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演題詳細

Poster

軸索輸送、細胞骨格
Axonal Transport and Cytoskeleton

開催日 2014/9/13
時間 11:00 - 12:00
会場 Poster / Exhibition(Event Hall B)

FILIPとシャペロン分子によるシナプス形態調節
Filamin A-interacting protein is involved in the morphology of neuronal spines with one of chaperone proteins

  • P3-013
  • 八木 秀司 / Hideshi Yagi:1 佐藤 真 / Makoto Sato:2,3,4 野口 光一 / Koichi Naguchi:1 
  • 1:兵庫医大医解剖(神経) / Dept Anat & Neurosci, Hyogo Col of Med, Hyogo, Japan 2:大阪大院連合小児発達子どものこころ / United Grad Sch of Child Development, Osaka Univ, Kanazawa Univ, Hamamatsu Univ Sch of Med, Chiba Univ and Univ of Fukui, Osaka, Japan 3:福井大子どものこころの発達研究センター / Res Edu Program Life Sci, Univ of Fukui, Fukui, Japan 4:大阪大院医神経機能形態学 / Dept Anatomy and Neuroscience, Grad Sch Med, Osaka Univ, Osaka, Japan 

Filamin A-interacting protein (FILIP) is a filamin A binding protein and is involved in the radial migration of neurons via the acceleration of filamin A degradation. FILIP contributed to the characteristic morphology of the dendritic spine of neurons of the adult piriform cortex, where it is localized in the dendrites and spines. Several lines of evidence indicate that inhibition nonmuscle myosin IIb function in the neurons leads to the elongation of the spine. We found that FILIP bound to the head domain of nonmuscle myosin IIb, where the actin-binding domain is localized, and blocked its binding to actin fibers. Since FILIP has no apparent functional domains that cause alteration in the intracellular distribution of nonmuscle myosin IIb, we further tried to ascertain the region of FILIP responsible for the intracellular localization of nonmuscle myosin IIb. We observed that one of the chaperone proteins bound to C-terminal of FILIP was partially responsible for the alteration of intracellular localization of nonmuscle myosin IIb. Further investigation revealed that the inhibitor of this chaperone protein blocked the functioning of FILIP, thereby preventing the action of FILIP on neuronal spine morphology.

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