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Anti-CD3 and nasal proinsulin combination therapy enhances remission from recent-onset autoimmune diabetes by inducing Tregs

机译:抗CD3和鼻前胰岛素联合疗法可通过诱导Tregs增强近期发作的自身免疫性糖尿病的缓解

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摘要

Safe induction of autoantigen-specific long-term tolerance is the “holy grail” for the treatment of autoimmune diseases. In animal models of type 1 diabetes, oral or i.n. immunization with islet antigens induces Tregs that are capable of bystander suppression. However, such interventions are only effective early in the prediabetic phase. Here, we demonstrate that a novel combination treatment with anti-CD3ε–specific antibody and i.n. proinsulin peptide can reverse recent-onset diabetes in 2 murine diabetes models with much higher efficacy than with monotherapy with anti-CD3 or antigen alone. In vivo, expansion of CD25+Foxp3+ and insulin-specific Tregs producing IL-10, TGF-β, and IL-4 was strongly enhanced. These cells could transfer dominant tolerance to immunocompetent recent-onset diabetic recipients and suppressed heterologous autoaggressive CD8 responses. Thus, combining a systemic immune modulator with antigen-specific Treg induction is more efficacious in reverting diabetes. Since Tregs act site-specifically, this strategy should also be expected to reduce the potential for systemic side effects.
机译:安全诱导自身抗原特异性长期耐受性是治疗自身免疫性疾病的“圣杯”。在1型糖尿病的动物模型中,口服或i.n.用胰岛抗原免疫可诱导能够旁观者抑制的Treg。但是,此类干预仅在糖尿病前期的早期有效。在这里,我们证明了抗CD3ε特异性抗体和i.n.的新型联合治疗。与2种单独使用抗CD3或抗原的单一疗法相比,胰岛素原肽可以在2种鼠类糖尿病模型中逆转最近发作的糖尿病。在体内,CD25 + Foxp3 + 和胰岛素特异性Tregs产生IL-10,TGF-β和IL-4的扩增得到了强烈增强。这些细胞可以将主要的耐受性转移给具有免疫功能的新近发作的糖尿病受体,并抑制异源的自激性CD8反应。因此,将全身性免疫调节剂与抗原特异性Treg诱导相结合在逆转糖尿病方面更为有效。由于Treg的作用是针对特定部位的,因此也应期望采用这种策略来减少全身性副作用的可能性。

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