肾移植后巨细胞病毒治疗的新方法

Nephrologie & therapeutique Pub Date : 2024-08-01 Epub Date: 2024-08-12 DOI:10.1684/ndt.2024.84
Nassim Kamar, Olivier Marion, Arnaud Del Bello
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引用次数: 0

摘要

巨细胞病毒(CMV)感染是肾移植后出现的主要机会性感染。尽管采取了预防策略,但 CMV 病仍时有发生,尤其是在高危患者(供体血清反应阳性/受体血清反应阴性)中。患者可能会出现复杂的 CMV,即复发性、难治性或耐药性 CMV 感染。预防 CMV 主要依靠普遍预防或先期治疗。对于高危患者,通常首选普遍预防。目前,缬更昔洛韦被用于这种情况。然而,缬更昔洛韦会导致严重的白细胞减少症和中性粒细胞减少症。最近,一种新型抗病毒药物--来特莫韦与缬更昔洛韦进行了比较。在预防 CMV 疾病方面,它与缬更昔洛韦一样有效,而且引起的血液学副作用较小。法国目前仍未将其用于这一适应症。最近的研究表明,通过 ELISPOT 或 Quantiferon 进行免疫监测有助于确定预防性治疗的持续时间。其他研究表明,对于接受 mTOR 抑制剂治疗的 CMV 血清阳性肾移植患者,可以不进行预防性治疗。对于难治性 CMV 感染,应寻找耐药突变。目前,马立巴韦是治疗难治/耐药 CMV 的金标准疗法。在治疗 8 周和 8 周后,其疗效明显优于其他抗病毒药物,如大剂量更昔洛韦、福斯卡尼或西多福韦。然而,在停止治疗后发现复发率很高。因此,应评估其他治疗策略,以提高持续病毒学率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Novelties for the management of cytomegalovirus after kidney transplantation

Cytomegalovirus (CMV) infection is the main opportunistic infection observed after kidney transplantation. Despite the use of prevention strategies, CMV disease still occurs, especially in high-risk patients (donor seropositive/recipient seronegative). Patients may develop complicated CMV, i.e. recurrent, refractory or resistant CMV infection. CMV prevention relies on either universal prophylaxis or preemptive therapy. In high-risk patients, universal prophylaxis is usually preferred. Currently, valganciclovir is used in this setting. However, valganciclovir can be responsible for severe leucopenia and neutropenia. A novel anti-viral drug, letermovir, has been recently compared to valganciclovir. It was as efficient as valganciclovir to prevent CMV disease and induced less hematological side-effects. It is still not available in France in this indication. Recent studies suggest that immune monitoring by ELISPOT or Quantiferon can be useful to determine the duration of prophylaxis. Other studies suggest that prophylaxis may be skipped in CMV-seropositive kidney-transplant patients given mTOR inhibitors. Refractory CMV is defined by the lack of decrease of CMV DNAemia of at least 1 log10 at 2 weeks after effective treatment. In case of refractory CMV infection, drug resistant mutations should be looked for. Currently, maribavir is the gold standard therapy for refractory/resistant CMV. At 8 weeks therapy and 8 weeks later, it has been shown to be significantly more effective than other anti-viral drugs, i.e. high dose of ganciclovir, foscarnet or cidofovir. However, a high rate of relapse was observed after ceasing therapy. Hence, other therapeutic strategies should be evaluated in order to improve the sustained virological rate.

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