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Targeting CD28 to prevent transplant rejection

机译:靶向CD28以防止移植排斥

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Introduction: The pivotal role of costimulatory pathways in regulating T-cell activation versus tolerance has stimulated tremendous interest in their manipulation for therapeutic purposes. Of these, the CD28-B7 pathway is arguably the most important and best studied. Therapeutic targets of CD28 are currently used in the treatment of melanoma, autoimmune diseases and in transplantation. Areas covered: In this review, we summarize our current knowledge of CD28 and cytotoxic T-lymphocyte antigen-4 (CTLA-4) signaling, and review the current state and challenges of harnessing them to promote transplant tolerance. Expert opinion: Despite the success of belatacept, a first-in-class CTLA-4 fusion protein now clinically used in transplantation, it is apparent that we have only scratched the surface in understanding the complexities of how costimulatory pathways modulate the immune system. Our initial assumption that positive costimulators activate effector T cells and prevent tolerance, while negative costimulators inhibit effector T cells and promote tolerance, is clearly an oversimplified view. Indeed, belatacept is not only capable of blocking deleterious CD28-B7 interactions that promote effector T-cell responses but can also have undesired effects on tolerogenic regulatory T-cell populations.
机译:简介:共刺激途径在调节T细胞活化与耐受性中的关键作用激发了人们对其治疗目的的极大兴趣。其中,CD28-B7途径可以说是最重要和研究最好的途径。 CD28的治疗靶标目前用于治疗黑素瘤,自身免疫性疾病和移植。涵盖的领域:在本综述中,我们总结了我们对CD28和细胞毒性T淋巴细胞抗原4(CTLA-4)信号传导的当前了解,并综述了利用它们来提高移植耐受性的现状和挑战。专家意见:尽管现在已经临床上用于移植的一流CTLA-4融合蛋白belatacept取得了成功,但是很明显,我们只是在了解共刺激途径如何调节免疫系统的复杂性方面才摸到了水面。我们最初的假设是,积极的共刺激物激活效应T细胞并防止耐受,而消极的共刺激物抑制效应T细胞并促进耐受,这显然是一种过于简化的观点。实际上,贝拉西普不仅能够阻断促进效应T细胞反应的有害CD28-B7相互作用,而且还可以对致耐受性调节性T细胞群体产生不良影响。

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