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Notch and the regulation of osteoclast differentiation and function

机译:缺口和骨壳分化和功能的调节

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Notch 1 through 4 are transmembrane receptors that play a pivotal role in cell differentiation and function; this review addresses the role of Notch signaling in osteoclastogenesis and bone resorption. Notch receptors are activated following interactions with their ligands of the Jagged and Delta-like families. In the skeleton, Notch signaling controls osteoclast differentiation and bone-resorbing activity either directly acting on osteoclast precursors, or indirectly acting on cells of the osteoblast lineage and cells of the immune system. NOTCH1 inhibits osteoclastogenesis, whereas NOTCH2 enhances osteoclast differentiation and function by direct and indirect mechanisms. NOTCH3 induces the expression of RANKL in osteoblasts and osteocytes and as a result induces osteoclast differentiation. There is limited expression of NOTCH4 in skeletal cells. Selected congenital disorders and skeletal malignancies are associated with dysregulated Notch signaling and enhanced bone resorption. In conclusion, Notch signaling is a critical pathway that controls osteoblast and osteoclast differentiation and function and regulates skeletal homeostasis in health and disease.
机译:Notch1至4是在细胞分化和功能中起枢转作用的跨膜受体;该审查涉及陷波信号传导在骨溶骨细胞发生和骨吸收中的作用。在与锯齿状和δ样家族的配体相互作用后,凹口受体被激活。在骨架中,Notch信号传导控制骨壳分化和骨再吸收活性,即直接作用于破骨细胞前体,或间接作用于免疫系统的成骨细胞谱系和细胞的细胞。 Notch1抑制骨溶骨细胞发生,而Notch2通过直接和间接机制增强了骨质体分化和功能。 NOTCH3诱导骨细胞和骨细胞中RANK1的表达,结果诱导骨细胞分化。骨骼细胞中Notch4的表达有限。所选的先天性疾病和骨骼恶性肿瘤与具有失调的凹口信号传导和增强的骨吸收有关。总之,Notch信号传导是一种治疗成骨细胞和破骨细胞分化和功能的关键途径,并调节健康和疾病的骨骼稳态。

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