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运动终板病小鼠T淋巴细胞功能受损。

Impairment of T lymphocyte functions in mice with motor end-plate disease.

作者信息

Papiernik M, Rieger F, Ezine S, Pincon-Raymond M

出版信息

Clin Exp Immunol. 1982 May;48(2):429-36.

Abstract

The present paper reports complex immunological anomalies associated with motor end-plate disease (Med) in mice. Motor end-plate disease is a severe neuromuscular disorder which leads to death (around the 25th of life) in the Medj/Medj mutant, while the heterozygotes quickly recover from mild manifestations. Medj/Medj and Medj/ + mice share some of the immunological aberrations: reduced PFC response to SRBC in 14-16 day old mice, with reduced suppressor cell function and precocious maturation of the cytotoxic response to allogeneic cells in 21-23 day old mice. The diminished PFC response is corrected in adult Medj/ + mice but persists in the small group of Medj/Medj which escape death and which were studied between the 6th and 16th week of life. In addition, the thymus and spleen of Medj/Medj mice are greatly reduced in size, a symptom which appears with the onset of the clinical disease. Also, a reduction in the NK activity in the small group of older, surviving mice was noted. T and B lymphocyte proportions and the proliferative responses to T cell mitogens were not impaired in 14-16 day old mice. The role of these abnormalities in the pathogenesis of the disease is not known. Since some of these anomalies are shared by Medj/Medj and Medj/ +, the latter of which present no or mild and transient neurological manifestations, there is no clear link between the immunological and neuromuscular disorders.

摘要

本文报道了与小鼠运动终板疾病(Med)相关的复杂免疫异常。运动终板疾病是一种严重的神经肌肉疾病,在Medj/Medj突变体中会导致死亡(约在生命的第25天),而异合子则能从轻微症状中迅速恢复。Medj/Medj和Medj/+小鼠存在一些共同的免疫异常:14 - 16日龄小鼠对绵羊红细胞(SRBC)的PFC反应降低,21 - 23日龄小鼠抑制细胞功能降低,对异基因细胞的细胞毒性反应早熟。成年Medj/+小鼠中降低的PFC反应得到纠正,但在一小群逃脱死亡且在生命的第6至16周进行研究的Medj/Medj小鼠中持续存在。此外,Medj/Medj小鼠的胸腺和脾脏大小显著减小,这一症状在临床疾病发作时出现。另外,还注意到一小群存活的老年小鼠的自然杀伤(NK)活性降低。14 - 16日龄小鼠的T和B淋巴细胞比例以及对T细胞有丝分裂原的增殖反应未受损。这些异常在疾病发病机制中的作用尚不清楚。由于Medj/Medj和Medj/+存在一些共同的异常,而后者没有或仅有轻微且短暂的神经学表现,因此免疫和神经肌肉疾病之间没有明确的联系。

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