Frontiers in Neurology (Aug 2022)

Identification of protein biomarkers in host cerebrospinal fluid for differential diagnosis of tuberculous meningitis and other meningitis

  • Mailing Huang,
  • Mailing Huang,
  • Zeyu Ding,
  • Wensheng Li,
  • Wensheng Li,
  • Weibi Chen,
  • Yadong Du,
  • Yadong Du,
  • Hongyan Jia,
  • Hongyan Jia,
  • Qi Sun,
  • Qi Sun,
  • Boping Du,
  • Boping Du,
  • Rongrong Wei,
  • Rongrong Wei,
  • Aiying Xing,
  • Aiying Xing,
  • Qi Li,
  • Naihui Chu,
  • Liping Pan,
  • Liping Pan

DOI
https://doi.org/10.3389/fneur.2022.886040
Journal volume & issue
Vol. 13

Abstract

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Background and purposeThe diagnosis of tuberculous meningitis (TBM) is difficult due to the lack of sensitive methods. Identification of TBM-specific biomarkers in the cerebrospinal fluid (CSF) may help diagnose and improve our understanding of TBM pathogenesis.Patients and methodsOf the 112 suspected patients with TBM prospectively enrolled in the study, 32 patients with inconclusive diagnosis, non-infectious meningitis, and long-term treatment with hormones and immunosuppressants were excluded. The expression of 8 proteins in the CSF was analyzed using ELISA in 22 patients with definite TBM, 18 patients with probable TBM, and 40 patients with non-TBM.ResultsSignificant differences in the expression of 7 proteins were detected between the TBM and non-TBM groups (P < 0.01). Unsupervised hierarchical clustering (UHC) analysis revealed a disease-specific profile consisting of 7 differentially expressed proteins for TBM diagnosis, with an accuracy of 82.5% (66/80). Logistic regression with forward stepwise analysis indicated that a combination of 3 biomarkers (APOE_APOAI_S100A8) showed a better ability to discriminate TBM from patients with non-TBM [area under the curve (AUC) = 0.916 (95%CI: 0.857–0.976)], with a sensitivity of 95.0% (95%CI: 83.1–99.4%) and a specificity of 77.5% (95%CI: 61.5–89.2%).ConclusionOur results confirmed the potential ability of CSF proteins to distinguish TBM from patients with non-TBM and provided a useful panel for the diagnosis of TBM.

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