| Literature DB >> 27305362 |
A Razzaque Ahmed1, Marco Carrozzo2, Frédéric Caux3, Nicola Cirillo4, Marian Dmochowski5, Agustín España Alonso6, Robert Gniadecki7, Michael Hertl8, Maria J López-Zabalza9, Roberta Lotti10, Carlo Pincelli10, Mark Pittelkow11, Enno Schmidt12, Animesh A Sinha13, Eli Sprecher14, Sergei A Grando15.
Abstract
This viewpoint highlights major, partly controversial concepts about the pathogenesis of pemphigus. The monopathogenic theory explains intra-epidermal blistering through the "desmoglein (Dsg) compensation" hypothesis, according to which an antibody-dependent disabling of Dsg 1- and/or Dsg 3-mediated cell-cell attachments of keratinocytes (KCs) is sufficient to disrupt epidermal integrity and cause blistering. The multipathogenic theory explains intra-epidermal blistering through the "multiple hit" hypothesis stating that a simultaneous and synchronized inactivation of the physiological mechanisms regulating and/or mediating intercellular adhesion of KCs is necessary to disrupt epidermal integrity. The major premise for a multipathogenic theory is that a single type of autoantibody induces only reversible changes, so that affected KCs can recover due to a self-repair. The damage, however, becomes irreversible when the salvage pathway and/or other cell functions are altered by a partnering autoantibody and/or other pathogenic factors. Future studies are needed to (i) corroborate these findings, (ii) characterize in detail patient populations with non-Dsg-specific autoantibodies, and (iii) determine the extent of the contribution of non-Dsg antibodies in disease pathophysiology.Entities:
Keywords: FcRn; acantholysis; antimitochondrial antibody; autoantibody; autoantigen; autoimmunity; desmogleins 1 and 3; pemphigus vulgaris
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Year: 2016 PMID: 27305362 DOI: 10.1111/exd.13106
Source DB: PubMed Journal: Exp Dermatol ISSN: 0906-6705 Impact factor: 3.960