Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid

Lan Lin; Tomoko Betsuyaku; Lisa Heimbach; Ning Li; David Rubenstein; Steven D. Shapiro; Lijia An; George J. Giudice; Luis A. Diaz; Robert M. Senior; Zhi Liu

doi:10.1016/j.matbio.2011.09.003

Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid

Lan Lin, Tomoko Betsuyaku, Lisa Heimbach, Ning Li, David Rubenstein, Steven D. Shapiro, Lijia An, George J. Giudice, Luis A. Diaz, Robert M. Senior, Zhi Liu

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54 Citations (Scopus)

Abstract

Bullous pemphigoid (BP) is an autoimmune subepidermal blistering disease associated with autoantibodies against the hemidesmosomal proteins BP180 and BP230. In the IgG passive transfer model of BP, blister formation is triggered by anti-BP180 IgG and depends on complement activation, mast cell degranulation, and neutrophil recruitment. Mice lacking neutrophil elastase (NE) do not develop experimental BP. Here, we demonstrated that NE degrades recombinant mouse BP180 within the immunodominant extracellular domain at amino acid positions 506 and 561, generating peptide p561 and peptide p506. Peptide p561 is chemotactic for neutrophils both in vitro and in vivo. Local injection of NE into B6 mice recruits neutrophils to the skin, and neutrophil infiltration is completely blocked by co-injection with the NE inhibitor α1-proteinase inhibitor. More importantly, NE directly cleaves BP180 in mouse and human skin, as well as the native human BP180 trimer molecule. These results demonstrate that (i) NE directly damages the extracellular matrix and (ii) NE degradation of mouse BP180 generates neutrophil chemotactic peptides that amplify disease severity at the early stage of the disease.

Original language	English
Pages (from-to)	38-44
Number of pages	7
Journal	Matrix Biology
Volume	31
Issue number	1
DOIs	https://doi.org/10.1016/j.matbio.2011.09.003
Publication status	Published - 2012 Jan
Externally published	Yes

Keywords

Autoimmune mouse model
BP180
Basement membrane
Bullous pemphigoid
Chemotaxis
Neutrophil elastase

ASJC Scopus subject areas

Molecular Biology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.matbio.2011.09.003

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Lin, L., Betsuyaku, T., Heimbach, L., Li, N., Rubenstein, D., Shapiro, S. D., An, L., Giudice, G. J., Diaz, L. A., Senior, R. M., & Liu, Z. (2012). Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid. Matrix Biology, 31(1), 38-44. https://doi.org/10.1016/j.matbio.2011.09.003

Lin, L, Betsuyaku, T, Heimbach, L, Li, N, Rubenstein, D, Shapiro, SD, An, L, Giudice, GJ, Diaz, LA, Senior, RM & Liu, Z 2012, 'Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid', Matrix Biology, vol. 31, no. 1, pp. 38-44. https://doi.org/10.1016/j.matbio.2011.09.003

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title = "Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid",

abstract = "Bullous pemphigoid (BP) is an autoimmune subepidermal blistering disease associated with autoantibodies against the hemidesmosomal proteins BP180 and BP230. In the IgG passive transfer model of BP, blister formation is triggered by anti-BP180 IgG and depends on complement activation, mast cell degranulation, and neutrophil recruitment. Mice lacking neutrophil elastase (NE) do not develop experimental BP. Here, we demonstrated that NE degrades recombinant mouse BP180 within the immunodominant extracellular domain at amino acid positions 506 and 561, generating peptide p561 and peptide p506. Peptide p561 is chemotactic for neutrophils both in vitro and in vivo. Local injection of NE into B6 mice recruits neutrophils to the skin, and neutrophil infiltration is completely blocked by co-injection with the NE inhibitor α1-proteinase inhibitor. More importantly, NE directly cleaves BP180 in mouse and human skin, as well as the native human BP180 trimer molecule. These results demonstrate that (i) NE directly damages the extracellular matrix and (ii) NE degradation of mouse BP180 generates neutrophil chemotactic peptides that amplify disease severity at the early stage of the disease.",

keywords = "Autoimmune mouse model, BP180, Basement membrane, Bullous pemphigoid, Chemotaxis, Neutrophil elastase",

author = "Lan Lin and Tomoko Betsuyaku and Lisa Heimbach and Ning Li and David Rubenstein and Shapiro, {Steven D.} and Lijia An and Giudice, {George J.} and Diaz, {Luis A.} and Senior, {Robert M.} and Zhi Liu",

