Department of Hematology, St. Jude Children's Research Hospital, Memphis, Tennessee, USA.
Department of Biostatistics, St. Jude Children's Research Hospital, Memphis, Tennessee, USA.
Stem Cells. 2018 Jun;36(6):943-950. doi: 10.1002/stem.2800. Epub 2018 Feb 27.
Hematopoietic stem and progenitor cells (HSPCs) are necessary for life-long blood production and replenishment of the hematopoietic system during stress. We recently reported that nuclear factor I/X (Nfix) promotes HSPC survival post-transplant. Here, we report that ectopic expression of Nfix in primary mouse HSPCs extends their ex vivo culture from about 20 to 40 days. HSPCs overexpressing Nfix display hypersensitivity to supportive cytokines and reduced apoptosis when subjected to cytokine deprivation relative to controls. Ectopic Nfix resulted in elevated levels of c-Mpl transcripts and cell surface protein on primary murine HSPCs as well as increased phosphorylation of STAT5, which is known to be activated down-stream of c-MPL. Blocking c-MPL signaling by removal of thrombopoietin or addition of a c-MPL neutralizing antibody negated the antiapoptotic effect of Nfix overexpression on cultured HSPCs. Furthermore, NFIX was capable of binding to and transcriptionally activating a proximal c-Mpl promoter fragment. In sum, these data suggest that NFIX-mediated upregulation of c-Mpl transcription can protect primitive hematopoietic cells from stress ex vivo. Stem Cells 2018;36:943-950.
造血干细胞和祖细胞(HSPCs)是终身血液生成所必需的,并且在应激期间可补充造血系统。我们最近报道,核因子 I/X(Nfix)可促进移植后 HSPC 的存活。在这里,我们报告外源表达 Nfix 可将原代小鼠 HSPC 的体外培养时间从约 20 天延长至 40 天。与对照相比,过表达 Nfix 的 HSPC 对支持细胞因子表现出超敏性,并且在受到细胞因子剥夺时凋亡减少。外源 Nfix 导致原代鼠 HSPC 上 c-Mpl 转录物和细胞表面蛋白水平升高,以及已知在 c-MPL 下游激活的 STAT5 磷酸化增加。通过去除血小板生成素或添加 c-MPL 中和抗体阻断 c-MPL 信号,可消除 Nfix 过表达对培养 HSPC 凋亡的保护作用。此外,NFIX 能够结合并转录激活 c-Mpl 启动子的近端片段。总而言之,这些数据表明,NFIX 介导的 c-Mpl 转录上调可保护原始造血细胞免受体外应激。《干细胞》2018;36:943-950.
