Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology

A. Razzaque Ahmed; Marco Carrozzo; Frédéric Caux; Nicola Cirillo; Marian Dmochowski; Agustín España Alonso; Robert Gniadecki; Michael Hertl; Maria J. López-Zabalza; Roberta Lotti; Carlo Pincelli; Mark Pittelkow; Enno Schmidt; Animesh A. Sinha; Eli Sprecher; Sergei A. Grando

doi:10.1111/exd.13106

Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology

A. Razzaque Ahmed
, Marco Carrozzo
, Frédéric Caux
, Nicola Cirillo
, Marian Dmochowski
, Agustín España Alonso
, Robert Gniadecki
, Michael Hertl
, Maria J. López-Zabalza
, Roberta Lotti
, Carlo Pincelli
, Mark Pittelkow
, Enno Schmidt
, Animesh A. Sinha
, Eli Sprecher
, Sergei A. Grando

Department of Dermatology

Tufts University
Newcastle University
Université Paris 13
University of Melbourne
University of Medical Sciences Poznan
University of Navarra
University of Alberta
University of Marburg
University of Modena and Reggio Emilia
Mayo Clinic Arizona
University of Lübeck
Tel Aviv Sourasky Medical Center
University of California at Irvine

Research output: Contribution to journal › Article › peer-review

73 Scopus citations

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-Dsgspecific autoantibodies, and (iii) determine the extent of the contribution of non-Dsg antibodies in disease pathophysiology.

Original language	English
Pages (from-to)	839-846
Number of pages	8
Journal	Experimental Dermatology
Volume	25
Issue number	11
DOIs	https://doi.org/10.1111/exd.13106
State	Published - Nov 1 2016

Keywords

Acantholysis
Antimitochondrial antibody
Autoantibody
Autoantigen
Autoimmunity
Desmogleins 1 and 3
FcRn
Pemphigus vulgaris

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10.1111/exd.13106

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Ahmed, A. R., Carrozzo, M., Caux, F., Cirillo, N., Dmochowski, M., Alonso, A. E., Gniadecki, R., Hertl, M., López-Zabalza, M. J., Lotti, R., Pincelli, C., Pittelkow, M., Schmidt, E., Sinha, A. A., Sprecher, E., & Grando, S. A. (2016). Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology. Experimental Dermatology, 25(11), 839-846. https://doi.org/10.1111/exd.13106

@article{a23a0b20323748479ea87701d297f089,

title = "Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology",

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-Dsgspecific autoantibodies, and (iii) determine the extent of the contribution of non-Dsg antibodies in disease pathophysiology.",

keywords = "Acantholysis, Antimitochondrial antibody, Autoantibody, Autoantigen, Autoimmunity, Desmogleins 1 and 3, FcRn, Pemphigus vulgaris",

author = "Ahmed, \{A. Razzaque\} and Marco Carrozzo and Fr{\'e}d{\'e}ric Caux and Nicola Cirillo and Marian Dmochowski and Alonso, \{Agust{\'i}n Espa{\~n}a\} and Robert Gniadecki and Michael Hertl and L{\'o}pez-Zabalza, \{Maria J.\} and Roberta Lotti and Carlo Pincelli and Mark Pittelkow and Enno Schmidt and Sinha, \{Animesh A.\} and Eli Sprecher and Grando, \{Sergei A.\}",

note = "Publisher Copyright: {\textcopyright} 2016 The Authors Experimental Dermatology.",

year = "2016",

month = nov,

day = "1",

doi = "10.1111/exd.13106",

language = "English",

volume = "25",

pages = "839--846",

journal = "Experimental Dermatology",

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Ahmed, AR, Carrozzo, M, Caux, F, Cirillo, N, Dmochowski, M, Alonso, AE, Gniadecki, R, Hertl, M, López-Zabalza, MJ, Lotti, R, Pincelli, C, Pittelkow, M, Schmidt, E, Sinha, AA, Sprecher, E & Grando, SA 2016, 'Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology', Experimental Dermatology, vol. 25, no. 11, pp. 839-846. https://doi.org/10.1111/exd.13106

TY - JOUR

T1 - Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology

AU - Ahmed, A. Razzaque

AU - Carrozzo, Marco

AU - Caux, Frédéric

AU - Cirillo, Nicola

AU - Dmochowski, Marian

AU - Alonso, Agustín España

AU - Gniadecki, Robert

AU - Hertl, Michael

AU - López-Zabalza, Maria J.

AU - Lotti, Roberta

AU - Pincelli, Carlo

AU - Pittelkow, Mark

AU - Schmidt, Enno

AU - Sinha, Animesh A.

AU - Sprecher, Eli

AU - Grando, Sergei A.

PY - 2016/11/1

Y1 - 2016/11/1

N2 - 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-Dsgspecific autoantibodies, and (iii) determine the extent of the contribution of non-Dsg antibodies in disease pathophysiology.

AB - 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-Dsgspecific autoantibodies, and (iii) determine the extent of the contribution of non-Dsg antibodies in disease pathophysiology.

KW - Acantholysis

KW - Antimitochondrial antibody

KW - Autoantibody

KW - Autoantigen

KW - Autoimmunity

KW - Desmogleins 1 and 3

KW - FcRn

KW - Pemphigus vulgaris

UR - https://www.scopus.com/pages/publications/85008352849

U2 - 10.1111/exd.13106

DO - 10.1111/exd.13106

M3 - Article

C2 - 27305362

AN - SCOPUS:85008352849

SN - 0906-6705

VL - 25

SP - 839

EP - 846

JO - Experimental Dermatology

JF - Experimental Dermatology

IS - 11

ER -

Monopathogenic vs multipathogenic explanations of pemphigus pathophysiology

Abstract

Keywords

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