A prospective study of risk factors for neurological complications in childhood bacterial meningitis

Namani, Sadie; Milenković, Zvonko; Koci, Bulëza

doi:10.1016/j.jped.2012.10.001

Abstracts

OBJECTIVE: To prospectively analyze the prognostic factors for neurological complications of childhood bacterial meningitis. METHODS: This prospective study enrolled 77 children from 1 month until 16 years of age, treated for bacterial meningitis during the period of January 1, 2009 through December 31, 2010. 16 relevant predictors were chosen to analyze their association with the incidence of neurological complications. p-values < 0.05 were considered statistically significant. RESULTS: Of the 77 children treated for bacterial meningitis, 33 patients developed neurological complications (43%), and two children died (2.6%). The etiology of bacterial meningitis cases was proven in 57/77 (74%) cases: 32 meningococci, eight pneumococci, six Gram-negative bacilli, five H. influenzae, five staphylococci, and one S. viridans isolates were found. Factors found to be associated with increased risk of development of neurological complications were age < 12 months, altered mental status, seizures prior to admission, initial therapy with two antibiotics, dexamethasone use, presence of focal neurological deficit on admission and increased proteins in cerebrospinal fluid (CSF) (p < 0.05). Initial pleocytosis > 5,000 cells/mm³, pleocytosis > 5,000 cells/mm³ after 48 hours, CSF/blood glucose ratio < 0.20, female gender, previous treatment with antibiotics, community-acquired infection, duration of illness > 48 hours, presence of comorbidity, and primary focus of infection were not associated with increased risk for the development of neurological complications. CONCLUSION: Age < 12 months and severity of clinical presentation at admission were identified as the strongest predictors of neurological complications and may be of value in selecting patients for more intensive care and treatment.

Bacterial meningitis; Neurological complications; Children; Outcomes

OBJETIVO: Análise prospectiva de fatores de prognóstico para complicações neurológicas da meningite bacteriana infantil. MÉTODOS: Este estudo prospectivo recrutou 77 crianças de um mês a 16 anos de idade tratadas de meningite bacteriana durante o período de 1/1/2009 a 31/12/2010. Foram escolhidos 16 preditores relevantes para analisar sua associação com a incidência de complicações neurológicas. Valores P abaixo de 0,05 foram considerados estatisticamente significativos. RESULTADOS: Das 77 crianças tratadas para meningite bacteriana, desenvolveram-se complicações neurológicas em 33 pacientes (43%), e duas crianças morreram (2,6%). A etiologia dos casos de meningite bacteriana foi comprovada em 57/77 (74%) dos casos: foram encontrados 32 isolados de meningococos; 8 de pneumococos; 6 de bacilos gram-negativos; 5 de H. influenzae; 5 de estafilococos e 1 de S. viridans. Os fatores que se mostraram associados a aumento do risco de desenvolvimento de complicações neurológicas foram idade < 12 meses, alteração do estado mental, crises convulsivas antes da admissão, terapia inicial com dois antibióticos, uso de dexametasona, presença de déficit neurológico focal na admissão e aumento das proteínas do líquido cerebrospinal (LCS) (p < 0,05). Pleiocitose inicial > 5.000 células/mm³, pleiocitose > 5.000 células/mm³ depois de 48 horas, baixa relação da glicose no LCS/sangue < 0,20, gênero feminino, tratamento prévio com antibióticos, infecção adquirida na comunidade, duração da doença > 48 horas, presença de comorbidade e foco primário de infecção não se associaram a aumento do risco para o desenvolvimento de complicações neurológicas. CONCLUSÃO: Idade inferior a 12 meses e gravidade da apresentação clínica na admissão foram identificadas como os preditores mais fortes de complicações neurológicas e podem ter valor para selecionar pacientes para tratamento mais intensivo.

Meningite bacteriana; Complicações neurológicas; Crianças; Resultados

ORIGINAL ARTICLE

A prospective study of risk factors for neurological complications in childhood bacterial meningitis

Sadie Naman^I,^* * Corresponding author. E-mail: sadie_namani@yahoo.com (S. Namani). ; Zvonko Milenković^II; Bulëza Koci^III

^IPhD. Infectious Diseases Clinic, University Clinical Center of Kosovo, Medical Faculty, University of Prishtina, Kosovo

^IIPhD. Clinic for Infectious Diseases and Febrile Conditions, Skopje, R. Macedonia

^IIIMSc. Burg-Apotheke, Konigstein am Taunus, Germany

ABSTRACT

OBJECTIVE: To prospectively analyze the prognostic factors for neurological complications of childhood bacterial meningitis.

METHODS: This prospective study enrolled 77 children from 1 month until 16 years of age, treated for bacterial meningitis during the period of January 1, 2009 through December 31, 2010. 16 relevant predictors were chosen to analyze their association with the incidence of neurological complications. p-values < 0.05 were considered statistically significant.

