In vivo antimalarial activity of stem bark extracts of <em>Plumeria alba</em> against <em>Plasmodium berghei</em> in imprinting control region mice

Johnson Nyarko Boampong; Elvis Ofori Ameyaw; Samuel Kyei; Benjamin Aboagye; Kwame Asare; Richmond Afoakwah; Alex Boye; Jean Hubert Donfack

doi:10.2147/RIP.S45492

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In vivo antimalarial activity of stem bark extracts of Plumeria alba against Plasmodium berghei in imprinting control region mice

Authors Boampong JN, Ameyaw EO, Kyei S , Aboagye B, Asare K, Afoakwah R, Boye A, Donfack JH

Received 20 March 2013

Accepted for publication 13 June 2013

Published 21 October 2013 Volume 2013:3 Pages 19—25

DOI https://doi.org/10.2147/RIP.S45492

Checked for plagiarism Yes

Review by Single anonymous peer review

Peer reviewer comments 3

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Johnson Nyarko Boampong,¹Elvis Ofori Ameyaw,¹ Samuel Kyei,² Benjamin Aboagye,¹ Kwame Asare,¹ Richmond Afoakwah,¹ Alex Boye,³ Jean Hubert Donfack⁴
¹Department of Biomedical and Forensic Sciences, School of Biological Sciences, ²Department of Optometry, School of Physical Sciences, ³Department of Laboratory Technology, School of Physical Sciences, University of Cape Coast, Cape Coast, Ghana; ⁴Department of Biomedical Sciences, Faculty of Sciences, University of Dschang, Dschang, Cameroon

Background: The need for new antimalarial agents with a transcriptional mode of action but fewer side effects compared with artemisinin-based combination therapy for malaria has been the preoccupation of scientists in areas where malaria is a menace. Stem bark extracts of Plumeria alba, used traditionally for the treatment of malaria in Ghana, were investigated to evaluate their prophylactic and curative antimalarial properties.
Methods: The antimalarial properties of P. abla were probed using aqueous (30–300 mg/kg) and dichloromethane/methanol (30–300 mg/kg) extracts of the plant in imprinting control region mice infected with Plasmodium berghei. For the curative test, the extracts were administered to the infected mice 4 days post-infection. In the prophylactic test, the animals were pre-treated with the extracts for 3 days before challenging them with P. berghei infected erythrocytes.
Results: The aqueous extract exerted significant (P < 0.05–0.001) effects on P. berghei infection, similar to artemether and lumefantrine curatively and sulfadoxine/pyrimethamine prophylactically. However, the dichloromethane/methanol extract reduced the parasitemia curatively (P < 0.05–0.01) but not prophylactically.
Conclusion: This study provides evidence to support the antimalarial properties of stem bark extract of P. alba in mice.

Keywords: malaria, parasitemia, artemether, lumefantrine, sulfadoxine/pyrimethamine, Ghana

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