Population pharmacokinetic analysis of tesamorelin in HIV-infected patients and healthy subjects.

Clinical pharmacokinetics2015PMID: 25358450

View on PubMed DOI: 10.1007/s40262-014-0202-x

Randomized Controlled TrialTesamorelin

Plain Language Summary

Population pharmacokinetic analysis of tesamorelin using data from 38 HIV-infected patients and healthy subjects receiving 1–2 mg subcutaneous tesamorelin daily for 14 days, developing an open one-compartment PK model characterizing absorption, distribution, and elimination—establishing the first population-level PK model for this synthetic GHRH analog. Provides foundational tesamorelin PK data. Establishes the pharmacokinetic parameters governing tesamorelin's systemic exposure—including interindividual variability and the exposure-response relationship needed to understand dose selection, and providing a framework for evaluating dose adjustments in special populations.

Abstract

BACKGROUND AND OBJECTIVES: Tesamorelin is a synthetic analogue of growth hormone-releasing factor (GRF), which increases basal and pulsatile growth hormone (GH) secretion and subsequently increases insulin-like growth factor (IGF)-1. Limited information is available about the pharmacokinetics of this compound. Consequently, the aim of this study was to characterize the population pharmacokinetics of tesamorelin in HIV-infected patients and healthy subjects. METHODS: A total of 38 HIV-infected patients and healthy subjects receiving subcutaneous tesamorelin doses of 1 or 2 mg administered daily during 14 consecutive days were included in the analysis. An open one-compartment model with first- and zero-order absorption and first-order elimination was developed to best describe the data using NONMEM(®) VII. The effect of different covariates on tesamorelin pharmacokinetics was investigated. Model evaluation was performed using predictive checks and non-parametric bootstrap. RESULTS: Plasma clearance and its interindividual variability [% coefficient of variation (CV)] was estimated to be 1,060 L/h (33.6 %). Volume of distribution was calculated to be 200 L (17.7 %). Age, body size measures, race and health status were not related to tesamorelin pharmacokinetic parameters within the range of covariates studied. The fraction of tesamorelin absorbed by a first-order process is 13.1 % higher on day 14 compared with day 1. Predictive checks and non-parametric bootstrap demonstrated that the model is appropriate in describing the time course of tesamorelin plasma concentrations in both HIV-infected patients and healthy subjects. CONCLUSIONS: An open one-compartment model with first and zero order absorption processes and linear elimination is suitable to characterize the pharmacokinetics of tesamorelin. The fraction of tesamorelin absorbed by a first-order process evolves with time. No clinically relevant covariates were identified as predictors of tesamorelin pharmacokinetics.

Authors

González-Sales, Mario; Barrière, Olivier; Tremblay, Pierre Olivier; Nekka, Fahima; Mamputu, Jean-Claude; Boudreault, Sylvie; Tanguay, Mario