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成骨细胞介导白细胞介素1对大鼠破骨细胞骨吸收的刺激作用。

Osteoblasts mediate interleukin 1 stimulation of bone resorption by rat osteoclasts.

作者信息

Thomson B M, Saklatvala J, Chambers T J

出版信息

J Exp Med. 1986 Jul 1;164(1):104-12. doi: 10.1084/jem.164.1.104.

Abstract

A monocyte-derived factor with IL-1-like properties has recently been shown to cause resorption of bone in organ culture. We have investigated the action of IL-1 on disaggregated populations of osteoclasts, incubated alone or in the presence of osteoblastic cells, in an attempt to identify the target cell for IL-1 in bone, and to elucidate the mechanism by which IL-1 induces osteoclastic resorption. Osteoclasts were disaggregated from neonatal rat long bones and incubated on slices of human femoral cortical bone. Under these conditions, the majority of osteoclasts form distinctive excavations in the bone surface within 24 h, the volume of which can be quantified by computer-assisted morphometric and stereophotogrammetic techniques. IL-1 had no effect on bone resorption by osteoclasts alone, but when incubated in the presence of calvarial cells or cloned osteosarcoma cells, it induced a 3.8 (+/- 0.38)-fold increase in osteoclastic bone resorption, with significant enhancement at concentrations of greater than or equal to 30 pg/ml. The osteoblastic populations themselves did not resorb bone. The mechanism by which osteoblastic cells stimulate osteoclasts did not appear to depend upon PG synthesis; nor could we detect a diffusible substance in the medium of stimulated cocultures. These results indicate that IL-1 stimulates bone resorption through a primary action on osteoblasts, which are induced by IL-1 to transmit a short-range signal that stimulates osteoclastic bone resorption.

摘要

最近发现一种具有白细胞介素-1样特性的单核细胞衍生因子可在器官培养中引起骨吸收。我们研究了白细胞介素-1对破骨细胞离散群体的作用,这些破骨细胞单独培养或在成骨细胞存在的情况下培养,旨在确定骨中白细胞介素-1的靶细胞,并阐明白细胞介素-1诱导破骨细胞吸收的机制。破骨细胞从新生大鼠长骨中分离出来,接种于人股骨皮质骨切片上。在这些条件下,大多数破骨细胞在24小时内在骨表面形成独特的凹陷,其体积可通过计算机辅助形态计量学和立体摄影测量技术进行量化。白细胞介素-1单独对破骨细胞的骨吸收没有影响,但当在颅盖细胞或克隆的骨肉瘤细胞存在的情况下培养时,它可诱导破骨细胞骨吸收增加3.8(±0.38)倍,在浓度大于或等于30 pg/ml时显著增强。成骨细胞群体本身不会吸收骨。成骨细胞刺激破骨细胞的机制似乎不依赖于前列腺素合成;我们也未能在受刺激的共培养物培养基中检测到可扩散物质。这些结果表明,白细胞介素-1通过对成骨细胞的主要作用刺激骨吸收,成骨细胞被白细胞介素-1诱导传递一个短程信号,刺激破骨细胞骨吸收。

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