Gene expression patterns associated with multidrug therapy in multibacillary leprosy

Author:

Ferreira Helen,Leal-Calvo Thyago,Mendes Mayara Abud,Avanzi Charlotte,Busso Philippe,Benjak Andrej,Sales Anna Maria,Ferreira Cássio Porto,de Berrêdo-Pinho Márcia,Cole Stewart Thomas,Sarno Euzenir Nunes,Moraes Milton Ozório,Pinheiro Roberta Olmo

Abstract

Multidrug therapy (MDT) has been successfully used in the treatment of leprosy. However, although patients are cured after the completion of MDT, leprosy reactions, permanent disability, and occasional relapse/reinfection are frequently observed in patients. The immune system of multibacillary patients (MB) is not able to mount an effective cellular immune response against M. leprae. Consequently, clearance of bacilli from the body is a slow process and after 12 doses of MDT not all MB patients reduce bacillary index (BI). In this context, we recruited MB patients at the uptake and after 12-month of MDT. Patients were stratified according to the level of reduction of the BI after 12 doses MDT. A reduction of at least one log in BI was necessary to be considered a responder patient. We evaluated the pattern of host gene expression in skin samples with RNA sequencing before and after MDT and between samples from patients with or without one log reduction in BI. Our results demonstrated that after 12 doses of MDT there was a reduction in genes associated with lipid metabolism, inflammatory response, and cellular immune response among responders (APOBEC3A, LGALS17A, CXCL13, CXCL9, CALHM6, andIFNG). Also, by comparing MB patients with lower BI reduction versus responder patients, we identified high expression ofCDH19, TMPRSS4, PAX3, FA2H, HLA-V, FABP7, andSERPINA11before MDT. From the most differentially expressed genes, we observed that MDT modulates pathways related to immune response and lipid metabolism in skin cells from MB patients after MDT, with higher expression of genes likeCYP11A1, that are associated with cholesterol metabolism in the group with the worst response to treatment. Altogether, the data presented contribute to elucidate gene signatures and identify differentially expressed genes associated with MDT outcomes in MB patients.

Publisher

Frontiers Media SA

Subject

Infectious Diseases,Microbiology (medical),Immunology,Microbiology

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