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IgM记忆:蝾螈(绿红东美螈)中针对半抗原的长寿特异性记忆。

IgM memory: long lived hapten-specific memory in the newt, Notophthalmus viridescens.

作者信息

Ruben L N

出版信息

Immunology. 1983 Feb;48(2):385-92.

Abstract

While enhanced long lived secondary humoral immune responses to thymus-dependent (TD) immunogens are known to occur in mammals, they have yet to be characterized in extant ectothermic vertebrates which do not normally generate immunoglobulin isotype diversity. Moreover, examination of memory in such a vertebrate may provide insights into the controversial issue of IgM memory in mammalia. Trinitrophenyl (TNP) conjugated to horse erythrocytes (HRBC) and to lipopolysaccharide (LPS) have been used to study primitive long lived (5 months) memory in the newt, . The ability to recall TNP response memory was tested by secondary immunization with hapten conjugates of the same or a different carrier from the one used to initiate the primary response. All responses were monitored by immunocyto-adherence of pooled sensitized spleen cells. While carrier-specific priming was necessary to initiate primary anti-TNP responses when TD carriers (RBC) were used, it was not required when the more rapid secondary responses were tested. No enhanced anti-carrier responses were found. However, carrier-specific suppression of the secondary anti-hapten response was observed. Anamnesis which was both more rapid and intense developed only when TNP-LPS was used as the primary immunogen and anti-hapten memory was recalled with TNP-sheep erythrocytes (SRBC). Daily injections of Cyclosporin A from 1 day before reimmunization, affected the resultant primary (anti-SRBC) and secondary (anti-TNP) responses differentially. Colloidal carbon injection reduced the memory response by one-half. These results suggest that cellular regulatory controls may be involved in newt memory. However, no increase in TNP-specific antigen-binding cell affinity was found in comparisons of primary and secondary responses. Since reimmunization with TNP-LPS failed to produce enhanced responses following TNP-LPS priming, one can conclude that a thymus-independent (TI) carrier of the hapten will stimulate the generation of hapten-specific memory cells in the newt; however, their functional differentiation depends on collaborative events initiated by a TD carrier used to present the hapten.

摘要

虽然已知在哺乳动物中对胸腺依赖性(TD)免疫原会产生增强的长寿次级体液免疫反应,但在现存的通常不会产生免疫球蛋白同种型多样性的变温脊椎动物中,这些反应尚未得到表征。此外,研究这种脊椎动物的记忆可能会为哺乳动物中IgM记忆这一有争议的问题提供见解。与马红细胞(HRBC)和脂多糖(LPS)偶联的三硝基苯(TNP)已被用于研究蝾螈中原始的长寿(5个月)记忆。通过用与用于引发初次反应的载体相同或不同的载体的半抗原偶联物进行二次免疫来测试回忆TNP反应记忆的能力。所有反应均通过汇集的致敏脾细胞的免疫细胞粘附进行监测。当使用TD载体(RBC)时,载体特异性引发对于启动初次抗TNP反应是必要的,但在测试更快的二次反应时则不需要。未发现抗载体反应增强。然而,观察到了载体特异性对二次抗半抗原反应的抑制。仅当TNP-LPS用作初次免疫原且用TNP-绵羊红细胞(SRBC)回忆抗半抗原记忆时,才会出现更快且更强烈的回忆反应。从再次免疫前1天开始每天注射环孢素A,对产生的初次(抗SRBC)和二次(抗TNP)反应有不同影响。注射胶体碳使记忆反应降低了一半。这些结果表明细胞调节控制可能参与了蝾螈的记忆。然而,在初次和二次反应的比较中未发现TNP特异性抗原结合细胞亲和力增加。由于用TNP-LPS再次免疫在TNP-LPS引发后未能产生增强反应,因此可以得出结论,半抗原的胸腺非依赖性(TI)载体将刺激蝾螈中半抗原特异性记忆细胞的产生;然而,它们的功能分化取决于用于呈递半抗原的TD载体引发的协同事件。

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