首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Organization of a unique net-like meshwork of CGRP+ sensory fibers in the mouse periosteum: implications for the generation and maintenance of bone fracture pain.
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Organization of a unique net-like meshwork of CGRP+ sensory fibers in the mouse periosteum: implications for the generation and maintenance of bone fracture pain.

机译:小鼠骨膜中CGRP +感觉纤维的独特网状网状组织:对骨折疼痛的产生和维持的影响。

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Although bone fracture frequently results in significant pain and can lead to increased morbidity and mortality, it is still not clearly understood how sensory neurons are organized to detect fracture pain. In the present report we focused on the periosteum, as this thin tissue is highly innervated and tightly adherent to the outer surface of bone. To define the organization and distribution of the sensory and sympathetic fibers in the mouse femoral periosteum, we used whole-mount preparations, transverse sections, immunofluoresence and laser scanning confocal microscopy. While both the outer fibrous layer and the inner more cellular cambium layer of the periosteum receive an extensive innervation by calcitonin gene-related peptide (CGRP) and 200-kDa neurofilament (NF200) positive sensory fibers as well as tyrosine hydroxylase (TH) positive sympathetic fibers, there is a differential organization of sensory vs. sympathetic fibers within the periosteum. In both layers, the great majority of TH+ fibers are closely associated with CD31+ blood vessels and wind around the larger vessels in a corkscrew pattern. In contrast, the majority of CGRP+ and NF200+ sensory fibers in both layers lack a clear association with CD31+ blood vessels and appear to be organized in a dense net-like meshwork to detect mechanical distortion of periosteum and bone. This organization would explain why stabilization/fixation causes a marked attenuation of movement-evoked fracture pain. Understanding the organization, plasticity and molecular characteristics of sensory and sympathetic nerve fibers innervating the skeleton may permit the development of novel mechanism-based therapies for treating non-malignant skeletal pain.
机译:尽管骨折经常导致严重的疼痛,并可能导致发病率和死亡率增加,但仍不清楚如何组织感觉神经元来检测骨折疼痛。在本报告中,我们将重点放在骨膜上,因为该薄组织高度被神经支配并紧密粘附于骨的外表面。为了定义小鼠股骨骨膜中感觉和交感纤维的组织和分布,我们使用了整装制剂,横切面,免疫荧光和激光扫描共聚焦显微镜。骨膜的外纤维层和内层细胞形成层都受到降钙素基因相关肽(CGRP)和200 kDa神经丝(NF200)阳性感觉纤维以及酪氨酸羟化酶(TH)阳性交感的广泛支配纤维,在骨膜内存在感觉纤维与交感纤维的不同组织。在这两层中,绝大多数TH +纤维与CD31 +血管紧密相关,并以开瓶器的形式缠绕在较大的血管周围。相比之下,这两层中的大多数CGRP +和NF200 +感觉纤维与CD31 +血管缺乏明确的联系,似乎组织成密集的网状网状结构,以检测骨膜和骨骼的机械变形。该组织将解释为什么稳定/固定会明显减轻运动诱发的骨折疼痛。理解支配骨骼的感觉神经和交感神经纤维的组织,可塑性和分子特征,可能允许开发新的基于机制的疗法来治疗非恶性骨骼痛。

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