Signaling pathways involved in the biological functions of dendritic cells and their implications for disease treatment.

IF 6.3 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular biomedicine Pub Date : 2023-05-15 DOI:10.1186/s43556-023-00125-3
Hao Cheng, Wenjing Chen, Yubin Lin, Jianan Zhang, Xiaoshuang Song, Dunfang Zhang
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Abstract

The ability of dendritic cells (DCs) to initiate and regulate adaptive immune responses is fundamental for maintaining immune homeostasis upon exposure to self or foreign antigens. The immune regulatory function of DCs is strictly controlled by their distribution as well as by cytokines, chemokines, and transcriptional programming. These factors work in conjunction to determine whether DCs exert an immunosuppressive or immune-activating function. Therefore, understanding the molecular signals involved in DC-dependent immunoregulation is crucial in providing insight into the generation of organismal immunity and revealing potential clinical applications of DCs. Considering the many breakthroughs in DC research in recent years, in this review we focused on three basic lines of research directly related to the biological functions of DCs and summarized new immunotherapeutic strategies involving DCs. First, we reviewed recent findings on DC subsets and identified lineage-restricted transcription factors that guide the development of different DC subsets. Second, we discussed the recognition and processing of antigens by DCs through pattern recognition receptors, endogenous/exogenous pathways, and the presentation of antigens through peptide/major histocompatibility complexes. Third, we reviewed how interactions between DCs and T cells coordinate immune homeostasis in vivo via multiple pathways. Finally, we summarized the application of DC-based immunotherapy for autoimmune diseases and tumors and highlighted potential research prospects for immunotherapy that targets DCs. This review provides a useful resource to better understand the immunomodulatory signals involved in different subsets of DCs and the manipulation of these immune signals can facilitate DC-based immunotherapy.

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参与树突状细胞生物学功能的信号通路及其对疾病治疗的意义。
树突状细胞(dc)启动和调节适应性免疫反应的能力是在暴露于自身或外来抗原时维持免疫稳态的基础。dc的免疫调节功能受其分布以及细胞因子、趋化因子和转录编程的严格控制。这些因素共同决定dc是否发挥免疫抑制或免疫激活功能。因此,了解dc依赖性免疫调节中涉及的分子信号对于了解机体免疫的产生和揭示dc的潜在临床应用至关重要。鉴于近年来DC研究取得的诸多突破,本文重点介绍了与DC生物学功能直接相关的三个基本研究方向,并总结了涉及DC的新的免疫治疗策略。首先,我们回顾了最近关于DC亚群的研究结果,并确定了指导不同DC亚群发展的谱系限制性转录因子。其次,我们讨论了dc通过模式识别受体对抗原的识别和加工,内源性/外源性途径,以及抗原通过肽/主要组织相容性复合物的递呈。第三,我们回顾了dc和T细胞之间的相互作用如何通过多种途径协调体内的免疫稳态。最后,我们总结了基于dc的免疫治疗在自身免疫性疾病和肿瘤中的应用,并强调了针对dc的免疫治疗的潜在研究前景。这一综述为更好地了解不同dc亚群的免疫调节信号以及对这些免疫信号的操纵可以促进dc免疫治疗提供了有用的资源。
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CiteScore
6.30
自引率
0.00%
发文量
0
审稿时长
10 weeks
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