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关于人及牛少突胶质细胞纯化制剂致脑炎性作用的研究。

Studies on the encephalitogenic effects of purified preparations of human and bovine oligodendrocytes.

作者信息

Raine C S, Wiśniewski H M, Iqbal K, Grundkeiqbal I, Norton W T

出版信息

Brain Res. 1977 Jan 21;120(2):269-86. doi: 10.1016/0006-8993(77)90906-4.

Abstract

Bulk-isolated human and bovine oligodendroglia, practically free from myelin, have been used in attempts to elicit an autoimmune response which has been compared with acute experimental allergic encephalomyelitis (EAE). For these experiments, a total of 20 Hartley guinea pigs, 33 Lewis rats and 16 rabbits have been studied. Animals were inoculated with a range of doses of purified preparations of both human and bovine oligodendroglial cells in complete Freund's adjuvant (CFA) and compared with others challenged with whole white matter in CFA. The latter animals all developed clinical and histological signs of experimental allergic encephalomyelitis (EAE) 2-3 weeks post-inoculation. In general, oligodendroglial cells were encephalitogenically less potent than white matter. Guinea pigs were the most susceptible to inoculations of oligodendroglia. In several given human oligodendroglia 14 days earlier, a paraparesis indistinguishable from conventional EAE was seen. Animals receiving bovine cells showed no clinical signs. Histologically, the CNS of afflicted guinea pigs displayed severe inflammation but, in contrast to conventional EAE in the same species, demyelination was rare in the small group of animals tested. After sensitization with oligodendroglia, rats displayed no clinical disease. Histologically, some given human cells had positive evidence of disease while bovine cells in others gave a mild response. Rabbits showed no clinical and very little histological disease. Although more extensive studies are needed to confirm the findings, from the animals studied it appears that (1) variation in response to inocula containing oligodendroglia exists among the species tested, (2) that human oligodendroglia are more potent immunologically than bovine cells, (3) that CNS lesions produced by these cells in guinea pigs, lack a strong demyelinative component and (4) a specific antigen might exist in oligodendrocytes which is distinct from myelin basic protein. The possible reasons underlying our findings are discussed.

摘要

大量分离得到的、几乎不含髓磷脂的人及牛少突胶质细胞,已被用于引发自身免疫反应,并与急性实验性过敏性脑脊髓炎(EAE)进行比较。在这些实验中,共研究了20只哈特利豚鼠、33只刘易斯大鼠和16只兔子。给动物接种了一系列剂量的纯化的人及牛少突胶质细胞制剂,佐剂为完全弗氏佐剂(CFA),并与用CFA中的全白质攻击的其他动物进行比较。后一组动物在接种后2 - 3周均出现了实验性过敏性脑脊髓炎(EAE)的临床和组织学体征。一般来说,少突胶质细胞的致脑炎能力比白质弱。豚鼠对接种少突胶质细胞最敏感。在14天前接种几种给定的人少突胶质细胞后,出现了与传统EAE难以区分的轻瘫。接受牛细胞的动物未表现出临床体征。组织学上,患病豚鼠的中枢神经系统显示出严重炎症,但与同一物种的传统EAE不同的是,在测试的一小群动物中脱髓鞘很少见。用少突胶质细胞致敏后,大鼠未出现临床疾病。组织学上,一些给定的人细胞有疾病的阳性证据,而其他动物中的牛细胞反应轻微。兔子未出现临床疾病,组织学疾病也很少。尽管需要更广泛的研究来证实这些发现,但从所研究的动物来看,似乎(1)在所测试的物种中,对接种含少突胶质细胞制剂的反应存在差异,(2)人少突胶质细胞在免疫方面比牛细胞更具效力,(3)这些细胞在豚鼠中产生的中枢神经系统病变缺乏强烈的脱髓鞘成分,(4)少突胶质细胞中可能存在一种与髓磷脂碱性蛋白不同的特异性抗原。讨论了我们研究结果背后的可能原因。

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