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通过深度 CAGE 测序重新定义人类肥大细胞转录组。

Redefinition of the human mast cell transcriptome by deep-CAGE sequencing.

机构信息

RIKEN Center for Life Science Technologies, Division of Genomic Technologies, Yokohama, Kanagawa, Japan;

出版信息

Blood. 2014 Apr 24;123(17):e58-67. doi: 10.1182/blood-2013-02-483792. Epub 2014 Mar 26.

Abstract

Mast cells (MCs) mature exclusively in peripheral tissues, hampering research into their developmental and functional programs. Here, we employed deep cap analysis of gene expression on skin-derived MCs to generate the most comprehensive view of the human MC transcriptome ever reported. An advantage is that MCs were embedded in the FANTOM5 project, giving the opportunity to contrast their molecular signature against a multitude of human samples. We demonstrate that MCs possess a unique and surprising transcriptional landscape, combining hematopoietic genes with those exclusively active in MCs and genes not previously reported as expressed by MCs (several of them markers of unrelated tissues). We also found functional bone morphogenetic protein receptors transducing activatory signals in MCs. Conversely, several immune-related genes frequently studied in MCs were not expressed or were weakly expressed. Comparing MCs ex vivo with cultured counterparts revealed profound changes in the MC transcriptome in in vitro surroundings. We also determined the promoter usage of MC-expressed genes and identified associated motifs active in the lineage. Befitting their uniqueness, MCs had no close relative in the hematopoietic network (also only distantly related with basophils). This rich data set reveals that our knowledge of human MCs is still limited, but with this resource, novel functional programs of MCs may soon be discovered.

摘要

肥大细胞(MCs)仅在外周组织中成熟,这阻碍了对其发育和功能程序的研究。在这里,我们采用深度帽分析技术对皮肤来源的 MCs 进行基因表达分析,生成了迄今为止报道的最全面的人类 MC 转录组视图。一个优势是 MCs 被嵌入 FANTOM5 项目中,有机会将其分子特征与大量人类样本进行对比。我们证明 MCs 具有独特而令人惊讶的转录景观,将造血基因与仅在 MCs 中活跃的基因以及以前未报道过的由 MCs 表达的基因(其中一些是无关组织的标志物)结合在一起。我们还发现了功能性骨形态发生蛋白受体在 MCs 中传递激活信号。相反,在 MCs 中经常研究的几个与免疫相关的基因没有表达或表达较弱。将 MCs 在体与培养的对应物进行比较,揭示了在体外环境中 MC 转录组的深刻变化。我们还确定了 MC 表达基因的启动子使用情况,并鉴定了与该谱系相关的活性基序。由于其独特性,MCs 在造血网络中没有密切相关的(也与嗜碱性粒细胞只有远亲关系)。这个丰富的数据集表明,我们对人类 MCs 的了解仍然有限,但有了这个资源,MCs 的新功能程序可能很快就会被发现。

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