[正常和脱垂二尖瓣的神经支配]。

Journal of cardiology. Supplement Pub Date : 1989-01-01
T Kawano, T Oki, T Uchida, A Iuchi, S Ogawa, M Hayashi, N Fukuda, H Mori, K Ii, K Hizawa
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引用次数: 0

摘要

为了评估二尖瓣脱垂(MVP)与自主神经功能障碍的关系,我们进行了临床和免疫组织化学研究。1 .临床研究对60例MVP患者(35岁以下41例,35岁及以上19例)进行自主神经功能测试和仰卧自行车运动,并与正常对照31例,35岁以下19例,35岁及以上12例进行比较。体位应激和冷压试验阳性反应的病例在两组MVP中均高于对照组。在运动过程中,MVP组的血浆无肾上腺素水平高于对照组。我们的临床观察表明,自主神经功能障碍,特别是交感神经过度活跃,可能存在于MVP,而与年龄无关。2免疫组化检测23个二尖瓣(正常对照组15个,MVP 8个)、3个正常三尖瓣、3个正常主动脉瓣和3个正常肺动脉瓣,检测S-100蛋白、胶质纤维酸性蛋白(GFAP)和神经丝蛋白(NFP)的免疫组化定位,检测所有神经末梢的分布,检测胆碱乙酰转移酶(ChAT)的免疫组化定位,检测胆碱能神经纤维的分布。以及神经肽Y (NPY)和降钙素基因相关肽(CGRP)检测传入神经纤维的分布,采用亲和素-生物素过氧化物酶复合物(ABC)法。用乙醛酸法荧光检测肾上腺素能神经纤维的分布。在正常瓣膜中,S-100蛋白主要存在于瓣尖基部和瓣尖体。它在尖端非常稀少,仅在配合区即心房层或沿心房与房室瓣海绵状膜的边界处发现。S-100蛋白在脱垂二尖瓣中的分布与正常二尖瓣相同,只是退化部分缺乏S-100蛋白。GFAP、NFP、ChAT、NPY、CGRP和肾上腺素能荧光在正常和脱垂二尖瓣中的分布与S-100蛋白相同。提示上述神经在二尖瓣内的解剖分布与二尖瓣脱垂情况下自主神经系统功能障碍密切相关,因为二尖瓣体内有丰富的神经末梢,该区域最容易因适应异常而受到机械刺激的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[Innervation of the mitral valve in normal and prolapsed mitral valves].

To evaluate the relationship between mitral valve prolapse (MVP) and autonomic nerve dysfunction, clinical and immunohistochemical studies were performed. I. Clinical study Autonomic function tests and supine bicycle exercise were performed in 60 patients with MVP, 41 under 35 years of age and 19 of 35 years and older, and the results were compared with those of 31 normal controls, 19 under 35 years of age and 12 of 35 years and older. Case with positive response on postural stress and cold pressor tests were more frequent in both MVP groups than those of controls. Plasma nor-adrenaline levels were higher in the MVP groups than in the control groups during exercise. Our clinical observation suggested that autonomic dysfunction, particularly sympathetic hyperactivity, probably is present in MVP irrespective of age. II. Immunohistochemical study In 23 mitral valves (15 of normal controls and eight of MVP), three normal tricuspid, three normal aortic and three normal pulmonic valves, immunohistochemical localizations of S-100 protein, glial fibrillary acidic protein (GFAP) and neurofilament protein (NFP) were examined to detect the distribution of all nerve endings, choline acetyltransferase (ChAT) to detect the distribution of cholinergic nerve fibers, and neuropeptide Y (NPY) and calcitonin gene related peptide (CGRP) to detect the distribution of afferent nerve fibers, using the avidin-biotin peroxidase complex (ABC) method. The distribution of adrenergic nerve fibers was examined by fluorescence with the glyoxylic acid method. In normal valves, S-100 protein was mainly demonstrated in the base and body of the valve cusp. It was very scanty in the tip, and was only found in the coaptation zone that is, the layer of the atrialis or along the boundary between the atrialis and the spongiosa in the atrioventricular valves. The distribution of S-100 protein in the prolapsed mitral valve was the same as that of the normal valve except for the lack of S-100 protein in the degenerated portion. The distribution of GFAP, NFP, ChAT, NPY, CGRP and adrenergic fluorescence were the same as that of S-100 protein in both the normal and prolapsed mitral valves. It is suggested that the above-mentioned anatomical distribution of the nerve in the mitral valve is closely related to the dysfunction of the autonomic nerve system in the condition of mitral valve prolapse, because the body of the mitral valve is rich in nerve endings and this area is most easily influenced by the mechanical stimulation due to abnormal coaptation.

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