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在人类背根神经节中,营养不良性轴突肿胀随年龄和糖尿病而发展。

Dystrophic axonal swellings develop as a function of age and diabetes in human dorsal root ganglia.

作者信息

Schmidt R E, Dorsey D, Parvin C A, Beaudet L N, Plurad S B, Roth K A

机构信息

Department of Pathology, Washington University School of Medicine, St. Louis, MO 63110, USA.

出版信息

J Neuropathol Exp Neurol. 1997 Sep;56(9):1028-43. doi: 10.1097/00005072-199709000-00008.

Abstract

Neuroaxonal dystrophy, characterized by swollen axon terminals and, to a lesser degree, enlarged initial segments of axons or perikaryal projections, develops in human dorsal root sensory ganglia as a function of aging and diabetes. Lesions are typically located within the satellite cell capsule and are intimately applied to sensory neuronal perikarya, which are compressed and distorted but are otherwise normal. Swollen axons contain large numbers of neurofilaments that are immunoreactive with antisera to highly phosphorylated neurofilament epitopes but fail to stain with antisera directed against hypophosphorylated neurofilament epitopes. Other dystrophic swellings contain collections of tubulovesicular profiles admixed with neurotransmitter granules. Neuroaxonal dystrophy involves subpopulations of intraganglionic axons and apparent terminals, notably those containing CGRP, while apparently sparing others, including noradrenergic sympathetic axons. Diabetic subjects develop lesions prematurely and in greater numbers than in aged subjects. Individual dystrophic axons in diabetics and aged human subjects are identical in their light microscopic, immunohistochemical and ultrastructural appearance, suggesting the possibility of shared pathogenetic mechanisms.

摘要

神经轴突营养不良的特征是轴突终末肿胀,在较小程度上,轴突起始段或核周突起也会增大,它在人类背根神经节中随着年龄增长和糖尿病的发生而发展。病变通常位于卫星细胞囊内,并紧密贴附于感觉神经元的核周体,核周体虽被压缩和扭曲,但其他方面正常。肿胀的轴突含有大量与抗高磷酸化神经丝表位的抗血清发生免疫反应的神经丝,但不能被针对低磷酸化神经丝表位的抗血清染色。其他营养不良性肿胀含有与神经递质颗粒混合的微管泡状结构集合。神经轴突营养不良累及神经节内轴突和明显的终末的亚群,尤其是那些含有降钙素基因相关肽的亚群,而其他神经纤维,包括去甲肾上腺素能交感神经轴突则明显未受影响。糖尿病患者比老年患者更早且更大量地出现病变。糖尿病患者和老年人类受试者中的单个营养不良性轴突在光学显微镜、免疫组织化学和超微结构外观上是相同的,这表明存在共同致病机制的可能性。

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