Protein studies in dysferlinopathy patients using llama-derived antibody fragments selected by phage display

被引:0
作者
Yanchao Huang
Peter Verheesen
Andreas Roussis
Wendy Frankhuizen
Ieke Ginjaar
Faye Haldane
Steve Laval
Louise V B Anderson
Theo Verrips
Rune R Frants
Hans de Haard
Kate Bushby
Johan den Dunnen
Silvère M van der Maarel
机构
[1] Center for Human and Clinical Genetics,Leiden University Medical Center
[2] University of Utrecht,Department of Molecular and Cellular Biology
[3] Institute of Human Genetics,undefined
[4] International Centre for Life,undefined
来源
European Journal of Human Genetics | 2005年 / 13卷
关键词
dysferlin; HCAb; phage display; immunohistochemistry; immunoprecipitation;
D O I
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学科分类号
摘要
Mutations in dysferlin, a member of the fer1-like protein family that plays a role in membrane integrity and repair, can give rise to a spectrum of neuromuscular disorders with phenotypic variability including limb-girdle muscular dystrophy 2B, Myoshi myopathy and distal anterior compartment myopathy. To improve the tools available for understanding the pathogenesis of the dysferlinopathies, we have established a large source of highly specific antibody reagents against dysferlin by selection of heavy-chain antibody fragments originating from a nonimmune llama-derived phage-display library. By utilizing different truncated forms of recombinant dysferlin for selection and diverse selection methodologies, antibody fragments with specificity for two different dysferlin domains could be identified. The selected llama antibody fragments are functional in Western blotting, immunofluorescence microscopy and immunoprecipitation applications. Using these antibody fragments, we found that calpain 3, which shows a secondary reduction in the dysferlinopathies, interacts with dysferlin.
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页码:721 / 730
页数:9
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