Neopterin and CXCL-13 in Diagnosis and Follow-Up of Trypanosoma brucei gambiense Sleeping Sickness: Lessons from the Field in Angola

Author:

Bonnet Julien1ORCID,Vignoles Philippe1,Tiberti Natalia23,Gedeão Vatunga4,Hainard Alexandre2,Turck Natacha2ORCID,Josenando Theophile4,Ndung’u Joseph M5,Sanchez Jean-Charles2ORCID,Courtioux Bertrand1ORCID,Bisser Sylvie16

Affiliation:

1. Institute of Neuroepidemiology and Tropical Neurology, School of Medicine, CNRS FR 3503 GEIST, University of Limoges, INSERM UMR1094 Tropical Neuroepidemiology, Limoges, France

2. Translational Biomarker Group, Department of Human Protein Sciences, University of Geneva, Geneva, Switzerland

3. Department of Infectious—Tropical Diseases and Microbiology, IRCCS Sacro Cuore Don Calabria Hospital, Negrar, Verona, Italy

4. Instituto de Combate e Controlo das Tripanossomiases (ICCT), Luanda, Angola

5. Foundation for Innovative New Diagnostics (FIND), Geneva, Switzerland

6. Pasteur Institute in French Guiana, 23 Boulevard Pasteur, 973006 Cayenne Cedex, French Guiana

Abstract

Human African Trypanosomiasis may become manageable in the next decade with fexinidazole. However, currently stage diagnosis remains difficult to implement in the field and requires a lumbar puncture. Our study of an Angolan cohort of T. b. gambiense-infected patients used other staging criteria than those recommended by the WHO. We compared WHO criteria (cell count and parasite identification in the CSF) with two biomarkers (neopterin and CXCL-13) which have proven potential to diagnose disease stage or relapse. Biological, clinical, and neurological data were analysed from a cohort of 83 patients. A neopterin concentration below 15.5 nmol/L in the CSF denoted patients with stage 1 disease, and a concentration above 60.31 nmol/L characterized patients with advanced stage 2 (trypanosomes in CSF and/or cytorachia higher than 20 cells) disease. CXCL-13 levels below 91.208 pg/mL denoted patients with stage 1 disease, and levels of CXCL-13 above 395.45 pg/mL denoted patients with advanced stage 2 disease. Values between these cut-offs may represent patients with intermediate stage disease. Our work supports the existence of an intermediate stage in HAT, and CXCL-13 and neopterin levels may help to characterize it.

Funder

Foundation for New Innovative Diagnostics

Publisher

Hindawi Limited

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine

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