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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Smoothened signaling in the mouse osteoblastoid lineage is required for efficient B lymphopoiesis
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Smoothened signaling in the mouse osteoblastoid lineage is required for efficient B lymphopoiesis

机译:高效的B淋巴细胞素质需要平滑的小鼠OSTeooblastoid谱系中的信号传导

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The stromal signals that promote B lymphopoiesis remain poorly understood. Hedgehog (Hh) signaling promotes B lymphopoiesis in a non-cell-autonomous fashion in vitro, and depletion of the Hh effector Smoothened (Smo) from stromal cells is associated with the loss of osteoblastoid markers. These observations suggested that Hh signaling in the osteoblastoid lineage promotes B lymphopoiesis in vivo. To test this, we employed a mouse model for conditional ablation of Smo in the osteoblastoid lineage. Depletion of Smo from osteoblastoid cells is associated with profound and selective reductions in the number and proportion of bone marrow B-lymphoid progenitors. Upon partial bone marrow ablation, mutant animals exhibit delayed repopulation of the B-lymphoid compartment after the early lymphoid progenitor stage. Primary osteoblasts from mutant mice are defective in supporting B lymphopoiesis in vitro, whereas hematopoietic progenitors from mutant mice exhibit normal differentiation. Weconclude that efficient B lymphopoiesis in vivo is dependent on the maintenance of Hh signaling in the osteoblastoid lineage.
机译:促进B淋巴细胞的基质信号仍然明白很差。刺猬(HH)信号传导在体外以非细胞自主方式促进B淋巴细胞症,并且来自基质细胞的HH效应器(Smo)的耗尽与骨细胞标记物的损失有关。这些观察结果表明,骨细胞骨谱系中的HH信号传导促进体内B淋巴细胞。为了测试这一点,我们采用了一种小鼠模型,用于在骨丝细胞谱系中的条件消融Smo。从骨细胞细胞中耗尽来自骨细胞细胞的脱脂与骨髓B淋巴祖细胞血浆的数量和比例的深刻和选择性降低有关。在部分骨髓消融后,突变动物在早期淋巴祖级后表现出B淋巴室的延迟重新灌注。来自突变小鼠的初级成骨细胞在体外支持B淋巴细胞凋亡方面是缺陷的,而来自突变小鼠的造血祖细胞表现出正常分化。 Vivo中的高效B淋巴细胞症的WeConclude取决于骨细胞谱系中HH信号传导的维持。

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