Literature DB >> 9614116

Molecular features of the collagen V heparin binding site.

F Delacoux1, A Fichard, C Geourjon, R Garrone, F Ruggiero.   

Abstract

A heparin binding region is known to be present within the triple helical part of the alpha1(V) chain. Here we show that a recombinant alpha1(V) fragment (Ile824 to Pro950), referred to as HepV, is sufficient for heparin binding at physiological ionic strength. Both native individual alpha1(V) chains and HepV are eluted at identical NaCl concentrations (0.35 M) from a heparin-Sepharose column, and this binding can be inhibited specifically by the addition of free heparin or heparan sulfate. In contrast, a shorter 23-residue synthetic peptide, containing the putative heparin binding site in HepV, fails to bind heparin. Interestingly, HepV promotes cell attachment, and HepV-mediated adhesion is inhibited specifically by heparin or heparan sulfate, indicating that this region might behave as an adhesive binding site. The same site is equally functional on triple helical molecules as shown by heparin-gold labeling. However, the affinities for heparin of each of the collagen V molecular forms tested are different and increase with the number of alpha1(V) chains incorporated in the molecules. Molecular modeling of a sequence encompassing the putative HepV binding sequence region shows that all of the basic residues cluster on one side of the helical face. A highly positively charged ring around the molecule is thus particularly evident for the alpha1(V) homotrimer. This could strengthen its interaction with the anionic heparin molecules. We propose that a single heparin binding site is involved in heparin-related glycosaminoglycans-collagen V interactions, but the different affinities observed likely modulate cell and matrix interactions between collagen V and heparan sulfate proteoglycans in tissues.

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Year:  1998        PMID: 9614116

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  13 in total

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3.  Regulation of Collagen V Expression and Epithelial-Mesenchymal Transition by miR-185 and miR-186 during Idiopathic Pulmonary Fibrosis.

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Journal:  Am J Pathol       Date:  2016-07-05       Impact factor: 4.307

4.  COL5A1 haploinsufficiency is a common molecular mechanism underlying the classical form of EDS.

Authors:  R J Wenstrup; J B Florer; M C Willing; C Giunta; B Steinmann; F Young; M Susic; W G Cole
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5.  Enzymatic cleavage specificity of the proalpha1(V) chain processing analysed by site-directed mutagenesis.

Authors:  Christelle Bonod-Bidaud; Mickaël Beraud; Elisabeth Vaganay; Frédéric Delacoux; Bernard Font; David J S Hulmes; Florence Ruggiero
Journal:  Biochem J       Date:  2007-07-15       Impact factor: 3.857

6.  Comprehensive mass spectrometric mapping of the hydroxylated amino acid residues of the α1(V) collagen chain.

Authors:  Chenxi Yang; Arick C Park; Nicholas A Davis; Jason D Russell; Byoungjae Kim; David D Brand; Matthew J Lawrence; Ying Ge; Michael S Westphall; Joshua J Coon; Daniel S Greenspan
Journal:  J Biol Chem       Date:  2012-10-11       Impact factor: 5.157

Review 7.  Heparin-binding domains in vascular biology.

Authors:  Eva M Muñoz; Robert J Linhardt
Journal:  Arterioscler Thromb Vasc Biol       Date:  2004-07-01       Impact factor: 8.311

8.  Characterization of the six zebrafish clade B fibrillar procollagen genes, with evidence for evolutionarily conserved alternative splicing within the pro-alpha1(V) C-propeptide.

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Journal:  Matrix Biol       Date:  2010-01-25       Impact factor: 11.583

9.  Fell-Muir Lecture: Heparan sulphate and the art of cell regulation: a polymer chain conducts the protein orchestra.

Authors:  John Gallagher
Journal:  Int J Exp Pathol       Date:  2015-07-15       Impact factor: 1.925

10.  Type V collagen induced tolerance suppresses collagen deposition, TGF-β and associated transcripts in pulmonary fibrosis.

Authors:  Ragini Vittal; Elizabeth A Mickler; Amanda J Fisher; Chen Zhang; Katia Rothhaar; Hongmei Gu; Krista M Brown; Amir Emtiazjoo; Jeremy M Lott; Sarah B Frye; Gerald N Smith; George E Sandusky; Oscar W Cummings; David S Wilkes
Journal:  PLoS One       Date:  2013-10-21       Impact factor: 3.240

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