Plakoglobin rescues adhesive defects induced by ectodomain truncation of the desmosomal cadherin desmoglein 1: Implications for exfoliative toxin-mediated skin blistering

Cory L. Simpson; Shin Ichiro Kojima; Victoria Cooper-Whitehair; Spiro Getsios; Kathleen J. Green

doi:10.2353/ajpath.2010.100397

Plakoglobin rescues adhesive defects induced by ectodomain truncation of the desmosomal cadherin desmoglein 1: Implications for exfoliative toxin-mediated skin blistering

Cory L. Simpson, Shin Ichiro Kojima, Victoria Cooper-Whitehair, Spiro Getsios, Kathleen J. Green

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

27 Scopus citations

Abstract

Desmoglein 1 (Dsg1) is a desmosomal cadherin that is essential to epidermal integrity. In the blistering diseases bullous impetigo and staphylococcal scaldedskin syndrome, pathogenesis depends on cleavage of Dsg1 by a bacterial protease, exfoliative toxin A, which removes residues 1 to 381 of the Dsg1 ectodomain. However, the cellular responses to Dsg1 cleavage that precipitate keratinocyte separation to induce blister formation are unknown. Here, we show that ectodomain-deleted Dsg1 (Δ381-Dsg1) mimics the toxin-cleaved cadherin, disrupts desmosomes, and reduces the mechanical integrity of keratinocyte sheets. In addition, we demonstrate that truncated Dsg1 remains associated with its catenin partner, plakoglobin, and causes a reduction in the levels of endogenous desmosomal cadherins in a dose-dependent manner, leading us to hypothesize that plakoglobin sequestration by truncated Dsg1 destabilizes other cadherins. Accordingly, a triple-point mutant of the ectodomain-deleted cadherin, which is uncoupled from plakoglobin, does not impair adhesion, indicating that this interaction is essential to the pathogenic potential of truncated Dsg1. Moreover, we demonstrate that increasing plakoglobin levels rescues cadherin expression, desmosome organization, and functional adhesion in cells expressing Δ381-Dsg1 or treated with exfoliative toxin A. Finally, we report that histone deacetylase inhibition up-regulates desmosomal cadherins and prevents the loss of adhesion induced by Dsg1 truncation. These findings further our understanding of the mechanism of exfoliative toxin-induced pathology and suggest novel strategies to suppress blistering in bulbous impetigo and staphylococcal scalded-skin syndrome.

Original language	English (US)
Pages (from-to)	2921-2937
Number of pages	17
Journal	American Journal of Pathology
Volume	177
Issue number	6
DOIs	https://doi.org/10.2353/ajpath.2010.100397
State	Published - Dec 2010

Funding

Supported by the National Institutes of Health (NIH) National Institute of Arthritis & Musculoskeletal & Skin Diseases (NIAMS) (grant R01-AR041836 to K.J.G.) , NIH National Institute for Environmental Health Sciences (NIEHS) (pre-doctoral fellowship F30-ES014990 to C.L.S.) and NIH National Cancer Institute (grant R01-CA122151 to K.J.G.), the Joseph L. Mayberry Endowment (K.J.G.), a Malkin Family Scholarship from the Robert H. Lurie Comprehensive Cancer Center (C.L.S.), a Northwestern University Presidential Fellowship (C.L.S.) and a Dermatology Foundation Career Development Award (to S.G.). The Northwestern University Skin Disease Research Center is supported by NIH NIAMS (grant P30-AR057216 ). Human keratinocytes were provided by the Northwestern University Skin Disease Research Center supported by the NIH NIAMS (grant P30-AR057216 ). Tissue processing and sectioning were provided by the Mouse Histology and Phenotyping Laboratory of Northwestern University supported by the NIH NCI (grant P30-CA060553 ).

