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无自身抗原的调节性T细胞疫苗接种可预防实验性自身免疫性脑脊髓炎。

Regulatory T cell vaccination without autoantigen protects against experimental autoimmune encephalomyelitis.

作者信息

Ochoa-Repáraz Javier, Riccardi Carol, Rynda Agnieszka, Jun Sangmu, Callis Gayle, Pascual David W

机构信息

Veterinary Molecular Biology, Montana State University, Bozeman, MT 59717, USA.

出版信息

J Immunol. 2007 Feb 1;178(3):1791-9. doi: 10.4049/jimmunol.178.3.1791.

Abstract

Regulatory T (T(reg)) cells show promise for treating autoimmune diseases, but their induction to elevated potency has been problematic when the most optimally derived cells are from diseased animals. To circumvent reliance on autoantigen-reactive T(reg) cells, stimulation to myelin-independent Ags may offer a viable alternative while maintaining potency to treat experimental autoimmune encephalomyelitis (EAE). The experimental Salmonella vaccine expressing colonization factor Ag I possesses anti-inflammatory properties and, when applied therapeutically, reduces further development of EAE in SJL mice. To ascertain T(reg) cell dependency, a kinetic analysis was performed showing increased levels of FoxP3(+)CD25(+)CD4(+) T cells. Inactivation of these T(reg) cells resulted in loss of protection. Adoptive transfer of the vaccine-induced T(reg) cells protected mice against EAE with greater potency than naive or Salmonella vector-induced T(reg) cells, and cytokine analysis revealed enhanced production of TGF-beta, not IL-10. The development of these T(reg) cells in conjunction with immune deviation by Th2 cells optimally induced protective T(reg) cells when compared those induced in the absence of Th2 cells. These data show that T(reg) cells can be induced to high potency to non-disease-inducing Ags using a bacterial vaccine.

摘要

调节性T(T(reg))细胞在治疗自身免疫性疾病方面显示出前景,但当最优化获得的细胞来自患病动物时,将它们诱导至更高效力一直存在问题。为了避免依赖自身抗原反应性T(reg)细胞,刺激与髓磷脂无关的抗原可能提供一种可行的替代方案,同时保持治疗实验性自身免疫性脑脊髓炎(EAE)的效力。表达定居因子抗原I的实验性沙门氏菌疫苗具有抗炎特性,当用于治疗时,可减少SJL小鼠中EAE的进一步发展。为了确定T(reg)细胞的依赖性,进行了动力学分析,结果显示FoxP3(+)CD25(+)CD4(+) T细胞水平增加。这些T(reg)细胞的失活导致保护作用丧失。疫苗诱导的T(reg)细胞的过继转移比未活化的或沙门氏菌载体诱导的T(reg)细胞更有效地保护小鼠免受EAE侵害,细胞因子分析显示TGF-β而非IL-10的产生增加。与在没有Th2细胞诱导的情况下相比,这些T(reg)细胞与Th2细胞诱导的免疫偏离共同发展可最佳地诱导保护性T(reg)细胞。这些数据表明,使用细菌疫苗可将T(reg)细胞诱导至高效力以针对非疾病诱导性抗原。

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