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P物质及其在骨代谢中的受体

Substance P and its receptors in bone metabolism.

作者信息

Liu Da, Jiang Lei-Sheng, Dai Li-Yang

机构信息

Shanghai Jiaotong University School of Medicine, Xinhua Hospital, Department of Orthopaedic Surgery, 1665 Kongjiang Road, Shanghai 200092, China.

出版信息

Neuropeptides. 2007 Oct;41(5):271-83. doi: 10.1016/j.npep.2007.05.003. Epub 2007 Jul 25.

Abstract

Accumulating evidence on bone physiopathology has indicated that the skeleton contains numerous nerve fibers and its metabolism is regulated by the nervous system. Until now, more than 10 neuropeptides have been identified in bone. Substance P (SP) is a neuropeptide released from axons of sensory neurons, belongs to the tachykinin family and plays important roles in many physiological and pathological processes by acting as a neurotransmitter, neuromodulator, or trophic factor. It activates signal transduction cascades by acting on the neurokinin-1 receptor (NK(1)-R). Previous studies have confirmed that the SP-immunoreactive (IR) axons innervate bone and adjacent tissues, and that their density varies depending on the regions and physiological or pathological conditions. Over the past few decades, it has been found that SP takes part in the stimulation of bone resorption, and its receptors have been demonstrated to be located in osteoclasts. Notably, in studies of skeletal ontogeny, SP-IR axons have been shown to appear at an early stage, mostly coinciding with the sequence of long bone mineralization. These findings, together with data obtained from chemically or surgically targeted nerve deletions, strongly suggest that SP is a potent regulator of skeletal physiology. The specific distribution of SP-IR nerve fibers, the different amount of SP within regions, and the various levels of expression of NK(1)-R in targeted cells presumably related to and participate in bone metabolism. It can be predicted that the indirect roles of SP through other cytokines are as important as its direct roles in bone metabolism. This new regulating pathway of bone metabolism would have enormous implications in skeletal physiology and the relevant research might present curative potentials to a spectrum of bone diseases.

摘要

越来越多关于骨生理病理学的证据表明,骨骼含有大量神经纤维,其代谢受神经系统调节。到目前为止,已在骨中鉴定出10多种神经肽。P物质(SP)是一种从感觉神经元轴突释放的神经肽,属于速激肽家族,通过作为神经递质、神经调质或营养因子在许多生理和病理过程中发挥重要作用。它通过作用于神经激肽-1受体(NK(1)-R)激活信号转导级联反应。先前的研究证实,SP免疫反应性(IR)轴突支配骨及相邻组织,其密度因区域和生理或病理状况而异。在过去几十年中,已发现SP参与刺激骨吸收,并且其受体已被证明位于破骨细胞中。值得注意的是,在骨骼个体发育研究中,SP-IR轴突已显示在早期出现,大多与长骨矿化顺序一致。这些发现,连同从化学或手术靶向神经缺失获得的数据,强烈表明SP是骨骼生理的有效调节因子。SP-IR神经纤维的特定分布、区域内SP的不同含量以及靶向细胞中NK(1)-R的不同表达水平可能与骨代谢相关并参与其中。可以预测,SP通过其他细胞因子的间接作用与其在骨代谢中的直接作用同样重要。这种新的骨代谢调节途径将对骨骼生理学产生巨大影响,相关研究可能为一系列骨疾病带来治疗潜力。

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