RESULTS: Of the 77 children treated for bacterial meningitis, 33 patients developed neurological complications (43%), and two children died (2.6%). The etiology of bacterial meningitis cases was proven in 57/77 (74%) cases: 32 meningococci, eight pneumococci, six Gram-negative bacilli, five H. influenzae, five staphylococci, and one S. viridans isolates were found. Factors found to be associated with increased risk of development of neurological complications were age < 12 months, altered mental status, seizures prior to admission, initial therapy with two antibiotics, dexamethasone use, presence of focal neurological deficit on admission and increased proteins in cerebrospinal fluid (csf) (p << 0.05). Initial pleocytosis > 5,000 cells/mm³, pleocytosis > 5,000 cells/mm³ after 48 hours, CSF/blood glucose ratio < 0.20, female gender, previous treatment with antibiotics, community-acquired infection, duration of illness > 48 hours, presence of comorbidity, and primary focus of infection were not associated with increased risk for the development of neurological complications.

CONCLUSION: Age < 12 months and severity of clinical presentation at admission were identified as the strongest predictors of neurological complications and may be of value in selecting patients for more intensive care and treatment.

Keywords: Bacterial meningitis; Neurological complications; Children; Outcomes

Introduction

Despite the development of antibiotics that are more effective in treating bacterial meningitis, the mortality rates continue to be high, ranging between 5% and 30%, while as many as 50% of survivors experience neurological sequelae, such as hearing impairment, seizure disorders, and learning and behavioral problems.^1--12 The neurological complications resulting from bacterial meningitis include subdural effusions or empyemas, cerebral abscesses, focal neurological deficits (e.g., hearing loss, cranial nerve palsies, hemiparesis, or quadriparesis), hydrocephalus, cerebrovascular abnormalities, altered mental status, and seizures. Acute bacterial meningitis is more common in resource-poor than resource-rich settings.³ The occurrence of negative consequences of bacterial meningitis in developed countries is strongly reduced by vaccination strategies, antibiotic treatment, and good care facilities.^1,4,5 The speed of diagnosis, the identification of the causative pathogen, and the initial antimicrobial therapy represent important factors for the prognosis of bacterial meningitis in children. Developing countries such as Kosovo are still facing cases of bacterial meningitis in children due to non-implementation of vaccination programs against meningeal pathogens. Furthermore, the shortage of antibiotics in hospitals makes it difficult to follow guidelines for the initial empirical therapy of children with bacterial meningitis. Late and insufficient results of cerebrospinal fluid (CSF) cultures and Gram-staining make treatment more difficult, particularly in cases with neurological complications.

Material and methods

Children aged between 1 month and 16 years, treated for bacterial meningitis at the Infectious Diseases Clinic in Prishtina (University Clinical Center of Kosovo) during the period from January 1, 2009 to December 31, 2010 were prospectively enrolled in the study. The furthest distance from Prishtina is estimated to be < 100 km or 1.5 hour driving. 57 children had a confirmed bacterial etiology. 20 patients were treated for probable bacterial meningitis, based on world health organization (who) criteria: clinical signs and symptoms of meningitis, changes in csf, and lack of an identifiable bacterial pathogen. children who didn't fulfill the criteria for bacterial meningitis were excluded from the study. cases of tuberculous meningitis and neurobrucellosis, as well as patients younger than 1 month old were excluded from the study. the following procedure was performed on admission for every child with suspected bacterial meningitis: lumbar puncture, fluid analysis (cell count with differential, glucose, protein), gram-staining, and bacterial culture, repeated lps after 48 hours. the treatment was followed by laboratory analysis; evaluation by a neurologist, an ophthalmologist, and an ear, nose, and throat (ent) specialist; and brain imaging when indicated. the diagnosis of neurologic complications was made by neurologic examination, neuroimaging, electroencephalography, and by the evaluation of a neurologist, ophthalmologist, ent specialist, and psychologist. indications for performing a computed tomography (ct) of the head after meningitis were: prolonged fever, focal neurological deficit, convulsions, worsening consciousness level, prolonged cyto-biochemical changes in csf, or worsening of clinical presentation. the physicians of the ward for treatment of meningitis, including the first author, treated these children and performed a one-year follow up, which included routine visits to the clinic and consultations by phone. the initial antibiotic therapy was selected based on the clinical presentation of illness with prognostic factors for an unfavorable outcome (altered mental state, seizures, and neurologic deficit); the possible pathogen for each age group and the local antibiotic resistance patterns; duration of illness prior to admission; previous treatment with antibiotics; the presence of a primary infectious focus; the identification of a community-or hospital-acquired infection (shunt intervention, neurosurgery, etc.); presentation of petechial skin rash; underlying diseases; antibiotics available in the ward; and the financial resources of the parents.

Initial single-agent antibiotic therapy was used in 42 children (55%), mainly ceftriaxone (36/77, 47%), while 35 children (45%) were treated with initial dual-agent antibiotic therapy, mostly the combination of ceftriaxone with vancomycin (18/77, 23%). Dexamethasone was used in 66 children (86%), and criteria for its use were clinical presentation on admission, altered mental status, presence of seizures, or focal neurological deficit on admission.

