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美国常规临床护理中福沙匹韦的免疫和病毒学反应:一项OPERA队列研究。

Immunological and virological response to fostemsavir in routine US clinical care: An OPERA cohort study.

作者信息

Hsu Ricky K, Brunet Laurence, Lackey Philip C, Pierone Gerald, Levis Brooke, Fusco Jennifer S, Henegar Cassidy, Vannappagari Vani, Clark Andrew, Fusco Gregory P

机构信息

NYU Langone Health, New York, New York, USA.

AIDS Healthcare Foundation, New York, New York, USA.

出版信息

HIV Med. 2025 Jan;26(1):17-25. doi: 10.1111/hiv.13700. Epub 2024 Aug 25.

Abstract

OBJECTIVES

Fostemsavir is a novel attachment inhibitor used with other antiretrovirals in heavily treatment-experienced (HTE) adults with multidrug-resistant HIV-1. Real-world immunological and virological responses were assessed in individuals starting fostemsavir in the OPERA cohort.

METHODS

Among adults with HIV-1 starting fostemsavir between 2 July 2020 and 1 September 2022, 6-month and 12-month changes in CD4 T-cell count and CD4%, and maintenance/achievement of viral load (VL) <50 copies/mL were described and stratified by baseline VL (suppressed: <50 copies/mL; viraemic: ≥50 copies/mL) and CD4 count (high: ≥350 cells/μL; low: <350 cells/μL).

RESULTS

Of 182 individuals starting fostemsavir, 64% were viraemic (34% low CD4, 30% high CD4) and 36% were suppressed (16% low CD4, 20% high CD4). The suppressed/low CD4 group had the largest median increases in CD4 count (6-month: 30 cells/μL [interquartile range {IQR} 9-66], 12-month: 66 cells/μL [IQR 17-125]), and CD4% (6-month: 1.0% [IQR -0.3-2.8], 12-month: 1.9% [IQR 1.3-3.9]). Regardless of baseline VL, those with a high baseline CD4 count experienced a greater variability in immunological response than those with low CD4 counts (12-month standard deviation range 172-231 cells/μL vs. 69-90 cells/μL). VL <50 copies/mL was maintained in most suppressed individuals; nearly half of the viraemic/high CD4 group and a third of the viraemic/low CD4 group achieved a VL <50 copies/mL at either timepoint.

CONCLUSIONS

After 6 or 12 months of fostemsavir use, virological response was low in viraemic individuals, although most suppressed individuals did maintain suppression. While immunological response varied across individuals, virologically suppressed HTE individuals with low CD4 counts may benefit from immunological improvements with fostemsavir.

摘要

目的

福斯特韦尔是一种新型附着抑制剂,与其他抗逆转录病毒药物联合用于治疗经历丰富(HTE)的多重耐药HIV-1成年患者。在OPERA队列中开始使用福斯特韦尔的个体中评估了实际的免疫和病毒学反应。

方法

在2020年7月2日至2022年9月1日期间开始使用福斯特韦尔的HIV-1成年患者中,描述了CD4 T细胞计数和CD4%在6个月和12个月时的变化,以及病毒载量(VL)维持/达到<50拷贝/mL的情况,并根据基线VL(抑制:<50拷贝/mL;病毒血症:≥50拷贝/mL)和CD4计数(高:≥350细胞/μL;低:<350细胞/μL)进行分层。

结果

在182名开始使用福斯特韦尔的个体中,64%为病毒血症患者(34% CD4低,30% CD4高),36%为病毒抑制患者(16% CD4低,20% CD4高)。病毒抑制/CD4低组的CD4计数中位数增加幅度最大(6个月:30细胞/μL [四分位间距{IQR} 9 - 66],12个月:66细胞/μL [IQR 17 - 125]),CD4%增加幅度也最大(6个月:1.0% [IQR -0.3 - 2.8],12个月:1.9% [IQR 1.3 - 3.9])。无论基线VL如何,基线CD4计数高的个体免疫反应的变异性都比CD4计数低的个体更大(12个月标准差范围172 - 231细胞/μL对69 - 90细胞/μL)。大多数病毒抑制个体维持VL<50拷贝/mL;在两个时间点,近一半的病毒血症/CD4高组和三分之一的病毒血症/CD4低组实现了VL<50拷贝/mL。

结论

使用福斯特韦尔6个月或12个月后,病毒血症个体的病毒学反应较低,尽管大多数病毒抑制个体确实维持了病毒抑制。虽然免疫反应因人而异,但病毒学抑制的HTE且CD4计数低的个体可能会从福斯特韦尔带来的免疫改善中获益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9ca5/11725415/6839d9346dd0/HIV-26-17-g001.jpg

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