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对III型肺炎球菌多糖抗体应答的调节。V. 影响噬斑形成细胞应答强度的因素的个体发生

Regulation of the antibody response to type III pneumococcal polysaccharide. V. Ontogeny of factors influencing the magnitude of the plaque-forming cell response.

作者信息

Morse H C, Prescott B, Cross S S, Stashak P W, Baker P J

出版信息

J Immunol. 1976 Feb;116(2):279-87.

PMID:2633
Abstract

Mice of different ages were evaluated with respect to their ability to give a plaque-forming cell (PFC) response to Type III pneumococcal polysaccharide (SSSIII), as well as the degree of amplifier and suppressor thymus-derived(T) cell activity present. Although the magnitude of the PFC response to an optimally immunogenic dose of SSS-III for 2-and 3-week old mice was only 7% and 14%, respectively, of that produced by adult (8-week old) mice, values comparable to those of adult animals were attained by 4 weeks of age; no significant changes in the ability to respond to SSS-III occurred thereafter. Amplifier T cell activity, which was minimal at 2 to 4 weeks of age, matured slowly and did not reach a maximum until 8 to 10 weeks of age. By contrast, suppressor T cell activity appeared to be fully developed at least as early as 2 weeks of age; here, the inhibitory effects produced could by abrogated by depletion of T cells, indicating that the unresponsiveneness induced by such cells does not result in the depletion ot irreversible inactivation of B cells capable of responding to SSS-III. These findings suggest that the inhibitory effects of suppressor T cells are predominant in young mice and that such cells may play an important role in determining the ease with which unresponsiveness is induced in neonates, and in the prevention of autoimmune disease. Also, studies conducted with adult-thymectomized mice showed that both amplifier and suppressor T cells, once seeded to the periphery, are stable and do not depend upon the presence of intact thymus for the expression or renewal of their activity.

摘要

对不同年龄的小鼠进行了评估,观察它们对III型肺炎球菌多糖(SSSIII)产生空斑形成细胞(PFC)反应的能力,以及存在的放大和抑制性胸腺来源(T)细胞活性的程度。尽管2周龄和3周龄小鼠对最佳免疫原剂量的SSS-III的PFC反应强度分别仅为成年(8周龄)小鼠产生反应强度的7%和14%,但4周龄时达到了与成年动物相当的值;此后对SSS-III的反应能力没有显著变化。放大性T细胞活性在2至4周龄时最低,成熟缓慢,直到8至10周龄才达到最大值。相比之下,抑制性T细胞活性至少在2周龄时似乎就已完全发育;在此,通过T细胞耗竭可消除产生的抑制作用,这表明此类细胞诱导的无反应性不会导致能够对SSS-III作出反应的B细胞耗竭或不可逆失活。这些发现表明,抑制性T细胞的抑制作用在幼鼠中占主导地位,并且此类细胞可能在决定新生儿诱导无反应性的难易程度以及预防自身免疫性疾病方面发挥重要作用。此外,对成年去胸腺小鼠进行的研究表明,放大性和抑制性T细胞一旦植入外周,都是稳定的,其活性的表达或更新不依赖于完整胸腺的存在。

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