Simulation of metabolism-based herb-drug interaction: towards safe and efficacious use of NIPRD-AM1

Bulus Adzu; Kudirat Bola Mustapha; Collen Masimirembwa; Obiageri Obodozie; Rukaiyatu Abdullahi Kirim; Karniyus Shingu Gamaniel

Avicenna Journal of Phytomedicine (May 2013)

Simulation of metabolism-based herb-drug interaction: towards safe and efficacious use of NIPRD-AM1

Bulus Adzu,
Kudirat Bola Mustapha,
Collen Masimirembwa,
Obiageri Obodozie,
Rukaiyatu Abdullahi Kirim,
Karniyus Shingu Gamaniel

Affiliations

Bulus Adzu: Department of Pharmacology and Toxicology, National Institute for Pharmaceutical Research and Development, PMB 21, Abuja, Nigeria
Kudirat Bola Mustapha: Department of Medicinal Chemistry and Quality Control, National Institute for Pharmaceutical Research and Development, PMB 21, Abuja, Nigeria
Collen Masimirembwa: African Institute of Biomedical Science and Technology (AiBST), Cnr Chinhoyi Str./Jason Moyo Ave. No. 9 at LAPF Centre, Harare, Zimbabwe
Obiageri Obodozie: Department of Medicinal Chemistry and Quality Control, National Institute for Pharmaceutical Research and Development, PMB 21, Abuja, Nigeria
Rukaiyatu Abdullahi Kirim: Department of Medicinal Chemistry and Quality Control, National Institute for Pharmaceutical Research and Development, PMB 21, Abuja, Nigeria
Karniyus Shingu Gamaniel: Director General/Chief Executive Officer, National Institute for Pharmaceutical Research and Development, PMB 21, Abuja, Nigeria

Journal volume & issue: Vol. 3, no. 3
pp. 201 – 204

Abstract

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Objective: To evaluate the effect of NIPRD-AM1 on CYP3A4 in order to generate clinically significant data for its safe and efficacious use. Materials and Methods: NIPRD-AM1 is a phytomedicine developed from aqueous root extracts of Nauclea latifolia Smith (Rubiaceae) for the treatment of uncomplicated malaria. The effect of NIPRD-AM1 on CYP3A4 was measured with and without the addition of NIPRD-AM1, by testing different concentrations of the product at 37 °C in reactive mixtures with ketoconazole (2.5 µM) as the positive control. Results: Results showed a very low IC50 value of 0.01 mg/ml similar to that of ketoconazole (0.016 mg/ml). Conclusion: Metabolic processes of NIPRD-AM1 are likely to inhibit CYP3A4, with potential implication on drugs that are CYP3A4 substrates. This is a promising approach for guidance towards the safe and efficacious use of NIPRD-AM1.

Published in Avicenna Journal of Phytomedicine

ISSN: 2228-7930 (Print); 2228-7949 (Online)
Publisher: Mashhad University of Medical Sciences
Country of publisher: Iran, Islamic Republic of
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: http://ajp.mums.ac.ir/

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