A new mouse mutant with cleavage-resistant versican and isoform-specific versican mutants demonstrate that proteolysis at the Glu<sup>441</sup>-Ala<sup>442</sup> peptide bond in the V1 isoform is essential for interdigital web regression

Nandadasa, Sumeda; Burin des Roziers, Cyril; Koch, Christopher; Tran-Lundmark, Karin; Dours-Zimmermann, María T.; Zimmermann, Dieter R.; Valleix, Sophie; Apte, Suneel S.

A new mouse mutant with cleavage-resistant versican and isoform-specific versican mutants demonstrate that proteolysis at the Glu⁴⁴¹-Ala⁴⁴² peptide bond in the V1 isoform is essential for interdigital web regression

Mark

Nandadasa, Sumeda ; Burin des Roziers, Cyril ; Koch, Christopher ; Tran-Lundmark, Karin ^LU ; Dours-Zimmermann, María T. ; Zimmermann, Dieter R. ; Valleix, Sophie and Apte, Suneel S. (2021) In Matrix Biology Plus 10.

Abstract: Two inherent challenges in the mechanistic interpretation of protease-deficient phenotypes are defining the specific substrate cleavages whose reduction generates the phenotypes and determining whether the phenotypes result from loss of substrate function, substrate accumulation, or loss of a function(s) embodied in the substrate fragments. Hence, recapitulation of a protease-deficient phenotype by a cleavage-resistant substrate would stringently validate the importance of a proteolytic event and clarify the underlying mechanisms. Versican is a large proteoglycan required for development of the circulatory system and proper limb development, and is cleaved by ADAMTS proteases at the Glu⁴⁴¹-Ala⁴⁴² peptide bond... (More); Two inherent challenges in the mechanistic interpretation of protease-deficient phenotypes are defining the specific substrate cleavages whose reduction generates the phenotypes and determining whether the phenotypes result from loss of substrate function, substrate accumulation, or loss of a function(s) embodied in the substrate fragments. Hence, recapitulation of a protease-deficient phenotype by a cleavage-resistant substrate would stringently validate the importance of a proteolytic event and clarify the underlying mechanisms. Versican is a large proteoglycan required for development of the circulatory system and proper limb development, and is cleaved by ADAMTS proteases at the Glu⁴⁴¹-Ala⁴⁴² peptide bond located in its alternatively spliced GAGβ domain. Specific ADAMTS protease mutants have impaired interdigit web regression leading to soft tissue syndactyly that is associated with reduced versican proteolysis. Versikine, the N-terminal proteolytic fragment generated by this cleavage, restores interdigit apoptosis in ADAMTS mutant webs. Here, we report a new mouse transgene, Vcan^AA, with validated mutations in the GAGβ domain that specifically abolish this proteolytic event. Vcan^AA/AA mice have partially penetrant hindlimb soft tissue syndactyly. However, Adamts20 inactivation in Vcan^AA/AA mice leads to fully penetrant, more severe syndactyly affecting all limbs, suggesting that ADAMTS20 cleavage of versican at other sites or of other substrates is an additional requirement for web regression. Indeed, immunostaining with a neoepitope antibody against a cleavage site in the versican GAGα domain demonstrated reduced staining in the absence of ADAMTS20. Significantly, mice with deletion of Vcan exon 8, encoding the GAGβ domain, consistently developed soft tissue syndactyly, whereas mice unable to include exon 7, encoding the GAGα domain in Vcan transcripts, consistently had fully separated digits. These findings suggest that versican is cleaved within each GAG-bearing domain during web regression, and affirms that proteolysis in the GAGβ domain, via generation of versikine, has an essential role in interdigital web regression.
(Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/366a709f-dd35-4a41-b0ee-a659d32494b4

author

Nandadasa, Sumeda ; Burin des Roziers, Cyril ; Koch, Christopher ; Tran-Lundmark, Karin ^LU ; Dours-Zimmermann, María T. ; Zimmermann, Dieter R. ; Valleix, Sophie and Apte, Suneel S.

