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Membrane Trafficking in Osteoblasts and Osteoclasts: New Avenues for Understanding and Treating Skeletal Diseases

机译:膜在成骨细胞和骨质体中的膜:用于理解和治疗骨骼疾病的新途径

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摘要

The endocytic and exocytic/secretory pathways are two major intracellular membrane trafficking routes that regulate numerous cellular functions in a variety of cell types. Osteoblasts and osteoclasts, two major bone cells responsible for bone remodeling and homeostasis, are no exceptions. During the past few years emerging evidence has pinpointed a critical role for endocytic and secretory pathways in osteoblast and osteoclast differentiation and function. The endosomal membrane provides a platform to integrate bone tropic signals of hormones and growth factors in osteoblasts. In osteoclasts, endocytosis, followed by transcytosis, of degraded bone matrix promotes bone resorption. Secretory pathways, especially lysosome secretion, not only participate in bone matrix deposition by osteoblasts and degradation of mineralized bone matrix by osteoclasts; they may also be involved in the coupling of bone resorption and bone formation during bone remodeling. More importantly, mutations in genes encoding regulatory factors within the endocytic and secretory pathways have been identified as causes for bone diseases. Identification of the molecular mechanisms of these genes in bone cells may provide new therapeutic targets for skeletal disorders.
机译:内吞途径和外吞途径/分泌途径是两种主要的细胞内膜运输途径,其调节多种细胞类型中的许多细胞功能。成骨细胞和破骨细胞是负责骨骼重塑和体内稳态的两个主要骨细胞,也不例外。在过去的几年中,越来越多的证据明确指出了内吞和分泌途径在成骨细胞和破骨细胞分化和功能中的关键作用。内体膜提供了整合成骨细胞中激素和生长因子的骨向信号的平台。在破骨细胞中,降解的骨基质的胞吞作用,然后是胞吞作用,会促进骨吸收。分泌途径,特别是溶酶体的分泌,不仅参与成骨细胞的骨基质沉积和破骨细胞对矿化的骨基质的降解;而且它们也可能参与骨重塑过程中骨吸收与骨形成的耦合。更重要的是,内吞和分泌途径中编码调节因子的基因突变已被确定为骨病的病因。鉴定骨细胞中这些基因的分子机制可能为骨骼疾病提供新的治疗靶标。

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