选择性血清素再摄取抑制剂(SSRIs)对骨折愈合的临床影响。

Devan Mehta, Abhishek Ganta, Vivian Bradaschia-Correa, Sanjit R Konda, Kenneth A Egol, Philipp Leucht
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引用次数: 0

摘要

目的:长期使用选择性血清素再摄取抑制剂(SSRIs)治疗抑郁症与骨代谢失衡导致骨质疏松症有关。最近,在小鼠模型中使用SSRIs已被证明通过减少成骨细胞分化和矿化来延缓体内和体外的骨愈合。本研究的目的是评估不愈合患者长期使用SSRI类药物是否会增加手术干预后的愈合时间。方法:我们回顾性分析了343例骨不连数据库中的患者,以确定哪些患者正在服用SSRI药物。在这些患者中,139人可以联系到,其中102人没有服用SSRIs, 37人正在服用SSRIs。在我们机构的每个队列中,记录患者从手术不愈合到愈合的时间作为主要结局。患者的医疗合并症,如糖尿病和吸烟状况也可能影响结合率。从手术不愈合时及最后一次随访开始,记录患者的基线短肌骨骼功能评估(SMFA)指数。结果:与最近的人口普查数据相比,我们发现使用SSRIs的不连症患者(26.6%)明显多于使用任何类型抗抑郁药的普通人群(11%)。两组患者基线特征差异无统计学意义(p = 0.048, p = 0.043),仅SSRI组患者BMI和年龄较高。骨折类型差异无统计学意义(p = 0.2063)。SSRIs组患者随访时SMFA困扰指数和功能指数较高(p = 0.0103, p = 0.0147)。SSRI组患者术后不愈合的平均时间为6.1个月,而未使用SSRI的患者为6.0个月(p = 0.74)。当对股骨、胫骨和肱骨的长骨骨折进行亚队列分析时,这些结果没有达到统计学意义。结论:据我们所知,这是第一个研究SSRIs对骨折愈合影响的临床研究。虽然体内和体外小鼠模型显示SSRI类药物对成骨细胞活性有有害影响,但我们的回顾性分析并未显示慢性SSRI患者和未服用SSRI类药物的患者在愈合时间上存在显著差异。然而,这项调查确实显示,与一般人群相比,非骨连队列中SSRI的使用发生率更高。在最近的动物模型研究中,这可能表明SSRI对急性骨折愈合过程有负面影响。
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Clinical Effect of Selective Serotonin Reuptake Inhibitors (SSRIs) on Fracture Healing.

Purpose: Chronic use of selective serotonin reuptake inhibitors (SSRIs) for the treatment of depression has been linked to an imbalance in bone metabolism leading to osteoporosis. More recently, the use of SSRIs in murine models has been shown to delay bone healing both in vivo and in vitro by decreasing the osteoblastic differentiation and mineralization. The purpose of this study was to evaluate whether or not chronic use of SSRI's in nonunion patients increases their time to union after surgical intervention.

Methods: We retrospectively analyzed 343 patients in a nonunion database to determine which patients were on SSRI medication. Of these patients, 139 could be contacted and of those 102 were not taking SSRIs and 37 were taking SSRIs. Patient's time to union from nonunion surgical intervention between each cohort at our institution was recorded as the primary outcome. Patient's medical comorbidities that could affect union rates such as diabetes and smoking status were also noted. Baseline Short Musculoskeletal Function Assessment (SMFA) index for bother and function were recorded from the time of nonunion surgery as well as last follow-up.

Results: Compared to recent census data, we found significantly more patients in the nonunion cohort using SSRIs (26.6%) than patients in the general population using any type of antidepressant (11%). There was no significant difference in the patients' baseline characteristics other than patients on SSRI treatment had a higher body mass index (BMI) and age (p = 0.048 and p = 0.043, respectively). There was no significant difference noted in the fracture types (p = 0.2063). Patients on SSRIs had a higher SMFA bother index and function index on follow-up (p = 0.0103, p = 0.0147). Patients in the SSRI group had a mean time to union from nonunion surgery of 6.1 months compared to 6.0 in patients without SSRI usage (p = 0.74). These did not reach statistical significance when subcohort analysis for long bone fractures was performed for the femur, tibia, and humerus.

Conclusion: To our knowledge, this is the first clinical study to investigate the effects of SSRIs on fracture healing. While in vivo and in vitro murine models have shown that SSRIs can have a deleterious effect on osteoblastic activity, our retrospective analysis did not show a significant difference in time to union between patients with chronic SSRI use and patients who have not been on SSRIs. However, this investigation did show a higher incidence of SSRI use in the nonunion cohort when compared to the general population. In the context of the recent animal model study, this may point to a negative effect of SSRI use on the acute fracture healing process.

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