Department of Pediatrics, Emory University School of Medicine, Atlanta, GA.
Department of Internal Medicine, University of Utah School of Medicine, Salt Lake City, UT.
Exp Hematol. 2022 Aug-Sep;112-113:24-34. doi: 10.1016/j.exphem.2022.06.002. Epub 2022 Jul 6.
Germline mutations in ETV6 are associated with a syndrome of thrombocytopenia and leukemia predisposition, and ETV6 is among the most commonly mutated genes in leukemias, especially childhood B-cell acute lymphoblastic leukemia. However, the mechanisms underlying disease caused by ETV6 dysfunction are poorly understood. To address these gaps in knowledge, using CRISPR/Cas9, we developed a mouse model of the most common recurrent, disease-causing germline mutation in ETV6. We found defects in hematopoiesis related primarily to abnormalities of the multipotent progenitor population 4 (MPP4) subset of hematopoietic progenitor cells and evidence of sterile inflammation. Expression of ETV6 in Ba/F3 cells altered the expression of several cytokines, some of which were also detected at higher levels in the bone marrow of the mice with Etv6 mutation. Among these, interleukin-18 and interleukin-13 abrogated B-cell development of sorted MPP4 cells, but not common lymphoid progenitors, suggesting that inflammation contributes to abnormal hematopoiesis by impairing lymphoid development. These data, along with those from humans, support a model in which ETV6 dysfunction promotes inflammation, which adversely affects thrombopoiesis and promotes leukemogenesis.
ETV6 种系突变与血小板减少和白血病易感性综合征相关,并且 ETV6 是白血病中最常突变的基因之一,尤其是儿童 B 细胞急性淋巴细胞白血病。然而,ETV6 功能障碍引起疾病的机制还知之甚少。为了解决这些知识空白,我们使用 CRISPR/Cas9 技术,开发了一种 ETV6 最常见的复发性、致病变异体系突变的小鼠模型。我们发现造血功能缺陷主要与造血祖细胞的多能祖细胞 4 (MPP4)亚群的异常有关,并存在无菌性炎症的证据。在 Ba/F3 细胞中表达 ETV6 改变了几种细胞因子的表达,其中一些细胞因子在 Etv6 突变小鼠的骨髓中也检测到更高水平。其中,白细胞介素-18 和白细胞介素-13 可破坏分选的 MPP4 细胞的 B 细胞发育,但不能破坏普通淋巴祖细胞,表明炎症通过损害淋巴样发育而导致异常造血。这些数据以及来自人类的数据支持了一种模型,即 ETV6 功能障碍会促进炎症,从而对血小板生成产生不利影响并促进白血病发生。