ASJC Scopus subject areas

Pathology and Forensic Medicine

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10.2353/ajpath.2010.100397

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@article{d372dc1a25f1481c8e0e6d57fa3cbf91,

title = "Plakoglobin rescues adhesive defects induced by ectodomain truncation of the desmosomal cadherin desmoglein 1: Implications for exfoliative toxin-mediated skin blistering",

abstract = "Desmoglein 1 (Dsg1) is a desmosomal cadherin that is essential to epidermal integrity. In the blistering diseases bullous impetigo and staphylococcal scaldedskin syndrome, pathogenesis depends on cleavage of Dsg1 by a bacterial protease, exfoliative toxin A, which removes residues 1 to 381 of the Dsg1 ectodomain. However, the cellular responses to Dsg1 cleavage that precipitate keratinocyte separation to induce blister formation are unknown. Here, we show that ectodomain-deleted Dsg1 (Δ381-Dsg1) mimics the toxin-cleaved cadherin, disrupts desmosomes, and reduces the mechanical integrity of keratinocyte sheets. In addition, we demonstrate that truncated Dsg1 remains associated with its catenin partner, plakoglobin, and causes a reduction in the levels of endogenous desmosomal cadherins in a dose-dependent manner, leading us to hypothesize that plakoglobin sequestration by truncated Dsg1 destabilizes other cadherins. Accordingly, a triple-point mutant of the ectodomain-deleted cadherin, which is uncoupled from plakoglobin, does not impair adhesion, indicating that this interaction is essential to the pathogenic potential of truncated Dsg1. Moreover, we demonstrate that increasing plakoglobin levels rescues cadherin expression, desmosome organization, and functional adhesion in cells expressing Δ381-Dsg1 or treated with exfoliative toxin A. Finally, we report that histone deacetylase inhibition up-regulates desmosomal cadherins and prevents the loss of adhesion induced by Dsg1 truncation. These findings further our understanding of the mechanism of exfoliative toxin-induced pathology and suggest novel strategies to suppress blistering in bulbous impetigo and staphylococcal scalded-skin syndrome.",

author = "Simpson, {Cory L.} and Kojima, {Shin Ichiro} and Victoria Cooper-Whitehair and Spiro Getsios and Green, {Kathleen J.}",

note = "Funding Information: Supported by the National Institutes of Health (NIH) National Institute of Arthritis & Musculoskeletal & Skin Diseases (NIAMS) (grant R01-AR041836 to K.J.G.) , NIH National Institute for Environmental Health Sciences (NIEHS) (pre-doctoral fellowship F30-ES014990 to C.L.S.) and NIH National Cancer Institute (grant R01-CA122151 to K.J.G.), the Joseph L. Mayberry Endowment (K.J.G.), a Malkin Family Scholarship from the Robert H. Lurie Comprehensive Cancer Center (C.L.S.), a Northwestern University Presidential Fellowship (C.L.S.) and a Dermatology Foundation Career Development Award (to S.G.). The Northwestern University Skin Disease Research Center is supported by NIH NIAMS (grant P30-AR057216 ). Human keratinocytes were provided by the Northwestern University Skin Disease Research Center supported by the NIH NIAMS (grant P30-AR057216 ). Tissue processing and sectioning were provided by the Mouse Histology and Phenotyping Laboratory of Northwestern University supported by the NIH NCI (grant P30-CA060553 ). ",

year = "2010",

month = dec,

doi = "10.2353/ajpath.2010.100397",

language = "English (US)",

volume = "177",

pages = "2921--2937",

journal = "American Journal of Pathology",

issn = "0002-9440",

publisher = "Elsevier Inc.",

number = "6",

}

Plakoglobin rescues adhesive defects induced by ectodomain truncation of the desmosomal cadherin desmoglein 1: Implications for exfoliative toxin-mediated skin blistering. / Simpson, Cory L.; Kojima, Shin Ichiro; Cooper-Whitehair, Victoria et al.
In: American Journal of Pathology, Vol. 177, No. 6, 12.2010, p. 2921-2937.

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

TY - JOUR

T1 - Plakoglobin rescues adhesive defects induced by ectodomain truncation of the desmosomal cadherin desmoglein 1

T2 - Implications for exfoliative toxin-mediated skin blistering

AU - Simpson, Cory L.

AU - Kojima, Shin Ichiro

AU - Cooper-Whitehair, Victoria

AU - Getsios, Spiro

AU - Green, Kathleen J.

