Preclinical Evaluation of Long-Acting Emtricitabine Semi-Solid Prodrug Nanoparticle Formulations

Paul Curley; James J. Hobson; Neill J. Liptrott; Edward Makarov; Amer Al-khouja; Lee Tatham; Christopher A.W. David; Helen Box; Megan Neary; Joanne Sharp; Henry Pertinez; David Meyers; Charles Flexner; Caren L. Freel Meyers; Larisa Poluektova; Steve Rannard; Andrew Owen

doi:10.3390/pharmaceutics15071835

Preclinical Evaluation of Long-Acting Emtricitabine Semi-Solid Prodrug Nanoparticle Formulations

Paul Curley, James J. Hobson, Neill J. Liptrott, Edward Makarov, Amer Al-khouja, Lee Tatham, Christopher A.W. David, Helen Box, Megan Neary, Joanne Sharp, Henry Pertinez, David Meyers, Charles Flexner, Caren L. Freel Meyers, Larisa Poluektova, Steve Rannard, Andrew Owen

Pharmacology & Experimental Neuroscience (PEN)

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

Long-acting injectable (LAI) formulations promise to deliver patient benefits by overcoming issues associated with non-adherence. A preclinical assessment of semi-solid prodrug nanoparticle (SSPN) LAI formulations of emtricitabine (FTC) is reported here. Pharmacokinetics over 28 days were assessed in Wistar rats, New Zealand white rabbits, and Balb/C mice following intramuscular injection. Two lead formulations were assessed for the prevention of an HIV infection in NSG-cmah^−/− humanised mice to ensure antiviral activities were as anticipated according to the pharmacokinetics. Cmax was reached by 12, 48, and 24 h in rats, rabbits, and mice, respectively. Plasma concentrations were below the limit of detection (2 ng/mL) by 21 days in rats and rabbits, and 28 days in mice. Mice treated with SSPN formulations demonstrated undetectable viral loads (700 copies/mL detection limit), and HIV RNA remained undetectable 28 days post-infection in plasma, spleen, lung, and liver. The in vivo data presented here demonstrate that the combined prodrug/SSPN approach can provide a dramatically extended pharmacokinetic half-life across multiple preclinical species. Species differences in renal clearance of FTC mean that longer exposures are likely to be achievable in humans than in preclinical models.

Original language	English (US)
Article number	1835
Journal	Pharmaceutics
Volume	15
Issue number	7
DOIs	https://doi.org/10.3390/pharmaceutics15071835
State	Published - Jul 2023

Keywords

HIV
emtricitabine
long-acting
nano
pre-exposure prophylaxis

ASJC Scopus subject areas

Pharmaceutical Science

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10.3390/pharmaceutics15071835

Cite this

Curley, P., Hobson, J. J., Liptrott, N. J., Makarov, E., Al-khouja, A., Tatham, L., David, C. A. W., Box, H., Neary, M., Sharp, J., Pertinez, H., Meyers, D., Flexner, C., Freel Meyers, C. L., Poluektova, L., Rannard, S., & Owen, A. (2023). Preclinical Evaluation of Long-Acting Emtricitabine Semi-Solid Prodrug Nanoparticle Formulations. Pharmaceutics, 15(7), Article 1835. https://doi.org/10.3390/pharmaceutics15071835

Curley, P, Hobson, JJ, Liptrott, NJ, Makarov, E, Al-khouja, A, Tatham, L, David, CAW, Box, H, Neary, M, Sharp, J, Pertinez, H, Meyers, D, Flexner, C, Freel Meyers, CL, Poluektova, L, Rannard, S & Owen, A 2023, 'Preclinical Evaluation of Long-Acting Emtricitabine Semi-Solid Prodrug Nanoparticle Formulations', Pharmaceutics, vol. 15, no. 7, 1835. https://doi.org/10.3390/pharmaceutics15071835

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Preclinical Evaluation of Long-Acting Emtricitabine Semi-Solid Prodrug Nanoparticle Formulations

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Keywords

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