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Preoperative irradiation for the prevention of heterotopic ossification induces local inflammation in humans

机译:术前照射预防异位骨化可引起人体局部炎症

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摘要

Radiation of the hip is an established method to prevent heterotopic ossification (HO) following total hip arthroplasty (THA) but the precise mechanism is unclear. As inflammatory processes are suggested to be involved in the pathogenesis of HO, we hypothesized that the preoperative irradiation impacts local immune components. Therefore, we quantified immune cell populations and cytokines in hematomas resulting from the transection of the femur in two groups of patients receiving THA: patients irradiated preoperatively (THA-X-hematoma: THA-X-H group) in the hip region (7Gy) in order to prevent HO and patients who were not irradiated (THA-H group) but were postoperatively treated with non-steroidal anti-inflammatory drugs (NSAIDs). Radiation resulted in significantly increased frequencies of T cells, cytotoxic T cells, NKT cells and CD25+CD127- Treg cells, whereas the number of naive CD45RA-expressing cytotoxic T cells was reduced. These results indicate differential immune cell activation, corroborated by our findings of significantly higher concentrations of pro-inflammatory cytokines (e.g. IL-6, IFNγ) and chemokines (e.g. MCP-1, RANTES) in the THA-X-H group as compared to THA-H group. In contrast, the concentration of the angiogenic VEGF was significantly suppressed in the THA-X-H group. We conclude that preoperative irradiation results in significant changes in immune cell composition and cytokine secretion in THA-hematomas, establishing a specific - rather proinflammatory - milieu. This increase of inflammatory activity together with the observed suppression in VEGF secretion may contribute to the prevention of HO.
机译:髋部放射是预防全髋关节置换术(THA)后异位骨化(HO)的既定方法,但确切的机制尚不清楚。由于炎症过程被认为与HO的发病机制有关,我们假设术前照射会影响局部免疫成分。因此,我们对接受THA的两组患者的股骨横断所致的血肿中的免疫细胞群和细胞因子进行了定量分析:术前在髋部区域(7Gy)接受过放射治疗的患者(THA-X-血肿:THA-XH组)预防HO和未接受辐照的患者(THA-H组),但术后接受非甾体抗炎药(NSAIDs)治疗。辐射导致T细胞,细胞毒性T细胞,NKT细胞和CD25 + CD127-Treg细胞的频率显着增加,而幼稚表达CD45RA的细胞毒性T细胞的数量减少。这些结果表明免疫细胞的差异激活,这一点得到了我们的发现的佐证:与THA-XH组相比,THA-XH组的促炎性细胞因子(例如IL-6,IFNγ)和趋化因子(例如MCP-1,RANTES)的浓度明显更高。 H组。相反,在THA-X-H组中,显着抑制了血管生成性VEGF的浓度。我们得出的结论是,术前照射导致THA血肿中免疫细胞组成和细胞因子分泌的显着变化,从而建立了一种特定的-促炎性环境。炎症活性的这种增加以及观察到的VEGF分泌的抑制可能有助于预防HO。

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