note = "Funding Information: We thank Dr. Pamela Groben Ms. Joy Miller for routine histology. This work was supported in part by U.S. Public Health Service NIH grants AI40768 and AI61430 (Z. L.), AR052109 and AR053313 (N.L.), AI49427 (D.S.R.), AR32599 and AR32081 (L.A.D.), R01 HL082541 (S.D.S.), NHLBI/NIH P01 HL29594 and the Alan A. and Edith L. Wolf Charitable Trust/Barnes-Jewish Hospital Foundation (R.S.). L.L. was supported in part by a pre-doctoral fellowship from China Scholarship Council . L.H. was supported in part by a pre-doctoral fellowship from NIH AI007273 .",

year = "2012",

month = jan,

doi = "10.1016/j.matbio.2011.09.003",

language = "English",

volume = "31",

pages = "38--44",

journal = "Matrix Biology",

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T1 - Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid

AU - Lin, Lan

AU - Betsuyaku, Tomoko

AU - Heimbach, Lisa

AU - Li, Ning

AU - Rubenstein, David

AU - Shapiro, Steven D.

AU - An, Lijia

AU - Giudice, George J.

AU - Diaz, Luis A.

AU - Senior, Robert M.

AU - Liu, Zhi

N1 - Funding Information: We thank Dr. Pamela Groben Ms. Joy Miller for routine histology. This work was supported in part by U.S. Public Health Service NIH grants AI40768 and AI61430 (Z. L.), AR052109 and AR053313 (N.L.), AI49427 (D.S.R.), AR32599 and AR32081 (L.A.D.), R01 HL082541 (S.D.S.), NHLBI/NIH P01 HL29594 and the Alan A. and Edith L. Wolf Charitable Trust/Barnes-Jewish Hospital Foundation (R.S.). L.L. was supported in part by a pre-doctoral fellowship from China Scholarship Council . L.H. was supported in part by a pre-doctoral fellowship from NIH AI007273 .

PY - 2012/1

Y1 - 2012/1

N2 - Bullous pemphigoid (BP) is an autoimmune subepidermal blistering disease associated with autoantibodies against the hemidesmosomal proteins BP180 and BP230. In the IgG passive transfer model of BP, blister formation is triggered by anti-BP180 IgG and depends on complement activation, mast cell degranulation, and neutrophil recruitment. Mice lacking neutrophil elastase (NE) do not develop experimental BP. Here, we demonstrated that NE degrades recombinant mouse BP180 within the immunodominant extracellular domain at amino acid positions 506 and 561, generating peptide p561 and peptide p506. Peptide p561 is chemotactic for neutrophils both in vitro and in vivo. Local injection of NE into B6 mice recruits neutrophils to the skin, and neutrophil infiltration is completely blocked by co-injection with the NE inhibitor α1-proteinase inhibitor. More importantly, NE directly cleaves BP180 in mouse and human skin, as well as the native human BP180 trimer molecule. These results demonstrate that (i) NE directly damages the extracellular matrix and (ii) NE degradation of mouse BP180 generates neutrophil chemotactic peptides that amplify disease severity at the early stage of the disease.

AB - Bullous pemphigoid (BP) is an autoimmune subepidermal blistering disease associated with autoantibodies against the hemidesmosomal proteins BP180 and BP230. In the IgG passive transfer model of BP, blister formation is triggered by anti-BP180 IgG and depends on complement activation, mast cell degranulation, and neutrophil recruitment. Mice lacking neutrophil elastase (NE) do not develop experimental BP. Here, we demonstrated that NE degrades recombinant mouse BP180 within the immunodominant extracellular domain at amino acid positions 506 and 561, generating peptide p561 and peptide p506. Peptide p561 is chemotactic for neutrophils both in vitro and in vivo. Local injection of NE into B6 mice recruits neutrophils to the skin, and neutrophil infiltration is completely blocked by co-injection with the NE inhibitor α1-proteinase inhibitor. More importantly, NE directly cleaves BP180 in mouse and human skin, as well as the native human BP180 trimer molecule. These results demonstrate that (i) NE directly damages the extracellular matrix and (ii) NE degradation of mouse BP180 generates neutrophil chemotactic peptides that amplify disease severity at the early stage of the disease.

KW - Autoimmune mouse model

KW - BP180

KW - Basement membrane

KW - Bullous pemphigoid

KW - Chemotaxis

KW - Neutrophil elastase

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AN - SCOPUS:84855599954

SN - 0945-053X

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JO - Matrix Biology

JF - Matrix Biology

IS - 1

ER -

Neutrophil elastase cleaves the murine hemidesmosomal protein BP180/type XVII collagen and generates degradation products that modulate experimental bullous pemphigoid

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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