TY - JOUR
T1 - Bioavailability of three novel oral, sustained-release pellets, relative to an immediate-release tablet containing 500 mg flucytosine
T2 - A randomized, open-label, crossover study in healthy volunteers
AU - Goyal, Vishal
AU - Krantz, Edrich
AU - Simon, Francois
AU - Neven, Anouk
AU - Eriksson, Johanna
AU - Saayman, Amaria
AU - Ibnou Zekri Lassout, Nabila
AU - Louis, Mathieu
AU - Robinson, Stephen
AU - Deshmukh, Abhijit
AU - Antarkar, Amit
AU - Ruffell, Carol
AU - Victor, Sarika
AU - Chenel, Marylore
AU - Celebic, Aljosa
AU - Caplain, Henri
AU - Gillon, Jean Yves
AU - Ribeiro, Isabela
N1 - FUNDING INFORMATION
The study was funded through Drugs for Neglected Diseases initiative and supported by grants from the European and Developing Countries Clinical Trials Partnership Association (EDCTP2) programme supported by the European Union (grant RIA2018CO-2516); Médecins Sans Frontières International; Swiss Agency for Development and Cooperation (SDC), Switzerland; and other private foundations and individuals.
Publisher Copyright:
© 2024 DNDI. Luxembourg Institute of Health. Pharmetheus AB. Mylan Laboratories Ltd. FARMOVS (Pty) Ltd and The Authors. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.
PY - 2024/3
Y1 - 2024/3
N2 - The opportunistic fungal infection cryptococcal meningoencephalitis is a major cause of death among people living with HIV in sub-Saharan Africa. We report pharmacokinetic (PK) and safety data from a randomized, four-period crossover phase I trial of three sustained-release (SR) oral pellet formulations of 5-flucytosine conducted in South Africa. These formulations were developed to require less frequent administration, to provide a convenient alternative to the current immediate release (IR) formulation, A. Formulations B, C, and D were designed to release 5-flucytosine as a percentage of the nominal dose in vitro. We assessed their safety and PK profiles in a single dose (1 × 3000 mg at 0 h), relative to commercial IR tablets (Ancotil 500 mg tablets; 3 × 500 mg at 0 h and 3 × 500 mg at 6 h) in healthy, fasted participants. Forty-two healthy participants were included. All treatments were well-tolerated. The primary PK parameters, maximum observed plasma concentration (Cmax) and area under the concentration-time profiles, were significantly lower for the SR formulations than for the IR tablets, and the geometric mean ratios fell outside the conventional bioequivalence limits. The median maximum time to Cmax was delayed for the SR pellets. Physiologically-based PK modeling indicated a twice-daily 6400 mg dose of SR formulation D in fasted condition would be optimal for further clinical development. This regimen is predicted to result in a rapid steady-state plasma exposure with effective and safe trough plasma concentration and Cmax values, within the therapeutic boundaries relative to plasma exposure after four times per day administration of IR tablets (PACTR202201760181404).
AB - The opportunistic fungal infection cryptococcal meningoencephalitis is a major cause of death among people living with HIV in sub-Saharan Africa. We report pharmacokinetic (PK) and safety data from a randomized, four-period crossover phase I trial of three sustained-release (SR) oral pellet formulations of 5-flucytosine conducted in South Africa. These formulations were developed to require less frequent administration, to provide a convenient alternative to the current immediate release (IR) formulation, A. Formulations B, C, and D were designed to release 5-flucytosine as a percentage of the nominal dose in vitro. We assessed their safety and PK profiles in a single dose (1 × 3000 mg at 0 h), relative to commercial IR tablets (Ancotil 500 mg tablets; 3 × 500 mg at 0 h and 3 × 500 mg at 6 h) in healthy, fasted participants. Forty-two healthy participants were included. All treatments were well-tolerated. The primary PK parameters, maximum observed plasma concentration (Cmax) and area under the concentration-time profiles, were significantly lower for the SR formulations than for the IR tablets, and the geometric mean ratios fell outside the conventional bioequivalence limits. The median maximum time to Cmax was delayed for the SR pellets. Physiologically-based PK modeling indicated a twice-daily 6400 mg dose of SR formulation D in fasted condition would be optimal for further clinical development. This regimen is predicted to result in a rapid steady-state plasma exposure with effective and safe trough plasma concentration and Cmax values, within the therapeutic boundaries relative to plasma exposure after four times per day administration of IR tablets (PACTR202201760181404).
UR - http://www.scopus.com/inward/record.url?scp=85187969045&partnerID=8YFLogxK
UR - https://pubmed.ncbi.nlm.nih.gov/38488418
U2 - 10.1111/cts.13756
DO - 10.1111/cts.13756
M3 - Article
C2 - 38488418
AN - SCOPUS:85187969045
SN - 1752-8054
VL - 17
JO - Clinical and Translational Science
JF - Clinical and Translational Science
IS - 3
M1 - e13756
ER -