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Reduced insulin signaling maintains electrical transmission in a neural circuit in aging flies
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نویسنده
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augustin h. ,mcgourty k. ,allen m.j. ,madem s.k. ,adcott j. ,kerr f. ,wong c.t. ,vincent a. ,godenschwege t. ,boucrot e. ,partridge l.
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منبع
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plos biology - 2017 - دوره : 15 - شماره : 9
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چکیده
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Lowered insulin/insulin-like growth factor (igf) signaling (iis) can extend healthy lifespan in worms,flies,and mice,but it can also have adverse effects (the “insulin paradox”). chronic,moderately lowered iis rescues age-related decline in neurotransmission through the drosophila giant fiber system (gfs),a simple escape response neuronal circuit,by increasing targeting of the gap junctional protein innexin shaking-b to gap junctions (gjs). endosomal recycling of gjs was also stimulated in cultured human cells when iis was reduced. furthermore,increasing the activity of the recycling small guanosine triphosphatases (gtpases) rab4 or rab11 was sufficient to maintain gjs upon elevated iis in cultured human cells and in flies,and to rescue age-related loss of gjs and of gfs function. lowered iis thus elevates endosomal recycling of gjs in neurons and other cell types,pointing to a cellular mechanism for therapeutic intervention into aging-related neuronal disorders. © 2017 augustin et al.
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آدرس
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max planck institute for biology of aging,köln,germany,institute of healthy aging,and genetics,evolution and environment,university college london,london, United Kingdom, department of structural and molecular biology,london, United Kingdom, school of biosciences,university of kent,canterbury,kent, United Kingdom, department of biological sciences,florida atlantic university,jupiter,fl, United States, max planck institute for biology of aging,köln,germany,institute of healthy aging,and genetics,evolution and environment,university college london,london, United Kingdom, max planck institute for biology of aging,köln,germany,institute of healthy aging,and genetics,evolution and environment,university college london,london, United Kingdom, max planck institute for biology of aging,köln, Germany, max planck institute for biology of aging,köln, Germany, department of biological sciences,florida atlantic university,jupiter,fl, United States, department of structural and molecular biology,london, United Kingdom, max planck institute for biology of aging,köln,germany,institute of healthy aging,and genetics,evolution and environment,university college london,london, United Kingdom
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Authors
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