Feinberg School of Medicine and Robert H. Lurie Comprehensive Cancer Center, Northwestern University, Chicago, Illinois 60611, USA.
J Clin Invest. 2013 Sep;123(9):3952-66. doi: 10.1172/JCI69032. Epub 2013 Aug 8.
Emergency granulopoiesis is a component of the innate immune response that is induced in response to infectious or inflammatory challenge. It is characterized by the rapid expansion and differentiation of granulocyte/monocyte progenitor (GMP) populations, which is due in part to a shortened S-phase of the cell cycle. We found that IRF8 (also known as ICSBP), an interferon regulatory transcription factor that activates phagocyte effector genes during the innate immune response, activates the gene encoding Fanconi C (Fancc) in murine myeloid progenitor cells. Moreover, IRF8-induced Fancc transcription was augmented by treatment with IL-1β, an essential cytokine for emergency granulopoiesis. The Fanconi pathway participates in repair of stalled or collapsed replication forks during DNA replication, leading us to hypothesize that the Fanconi pathway contributes to genomic stability during emergency granulopoiesis. In support of this hypothesis, Fancc(-/-) mice developed anemia and neutropenia during repeated, failed episodes of emergency granulopoiesis. Failed emergency granulopoiesis in Fancc(-/-) mice was associated with excess apoptosis of HSCs and progenitor cells in the bone marrow and impaired HSC function. These studies have implications for understanding the pathogenesis of bone marrow failure in Fanconi anemia and suggest possible therapeutic approaches.
应急性粒细胞生成是先天免疫反应的一个组成部分,它是对感染或炎症挑战的反应而诱导产生的。其特征是粒细胞/单核细胞祖细胞 (GMP) 群体的快速扩增和分化,部分原因是细胞周期的 S 期缩短。我们发现,IRF8(也称为 ICSBP),一种在先天免疫反应中激活吞噬细胞效应基因的干扰素调节转录因子,在鼠骨髓祖细胞中激活编码范可尼 C(Fancc)的基因。此外,IL-1β(应急性粒细胞生成所必需的细胞因子)处理增强了 IRF8 诱导的 Fancc 转录。范可尼途径参与在 DNA 复制过程中修复停滞或崩溃的复制叉,这使我们假设范可尼途径在应急性粒细胞生成过程中有助于基因组稳定性。支持这一假说,在反复发生的应急性粒细胞生成失败中,Fancc(-/-) 小鼠出现贫血和中性粒细胞减少。Fancc(-/-) 小鼠中应急性粒细胞生成失败与骨髓中 HSCs 和祖细胞的过度凋亡以及 HSC 功能受损有关。这些研究对于理解范可尼贫血中骨髓衰竭的发病机制具有重要意义,并提示可能的治疗方法。
