Single and Combined Serum Proteins Expressed in TB Infection are Candidates for Point-of-care Diagnostic Testing of Active TB Patients in Lambaréné, Gabon

Author:

Essone Paulin N12,Lotola-Mougeni Fabrice1,Adegbite Bayode R134,Kokou Kossiwa1,Otogo N'Nang E1,Mabicka Eddy1,Alabi Ayodele1,Djoba Siawaya Joel F2,Kremsner Peter G13,Grobusch Martin P134,Agnandji Selidji T135ORCID

Affiliation:

1. Centre de Recherches Médicales de Lambaréné , Biomedicine and Social Sciences Research Group, Department of Biologicals and Therapeutics, Lambaréné , Gabon

2. Unité de Recherche et de Diagnostics Spécialisés, Laboratoire National de Santé Publique/Centre Hospitalier Universitaire Mère Enfant Fondation Jeanne EBORI , Libreville , Gabon

3. Institut für Tropenmedizin, Universität Tübingen and German Center for Infection Research Tübingen , Tübingen , Germany

4. Department of Infectious Diseases, Center of Tropical Medicine and Travel Medicine, Amsterdam University Medical Centers, location University of Amsterdam, Amsterdam Infection & Immunity, Amsterdam Public Health, University of Amsterdam , Amsterdam , The Netherlands

5. Institute of Medical Microbiology, University Hospital Münster , Münster , Germany

Abstract

Abstract Background and Objectives Point-of-care testing using nonsputum samples like serum or plasma proteins can improve tuberculosis (TB) patients access to a definitive diagnosis, especially in resource-constrained and remote areas. Recently, approximately 400 proteins were identified as playing a role in the pathogenesis of TB, offering a translational clinical research repository for TB. In a previous manuscript, we proved the potential use of these proteins for point-of-care testing for active TB diagnosis. The present work aims to confirm the performance of single and combination proteins to select the best candidate biomarkers for further development as a diagnostic testing tool for active TB. Methods Seventy-four participants were assessed on the diagnostic performance of 17 single proteins and combinations of 2 to 4 proteins to diagnose active TB. The selection criteria included differential expression of the proteins between active TB and community-acquired pneumonia (CAP) and a performance rate ≥70% for active TB. Results SULT4A1, WASPF3, SPTLC1, FAM107B, SORCS2, and CYTOb561 were differentially expressed in TB compared to CAP patients. Two single proteins, SULT4A1 and WASPF3, performed ≥70% to discriminate active TB from CAP patients. The diagnostic performance of 3 protein-based combinations of active TB was 81% after leave-one-out cross-validation. Conclusion Single proteins and 3 protein-based combinations are candidate biomarkers for diagnosing active TB disease. A large and prospective study will confirm their performance as complementary diagnostic tools to rapid diagnostic methods for detecting active TB.

Funder

European and Developing Countries Clinical Trials Partnership

Publisher

Oxford University Press (OUP)

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