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Radboudumc researchers used metabolomics to study cerebrospinal fluid (CSF) samples from tuberculous meningitis patients in Vietnam and Indonesia, with long-standing collaborators from Bandung and Jakarta (Indonesia), the Broad Institute (Boston) and the Oxford University Research Unit in Ho Chi Minh City (Vietnam).

The paper is published in the journal Med.

Meningitis is the most severe form of tuberculosis. Damaging inflammation contributes to its poor prognosis. Corticosteroids reduce mortality, but nearly 50% of patients still die or are left disabled.

The researchers, Kirsten van Abeelen, Edwin Ardiansyah, Sofiati Dian, Vinod Kumar, Reinout van Crevel and Arjan van Laarhoven, hypothesized that metabolic pathways may influence disease outcome and help develop more effective host-directed therapy.

They measured levels of 469 metabolites in cerebrospinal fluid obtained from 1, 067 Vietnamese and Indonesian tuberculous meningitis patients with and without HIV before the start of treatment, and observed these patients for clinical outcome.

Mortality was strongly associated with 10 metabolites, including three hydroxylated fatty acids with a maximum carbon length of eight. These metabolites predicted mortality, regardless of HIV status, disease severity and cerebrospinal fluid tryptophan levels, which they previously identified as an important prognostic metabolite.

The results suggest that dysregulated β-oxidation may be an important and potentially modifiable contributor to mortality in tuberculous meningitis.

Follow-up studies are underway, including quantitative trait locus mapping and rare genetic variant analysis, in the same patient groups. Future intervention studies should examine whether interventions targeting cerebral metabolism or oxygenation can improve survival of this deadly disease.

More information: Pre-treatment untargeted cerebrospinal fluid metabolomic profiling in tuberculous meningitis reveals multiple pathways associated with mortality, Med (2025). DOI: 10.1016/j.medj.2025.100703. www.cell.com/med/fulltext/S2666-6340(25)00130-8  Journal information: Med