Nanostructured lipid carriers of artemether-lumefantrine combination for intravenous therapy of cerebral malaria
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- 作者:Priyanka Prabhua ; Shital Suryavanshib ; Sulabha Pathakb ; Aditya Patrab ; Shobhona Sharmab ; Vandana Patravalea ; vbp_muict@yahoo.co.in" class="auth_mail" title="E-mail the corresponding author ; vb.patravale@ictmumbai.edu.in" class="auth_mail" title="E-mail the corresponding author
- 关键词:Artemether ; Lumefantrine ; Nanostructured lipid carriers ; Intravenous ; Cerebral malaria ; Plasmodium
- 刊名:International Journal of Pharmaceutics
- 出版年:2016
- 出版时间:20 November 2016
- 年:2016
- 卷:513
- 期:1-2
- 页码:504-517
- 全文大小:5392 K
文摘
Patients with cerebral malaria (CM) are unable to take oral medication due to impaired consciousness and vomiting thus necessitating parenteral therapy. Quinine, artemether, and artesunate which are currently used for parenteral malaria therapy have their own drawbacks. The World Health Organization (WHO) has now banned monotherapy and recommends artemisinin-based combination therapy for malaria treatment. However, presently there is no intravenous formulation available for combination therapy of malaria. Artemether–Lumefantrine (ARM–LFN) is a WHO approved combination for oral malaria therapy. However, the low aqueous solubility of ARM and LFN hinders their intravenous delivery. The objective of this study was to formulate ARM–LFN nanostructured lipid carriers (NLC) for intravenous therapy of CM. ARM–LFN NLC were prepared by microemulsion template technique and characterized for size, drug content, entrapment efficiency, drug release, crystallinity, morphology, amenability to autoclaving, compatibility with infusion fluids, stability, antimalarial efficacy in mice, and toxicity in rats. The ARM–LFN NLC showed sustained drug release, amenability to autoclaving, compatibility with infusion fluids, good stability, complete parasite clearance and reversal of CM symptoms with 100% survival in Plasmodium berghei-infected mice, and safety in rats. The biocompatible ARM–LFN NLC fabricated by an industrially feasible technique offer a promising solution for intravenous therapy of CM.