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T细胞植入:抗髓鞘碱性蛋白T细胞系的新生期转移使Fischer大鼠在生命后期易被主动诱导发生实验性自身免疫性脑脊髓炎。

T-cell seeding: neonatal transfer of anti-myelin basic protein T-cell lines renders Fischer rats susceptible later in life to the active induction of experimental autoimmune encephalitis.

作者信息

Volovitz Ilan, Mor Felix, Machlenkin Arthur, Goldberger Ofir, Marmor Yotvat, Eisenbach Lea, Cohen Irun R

机构信息

Department of Immunology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Immunology. 2009 Sep;128(1):92-102. doi: 10.1111/j.1365-2567.2009.03074.x.

Abstract

Fischer strain rats resist active induction of experimental autoimmune encephalomyelitis (EAE) following immunization with guinea-pig myelin basic protein (MBP) in complete Freund's adjuvant (CFA). Nevertheless, we now report that an encephalitogenic CD4(+) anti-MBP T-cell line could be developed from actively immunized Fischer rats. Adoptive transfer of the activated line mediated acute EAE in adult Fischer rats, but not in 1-day-old rats. Moreover, we found that both resting and activated anti-MBP T cells injected 1 day post-natally rendered these rats susceptible later in life to the active induction of EAE by immunization with MBP/CFA. The actively induced EAE manifested the accelerated onset of a secondary, memory-type response. Resting anti-MBP T cells injected even up to 2 weeks post-natally produced no clinical signs but seeded 50-100% of the recipients for an active encephalitogenic immune response to MBP. An earlier T-cell injection (1-2 days) produced a higher incidence and stronger response. The transferred resting T cells entered the neonatal spleen and thymus and proliferated there but did not change the total anti-MBP precursor number in adults. Splenocytes harvested from rats that were injected neonatally but not exposed to MBP in vivo proliferated strongly and produced significant amounts of interferon-gamma to MBP in vitro. Similar results were observed in rats injected with resting T-cell lines reactive to ovalbumin, suggesting that the neonatal injection of resting T cells specific for a self or for a foreign antigen can seed the immune system with the potential for an enhanced effector response to that antigen later in life.

摘要

费舍尔品系大鼠在用豚鼠髓鞘碱性蛋白(MBP)于完全弗氏佐剂(CFA)中免疫后,能抵抗实验性自身免疫性脑脊髓炎(EAE)的主动诱导。然而,我们现在报告,可从主动免疫的费舍尔大鼠中培养出致脑炎性CD4(+)抗MBP T细胞系。活化细胞系的过继转移在成年费舍尔大鼠中介导了急性EAE,但在1日龄大鼠中则不然。此外,我们发现出生后1天注射的静止和活化抗MBP T细胞,使这些大鼠在生命后期对用MBP/CFA免疫主动诱导EAE变得易感。主动诱导的EAE表现出二次记忆型反应的加速发作。即使在出生后2周注射静止抗MBP T细胞也不会产生临床症状,但为50 - 100%的受体植入了针对MBP的主动致脑炎性免疫反应。更早的T细胞注射(1 - 2天)产生更高的发生率和更强的反应。转移的静止T细胞进入新生大鼠的脾脏和胸腺并在那里增殖,但未改变成年大鼠中总的抗MBP前体细胞数量。从未在体内接触过MBP但在出生时注射过的大鼠收获的脾细胞,在体外对MBP强烈增殖并产生大量干扰素 - γ。在用对卵清蛋白有反应的静止T细胞系注射的大鼠中观察到类似结果,这表明出生时注射针对自身或外来抗原的静止T细胞,可在免疫系统中植入在生命后期对该抗原增强效应反应的潜力。

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