In order to determine their association with the incidence of neurological complications of bacterial meningitis in children treated in this ward, 16 potentially relevant predictors were chosen to be analyzed. p-values < 0.05 were considered statistically significant. there were no missing data on the 16 variables collected from the medical records including: 1) age (which was later categorized into specific age groups); 2) gender; 3) duration of the patients^' illness prior to admission, < or > 48 hours; 4) previous treatment with antibiotics; 5) presence of altered mental status at the time of presentation; 6) presence of focal neurological deficits that occurred in the period between the start of symptoms and arrival at the admission room (cranial nerve involvement or hemiparesis/quadriparesis); 7) occurrence of seizures prior to admission; 8) initial single-or dual-agent antibiotic therapy; 9) use of dexamethasone; 10) presence/absence of a primary infectious focus; 11) presence/absence of comorbidity; 12) initial turbid CSF with pleocytosis > 5,000 cells/mm³ ; 13) pleocytosis > 5,000 cells/mm³ after 48 hoursl 14) CSF/blood glucose ratio < 0.20; 15) increased proteinorrhachia (> 0.50 g/L); and 16) whether the infection was communityor hospital-acquired. Good outcome was considered treatment without any obvious neurological complications at discharge, and adverse outcome was considered the manifestation of neurological complications during the course of illness, or death. There were only two death cases who manifested neurological complications (obstructive hydrocephalus and cerebral abscesses), thus both were included in the group of children with neurological complications. All children were followed-up for a minimum of 12 months.

This study was approved by the Ethic-Professional Committee of the University Clinical Center of Kosova.

Statistical analysis

Data were analyzed using Stata 7.1 and the Statistical Package for Social Sciences (SPSS) 13. The statistical parameters analyzed included structure index, mean, and standard deviation. p-values < 0.05 were considered statistically significant.

Results

During the two-year study period, 77 children aged between 1 month and 16 years (57 children < 6 years; 48/77 males) were treated for bacterial meningitis. 57 children had a confirmed bacterial etiology, as follows: 32, Neisseria meningitidis; eight, Streptococcus pneumoniae; six, Gramnegative bacilli (three P. aeruginosa, two E. coli, and one K. pneumonia); five, Haemophilus influenzae type b; five, Staphylococcus aureus; and one, S. viridans. 20 patients were treated for probable bacterial meningitis, based upon the criteria mentioned in the Material and Methods section.

Of the 77 children treated for bacterial meningitis, 33 developed neurological complications (43%), and two children who presented with > 48 hours of illness died (14month-old child due to S. pneumoniae and 1-month-old child due to Pseudomonas aeruginosa).

The neurological complications observed were: subdural effusion (22/77; 28.6%); recurrent seizures (6/77; 7.8%); hemiparesis (5/77; 6.5%); intracerebral hemorrhage (3/77; 3.9%); cerebritis (3/77; 3.9%); facial nerve palsy (3/77; 3.9%); hydrocephalus (2/77; 2.6%); and single cases of subdural hematoma, cerebral abscess, subdural empyema, and purulent ventriculitis (1.3%).

The highest incidence of neurological complications was observed in children < 12 months of age (p < 0.05) (Table 1).

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A total of 47 patients (61%) were admitted with duration of illness < 48 hours. the mean duration of illness was 2.2 days, and there were no statistically significant differences in duration of illness according to age groups ( p > 0.05). A lower incidence of neurological complications was observed in children with duration of illness < 48 hours (19 patients [40%]), as compared to patients who were admitted after two days of illness. the observed differences were not statistically significant ( p > 0.05) (Table 2).

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Children who had seizures prior to admission (n = 14, 18%) and those who were admitted with an altered mental status (n = 44, 57%) were found to have higher incidence of neurological complications (p < 0.05). there were no statistically significant differences in presentation of seizures, presence of neurological deficit, or alteration of mental status according to age group.

In addition, children who had focal neurological deficits at the time of admission (n = 13, 17%) were found to be at increased risk for developing neurological complications (p < 0.05).

The incidence of neurological complications was higher in patients treated with dexamethasone, compared to those who were not (p < 0.05). the mean duration of illness before dexamethasone use was three days. almost half of the patients (33 children, 49%) were previously treated with antibiotics, but they were not associated with increased incidence of neurological complications ( p > 0.05).

The incidence of neurological complications was higher in patients who, during the initial antibiotic treatment, were treated with two antibiotics (n = 35; 45%), compared to those treated with one antibiotic (n = 42; 55%) (p < 0.05).

Increased protein levels (mean 1.63 g/L) were found in 65 patients (84%), who also had higher incidence of neurological complications (p < 0.05).

Initial turbid CSF with pleocytosis > 5,000 cells/mm³ (n = 46; 60%) and turbid CSF with pleocytosis > 5,000 cells/mm³ after 48 hours (n = 15; 19%) were not associated with increased risk for developing neurological complications ( p > 0.05).

Patients who had, at the initial lumbar puncture, a CSF/blood glucose ratio < 0.20 were not at increased risk for developing neurological complications ( p > 0.05).

The presence of a primary infectious focus (n = 53; 69%), the presence of comorbidity (n = 18; 23%), communityacquired infection (n = 73; 95%), and female gender (n = 29; 38%) were not associated with increased incidence of neurological complications ( p > 0.05).

