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Lack of nidogen-1 and -2 prevents basement membrane assembly in skin-organotypic coculture

Lack of nidogen-1 and -2 prevents basement membrane assembly in skin-organotypic coculture
Lack of nidogen-1 and -2 prevents basement membrane assembly in skin-organotypic coculture
Nidogens are considered as classical linkers joining laminin and collagen IV networks in basement membranes (BMs); however, recent genetic approaches have suggested that nidogens function in a tissue-specific and developmental context. Thus, in mice lacking both nidogen-1 and -2 heart and lung were severely affected, causing neonatal death. Furthermore, in various locations, extravasation of erythrocytes was observed implying microvascular defects. Mice expressing solely either isoform, had a functional BM, although nidogen-2 binds with lower affinity to the laminin 1 chain. Having previously blocked BM formation by interfering with nidogen-1 binding to laminin in skin-organotypic cocultures, here we investigated the roles of nidogen-1 and -2 in this model. For that purpose, human HaCaT cells were grown in three-dimensional cocultures on collagen matrices containing murine fibroblasts of varying nidogen deficiency. As with our experiments blocking laminin–nidogen interaction, lack of both nidogens completely prevented BM deposition and ultrastructural assembly of BM and hemidesmosomes, although other BM proteins remained detectable at comparable levels with no signs of degradation. Supplementation by recombinant nidogen-1 or -2 restored these structures, as shown by immunofluorescence and electron microscopy, confirming that in this system nidogen-2 is equivalent to nidogen-1, and both can promote the development of a functional BM zone.
0022-202X
545-554
Nischt, Roswitha
a21a90aa-1297-42f1-acff-25b2fdb890e5
Schmidt, Cathrine
74cdee4e-fdf1-49cf-b193-fc4cbc5494b1
Mirancea, Nicolae
7266daa5-efd9-407e-bf90-fdf966e73ad5
Baranowsky, Anke
0f3869ce-94e3-4f5e-b1c6-b6069b77a200
Mokkapati, Sharada
2450f3e7-fbb4-4ec3-a856-b74035a2370a
Smyth, Neil
0eba2a40-3b43-4d40-bb64-621bd7e9d505
Woenne, Eva C.
e6848880-11b1-4bf6-addd-29feda2aa52a
Stark, Hans-Jürgen
5d309878-86ca-4070-b1a0-525a0b180002
Boukamp, Petra
d1e4a3ec-ba35-4000-89d4-c3535220c6e1
Breitkreutz, Dirk
2bb033ee-bdb7-408b-8a8a-68ce82f31816
Nischt, Roswitha
a21a90aa-1297-42f1-acff-25b2fdb890e5
Schmidt, Cathrine
74cdee4e-fdf1-49cf-b193-fc4cbc5494b1
Mirancea, Nicolae
7266daa5-efd9-407e-bf90-fdf966e73ad5
Baranowsky, Anke
0f3869ce-94e3-4f5e-b1c6-b6069b77a200
Mokkapati, Sharada
2450f3e7-fbb4-4ec3-a856-b74035a2370a
Smyth, Neil
0eba2a40-3b43-4d40-bb64-621bd7e9d505
Woenne, Eva C.
e6848880-11b1-4bf6-addd-29feda2aa52a
Stark, Hans-Jürgen
5d309878-86ca-4070-b1a0-525a0b180002
Boukamp, Petra
d1e4a3ec-ba35-4000-89d4-c3535220c6e1
Breitkreutz, Dirk
2bb033ee-bdb7-408b-8a8a-68ce82f31816

Nischt, Roswitha, Schmidt, Cathrine, Mirancea, Nicolae, Baranowsky, Anke, Mokkapati, Sharada, Smyth, Neil, Woenne, Eva C., Stark, Hans-Jürgen, Boukamp, Petra and Breitkreutz, Dirk (2007) Lack of nidogen-1 and -2 prevents basement membrane assembly in skin-organotypic coculture. Journal of Investigative Dermatology, 127 (3), 545-554. (doi:10.1038/sj.jid.5700562).

Record type: Article

Abstract

Nidogens are considered as classical linkers joining laminin and collagen IV networks in basement membranes (BMs); however, recent genetic approaches have suggested that nidogens function in a tissue-specific and developmental context. Thus, in mice lacking both nidogen-1 and -2 heart and lung were severely affected, causing neonatal death. Furthermore, in various locations, extravasation of erythrocytes was observed implying microvascular defects. Mice expressing solely either isoform, had a functional BM, although nidogen-2 binds with lower affinity to the laminin 1 chain. Having previously blocked BM formation by interfering with nidogen-1 binding to laminin in skin-organotypic cocultures, here we investigated the roles of nidogen-1 and -2 in this model. For that purpose, human HaCaT cells were grown in three-dimensional cocultures on collagen matrices containing murine fibroblasts of varying nidogen deficiency. As with our experiments blocking laminin–nidogen interaction, lack of both nidogens completely prevented BM deposition and ultrastructural assembly of BM and hemidesmosomes, although other BM proteins remained detectable at comparable levels with no signs of degradation. Supplementation by recombinant nidogen-1 or -2 restored these structures, as shown by immunofluorescence and electron microscopy, confirming that in this system nidogen-2 is equivalent to nidogen-1, and both can promote the development of a functional BM zone.

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Published date: March 2007

Identifiers

Local EPrints ID: 56276
URI: http://eprints.soton.ac.uk/id/eprint/56276
ISSN: 0022-202X
PURE UUID: 3ca55af3-f541-4bcf-86b0-2da6ae54e593

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Date deposited: 08 Aug 2008
Last modified: 15 Mar 2024 11:00

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Contributors

Author: Roswitha Nischt
Author: Cathrine Schmidt
Author: Nicolae Mirancea
Author: Anke Baranowsky
Author: Sharada Mokkapati
Author: Neil Smyth
Author: Eva C. Woenne
Author: Hans-Jürgen Stark
Author: Petra Boukamp
Author: Dirk Breitkreutz

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