Adult meningitis in a setting of high HIV and TB prevalence: findings from 4961 suspected cases

Patients undergoing lumbar-punctures (LPs) between 1^st January 2006 and 31^st December 2008 were studied. Results of all LPs performed for any indication were recorded, the majority being for suspected meningitis in acute admissions, with demographic information from laboratory request forms and clinical notes. Cerebrospinal-fluid (CSF) samples underwent macroscopic examination, protein and glucose quantification, cell counts using a Neubauer counting chamber following crystal violet staining, Gram-staining of centrifuged sediment, and bacterial culture on blood and chocolate agar for 72 hours. India-ink staining of centrifuged CSF, cryptococcal antigen (CrAg) testing (Meridian Cryptococcal Latex Agglutination System, Meridian Bioscience) if India-ink negative, and fungal culture of all samples on potato dextrose agar (PDA) slopes for 14 days were carried out. TB microscopy (Auramine-flourescent stain of the sediment when sufficient sample), liquid culture in mycobacterial growth indicator tubes (MGIT, Becton-Dickenson), Lowenstein-Jensen agar slopes if sufficient sample, and TB-PCR (Genotype MTBDRplus, Hain Lifesciences) on positive culture samples from MGIT were performed in cases of suspected TB meningitis (TBM) at the clinician's request, or when CSF findings were suggestive of TBM. In a limited number of cases TB-PCR was performed directly on CSF samples in an effort to rapidly obtain drug susceptibility data. VDRL and TPHA testing were carried out at the clinician's request.

When a patient had more than one LP, a separate clinical episode was defined when there was ≥1 month between LPs, except in cases of TBM, where any repeat LP within 6 months was considered part of the same episode. These definitions were based on the best available evidence, and aimed to reflect the total burden of meningitis due to differing aetiologies, including relapse episodes. Median duration of admission for cryptococcal meningitis at our hospital is 15 days, with an inter-quartile range (IQR) of 13 to 20 days (unpublished data). For TB meningitis a cut-of off 6 months was chosen, as patients are treated with 6-9 months of therapy, and the TB programme regards a re-presentation with TBM during treatment as a deterioration of the initial episode, rather than a "recurrence" or "relapse".

Cases were classified by microbiological diagnosis, or in the absence of definitive microbiology as:

1) normal CSF (neutrophils ≤ 1 × 10⁶/L, lymphocytes ≤ 5 × 10⁶/L, protein ≤ 0.5 g/dL, and glucose ≥1.5 mmol/L with no organism isolated),

2) minor abnormalities (neutrophils 2-5 × 10⁶/L, lymphocytes 6-20 × 10⁶/L, protein 0.51-1.0 g/dL, or glucose 1.0-1.49 mmol/L and no organism isolated) or

3) markedly abnormal (neutrophils>5 × 10⁶/L, lymphocytes>20 × 10⁶/L, protein>1.0 g/dL, or glucose<1.0 mmol/L and no organism isolated).

Markedly abnormal cases were further classified into lymphocytic (lymphocyte predominance, L_Ø:N_Ø ratio ≥3:1), mixed (L_Ø:N_Ø ratio between 3 and 0.33), and pyogenic (neutrophil predominance, N_Ø:L_Ø ratio ≥3:1).

HIV status was determined for all patients with microbiologically confirmed disease during the last 2 years of the study from laboratory records and clinical notes.

Cryptococcus (CM) accounted for 63% (514) of microbiological diagnoses, 93 (18%) of which were relapses of previously treated episodes. The CM relapse episodes occurred a median of 92 days after the initial episode (IQR 56-131 days). TB accounted for 28% (227), bacterial meningitis for 8% (68) and neurosyphillis for 3% (22)(figure 1). There were 2 patients who had 2 distinct episodes of TBM, one occurring 7 months and one occurring 10 months after the initial episode. CM was initially diagnosed on India-ink staining in 60% of cases, and CrAg testing in 40%. Cultures were positive in 68%. Laboratory confirmation of TBM was almost exclusively by culture, with smear positive microscopy in only 3 of the 227 cases. Of the culture confirmed bacterial meningitis, Streptococcus pneumoniae accounted for 90% (57 of 64), and Neisseria meningitides 3% (2 of 64). Gram-staining was positive in 58 (85%) of the 68 patients.

Of the 917 cases with markedly abnormal CSF and no microbiological diagnosis, 539 (59%) had a lymphocytic predominance, 114 (12%) a mixed picture, 75 (8%) a polymorph predominance and 189 (21%) a normo-cellular picture with abnormal protein and/or glucose.

Of note 16% (81) patients with confirmed CM, 5% (12) with TBM and 4% (3) with bacterial meningitis had normal CSF cell counts, protein and glucose (table 1).

During the last two years of the study period HIV status was ascertained for all but 2 of the CM patients (n = 339), of whom 99% (337) were HIV positive, median CD4 cell count of 39 cells/μL; 134 of 158 TBM patients, 94% (126) of whom were HIV positive, median CD4 cell count 126 cells/μL; and 30 of the 46 bacterial meningitis cases, of whom 97% (29) were HIV positive, median CD4 cell count 287 cells/μL.