Neuropsychological sequelae of bacterial and viral meningitis

doi:10.1093/brain/awh711

Brain Advance Access originally published online on December 19, 2005
Brain 2006 129(2):333-345; doi:10.1093/brain/awh711

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Neuropsychological sequelae of bacterial and viral meningitis

H. Schmidt¹, B. Heimann³, M. Djukic¹, C. Mazurek¹, C. Fels², C.-W. Wallesch³ and R. Nau¹

Georg August University Göttingen ¹ Department of Neurology, ² Department of Neuroradiology, Robert-Koch-Street 40, D-37075 Göttingen and Otto von Guericke University of Magdeburg, ³ Department of Neurology, Magdeburg, Germany

Correspondence to: H. Schmidt, University of Göttingen, Department of Neurology, Robert-Koch-Street 40, 37099 Göttingen, Germany E-mail: hschmid2{at}gwdg.de

Survivors of meningitis often complain about neurological andneuropsychological consequences. In this study, the extent ofthese sequelae was quantified and correlated to MRI findings.Neurological, neuropsychological and neuroradiological examinationswere performed with adult patients younger than 70 years, 1–12years after recovery from bacterial meningitis (BM; n = 59),or from viral meningitis (VM; n = 59). Patients with other potentialcauses for neuropsychological deficits (e.g. alcoholism) werecarefully excluded. Patients were compared to 30 healthy subjectsadjusted for age, gender and length of school education. Withthe exception of attention functions, both patient groups showedmore frequently pathological results than the control groupfor all domains examined. Applying an overall cognitive sumscore, patients after BM did not differ significantly in theirperformance from patients after VM. Separate analyses of variouscognitive domains, however, revealed a higher rate of persistentdisturbances in short-term and working memory after BM thanafter VM. Moreover, patients after BM exhibited greater impairmentof executive functions. Associative learning of verbal materialwas also reduced. These deficits could not be ascribed to impairedalertness functions or decreased motivation in BM patients.Applying a logistic regression model, the neuropsychologicaloutcome was related to the neurological outcome. Patients witha Glasgow Outcome Scale (GOS) of <5 had more frequently impairedtest results for non-verbal learning and memory. GOS was alsocorrelated with performance in executive functions. Brain volumewas lower and ventricular volume was higher in the bacterialthan in the VM group, and cerebral volume and the amount ofwhite matter lesions of patients after BM were negatively correlatedwith short-term and working memory. In conclusion, patientsafter both BM and VM with favourable outcome showed affectedlearning and memory functions. More patients after BM than afterVM displayed pathological short-term and working memory. BMresulted in poorer performance in executive functions, language,short-term memory and verbal learning/memory tests. As a resultof neurological and neuropsychological sequelae, BM with a GOS $≥$ 4 led to decreased activities of daily living but only a minorityof patients were disabled in a way that social functions wereaffected. The extent of neuropsychological sequelae of BM mighthave been overestimated in earlier studies which often had notbeen controlled for comorbidity factors such as alcoholism.

Key Words: bacterial meningitis; viral meningitis; neuropsychological sequelae; neurological sequelae; MRI

Abbreviations: AAT = Aachen Aphasia Test; BM = bacterial meningitis; CVLT = California Verbal Learning Test; GCS = Glasgow Coma Scale; GOS = Glasgow Outcome Scale; HAWIE-R = Hamburg-Wechsler Intelligenztest für Erwachsene-R; SD = standard deviation; SNRS = Scripps Neurological Rating Scale; VM = viral meningitis; VV = ventricular volume; WMS-R = Wechsler Memory Scale-R

Received February 3, 2005. Revised October 20, 2005. Accepted November 3, 2005.

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