Literature DB >> 11472837

The human chordin gene encodes several differentially expressed spliced variants with distinct BMP opposing activities.

C Millet1, P Lemaire, B Orsetti, P Guglielmi, V François.   

Abstract

During early embryogenesis of both vertebrates and invertebrates, antagonism between bone morphogenetic proteins (BMPs) and several unrelated secreted factors including Chordin (Chd) is a general mechanism by which the dorso-ventral axis is established. High affinity binding of Chd sequesters the BMP ligands in the extracellular space, preventing interactions with their membrane receptors. Another level of regulation consists in processing of vertebrate Chd or its Drosophila counterpart Sog by astacine metalloproteases like Xolloid-BMP-1/Tolloid, respectively, which releases an active BMP. Recently, it was shown that cleavage of Sog by Tolloid could generate novel BMP inhibitory activity and that sog is also capable of stimulation of BMP activity in a tolloid-dependant way. Activity and/or cleavage of Chd/Sog are influenced by other secreted factors like twisted gastrulation. In this study, we have cloned cDNAs of the human chordin gene (CHRD) and characterized alternative splice variants that code for C-truncated forms of the protein. We have found that CHRD is expressed in fetal as well as in adult tissues with relatively high levels in liver, cerebellum and female genital tract, suggesting functions in late embryogenesis and adult physiology. We also show that spliced variants are present with specific patterns in various tissues. When tested in an axis-duplication assay in Xenopus, we find that these variants can antagonize BMP activity. Altogether, these results suggest that, in addition to processing by metalloproteases, alternative splicing (AS) is another mechanism by which sub-products of CHRD can be generated to influence BMP activity in different developmental and physiological situations.

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Year:  2001        PMID: 11472837     DOI: 10.1016/s0925-4773(01)00423-3

Source DB:  PubMed          Journal:  Mech Dev        ISSN: 0925-4773            Impact factor:   1.882


  8 in total

1.  Nanoscale structure of the BMP antagonist chordin supports cooperative BMP binding.

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2.  Differential regulation of the bone morphogenic protein antagonist chordin in human normal and osteoarthritic chondrocytes.

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4.  Cysteine repeat domains and adjacent sequences determine distinct bone morphogenetic protein modulatory activities of the Drosophila Sog protein.

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Review 6.  The role of chordin fragments generated by partial tolloid cleavage in regulating BMP activity.

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Authors:  Yasser M Sanad; Kwonil Jung; Isaac Kashoma; Xiaoli Zhang; Issmat I Kassem; Yehia M Saif; Gireesh Rajashekara
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8.  Structural characterization of twisted gastrulation provides insights into opposing functions on the BMP signalling pathway.

Authors:  Helen Troilo; Anne L Barrett; Alexandra V Zuk; Michael P Lockhart-Cairns; Alexander P Wohl; Christopher P Bayley; Rana Dajani; Richard B Tunnicliffe; Lewis Green; Thomas A Jowitt; Gerhard Sengle; Clair Baldock
Journal:  Matrix Biol       Date:  2016-01-29       Impact factor: 11.583

  8 in total

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