实体器官移植受者的间质性肺病与 mTOR 抑制剂有关:依维莫司大型 III 期临床试验计划的结果及文献综述》。

IF 0.9 Q3 SURGERY
Journal of Transplantation Pub Date : 2014-01-01 Epub Date: 2014-12-18 DOI:10.1155/2014/305931
Patricia Lopez, Sven Kohler, Seema Dimri
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引用次数: 0

摘要

据报道,使用哺乳动物雷帕霉素靶点抑制剂(mTORi)会导致间质性肺病(ILD)。我们使用标准化 MedDRA 查询 (SMQ) 对 ILD 进行了检索,然后逐例进行医学评估,检索了依维莫司在新肾脏 (A2309)、心脏 (A2310) 和肝脏 (H2304) 移植受者 (TxR) 中进行的三项 III 期试验的临床和安全性数据库。在 MEDLINE 和 EMBASE 中进行了文献检索。在 1,473 例接受依维莫司治疗的新发 TxR 中,有 6 例(1 例肾脏、4 例心脏和 1 例肝脏 TxR)确诊为依维莫司相关 ILD,发生率为 0.4%。在四例心脏TxR中,有三例停用依维莫司后,ILD得到改善或缓解。肾移植患者(继续接受依维莫司治疗)和肝移植患者尽管停用了依维莫司,但结果均为死亡。文献综述发现了57篇关于接受依维莫司或西罗莫司治疗的实体器官TxR出现ILD的文献。ILD 在开始使用 mTORi 后数月或数年出现,症状为非特异性和隐匿性。在晚期改用 mTORi 的患者中,这种情况更为常见。在大多数病例中,及时停用 mTORi 后,ILD 会得到逆转。mTORi诱发的ILD是一种不常见的潜在致命疾病,应及早识别并停药。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Interstitial Lung Disease Associated with mTOR Inhibitors in Solid Organ Transplant Recipients: Results from a Large Phase III Clinical Trial Program of Everolimus and Review of the Literature.

Interstitial Lung Disease Associated with mTOR Inhibitors in Solid Organ Transplant Recipients: Results from a Large Phase III Clinical Trial Program of Everolimus and Review of the Literature.

Interstitial Lung Disease Associated with mTOR Inhibitors in Solid Organ Transplant Recipients: Results from a Large Phase III Clinical Trial Program of Everolimus and Review of the Literature.

Interstitial lung disease (ILD) has been reported with the use of mammalian target of rapamycin inhibitors (mTORi). The clinical and safety databases of three Phase III trials of everolimus in de novo kidney (A2309), heart (A2310), and liver (H2304) transplant recipients (TxR) were searched using a standardized MedDRA query (SMQ) search for ILD followed by a case-by-case medical evaluation. A literature search was conducted in MEDLINE and EMBASE. Out of the 1,473 de novo TxR receiving everolimus in Phase III trials, everolimus-related ILD was confirmed in six cases (one kidney, four heart, and one liver TxR) representing an incidence of 0.4%. Everolimus was discontinued in three of the four heart TxR, resulting in ILD improvement or resolution. Outcome was fatal in the kidney TxR (in whom everolimus therapy was continued) and in the liver TxR despite everolimus discontinuation. The literature review identified 57 publications on ILD in solid organ TxR receiving everolimus or sirolimus. ILD presented months or years after mTORi initiation and symptoms were nonspecific and insidious. The event was more frequent in patients with a late switch to mTORi. In most cases, ILD was reversed after prompt mTORi discontinuation. ILD induced by mTORi is an uncommon and potentially fatal event warranting early recognition and drug discontinuation.

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自引率
4.00%
发文量
5
审稿时长
16 weeks
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