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Macoilin,a conserved nervous system-specific ER membrane protein that regulates neuronal excitability
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نویسنده
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arellano-carbajal f. ,briseño-roa l. ,couto a. ,cheung b.h.h. ,labouesse m. ,de bono m.
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منبع
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plos genetics - 2011 - دوره : 7 - شماره : 3
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چکیده
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Genome sequence comparisons have highlighted many novel gene families that are conserved across animal phyla but whose biological function is unknown. here,we functionally characterize a member of one such family,the macoilins. macoilins are characterized by several highly conserved predicted transmembrane domains towards the n-terminus and by coiled-coil regions c-terminally. they are found throughout eumetazoa but not in other organisms. mutants for the single caenorhabditis elegans macoilin,maco-1,exhibit a constellation of behavioral phenotypes,including defects in aggregation,o2 responses,and swimming. maco-1 protein is expressed broadly and specifically in the nervous system and localizes to the rough endoplasmic reticulum; it is excluded from dendrites and axons. apart from subtle synapse defects,nervous system development appears wild-type in maco-1 mutants. however,maco-1 animals are resistant to the cholinesterase inhibitor aldicarb and sensitive to levamisole,suggesting pre-synaptic defects. using in vivo imaging,we show that macoilin is required to evoke ca2+ transients,at least in some neurons: in maco-1 mutants the o2-sensing neuron pqr is unable to generate a ca2+ response to a rise in o2. by genetically disrupting neurotransmission,we show that pre-synaptic input is not necessary for pqr to respond to o2,indicating that the response is mediated by cell-intrinsic sensory transduction and amplification. disrupting the sodium leak channels nca-1/nca-2,or the n-,p/q,r-type voltage-gated ca2+ channels,also fails to disrupt ca2+ responses in the pqr cell body to o2 stimuli. by contrast,mutations in egl-19,which encodes the only caenorhabditis elegans l-type voltage-gated ca2+ channel α1 subunit,recapitulate the ca2+ response defect we see in maco-1 mutants,although we do not see defects in localization of egl-19. together,our data suggest that macoilin acts in the er to regulate assembly or traffic of ion channels or ion channel regulators. © 2011 arellano-carbajal et al.
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آدرس
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medical research council-laboratory of molecular biology,cambridge,united kingdom,facultad de ciencias naturales,universidad autónoma de querétaro,juriquilla,querétaro, Mexico, medical research council-laboratory of molecular biology,cambridge,united kingdom,inserm u1024,école normale supérieure,paris, France, medical research council-laboratory of molecular biology,cambridge, United Kingdom, medical research council-laboratory of molecular biology,cambridge, United Kingdom, institute of genetics and molecular and cellular biology,illkirch, France, medical research council-laboratory of molecular biology,cambridge, United Kingdom
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Authors
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