Cerebrospinal fluid neopterin as marker of the meningo-encephalitic stage of trypanosoma brucei gambiense sleeping sickness

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Abstract

Background: Sleeping sickness, or human African trypanosomiasis (HAT), is a protozoan disease that affects rural communities in sub-Saharan Africa. Determination of the disease stage, essential for correct treatment, represents a key issue in the management of patients. In the present study we evaluated the potential of CXCL10, CXCL13, ICAM-1, VCAM-1, MMP-9, B2MG, neopterin and IgM to complement current methods for staging Trypanosoma brucei gambiense patients. Methods and Findings: Five hundred and twelve T. b. gambiense HAT patients originated from Angola, Chad and the Democratic Republic of the Congo (D.R.C.). Their classification as stage 2 (S2) was based on the number of white blood cells (WBC) (>5/μL) or presence of parasites in the cerebrospinal fluid (CSF). The CSF concentration of the eight markers was first measured on a training cohort encompassing 100 patients (44 S1 and 56 S2). IgM and neopterin were the best in discriminating between the two stages of disease with 86.4% and 84.1% specificity respectively, at 100% sensitivity. When a validation cohort (412 patients) was tested, neopterin (14.3 nmol/L) correctly classified 88% of S1 and S2 patients, confirming its high staging power. On this second cohort, neopterin also predicted both the presence of parasites, and of neurological signs, with the same ability as IgM and WBC, the current reference for staging. Conclusions: This study has demonstrated that neopterin is an excellent biomarker for staging T. b. gambiense HAT patients. A rapid diagnostic test for detecting this metabolite in CSF could help in more accurate stage determination. © 2012 Tiberti et al.

Figures

  • Table 1. Description of the training and the validation cohorts.
  • Table 2. Results obtained for the eight markers assessed on the training cohort.
  • Table 3. Results obtained for IgM and neopterin on the validation cohort after application of the cut-off calculated on the training cohort.
  • Table 4. Results obtained for IgM and neopterin on the validation cohort after application of the cut-off calculated on the training cohort and removal of early-late stage patients (n = 41).
  • Table 5. Detailed description of false negative patients obtained according to neopterin and IgM after removal of early–late stage patients from S2 group.
  • Table 6. Ability of WBC, IgM and neopterin in discriminating between patients without or with parasites in CSF.
  • Table 7. Ability of WBC, IgM and neopterin in discriminating between patients without or with neurological signs.
  • Figure 1. Classification of HAT patients according to WBC and IgM, or according to WBC and neopterin. A) Comparison of the classification of HAT patients (validation cohort) according to WBC and IgM. The staging cut-off of 5 WBC/mL recommended by WHO is reported on the graph as well as the staging cut-off of 3.4 mg/mL for IgM calculated on the training cohort. Black dots represent stage 1 patients, white dots represent early-late stage patients and gray dots represent stage 2 patients. B) Detailed classification of early-late stage patients (n = 41) according to IgM. Colours indicate the absence (white) or presence of neurological (black) signs. The staging cut-off of 5 WBC/mL recommended by WHO is reported on the graph as well as the staging cut-off of 3.4 mg/mL for IgM calculated on the training cohort. C) Comparison of the classification of HAT patients (validation cohort) according to WBC and neopterin. The staging cut-off of 5 WBC/mL recommended by WHO is reported on the graph as well as the staging cut-off of 14.3 nmol/L for neopterin calculated on the training cohort. Black dots represent stage 1 patients, white dots represent early-late stage patients and gray dots represent stage 2 patients. D) Detailed classification of early-late stage patients (n = 41) according to neopterin. Colours indicate the absence (white) or presence (black) of neurological signs. The staging cut-off of 5 WBC/mL recommended by WHO is reported on

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APA

Tiberti, N., Hainard, A., Lejon, V., Courtioux, B., Matovu, E., Enyaru, J. C., … Sanchez, J. C. (2012). Cerebrospinal fluid neopterin as marker of the meningo-encephalitic stage of trypanosoma brucei gambiense sleeping sickness. PLoS ONE, 7(7). https://doi.org/10.1371/journal.pone.0040909

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