Department of Pharmacy, Hartford Hospital, Hartford, CT, USA.
Department of Research Administration, Hartford Healthcare, Hartford, CT, USA.
Transpl Infect Dis. 2021 Aug;23(4):e13573. doi: 10.1111/tid.13573. Epub 2021 Feb 18.
Cytomegalovirus (CMV) is a significant cause of morbidity in kidney transplant recipients (KTR). Historically at our institution, KTR with low and intermediate CMV risk received 6 months of valganciclovir if they received lymphocyte depleting induction therapy. This study evaluates choice and duration of CMV prophylaxis based on donor (D) and recipient (R) CMV serostatus and the incidence of post-transplant CMV viremia in low (D-/R-) and intermediate (R+) risk KTR receiving lymphocyte-depleting induction therapy. A protocol utilizing valacyclovir for 3 months for D-/R- and valganciclovir for 3 months for R+ was evaluated. Adult D-/R- and R+ KTR receiving anti-thymocyte globulin, rabbit or alemtuzumab induction from 8/20/2016 to 9/30/2018 were evaluated through 1 year post-transplant. Patients were excluded if their CMV serostatus was D+/R-, received a multi-organ transplant, or received basiliximab. Seventy-seven subjects met the inclusion criteria: 25 D-/R- (4 historic group, 21 experimental group) and 52 R+ (31 historic, 21 experimental). No D-/R- patients experienced CMV viremia. Among the R+ historic and experimental groups, there was no significant difference in viremia incidence (35.5% vs 52.4%; P = .573). Of these cases, the peak viral load was similar between the groups (median [IQR], 67 [<200-444] vs <50 [<50-217]; P = .711), and there was no difference in the incidence of CMV syndrome (16.1% vs 14.3%; P = 1.000) or CMV related hospitalization (12.9% vs 14.3%; P = 1.000). No patient experienced tissue invasive disease. These results suggest limiting valganciclovir exposure may be possible in low and intermediate risk KTR receiving lymphocyte-depleting induction therapy with no apparent impact on CMV-related outcomes.
巨细胞病毒(CMV)是肾移植受者(KTR)发病的重要原因。在我们医院,既往低危和中危 CMV 风险的 KTR 如果接受淋巴细胞耗竭诱导治疗,则接受 6 个月的缬更昔洛韦预防。本研究评估了根据供体(D)和受体(R)CMV 血清状态以及接受淋巴细胞耗竭诱导治疗的低危(D-/R-)和中危(R+)风险 KTR 中 CMV 血症的发生率选择和 CMV 预防的持续时间。评估了一种使用伐昔洛韦治疗 3 个月用于 D-/R-和缬更昔洛韦治疗 3 个月用于 R+的方案。评估了 2016 年 8 月 20 日至 2018 年 9 月 30 日期间接受抗胸腺细胞球蛋白、兔抗胸腺细胞球蛋白或阿仑单抗诱导的成年 D-/R-和 R+KTR,随访 1 年。如果 CMV 血清状态为 D+/R-、接受多器官移植或接受巴利昔单抗,则排除患者。77 例符合纳入标准:25 例 D-/R-(4 例历史组,21 例实验组)和 52 例 R+(31 例历史组,21 例实验组)。没有 D-/R-患者发生 CMV 血症。在 R+历史组和实验组中,病毒血症发生率无显著差异(35.5% vs 52.4%;P=0.573)。在这些病例中,两组之间的峰值病毒载量相似(中位数[IQR],67[200-444] vs <50[50-217];P=0.711),CMV 综合征的发生率也没有差异(16.1% vs 14.3%;P=1.000)或与 CMV 相关的住院率(12.9% vs 14.3%;P=1.000)。没有患者发生组织侵袭性疾病。这些结果表明,在接受淋巴细胞耗竭诱导治疗的低危和中危 KTR 中,限制缬更昔洛韦的暴露可能是可能的,而对 CMV 相关结局没有明显影响。
