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肿瘤坏死因子阻断治疗的感染性并发症

Infectious complications of tumor necrosis factor blockade.

作者信息

Wallis Robert S

机构信息

Pfizer, New London, Connecticut 06320, USA.

出版信息

Curr Opin Infect Dis. 2009 Aug;22(4):403-9. doi: 10.1097/QCO.0b013e32832dda55.

Abstract

PURPOSE OF REVIEW

Our understanding of the infection risks posed by tumor necrosis factor (TNF) antagonists has continued to evolve in the 10 years since these drugs were first introduced. This review summarizes recent data regarding infection risk, examines potential structure-function relationships that may account for the differences, and discusses their implications with regard to tuberculosis prevention and management.

RECENT FINDINGS

Recent prospective studies have confirmed the risk of tuberculosis reactivation posed by TNF antibodies to be several fold greater than soluble TNF receptor. Certolizumab pegol, a monovalent anti-TNF Fab' fragment appears to share this risk, despite its lack of Fc and its inability to cross-link transmembrane TNF. Screening and initiation of treatment for latent tuberculosis (TB) infection can greatly reduce the TB risk of anti-TNF treatment in western countries. However, alternative strategies to prevent TB because of new transmission may be required as these therapies become available worldwide. Current recommendations for withdrawal of anti-TNF therapy when TB is diagnosed place patients at risk for paradoxical worsening because of recovery of TNF-dependent inflammation. Recent case reports suggest reinstitution of TNF blockade may be safe and effective adjunctive treatment in such cases, but prospective studies are needed to confirm these observations.

SUMMARY

TNF blockers have transformed treatment of several chronic inflammatory conditions. Further research is needed to determine how best to prevent and manage their infectious complications and to determine their potential adjunctive therapeutic role in chronic infection diseases.

摘要

综述目的

自肿瘤坏死因子(TNF)拮抗剂首次应用以来的10年里,我们对其所致感染风险的认识不断发展。本综述总结了关于感染风险的最新数据,研究了可能导致差异的潜在结构 - 功能关系,并讨论了它们在结核病预防和管理方面的意义。

最新发现

最近的前瞻性研究证实,TNF抗体引发的结核病再激活风险比可溶性TNF受体高几倍。赛妥珠单抗,一种单价抗TNF Fab'片段,尽管缺乏Fc且无法交联跨膜TNF,但似乎也有这种风险。在西方国家,对潜伏性结核感染进行筛查和开始治疗可大大降低抗TNF治疗的结核病风险。然而,随着这些疗法在全球范围内应用,可能需要采取替代策略来预防因新传播导致的结核病。目前关于结核病诊断时停用抗TNF治疗的建议使患者因TNF依赖性炎症恢复而面临矛盾性恶化的风险。最近的病例报告表明,在这种情况下重新使用TNF阻滞剂可能是安全有效的辅助治疗方法,但需要前瞻性研究来证实这些观察结果。

总结

TNF阻滞剂改变了几种慢性炎症性疾病的治疗方式。需要进一步研究以确定如何最好地预防和管理其感染并发症,并确定它们在慢性感染性疾病中的潜在辅助治疗作用。

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