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LAG-3的七个谜团:一个日益复杂的多面免疫受体

Seven mysteries of LAG-3: a multi-faceted immune receptor of increasing complexity.

作者信息

Burnell Stephanie E A, Capitani Lorenzo, MacLachlan Bruce J, Mason Georgina H, Gallimore Awen M, Godkin Andrew

机构信息

Division of Infection and Immunity, Henry Wellcome Building, Cardiff University, Cardiff, UK.

Department of Gastroenterology and Hepatology, University Hospital of Wales, Heath Park, Cardiff, UK.

出版信息

Immunother Adv. 2021 Dec 20;2(1):ltab025. doi: 10.1093/immadv/ltab025. eCollection 2022.

Abstract

Despite three decades of research to its name and increasing interest in immunotherapies that target it, LAG-3 remains an elusive co-inhibitory receptor in comparison to the well-established PD-1 and CTLA-4. As such, LAG-3 targeting therapies have yet to achieve the clinical success of therapies targeting other checkpoints. This could, in part, be attributed to the many unanswered questions that remain regarding LAG-3 biology. Of these, we address: (i) the function of the many LAG-3-ligand interactions, (ii) the hurdles that remain to acquire a high-resolution structure of LAG-3, (iii) the under-studied LAG-3 signal transduction mechanism, (iv) the elusive soluble form of LAG-3, (v) the implications of the lack of (significant) phenotype of LAG-3 knockout mice, (vi) the reports of LAG-3 expression on the epithelium, and (vii) the conflicting reports of LAG-3 expression (and potential contributions to pathology) in the brain. These mysteries which surround LAG-3 highlight how the ever-evolving study of its biology continues to reveal ever-increasing complexity in its role as an immune receptor. Importantly, answering the questions which shroud LAG-3 in mystery will allow the maximum therapeutic benefit of LAG-3 targeting immunotherapies in cancer, autoimmunity and beyond.

摘要

尽管LAG-3已有三十年的研究历史,且针对它的免疫疗法越来越受到关注,但与已被充分了解的PD-1和CTLA-4相比,LAG-3仍然是一种难以捉摸的共抑制受体。因此,靶向LAG-3的疗法尚未取得靶向其他检查点的疗法那样的临床成功。这在一定程度上可能归因于关于LAG-3生物学仍有许多未解答的问题。在这些问题中,我们探讨:(i)众多LAG-3-配体相互作用的功能,(ii)获得LAG-3高分辨率结构仍存在的障碍,(iii)研究不足的LAG-3信号转导机制,(iv)难以捉摸的可溶性LAG-3形式,(v)LAG-3基因敲除小鼠缺乏(明显)表型的影响,(vi)关于LAG-3在上皮细胞上表达的报道,以及(vii)关于LAG-3在大脑中的表达(以及对病理学的潜在贡献)的相互矛盾的报道。围绕LAG-3的这些谜团凸显了对其生物学不断发展的研究如何持续揭示其作为免疫受体的作用中日益增加的复杂性。重要的是,解答笼罩LAG-3的谜团将使靶向LAG-3的免疫疗法在癌症、自身免疫及其他领域发挥最大的治疗效益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/92b2/9327114/8bfc780f05e0/ltab025_fig1.jpg

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