A new web-based method for automated analysis of muscle histology

Duchenne muscular dystrophy is an inherited degenerative neuromuscular disease characterised by rapidly progressive muscle weakness. Currently, curative treatment is not available. Approaches for new treatments that improve muscle strength and quality of life depend on preclinical testing in animal...

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Bibliographic Details
Published in:BMC musculoskeletal disorders 2013-01, Vol.14 (1), p.26-26, Article 26
Main Authors: Pertl, Cordula, Eblenkamp, Markus, Pertl, Anja, Pfeifer, Stefan, Wintermantel, Erich, Lochmüller, Hanns, Walter, Maggie C, Krause, Sabine, Thirion, Christian
Format: Article
Language:English
Subjects:
Analysis
Animals
Automation
Automation, Laboratory
Biomarkers - analysis
Bisbenzimidazole
Cell Size
Disease Models, Animal
Duchenne muscular dystrophy
Dystrophin
Fluorescence
Fluorescent Dyes
Genes
Genetic aspects
Histological muscle fibre analysis
Histology
Image Processing, Computer-Assisted - standards
Immunohistochemistry - methods
Immunohistochemistry - standards
Internet
Laboratories
Male
mdx mouse
Mechanization
Medical research
Medicine, Experimental
Methods
Mice
Mice, Inbred mdx
Microscopy, Fluorescence - standards
Minimal Feret’s diameter
Muscle Fibers, Skeletal - chemistry
Muscle Fibers, Skeletal - pathology
Muscles
Muscular dystrophy
Muscular Dystrophy, Duchenne - metabolism
Muscular Dystrophy, Duchenne - pathology
Muscular system
Musculoskeletal diseases
Myosin
Myosin Heavy Chains - analysis
Proteins
Rodents
Standardised and automated quantitative analysis
Technical Advance
Technology application
Utrophin
Wheat Germ Agglutinins
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Summary:Duchenne muscular dystrophy is an inherited degenerative neuromuscular disease characterised by rapidly progressive muscle weakness. Currently, curative treatment is not available. Approaches for new treatments that improve muscle strength and quality of life depend on preclinical testing in animal models. The mdx mouse model is the most frequently used animal model for preclinical studies in muscular dystrophy research. Standardised pathology-relevant parameters of dystrophic muscle in mdx mice for histological analysis have been developed in international, collaborative efforts, but automation has not been accessible to most research groups. A standardised and mainly automated quantitative assessment of histopathological parameters in the mdx mouse model is desirable to allow an objective comparison between laboratories. Immunological and histochemical reactions were used to obtain a double staining for fast and slow myosin. Additionally, fluorescence staining of the myofibre membranes allows defining the minimal Feret's diameter. The staining of myonuclei with the fluorescence dye bisbenzimide H was utilised to identify nuclei located internally within myofibres. Relevant structures were extracted from the image as single objects and assigned to different object classes using web-based image analysis (MyoScan). Quantitative and morphometric data were analysed, e.g. the number of nuclei per fibre and minimal Feret's diameter in 6 month old wild-type C57BL/10 mice and mdx mice. In the current version of the module "MyoScan", essential parameters for histologic analysis of muscle sections were implemented including the minimal Feret's diameter of the myofibres and the automated calculation of the percentage of internally nucleated myofibres. Morphometric data obtained in the present study were in good agreement with previously reported data in the literature and with data obtained from manual analysis. A standardised and mainly automated quantitative assessment of histopathological parameters in the mdx mouse model is now available. Automated analysis of histological parameters is more rapid and less time-consuming. Moreover, results are unbiased and more reliable. Efficacy of therapeutic interventions, e.g. within the scope of a drug screening or therapeutic exon skipping, can be monitored. The automatic analysis system MyoScan used in this study is not limited exclusively to dystrophin-deficient mice but also represents a useful tool for applications in
ISSN:1471-2474
1471-2474
DOI:10.1186/1471-2474-14-26