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新冠疫情后时代的炎症衰老与免疫衰老:小分子,大挑战。

Inflammaging and Immunosenescence in the Post-COVID Era: Small Molecules, Big Challenges.

作者信息

Francavilla Fabio, Intranuovo Francesca, La Spada Gabriella, Lacivita Enza, Catto Marco, Graps Elisabetta Anna, Altomare Cosimo Damiano

机构信息

Department of Pharmacy-Pharmaceutical Sciences, University of Bari Aldo Moro, Via E. Orabona 4, 70125, Bari, Italy.

ARESS Puglia - Agenzia Regionale strategica per la Salute ed il Sociale, Lungomare Nazario Sauro 33, 70121, Bari, Italy.

出版信息

ChemMedChem. 2025 Mar 15;20(6):e202400672. doi: 10.1002/cmdc.202400672. Epub 2024 Dec 16.

DOI:10.1002/cmdc.202400672
PMID:39651728
Abstract

Aging naturally involves a decline in biological functions, often triggering a disequilibrium of physiological processes. A common outcome is the altered response exerted by the immune system to counteract infections, known as immunosenescence, which has been recognized as a primary cause, among others, of the so-called long-COVID syndrome. Moreover, the uncontrolled immunoreaction leads to a state of subacute, chronic inflammatory state known as inflammaging, responsible in turn for the chronicization of concomitant pathologies in a self-sustaining process. Anti-inflammatory and immunosuppressant drugs are the current choice for the therapy of inflammaging in post-COVID complications, with contrasting results. The increasing knowledge of the biochemical pathways of inflammaging led to disclose new small molecules-based therapies directed toward different biological targets involved in inflammation, immunological response, and oxidative stress. Herein, paying particular attention to recent clinical data and preclinical literature, we focus on the role of endocannabinoid system in inflammaging, and the promising therapeutic option represented by the CB2R agonists, the role of novel ligands of the formyl peptide receptor 2 and ultimately the potential of newly discovered monoamine oxidase (MAO) inhibitors with neuroprotective activity in the treatment of immunosenescence.

摘要

自然衰老涉及生物功能的衰退,常常引发生理过程的失衡。一个常见的结果是免疫系统对抗感染的反应发生改变,即免疫衰老,这已被认为是所谓的长新冠综合征的主要原因之一。此外,不受控制的免疫反应会导致一种亚急性、慢性炎症状态,即炎症衰老,而炎症衰老又会在一个自我维持的过程中导致伴随疾病的慢性化。抗炎和免疫抑制药物是目前治疗新冠后并发症中炎症衰老的选择,但结果不一。对炎症衰老生化途径的了解日益增加,促使人们发现了针对参与炎症、免疫反应和氧化应激的不同生物靶点的新型小分子疗法。在此,我们特别关注近期的临床数据和临床前文献,重点探讨内源性大麻素系统在炎症衰老中的作用,以及CB2R激动剂所代表的有前景的治疗选择、甲酰肽受体2新型配体的作用,以及最终新发现的具有神经保护活性的单胺氧化酶(MAO)抑制剂在治疗免疫衰老方面的潜力。

相似文献

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Inflammaging and Immunosenescence in the Post-COVID Era: Small Molecules, Big Challenges.新冠疫情后时代的炎症衰老与免疫衰老:小分子,大挑战。
ChemMedChem. 2025 Mar 15;20(6):e202400672. doi: 10.1002/cmdc.202400672. Epub 2024 Dec 16.
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Immunosenescence, Inflammaging and Resilience: An Evolutionary Perspective of Adaptation in the Light of COVID-19 Pandemic.免疫衰老、炎症衰老与韧性:COVID-19 大流行背景下适应的进化视角。
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Front Immunol. 2020 Aug 7;11:1748. doi: 10.3389/fimmu.2020.01748. eCollection 2020.

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