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胸腺细胞分化的单细胞分析:转录因子相互作用的鉴定以及αβ谱系定向中的一个主要随机成分。

Single-cell analysis of thymocyte differentiation: identification of transcription factor interactions and a major stochastic component in αβ-lineage commitment.

作者信息

Boudil Amine, Skhiri Lamia, Candéias Serge, Pasqualetto Valérie, Legrand Agnès, Bedora-Faure Marie, Gautreau-Rolland Laetitia, Rocha Benedita, Ezine Sophie

机构信息

Institut National de la Santé et de la Recherche Médicale, Unité 1020, and Université Paris Descartes, Unité Mixte de Recherche, Paris, France.

出版信息

PLoS One. 2013 Oct 1;8(10):e73098. doi: 10.1371/journal.pone.0073098. eCollection 2013.

Abstract

T cell commitment and αβ/γδ lineage specification in the thymus involves interactions between many different genes. Characterization of these interactions thus requires a multiparameter analysis of individual thymocytes. We developed two efficient single-cell methods: (i) the quantitative evaluation of the co-expression levels of nine different genes, with a plating efficiency of 99-100% and a detection limit of 2 mRNA molecules/cell; and (ii) single-cell differentiation cultures, in the presence of OP9 cells transfected with the thymus Notch1 ligand DeltaL4. We show that during T cell commitment, Gata3 has a fundamental, dose-dependent role in maintaining Notch1 expression, with thymocytes becoming T-cell-committed when they co-express Notch1, Gata3 and Bc11b. Of the transcription factor expression patterns studied here, only that of Bcl11b was suggestive of a role in Pu1 down-regulation. Individual thymocytes became αβ/γδ lineage-committed at very different stages (from the TN2a stage onwards). However, 20% of TN3 cells are not αβ/γδ-lineage committed and TN4 cells comprise two main subpopulations with different degrees of maturity. The existence of a correlation between differentiation potential and expression of the pre-TCR showed that 83% of αβ-committed cells do not express the pre-TCR and revealed a major stochastic component in αβ-lineage specification.

摘要

胸腺中T细胞的定向分化以及αβ/γδ谱系的确定涉及许多不同基因之间的相互作用。因此,对这些相互作用的表征需要对单个胸腺细胞进行多参数分析。我们开发了两种高效的单细胞方法:(i)对9种不同基因的共表达水平进行定量评估,接种效率为99 - 100%,检测限为2个mRNA分子/细胞;(ii)在转染了胸腺Notch1配体DeltaL4的OP9细胞存在下进行单细胞分化培养。我们发现,在T细胞定向分化过程中,Gata3在维持Notch1表达方面具有重要的剂量依赖性作用,当胸腺细胞共表达Notch1、Gata3和Bc11b时,它们就会成为定向分化的T细胞。在此研究的转录因子表达模式中,只有Bcl11b的表达模式提示其在下调Pu1方面具有作用。单个胸腺细胞在非常不同的阶段(从TN2a阶段开始)成为αβ/γδ谱系定向分化的细胞。然而,20%的TN3细胞未定向分化为αβ/γδ谱系,TN4细胞包含两个具有不同成熟度的主要亚群。前TCR的表达与分化潜能之间存在相关性,这表明83%的αβ定向分化细胞不表达前TCR,并揭示了αβ谱系确定过程中存在一个主要的随机成分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/529a/3787938/a83c15d0f941/pone.0073098.g001.jpg

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