Polytrauma impairs fracture healing accompanied by increased persistence of innate inflammatory stimuli and reduced adaptive response.

IF 2.1 3区 医学 Q2 ORTHOPEDICS Journal of Orthopaedic Research® Pub Date : 2024-11-17 DOI:10.1002/jor.26015
Augustine Mark Saiz, Maryam Rahmati, Robert Charles Henry Gresham, Tony Daniel Baldini, Jane Burgan, Mark A Lee, Benjamin Osipov, Blaine A Christiansen, Thaqif El Khassawna, D C Florian Wieland, André Lopes Marinho, Clement Blanchet, Molly Czachor, Zachary M Working, Chelsea S Bahney, J Kent Leach
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Abstract

The field of bone regeneration has primarily focused on investigating fracture healing and nonunion in isolated musculoskeletal injuries. Compared to isolated fractures, which frequently heal well, fractures in patients with multiple bodily injuries (polytrauma) may exhibit impaired healing. While some papers have reported the overall cytokine response to polytrauma conditions, significant gaps in our understanding remain in how fractures heal differently in polytrauma patients. We aimed to characterize fracture healing and the temporal local and systemic immune responses to polytrauma in a murine model of polytrauma composed of a femur fracture combined with isolated chest trauma. We collected serum, bone marrow from the uninjured limb, femur fracture tissue, and lung tissue over 3 weeks to study the local and systemic immune responses and cytokine expression after injury. Immune cell distribution was assessed by flow cytometry. Fracture healing was characterized using microcomputed tomography (microCT), histological staining, immunohistochemistry, mechanical testing, and small angle X-ray scattering. We detected more innate immune cells in the polytrauma group, both locally at the fracture site and systemically, compared to other groups. The percentage of B and T cells was dramatically reduced in the polytrauma group 6 h after injury and remained low throughout the study duration. Fracture healing in the polytrauma group was impaired, evidenced by the formation of a poorly mineralized and dysregulated fracture callus. Our data confirm the early, dysregulated inflammatory state in polytrauma that correlates with disorganized and impaired fracture healing.

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多发性创伤会影响骨折愈合,并伴随先天性炎症刺激的持续性增加和适应性反应的降低。
骨再生领域主要侧重于研究孤立的肌肉骨骼损伤的骨折愈合和不愈合。与通常愈合良好的孤立性骨折相比,身体多处受伤(多发性创伤)患者的骨折可能会出现愈合障碍。虽然一些论文报道了多发性创伤情况下细胞因子的整体反应,但我们对多发性创伤患者骨折愈合的不同方式的理解仍存在很大差距。我们的目的是在一个由股骨骨折和孤立的胸部创伤组成的多发性创伤小鼠模型中,描述骨折愈合以及对多发性创伤的局部和全身免疫反应的时间特征。我们收集了未受伤肢体的血清、骨髓、股骨骨折组织和肺组织,历时 3 周,以研究受伤后的局部和全身免疫反应及细胞因子表达。流式细胞术评估了免疫细胞的分布。利用微型计算机断层扫描(microCT)、组织学染色、免疫组化、机械测试和小角 X 射线散射对骨折愈合进行了表征。与其他组别相比,我们在多发性创伤组的骨折部位和全身检测到了更多的先天性免疫细胞。多发性创伤组的 B 细胞和 T 细胞比例在受伤 6 小时后急剧下降,并在整个研究期间保持较低水平。多发性创伤组的骨折愈合受损,表现为形成矿化度低、调节失调的骨折胼胝体。我们的数据证实了多发性创伤的早期炎症失调状态与骨折愈合紊乱和受损有关。
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来源期刊
Journal of Orthopaedic Research®
Journal of Orthopaedic Research® 医学-整形外科
CiteScore
6.10
自引率
3.60%
发文量
261
审稿时长
3-6 weeks
期刊介绍: The Journal of Orthopaedic Research is the forum for the rapid publication of high quality reports of new information on the full spectrum of orthopaedic research, including life sciences, engineering, translational, and clinical studies.
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