The etiology of bacterial meningitis cases was proven in 57/77 cases (74%): 32 meningococci, eight pneumococci, six Gram-negative bacilli, five H. influenzae type B, five staphylococci, and one S. viridans isolates were found. Neurological complications developed more frequently in patients who were infected with S. pneumoniae (6/8), S. aureus (3/5), Gram-negative bacilli (2/6), N. meningitidis (8/32), and H. influenzae (1/5).

Children with bacterial meningitis were equally from rural (n = 39) and urban places (n = 38). A higher incidence of neurological complications was recorded in children from urban places (18/38; 47%) compared to children from rural places (15/39; 38%). None of the children attended kindergarten.

Discussion

Despite the progress in medicine, bacterial meningitis causes substantial morbidity and mortality in children in both developed^1,2,9,11-16 and developing countries.^6,10,17-20 Sensorineural hearing loss, seizures, motor problems, hydrocephalus and mental retardation, as well as more subtle outcomes like cognitive, academic, and behavioral problems are observed in post-meningitis children.^7,9,12,13 Chandran A. et al., in their systematic literature search, found that 49% of survivors of childhood bacterial meningitis were reported to have one or more long-term sequelae. The majority of reported sequelae were behavioral and/or intellectual disorders (45%).²¹ The risk of long term sequelae is higher in individuals who have acute neurological complications during the course of the disease.^6,8 Identification of predictors for early neurological complications is extremely important, since they are also the first predictors of long-term sequelae of childhood bacterial meningitis.

Several studies of clinical features and prognostic factors in children with bacterial meningitis have been performed,^{2,6-8,11-14,17,22,23} and the majority were conducted in developed countries. In the present study, the influence of 16 potentially important prognostic factors for neurological complications in children with bacterial meningitis were prospectively analyzed in a developing country. Young age (indicated as younger than two years old), is considered an important prognostic factor for adverse outcome of children with bacterial meningitis.^2,18 In this study, age < 12 months was also identified as predictor for neurological complications. from a previous report by the authors, age < 12 months was a risk factor for both early neurological complications and long-term sequelae of bacterial meningitis in children.²⁴

Severity of clinical presentation, manifested by the alteration of mental status and the occurrence of seizures, are identified as the strongest prognostic factors for neurological complications in the present study, similar to that indicated in numerous studies from developed countries.^{6,17-20,27,28} Klinger et al. found that duration of seizures for > 72 hours and presence of coma were the most important predictors of adverse outcome.²⁵

Time required for establishing a diagnosis of bacterial meningitis depends on the ability of primary health care services to accurately assess the symptoms and to order immediate patient transfer to specialized institutions in which the prompt diagnosis can be confirmed and a suitable antimicrobial therapy can be initiated. Delay in treatment is associated with an increased risk of neurological disability and death in both developed^13,22,25 and developing countries.^10,17,19,28 In the present study, duration of illness > 48 hours was associated with increased incidence of neurological complications in survivors compared to children with duration of illness < 48 hours, but the differences were not statistically significant. the mean duration of illness prior to admission was 2.2 days, which the authors consider to be an improvement of their health care system and socioeconomic conditions compared to previous reports, where the mean duration of illness in children with bacterial meningitis was 3.7 days.¹⁰ Two other benefit factors are existence of the specialized ward for treatment of CNS infections in children at the Infectious Diseases Clinic in Prishtina (the capital city of Kosovo) for more than 36 years, and that the furthest distance from Prishtina is estimated to be < 100 km or 1.5 hours of driving.

A decade after the war in Kosovo (1999), many private clinics opened, with no control of which first-line antibiotics were given to children. Most pediatricians and family doctors prescribe third generation cephalosporins, especially ceftriaxone, as a first-line antibiotic therapy for febrile illness in children. Almost half of the patients (49%) were previously treated with antibiotics, but they were not associated with an increased incidence of neurological complications. In the authors' prior study, previous treatment with antibiotics was found to be associated with increased risk for death.¹⁰

Children who manifested focal neurological deficit at admission had a significantly higher incidence of neurological complications. Oostenbrik et al. found that children with acute focal neurological symptoms tend to have the worst prognosis.¹²

The incidence of neurological complications was significantly higher in patients who were initially treated with two antibiotics (n = 35; 45%), as those children presented severe clinical presentation at admission. The most administered initial antibiotic therapy was the combination of ceftriaxone with vancomycin (23%).

Many clinical trials were undertaken to determine the effects of adjunctive dexamethasone on the outcome in children with bacterial meningitis.^10,16,22,29 The results, however, do not point unequivocally to a beneficial effect.^29,30 In this study, adjunctive dexamethasone therapy did not reduce the incidence of neurological complications in children with bacterial meningitis. The beneficial effect of dexamethasone use could not be proved, as a result of several factors: dexamethasone was used in patients who presented with the severe clinical form of illness at admission, the mean duration of illness prior to dexamethasone use was three days, and half of children were previously treated with antibiotics.

