Improved antimalarial activity of caprol-based nanostructured lipid carriers encapsulating artemether-lumefantrine for oral administration

Paul Achile Akpa; Joseph Abuchi Ugwuoke; Anthony Amaechi Attama; Chinenye Nnenna Ugwu; Ezinwanne Nneoma Ezeibe; Mumuni Audu Momoh; Adaeze Chidiebere Echezona; Franklin Chimaobi Kenechukwu

doi:10.4314/ahs.v20i4.20

Improved antimalarial activity of caprol-based nanostructured lipid carriers encapsulating artemether-lumefantrine for oral administration

Afr Health Sci. 2020 Dec;20(4):1679-1697. doi: 10.4314/ahs.v20i4.20.

Authors

Paul Achile Akpa¹, Joseph Abuchi Ugwuoke¹, Anthony Amaechi Attama¹, Chinenye Nnenna Ugwu², Ezinwanne Nneoma Ezeibe², Mumuni Audu Momoh¹, Adaeze Chidiebere Echezona¹, Franklin Chimaobi Kenechukwu¹

Affiliations

¹ Department of Pharmaceutics, University of Nigeria, Nsukka.
² Department of Pharmaceutical Microbiology and Biotechnology, University of Nigeria, Nsukka.

Abstract

Background: Artemether and lumefantrine display low aqueous solubility leading to poor release profile; hence the need for the use of lipid-based systems to improve their oral bioavailability so as to improve their therapeutic efficacy.

Aim and objective: The objective of this work was to utilize potentials of nanostructured lipid carriers (NLCs) for improvement of the oral bioavailability of artemether and lumefantrine combination and to evaluate its efficacy in the treatment of malaria. This study reports a method of formulation, characterization and evaluation of the therapeutic efficacies of caprol-based NLC delivery systems with artemether and lumefantrine.

Method: The artemether-lumefantrine co-loaded NLCs were prepared using the lipid matrix (5% w/w) (containing beeswax and Phospholipon® 90H and Caprol-PGE 860), artemether (0.1%w/w) and lumefantrine (0.6%w/w), sorbitol (4%w/w), Tween® 80(2%w/w as surfactant) and distilled water (q.s to 100%) by high shear homogenization and evaluated for physicochemical performance. The in vivo antimalarial activities of the NLC were tested in chloroquine-sensitive strains of Plasmodium berghei (NK-65) using Peter´s 4-day suppressive protocol in mice and compared with controls. Histopathological studies were also carried out on major organs implicated in malaria.

Results: The NLC showed fairly polydispersed nano-sized formulation (z-average:188.6 nm; polydispersity index, PDI=0.462) with no major interaction occurring between the components while the in vivo study showed a gradual but sustained drug release from the NLC compared with that seen with chloroquine sulphate and Coartem®. Results of histopathological investigations also revealed more organ damage with the untreated groups than groups treated with the formulations.

Conclusion: This study has shown the potential of caprol-based NLCs for significant improvement in oral bioavailability and hence antimalarial activity of poorly soluble artemether and lumefantrine. Importantly, this would improve patient compliance due to decrease in dosing frequency as a sustained release formulation.

Keywords: Caprol; Nanostructured lipid carriers; artemether-lumefantrine; malaria.

MeSH terms

Administration, Oral
Animals
Antimalarials / administration & dosage*
Antimalarials / pharmacology*
Artemether, Lumefantrine Drug Combination / administration & dosage*
Artemether, Lumefantrine Drug Combination / pharmacology*
Biological Availability
Humans
Lipids
Malaria / drug therapy*
Mice
Nanostructures / administration & dosage
Nanostructures / chemistry
Particle Size
Plasmodium berghei / drug effects*

Substances

Antimalarials
Artemether, Lumefantrine Drug Combination
Lipids