血清素:一种新的骨量控制器可能对牙槽骨有影响。

Carlo Galli, Guido Macaluso, Giovanni Passeri
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引用次数: 27

摘要

由于最近的研究强调了控制骨转换的其他机制的重要性,可以设想新的治疗方法来治疗骨病和牙周炎引起的骨质流失。最近有研究表明,氟西汀和文拉法辛这两种血清素再摄取抑制剂通常被用作抗抑郁药,对大鼠牙周炎模型的骨质流失有积极或消极的影响。血清素是一种神经递质,可以在中枢神经系统的特定细胞核中发现,但也可以在肠道中产生并被隔离在血小板颗粒中。虽然已知它主要参与情绪、睡眠和肠道生理的控制,但最近的证据表明,作为Lrp5(一种通常与Wnt规范信号传导和成骨细胞分化相关的膜受体)作用的介质,它对骨代谢有深远的影响。在小鼠中,Lrp5的缺失导致色氨酸羟化酶1的表达增加,色氨酸羟化酶1是合成血清素所需的酶的肠道异构体,从而增加血清血清素水平。反过来,血清素可以与成骨细胞上的HTR1B受体结合,并通过激活PKA和CREB来阻止它们的增殖。尽管不同的研究小组对lrp5 - 5-羟色胺轴的存在和5-羟色胺在骨重塑中的作用的研究结果存在争议,但有令人信服的证据表明,5-羟色胺调节剂如SSRIs可以影响骨转换。因此,该药物家族对牙周生理的影响应深入探讨。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Serotonin: a novel bone mass controller may have implications for alveolar bone.

As recent studies highlight the importance of alternative mechanisms in the control of bone turnover, new therapeutic approaches can be envisaged for bone diseases and periodontitis-induced bone loss. Recently, it has been shown that Fluoxetine and Venlafaxine, serotonin re-uptake inhibitors commonly used as antidepressants, can positively or negatively affect bone loss in rat models of induced periodontitis. Serotonin is a neurotransmitter that can be found within specific nuclei of the central nervous system, but can also be produced in the gut and be sequestered inside platelet granules. Although it is known to be mainly involved in the control of mood, sleep, and intestinal physiology, recent evidence has pointed at far reaching effects on bone metabolism, as a mediator of the effects of Lrp5, a membrane receptor commonly associated with Wnt canonical signaling and osteoblast differentiation. Deletion of Lrp5 in mice lead to increased expression of Tryptophan Hydroxylase 1, the gut isoform of the enzyme required for serotonin synthesis, thus increasing serum levels of serotonin. Serotonin, in turn, could bind to HTR1B receptors on osteoblasts and stop their proliferation by activating PKA and CREB.Although different groups have reported controversial results on the existence of an Lrp5-serotonin axis and the action of serotonin in bone remodeling, there is convincing evidence that serotonin modulators such as SSRIs can affect bone turnover. Consequently, the effects of this drug family on periodontal physiology should be thoroughly explored.

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