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Cerebrospinal fluid transcriptional immune pathways linked to survival in HIV-associated tuberculous meningitis.

Created on 18 Jun 2026

Authors

Martineau Louine, Ravi Dandekar, Sumanth P Reddy, Mary C Karalius, Greer Waldrop, Shiyin Wang, Jane Gakuru, Sarah Kimuda, Timothy Mugabi, Abdu K Musubire, Enock Kagimu, Mahsa Abassi, Mable Kabahubya, Darlisha A Williams, Hoang Van Phan, Biyue Dai, Maham Zia, Kelsey C Zorn, Camille Fouassier, Chloe Gerungan, Pedro S Marra, Caleb P Skipper, Nathan C Bahr, Charles R Langelier, Fiona V Creswell, David R Boulware, David B Meya, Michael R Wilson

Published in

The Journal of infectious diseases. Jun 18, 2026. Epub Jun 18, 2026.

Abstract

TB meningitis (TBM) has up to 50% mortality in people living with HIV. We investigated differences in cerebrospinal fluid (CSF) host immune responses associated with short-term mortality.
We enrolled a prospective cohort of adults with definite, probable and possible HIV-related TBM in Kampala, Uganda. Metagenomic next-generation sequencing (mNGS) of bulk CSF RNA was used to detect co-infecting or alternate CNS pathogens and refine cohort diagnosis. Host transcriptomic profiles from the refined cohort were then compared between 14-day survivors and non-survivors.
CSF mNGS reclassified or excluded 14% of participants based on pathogen detection, yielding 110 participants for transcriptomic analysis, of whom 23% (n=25) died within 14 days. More than 2000 genes were differentially expressed in the CSF based on 14-day mortality (adjusted p-value <0.05). Survivors upregulated T-cell receptor signaling (LCK, FYN, LAT), T-cell survival and differentiation (IL7, CD27, IL12RB1), B-cell receptor signaling (CD81, PLCG2, TNFRSF13C), cytotoxic lymphocyte and NK cell genes (KLRD1, ULBP1), TNF signaling, and class I MHC antigen processing pathways, while downregulating neutrophil chemoattractant CXCL1 and classical complement genes C4A and C4B. Unsupervised clustering identified a hypoinflammatory subgroup with significantly elevated mortality.
Short-term TBM survival was associated with upregulation of adaptive immunity - including T-cell, B-cell, NK cell, and cytotoxic lymphocyte signaling - alongside TNF signaling and IFN-γ-driven class I MHC antigen processing pathways, with concurrent restraint of complement and neutrophil pathways. This supports investigation of targeted immunomodulatory agents that preserve protective responses while selectively dampening injurious innate pathways, rather than broad immunosuppression with corticosteroids.

PMID:
42313402
Bibliographic data and abstract were imported from PubMed on 18 Jun 2026.

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