首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Isogenic blood–brain barrier models based on patient‐derived stem cells display inter‐individual differences in cell maturation and functionality
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Isogenic blood–brain barrier models based on patient‐derived stem cells display inter‐individual differences in cell maturation and functionality

机译:基于患者衍生的干细胞的来自血管血脑屏障模型显示细胞成熟和功能间的个体间差异

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Abstract The blood–brain barrier ( BBB ) constitutes an important component of the neurovascular unit formed by specialized brain microvascular endothelial cells ( BMEC s) surrounded by astrocytes, pericytes, and neurons. Recently, isogenic in?vitro models of the BBB based on human pluripotent stem cells have been documented, yet the impact of inter‐individual variability on the yield and phenotype of such models remains to be documented. In this study, we investigated the impact of inter‐individual variability on the yield and phenotype of isogenic models of the BBB , using patient‐derived induced pluripotent stem cells ( iPSC s). Astrocytes, BMEC s, and neurons were differentiated from four asymptomatic patient‐derived iPSC s (two males, two females). We differentiated such cells using existing differentiation protocols and quantified expression of cell lineage markers, as well as BBB phenotype, barrier induction, and formation of neurite processes. iPSC ‐derived BMEC s showed barrier properties better than hCMEC /D3 monolayers; however, we noted differences in the expression and activity among iPSC lines. In addition, we noted differences in the differentiation efficiency of these cells into neural stem cells and progenitor cells (as noted by differences in expression of cell lineage markers). Such differences were reflected later in the terminal differentiation, as seen as ability to induce barrier function and to form neurite processes. Although we demonstrated our ability to obtain an isogenic model of the BBB with different patients’ iPSC s, we also noted subtle differences in the expression of cell lineage markers and cell maturation processes, suggesting the presence of inter‐individual polymorphisms.
机译:摘要血脑屏障(BBB)构成由星形细胞,周围和神经元包围的专用脑微血管内皮细胞(BMEC)形成的神经血管单元的重要组成部分。最近,已经记录了基于人多能干细胞的BBB的体外模型的Isogensic,然而,个体间可变性对这些模型的产量和表型的影响仍有待记录。在这项研究中,我们使用患者衍生的诱导多能干细胞(IPSC S)来研究各种变异性对BBB的等源模型的产量和表型的影响。星形胶质细胞,BMEC S和神经元由四种无症状患者衍生的IPSC S(两只男性,两名女性)分化。我们使用现有的分化方案和细胞谱系标记的量化表达,以及BBB表型,阻隔诱导和形成神经突方法的表达。 IPSC -Derived BMEC S比HCMEC / D3单层更好地显示屏性能;但是,我们注意到IPSC线路之间表达和活动的差异。此外,我们注意到这些细胞的分化效率的差异在神经干细胞和祖细胞中(如细胞谱系标记表达的差异所指出的)。在末端分化中稍后将这种差异反映,视为诱导阻隔功能和形成神经突方法的能力。虽然我们证明了我们用不同患者的IPSC S获得BBB的同质模型的能力,但我们还注意到细胞谱系标记和细胞成熟过程表达的微妙差异,表明存在间间多态性。

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