Effectiveness of rectal artesunate as pre-referral treatment for severe malaria in children <5 years of age

Author:

Hetzel Manuel W.ORCID,Okitawutshu JeanORCID,Tshefu AntoinetteORCID,Omoluabi ElizabethORCID,Awor PhyllisORCID,Signorell AitaORCID,Brunner Nina C.ORCID,Kalenga Jean-Claude,Akano Babatunde,Ayodeji Kazeem,Okon Charles,Yusuf Ocheche,Athieno Proscovia,Kimera Joseph,Tumukunde GloriaORCID,Angiro Irene,Delvento Giulia,Lee Tristan,Lambiris MarkORCID,Kwiatkowski Marek,Cereghetti Nadja,Visser TheodoorORCID,Napier Harriet G.,Cohen Justin M.ORCID,Buj Valentina,Burri ChristianORCID,Lengeler Christian

Abstract

AbstractBackgroundTo prevent child deaths from severe malaria, early parenteral treatment is essential. Yet, in remote rural areas, higher-level facilities offering parenteral antimalarials are often difficult to access. A randomised controlled trial found pre-referral rectal artesunate (RAS) to reduce death and disability in children who delay arriving at a referral facility. This study examined the effectiveness of pre-referral RAS treatment in established community-based health care systems.MethodsAn observational study accompanied the roll-out of RAS in the Democratic Republic of the Congo, Nigeria and Uganda. Children < 5 years presenting to a community-based health provider with a positive malaria test and signs of severe malaria were followed-up during admission and after 28 days to assess their health status and treatment history. The primary outcome was death; covariates of interest included RAS use, referral completion, and post-referral treatment.FindingsPost-roll-out, RAS was administered to 88% of patients in DRC, 52% in Nigeria, and 70% in Uganda. The overall case fatality rate (CFR) was 6.7% (135/2011) in DRC, 11.7% (69/589) in Nigeria, and 0.5% (19/3686) in Uganda; 865/6286 patients were sick at follow-up. In all countries, the CFR was higher after RAS-roll-out (6.7 vs. 6.6% in DRC, 16.1 vs. 4.2% in Nigeria, 0.7 vs. 0.3% in Uganda). In DRC and Nigeria, children receiving RAS were more likely to die than those not receiving RAS (aOR = 3.31, 95% CI 1.43-7.65 and aOR = 2.42, 95% CI 1.25-4.70, respectively). In Uganda, RAS users were less likely to be dead or sick at follow-up (aOR = 0.61, 95% CI 0.46-0.80). Post-referral parenteral antimalarials were protective in all countries; however, the effect of ACT administration was inconsistent.InterpretationRAS pre-referral treatment had no beneficial effect on child survival in three highly malaria endemic settings. RAS is unlikely to reduce malaria deaths unless health system shortfalls such as referral and post-referral treatment are addressed.

Publisher

Cold Spring Harbor Laboratory

Reference26 articles.

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