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体外模拟神经退行性疾病中铁代谢异常:范例、陷阱、可能性及实际考量

Modelling iron mismanagement in neurodegenerative disease in vitro: paradigms, pitfalls, possibilities & practical considerations.

作者信息

Healy Sinead, McMahon Jill M, FitzGerald Una

机构信息

Galway Neuroscience Centre, School of Natural Sciences, Biomedical Sciences Building, National University of Ireland, Galway, Ireland.

Galway Neuroscience Centre, School of Natural Sciences, Biomedical Sciences Building, National University of Ireland, Galway, Ireland.

出版信息

Prog Neurobiol. 2017 Nov;158:1-14. doi: 10.1016/j.pneurobio.2017.08.004. Epub 2017 Sep 25.

Abstract

Although aberrant metabolism and deposition of iron has been associated with aging and neurodegeneration, the contribution of iron to neuropathology is unclear. Well-designed model systems that are suited to studying the putative pathological effect of iron are likely to be essential if such unresolved details are to be clarified. In this review, we have evaluated the utility and effectiveness of the reductionist in vitro platform to study the molecular mechanisms putatively underlying iron perturbations of neurodegenerative disease. The expression and function of iron metabolism proteins in glia and neurons and the extent to which this iron regulatory system is replicated in in vitro models has been comprehensively described, followed by an appraisal of the inherent suitability of different in vitro and ex vivo models that have been, or might be, used for iron loading. Next, we have identified and critiqued the relevant experimental parameters that have been used in in vitro iron loading experiments, including the choice of iron reagent, relevant iron loading concentrations and supplementation with serum or ascorbate, and propose optimal iron loading conditions. Finally, we have provided a synthesis of the differential iron accumulation and toxicity in glia and neurons from reported iron loading paradigms. In summary, this review has amalgamated the findings and paradigms of the published reports modelling iron loading in monocultures, discussed the limitations and discrepancies of such work to critically propose a robust, relevant and reliable model of iron loading to be used for future investigations.

摘要

尽管铁的异常代谢和沉积与衰老及神经退行性变有关,但铁对神经病理学的作用尚不清楚。如果要阐明这些未解决的细节,适合研究铁的假定病理效应的精心设计的模型系统可能至关重要。在本综述中,我们评估了简化的体外平台在研究神经退行性疾病铁紊乱潜在分子机制方面的实用性和有效性。全面描述了神经胶质细胞和神经元中铁代谢蛋白的表达和功能,以及该铁调节系统在体外模型中的复制程度,随后对已使用或可能用于铁加载的不同体外和离体模型的内在适用性进行了评估。接下来,我们确定并批评了体外铁加载实验中使用的相关实验参数,包括铁试剂的选择、相关铁加载浓度以及血清或抗坏血酸的补充,并提出了最佳铁加载条件。最后,我们综合了已报道的铁加载模式中神经胶质细胞和神经元中铁的差异积累和毒性。总之,本综述整合了已发表的关于单培养中铁加载建模报告的研究结果和模式,讨论了此类工作的局限性和差异,以批判性地提出一个强大、相关且可靠的铁加载模型,供未来研究使用。

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