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A 3D iPSC-differentiation model identifies interleukin-3 as a regulator of early human hematopoietic specification

机译:3D IPSC差异化模型将白细胞介素-3识别为早期人造血规范的调节器

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Hematopoietic development is spatiotemporally tightly regulated by defined cell-intrinsic and extrinsic modifiers. The role of cytokines has been intensively studied in adult hematopoiesis; however, their role in embryonic hematopoietic specification remains largely unexplored. Here, we used induced pluripotent stem cell (iPSC) technology and established a 3-dimensional (3D), organoid-like differentiation system (“hemanoid”) maintaining the structural cellular integrity to evaluate the effect of cytokines on embryonic hematopoietic development. We show that defined stages of early human hematopoietic development were recapitulated within the generated hemanoids. We identified KDR+/CD34 ~(high)/CD144+/CD43 ~(–)/CD45 ~(–) hemato-endothelial progenitors (HEP) forming organized, vasculature-like structures and giving rise to CD34 ~(low)/CD144 ~(–)/CD43 ~(+)/CD45 ~(+) hematopoietic progenitor cells. We demonstrate that the endothelial to hematopoietic transition of HEP is dependent on the presence of interleukin 3 (IL-3). Inhibition of IL-3 signaling blocked hematopoietic differentiation and arrested the cells in the HEP stage. Thus, our data suggest an important role for IL-3 in early human hematopoiesis by supporting the endothelial to hematopoietic transition of HEP and highlight the potential of a hemanoid-based model to study human hematopoietic development.
机译:造血发育是由定义的细胞内在和外在修饰剂进行施用的瞬间受压。细胞因子的作用在成人血液缺陷中已经集中研究;然而,它们在胚胎造血规范中的作用仍然很大程度上是未开发的。这里,我们使用诱导多能干细胞(IPSC)技术,并建立了三维(3D),有机体状分化系统(“血红素”),保持结构细胞完整性,以评估细胞因子对胚胎造血发育的影响。我们表明,在生成的血管内概括了早期人造血发育的定义阶段。我们鉴定了KDR + / CD34〜(HIGH)/ CD144 + / CD43〜( - )/ CD45〜( - )血液内皮祖细胞(HEP)形成有组织,脉管系统的结构并产生CD34〜(低)/ CD144〜( - )/ CD43〜(+)/ CD45〜(+)造血祖细胞。我们证明HEP的造血转变的内皮依赖于白细胞介素3(IL-3)的存在。抑制IL-3信号传导阻断的造血分化并在HEP阶段捕获细胞。因此,我们的数据通过支持HEP的造血转变,突出了血外转变,为早期人造血中的IL-3在早期的人造血中表达了重要作用。

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