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在有和没有感染艾滋病毒的成年人中,经大腿肌肉注射后卡博特韦的群体药代动力学。

Population pharmacokinetics of cabotegravir following intramuscular thigh injections in adults with and without HIV.

作者信息

Han Kelong, D'Amico Ronald D, Spreen William R, Ford Susan L

机构信息

GSK, Collegeville, Pennsylvania, USA.

ViiV Healthcare, Durham, North Carolina, USA.

出版信息

Antimicrob Agents Chemother. 2024 Dec 5;68(12):e0088024. doi: 10.1128/aac.00880-24. Epub 2024 Oct 23.

Abstract

Cabotegravir intramuscular gluteal injection is approved for HIV treatment (with rilpivirine) and prevention. Thigh muscle is a potential alternative injection site. We aim to characterize cabotegravir pharmacokinetics and its association with demographics following intramuscular thigh injection in comparison with gluteal injection using population pharmacokinetic (PPK) analysis. Fourteen HIV-negative participants received 600 mg single thigh injection in phase 1 study 208832 and 118 participants with HIV received thigh injections 400 mg monthly 4× or 600 mg once-every-2-months 2× after ≥3 years of gluteal injections in phase 3b study ATLAS-2M provided 1,249 cabotegravir concentrations from 366 thigh injections and 1,998 concentrations from 1,618 gluteal injections. The established gluteal PPK model was modified by adding thigh injection compartment and fit to pharmacokinetic data following both gluteal and thigh injections, enabling within-person comparison in ATLAS-2M. Gluteal parameters were fixed. Similar to the gluteal absorption rate constant (KA), the thigh absorption rate constant (KA) was slower in females than males and in participants with higher BMI. KA was strongly correlated with KA (correlation coefficient 0.766), best described by the additive linear relationship KA = KA + 0.0002527 h. Terminal half-life of thigh injection was 26% (male) and 39% (female) shorter than gluteal injection. Relative bioavailability of thigh to gluteal was estimated to be 89.9%. The impact of covariates on cabotegravir exposure following thigh injections was ≤35%. In conclusion, cabotegravir absorption following thigh injection was correlated with, faster than, and 10% less bioavailable than gluteal injection, and correlated with sex and BMI. The cabotegravir thigh PPK model can inform dosing strategies and future study design.

摘要

卡博特韦肌内臀肌注射已被批准用于HIV治疗(与利匹韦林联合)及预防。大腿肌肉是一个潜在的替代注射部位。我们旨在通过群体药代动力学(PPK)分析,比较肌内大腿注射与臀肌注射后卡博特韦的药代动力学特征及其与人口统计学的关系。14名HIV阴性参与者在1期研究208832中接受了600mg单次大腿注射,118名HIV感染者在3b期研究ATLAS-2M中,在进行了≥3年的臀肌注射后,每月接受400mg大腿注射4次,或每2个月接受600mg大腿注射2次。研究提供了来自366次大腿注射的1249个卡博特韦浓度数据以及来自1618次臀肌注射的1998个浓度数据。通过添加大腿注射房室对已建立的臀肌PPK模型进行修改,并使其适用于臀肌和大腿注射后的药代动力学数据,从而能够在ATLAS-2M中进行个体内比较。臀肌参数保持不变。与臀肌吸收速率常数(KA)类似,女性和BMI较高的参与者的大腿吸收速率常数(KA)比男性慢。KA与KA高度相关(相关系数0.766),最佳描述为加性线性关系KA = KA + 0.0002527 h。大腿注射的终末半衰期比臀肌注射短26%(男性)和39%(女性)。大腿注射相对于臀肌注射的相对生物利用度估计为89.9%。协变量对大腿注射后卡博特韦暴露的影响≤35%。总之,大腿注射后卡博特韦的吸收与臀肌注射相关,比臀肌注射更快,生物利用度低10%,且与性别和BMI相关。卡博特韦大腿PPK模型可为给药策略和未来研究设计提供参考。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0031/11619381/6a5e320f14e2/aac.00880-24.f001.jpg

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