肝缺血再灌注损伤中的无菌炎症和细胞死亡途径：综述与展望。

IF 2

Endocrine, metabolic & immune disorders drug targets Pub Date : 2025-05-19 DOI:10.2174/0118715303401342250514102731

Weifan Huang, Wanting Meng, Jianan Zhao, Binbin Zhang

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引用次数: 0

摘要

背景：肝缺血再灌注损伤（IRI）是肝移植和肝切除术中的一个重要并发症，由损伤相关分子模式（DAMPs）介导的氧化应激和无菌炎症驱动。目前的治疗挑战来自相互关联的细胞死亡途径和冗余的炎症机制。目的：本综述综合了对IRI中DAMP信号传导和调节细胞死亡模式的机制见解，旨在确定翻译空白并提出精确靶向治疗。方法：使用关键词“IRI”、“DAMPs”和细胞死亡模式在PubMed中进行文献检索，无日期限制。包括同行评议的人类/动物模型研究，定性合成damp -细胞死亡相互作用。结果：缺血时，线粒体功能障碍释放HMGB1、ATP和mtDNA，激活Kupffer细胞TLR4/RAGE和cGAS-STING通路，触发NLRP3炎性小体驱动的细胞因子风暴。再灌注会放大ROS爆发、脂质过氧化和铁超载，形成一个自我维持的损伤循环。细胞死亡方式表现出时空特异性：肝细胞铁下垂在早期损伤中占主导地位，而巨噬细胞热下垂和坏死下垂在晚期脂肪变性肝中占主导地位。HMGB1乙酰化和mtDNA-cGAS信号是关键的调控因子。机器灌注（如低温氧灌注）通过线粒体复苏减少胆道并发症，优于传统的药物治疗。结论：由于IRI的复杂性，目前的单途径靶向治疗效果有限。未来的策略应该整合时间靶向(铁下垂抑制剂预再灌注；再灌注后焦亡阻滞剂)，damp中和剂（抗hmgb1抗体），以及结合多组学生物标志物和体外药物预处理的精确保存。解决脂肪肝的代谢脆弱性和完善细胞死亡特异性干预对于弥合翻译空白至关重要。

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Sterile Inflammation and Cell Death Pathways in Liver Ischemia-Reperfusion Injury: A Review and Perspective.

Background: Hepatic Ischemia-Reperfusion Injury (IRI) is a critical complication in liver transplantation and resection, driven by oxidative stress and sterile inflammation mediated by damage-associated molecular patterns (DAMPs). Current therapeutic challenges arise from interconnected cell death pathways and redundant inflammatory mechanisms.

Objective: This review synthesizes mechanistic insights into DAMP signaling and regulated cell death modalities in IRI, aiming to identify translational gaps and propose precision-targeted therapies.

Methods: A literature search in PubMed using keywords "IRI," "DAMPs," and cell death modes was conducted without date restrictions. Peer-reviewed studies on human/animal models were included, with qualitative synthesis of DAMP-cell death interactions.

Results: During ischemia, mitochondrial dysfunction releases HMGB1, ATP, and mtDNA, activating Kupffer cell TLR4/RAGE and cGAS-STING pathways, triggering NLRP3 inflammasome-- driven cytokine storms. Reperfusion amplifies ROS bursts, lipid peroxidation, and iron overload, creating a self-sustaining cycle of damage. Cell death modalities exhibit spatiotemporal specificity: hepatocyte ferroptosis dominates early injury, while macrophage pyroptosis and necroptosis predominate in steatotic livers during late phases. HMGB1 lactylation and mtDNA-cGAS signaling emerge as key regulators. Machine perfusion (e.g., hypothermic oxygenated perfusion) reduces biliary complications via mitochondrial resuscitation, outperforming conventional drugbased therapies.

Conclusion: Current single-pathway targeting shows limited efficacy due to IRI's complexity. Future strategies should integrate temporal targeting (ferroptosis inhibitors pre-reperfusion; pyroptosis blockers post-reperfusion), DAMP-neutralizing agents (anti-HMGB1 antibodies), and precision preservation combining multi-omics biomarkers with ex vivo pharmacological preconditioning. Addressing metabolic vulnerabilities in fatty livers and refining cell death-specific interventions are critical for bridging translational gaps.

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Endocrine, metabolic & immune disorders drug targets

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