首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Novel, Non-Gene-Destructive Knock-In Reporter Mice Refute the Concept of Monoallelic Gata3 Expression
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Novel, Non-Gene-Destructive Knock-In Reporter Mice Refute the Concept of Monoallelic Gata3 Expression

机译:新颖的,非基因破坏性敲入的记者小鼠反驳单方面GATA3表达的概念

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Accurately tuned expression levels of the transcription factor GATA-3 are crucial at several stages of T cell and innate lymphoid cell development and differentiation. Moreover, several lines of evidence suggest that Gata3 expression might provide a reliable molecular marker for the identification of elusive progenitor cell subsets at the earliest stages of T lineage commitment. To be able to faithfully monitor Gata3 expression noninvasively at the single-cell level, we have generated a novel strain of knock-in reporter mice, termed GATIR, by inserting an expression cassette encoding a bright fluorescent marker into the 3'-untranslated region of the endogenous Gata3 locus. Importantly, in contrast to three previously published strains of Gata3 reporter mice, GATIR mice preserve physiological Gata3 expression on the targeted allele. In this study, we show that GATIR mice faithfully reflect endogenous Gata3 expression without disturbing the development of GATA-3-dependent lymphoid cell populations. We further show that GATIR mice provide an ideal tool for noninvasive monitoring of Th2 polarization and straightforward identification of innate lymphoid cell 2 progenitor populations. Finally, as our reporter is non-gene-destructive, GATIR mice can be bred to homozygosity, not feasible with previously published strains of Gata3 reporter mice harboring disrupted alleles. The availability of hetero- and homozygous Gata3 reporter mice with an exceptionally bright fluorescent marker, allowed us to visualize allelic Gata3 expression in individual cells simply by flow cytometry. The unambiguous results obtained provide compelling evidence against previously postulated monoallelic Gata3 expression in early T lineage and hematopoietic stem cell subsets.
机译:转录因子GATA-3的精确调谐表达水平在T细胞的几个阶段和先天淋巴细胞发育和分化的关键。此外,几种证据表明,GATA3表达可以提供可靠的分子标记,用于识别T谱系承诺的最早阶段的难以捉摸的祖细胞亚群。为了能够忠实地在单细胞水平下忠实地监测GATA3表达,我们通过将编码明亮荧光标记物的表达盒插入到3' - 未转换区域的表达式盒中产生了一种新的敲入报道小鼠的新敲击报道小鼠菌株内源性gata3基因座。重要的是,与三个先前发表的GATA3报告小鼠的三种发表的菌株相比,GATIR​​小鼠在靶向等位基因上保留生理GATA3表达。在这项研究中,我们表明GATIR​​小鼠忠实地反映内源性GATA3表达,而不会扰乱GATA-3依赖性淋巴细胞群的发育。我们进一步表明,Gatir小鼠提供了一种非侵入性监测Th2偏振的理想工具,并直接鉴定先天​​淋巴细胞2个祖细胞群。最后,由于我们的记者是非基因破坏性的,加入小鼠可以培育纯合子,而不可行,与之前发表过的GATA3报告小鼠窝藏中断的等位基因的溶胀不可行。具有异常明亮的荧光标记物的异质和纯合GATA3报告小鼠的可用性使我们能够仅通过流式细胞术来可视化个体细胞中的等位基因GATA3表达。获得的明确结果提供了针对早期T谱系和造血干细胞亚群中的先前假定的单邻型GATA3表达的引人注目的证据。

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