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   Survival motor neuron protein regulates stem cell division,proliferation,and differentiation in drosophila  
   
نویسنده grice s.j. ,liu j.-l.
منبع plos genetics - 2011 - دوره : 7 - شماره : 4
چکیده    Spinal muscular atrophy is a severe neurogenic disease that is caused by mutations in the human survival motor neuron 1 (smn1) gene. smn protein is required for the assembly of small nuclear ribonucleoproteins and a dramatic reduction of the protein leads to cell death. it is currently unknown how the reduction of this ubiquitously essential protein can lead to tissue-specific abnormalities. in addition,it is still not known whether the disease is caused by developmental or degenerative defects. using the drosophila system,we show that smn is enriched in postembryonic neuroblasts and forms a concentration gradient in the differentiating progeny. in addition to the developing drosophila larval cns,drosophila larval and adult testes have a striking smn gradient. when smn is reduced in postembryonic neuroblasts using marcm clonal analysis,cell proliferation and clone formation defects occur. these smn mutant neuroblasts fail to correctly localise miranda and have reduced levels of snrnas. when smn is removed,germline stem cells are lost more frequently. we also show that changes in smn levels can disrupt the correct timing of cell differentiation. we conclude that highly regulated smn levels are essential to drive timely cell proliferation and cell differentiation. © 2011 grice,liu.
آدرس medical research council functional genomics unit,department of physiology,anatomy,and genetics,university of oxford,oxford, United Kingdom, medical research council functional genomics unit,department of physiology,anatomy,and genetics,university of oxford,oxford, United Kingdom
 
     
   
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