Viral infections as triggers for CNS autoimmune diseases via molecular mimicry

Top
Oral presentation

BMC Proceedings
Volume 2
Suppl 1

Viewing options:

Full text
PDF (128KB)

Related literature:

Articles citing this article
on Google Scholar
Other articles by authors
on Google Scholar

Martin R
Sospedra M

on PubMed

Martin R
Sospedra M
Related articles/pages
on Google

on Google Scholar

Tools:

Post to:

This article is part of the supplement: Infectious diseases of the nervous system: pathogenesis and worldwide impact .

Oral presentation

Viral infections as triggers for CNS autoimmune diseases via molecular mimicry

Roland Martin and Mireia Sospedra

Institute for Neuroimmunology and Clinical MS Resarch (inims*), Center for Molecular Neurobiology Hamburg (ZMNH), University Medical Center Eppendorf, Hamburg, Germany

author email corresponding author email

from Infectious diseases of the nervous system: pathogenesis and worldwide impact
Paris, France. 10–13 September 2008

BMC Proceedings 2008, 2(Suppl 1):S29

The electronic version of this abstract is the complete one and can be found online at: http://www.biomedcentral.com/1753-6561/2/S1/S29

Published:

23 September 2008

Oral presentation

It is well supported by epidemiological evidence that disease exacerbations of CNS autoimmune disorders such as multiple sclerosis can be triggered by viral infections. Similarly, it has been claimed that the development of MS is linked to environmental factors, particularly infections with specific viruses including EBV, HHV-6 and others. Two main mechanisms, by which autoimmune responses against CNS tissue can be induced, have been described, a) molecular mimicry, i.e. similarities in antigenic epitopes of viruses and tissue-specific autoantigens, and b) bystander activation, i.e. the induction of immune responses against autoantigens by unspecific activation of the innate immune system in the context of an infection.

The focus of the presentation will be on the mechanisms of molecular mimicry. This concept, which had originally been described by Fujinami and Oldstone and stipulated identical amino acid sequences between a peptide from self- and a viral protein, has evolved considerably during recent years. With a better understanding of the activation requirements and broader specificity of T cells, it has become clear that molecular mimicry is likely a frequent event and physiological under most circumstances. The context, in which molecular mimicry may become pathogenic and the evidence supporting its involvement in MS will be discussed.

This article is part of the supplement: Infectious diseases of the nervous system: pathogenesis and worldwide impact .

Viral infections as triggers for CNS autoimmune diseases via molecular mimicry

Oral presentation

Have something to say? Post a comment on this article!