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神经肌肉多发伤疼痛通过巨噬细胞 COX-2 纳米免疫调节得以缓解。

Neuromuscular Polytrauma Pain is Resolved by Macrophage COX-2 Nanoimmunomodulation.

机构信息

Laboratories of Neuroimmunology, Department of Symptom Research, the University of Texas MD Anderson Cancer Center, Houston, TX, 77030, USA.

School of Pharmacy, Duquesne University, Pittsburgh, PA, 15282, USA.

出版信息

Int J Nanomedicine. 2024 Jul 18;19:7253-7271. doi: 10.2147/IJN.S460418. eCollection 2024.

Abstract

Soft tissue injuries often involve muscle and peripheral nerves and are qualitatively distinct from single-tissue injuries. Prior research suggests that damaged innervation compromises wound healing. To test this in a traumatic injury context, we developed a novel mouse model of nerve and lower limb polytrauma, which features greater pain hypersensitivity and more sustained macrophage infiltration than either injury in isolation. We also show that macrophages are crucial mediators of pain hypersensitivity in this model by delivering macrophage-targeted nanoemulsions laden with the cyclooxygenase-2 (COX-2) inhibitor celecoxib. This treatment was more effective in males than females, and more effective when delivered 3 days post-injury than 7 days post-injury. The COX-2 inhibiting nanoemulsion drove widespread anti-inflammatory changes in cytokine expression in polytrauma-affected peripheral nerves. Our data shed new light on the modulation of inflammation by injured nerve input and demonstrate macrophage-targeted nanoimmunomodulation can produce rapid and sustained pain relief following complex injuries.

摘要

软组织损伤通常涉及肌肉和周围神经,与单一组织损伤在性质上有所不同。先前的研究表明,受损的神经支配会损害伤口愈合。为了在创伤性损伤的背景下检验这一点,我们开发了一种新的小鼠神经和下肢多发伤模型,与单一损伤相比,该模型表现出更高的痛觉过敏和更持续的巨噬细胞浸润。我们还通过递送负载环氧化酶-2(COX-2)抑制剂塞来昔布的巨噬细胞靶向纳米乳液,证明巨噬细胞是该模型中痛觉过敏的关键介质。这种治疗在雄性小鼠中比雌性小鼠更有效,在损伤后 3 天给药比 7 天给药更有效。COX-2 抑制纳米乳液驱动多发伤外周神经中细胞因子表达的广泛抗炎变化。我们的数据为受伤神经输入对炎症的调节提供了新的见解,并证明了针对巨噬细胞的纳米免疫调节可以在复杂损伤后迅速和持续地缓解疼痛。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0c81/11268785/90094c17864e/IJN-19-7253-g0001.jpg

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