Department of Cell and Developmental Biology, University of Michigan Medical School, Ann Arbor, MI;
Blood. 2013 Nov 28;122(23):3798-807. doi: 10.1182/blood-2013-04-496166. Epub 2013 Oct 3.
In previous mass spectrometry and coimmune precipitation studies, we identified tripartite motif-containing 28 (TRIM28; also known as transcriptional intermediary factor1β and Krüppel-associated box-associated protein-1) as a cofactor that specifically copurified with an NR2C1/NR2C2 (TR2/TR4) orphan nuclear receptor heterodimer that previous studies had implicated as an embryonic/fetal β-type globin gene repressor. TRIM28 has been characterized as a transcriptional corepressor that can associate with many different transcription factors and can play functional roles in multiple tissues and cell types. Here, we tested the contribution of TRIM28 to globin gene regulation and erythropoiesis using a conditional loss-of-function in vivo model. We discovered that Trim28 genetic loss in the adult mouse leads to defective immature erythropoiesis in the bone marrow and consequently to anemia. We further found that TRIM28 controls erythropoiesis in a cell-autonomous manner by inducibly deleting Trim28 exclusively in hematopoietic cells. Finally, in the absence of TRIM28, we observed increased apoptosis as well as diminished expression of multiple erythroid transcription factors and heme biosynthetic enzymes in immature erythroid cells. Thus, TRIM28 is essential for the cell-autonomous development of immature erythroblasts in the bone marrow.
在先前的质谱分析和共免疫沉淀研究中,我们鉴定出三部分基序蛋白 28(TRIM28;也称为转录中介因子 1β和 Krüppel 相关盒相关蛋白 1)作为一个辅助因子,它可以与先前研究表明的 NR2C1/NR2C2(TR2/TR4)孤儿核受体异二聚体特异性共纯化,该异二聚体被认为是胚胎/胎儿β型珠蛋白基因的抑制剂。TRIM28 已被描述为一种转录共抑制因子,它可以与许多不同的转录因子结合,并在多种组织和细胞类型中发挥功能作用。在这里,我们使用体内条件性基因缺失模型来测试 TRIM28 对珠蛋白基因调控和红细胞生成的贡献。我们发现,成年小鼠中的 Trim28 基因缺失导致骨髓中未成熟红细胞生成缺陷,进而导致贫血。我们进一步发现,TRIM28 通过在造血细胞中特异性缺失 Trim28 以细胞自主的方式控制红细胞生成。最后,在没有 TRIM28 的情况下,我们观察到未成熟红细胞中的细胞凋亡增加,以及多个红细胞转录因子和血红素生物合成酶的表达减少。因此,TRIM28 对于骨髓中未成熟红细胞的细胞自主发育是必需的。
