Gene set signature of reversal reaction type I in leprosy patients.

Leprosy reversal reactions type 1 (T1R) are acute immune episodes that affect a subset of leprosy patients and remain a major cause of nerve damage. Little is known about the relative importance of innate versus environmental factors in the pathogenesis of T1R. In a retrospective design, we evaluate...

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Main Authors: Marianna Orlova, Aurélie Cobat, Nguyen Thu Huong, Nguyen Ngoc Ba, Nguyen Van Thuc, John Spencer, Yohann Nédélec, Luis Barreiro, Vu Hong Thai, Laurent Abel, Alexandre Alcaïs, Erwin Schurr
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC3708838?pdf=render
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spelling doaj-3f698fb2adf94e9b9903d22fdb5004312020-11-24T21:32:48ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042013-01-0197e100362410.1371/journal.pgen.1003624Gene set signature of reversal reaction type I in leprosy patients.Marianna OrlovaAurélie CobatNguyen Thu HuongNguyen Ngoc BaNguyen Van ThucJohn SpencerYohann NédélecLuis BarreiroVu Hong ThaiLaurent AbelAlexandre AlcaïsErwin SchurrLeprosy reversal reactions type 1 (T1R) are acute immune episodes that affect a subset of leprosy patients and remain a major cause of nerve damage. Little is known about the relative importance of innate versus environmental factors in the pathogenesis of T1R. In a retrospective design, we evaluated innate differences in response to Mycobacterium leprae between healthy individuals and former leprosy patients affected or free of T1R by analyzing the transcriptome response of whole blood to M. leprae sonicate. Validation of results was conducted in a subsequent prospective study. We observed the differential expression of 581 genes upon exposure of whole blood to M. leprae sonicate in the retrospective study. We defined a 44 T1R gene set signature of differentially regulated genes. The majority of the T1R set genes were represented by three functional groups: i) pro-inflammatory regulators; ii) arachidonic acid metabolism mediators; and iii) regulators of anti-inflammation. The validity of the T1R gene set signature was replicated in the prospective arm of the study. The T1R genetic signature encompasses genes encoding pro- and anti-inflammatory mediators of innate immunity. This suggests an innate defect in the regulation of the inflammatory response to M. leprae antigens. The identified T1R gene set represents a critical first step towards a genetic profile of leprosy patients who are at increased risk of T1R and concomitant nerve damage.http://europepmc.org/articles/PMC3708838?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Marianna Orlova
Aurélie Cobat
Nguyen Thu Huong
Nguyen Ngoc Ba
Nguyen Van Thuc
John Spencer
Yohann Nédélec
Luis Barreiro
Vu Hong Thai
Laurent Abel
Alexandre Alcaïs
Erwin Schurr
spellingShingle Marianna Orlova
Aurélie Cobat
Nguyen Thu Huong
Nguyen Ngoc Ba
Nguyen Van Thuc
John Spencer
Yohann Nédélec
Luis Barreiro
Vu Hong Thai
Laurent Abel
Alexandre Alcaïs
Erwin Schurr
Gene set signature of reversal reaction type I in leprosy patients.
PLoS Genetics
author_facet Marianna Orlova
Aurélie Cobat
Nguyen Thu Huong
Nguyen Ngoc Ba
Nguyen Van Thuc
John Spencer
Yohann Nédélec
Luis Barreiro
Vu Hong Thai
Laurent Abel
Alexandre Alcaïs
Erwin Schurr
author_sort Marianna Orlova
title Gene set signature of reversal reaction type I in leprosy patients.
title_short Gene set signature of reversal reaction type I in leprosy patients.
title_full Gene set signature of reversal reaction type I in leprosy patients.
title_fullStr Gene set signature of reversal reaction type I in leprosy patients.
title_full_unstemmed Gene set signature of reversal reaction type I in leprosy patients.
title_sort gene set signature of reversal reaction type i in leprosy patients.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2013-01-01
description Leprosy reversal reactions type 1 (T1R) are acute immune episodes that affect a subset of leprosy patients and remain a major cause of nerve damage. Little is known about the relative importance of innate versus environmental factors in the pathogenesis of T1R. In a retrospective design, we evaluated innate differences in response to Mycobacterium leprae between healthy individuals and former leprosy patients affected or free of T1R by analyzing the transcriptome response of whole blood to M. leprae sonicate. Validation of results was conducted in a subsequent prospective study. We observed the differential expression of 581 genes upon exposure of whole blood to M. leprae sonicate in the retrospective study. We defined a 44 T1R gene set signature of differentially regulated genes. The majority of the T1R set genes were represented by three functional groups: i) pro-inflammatory regulators; ii) arachidonic acid metabolism mediators; and iii) regulators of anti-inflammation. The validity of the T1R gene set signature was replicated in the prospective arm of the study. The T1R genetic signature encompasses genes encoding pro- and anti-inflammatory mediators of innate immunity. This suggests an innate defect in the regulation of the inflammatory response to M. leprae antigens. The identified T1R gene set represents a critical first step towards a genetic profile of leprosy patients who are at increased risk of T1R and concomitant nerve damage.
url http://europepmc.org/articles/PMC3708838?pdf=render
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