Population Pharmacokinetics of Pediatric Lopinavir/Ritonavir Oral Pellets in Children Living with HIV in Africa

Author:

Chupradit Suthunya1ORCID,Wamalwa Dalton C.2ORCID,Maleche‐Obimbo Elizabeth2ORCID,Kekitiinwa Adeodata R.3ORCID,Mwanga‐Amumpaire Juliet4ORCID,Bukusi Elizabeth A.5ORCID,Nyandiko Winstone M.6ORCID,Mbuthia Joseph K.7ORCID,Swanson Alistair8910ORCID,Cressey Tim R.1112ORCID,Punyawudho Baralee13ORCID,Musiime Victor1415ORCID, ,

Affiliation:

1. PhD's Degree Program in Pharmacy, Faculty of Pharmacy Chiang Mai University Chiang Mai Thailand

2. Department of Paediatrics and Child Health University of Nairobi Nairobi Kenya

3. Baylor College of Medicine Children's Foundation Kampala Uganda

4. Epicentre Mbarara Uganda

5. Centre for Microbiology Research, Kenya Medical Research Institute Kisumu Kenya

6. Department of Child Health and Paediatrics – Moi University AMPATH and Moi Teaching and Referral Hospital Eldoret Kenya

7. Gertrude's Children's Hospital Nairobi Kenya

8. Drugs for Neglected Diseases Initiative Geneva Switzerland

9. Drugs for Neglected Diseases Initiative Nairobi Kenya

10. Drugs for Neglected Diseases Initiative Bethesda Maryland USA

11. AMS‐PHPT Research Collaboration, Faculty of Associated Medical Sciences Chiang Mai University Chiang Mai Thailand

12. Department of Molecular & Clinical Pharmacology University of Liverpool Liverpool UK

13. Department of Pharmaceutical Care, Faculty of Pharmacy Chiang Mai University Chiang Mai Thailand

14. Joint Clinical Research Centre Kampala Uganda

15. Department of Paediatrics and Child Health Makerere University Kampala Uganda

Abstract

Antiretroviral therapy for children living with HIV (CLHIV) under 3 years of age commonly includes lopinavir/ritonavir (LPV/r). However, the original liquid LPV/r formulation has taste and cold storage difficulties. To address these challenges, LPV/r oral pellets have been developed. These pellets can be mixed with milk or food for administration and do not require refrigeration. We developed the population pharmacokinetic (PK) model and assessed drug exposure of LPV/r oral pellets administered twice daily to CLHIV per World Health Organization (WHO) weight bands. The PK analysis included Kenyan and Ugandan children participating in the LIVING studies (NCT02346487) receiving LPV/r pellets (40/10 mg) and ABC/3TC (60/30 mg) dispersible tablets. Population PK models were developed for lopinavir (LPV) and ritonavir (RTV) to evaluate the impact of RTV on the oral clearance (CL/F) of LPV. The data obtained from the study were analyzed using nonlinear mixed‐effects modeling approach. Data from 514 children, comprising a total of 2,998 plasma concentrations of LPV/r were included in the analysis. The LPV and RTV concentrations were accurately represented by a one‐compartment model with first‐order absorption (incorporating a lag‐time) and elimination. Body weight influenced LPV and RTV PK parameters. The impact of RTV concentrations on the CL/F of LPV was characterized using a maximum effect model. Simulation‐predicted target LPV exposures were achieved in children with this pellet formulation across the WHO weight bands. The LPV/r pellets dosed in accordance with WHO weight bands provide adequate LPV exposures in Kenyan and Ugandan children weighing 3.0 to 24.9 kg.

Publisher

Wiley

Subject

Pharmacology (medical),Pharmacology

Reference26 articles.

1. Acceptability of lopinavir/r pellets (minitabs), tablets and syrups in HIV-infected children

2. Oral abstracts of the 22nd international AIDS conference, 23–27 July 2018, Amsterdam, The Netherlands;Andrieux‐Meyer I.;J. Int. AIDS Soc.,2018

3. The Pharmacokinetics and Acceptability of Lopinavir/Ritonavir Minitab Sprinkles, Tablets, and Syrups in African HIV-Infected Children

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