首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Rac signaling in osteoblastic cells is required for normal bone development but is dispensable for hematopoietic development.
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Rac signaling in osteoblastic cells is required for normal bone development but is dispensable for hematopoietic development.

机译:成骨细胞中的Rac信号是正常骨骼发育所必需的,但对于造血发育却是必不可少的。

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摘要

Hematopoietic stem cells (HSCs) interact with osteoblastic, stromal, and vascular components of the BM hematopoietic microenvironment (HM) that are required for the maintenance of long-term self-renewal in vivo. Osteoblasts have been reported to be a critical cell type making up the HSC niche in vivo. Rac1 GTPase has been implicated in adhesion, spreading, and differentiation of osteoblast cell lines and is critical for HSC engraftment and retention. Recent data suggest a differential role of GTPases in endosteal/osteoblastic versus perivascular niche function. However, whether Rac signaling pathways are also necessary in the cell-extrinsic control of HSC function within the HM has not been examined. In the present study, genetic and inducible models of Rac deletion were used to demonstrate that Rac depletion causes impaired proliferation and induction of apoptosis in the OP9 cell line and in primary BM stromal cells. Deletion of Rac proteins caused reduced trabecular and cortical long bone growth in vivo. Surprisingly, HSC function and maintenance of hematopoiesis in vivo was preserved despite these substantial cell-extrinsic changes. These data have implications for therapeutic strategies to target Rac signaling in HSC mobilization and in the treatment of leukemia and provide clarification to our evolving concepts of HSC-HM interactions.
机译:造血干细胞(HSC)与BM造血微环境(HM)的成骨,基质和血管成分相互作用,这是维持体内长期自我更新所必需的。据报道,成骨细胞是构成体内HSC位的关键细胞类型。 Rac1 GTPase与成骨细胞系的粘附,扩散和分化有关,对于HSC的植入和保留至关重要。最近的数据表明GTPases在骨内/成骨细胞与血管周围生境功能中的作用不同。但是,尚未研究过Rac信号通路是否在HM内HSC功能的细胞外控制中也必需。在本研究中,Rac缺失的遗传模型和诱导模型用于证明Rac耗竭会导致OP9细胞系和原代BM基质细胞增殖和凋亡诱导减弱。 Rac蛋白的删除导致体内小梁和皮质长骨生长减少。出人意料的是,尽管有这些实质性的细胞外源性变化,HSC功能和体内造血功能的维持仍得以保留。这些数据对在HSC动员和白血病治疗中靶向Rac信号传导的治疗策略具有意义,并为我们不断发展的HSC-HM相互作用概念提供了澄清。

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