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RNA sequencing demonstrates large-scale temporal dysregulation of gene expression in stimulated macrophages derived from MHC-defined chicken haplotypes

机译:RNA测序证明了源自MHC定义的鸡单倍型的受刺激巨噬细胞中基因表达的大规模时间失调

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摘要

Discovering genetic biomarkers associated with disease resistance and enhanced immunity is critical to developing advanced strategies for controlling viral and bacterial infections in different species. Macrophages, important cells of innate immunity, are directly involved in cellular interactions with pathogens, the release of cytokines activating other immune cells and antigen presentation to cells of the adaptive immune response. IFNγ is a potent activator of macrophages and increased production has been associated with disease resistance in several species. This study characterizes the molecular basis for dramatically different nitric oxide production and immune function between the B2 and the B19 haplotype chicken macrophages.A large-scale RNA sequencing approach was employed to sequence the RNA of purified macrophages from each haplotype group (B2 vs. B19) during differentiation and after stimulation. Our results demonstrate that a large number of genes exhibit divergent expression between B2 and B19 haplotype cells both prior and after stimulation. These differences in gene expression appear to be regulated by complex epigenetic mechanisms that need further investigation.
机译:发现与疾病抗性和增强的免疫力相关的遗传生物标志物对于制定先进的策略来控制不同物种的病毒和细菌感染至关重要。巨噬细胞是先天免疫的重要细胞,直接参与与病原体的细胞相互作用,激活其他免疫细胞的细胞因子的释放以及向适应性免疫应答细胞的抗原呈递。 IFNγ是巨噬细胞的有效激活剂,在几种物种中,增加的产量与抗病性有关。这项研究描述了B2和B19单倍型鸡巨噬细胞之间一氧化氮产生和免疫功能显着不同的分子基础。采用大规模RNA测序方法对每个单倍型组的纯化巨噬细胞的RNA进行测序(B2 vs.B19) )在分化过程中和刺激后。我们的结果表明,大量的基因在刺激之前和之后都在B2和B19单倍型细胞之间表现出不同的表达。基因表达的这些差异似乎受复杂的表观遗传机制调控,需要进一步研究。

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