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靶向整合素途径:机制与治疗进展。

Targeting integrin pathways: mechanisms and advances in therapy.

机构信息

Department of Pharmacy, Peking University First Hospital, Xishiku Street, Xicheng District, 100034, Beijing, China.

Institute of Clinical Pharmacology, Peking University First Hospital, Xueyuan Road 38, Haidian District, 100191, Beijing, China.

出版信息

Signal Transduct Target Ther. 2023 Jan 2;8(1):1. doi: 10.1038/s41392-022-01259-6.

DOI:10.1038/s41392-022-01259-6
PMID:36588107
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9805914/
Abstract

Integrins are considered the main cell-adhesion transmembrane receptors that play multifaceted roles as extracellular matrix (ECM)-cytoskeletal linkers and transducers in biochemical and mechanical signals between cells and their environment in a wide range of states in health and diseases. Integrin functions are dependable on a delicate balance between active and inactive status via multiple mechanisms, including protein-protein interactions, conformational changes, and trafficking. Due to their exposure on the cell surface and sensitivity to the molecular blockade, integrins have been investigated as pharmacological targets for nearly 40 years, but given the complexity of integrins and sometimes opposite characteristics, targeting integrin therapeutics has been a challenge. To date, only seven drugs targeting integrins have been successfully marketed, including abciximab, eptifibatide, tirofiban, natalizumab, vedolizumab, lifitegrast, and carotegrast. Currently, there are approximately 90 kinds of integrin-based therapeutic drugs or imaging agents in clinical studies, including small molecules, antibodies, synthetic mimic peptides, antibody-drug conjugates (ADCs), chimeric antigen receptor (CAR) T-cell therapy, imaging agents, etc. A serious lesson from past integrin drug discovery and research efforts is that successes rely on both a deep understanding of integrin-regulatory mechanisms and unmet clinical needs. Herein, we provide a systematic and complete review of all integrin family members and integrin-mediated downstream signal transduction to highlight ongoing efforts to develop new therapies/diagnoses from bench to clinic. In addition, we further discuss the trend of drug development, how to improve the success rate of clinical trials targeting integrin therapies, and the key points for clinical research, basic research, and translational research.

摘要

整合素被认为是主要的细胞黏附跨膜受体,在健康和疾病的各种状态下,作为细胞外基质 (ECM)-细胞骨架连接物和细胞与其环境之间生化和机械信号的转导物,发挥着多方面的作用。整合素的功能依赖于通过多种机制(包括蛋白质-蛋白质相互作用、构象变化和运输)维持其活性和非活性状态之间的微妙平衡。由于其在细胞表面的暴露和对分子阻断的敏感性,整合素已被研究作为近 40 年的药理学靶点,但由于整合素的复杂性和有时相反的特征,靶向整合素治疗一直是一个挑战。迄今为止,只有七种靶向整合素的药物成功上市,包括阿昔单抗、依替巴肽、替罗非班、那他珠单抗、vedolizumab、利昔单抗和卡替格拉斯特。目前,大约有 90 种基于整合素的治疗药物或成像剂正在进行临床研究,包括小分子、抗体、合成模拟肽、抗体药物偶联物 (ADC)、嵌合抗原受体 (CAR) T 细胞疗法、成像剂等。从过去的整合素药物发现和研究工作中吸取的一个严重教训是,成功既依赖于对整合素调节机制的深刻理解,也依赖于未满足的临床需求。在此,我们对所有整合素家族成员和整合素介导的下游信号转导进行了系统而完整的综述,以强调从基础到临床开发新疗法/诊断的持续努力。此外,我们进一步讨论了药物开发的趋势、如何提高靶向整合素治疗的临床试验成功率以及临床研究、基础研究和转化研究的要点。

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