N1 - Funding Information: Supported by the National Institutes of Health (NIH) National Institute of Arthritis & Musculoskeletal & Skin Diseases (NIAMS) (grant R01-AR041836 to K.J.G.) , NIH National Institute for Environmental Health Sciences (NIEHS) (pre-doctoral fellowship F30-ES014990 to C.L.S.) and NIH National Cancer Institute (grant R01-CA122151 to K.J.G.), the Joseph L. Mayberry Endowment (K.J.G.), a Malkin Family Scholarship from the Robert H. Lurie Comprehensive Cancer Center (C.L.S.), a Northwestern University Presidential Fellowship (C.L.S.) and a Dermatology Foundation Career Development Award (to S.G.). The Northwestern University Skin Disease Research Center is supported by NIH NIAMS (grant P30-AR057216 ). Human keratinocytes were provided by the Northwestern University Skin Disease Research Center supported by the NIH NIAMS (grant P30-AR057216 ). Tissue processing and sectioning were provided by the Mouse Histology and Phenotyping Laboratory of Northwestern University supported by the NIH NCI (grant P30-CA060553 ).

PY - 2010/12

Y1 - 2010/12

N2 - Desmoglein 1 (Dsg1) is a desmosomal cadherin that is essential to epidermal integrity. In the blistering diseases bullous impetigo and staphylococcal scaldedskin syndrome, pathogenesis depends on cleavage of Dsg1 by a bacterial protease, exfoliative toxin A, which removes residues 1 to 381 of the Dsg1 ectodomain. However, the cellular responses to Dsg1 cleavage that precipitate keratinocyte separation to induce blister formation are unknown. Here, we show that ectodomain-deleted Dsg1 (Δ381-Dsg1) mimics the toxin-cleaved cadherin, disrupts desmosomes, and reduces the mechanical integrity of keratinocyte sheets. In addition, we demonstrate that truncated Dsg1 remains associated with its catenin partner, plakoglobin, and causes a reduction in the levels of endogenous desmosomal cadherins in a dose-dependent manner, leading us to hypothesize that plakoglobin sequestration by truncated Dsg1 destabilizes other cadherins. Accordingly, a triple-point mutant of the ectodomain-deleted cadherin, which is uncoupled from plakoglobin, does not impair adhesion, indicating that this interaction is essential to the pathogenic potential of truncated Dsg1. Moreover, we demonstrate that increasing plakoglobin levels rescues cadherin expression, desmosome organization, and functional adhesion in cells expressing Δ381-Dsg1 or treated with exfoliative toxin A. Finally, we report that histone deacetylase inhibition up-regulates desmosomal cadherins and prevents the loss of adhesion induced by Dsg1 truncation. These findings further our understanding of the mechanism of exfoliative toxin-induced pathology and suggest novel strategies to suppress blistering in bulbous impetigo and staphylococcal scalded-skin syndrome.

AB - Desmoglein 1 (Dsg1) is a desmosomal cadherin that is essential to epidermal integrity. In the blistering diseases bullous impetigo and staphylococcal scaldedskin syndrome, pathogenesis depends on cleavage of Dsg1 by a bacterial protease, exfoliative toxin A, which removes residues 1 to 381 of the Dsg1 ectodomain. However, the cellular responses to Dsg1 cleavage that precipitate keratinocyte separation to induce blister formation are unknown. Here, we show that ectodomain-deleted Dsg1 (Δ381-Dsg1) mimics the toxin-cleaved cadherin, disrupts desmosomes, and reduces the mechanical integrity of keratinocyte sheets. In addition, we demonstrate that truncated Dsg1 remains associated with its catenin partner, plakoglobin, and causes a reduction in the levels of endogenous desmosomal cadherins in a dose-dependent manner, leading us to hypothesize that plakoglobin sequestration by truncated Dsg1 destabilizes other cadherins. Accordingly, a triple-point mutant of the ectodomain-deleted cadherin, which is uncoupled from plakoglobin, does not impair adhesion, indicating that this interaction is essential to the pathogenic potential of truncated Dsg1. Moreover, we demonstrate that increasing plakoglobin levels rescues cadherin expression, desmosome organization, and functional adhesion in cells expressing Δ381-Dsg1 or treated with exfoliative toxin A. Finally, we report that histone deacetylase inhibition up-regulates desmosomal cadherins and prevents the loss of adhesion induced by Dsg1 truncation. These findings further our understanding of the mechanism of exfoliative toxin-induced pathology and suggest novel strategies to suppress blistering in bulbous impetigo and staphylococcal scalded-skin syndrome.

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Plakoglobin rescues adhesive defects induced by ectodomain truncation of the desmosomal cadherin desmoglein 1: Implications for exfoliative toxin-mediated skin blistering

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