Meta-analysis ranking showed that Galcanezumab 240 mg/month> Fremanezumab 675 mg/3 months>Galcanezumab 120 mg/month>Galcanezumab 300 mg/month>Eptinezumab 300 mg/3 months>Fremanezumab 225 mg/month>Eptinezumab 100 mg/3 months>placebo>Erenumab 140 mg/month>Erenumab 70 mg/month. CONCLUSIONS :Four kinds of CGRP monoclonal antibodies are effective in the preventive treatment of migraine , among which Fremanezumab 225 mg/month is most likely to have the best efficacy and Erenumab 70 mg/month is most likely to have the highest safety.
期刊: 2020年第31卷第18期
作者: 刘鑫,钟小燕,李梦雅,徐昌静,付礼亚,田冬梅,黄毅岚
AUTHORS: LIU Xin,ZHONG Xiaoyan ,LI Mengya ,XU Changjing ,FU Liya,TIAN Dongmei ,HUANG Yilan
关键字: 降钙素基因相关肽单克隆抗体;预防性治疗;偏头痛;贝叶斯网状Meta分析;疗效;安全性
KEYWORDS: Calcitonin gene-related peptide monoclonal antibodies ; Preventive treatment ;Migraine; Bayesian network
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