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优化炎症性肠病的药物治疗管理。

Optimizing pharmacologic management of inflammatory bowel disease.

机构信息

a Division of Gastroenterology , New York University Langone Medical Center , New York , NY , USA.

b Division of Gastroenterology , Northwestern University Feinberg School of Medicine , Chicago , IL , USA.

出版信息

Expert Rev Clin Pharmacol. 2017 Jun;10(6):595-607. doi: 10.1080/17512433.2017.1318062. Epub 2017 May 5.

DOI:10.1080/17512433.2017.1318062
PMID:28475384
Abstract

As our medical armamentarium for IBD continues to expand, it is essential that clinicians understand both optimizing and sequencing of individual and combination therapeutic approaches with available medications. Areas covered: This review summarizes dosing strategies and therapeutic drug monitoring for pharmacologic optimization in IBD. Aminosalicylates remain first-line therapies for mild-to-moderate UC but have limited evidence of efficacy in CD. Budesonide provides an alternative to aminosalicylates when targeted to appropriate sites in the distal small bowel and colon, as do conventional corticosteroids when applied rectally. Systemic steroids are highly efficacious but burdened by toxicity. Thiopurines or methotrexate can be utilized as steroid-sparing agents. Biologic agents targeting TNF remain important for steroid-sparing therapy in moderate-to-severe UC and CD. Newer biologics targeting lymphocyte trafficking and lymphocyte activation are also efficacious for moderate-to-severe IBD. Near future conventional drug options include oral agents such as tofacitinib and mongersen. Expert commentary: Positioning therapies according to the location, phenotypes, and severity, as well as the use of therapeutic and clinical targets, will improve outcomes and minimize toxicities and therapeutic futilities. Future IBD treatment should focus on personalized therapy plans based on genetic determinants, targeted mechanisms of action, and pharmacologic optimization.

摘要

随着我们用于治疗 IBD 的医学手段不断增加,临床医生了解如何优化和调整各种单独和联合治疗方法的药物使用顺序至关重要。涵盖领域:本篇综述总结了 IBD 中药物优化的给药策略和治疗药物监测。氨基水杨酸盐仍然是轻中度 UC 的一线治疗药物,但在 CD 中的疗效证据有限。当将布地奈德靶向应用于远端小肠和结肠的适当部位时,其可替代氨基水杨酸盐;当直肠应用时,传统皮质类固醇也可替代氨基水杨酸盐。全身皮质类固醇具有高度疗效,但存在毒性负担。硫唑嘌呤或甲氨蝶呤可用作皮质类固醇保留剂。针对 TNF 的生物制剂仍然是中重度 UC 和 CD 中皮质类固醇保留治疗的重要手段。针对淋巴细胞迁移和淋巴细胞激活的新型生物制剂也对中重度 IBD 有效。未来的常规药物选择包括口服药物,如托法替尼和蒙吉森。专家评论:根据位置、表型和严重程度以及治疗和临床靶点定位治疗,将改善结果并最大程度地减少毒性和治疗无效。未来的 IBD 治疗应侧重于基于遗传决定因素、靶向作用机制和药物优化的个性化治疗计划。

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