Department of Medicine, University of Colorado Denver, Aurora, CO, United States.
Department of Research, Rocky Mountain Regional Veteran Affairs (VA) Medical Center, Aurora, CO, United States.
Front Immunol. 2024 Jul 30;15:1422249. doi: 10.3389/fimmu.2024.1422249. eCollection 2024.
Decades of evidence positioned IL-1β as a master regulatory cytokine in acute and chronic inflammatory diseases. Approved biologics aimed at inhibiting IL-1 signaling have shown efficacy but variable safety. More recently, targeting NLRP3 activation, an upstream mediator of IL-1β, has garnered the most attention. Aberrant NLRP3 activation has been demonstrated to participate in the progression of several pathological conditions from neurogenerative diseases to cardio-metabolic syndromes and cancer. Pharmacological and genetic strategies aimed to limit NLRP3 function have proven effective in many preclinical models of diseases. These evidences have lead to a significant effort in the generation and clinical testing of small orally active molecules that can target NLRP3. In this report, we discuss different properties of these molecules with translational potential and describe the technologies currently available to screen NLRP3 targeting molecules highlighting advantages and limitations of each method.
几十年来的证据表明,IL-1β 是急性和慢性炎症性疾病的主要调节细胞因子。已批准的针对抑制 IL-1 信号的生物制剂已显示出疗效,但安全性存在差异。最近,靶向 NLRP3 激活(IL-1β 的上游介质)引起了最多的关注。已经证明,异常的 NLRP3 激活参与了从神经退行性疾病到心血管代谢综合征和癌症等多种病理状况的进展。旨在限制 NLRP3 功能的药理学和遗传学策略已被证明在许多疾病的临床前模型中有效。这些证据促使人们大力开发和临床测试能够靶向 NLRP3 的小分子口服药物。在本报告中,我们讨论了具有转化潜力的这些分子的不同特性,并描述了目前可用于筛选 NLRP3 靶向分子的技术,强调了每种方法的优点和局限性。