Other risk factors identified by previous studies include alterations in various CSF parameters. Low CSF leukocyte count, low CSF glucose level, low CSF/blood glucose level, and high CSF protein level have been identified as significant factors predicting neurological complications of bacterial meningitis in children in both developed^{9,11,13-16,26}and developing countries.^17-20,28

In this study, only increased CSF protein level was identified as risk factor for neurological complications. Initial turbid CSF with pleocytosis > 5,000 cells/mm³, turbid CSF after 48 hours, and CSF/blood glucose ratio < 0.20 were not identified as statistically significant factors for the development of neurological complications.

An association between meningitis caused by S. pneumoniae and unfavorable evolution has been suggested in the literature.^{11-13,16,17,19} According to Antoniuk et al., infection with S. pneumoniae is considered a risk factor for acute neurological complication.⁶ In the present study, neurological complications developed more frequently in patients who were infected with S. pneumoniae.

Presence of a primary focus of infection, presence of comorbidity, community-acquired infection, and female gender were not found to be associated with increased risk for the development of neurological complications.

The primary meningeal pathogen involved in causing community-acquired bacterial meningitis in children from Kosovo continues to be N. meningitidis. Hib vaccination during routine childhood immunization in Kosovo has been implemented only since 2010, giving hope to reduce the burden of bacterial meningitis in children. The implementation of protocols for the empirical treatment of bacterial meningitis to reduce the mortality rate and the incidence of neurological complications is the goal of future treatments of children.

In conclusion, age < 12 months and severity of clinical presentation at admission (alteration of mental status and the occurrence of seizures) were identified as the strongest predictors for neurological complications, and may be of value in selecting patients for more intensive care and treatment.

Conflicts of interest

The authors declare no conflicts of interest.

Acknowledgements

The authors would like to thank the personnel of Infectious Diseases Clinic of Prishtina for their support during this study.

References

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2. de Jonge RC, van Furth AM, Wassenaar M, Gemke RJ, Terwee CB. Predicting sequelae and death after bacterial meningitis in childhood: a systematic review of prognostic studies. BMC Infect Dis. 2010;10:232.

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6. Antoniuk SA, Hamdar F, Ducci RD, Kira AT, Cat MN, Cruz CR. Childhood acute bacterial meningitis: risk factors for acute neurological complications and neurological sequelae. J Pediatr (Rio J). 2011;87:535-40.

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8. Grimwood K, Anderson P, Anderson V, Tan L, Nolan T. Twelve year outcomes following bacterial meningitis: further evidence for persisting effects. Arch Dis Child. 2000;83:111-6.

9. Koomen I, Grobbee DE, Jennekens-Schinkel A, Roord JJ, van Furth AM. Parental perception of educational, behavioural and general health problems in school-age survivors of bacterial meningitis. Acta Paediatr. 2003;92:177-85.

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11. Koomen I, Grobbee DE, Roord JJ, Donders R, Jennekens-Schinkel A, van Furth AM. Hearing loss at school age in survivors of bacterial meningitis: assessment, incidence, and prediction. Pediatrics. 2003;112:1049-53.

12. Oostenbrink R, Maas M, Moons KG, Moll HA. Sequelae after bacterial meningitis in childhood. Scand J Infect Dis. 2002;34:379-82.

13. Chávez-Bueno S, McCracken GH Jr. Bacterial meningitis in children. Pediatr Clin North Am. 2005;52:795-810.

14. Vasilopoulou VA, Karanika M, Theodoridou K, Katsioulis AT, Theodoridou MN, Hadjichristodoulou CS. Prognostic factors related to sequelae in childhood bacterial meningitis: data from a Greek meningitis registry. BMC Infect Dis. 2011;11:214.

15. Koomen I, Grobbee DE, Roord JJ, Jennekens-Schinkel A, van der Lei HD, Kraak MA, et al. Prediction of academic and behavioural limitations in school-age survivors of bacterial meningitis. Acta Paediatr. 2004;93:1378-85.

16. Pagliano P, Fusco U, Attanasio V, Rossi M, Pantosti A, Conte M, et al. Pneumococcal meningitis in childhood: a longitudinal prospective study. FEMS Immunol Med Microbiol. 2007;51:488-95.

17. Roine I, Peltola H, Fernández J, Zavala I, González Mata A, González Ayala S, et al. Influence of admission findings on death and neurological outcome from childhood bacterial meningitis. Clin Infect Dis. 2008;46:1248-52.

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19. Pelkonen T, Roine I, Monteiro L, Correia M, Pitkäranta A, Bernardino L, et al. Risk factors for death and severe neurological sequelae in childhood bacterial meningitis in sub-Saharan Africa. Clin Infect Dis. 2009;48:1107-10.

20. Singhi P, Bansal A, Geeta P, Singhi S. Predictors of long term neurological outcome in bacterial meningitis. Indian J Pediatr. 2007;74:369-74.

21. Chandran A, Herbert H, Misurski D, Santosham M. Long-term sequelae of childhood bacterial meningitis: an underappreciated problem. Pediatr Infect Dis J. 2011;30:3-6.

22. McIntyre PB, Macintyre CR, Gilmour R, Wang H. A population based study of the impact of corticosteroid therapy and delayed diagnosis on the outcome of childhood pneumococcal meningitis. Arch Dis Child. 2005;90:391-6.

