重新利用有害抗体表位作为败血症和类风湿关节炎的靶向治疗。

IF 22.9 2区医学 Q1 MEDICINE, GENERAL & INTERNAL

Military Medical Research Pub Date : 2026-02-17 eCollection Date: 2025-01-01 DOI:10.1186/s40779-026-00686-8

Wei-Qiang Chen, Li Lou, Xiao-Ling Qiang, Cassie Shu Zhu, Jian-Hua Li, Shu-Jin Chen, Brian Xiong, Huan Yang, Ping Wang, Kevin J Tracey, Hai-Chao Wang

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引用次数: 0

摘要

背景：脓毒症和类风湿关节炎（RA）是两种不同但机制相关的疾病，通常由炎症反应失调驱动。在这里，我们探索了一个违反直觉的假设，即来自有害的抗四联蛋白（TN）抗体（mAb9）的表位可能具有不可预见的治疗潜力。方法：通过将mAb9的表位定位到P2（残基55-70），这是TN保护功能的关键区域，我们开发了P2-1，一种水溶性衍生物作为靶向治疗。然后，我们采用脓毒症（盲肠结扎和穿刺）和关节炎（胶原抗体诱导的关节炎）的动物模型，通过评估脓毒症存活率、关节炎严重程度、疼痛敏感性和关节组织组织学来评估P2、P2-1和原肝蛋白酶L （pCTS-L）中和抗体的治疗效果。同时，我们利用表面等离子体共振（SPR）实验和计算模型来研究P2-1/高迁移率组盒1 （HMGB1）相互作用。最后，我们利用原代人外周血单核细胞（PBMCs）阐明了P2-1对hmgb1诱导的pCTS-L和其他细胞因子和趋化因子释放的影响。结果：在脓毒症模型中，P2-1显著提高了生存率，减少了全身炎症，在RA模型中，即使在发病后给予治疗，也能减轻关节炎的严重程度和疼痛敏感性。在机制上，P2-1表现出与HMGB1的高亲和力结合，并选择性地抑制HMGB1诱导的组织蛋白酶L (Ctsl) mRNA上调和人免疫细胞pCTS-L分泌，关键是不干扰HMGB1诱导的其他细胞因子和趋化因子。我们进一步验证了pCTS-L作为治疗靶点，证明了中和抗体具有有效的抗关节炎作用，减少关节炎症、疼痛和结构损伤。结论：我们的研究结果引入了一种范式转换的药物发现策略，将有害抗体作用的见解转化为针对HMGB1-pCTS-L轴的靶向治疗。该方法不仅将P2-1作为一种有效的治疗方法，而且还确立了pCTS-L作为炎症性疾病（如败血症和RA）的重要介质。补充信息：在线版本包含补充资料，下载地址：10.1186/s40779-026-00686-8。

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Repurposing a detrimental antibody epitope as targeted therapeutics for sepsis and rheumatoid arthritis.

Background: Sepsis and rheumatoid arthritis (RA) are distinct yet mechanistically related conditions commonly driven by dysregulated inflammatory responses. Here, we explored the counterintuitive hypothesis that an epitope from a deleterious anti-tetranectin (TN) antibody (mAb9) could hold unforeseen therapeutic potential.

Methods: By mapping mAb9's epitope to P2 (residues 55-70), a region crucial for TN's protective functions, we developed P2-1, a water-soluble derivative as a targeted therapy. We then employed animal models of sepsis (cecal ligation and puncture) and arthritis (collagen antibody-induced arthritis) to evaluate the therapeutic effects of P2, P2-1, and a procathepsin L (pCTS-L)-neutralizing antibody by assessing septic survival, arthritis severity, pain sensitivity, and joint tissue histology. In parallel, we utilized a surface plasmon resonance (SPR) assay and computational modeling to examine the P2-1/high mobility group box 1 (HMGB1) interaction. Finally, we elucidate the effect of P2-1 on the HMGB1-induced release of pCTS-L and other cytokines and chemokines using primary human peripheral blood mononuclear cells (PBMCs).

Results: P2-1 significantly improved survival and reduced systemic inflammation in a sepsis model, and attenuated arthritis severity and pain sensitivity in an RA model, even with therapeutic administration after disease onset. Mechanistically, P2-1 exhibited high-affinity binding to HMGB1 and selectively suppressed HMGB1-induced cathepsin L (Ctsl) mRNA upregulation and pCTS-L secretion from human immune cells, crucially without perturbing other HMGB1-induced cytokines and chemokines. We further validated pCTS-L as a therapeutic target by demonstrating that a neutralizing antibody conferred potent antiarthritic effects, reducing joint inflammation, pain, and structural damage.

Conclusions: Our findings introduce a paradigm-shifting drug discovery strategy that transforms insights from harmful antibody action into targeted therapeutics for the HMGB1-pCTS-L axis. This approach not only delivers P2-1 as a potent therapy but also establishes pCTS-L as a crucial mediator in inflammatory diseases such as sepsis and RA.

Supplementary information: The online version contains supplementary material available at 10.1186/s40779-026-00686-8.

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来源期刊

Military Medical Research Medicine-General Medicine

CiteScore

38.40

自引率

2.80%

发文量

485

审稿时长

8 weeks

期刊介绍： Military Medical Research is an open-access, peer-reviewed journal that aims to share the most up-to-date evidence and innovative discoveries in a wide range of fields, including basic and clinical sciences, translational research, precision medicine, emerging interdisciplinary subjects, and advanced technologies. Our primary focus is on modern military medicine; however, we also encourage submissions from other related areas. This includes, but is not limited to, basic medical research with the potential for translation into practice, as well as clinical research that could impact medical care both in times of warfare and during peacetime military operations.