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T cells osteoblasts and osteocytes: interacting lineages key for the bone anabolic and catabolic activities of parathyroid hormone

机译:T细胞成骨细胞和骨细胞:相互作用的谱系是甲状旁腺激素的骨合成代谢和分解代谢活动的关键

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摘要

Osteoimmunology is field of research dedicated to the study of the interactions between the immune system and bone. Among the cells of the immune system that regulate bone turnover and the responsiveness of bone cells to calciothropic hormones are bone marrow T lymphocytes. T cells secrete osteoclastogenic cytokines such as RANKL and TNF-α, as well as factors that stimulate bone formation, one of which is Wnt10b. In addition, T cells regulate the differentiation and life span of stromal cells and their responsiveness to parathyroid hormone (PTH) via costimulatory molecules expressed on their surface. The conditioning effect of T cells on stromal cells (SCs) is inherited by the osteoblastic and osteocytic progeny of SCs. As a result, osteoblastic cells of T cell–deficient mice have functional characteristics different from corresponding cells of T cell–replete mice. These differences include the ratio of RANKL/OPG produced in response to continuous PTH treatment, and the osteoblastogenic response to intermittent PTH treatment. This article reviews the evidence indicating that the effects of parathyroid hormone are mediated not only by osteoblasts and osteocytes but also by T cells.
机译:骨免疫学是致力于免疫系统和骨骼之间相互作用的研究领域。调节骨骼更新和骨骼细胞对钙人类激素反应的免疫系统细胞中有骨髓T淋巴细胞。 T细胞分泌破骨细胞因子,例如RANKL和TNF-α,以及刺激骨形成的因子,其中之一就是Wnt10b。此外,T细胞通过在其表面表达的共刺激分子来调节基质细胞的分化和寿命,以及它们对甲状旁腺激素(PTH)的反应能力。 T细胞对基质细胞(SCs)的调节作用是由SC的成骨细胞和成骨细胞后代继承的。结果,缺乏T细胞的小鼠的成骨细胞的功能特性不同于富含T细胞的小鼠的相应细胞。这些差异包括对连续PTH治疗产生的RANKL / OPG的比例,以及对PTH间歇治疗的成骨反应。本文回顾了证据,表明甲状旁腺激素的作用不仅由成骨细胞和骨细胞介导,而且还由T细胞介导。

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