Severe malaria in children leads to a significant impairment of transitory otoacoustic emissions--a prospective multicenter cohort study.

Joachim Schmutzhard,Patrick Zorowka,Allan Otieno,Natalie Fischer,Benjamin Mordmüller,Raimund Helbok,Peter Lackner,Lukas Oberhammer,Sanjeev Krishna,Erich Schmutzhard,Fabian Cedric Aregger,Josua Kegele,Saadou Issifou,Tsiri Agbenyega,Leyla Pinggera,Veronika Muigg,Sebastian Bunk,Bernards Ogutu,Daniel Ansong,Helene Hurth ,Ayôla Akim Adegnika ,Peter G Kremsner

doi:10.1186/s12916-015-0366-8

Abstract

BackgroundSevere malaria may influence inner ear function, although this possibility has not been examined prospectively. In a retrospective analysis, hearing impairment was found in 9 of 23 patients with cerebral malaria. An objective method to quickly evaluate the function of the inner ear are the otoacoustic emissions. Negative transient otoacoustic emissions are associated with a threshold shift of 20 dB and above.MethodsThis prospective multicenter study analyses otoacoustic emissions in patients with severe malaria up to the age of 10 years. In three study sites (Ghana, Gabon, Kenya) 144 patients with severe malaria and 108 control children were included. All malaria patients were treated with parental artesunate.ResultsIn the control group, 92.6 % (n = 108, 95 % confidence interval 86.19–6.2 %) passed otoacoustic emission screening. In malaria patients, 58.5 % (n = 94, malaria vs controls p < 0.001, 95 % confidence interval 48.4–67.9 %) passed otoacoustic emission screening at the baseline measurement. The value increased to 65.2 % (n = 66, p < 0.001, 95 % confidence interval 53.1–75.5 %) at follow up 14–28 days after diagnosis of malaria.The study population was divided into severe non-cerebral malaria and severe malaria with neurological symptoms (cerebral malaria). Whereas otoacoustic emissions in severe malaria improved to a passing percentage of 72.9 % (n = 48, 95 % confidence interval 59–83.4 %) at follow-up, the patients with cerebral malaria showed a drop in the passing percentage to 33 % (n = 18) 3–7 days after diagnosis. This shows a significant impairment in the cerebral malaria group (p = 0.012 at days 3–7, 95 % confidence interval 16.3–56.3 %; p = 0.031 at day 14–28, 95 % confidence interval 24.5–66.3 %).ConclusionThe presented data show that 40 % of children have involvement of the inner ear early in severe malaria. In children, audiological screening after severe malaria infection is not currently recommended, but is worth investigating in larger studies.

Highlights

Severe malaria may influence inner ear function, this possibility has not been examined prospectively
The present study shows that severe non-cerebral and cerebral malaria [23] may lead to a significant impairment of the inner ear function in the acute stage of the disease
Our results suggest that artemisinin does not influence inner ear function in patients with severe malaria, because the recorded otoacoustic impairment was present prior to the first treatment and did gradually improve

Summary

Introduction

Severe malaria may influence inner ear function, this possibility has not been examined prospectively. In an artemisinin combination therapy trial in children aged 0.5–-14 years, uncomplicated malaria has been suspected to be the cause of elevated hearing thresholds. Prior to therapy, hearing thresholds in children with malaria were significantly higher than those seen in the control group [8]. Carter et al suspected severe malaria to be a cause of acquired language disorders [9]. In children, hearing impairment is one of the fundamental causes of language and developmental disorders. Nine out of 23 children with cerebral malaria had impaired hearing in addition to other neurological and cognitive sequelae [10]. No prospective study evaluating hearing with objective tests has been performed for severe malaria

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