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利用半抗原修饰的自身抗原诱导自身免疫性MRL小鼠的免疫耐受和抑制。

The induction of tolerance and suppression in autoimmune MRL mice using hapten-modified self.

作者信息

Santoro T J, Scott D W, Pisetsky D S

出版信息

J Immunol. 1981 Aug;127(2):690-3.

PMID:7252156
Abstract

Disturbances in suppressor cell function have been considered important in the pathogenesis of systemic lupus erythematosus (SLE), a conclusion supported by studies with New Zealand mice. To determine whether other SLE mice display similar immunoregulatory defects, we investigated the susceptibility of autoimmune MRL mice to unresponsiveness induced by hapten-modified self (HMS). The response of splenocytes from MRL-lpr/lpr mice (lpr) was compared with those of sex- and age-matched, congenic MRL-+/+ mice (+/+), and H-2-identical (H-2k) CBA/J mice. Spleen cells (NSC) were cultured in vitro with hapten-modified syngeneic splenocytes (TNP-SC) and tested for responsiveness to TNP-LPS (for tolerance) or their ability to suppress the response of fresh cells. There was no difference in the susceptibility of lpr splenocytes from 3- and 10-mo-old mice to the induction of tolerance or suppression when compared with those from age-matched +/+ or CBA mice. To evaluate any quantitative defects in the responsiveness of lpr splenocytes to HMS, we modified the conditions under which suppressor activity was generated. Varying the ratio of NSC to TNP-SC from 10:1 to 2000:1, or changing the concentration of TNBS for haptenation from 10 mM to 0.5 mM per 10(8) spleen cells revealed no differences in the dose-response curves of lpr splenocytes for both tolerance and suppression when compared with those of the CBA. These results indicate that clinically affected MRL mice have intact suppressor cell activity in response to antigen-modified self and suggest a possible therapeutic role of this modality in inducing tolerance to self-antigens.

摘要

抑制细胞功能紊乱被认为在系统性红斑狼疮(SLE)的发病机制中起重要作用,这一结论得到了对新西兰小鼠研究的支持。为了确定其他SLE小鼠是否表现出类似的免疫调节缺陷,我们研究了自身免疫性MRL小鼠对半抗原修饰自身(HMS)诱导的无反应性的易感性。将MRL-lpr/lpr小鼠(lpr)的脾细胞反应与性别和年龄匹配的同基因MRL-+/+小鼠(+/+)以及H-2相同(H-2k)的CBA/J小鼠的脾细胞反应进行比较。脾细胞(NSC)在体外与半抗原修饰的同基因脾细胞(TNP-SC)一起培养,并测试其对TNP-LPS的反应性(用于耐受性)或其抑制新鲜细胞反应的能力。与年龄匹配的+/+或CBA小鼠相比,3个月和10个月大的lpr小鼠的脾细胞在诱导耐受性或抑制方面的易感性没有差异。为了评估lpr脾细胞对HMS反应性的任何定量缺陷,我们改变了产生抑制活性的条件。将NSC与TNP-SC的比例从10:1变化到2000:1,或者将每10(8)个脾细胞用于半抗原化的TNBS浓度从10 mM变化到0.5 mM,结果显示与CBA相比,lpr脾细胞在耐受性和抑制方面的剂量反应曲线没有差异。这些结果表明,临床上受影响的MRL小鼠在对半抗原修饰自身的反应中具有完整的抑制细胞活性,并提示这种方式在诱导对自身抗原的耐受性方面可能具有治疗作用。

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