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Immunocytochemical analysis of valproic acid induced histone H3 and H4 acetylation during differentiation of rat adipose derived stem cells into neuron-like cells

机译:大鼠脂肪衍生干细胞分化到神经元样细胞中丙戊酸诱导组蛋白H3和H4乙酰化的免疫细胞化学分析

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摘要

Valproic acid (VPA) is an inhibitor of histone deacetylases (HDACs) that can regulate differentiation and proliferation of stem cells by epigenetic mechanisms. We investigated VPA induced histone H3 and H4 acetylation in adipose derived stem cells (ADSCs) transdifferentiated into neuron-like cells (NLCs). Rat ADSCs were transdifferentiated into neural stem cells (NSCs) that had been generated from neurospheres. The NSCs were differentiated into NLCs by induction with different concentrations of VPA at 24, 48 and 72 h. The NLCs were evaluated using anti-H3 and -H4 antibodies, and ADSCs, NSCs and NLCs were evaluated using immunofluorescence. The ADSCs were immunoreactive to CD90 and CD49d, but not to CD45 and CD31. Both the neurospheres and NSCs were immunostained with nestin and neurofilament 68. The neurospheres expressed Musashi1, Sox2 and Neu N genes as determined by RT-PCR. Our dose-response study indicated that the optimal concentration of VPA was 1 mM at 72 h. Histone acetylation levels of H3 and H4 immunostaining intensities in NLCs were significantly greater than for ADSCs and NSCs. VPA alters H4 and H3 acetylation immunoreactivities of ADSCs transdifferentiated into NLCs.
机译:丙戊酸(VPA)是组蛋白脱乙酰酶(HDACs)的抑制剂,其可以通过表观遗传机制调节干细胞的分化和增殖。我们研究了VPA诱导的组蛋白H3和H4乙酰化在转向神经元样细胞(NLC)中的脂肪衍生的干细胞(ADSC)中。将大鼠ADSC转化为从神经球产生的神经干细胞(NSCs)中。通过在24,48和72小时的不同浓度VPA诱导,NSCs与NLC分化为NLC。使用抗H3和-H4抗体评估NLC,使用免疫荧光评估ADSC,NSCs和NLC。 ADSCs对CD90和CD49D免疫反应,但不是CD45和CD31。 Neuropheres和NSCs均用巢蛋白和神经丝68免疫染色。神经球体表达了由RT-PCR测定的Musashi1,Sox2和Neu n基因。我们的剂量反应研究表明,72小时的VPA的最佳浓度为1mm。 NLC中H3和H4免疫染色强度的组肽乙酰化水平明显大于ADSC和NSCs。 VPA改变H4和H3乙酰化免疫反转转化为NLC的ADSC的免疫功能性。

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