Clin Gastroenterlogy and Hepatology: Vedolizumab浓度,抗药物抗体和α4β7基因与炎症性肠病患者反应的关系

2018-05-29 MedSci MedSci原创

关于整联蛋白α4β7单克隆抗体vedolizumab的实际药代动力学和药效学特征的资料目前很少。研究人员对用vedolizumab治疗的炎症性肠病(IBD)患者进行了前瞻性研究,以确定血清药物浓度,抗动脉滴注抗体(AVA)的形成和整合素α4β7饱和度与治疗效果之间的关系。

背景:
关于整联蛋白α4β7单克隆抗体vedolizumab的实际药代动力学和药效学特征的资料目前很少。研究人员对用vedolizumab治疗的炎症性肠病IBD)患者进行了前瞻性研究,以确定血清药物浓度,抗动脉滴注抗体(AVA)的形成和整合素α4β7饱和度与治疗效果之间的关系。

方法
研究人员对2014年9月至2017年3月在以色列2所三级医疗中心接受维多珠单抗治疗的106例IBD患者(67例克罗恩病和39例溃疡性结肠炎)进行了前瞻性研究。在诱导和维持治疗之前和治疗期间收集临床数据和血清样品。临床缓解定义为Harvey-Bradshaw指数低于5或简单临床结肠炎活动指数评分为3或更低。研究人员测量了vedolizumab,AVAs和炎症标志物的血清水平。在指定的波谷时间点从一些患者获得外周血单核细胞,并从36个样品中分离CD3 + CD45RO + T细胞。用荧光标记的vedolizumab孵育细胞,并使用流式细胞术来量化α4β7整合素饱和度。

结果:
在第6周时,106例患者中有48例(45%)达到临床缓解,第14周时106例患者中有50例(48%)达到临床缓解。临床缓解患者第6周的维多珠单抗中位数水平(40.2μg/ mL)高于活动性疾病患者(29.7μg/ mL; P  = 0.05)。在维持期间,具有正常C-反应蛋白水平的患者相对于具有高水平C-反应蛋白的水平的患者的维多珠单抗的血清水平显着更高(P = .0006)。诱导治疗期间17%的患者和维持治疗期间3%的患者检测到AVAs,但与临床结果无关。流式细胞术分析外周血记忆T细胞(n = 36)显示,在第2周和第14周以及维持阶段,α4β7整合蛋白几乎完全占用,无论其反应状态或药物水平如何

结论
在IBD患者中,维多珠单抗药物水平与缓解和炎症标记是密切相关的。无论药物的血清水平或对治疗的反应如何,整体蛋白α4β7在来自用维多珠单抗治疗的患者的几乎所有T细胞中都被阻断。

原始出处:

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    2018-09-06 许安
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    2018-12-31 snf701207
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    2018-06-11 1e145228m78(暂无匿称)

    学习了.谢谢作者分享!

    0

  5. 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    2018-05-31 gwc384
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    2018-05-29 cscdliu

    学习了.谢谢

    0