23. Tsai MH, Chen SH, Hsu CY, Yan DC, Yen MH, Chiu CH, et al. Pneumococcal meningitis in Taiwanese children: emphasis on clinical outcomes and prognostic factors. J Trop Pediatr. 2008;54:390-4.

24. Namani SA, Koci BM, Milenković Z, Koci R, Qehaja-Buçaj E, Ajazaj L, et al. Early neurologic complications and long-term sequelae of childhood bacterial meningitis in a limited-resource country (Kosovo). Childs Nerv Syst. 2012 Sep 12. [Epub ahead of print ]

25. Klinger G, Chin CN, Beyene J, Perlman M. Predicting the outcome of neonatal bacterial meningitis. Pediatrics. 2000;106:477-82.

26. Wasier AP, Chevret L, Essouri S, Durand P, Chevret S, Devictor D. Pneumococcal meningitis in a pediatric intensive care unit: prognostic factors in a series of 49 children. Pediatr Crit Care Med. 2005;6:568-72.

27. Chao YN, Chiu NC, Huang FY. Clinical features and prognostic factors in childhood pneumococcal meningitis. J Microbiol Immunol Infect. 2008;41:48-53.

28. Kirimi E, Tuncer O, Arslan S, Ataş B, Caksen H, Uner A, et al. Prognostic factors in children with purulent meningitis in Turkey. Acta Med Okayama. 2003;57:39-44.

29. Molyneux EM, Walsh AL, Forsyth H, Tembo M, Mwenechanya J, Kayira K, et al. Dexamethasone treatment in childhood bacterial meningitis in Malawi: a randomised controlled trial. Lancet. 2002;360:211-8.

30. van de Beek D, Farrar JJ, de Gans J, Mai NT, Molyneux EM, Peltola H, et al. Adjunctive dexamethasone in bacterial meningitis: a meta-analysis of individual patient data. Lancet Neurol. 2010;9:254-63.

