Gliadin as a stimulator of innate responses in celiac disease
Gliadin as a stimulator of innate responses in celiac disease
In celiac disease (CD) we have the prototype of an immune mediated response dominated by the activation of the adaptive immune system and in particular of CD4+ HLA class II restricted T cells. Various seminal studies have established the precise mechanism of how antigen (prolamine) specific activation of CD4+ mucosal T cells occurs. Thus, CD is a condition in which T cells and their activation is the essential hinge in the pathogenic process. These functional studies have provided the explanation for the genetic association between CD and certain HLA alleles (HLA DQ2 and DQ8). These genetic, molecular and functional studies have permitted the clarification of a powerful Th1 dominated pro-inflammatory response that characterises the small intestine of active CD patients. Despite this unassailable set of information and reports there are some intriguing points that have been raised by a series of studies which have indicated that CD is not only defined by an aberrant prolamine-induced activation of the adaptive immune system. New evidence and re-assessments of old studies, point to a more complex pathogenic cascade, which may help to unravel some of the residual obscure points of CD pathogenesis. Here, we outline the current concepts that indicate a direct involvement of the adaptive immune system and we discuss all the evidence supporting a direct activation of the innate immune system by fragments of prolamines, which are not recognized T cell epitopes and how they could influence CD. The gliadin-induced activation of the ‘innate’ immune system might also have a significant role in the induction and persistence of many CD complications and most definitively for the most aggressive one, namely mucosal T cell lymphomas. We further suggest a novel way to harness the unwanted immune response to toxic prolamine, and thus indicate new potential therapeutic strategies to treat or at least control CD.
innate immunity, Celiac disease, gluten/gliadin, IL-15
913-918
Londei, M.
2d82e120-d610-4bb3-9f93-441ee4c7d419
Ciacci, C.
1726213f-9664-4738-8e1a-d064540dbd14
Ricciardelli, I.
c0a412c8-69d3-4146-83d9-aa508bbbe471
Vacca, L.
0130f2fe-933c-47a5-bde3-c0ed1469130c
Quaratino, S.
e111fc36-bc7e-461b-996d-849e97c51e44
Maiuri, L.
11e256c3-912e-4479-b19d-1f64e4f2fd46
2005
Londei, M.
2d82e120-d610-4bb3-9f93-441ee4c7d419
Ciacci, C.
1726213f-9664-4738-8e1a-d064540dbd14
Ricciardelli, I.
c0a412c8-69d3-4146-83d9-aa508bbbe471
Vacca, L.
0130f2fe-933c-47a5-bde3-c0ed1469130c
Quaratino, S.
e111fc36-bc7e-461b-996d-849e97c51e44
Maiuri, L.
11e256c3-912e-4479-b19d-1f64e4f2fd46
Londei, M., Ciacci, C., Ricciardelli, I., Vacca, L., Quaratino, S. and Maiuri, L.
(2005)
Gliadin as a stimulator of innate responses in celiac disease.
Molecular Immunology, 42 (8), .
(doi:10.1016/j.molimm.2004.12.005).
Abstract
In celiac disease (CD) we have the prototype of an immune mediated response dominated by the activation of the adaptive immune system and in particular of CD4+ HLA class II restricted T cells. Various seminal studies have established the precise mechanism of how antigen (prolamine) specific activation of CD4+ mucosal T cells occurs. Thus, CD is a condition in which T cells and their activation is the essential hinge in the pathogenic process. These functional studies have provided the explanation for the genetic association between CD and certain HLA alleles (HLA DQ2 and DQ8). These genetic, molecular and functional studies have permitted the clarification of a powerful Th1 dominated pro-inflammatory response that characterises the small intestine of active CD patients. Despite this unassailable set of information and reports there are some intriguing points that have been raised by a series of studies which have indicated that CD is not only defined by an aberrant prolamine-induced activation of the adaptive immune system. New evidence and re-assessments of old studies, point to a more complex pathogenic cascade, which may help to unravel some of the residual obscure points of CD pathogenesis. Here, we outline the current concepts that indicate a direct involvement of the adaptive immune system and we discuss all the evidence supporting a direct activation of the innate immune system by fragments of prolamines, which are not recognized T cell epitopes and how they could influence CD. The gliadin-induced activation of the ‘innate’ immune system might also have a significant role in the induction and persistence of many CD complications and most definitively for the most aggressive one, namely mucosal T cell lymphomas. We further suggest a novel way to harness the unwanted immune response to toxic prolamine, and thus indicate new potential therapeutic strategies to treat or at least control CD.
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Published date: 2005
Keywords:
innate immunity, Celiac disease, gluten/gliadin, IL-15
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Local EPrints ID: 26442
URI: http://eprints.soton.ac.uk/id/eprint/26442
ISSN: 0161-5890
PURE UUID: 4cde5d9a-0037-4563-83c2-8914b5e949e3
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Date deposited: 10 Apr 2006
Last modified: 15 Mar 2024 07:10
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Author:
M. Londei
Author:
C. Ciacci
Author:
I. Ricciardelli
Author:
L. Vacca
Author:
S. Quaratino
Author:
L. Maiuri
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