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退行性椎间盘疾病患者椎体终板的感觉和交感神经支配

Sensory and sympathetic innervation of the vertebral endplate in patients with degenerative disc disease.

作者信息

Brown M F, Hukkanen M V, McCarthy I D, Redfern D R, Batten J J, Crock H V, Hughes S P, Polak J M

机构信息

Department of Histochemistry, Royal Postgraduate Medical School, Hammersmith Hospital, London, UK.

出版信息

J Bone Joint Surg Br. 1997 Jan;79(1):147-53. doi: 10.1302/0301-620x.79b1.6814.

Abstract

We obtained intervertebral discs with cartilage endplates and underlying cancellous bone at operation from patients with degenerative disc disease and then used immunohistochemical techniques to localise the nerves and nerve endings in the specimens. We used antibodies for the ubiquitous neuronal protein gene product 9.5 (PGP 9.5). Immunoreactivity to neuropeptide Y was used to identify autonomic nerves and calcitonin gene-related peptide (CGRP) and substance P to identify sensory nerves. Blood vessels were identified by immunoreactivity with platelet-endothelial cell-adhesion molecule (CD31; PECAM). In a control group with no known history of chronic back pain, nerve fibres immunoreactive to PGP 9.5 and neuropeptide Y were most closely related to blood vessels, with occasional substance P and CGRP immunoreactivity. In patients with severe back pain and markedly reduced disc height, proliferation of blood vessels and accompanying nerve fibres was observed in the endplate region and underlying vertebral bodies. Many of these nerves were immunoreactive to substance P or CGRP, and in addition, substance P- and CGRP-immunoreactive nociceptors were seen unrelated to blood vessels. Quantification by image analysis showed a marked increase in CGRP-containing sensory nerve fibres compared with normal control subjects. We speculate that a chemotactic response to products of disc breakdown is responsible for the proliferation of vascularity and CGRP-containing sensory nerves found in the endplate region and vertebral body adjacent to degenerate discs. The neuropeptides substance P and CGRP have potent vasodilatory as well as pain-transmitting effects. The increase in sensory nerve endings suggests increase in blood flow, perhaps as an attempt to augment the nutrition of the degenerate disc. The increase in the density of sensory nerves, and the presence of endplate cartilage defects, strongly suggest that the endplates and vertebral bodies are sources of pain; this may explain the severe pain on movement experienced by some patients with degenerative disc disease.

摘要

我们在手术中从患有椎间盘退变疾病的患者身上获取了带有软骨终板及下方松质骨的椎间盘,然后采用免疫组织化学技术对标本中的神经及神经末梢进行定位。我们使用了针对普遍存在的神经元蛋白基因产物9.5(PGP 9.5)的抗体。利用对神经肽Y的免疫反应性来识别自主神经,利用降钙素基因相关肽(CGRP)和P物质来识别感觉神经。通过与血小板内皮细胞黏附分子(CD31;PECAM)的免疫反应性来识别血管。在无慢性背痛病史的对照组中,对PGP 9.5和神经肽Y呈免疫反应性的神经纤维与血管关系最为密切,偶尔可见对P物质和CGRP的免疫反应性。在患有严重背痛且椎间盘高度明显降低的患者中,在终板区域及下方椎体观察到血管及伴随神经纤维的增生。这些神经中有许多对P物质或CGRP呈免疫反应性,此外,还可见到与血管无关的对P物质和CGRP呈免疫反应性的伤害感受器。通过图像分析进行定量显示,与正常对照受试者相比,含CGRP的感觉神经纤维显著增加。我们推测,对椎间盘分解产物的趋化反应是导致退变椎间盘相邻终板区域和椎体中血管增生及含CGRP感觉神经增生的原因。神经肽P物质和CGRP具有强大的血管舒张以及疼痛传递作用。感觉神经末梢增多提示血流增加,这可能是为增加退变椎间盘营养的一种尝试。感觉神经密度增加以及终板软骨缺损的存在,强烈提示终板和椎体是疼痛来源;这或许可以解释一些椎间盘退变疾病患者运动时所经历的剧痛。

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