Received 25 August 2012; accepted 31 October 2012

Available online 28 April 2013

1. Molyneux E, Riordan FA, Walsh A. Acute bacterial meningitis in children presenting to the Royal Liverpool Children's Hospital, Liverpool, UK and the Queen Elizabeth Central Hospital in Blantyre, Malawi: a world of difference. Ann Trop Paediatr. 2006;26:29-37.
2. de Jonge RC, van Furth AM, Wassenaar M, Gemke RJ, Terwee CB. Predicting sequelae and death after bacterial meningitis in childhood: a systematic review of prognostic studies. BMC Infect Dis. 2010;10:232.
3. Scarborough M, Thwaites GE. The diagnosis and management of acute bacterial meningitis in resource-poor settings. Lancet Neurol. 2008;7:637-48.
4. Sáez-Llorens X, McCracken GH Jr. Bacterial meningitis in children. Lancet. 2003;361:2139-48.
5. Theodoridou MN, Vasilopoulou VA, Atsali EE, Pangalis AM, Mostrou GJ, Syriopoulou VP, et al. Meningitis registry of hospitalized cases in children: epidemiological patterns of acute bacterial meningitis throughout a 32-year period. BMC Infect Dis. 2007;7:101.
6. Antoniuk SA, Hamdar F, Ducci RD, Kira AT, Cat MN, Cruz CR. Childhood acute bacterial meningitis: risk factors for acute neurological complications and neurological sequelae. J Pediatr (Rio J). 2011;87:535-40.
7. Anderson V, Anderson P, Grimwood K, Nolan T. Cognitive and executive function 12 years after childhood bacterial meningitis: effect of acute neurologic complications and age of onset. J Pediatr Psychol. 2004;29:67-81.
8. Grimwood K, Anderson P, Anderson V, Tan L, Nolan T. Twelve year outcomes following bacterial meningitis: further evidence for persisting effects. Arch Dis Child. 2000;83:111-6.
9. Koomen I, Grobbee DE, Jennekens-Schinkel A, Roord JJ, van Furth AM. Parental perception of educational, behavioural and general health problems in school-age survivors of bacterial meningitis. Acta Paediatr. 2003;92:177-85.
10. Namani S, Milenkovic Z, Kuchar E, Koci R, Mehmeti M. Mortality from bacterial meningitis in children in Kosovo. J Child Neurol. 2012;27:46-50.
11. Koomen I, Grobbee DE, Roord JJ, Donders R, Jennekens-Schinkel A, van Furth AM. Hearing loss at school age in survivors of bacterial meningitis: assessment, incidence, and prediction. Pediatrics. 2003;112:1049-53.
12. Oostenbrink R, Maas M, Moons KG, Moll HA. Sequelae after bacterial meningitis in childhood. Scand J Infect Dis. 2002;34:379-82.
13. Chávez-Bueno S, McCracken GH Jr. Bacterial meningitis in children. Pediatr Clin North Am. 2005;52:795-810.
14. Vasilopoulou VA, Karanika M, Theodoridou K, Katsioulis AT, Theodoridou MN, Hadjichristodoulou CS. Prognostic factors related to sequelae in childhood bacterial meningitis: data from a Greek meningitis registry. BMC Infect Dis. 2011;11:214.
15. Koomen I, Grobbee DE, Roord JJ, Jennekens-Schinkel A, van der Lei HD, Kraak MA, et al. Prediction of academic and behavioural limitations in school-age survivors of bacterial meningitis. Acta Paediatr. 2004;93:1378-85.
16. Pagliano P, Fusco U, Attanasio V, Rossi M, Pantosti A, Conte M, et al. Pneumococcal meningitis in childhood: a longitudinal prospective study. FEMS Immunol Med Microbiol. 2007;51:488-95.
17. Roine I, Peltola H, Fernández J, Zavala I, González Mata A, González Ayala S, et al. Influence of admission findings on death and neurological outcome from childhood bacterial meningitis. Clin Infect Dis. 2008;46:1248-52.
18. Lovera D, Arbo A. Risk factors for mortality in Paraguayan children with pneumococcal bacterial meningitis. Trop Med Int Health. 2005;10:1235-41.
19. Pelkonen T, Roine I, Monteiro L, Correia M, Pitkäranta A, Bernardino L, et al. Risk factors for death and severe neurological sequelae in childhood bacterial meningitis in sub-Saharan Africa. Clin Infect Dis. 2009;48:1107-10.
20. Singhi P, Bansal A, Geeta P, Singhi S. Predictors of long term neurological outcome in bacterial meningitis. Indian J Pediatr. 2007;74:369-74.
21. Chandran A, Herbert H, Misurski D, Santosham M. Long-term sequelae of childhood bacterial meningitis: an underappreciated problem. Pediatr Infect Dis J. 2011;30:3-6.
22. McIntyre PB, Macintyre CR, Gilmour R, Wang H. A population based study of the impact of corticosteroid therapy and delayed diagnosis on the outcome of childhood pneumococcal meningitis. Arch Dis Child. 2005;90:391-6.
23. Tsai MH, Chen SH, Hsu CY, Yan DC, Yen MH, Chiu CH, et al. Pneumococcal meningitis in Taiwanese children: emphasis on clinical outcomes and prognostic factors. J Trop Pediatr. 2008;54:390-4.
25. Klinger G, Chin CN, Beyene J, Perlman M. Predicting the outcome of neonatal bacterial meningitis. Pediatrics. 2000;106:477-82.
26. Wasier AP, Chevret L, Essouri S, Durand P, Chevret S, Devictor D. Pneumococcal meningitis in a pediatric intensive care unit: prognostic factors in a series of 49 children. Pediatr Crit Care Med. 2005;6:568-72.
27. Chao YN, Chiu NC, Huang FY. Clinical features and prognostic factors in childhood pneumococcal meningitis. J Microbiol Immunol Infect. 2008;41:48-53.
29. Molyneux EM, Walsh AL, Forsyth H, Tembo M, Mwenechanya J, Kayira K, et al. Dexamethasone treatment in childhood bacterial meningitis in Malawi: a randomised controlled trial. Lancet. 2002;360:211-8.
30. van de Beek D, Farrar JJ, de Gans J, Mai NT, Molyneux EM, Peltola H, et al. Adjunctive dexamethasone in bacterial meningitis: a meta-analysis of individual patient data. Lancet Neurol. 2010;9:254-63.

*

Corresponding author.

E-mail:

sadie_namani@yahoo.com (S. Namani).

Publication Dates

Publication in this collection
03 July 2013
Date of issue
June 2013

History

Received
27 Aug 2012
Accepted
31 Oct 2012

This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License.

[1] 1. Molyneux E, Riordan FA, Walsh A. Acute bacterial meningitis in children presenting to the Royal Liverpool Children's Hospital, Liverpool, UK and the Queen Elizabeth Central Hospital in Blantyre, Malawi: a world of difference. Ann Trop Paediatr. 2006;26:29-37.

[2] 2. de Jonge RC, van Furth AM, Wassenaar M, Gemke RJ, Terwee CB. Predicting sequelae and death after bacterial meningitis in childhood: a systematic review of prognostic studies. BMC Infect Dis. 2010;10:232.

[3] 3. Scarborough M, Thwaites GE. The diagnosis and management of acute bacterial meningitis in resource-poor settings. Lancet Neurol. 2008;7:637-48.

[4] 4. Sáez-Llorens X, McCracken GH Jr. Bacterial meningitis in children. Lancet. 2003;361:2139-48.

[5] 5. Theodoridou MN, Vasilopoulou VA, Atsali EE, Pangalis AM, Mostrou GJ, Syriopoulou VP, et al. Meningitis registry of hospitalized cases in children: epidemiological patterns of acute bacterial meningitis throughout a 32-year period. BMC Infect Dis. 2007;7:101.

[6] 6. Antoniuk SA, Hamdar F, Ducci RD, Kira AT, Cat MN, Cruz CR. Childhood acute bacterial meningitis: risk factors for acute neurological complications and neurological sequelae. J Pediatr (Rio J). 2011;87:535-40.

