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细胞命运决定因子 Scribble 对于维持造血干细胞功能是必需的。

The cell fate determinant Scribble is required for maintenance of hematopoietic stem cell function.

机构信息

Innere Medizin II, Hämatologie und Onkologie, Universitätsklinikum Jena, Jena, Germany.

Leibniz Institute on Aging, Fritz-Lipmann Institute, Jena, Germany.

出版信息

Leukemia. 2018 May;32(5):1211-1221. doi: 10.1038/s41375-018-0025-0. Epub 2018 Jan 30.

Abstract

Cell fate determinants influence self-renewal potential of hematopoietic stem cells. Scribble and Llgl1 belong to the Scribble polarity complex and reveal tumor-suppressor function in drosophila. In hematopoietic cells, genetic inactivation of Llgl1 leads to expansion of the stem cell pool and increases self-renewal capacity without conferring malignant transformation. Here we show that genetic inactivation of its putative complex partner Scribble results in functional impairment of hematopoietic stem cells (HSC) over serial transplantation and during stress. Although loss of Scribble deregulates transcriptional downstream effectors involved in stem cell proliferation, cell signaling, and cell motility, these effectors do not overlap with transcriptional targets of Llgl1. Binding partner analysis of Scribble in hematopoietic cells using affinity purification followed by mass spectometry confirms its role in cell signaling and motility but not for binding to polarity modules described in drosophila. Finally, requirement of Scribble for self-renewal capacity also affects leukemia stem cell function. Thus, Scribble is a regulator of adult HSCs, essential for maintenance of HSCs during phases of cell stress.

摘要

细胞命运决定因素影响造血干细胞的自我更新能力。Scribble 和 Llgl1 属于 Scribble 极性复合物,在果蝇中显示出肿瘤抑制功能。在造血细胞中,Llgl1 的基因失活导致干细胞池的扩张和自我更新能力的增加,而不会导致恶性转化。在这里,我们表明其假定的复合物伙伴 Scribble 的基因失活导致造血干细胞 (HSC) 在连续移植和应激期间的功能障碍。尽管 Scribble 的缺失会使参与干细胞增殖、细胞信号转导和细胞迁移的转录下游效应物失活,但这些效应物与 Llgl1 的转录靶标并不重叠。使用亲和纯化和质谱分析鉴定造血细胞中的 Scribble 结合伙伴,证实其在细胞信号转导和迁移中的作用,但不在果蝇中描述的极性模块中。最后,Scribble 对自我更新能力的要求也会影响白血病干细胞的功能。因此,Scribble 是成体 HSC 的调节剂,对细胞应激期间 HSC 的维持至关重要。

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