Di Paolo Gilbert, Sankaranarayanan Sethuraman, Wenk Markus R, Daniell Laurie, Perucco Ezio, Caldarone Barbara J, Flavell Richard, Picciotto Marina R, Ryan Timothy A, Cremona Ottavio, De Camilli Pietro
Howard Hughes Medical Institute, Yale University School of Medicine, New Haven, CT 06510, USA.
Neuron. 2002 Feb 28;33(5):789-804. doi: 10.1016/s0896-6273(02)00601-3.
The function of the clathrin coat in synaptic vesicle endocytosis is assisted by a variety of accessory factors, among which amphiphysin (amphiphysin 1 and 2) is one of the best characterized. A putative endocytic function of amphiphysin was supported by dominant-negative interference studies. We have now generated amphiphysin 1 knockout mice and found that lack of amphiphysin 1 causes a parallel dramatic reduction of amphiphysin 2 selectively in brain. Cell-free assembly of endocytic protein scaffolds is defective in mutant brain extracts. Knockout mice exhibit defects in synaptic vesicle recycling that are unmasked by stimulation and suggest impairments at multiple stages of the cycle. These defects correlate with increased mortality due to rare irreversible seizures and with major learning deficits, suggesting a critical role of amphiphysin for higher brain functions.
网格蛋白包被在突触小泡内吞作用中的功能得到多种辅助因子的协助,其中发动蛋白(发动蛋白1和2)是特征最为明确的因子之一。发动蛋白的假定内吞功能得到了显性负性干扰研究的支持。我们现已培育出发动蛋白1基因敲除小鼠,并发现缺乏发动蛋白1会导致大脑中发动蛋白2选择性地平行显著减少。突变型脑提取物中内吞蛋白支架的无细胞组装存在缺陷。基因敲除小鼠在突触小泡循环中表现出缺陷,这些缺陷在受到刺激时会显现出来,提示在循环的多个阶段存在损伤。这些缺陷与罕见的不可逆性癫痫导致的死亡率增加以及严重的学习缺陷相关,表明发动蛋白对高等脑功能具有关键作用。