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IF 8.8 2区医学 Q1 IMMUNOLOGY

Brain, Behavior, and Immunity Pub Date : 2025-01-25 DOI:10.1016/j.bbi.2025.01.015

Nathan T Fiore, Kendal F Willcox, Dorsa Dayani, Younus A Zuberi, Cobi J Heijnen, Peter M Grace

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引用次数: 0

摘要

临床前和临床研究已经证实，自身反应性免疫球蛋白 G（IgG）可引起神经性疼痛。我们最近证实，雄性和雌性小鼠坐骨神经慢性收缩损伤（CCI）会导致产生前感觉性 IgG，这种 IgG 会在腰部周围积聚，包括背根神经节（DRG）和脊髓内，从而促进神经性疼痛的发生。这些数据提出了一种耐人寻味的可能性，即通过减少 IgG 的积累来缓解神经性疼痛。为此，我们测试了新生儿 Fc 受体（FcRn）的生物抑制或基因缺失是否会减轻 CCI 诱导的机械过敏（异动症）和 IgG 沉积。FcRn 主要表达于骨髓细胞和内皮细胞，通过针吞作用和向细胞外环境的再循环延长 IgG 的半衰期。我们在此表明，与Fc片段对照组相比，在CCI后7天或28天服用FcRn阻断剂efgartigimod可缓解雄性和雌性小鼠的异动症。与野生型小鼠相比，FcRn缺陷（FcRn-）小鼠的CCI诱导的异动症也同样减轻。FcRn的生物抑制或基因缺失也减少了CCI诱导的巨噬细胞和腰部DRG神经元以及腰部背侧脊髓小胶质细胞上的IgG积聚。与对照组相比，经依加替莫德治疗或CCI后的FcRn-小鼠的Fc受体γ亚基（FcRγ）表达减少。FcRγ亚基是Fcγ受体（FcγRs）的关键组成部分，Fcγ受体由IgG免疫复合物激活。在受到 IgG 免疫复合物刺激的巨噬细胞培养物中，阻断 FcRn 也会抑制 FcγR 依赖性促炎细胞因子的产生。总之，我们的研究表明，阻断或缺失 FcRn 可减轻 CCI 后的机械异感并减少 IgG 累积，从而减弱腰部周围的代痛觉 IgG-FcγR 信号传导。阻断 FcRn 和减少 IgG 循环的策略作为 IgG 介导的神经病理性疼痛的潜在治疗方法值得进一步研究。

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Reducing IgG accumulation via neonatal Fc receptor (FcRn) blockade relieves neuropathic pain.

Preclinical and clinical studies have established that autoreactive immunoglobulin G (IgG) can drive neuropathic pain. We recently demonstrated that sciatic nerve chronic constriction injury (CCI) in male and female mice results in the production of pronociceptive IgG, which accumulates around the lumbar region, including within the dorsal root ganglia (DRG) and spinal cord, facilitating the development of neuropathic pain. These data raise the intriguing possibility that neuropathic pain may be alleviated by reducing the accumulation of IgG. To this end, we tested whether biologic inhibition or genetic deletion of the neonatal Fc receptor (FcRn) would attenuate mechanical hypersensitivity (allodynia) and IgG deposition induced by CCI. FcRn are prominently expressed on myeloid and endothelial cells and extend the half-life of IgG via pinocytosis and recycling into the extracellular milieu. We show here that administration of the FcRn blocker efgartigimod either 7- or 28-days post-CCI relieved allodynia among both male and female mice, compared to the Fc fragment control. Efgartigimod, administered systemically (intraperitoneal) or to the lumbar region (intrathecal), attenuated mechanical allodynia for at least one month w. CCI-induced allodynia was similarly reduced in FcRn-deficient (FcRn^-) mice compared to wild-type mice. Biologic inhibition or genetic deletion of FcRn also reduced CCI-induced accumulation of IgG on macrophages and neurons in lumbar DRG, as well as microglia in the lumbar dorsal spinal cord. Expression of the Fc receptor γ subunit (FcRγ) was reduced in efgartigimod-treated or FcRn^- mice post-CCI compared to controls. The FcRγ subunit is a key component of Fc gamma receptors (FcγRs), which are activated by IgG immune complexes. In macrophage cultures stimulated by IgG immune complexes, FcRn blockade also dampened FcγR-dependent production of proinflammatory cytokines. Collectively, our study demonstrates that FcRn blockade or deletion alleviates mechanical allodynia and reduces IgG accumulation after CCI, attenuating pronociceptive IgG-FcγR signaling around the lumbar region. Strategies to block FcRn and reduce IgG recycling warrant further investigation as potential treatments for IgG-mediated neuropathic pain.

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来源期刊

Brain, Behavior, and Immunity 医学-免疫学

CiteScore

29.60

自引率

2.00%

发文量

290

审稿时长

28 days

期刊介绍： Established in 1987, Brain, Behavior, and Immunity proudly serves as the official journal of the Psychoneuroimmunology Research Society (PNIRS). This pioneering journal is dedicated to publishing peer-reviewed basic, experimental, and clinical studies that explore the intricate interactions among behavioral, neural, endocrine, and immune systems in both humans and animals. As an international and interdisciplinary platform, Brain, Behavior, and Immunity focuses on original research spanning neuroscience, immunology, integrative physiology, behavioral biology, psychiatry, psychology, and clinical medicine. The journal is inclusive of research conducted at various levels, including molecular, cellular, social, and whole organism perspectives. With a commitment to efficiency, the journal facilitates online submission and review, ensuring timely publication of experimental results. Manuscripts typically undergo peer review and are returned to authors within 30 days of submission. It's worth noting that Brain, Behavior, and Immunity, published eight times a year, does not impose submission fees or page charges, fostering an open and accessible platform for scientific discourse.