Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains

Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains

Dystroglycan (DG) is an adhesion complex that links the cytoskeleton to the surrounding extracellular matrix in skeletal muscle and a wide variety of other tissues. It is composed of a highly glycosylated extracellular α-DG associated noncovalently with a transmembrane β-DG whose cytodomain interact...

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Main Authors: Christopher E. Dempsey, Maria Giulia Bigotti, Josephine C. Adams, Andrea Brancaccio
Format: Article
Language:English
Published: Frontiers Media S.A. 2019-03-01
Series:Frontiers in Molecular Biosciences
Subjects:
dystroglycan
laminin globular (LG) domains
binding affinities
protein modeling
protein structure
Online Access:https://www.frontiersin.org/article/10.3389/fmolb.2019.00018/full
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spelling doaj-455bf3ebd64b4ed8b4b85aa4c683574c2020-11-24T22:10:51ZengFrontiers Media S.A.Frontiers in Molecular Biosciences2296-889X2019-03-01610.3389/fmolb.2019.00018437989Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG DomainsChristopher E. Dempsey0Maria Giulia Bigotti1Josephine C. Adams2Andrea Brancaccio3Andrea Brancaccio4School of Biochemistry, University of Bristol, Bristol, United KingdomSchool of Biochemistry, University of Bristol, Bristol, United KingdomSchool of Biochemistry, University of Bristol, Bristol, United KingdomSchool of Biochemistry, University of Bristol, Bristol, United KingdomIstituto di Chimica del Riconoscimento Molecolare - CNR, Università Cattolica del Sacro Cuore, Rome, ItalyDystroglycan (DG) is an adhesion complex that links the cytoskeleton to the surrounding extracellular matrix in skeletal muscle and a wide variety of other tissues. It is composed of a highly glycosylated extracellular α-DG associated noncovalently with a transmembrane β-DG whose cytodomain interacts with dystrophin and its isoforms. Alpha-dystroglycan (α-DG) binds tightly and in a calcium-dependent fashion to multiple extracellular proteins and proteoglycans, each of which harbors at least one, or, more frequently, tandem arrays of laminin-globular (LG) domains. Considerable biochemical and structural work has accumulated on the α-DG-binding LG domains, highlighting a significant heterogeneity in ligand-binding properties of domains from different proteins as well as between single and multiple LG domains within the same protein. Here we review biochemical, structural, and functional information on the LG domains reported to bind α-dystroglycan. In addition, we have incorporated bioinformatics and modeling to explore whether specific motifs responsible for α-dystroglycan recognition can be identified within isolated LG domains. In particular, we analyzed the LG domains of slits and agrin as well as those of paradigmatic α-DG non-binders such as laminin-α3. While some stretches of basic residues may be important, no universally conserved motifs could be identified. However, the data confirm that the coordinated calcium atom within the LG domain is needed to establish an interaction with the sugars of α-DG, although it appears that this alone is insufficient to mediate significant α-DG binding. We develop a scenario involving different binding modes of a single LG domain unit, or tandemly repeated units, with α-DG. A variability of binding modes might be important to generate a range of affinities to allow physiological regulation of this interaction, reflecting its crucial biological importance.https://www.frontiersin.org/article/10.3389/fmolb.2019.00018/fulldystroglycanlaminin globular (LG) domainsbinding affinitiesprotein modelingprotein structure
collection DOAJ
language English
format Article
sources DOAJ
author Christopher E. Dempsey
Maria Giulia Bigotti
Josephine C. Adams
Andrea Brancaccio
Andrea Brancaccio
spellingShingle Christopher E. Dempsey
Maria Giulia Bigotti
Josephine C. Adams
Andrea Brancaccio
Andrea Brancaccio
Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains
Frontiers in Molecular Biosciences
dystroglycan
laminin globular (LG) domains
binding affinities
protein modeling
protein structure
author_facet Christopher E. Dempsey
Maria Giulia Bigotti
Josephine C. Adams
Andrea Brancaccio
Andrea Brancaccio
author_sort Christopher E. Dempsey
title Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains
title_short Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains
title_full Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains
title_fullStr Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains
title_full_unstemmed Analysis of α-Dystroglycan/LG Domain Binding Modes: Investigating Protein Motifs That Regulate the Affinity of Isolated LG Domains
title_sort analysis of α-dystroglycan/lg domain binding modes: investigating protein motifs that regulate the affinity of isolated lg domains
publisher Frontiers Media S.A.
series Frontiers in Molecular Biosciences
issn 2296-889X
publishDate 2019-03-01
description Dystroglycan (DG) is an adhesion complex that links the cytoskeleton to the surrounding extracellular matrix in skeletal muscle and a wide variety of other tissues. It is composed of a highly glycosylated extracellular α-DG associated noncovalently with a transmembrane β-DG whose cytodomain interacts with dystrophin and its isoforms. Alpha-dystroglycan (α-DG) binds tightly and in a calcium-dependent fashion to multiple extracellular proteins and proteoglycans, each of which harbors at least one, or, more frequently, tandem arrays of laminin-globular (LG) domains. Considerable biochemical and structural work has accumulated on the α-DG-binding LG domains, highlighting a significant heterogeneity in ligand-binding properties of domains from different proteins as well as between single and multiple LG domains within the same protein. Here we review biochemical, structural, and functional information on the LG domains reported to bind α-dystroglycan. In addition, we have incorporated bioinformatics and modeling to explore whether specific motifs responsible for α-dystroglycan recognition can be identified within isolated LG domains. In particular, we analyzed the LG domains of slits and agrin as well as those of paradigmatic α-DG non-binders such as laminin-α3. While some stretches of basic residues may be important, no universally conserved motifs could be identified. However, the data confirm that the coordinated calcium atom within the LG domain is needed to establish an interaction with the sugars of α-DG, although it appears that this alone is insufficient to mediate significant α-DG binding. We develop a scenario involving different binding modes of a single LG domain unit, or tandemly repeated units, with α-DG. A variability of binding modes might be important to generate a range of affinities to allow physiological regulation of this interaction, reflecting its crucial biological importance.
topic dystroglycan
laminin globular (LG) domains
binding affinities
protein modeling
protein structure
url https://www.frontiersin.org/article/10.3389/fmolb.2019.00018/full
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AT josephinecadams analysisofadystroglycanlgdomainbindingmodesinvestigatingproteinmotifsthatregulatetheaffinityofisolatedlgdomains
AT andreabrancaccio analysisofadystroglycanlgdomainbindingmodesinvestigatingproteinmotifsthatregulatetheaffinityofisolatedlgdomains
AT andreabrancaccio analysisofadystroglycanlgdomainbindingmodesinvestigatingproteinmotifsthatregulatetheaffinityofisolatedlgdomains
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