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Bioenergetic status modulates motor neuron vulnerability and pathogenesis in a zebrafish model of spinal muscular atrophy
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نویسنده
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boyd p.j. ,tu w.-y. ,shorrock h.k. ,groen e.j.n. ,carter r.n. ,powis r.a. ,thomson s.r. ,thomson d. ,graham l.c. ,motyl a.a.l. ,wishart t.m. ,highley j.r. ,morton n.m. ,becker t. ,becker c.g. ,heath p.r. ,gillingwater t.h.
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منبع
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plos genetics - 2017 - دوره : 13 - شماره : 4
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چکیده
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Degeneration and loss of lower motor neurons is the major pathological hallmark of spinal muscular atrophy (sma),resulting from low levels of ubiquitously-expressed survival motor neuron (smn) protein. one remarkable,yet unresolved,feature of sma is that not all motor neurons are equally affected,with some populations displaying a robust resistance to the disease. here,we demonstrate that selective vulnerability of distinct motor neuron pools arises from fundamental modifications to their basal molecular profiles. comparative gene expression profiling of motor neurons innervating the extensor digitorum longus (disease-resistant),gastrocnemius (intermediate vulnerability),and tibialis anterior (vulnerable) muscles in mice revealed that disease susceptibility correlates strongly with a modified bioenergetic profile. targeting of identified bioenergetic pathways by enhancing mitochondrial biogenesis rescued motor axon defects in sma zebrafish. moreover,targeting of a single bioenergetic protein,phosphoglycerate kinase 1 (pgk1),was found to modulate motor neuron vulnerability in vivo. knockdown of pgk1 alone was sufficient to partially mimic the sma phenotype in wild-type zebrafish. conversely,pgk1 overexpression,or treatment with terazosin (an fda-approved small molecule that binds and activates pgk1),rescued motor axon phenotypes in sma zebrafish. we conclude that global bioenergetics pathways can be therapeutically manipulated to ameliorate sma motor neuron phenotypes in vivo. © 2017 boyd et al.
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آدرس
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euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, sheffield institute for translation neuroscience,university of sheffield,sheffield, United Kingdom, euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, university/british heart foundation centre for cardiovascular science,university of edinburgh,queens medical research institute,edinburgh, United Kingdom, euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, division of neurobiology,roslin institute,university of edinburgh,edinburgh, United Kingdom, centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, division of neurobiology,roslin institute,university of edinburgh,edinburgh, United Kingdom, sheffield institute for translation neuroscience,university of sheffield,sheffield, United Kingdom, university/british heart foundation centre for cardiovascular science,university of edinburgh,queens medical research institute,edinburgh, United Kingdom, euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for neuroregeneration,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for neuroregeneration,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom, sheffield institute for translation neuroscience,university of sheffield,sheffield, United Kingdom, euan macdonald centre for motor neurone disease research,university of edinburgh,edinburgh,united kingdom,centre for integrative physiology,edinburgh medical school: biomedical sciences,university of edinburgh,edinburgh, United Kingdom
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Authors
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