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Protein aggregates stimulate macropinocytosis facilitating their propagation

机译:蛋白质聚集体刺激巨胞饮作用,促进其繁殖

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Temporal and spatial patterns of pathological changes such as loss of neurons and presence of pathological protein aggregates are characteristic of neurodegenerative diseases such as Amyotrophic Lateral Sclerosis, Frontotemporal Dementia, Alzheimer's disease and Parkinson's disease. These patterns are consistent with the propagation of protein misfolding and aggregation reminiscent of the prion diseases. There is a surge of evidence that suggests that large protein aggregates of a range of proteins are able to enter cells via macropinocytosis. Our recent work suggests that this process is activated by the binding of aggregates to the neuron cell surface. The current review considers the potential role of cell surface receptors in the triggering of macropinocytosis by protein aggregates and the possibility of utilizing macropinocytosis pathways as a therapeutic target.
机译:诸如神经元丢失和病理性蛋白质聚集体等病理变化的时空格局是神经退行性疾病(如肌萎缩性侧索硬化症,额颞痴呆,阿尔茨海默氏病和帕金森氏病)的特征。这些模式与蛋白质的错误折叠和聚集的传播一致,使人联想到the病毒疾病。大量证据表明,一系列蛋白质的大蛋白质聚集体能够通过巨胞饮作用进入细胞。我们最近的工作表明,这一过程被聚集体与神经元细胞表面的结合所激活。本篇综述考虑了细胞表面受体在蛋白质聚集体触发巨胞饮作用中的潜在作用,以及利用巨胞饮作用途径作为治疗靶点的可能性。

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