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Regulatory T-cell, endogenous antigen and neonatal environment in the prevention and induction of autoimmune disease.

机译:调节性T细胞,内源性抗原和新生儿环境可预防和诱导自身免疫性疾病。

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Recent studies on autoimmune ovarian disease (AOD) induced by thymectomy on d3 (d3tx), and AOD induced by immunization with the ovary-specific zona pellucida 3 peptide (pZP3), have yielded the following results. First, female tolerance to pZP3 depends on the persistence of endogenous antigen (Ag). Second, following regulatory T-cell depletion, endogenous Ag in prepubertal d3tx mice triggers AOD and drives disease progression. Third, endogenous ZP3 from ovaries without AOD stimulates a diversified IgG autoantibody (autoAb) response that rapidly follows pZP3 T epitope immunization. Fourth, induction of AOD and autoimmune memory in neonatal female mice by pZP3 in incomplete Freund's adjuvant depends on endogenous Ag stimulation within the neonatal week. Fifth, in a rodent pinworm-positive environment, neonatal but not adult female mice injected with pZP3 in water develop Th2-mediated AOD and Th2 memory. Sixth, neonatal T cells transfer AOD to syngeneic athymic recipients, whereas adult T cells are non-pathogenic and in fact suppress AOD conferred by neonatal T cells. Therefore: 1) the continuous presence of physiologically-expressed autoAg is critical for both tolerance maintenance and autoimmune disease pathogenesis; the outcome is determined by the integrity of regulatory T cells; and 2) the neonatal mice, deficient in the regulatory T-cell function, are more responsive than adults to Ag and environmental stimuli that promote autoimmune disease and memory.
机译:胸腺切除术在d3(d3tx)上诱导的自身免疫性卵巢疾病(AOD)和卵巢特异性透明带3肽(pZP3)免疫诱导的AOD的最新研究产生了以下结果。首先,女性对pZP3的耐受性取决于内源性抗原(Ag)的持久性。其次,在调节性T细胞耗竭后,青春期前d3tx小鼠中的内源性Ag触发AOD并驱动疾病进展。第三,来自卵巢的没有AOD的内源性ZP3刺激了多样化的IgG自身抗体(autoAb)反应,该反应在pZP3 T表位免疫后迅速发生。第四,在不完全弗氏佐剂中通过pZP3诱导新生雌性小鼠的AOD和自身免疫记忆取决于新生周内的内源性Ag刺激。第五,在啮齿动物pin虫阳性环境中,新生但未成年雌性小鼠在水中注射pZP3会产生Th2介导的AOD和Th2记忆。第六,新生儿T细胞将AOD转移至同型无胸腺受体,而成年T细胞是非致病性的,实际上抑制了新生儿T细胞赋予的AOD。因此:1)生理表达的自身抗原的持续存在对于维持耐受性和自身免疫性疾病的发病机理都至关重要;结果取决于调节性T细胞的完整性; 2)缺乏调节性T细胞功能的新生小鼠比成年小鼠对促进自身免疫性疾病和记忆的Ag和环境刺激的反应更为敏感。

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