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Discrete roles of canonical and non-canonical Wnt signaling in hematopoiesis and lymphopoiesis

机译:典范和非典范Wnt信号在造血和淋巴细胞生成中的离散作用

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摘要

The mechanisms that regulate proliferation, fate decisions and differentiation of hematopoietic stem cells (HSC) and thymic stem cells are highly complex. Several signaling pathways including Wnt signaling have important roles during these processes. Both canonical and non-canonical Wnt signaling are important in normal and malignant hematopoiesis and lymphoid development, yet their precise roles are controversial. In a side-by-side comparison, we investigated the roles of the canonical and non-canonical Wnt pathway in hematopoiesis and thymopoiesis. As complete loss-of-function models for non-canonical Wnt signaling are not yet available and highly complex for canonical Wnt signaling, we decided to use a gain-of-function approach. To this end, Wnt3a and Wn5a, two well-known prototypical canonical and non-canonical Wnt ligands were produced in hematopoiesis supporting stromal assays. High levels of Wnt3a signaling blocked T-cell development at early stages, whereas intermediate levels accelerated T-cell development. In contrast, Wnt5a signaling prompted apoptosis in developing thymocytes, without affecting differentiation at a particular stage. To explore the role of Wnt3a and Wnt5a in vivo , we transduced HSCs isolated from fetal liver, transduced with Wnt3a and Wnt5a vectors, and performed reconstitution assays in irradiated C57Bl/6 mice. Wnt3a overexpression led to increased lymphopoiesis, whereas Wnt5a augments myelopoiesis in the bone marrow (BM) and spleen. Thus, the canonical and non-canonical Wnt signaling have discrete roles in hematopoiesis and thymopoiesis, and understanding their right dose of action is crucial for prospective translational applications.
机译:调节造血干细胞(HSC)和胸腺干细胞增殖,命运决定和分化的机制非常复杂。在这些过程中,包括Wnt信号传导在内的几种信号传导途径都具有重要作用。经典和非经典的Wnt信号在正常和恶性造血和淋巴样发展中都很重要,但它们的确切作用尚存争议。在并排比较中,我们研究了经典和非经典Wnt通路在造血和胸腺生成中的作用。由于尚无用于非经典Wnt信号的完整功能丧失模型,并且对于经典Wnt信号而言非常复杂,因此,我们决定使用功能增益方法。为此,在支持基质测定的造血过程中产生了Wnt3a和Wn5a,这两个众所周知的原型经典和非经典Wnt配体。高水平的Wnt3a信号传导在早期阶段阻止了T细胞发育,而中等水平则加速了T细胞发育。相反,Wnt5a信号传导提示正在发育的胸腺细胞凋亡,而不影响特定阶段的分化。为了探索Wnt3a和Wnt5a在体内的作用,我们转导了从胎儿肝脏分离的HSC,转导了Wnt3a和Wnt5a载体,并在辐照过的C57Bl / 6小鼠中进行了重组分析。 Wnt3a过表达导致淋巴细胞生成增加,而Wnt5a增强骨髓(BM)和脾脏中的骨髓生成。因此,规范和非规范的Wnt信号在造血和胸腺生成中具有离散的作用,并且了解它们的正确剂量对于预期的翻译应用至关重要。

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