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The Distributions of Tau Short and Long Isoforms Fused with EGFP in Cultured Cells

机译:EGFP融合的Tau短和长同工型在培养细胞中的分布

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摘要

Frontotemporal dementia and parkinsonism linked to chromosome 1.7 (FTDP-17) are caused by mutations of the TAU gene. Many such mutations are located near the splicing site of exon 10 and affect the splicing ratio of 3-repeat/4-repeat tau isoforms (referred to as 3R-tau and 4R-tau) which contain 3 and 4 microtubule-binding domains, respectively. Little is known, however, concerning cellular localization of 3R-tau and 4R-tau. We examined the subcellular localization of tau isoforms in IMR-32 cells under differentiated conditions using the fusion proteins of tau isoforms probed with fluorescent protein (EGFP). 3R-tau was observed in spotty and rarely linear distributions while 4R-tau was observed in linear and sometimes spotty distributions. Together with findings of phase-contrast microscopy of cultured cells, these results indicated that 3R- and 4R-tau were predominantly localized at growth tips/branching points and along neurite processes, respectively. Due to their different localizations, balanced expression of 3R-and 4R-tau may coordinate plastic morphogenesis and stabilization of neurite processes.
机译:TAU基因突变引起与1.7号染色体(FTDP-17)相关的额颞叶痴呆和帕金森症。许多此类突变位于外显子10的剪接位点附近,并影响3重复/ 4重复tau亚型(分别称为3R-tau和4R-tau)的剪接比例,它们分别包含3和4个微管结合域。 。然而,关于3R-tau和4R-tau的细胞定位知之甚少。我们使用荧光蛋白(EGFP)探测的tau亚型融合蛋白,在分化条件下检查了IMR-32细胞中tau亚型的亚细胞定位。 3R-tau呈斑点状,很少呈线性分布,而4R-tau呈线性状,有时呈斑点状分布。连同培养细胞的相差显微镜的发现,这些结果表明3R-tau和4R-tau主要分别位于生长尖端/分支点和神经突过程。由于它们的不同定位,3R-和4R-tau的平衡表达可能协调塑性形态发生和神经突过程的稳定。

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