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Risk of tuberculosis reactivation during interleukin-17 inhibitor therapy for psoriasis: a systematic review

机译:白细胞介素-17抑制剂治疗牛皮癣治疗期间结核重新激活的风险:系统审查

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摘要

Immunosuppressive therapies, effective in treating inflammatory disorders such as psoriasis, increase the risk of serious infections, such as tuberculosis (TB). For example, tumour necrosis factor (TNF)-alpha inhibitors significantly increase the risk of TB reactivation in patients with latent TB infection (LTBI), which has led clinicians to routinely test for TB prior to initiation of these medications. This protocol has since extended to other, newer immunomodulatory therapies for psoriasis, such as interleukin (IL)-17 inhibitors, including secukinumab, ixekizumab and brodalumab. We conducted a systematic review to examine whether there is any evidence that IL-17 inhibitor therapy for psoriasis increases the risk of TB reactivation. Using PubMed and EMBASE, our literature search resulted in 139 total articles. After manually reviewing each article for the discussion of IL-17 inhibitors for psoriasis, with data originating from clinical trials, and assessment for incidence of TB reactivation, 23 articles met the full inclusion criteria for our review. Overall, we found no cases of TB reactivation in patients treated with IL-17 inhibitors for psoriasis. This suggests that IL-17 inhibitors may be safely used in psoriasis patients with LTBI who receive appropriate LTBI treatment. However, long-term real-world studies are warranted to further evaluate this risk.
机译:免疫抑制疗法有效治疗牛皮癣等炎症疾病,增加了严重感染的风险,如结核病(TB)。例如,肿瘤坏死因子(TNF)抑制剂显着提高潜伏TB感染(LTBI)患者TB再活化的风险,其LED临床医生在启动这些药物之前常规测试TB。该方案自扩大到牛皮癣的其他更新的免疫调节疗法,例如白细胞介素(IL)-17抑制剂,包括Secukinumab,Ixekizumab和Brodalumab。我们进行了系统的审查,以检查是否有任何证据表明牛皮癣的IL-17抑制剂治疗增加了TB Reactivation的风险。使用PubMed和Embase,我们的文献搜索导致了139篇总物品。在手动审查每种文章后,讨论牛皮癣的IL-17抑制剂后,源自临床试验的数据,以及结核病重新激活的发病率评估,23篇文章符合我们审查的全部纳入标准。总体而言,我们发现没有用IL-17抑制剂进行牛皮癣治疗的患者结核反弹的情况。这表明IL-17抑制剂可以安全地用于牛皮癣患者,所述LTBI接受适当的LTBI治疗。然而,有必要长期的现实研究进一步评估这一风险。

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