Artesunate to Treat Severe Malaria in Travellers: Review of Efficacy and Safety and Practical Implications

Overview

Journal J Travel Med

Publisher Oxford University Press

Specialties Infectious Diseases
Public Health

Date 2017 Apr 11

PMID 28395097

Citations 25

Authors

Camille Roussel

Eric Caumes

Marc Thellier

Papa Alioune Ndour

Pierre A Buffet

Stephane Jaureguiberry

Affiliations

Soon will be listed here.

Abstract

Background: Artesunate (AS) is the WHO first-line treatment of severe malaria in endemic countries, in adults and children. However, despite solid evidence that AS is safe and more effective than quinine in endemic areas, its deployment in non-endemic areas has been slow, due in part to the absence of a full good manufacturing practice (GMP) qualification (although prequalification has been granted in 2010). Prospective comparative trials were not conducted in travellers, but several retrospective studies and case reports are providing insights into the efficacy and safety of AS in imported severe malaria.

Methods: We performed a systematic review on AS use in non-endemic areas for the treatment of imported severe malaria, using the Prisma method for bibliographic reports. Post-AS delayed haemolysis (PADH) was defined by delayed haemolytic episodes occurring 7-30 days after treatment initiation. We summarized prescription guidelines and generated answers to frequently asked questions regarding the use of AS in travellers with severe malaria.

Results: We analysed 12 retrospectives and 1 prospective study as well as 7 case reports of AS treatment in 624 travellers. Of 574 patients with reported outcome, 23 died (4%). No death was attributed to AS toxicity. Non-haematological side effects were uncommon and mainly included mild hepatitis, neurological, renal, cutaneous and cardiac manifestations. PADH occurred in 15% of the treated patients. No death or sequelae were reported. Overall blood transfusion was administered in 50% of travellers with PADH.

Conclusion: AS is highly efficacious in travellers with severe malaria. The frequency of PADH supports the need of weekly follow-up of haematological parameters during 1 month. Full GMP qualification for the drug and rapid approval by drug agencies is warranted, backed by clear recommendations for optimal use.

Citing Articles

Artesunate protects against a mouse model of cerulein and lipopolysaccharide‑induced acute pancreatitis by inhibiting TLR4‑dependent autophagy.

Liu D, Liu C, Deng F, Ouyang F, Qin R, Zhai Z Int J Mol Med. 2024; 55(2).

PMID: 39635846 PMC: 11637502. DOI: 10.3892/ijmm.2024.5466.

Acute Kidney Injury and Post-Artesunate Delayed Haemolysis in the Course of Malaria.

Kubanek A, Sulima M, Szydlowska A, Sikorska K, Renke M Pathogens. 2024; 13(10).

PMID: 39452723 PMC: 11509981. DOI: 10.3390/pathogens13100851.

Artesunate improves learning and memory impairment in rats with vascular cognitive impairment by down-regulating the level of autophagy in cerebral cortex neurons.

Wei H, Wang X, Zhong H, Kong X, Zhu J, Li B Heliyon. 2024; 10(12):e33068.

PMID: 38948049 PMC: 11211894. DOI: 10.1016/j.heliyon.2024.e33068.

Artesunate Exerts Organ- and Tissue-Protective Effects by Regulating Oxidative Stress, Inflammation, Autophagy, Apoptosis, and Fibrosis: A Review of Evidence and Mechanisms.

Zhu M, Wang Y, Han J, Sun Y, Wang S, Yang B Antioxidants (Basel). 2024; 13(6).

PMID: 38929125 PMC: 11200509. DOI: 10.3390/antiox13060686.

Another Use for a Proven Drug: Experimental Evidence for the Potential of Artemisinin and Its Derivatives to Treat Alzheimer's Disease.

Kiss E, Kins S, Gorgas K, Venczel Szakacs K, Kirsch J, Kuhse J Int J Mol Sci. 2024; 25(8).

PMID: 38673751 PMC: 11049906. DOI: 10.3390/ijms25084165.