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Reduced variability of neural progenitor cells and improved purity of neuronal cultures using magnetic activated cell sorting

机译:用磁性活性细胞分选降低神经祖细胞的可变性,改善神经元培养的纯度

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摘要

Genetic and epigenetic variability between iPSC-derived neural progenitor cells (NPCs) combined with differences in investigator technique and selection protocols contributes to variability between NPC lines, which subsequently impacts the quality of differentiated neuronal cultures. We therefore sought to develop an efficient method to reduce this variability in order to improve the purity of NPC and neuronal cultures. Here, we describe a magnetic activated cell sorting (MACS) method for enriching NPC cultures for CD271-/CD133+ cells at both early (10) passage. MACS results in a similar sorting efficiency to fluorescence activated cell sorting (FACS), while achieving an increased yield of live cells and reduced cellular stress. Furthermore, neurons derived from MACS NPCs showed greater homogeneity between cell lines compared to those derived from unsorted NPCs. We conclude that MACS is a cheap technique for incorporation into standard NPC differentiation and maintenance protocols in order to improve culture homogeneity and consistency.
机译:IPSC衍生的神经祖细胞(NPC)与研究者技术和选择方案差异相结合的遗传和表观遗传变异有助于NPC线之间的可变性,这随后影响分化的神经元培养物的质量。因此,我们寻求开发一种有效的方法来减少这种可变性,以提高NPC和神经元培养物的纯度。这里,我们描述了一种磁性活性细胞分选(MACS)方法,用于在早期(10)段中,富集CD271- / CD133 +细胞的NPC培养物。 MACS导致荧光活性细胞分选(FACS)的类似分选效率,同时实现活细胞产率和细胞应激降低。此外,衍生自Macs NPC的神经元在细胞系比较与衍生自未排序的NPC的那些之间的均匀性均有更大的均匀性。我们得出结论,MAC是一种廉价的技术,用于纳入标准NPC分化和维护方案,以提高培养均匀性和一致性。

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