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通过特定细胞操作揭示的驱动蛋白介导的细胞器转运

Kinesin-mediated organelle translocation revealed by specific cellular manipulations.

作者信息

Feiguin F, Ferreira A, Kosik K S, Caceres A

机构信息

Instituto Mercedes y Martin Fereyra, Cordoba, Argentina.

出版信息

J Cell Biol. 1994 Nov;127(4):1021-39. doi: 10.1083/jcb.127.4.1021.

Abstract

The distribution of membrane-bound organelles was studied in cultured hippocampal neurons after antisense oligonucleotide suppression of the kinesin-heavy chain (KHC). We observed reduced 3,3'-dihexyloxacarbocyanine iodide (DiOC6(3)) fluorescent staining in neurites and growth cones. In astrocytes, KHC suppression results in the disappearance of the DiOC6(3)-positive reticular network from the cell periphery, and a parallel accumulation of label within the cell center. On the other hand, mitochondria microtubules and microfilaments display a distribution that closely resembles that observed in control cells. KHC suppression of neurons and astrocytes completely inhibited the Brefeldin A-induced spreading and tubulation of the Golgi-associated structure enriched in mannose-6-phosphate receptors. In addition, KHC suppression prevents the low pH-induced anterograde redistribution of late endocytic structures. Taken collectively, these observations suggest that in living neurons, kinesin mediates the anterograde transport of tubulovesicular structures originated in the central vacuolar system (e.g., the endoplasmic reticulum) and that the regulation of kinesin-membrane interactions may be of key importance for determining the intracellular distribution of selected organelles.

摘要

在通过反义寡核苷酸抑制驱动蛋白重链(KHC)后,研究了培养的海马神经元中膜结合细胞器的分布。我们观察到神经突和生长锥中3,3'-二己基氧羰花青碘化物(DiOC6(3))荧光染色减少。在星形胶质细胞中,KHC抑制导致细胞周边DiOC6(3)阳性网状网络消失,且标记物在细胞中心平行积累。另一方面,线粒体、微管和微丝的分布与对照细胞中观察到的分布非常相似。对神经元和星形胶质细胞的KHC抑制完全抑制了布雷菲德菌素A诱导的富含甘露糖-6-磷酸受体的高尔基体相关结构的扩散和管状化。此外,KHC抑制可防止低pH诱导的晚期内吞结构的顺向重新分布。总体而言,这些观察结果表明,在活神经元中,驱动蛋白介导源自中央液泡系统(如内质网)的微管泡状结构的顺向运输,并且驱动蛋白与膜相互作用的调节对于确定特定细胞器的细胞内分布可能至关重要。

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本文引用的文献

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The kinesin superfamily: tails of functional redundancy.驱动蛋白超家族:功能冗余的尾部
Trends Cell Biol. 1991 Oct;1(4):93-8. doi: 10.1016/0962-8924(91)90036-9.
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J Neurosci. 1993 Jul;13(7):3112-23. doi: 10.1523/JNEUROSCI.13-07-03112.1993.
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J Neurosci. 1988 Apr;8(4):1454-68. doi: 10.1523/JNEUROSCI.08-04-01454.1988.

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