Golan Yoav, Tang Yuexin, Mt-Isa Shahrul, Wan Hong, Teal Valerie, Badshah Cyrus, Dadwal Sanjeet
Department of Internal Medicine, Division of Infectious Diseases, Tufts Medical Center, Boston, MA, USA.
Merck & Co., Inc., Kenilworth, NJ, USA.
Pharmacoecon Open. 2021 Sep;5(3):469-473. doi: 10.1007/s41669-021-00264-9. Epub 2021 Apr 19.
Allogeneic hematopoietic stem cell transplantation (HSCT) is associated with substantial healthcare resource use, particularly when recipients develop cytomegalovirus (CMV) infection. Letermovir reduced post-HSCT CMV infection risk compared with placebo in a previous phase III trial. This analysis evaluated letermovir's impact on re-hospitalization post-transplant.
Using data from a phase III, multicenter, randomized clinical trial (NCT02137772, registered May 14, 2014), this study assessed CMV-associated and all-cause re-hospitalizations at weeks 14, 24, and 48 post-transplant among recipients of letermovir versus placebo. Unstandardized re-hospitalization rates and days were reported; standardized rates and days were estimated accounting for censoring due to death or early study discontinuation.
Unstandardized rates (95% confidence interval [CI]) of all-cause re-hospitalization in letermovir versus placebo recipients at weeks 14, 24, and 48 were 36.6% (31.4-42.1) versus 47.6% (39.9-55.4), 49.2% (43.7-54.8) versus 55.9% (48.1-63.5), and 55.7% (50.1-61.2) versus 60.6% (52.8-68.0), respectively. Unstandardized mean total duration (95% CI) of re-hospitalization with letermovir versus placebo at weeks 14, 24, and 48 were 7.6 (5.9-9.8) versus 11.3 (8.6-14.8), 13.9 (11.2-17.2) versus 15.5 (11.9-20.1), and 18.0 (14.8-21.9) versus 20.7 (15.8-27.1) days, respectively. Similar results were found in CMV-associated re-hospitalization outcomes and standardized rates and days of all-cause re-hospitalizations.
In this post-hoc analysis, letermovir was associated with lower rates of CMV-associated and all-cause re-hospitalizations with a shorter length of stay (especially within the first 14 weeks post-transplant).
异基因造血干细胞移植(HSCT)会消耗大量医疗资源,尤其是当受者发生巨细胞病毒(CMV)感染时。在之前的一项III期试验中,与安慰剂相比,来特莫韦降低了HSCT后CMV感染风险。本分析评估了来特莫韦对移植后再次住院的影响。
利用一项III期多中心随机临床试验(NCT02137772,于2014年5月14日注册)的数据,本研究评估了来特莫韦与安慰剂受者在移植后第14、24和48周时与CMV相关的再住院情况及全因再住院情况。报告了未标准化的再住院率和天数;估计了标准化率和天数,并考虑了因死亡或提前终止研究导致的删失情况。
来特莫韦与安慰剂受者在第14、24和48周时全因再住院的未标准化率(95%置信区间[CI])分别为36.6%(31.4 - 42.1)和47.6%(39.9 - 55.4),49.2%(43.7 - 54.8)和55.9%(48.1 - 63.5),以及55.7%(50.1 - 61.2)和60.6%(52.8 - 68.0)。来特莫韦与安慰剂受者在第14、24和48周时再住院的未标准化平均总时长(95%CI)分别为7.6(5.9 - 9.8)天和11.3(8.6 - 14.8)天,13.9(11.2 - 17.2)天和15.5(11.9 - 20.1)天,以及18.0(14.8 - 21.9)天和20.7(15.8 - 27.1)天。在与CMV相关的再住院结局以及全因再住院的标准化率和天数方面也发现了类似结果。
在这项事后分析中,来特莫韦与较低的CMV相关再住院率和全因再住院率相关,住院时间更短(尤其是在移植后的前14周内)。
