Regulation of procollagen amino-propeptide processing during mouse embryogenesis by specialization of homologous ADAMTS proteases: insights on collagen biosynthesis and dermatosparaxis

Le Goff, Carine; Somerville, Robert PT; Kesteloot, Frédéric; Powell, Kimerly; Birk, David E; Colige, Alain; Apte, Suneel S

doi:10.1242/dev.02308

Article (Scientific journals)

Regulation of procollagen amino-propeptide processing during mouse embryogenesis by specialization of homologous ADAMTS proteases: insights on collagen biosynthesis and dermatosparaxis

Le Goff, Carine; Somerville, Robert PT; Kesteloot, Frédéric et al.

2006 • In Development, 133 (8), p. 1587-1596

Peer Reviewed verified by ORBi

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https://hdl.handle.net/2268/1429

DOI
10.1242/dev.02308

PubMed
16556917

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Keywords :

ADAMTS; metalloprotease; procollagen; dermatosparaxis; Ehlers-Danlos syndrome

Abstract :

[en] Mutations in ADAMTS2, a procollagen amino-propeptidase, cause severe skin fragility, designated as dermatosparaxis in animals, and a subtype of the Ehlers-Danlos syndrome (dermatosparactic type or VIIC) in humans. Not all collagen-rich tissues are affected to the same degree, which suggests compensation by the ADAMTS2 homologs ADAMTS3 and ADAMTS14. In situ hybridization of Adamts2, Adamts3 and Adamts14, and of the genes encoding the major. brillar collagens, Col1a1, Col2a1 and Col3a1, during mouse embryogenesis, demonstrated distinct tissue-specific, overlapping expression patterns of the protease and substrate genes. Adamts3, but not Adamts2 or Adamts14, was co-expressed with Col2a1 in cartilage throughout development, and with Col1a1 in bone and musculotendinous tissues. ADAMTS3 induced procollagen I processing in dermatosparactic. broblasts, suggesting a role in procollagen I processing during musculoskeletal development. Adamts2, but not Adamts3 or Adamts14, was co-expressed with Col3a1 in many tissues including the lungs and aorta, and Adamts2(-/-) mice showed widespread defects in procollagen III processing. Adamts2(-/-) mice had abnormal lungs, characterized by a decreased parenchymal density. However, the aorta and collagen fibrils in the aortic wall appeared normal. Although Adamts14 lacked developmental tissue-specific expression, it was co-expressed with Adamts2 in mature dermis, which possibly explains the presence of some processed skin procollagen in dermatosparaxis. The data show how evolutionarily related proteases with similar substrate preferences may have distinct biological roles owing to tissue specific gene expression, and provide insights into collagen biosynthesis and the pathobiology of dermatosparaxis.

Disciplines :

Dermatology
Biochemistry, biophysics & molecular biology
Anatomy (cytology, histology, embryology...) & physiology

Author, co-author :

Le Goff, Carine; Lerner Research Institute, Cleveland Clinic Foundation - Cleveland, OH > Department of Biomedical Engineering and Orthopaedic Research Center

Somerville, Robert PT; Lerner Research Institute, Cleveland Clinic Foundation - Cleveland, OH > Department of Biomedical Engineering and Orthopaedic Research Center

Kesteloot, Frédéric ; Université de Liège - ULiège > Département des sciences biomédicales et précliniques > Protéines et glycoprot. de matr.extracell. et membran.basal.

Powell, Kimerly; Lerner Research Institute, Cleveland Clinic Foundation - Cleveland, OH > Department of Biomedical Engineering and Orthopaedic Research Center

Birk, David E; Thomas Jefferson University - Philadelphia, PA > Department of Cell Biology

Colige, Alain ; Université de Liège - ULiège > Département des sciences biomédicales et précliniques > Protéines et glycoprot. de matr.extracell. et membran.basal.

Apte, Suneel S; Lerner Research Institute, Cleveland Clinic Foundation - Cleveland, OH > Department of Biomedical Engineering and Orthopaedic Research Center

Language :

English

Title :

Regulation of procollagen amino-propeptide processing during mouse embryogenesis by specialization of homologous ADAMTS proteases: insights on collagen biosynthesis and dermatosparaxis

Publication date :

15 April 2006

Journal title :

Development

ISSN :

0950-1991

eISSN :

1477-9129

Publisher :

Company Of Biologists Ltd, Cambridge, United Kingdom

Volume :

133

Issue :

Pages :

1587-1596

Peer reviewed :

Peer Reviewed verified by ORBi

Available on ORBi :

since 27 November 2008

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