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环孢素A对实验性变态反应性神经炎的抑制作用

Suppression of experimental allergic neuritis by Cyclosporin-A.

作者信息

King R H, Craggs R I, Gross M L, Tompkins C, Thomas P K

出版信息

Acta Neuropathol. 1983;59(4):262-8. doi: 10.1007/BF00691491.

Abstract

Experimental allergic neuritis (EAN) was induced in guinea pigs and rats and treated with Cyclosporin-A (Cy-A). When Cy-A was given prophylactically for 1 month from the time of induction of the disease, it prevented the development of EAN during the course of its administration. When Cy-A was given therapeutically after the onset of neurological signs, it effectively prevented further deterioration. This effect was more marked after 3 weeks' treatment than after only 1 week's treatment. In both regimens, when dosing with Cy-A ceased there was a latent period before clinical signs of EAN developed. This latent period is similar to that seen in the development of EAN in normal control animals and is probably due to the continued presence of antigen at the injection sites. After primary treatment of EAN with Cy-A, animals that relapsed did not respond to further treatment with Cy-A. Histological examination revealed that the nature of the EAN lesions in both groups of animals given Cy-A were not as severe as those seen in control animals. Despite these observations, there was no statistically significant difference between the maximum clinical grades reached by animals in any one group. These experiments suggest that T-cells are important in the development of EAN and that Cy-A interferes with this process by suppressing T-helper cells. They also show that it is possible to influence favourably the course of immune mediated neurological disease.

摘要

在豚鼠和大鼠中诱发实验性变应性神经炎(EAN),并用环孢素A(Cy - A)进行治疗。从疾病诱发之时开始预防性给予Cy - A 1个月,在给药过程中它可预防EAN的发展。在神经症状出现后给予Cy - A进行治疗,它可有效防止病情进一步恶化。治疗3周后的效果比仅治疗1周更为显著。在这两种治疗方案中,停止给予Cy - A后,在EAN临床症状出现之前有一个潜伏期。这个潜伏期与正常对照动物中EAN发展过程中所见的潜伏期相似,可能是由于注射部位持续存在抗原。用Cy - A对EAN进行初次治疗后,复发的动物对再次给予Cy - A治疗无反应。组织学检查显示,两组给予Cy - A的动物中EAN病变的性质不如对照动物中所见的严重。尽管有这些观察结果,但任何一组动物达到的最大临床分级之间没有统计学上的显著差异。这些实验表明,T细胞在EAN的发展中起重要作用,并且Cy - A通过抑制辅助性T细胞来干扰这一过程。它们还表明,有可能对免疫介导的神经疾病的病程产生有利影响。

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