[7] 7. Anderson V, Anderson P, Grimwood K, Nolan T. Cognitive and executive function 12 years after childhood bacterial meningitis: effect of acute neurologic complications and age of onset. J Pediatr Psychol. 2004;29:67-81.

[8] 8. Grimwood K, Anderson P, Anderson V, Tan L, Nolan T. Twelve year outcomes following bacterial meningitis: further evidence for persisting effects. Arch Dis Child. 2000;83:111-6.

[9] 9. Koomen I, Grobbee DE, Jennekens-Schinkel A, Roord JJ, van Furth AM. Parental perception of educational, behavioural and general health problems in school-age survivors of bacterial meningitis. Acta Paediatr. 2003;92:177-85.

[10] 10. Namani S, Milenkovic Z, Kuchar E, Koci R, Mehmeti M. Mortality from bacterial meningitis in children in Kosovo. J Child Neurol. 2012;27:46-50.

[11] 11. Koomen I, Grobbee DE, Roord JJ, Donders R, Jennekens-Schinkel A, van Furth AM. Hearing loss at school age in survivors of bacterial meningitis: assessment, incidence, and prediction. Pediatrics. 2003;112:1049-53.

[12] 12. Oostenbrink R, Maas M, Moons KG, Moll HA. Sequelae after bacterial meningitis in childhood. Scand J Infect Dis. 2002;34:379-82.

[13] 13. Chávez-Bueno S, McCracken GH Jr. Bacterial meningitis in children. Pediatr Clin North Am. 2005;52:795-810.

[14] 14. Vasilopoulou VA, Karanika M, Theodoridou K, Katsioulis AT, Theodoridou MN, Hadjichristodoulou CS. Prognostic factors related to sequelae in childhood bacterial meningitis: data from a Greek meningitis registry. BMC Infect Dis. 2011;11:214.

[15] 15. Koomen I, Grobbee DE, Roord JJ, Jennekens-Schinkel A, van der Lei HD, Kraak MA, et al. Prediction of academic and behavioural limitations in school-age survivors of bacterial meningitis. Acta Paediatr. 2004;93:1378-85.

[16] 16. Pagliano P, Fusco U, Attanasio V, Rossi M, Pantosti A, Conte M, et al. Pneumococcal meningitis in childhood: a longitudinal prospective study. FEMS Immunol Med Microbiol. 2007;51:488-95.

[17] 17. Roine I, Peltola H, Fernández J, Zavala I, González Mata A, González Ayala S, et al. Influence of admission findings on death and neurological outcome from childhood bacterial meningitis. Clin Infect Dis. 2008;46:1248-52.

[18] 18. Lovera D, Arbo A. Risk factors for mortality in Paraguayan children with pneumococcal bacterial meningitis. Trop Med Int Health. 2005;10:1235-41.

[19] 19. Pelkonen T, Roine I, Monteiro L, Correia M, Pitkäranta A, Bernardino L, et al. Risk factors for death and severe neurological sequelae in childhood bacterial meningitis in sub-Saharan Africa. Clin Infect Dis. 2009;48:1107-10.

[20] 20. Singhi P, Bansal A, Geeta P, Singhi S. Predictors of long term neurological outcome in bacterial meningitis. Indian J Pediatr. 2007;74:369-74.

[21] 21. Chandran A, Herbert H, Misurski D, Santosham M. Long-term sequelae of childhood bacterial meningitis: an underappreciated problem. Pediatr Infect Dis J. 2011;30:3-6.

[22] 22. McIntyre PB, Macintyre CR, Gilmour R, Wang H. A population based study of the impact of corticosteroid therapy and delayed diagnosis on the outcome of childhood pneumococcal meningitis. Arch Dis Child. 2005;90:391-6.

[23] 23. Tsai MH, Chen SH, Hsu CY, Yan DC, Yen MH, Chiu CH, et al. Pneumococcal meningitis in Taiwanese children: emphasis on clinical outcomes and prognostic factors. J Trop Pediatr. 2008;54:390-4.

[25] 25. Klinger G, Chin CN, Beyene J, Perlman M. Predicting the outcome of neonatal bacterial meningitis. Pediatrics. 2000;106:477-82.

[26] 26. Wasier AP, Chevret L, Essouri S, Durand P, Chevret S, Devictor D. Pneumococcal meningitis in a pediatric intensive care unit: prognostic factors in a series of 49 children. Pediatr Crit Care Med. 2005;6:568-72.

[27] 27. Chao YN, Chiu NC, Huang FY. Clinical features and prognostic factors in childhood pneumococcal meningitis. J Microbiol Immunol Infect. 2008;41:48-53.

[29] 29. Molyneux EM, Walsh AL, Forsyth H, Tembo M, Mwenechanya J, Kayira K, et al. Dexamethasone treatment in childhood bacterial meningitis in Malawi: a randomised controlled trial. Lancet. 2002;360:211-8.

[30] 30. van de Beek D, Farrar JJ, de Gans J, Mai NT, Molyneux EM, Peltola H, et al. Adjunctive dexamethasone in bacterial meningitis: a meta-analysis of individual patient data. Lancet Neurol. 2010;9:254-63.

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A prospective study of risk factors for neurological complications in childhood bacterial meningitis

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