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脂质体结合的人髓鞘碱性蛋白对豚鼠实验性变应性脑脊髓炎的抑制作用

Suppression of experimental allergic encephalomyelitis in guinea/pigs by liposome-associated human myelin basic protein.

作者信息

Strejan G H, Percy D H, St Louis J, Surlan D, Paty D W

出版信息

J Immunol. 1981 Nov;127(5):2064-9.

PMID:6170686
Abstract

Human myelin basic protein (MBP) was inserted into phosphatidyl-serine liposomes and Hartley guinea pigs were treated with 1 or 2 injections of MBP-liposomes mixture by the intracardial route before an encephalitogenic challenge with MBP in CFA. Other groups of guinea pigs were pretreated with equivalent amounts of MBP in saline or of MBP in IFA. Of 24 untreated animals, 22 developed EAE and died or had to be sacrificed within 15 days after challenge. Only 4 of 29 guinea pigs treated with either 75 microgram or 112 microgram MBP-liposomes developed clinical signs of the disease. In the group pretreated with MBP in saline, 11 of 15 animals died, whereas in the MBP-IFA group, only 4 out of 10 died. Histologic modifications were also decreased in the MBP-liposomes and MBP-IFA groups, but in many instances, clinical normal guinea pigs showed disseminated perivascular infiltrates in the brain and spinal cord. Delayed hypersensitivity reactions to MBP were positive in all but 1 animal tested. Early T-rosette levels followed essentially the clinical course of the disease: they were drastically decreased 7 days after challenge in the untreated and MBP-saline-treated groups, but remained essentially normal in the MBP-liposomes group throughout the experiment. Lymphocyte transformation tests carried out in parallel with soluble MBP and with MBP-liposomes indicated that animals in certain groups responded preferentially to 1 form or the other of the antigen. Compared with prevailing procedures, the single i.v. injection of a relatively small amount of liposome-associated MBP appears to represent a promising approach for the antigen-specific suppression of EAE.

摘要

将人髓鞘碱性蛋白(MBP)插入磷脂酰丝氨酸脂质体中,在经完全弗氏佐剂(CFA)中的MBP进行致脑炎性攻击之前,通过心内途径给Hartley豚鼠注射1次或2次MBP-脂质体混合物。其他豚鼠组用等量的盐水中的MBP或不完全弗氏佐剂(IFA)中的MBP进行预处理。在24只未处理的动物中,22只发生了实验性自身免疫性脑脊髓炎(EAE),并在攻击后15天内死亡或不得不被处死。在用75微克或112微克MBP-脂质体处理的29只豚鼠中,只有4只出现了该病的临床症状。在盐水中MBP预处理组中,15只动物中有11只死亡,而在MBP-IFA组中,10只中只有4只死亡。MBP-脂质体组和MBP-IFA组的组织学改变也有所减少,但在许多情况下,临床正常的豚鼠在脑和脊髓中显示出散在的血管周围浸润。除1只受试动物外,所有动物对MBP的迟发型超敏反应均为阳性。早期T花环水平基本上遵循疾病的临床进程:在未处理组和MBP-盐水处理组中,攻击后7天急剧下降,但在整个实验过程中,MBP-脂质体组基本保持正常。与可溶性MBP和MBP-脂质体同时进行的淋巴细胞转化试验表明,某些组的动物对一种或另一种形式的抗原优先作出反应。与现有方法相比,单次静脉注射相对少量的脂质体相关MBP似乎是一种有前景的抗原特异性抑制EAE的方法。

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