Use of Protein Antigens for Early Serological Diagnosis of Leprosy

Overview

Journal Clin Vaccine Immunol

Publisher American Society for Microbiology

Specialties Allergy & Immunology
Pathology

Date 2007 Sep 28

PMID 17898185

Citations 64

Authors

Malcolm S Duthie

Wakako Goto

Greg C Ireton

Stephen T Reece

Ludimila P V Cardoso

Celina M T Martelli

Mariane M A Stefani

Maria Nakatani

Robson Crusue de Jesus

Eduardo M Netto

Ma V F Balagon

Esterlina Tan

Robert H Gelber

Yumi Maeda

Masahiko Makino

Dan Hoft

Steven G Reed

Affiliations

Soon will be listed here.

Abstract

Leprosy is a chronic and debilitating human disease caused by infection with the Mycobacterium leprae bacillus. Despite the marked reduction in the number of registered worldwide leprosy cases as a result of the widespread use of multidrug therapy, the number of new cases detected each year remains relatively stable. This indicates that M. leprae is still being transmitted and that, without earlier diagnosis, M. leprae infection will continue to pose a health problem. Current diagnostic techniques, based on the appearance of clinical symptoms or of immunoglobulin M (IgM) antibodies that recognize the bacterial phenolic glycolipid I, are unable to reliably identify early-stage leprosy. In this study we examine the ability of IgG within leprosy patient sera to bind several M. leprae protein antigens. As expected, multibacillary leprosy patients provided stronger responses than paucibacillary leprosy patients. We demonstrate that the geographic locations of the patients can influence the antigens they recognize but that ML0405 and ML2331 are recognized by sera from diverse regions (the Philippines, coastal and central Brazil, and Japan). A fusion construct of these two proteins (designated leprosy IDRI diagnostic 1 [LID-1]) retained the diagnostic activity of the component antigens. Upon testing against a panel of prospective sera from individuals who developed leprosy, we determined that LID-1 was capable of diagnosing leprosy 6 to 8 months before the onset of clinical symptoms. A serological diagnostic test capable of identifying and allowing treatment of early-stage leprosy could reduce transmission, prevent functional disabilities and stigmatizing deformities, and facilitate leprosy eradication.

Citing Articles

Challenges and advances in serological and molecular tests to aid leprosy diagnosis.

Lopes-Luz L, Saavedra D, Fogaca M, Buhrer-Sekula S, Stefani M Exp Biol Med (Maywood). 2023; 248(22):2083-2094.

PMID: 38059475 PMC: 10800132. DOI: 10.1177/15353702231209422.

HSP60 mimetic peptides from Mycobacterium leprae as new antigens for immunodiagnosis of Leprosy.

Lima M, Correa M, Moraes E, Oliveira J, de Souza Santos P, de Souza A AMB Express. 2023; 13(1):120.

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and host immune transcriptomic signatures for reactional states in leprosy.

Das M, David D, Horo I, van Hooij A, Tio-Coma M, Geluk A Front Microbiol. 2023; 14:1113318.

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In silico designing of a recombinant multi-epitope antigen for leprosy diagnosis.

Lemes M, Rodrigues T, Jaiswal A, Tiwari S, Sales-Campos H, Andrade-Silva L J Genet Eng Biotechnol. 2022; 20(1):128.

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Arginase 1 is a marker of protection against illness in contacts of leprosy patients.

Prata R, Mendes M, Soares V, Franca-Costa J, Maria Sales A, Duppre N Sci Rep. 2022; 12(1):7850.

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