Structural effects of fibulin 5 missense mutations associated with age-related macular degeneration and cutis laxa

Richard P O Jones, Caroline Ridley, Thomas A. Jowitt, Ming Chuan Wang, Marjorie Howard, Nicoletta Bobola, Tao Wang, Paul N. Bishop, Cay M. Kielty, Clair Baldock, Andrew J. Lotery, Dorothy Trump

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Purpose. AMD has a complex etiology with environmental and genetic risk factors. Ten fibulin 5 sequence variants have been associated with AMD and two other fibulin 5 mutations cause autosomal-recessive cutis laxa. Fibulin 5 is a 52-kDa calciumbinding epidermal growth factor (cbEGF)-rich extracellular matrix protein that is essential for the formation of elastic tissues. Biophysical techniques were used to detect structural changes in the fibulin 5 mutants and to determine whether changes are predictive of pathogenicity. Methods. Native PAGE, nonreduced SDS-PAGE, size-exclusion column multiangle laser light scattering, sedimentation velocity, and circular dichroism (CD) were used to investigate the mobility, hydrodynamic radii, folding, and oligomeric states of the fibulin 5 mutants in the absence and presence of Ca2+. Results. CD showed that all mutants are folded, although perturbations to secondary structure contents were detected. Both cutis laxa mutants increased dimerization. Most other mutants slightly increased self-association in the absence of Ca2+ but this was also demonstrated by G202R, a polymorphism detected in a control individual. The AMD-associated mutant G412E showed lower-than-expected mobility during native-PAGE, the largest hydrodynamic radius for the monomer form and the highest levels of aggregation in both the absence and presence of Ca2+. Conclusions. The results identified structural differences for the disease-causing cutis laxa mutants and for one AMD variant (G412E), suggesting that this may also be pathogenic. Although the other AMD-associated mutants showed no gross structural differences, they cannot be excluded as pathogenic by differences outside the scope of this study-for example, disruption of heterointeractions. © Association for Research in Vision and Ophthalmology.
    Original languageEnglish
    Pages (from-to)2356-2362
    Number of pages6
    JournalInvestigative Ophthalmology and Visual Science
    Volume51
    Issue number5
    DOIs
    Publication statusPublished - May 2010

    Keywords

    • Calcium/pharmacology
    • Chromatography, Gel
    • Circular Dichroism
    • Cutis Laxa/*genetics
    • Electrophoresis, Polyacrylamide Gel
    • Extracellular Matrix Proteins/*chemistry/*genetics
    • Humans
    • Macular Degeneration/*genetics
    • Molecular Structure
    • Mutagenesis, Site-Directed
    • *Mutation, Missense
    • Protein Folding

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