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创伤性骨:创伤诱导的异位骨化。

The traumatic bone: trauma-induced heterotopic ossification.

作者信息

Dey Devaveena, Wheatley Benjamin M, Cholok David, Agarwal Shailesh, Yu Paul B, Levi Benjamin, Davis Thomas A

机构信息

Regenerative Medicine Department, Naval Medical Research Center, Silver Spring, Md.

Regenerative Medicine Department, Naval Medical Research Center, Silver Spring, Md; The Department of Surgery, Uniformed Services University of the Health Sciences, Walter Reed National Military Medical Center, Bethesda, Md.

出版信息

Transl Res. 2017 Aug;186:95-111. doi: 10.1016/j.trsl.2017.06.004. Epub 2017 Jun 15.

Abstract

Heterotopic ossification (HO) is a common occurrence after multiple forms of extensive trauma. These include arthroplasties, traumatic brain and spinal cord injuries, extensive burns in the civilian setting, and combat-related extremity injuries in the battlefield. Irrespective of the form of trauma, heterotopic bone is typically endochondral in structure and is laid down via a cartilaginous matrix. Once formed, the heterotopic bone typically needs to be excised surgically, which may result in wound healing complications, in addition to a risk of recurrence. Refinements of existing diagnostic modalities, like micro- and nano-CT are being adapted toward early intervention. Trauma-induced HO is a consequence of aberrant wound healing, systemic and local immune system activation, infections, extensive vascularization, and innervation. This intricate molecular crosstalk culminates in activation of stem cells that initiate heterotopic endochondral ossification. Development of animal models recapitulating the unique traumatic injuries has greatly facilitated the mechanistic understanding of trauma-induced HO. These same models also serve as powerful tools to test the efficacy of small molecules which specifically target the molecular pathways underlying ectopic ossification. This review summarizes the recent advances in the molecular understanding, diagnostic and treatment modalities in the field of trauma-induced HO.

摘要

异位骨化(HO)在多种形式的广泛创伤后很常见。这些创伤包括关节成形术、创伤性脑损伤和脊髓损伤、 civilian环境中的大面积烧伤以及战场上与战斗相关的肢体损伤。无论创伤形式如何,异位骨的结构通常为软骨内成骨,并通过软骨基质形成。一旦形成,异位骨通常需要手术切除,这除了有复发风险外,还可能导致伤口愈合并发症。现有的诊断方法,如微型和纳米CT,正在进行改进以实现早期干预。创伤诱导的HO是异常伤口愈合、全身和局部免疫系统激活、感染、广泛血管化和神经支配的结果。这种复杂的分子相互作用最终导致启动异位软骨内成骨的干细胞激活。模拟独特创伤性损伤的动物模型的开发极大地促进了对创伤诱导HO机制的理解。这些相同的模型也作为强大的工具来测试专门针对异位骨化潜在分子途径的小分子的疗效。本综述总结了创伤诱导HO领域在分子理解、诊断和治疗方法方面的最新进展。

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