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Antagonist Anti-CD28 Therapeutics for the Treatment of Autoimmune Disorders

机译:拮抗剂抗CD28治疗自身免疫性疾病的疗法

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摘要

The effector functions of T lymphocytes are responsible for most autoimmune disorders and act by directly damaging tissues or by indirectly promoting inflammation and antibody responses. Co-stimulatory and co-inhibitory T cell receptor molecules are the primary pharmacological targets that enable interference with immune-mediated diseases. Among these, selective CD28 antagonists have drawn special interest, since they tip the co-stimulation/co-inhibition balance towards efficiently inhibiting effector T cells while promoting suppression by pre-existing regulatory T-cells. After having demonstrated outstanding therapeutic efficacy in multiple models of autoimmunity, inflammation and transplantation, and safety in phase-I studies in humans, selective CD28 antagonists are currently in early clinical development for the treatment of systemic lupus erythematous and rheumatoid arthritis. Here, we review the available proof of concept studies for CD28 antagonists in autoimmunity, with a special focus on the mechanisms of action.
机译:T淋巴细胞的效应子功能负责大多数自身免疫性疾病,并通过直接破坏组织或间接促进炎症和抗体反应发挥作用。共刺激和共抑制性T细胞受体分子是主要的药理靶标,能够干扰免疫介导的疾病。其中,选择性CD28拮抗剂引起了人们的特殊兴趣,因为它们使共刺激/共抑制平衡趋向于有效抑制效应T细胞,同时通过预先存在的调节性T细胞促进抑制。选择性CD28拮抗剂已在多种自身免疫,炎症和移植模型以及在人类I期研究中的安全性中显示出出色的治疗效果后,目前正在早期临床开发中,用于治疗系统性红斑狼疮和类风湿性关节炎。在这里,我们回顾了CD28拮抗剂在自身免疫中的可用概念验证研究,特别关注作用机理。

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