Neuromuscular endplate pathology in recessive desminopathies: Lessons from man and mice
Durmus H, Ayhan O, Cirak S, Deymeer F, Parman Y, Franke A, Eiber N, Chevessier F, Schlötzer-Schrehardt U, Clemen CS, Hashemolhosseini S, Schröder R, Hemmrich-Stanisak G, Tolun A, Serdaroglu-Oflazer P (2016)
Publication Type: Journal article
Publication year: 2016
Journal
Book Volume: 87
Pages Range: 799-805
Journal Issue: 8
DOI: 10.1212/WNL.0000000000003004
Abstract
To assess the clinical, genetic, and myopathologic findings in 2 cousins with lack of desmin, the response to salbutamol in one patient, and the neuromuscular endplate pathology in a knock-in mouse model for recessive desminopathy.We performed clinical investigations in the patients, genetic studies for linkage mapping, exome sequencing, and qPCR for transcript quantification, assessment of efficacy of (3-month oral) salbutamol administration by muscle strength assessment, 6-minute walking test (6MWT), and forced vital capacity, analysis of neuromuscular endplate pathology in a homozygous R349P desmin knock-in mouse by immunofluorescence staining of the hind limb muscles, and quantitative 3D morphometry and expression studies of acetylcholine receptor genes by quantitative PCR.Both patients had infantile-onset weakness and fatigability, facial weakness with bilateral ptosis and ophthalmoparesis, generalized muscle weakness, and a decremental response over 10% on repetitive nerve stimulation. Salbutamol improved 6MWT and subjective motor function in the treated patient. Genetic analysis revealed previously unreported novel homozygous truncating desmin mutation c.345dupC leading to protein truncation and consequent fast degradation of the mutant mRNA. In the recessive desminopathy mouse with low expression of the mutant desmin protein, we demonstrated fragmented motor endplates with increased surface areas, volumes, and fluorescence intensities in conjunction with increased ? and ? acetylcholine receptor subunit expression in oxidative soleus muscle.The patients were desmin-null and had myopathy, cardiomyopathy, and a congenital myasthenic syndrome. The data from man and mouse demonstrate that the complete lack as well as the markedly decreased expression of mutant R349P desmin impair the structural and functional integrity of neuromuscular endplates.
Authors with CRIS profile
Nane Eiber
Lehrstuhl für Biochemie und Pathobiochemie
Ursula Schlötzer-Schrehardt
Medizinische Fakultät
Said Hashemolhosseini
Lehrstuhl für Biochemie und Pathobiochemie
Rolf Schröder
Professur für Neuropathologie
Involved external institutions
Istanbul University / İstanbul Üniversitesi
Turkey (TR)
Bogazici University
Turkey (TR)
Christian-Albrechts-Universität zu Kiel
Germany (DE)
Universität zu Köln
Germany (DE)
Children’s National Health System
United States (USA) (US)
Turkey (TR)
Bogazici University
Turkey (TR)
Christian-Albrechts-Universität zu Kiel
Germany (DE)
Universität zu Köln
Germany (DE)
Children’s National Health System
United States (USA) (US)
How to cite
APA:
Durmus, H., Ayhan, O., Cirak, S., Deymeer, F., Parman, Y., Franke, A.,... Serdaroglu-Oflazer, P. (2016). Neuromuscular endplate pathology in recessive desminopathies: Lessons from man and mice. Neurology, 87(8), 799-805. https://doi.org/10.1212/WNL.0000000000003004
MLA:
Durmus, Hacer, et al. "Neuromuscular endplate pathology in recessive desminopathies: Lessons from man and mice." Neurology 87.8 (2016): 799-805.
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