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Immunoregulation of Experimental Allergic Encephalomyelitis: Conditions for Induction of Suppressor Cells and Analysis of Mechanism

机译:实验性变应性脑脊髓炎的免疫调节:抑制细胞诱导的条件和机制分析

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We determined requirements for the induction of immunoregulatory suppressor cells in experimental allergic encephalomyelitis (EAE) in Lewis rats. Pretreatment of rats with myelin basic protein (BP) in incomplete Freund's adjuvant (IFA) stimulates the proliferation of suppressor cells that localize in lymph nodes and spleen (but not thymus) and exert control over the development of clinical EAE. Dosage studies revealed that 3 × 107 suppressor cells can adoptively transfer suppression to syngeneic recipients. Transferred unresponsiveness wanes within 3 weeks, indicating that the suppressor cells are short-lived lymphocytes, although actively induced unresponsiveness persists for at least 8 weeks, probably as a result of continual proliferation under the influence of antigen. No evidence was obtained to suggest that antigen carry-over or blocking antibody production accounts for adoptive transfer of unresponsiveness. Suppressor cells apparently act at the inductive phase of the immune response since they had no inhibitory effect on adoptive transfer of disease by effector lymph node cells.Other mechanisms also may play a role in unresponsiveness to EAE, since rats pretreated i.v. with high dosages of soluble BP were temporarily rendered unresponsive, although suppressor cells could not be detected in these animals.
机译:我们确定了Lewis大鼠实验性变应性脑脊髓炎(EAE)中诱导免疫调节抑制细胞的要求。用不完全弗氏佐剂(IFA)中的髓鞘碱性蛋白(BP)预处理大鼠可刺激位于淋巴结和脾脏(而非胸腺)中的抑制细胞增殖,并控制临床EAE的发展。剂量研究表明,3×107抑制细胞可以过继转移抑制作用至同基因受体。转移的无反应性在3周内消失,表明抑制细胞是短命淋巴细胞,尽管主动诱导的无反应性持续至少8周,这可能是由于在抗原的影响下持续增殖的结果。没有证据表明抗原携带或阻断抗体的产生是导致无应答性的过继转移的原因。抑制细胞显然对免疫应答的诱导期起作用,因为它们对效应淋巴结细胞对疾病的过继转移没有抑制作用。由于大鼠在静脉内进行了预处理,其他机制也可能对EAE无反应。尽管在这些动物中未检测到抑制细胞,但高剂量的可溶性BP暂时没有反应。

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