organization

publishing date

2021

type

Contribution to journal

publication status

published

subject

Biochemistry and Molecular Biology

keywords

ADAMTS, Extracellular matrix, Limb development, Metalloprotease, Proteoglycan, Syndactyly

in

Matrix Biology Plus

volume

10

article number

100064

publisher

Elsevier

external identifiers

scopus:85108084251
pmid:34195596

ISSN

2590-0285

DOI

10.1016/j.mbplus.2021.100064

language

English

LU publication?

yes

id

366a709f-dd35-4a41-b0ee-a659d32494b4

date added to LUP

2021-07-16 11:22:30

date last changed

2024-06-16 16:12:47

@article{366a709f-dd35-4a41-b0ee-a659d32494b4,
  abstract     = {{<p>Two inherent challenges in the mechanistic interpretation of protease-deficient phenotypes are defining the specific substrate cleavages whose reduction generates the phenotypes and determining whether the phenotypes result from loss of substrate function, substrate accumulation, or loss of a function(s) embodied in the substrate fragments. Hence, recapitulation of a protease-deficient phenotype by a cleavage-resistant substrate would stringently validate the importance of a proteolytic event and clarify the underlying mechanisms. Versican is a large proteoglycan required for development of the circulatory system and proper limb development, and is cleaved by ADAMTS proteases at the Glu<sup>441</sup>-Ala<sup>442</sup> peptide bond located in its alternatively spliced GAGβ domain. Specific ADAMTS protease mutants have impaired interdigit web regression leading to soft tissue syndactyly that is associated with reduced versican proteolysis. Versikine, the N-terminal proteolytic fragment generated by this cleavage, restores interdigit apoptosis in ADAMTS mutant webs. Here, we report a new mouse transgene, Vcan<sup>AA</sup>, with validated mutations in the GAGβ domain that specifically abolish this proteolytic event. Vcan<sup>AA/AA</sup> mice have partially penetrant hindlimb soft tissue syndactyly. However, Adamts20 inactivation in Vcan<sup>AA/AA</sup> mice leads to fully penetrant, more severe syndactyly affecting all limbs, suggesting that ADAMTS20 cleavage of versican at other sites or of other substrates is an additional requirement for web regression. Indeed, immunostaining with a neoepitope antibody against a cleavage site in the versican GAGα domain demonstrated reduced staining in the absence of ADAMTS20. Significantly, mice with deletion of Vcan exon 8, encoding the GAGβ domain, consistently developed soft tissue syndactyly, whereas mice unable to include exon 7, encoding the GAGα domain in Vcan transcripts, consistently had fully separated digits. These findings suggest that versican is cleaved within each GAG-bearing domain during web regression, and affirms that proteolysis in the GAGβ domain, via generation of versikine, has an essential role in interdigital web regression.</p>}},
  author       = {{Nandadasa, Sumeda and Burin des Roziers, Cyril and Koch, Christopher and Tran-Lundmark, Karin and Dours-Zimmermann, María T. and Zimmermann, Dieter R. and Valleix, Sophie and Apte, Suneel S.}},
  issn         = {{2590-0285}},
  keywords     = {{ADAMTS; Extracellular matrix; Limb development; Metalloprotease; Proteoglycan; Syndactyly}},
  language     = {{eng}},
  publisher    = {{Elsevier}},
  series       = {{Matrix Biology Plus}},
  title        = {{A new mouse mutant with cleavage-resistant versican and isoform-specific versican mutants demonstrate that proteolysis at the Glu<sup>441</sup>-Ala<sup>442</sup> peptide bond in the V1 isoform is essential for interdigital web regression}},
  url          = {{http://dx.doi.org/10.1016/j.mbplus.2021.100064}},
  doi          = {{10.1016/j.mbplus.2021.100064}},
  volume       = {{10}},
  year         = {{2021}},
}

Lund University Publications

LUND UNIVERSITY LIBRARIES

A new mouse mutant with cleavage-resistant versican and isoform-specific versican mutants demonstrate that proteolysis at the Glu⁴⁴¹-Ala⁴⁴² peptide bond in the V1 isoform is essential for interdigital web regression