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Notch受体在造血谱系及髓系分化过程中的独特且受调控的表达。

Distinct and regulated expression of Notch receptors in hematopoietic lineages and during myeloid differentiation.

作者信息

Jönsson J I, Xiang Z, Pettersson M, Lardelli M, Nilsson G

机构信息

Department of Laboratory Medicine, Lund University, University Hospital MAS, Malmö, Sweden.

出版信息

Eur J Immunol. 2001 Nov;31(11):3240-7. doi: 10.1002/1521-4141(200111)31:11<3240::aid-immu3240>3.0.co;2-e.

Abstract

Hematopoietic development is a delicate balance of cell fate decisions in multipotent cells between self-renewal and differentiation. In multiple developmental systems, the Notch receptors are important factors regulating these processes. Hematopoietic progenitor cells have been shown to express Notch1, and studies with an activated intracellular form has revealed a functional role. To assess the function of other Notch members in hematopoiesis, we investigated the expression pattern of Notch1, Notch2, and Notch3 in hematopoietic lineages at the level of RNA and protein. We demonstrate that Notch1 and Notch2 are expressed in multiple lineages, and that Notch1 in particular appears to be regulated during myeloid differentiation. Notch1 was up-regulated and expressed at high levels in adherent macrophages. Mast cells expressed only low levels of Notch1 mRNA whereas Notch2 mRNA was highly expressed. In addition we could detect Notch3 mRNA and protein in cell lines representing mast cell progenitors. These expression patterns imply that the different Notch genes may have very distinct functions during hematopoiesis, and that Notch3 could be a specific regulator of mast cell development. The finding that Notch1 was up-regulated in the adherent cells developing from a multipotent progenitor cell line suggests that this protein may posses dual functions in hematopoiesis, i.e. at the stage of cell fate decision, and at the maturation stage of monocytes when adhesion to the specific microenvironment is accomplished.

摘要

造血发育是多能细胞在自我更新和分化之间细胞命运决定的微妙平衡。在多个发育系统中,Notch受体是调节这些过程的重要因素。造血祖细胞已被证明表达Notch1,对活化细胞内形式的研究揭示了其功能作用。为了评估其他Notch成员在造血中的功能,我们在RNA和蛋白质水平上研究了Notch1、Notch2和Notch3在造血谱系中的表达模式。我们证明Notch1和Notch2在多个谱系中表达,特别是Notch1在髓系分化过程中似乎受到调控。Notch1在贴壁巨噬细胞中上调并高水平表达。肥大细胞仅表达低水平的Notch1 mRNA,而Notch2 mRNA则高表达。此外,我们在代表肥大细胞祖细胞的细胞系中检测到了Notch3 mRNA和蛋白质。这些表达模式表明,不同的Notch基因在造血过程中可能具有非常不同的功能,并且Notch3可能是肥大细胞发育的特异性调节因子。从多能祖细胞系发育而来的贴壁细胞中Notch1上调的发现表明,这种蛋白在造血过程中可能具有双重功能,即在细胞命运决定阶段,以及在单核细胞成熟阶段,当与特定微环境粘附完成时。

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