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Laminin 5 Binds the NC-1 Domain of Type VII Collagen

Mutational analyses of genes that encode components of the anchoring complex underlying the basolateral surface of external epithelia indicate that this structure is the major element providing for resistance to external friction. Ultrastructurally, laminin 5 (α3β3γ2; a component of the anchoring fi...

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Autores principales: Rousselle, Patricia, Keene, Douglas R., Ruggiero, Florence, Champliaud, Marie-France, van der Rest, Michel, Burgeson, Robert E.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1997
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2141627/
https://www.ncbi.nlm.nih.gov/pubmed/9245798
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author Rousselle, Patricia
Keene, Douglas R.
Ruggiero, Florence
Champliaud, Marie-France
van der Rest, Michel
Burgeson, Robert E.
author_facet Rousselle, Patricia
Keene, Douglas R.
Ruggiero, Florence
Champliaud, Marie-France
van der Rest, Michel
Burgeson, Robert E.
author_sort Rousselle, Patricia
collection PubMed
description Mutational analyses of genes that encode components of the anchoring complex underlying the basolateral surface of external epithelia indicate that this structure is the major element providing for resistance to external friction. Ultrastructurally, laminin 5 (α3β3γ2; a component of the anchoring filament) appears as a thin filament bridging the hemidesmosome with the anchoring fibrils. Laminin 5 binds the cell surface through hemidesmosomal integrin α6β4. However, the interaction of laminin 5 with the anchoring fibril (type VII collagen) has not been elucidated. In this study we demonstrate that monomeric laminin 5 binds the NH(2)-terminal NC-1 domain of type VII collagen. The binding is dependent upon the native conformation of both laminin 5 and type VII collagen NC-1. Laminin 6 (α3β1γ1) has no detectable affinity for type VII collagen NC-1, indicating that the binding is mediated by the β3 and/or γ2 chains of laminin 5. Approximately half of the laminin 5 solubilized from human amnion or skin is covalently complexed with laminins 6 or 7 (α3β2γ1). The adduction occurs between the NH(2) terminus of laminin 5 and the branch point of the short arms of laminins 6 or 7. The results are consistent with the presumed orientation of laminin 5, having the COOH-terminal G domain apposed to the hemidesmosomal integrin, and the NH(2)-terminal domains within the lamina densa. The results also support a model predicting that monomeric laminin 5 constitutes the anchoring filaments and bridges integrin α6β4 with type VII collagen, and the laminin 5–6/7 complexes are present within the interhemidesmosomal spaces bound at least by integrin α3β1 where they may mediate basement membrane assembly or stability, but contribute less significantly to epithelial friction resistance.
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spelling pubmed-21416272008-05-01 Laminin 5 Binds the NC-1 Domain of Type VII Collagen Rousselle, Patricia Keene, Douglas R. Ruggiero, Florence Champliaud, Marie-France van der Rest, Michel Burgeson, Robert E. J Cell Biol Article Mutational analyses of genes that encode components of the anchoring complex underlying the basolateral surface of external epithelia indicate that this structure is the major element providing for resistance to external friction. Ultrastructurally, laminin 5 (α3β3γ2; a component of the anchoring filament) appears as a thin filament bridging the hemidesmosome with the anchoring fibrils. Laminin 5 binds the cell surface through hemidesmosomal integrin α6β4. However, the interaction of laminin 5 with the anchoring fibril (type VII collagen) has not been elucidated. In this study we demonstrate that monomeric laminin 5 binds the NH(2)-terminal NC-1 domain of type VII collagen. The binding is dependent upon the native conformation of both laminin 5 and type VII collagen NC-1. Laminin 6 (α3β1γ1) has no detectable affinity for type VII collagen NC-1, indicating that the binding is mediated by the β3 and/or γ2 chains of laminin 5. Approximately half of the laminin 5 solubilized from human amnion or skin is covalently complexed with laminins 6 or 7 (α3β2γ1). The adduction occurs between the NH(2) terminus of laminin 5 and the branch point of the short arms of laminins 6 or 7. The results are consistent with the presumed orientation of laminin 5, having the COOH-terminal G domain apposed to the hemidesmosomal integrin, and the NH(2)-terminal domains within the lamina densa. The results also support a model predicting that monomeric laminin 5 constitutes the anchoring filaments and bridges integrin α6β4 with type VII collagen, and the laminin 5–6/7 complexes are present within the interhemidesmosomal spaces bound at least by integrin α3β1 where they may mediate basement membrane assembly or stability, but contribute less significantly to epithelial friction resistance. The Rockefeller University Press 1997-08-11 /pmc/articles/PMC2141627/ /pubmed/9245798 Text en This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Rousselle, Patricia
Keene, Douglas R.
Ruggiero, Florence
Champliaud, Marie-France
van der Rest, Michel
Burgeson, Robert E.
Laminin 5 Binds the NC-1 Domain of Type VII Collagen
title Laminin 5 Binds the NC-1 Domain of Type VII Collagen
title_full Laminin 5 Binds the NC-1 Domain of Type VII Collagen
title_fullStr Laminin 5 Binds the NC-1 Domain of Type VII Collagen
title_full_unstemmed Laminin 5 Binds the NC-1 Domain of Type VII Collagen
title_short Laminin 5 Binds the NC-1 Domain of Type VII Collagen
title_sort laminin 5 binds the nc-1 domain of type vii collagen
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2141627/
https://www.ncbi.nlm.nih.gov/pubmed/9245798
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