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帕金森病是否与全髋关节置换术后死亡率增加、预后评分降低和翻修风险增加相关?来自瑞典髋关节置换登记处的研究结果。

Is Parkinson's Disease Associated with Increased Mortality, Poorer Outcomes Scores, and Revision Risk After THA? Findings from the Swedish Hip Arthroplasty Register.

机构信息

A. L. Wojtowicz, P. Cnudde, Hywel Dda University Health Board, Prince Philip Hospital, Trauma & Orthopaedics Department, Wales, UK M. Mohaddes, E, Bülow, S. Nemes, P. Cnudde, Institute of Clinical Sciences, Department of Orthopaedics, Sahlgrenska Academy, University of Gothenburg, Gothenburg, Sweden M. Mohaddes, D. Odin, E, Bülow, S. Nemes, P. Cnudde, Swedish Hip Arthroplasty Register, Register Centrum Västra Götaland, Gothenburg, Sweden.

出版信息

Clin Orthop Relat Res. 2019 Jun;477(6):1347-1355. doi: 10.1097/CORR.0000000000000679.

Abstract

BACKGROUND

Neurological conditions such as Parkinson's disease are commonly accepted as a risk factor for an increased likelihood of undergoing revision surgery or death after THA. However, the available evidence for an association between Parkinson's disease and serious complications or poorer patient-reported outcomes after THA is limited and contradictory.

QUESTIONS/PURPOSES: (1) Do patients with a preoperative diagnosis of Parkinson's disease have an increased risk of death after elective THA compared with a matched control group of patients? (2) After matching for patient- and surgery-related factors, do revision rates differ between the patients with Parkinson's disease and the matched control group? (3) Are there any differences in patient-reported outcome measures for patients with Parkinson's disease compared with the matched control group?

METHODS

Data were derived from a merged database with information from the Swedish Hip Arthroplasty Register and administrative health databases. We identified all patients with Parkinson's disease who underwent THA for primary osteoarthritis between January 1, 1999 and December 31, 2012 (n = 490 after exclusion criteria applied). A control group was generated through exact one-to-one matching for age, sex, Charlson comorbidity index, surgical approach, and fixation method. Risk of death and revision were compared between the groups using Kaplan-Meier and log-rank testing. Patient-reported outcome measures (PROMs), routinely recorded as EQ-5D, EQ VAS, and pain VAS, were measured at the preoperative visit and at 1-year postoperatively; mean absolute values for PROM scores and change in scores over time were compared between the two groups.

RESULTS

The risk of death did not differ at 90 days (control group risk = 0.61%; 95% CI = 0.00-1.3; Parkinson's disease group risk = 0.62%; 95% CI = 0.00-1.31; p = 0.998) or 1 year (control group = 2.11%; 95% CI = 0.81-3.39; Parkinson's disease group = 2.56%, 95% CI = 1.12-3.97; p = 0.670). At 9 years, the risk of death was increased for patients with Parkinson's disease (control group = 28.05%; 95% CI = 22.29-33.38; Parkinson's disease group = 54.35%; 95% CI = 46.72-60.88; p < 0.001). The risk of revision did not differ at 90 days (control group = 0.41%; 95% CI = 0.00-0.98; Parkinson's disease group = 1.03%; 95% CI = 0.13-1.92; p = 0.256). At 1 year, the risk of revision was higher for patients with Parkinson's disease (control group = 0.41%; 95% CI = 0.00-0.98; Parkinson's disease group = 2.10%; 95% CIs = 0.80-3.38; p = 0.021). This difference was more pronounced at 9 years (control group = 1.75%; 95% CI = 0.11-3.36; Parkinson's disease group = 5.44%; 95% CI = 2.89-7.91; p = 0.001) when using the Kaplan-Meier method. There was no difference between the control and Parkinson's disease groups for level of pain relief at 1 year postoperatively (mean reduction in pain VAS score for control group = 48.85, SD = 20.46; Parkinson's disease group = 47.18, SD = 23.96; p = 0.510). Mean change in scores for quality of life and overall health from preoperative measures to 1 year postoperatively were smaller for patients in the Parkinson's disease group compared with controls (mean change in EQ-5D scores for control group = 0.42, SD = 0.32; Parkinson's disease group = 0.30, SD = 0.37; p 0.003; mean change in EQ VAS scores for control group = 20.94, SD = 23.63; Parkinson's disease = 15.04, SD = 23.00; p = 0.027).

CONCLUSIONS

Parkinson's disease is associated with an increased revision risk but not with short-term mortality rates relevant to assessing risk versus benefit before undergoing THR. The traditional reluctance to perform THR in patients with Parkinson's disease may be too conservative given that the higher long-term risk of death is more likely due to the progressive neurological disorder and not THR itself, and patients with Parkinson's disease report comparable outcomes to controls. Further research on outcomes in THR for patients with other neurological conditions is needed to better address the broader assumptions underlying this traditional teaching.Level of Evidence Level III, therapeutic study.

摘要

背景

帕金森病等神经系统疾病通常被认为是髋关节置换术(THA)后再次手术或死亡风险增加的一个危险因素。然而,目前关于帕金森病与 THA 后严重并发症或患者报告结局较差之间关联的证据有限且相互矛盾。

问题/目的:(1)与匹配的对照组患者相比,术前诊断为帕金森病的患者在择期 THA 后死亡的风险是否增加?(2)在匹配患者和手术相关因素后,帕金森病患者与匹配对照组患者的翻修率是否存在差异?(3)与匹配对照组相比,帕金森病患者的患者报告结局测量指标(PROMs)是否存在差异?

方法

数据来自瑞典髋关节置换登记处和行政健康数据库的合并数据库。我们确定了所有因原发性骨关节炎接受 THA 的帕金森病患者(排除标准适用后,有 490 例)。通过年龄、性别、Charlson 合并症指数、手术入路和固定方法的精确一对一匹配生成对照组。使用 Kaplan-Meier 和对数秩检验比较两组之间的死亡率和翻修率。在术前就诊时和术后 1 年测量患者报告结局测量指标(PROMs),包括 EQ-5D、EQ VAS 和疼痛 VAS,比较两组之间的 PROM 评分的平均绝对值和随时间的变化。

结果

在 90 天(对照组风险 = 0.61%;95%CI = 0.00-1.3;帕金森病组风险 = 0.62%;95%CI = 0.00-1.31;p = 0.998)或 1 年(对照组 = 2.11%;95%CI = 0.81-3.39;帕金森病组 = 2.56%,95%CI = 1.12-3.97;p = 0.670)时,死亡率无差异。9 年时,帕金森病患者的死亡率增加(对照组 = 28.05%;95%CI = 22.29-33.38;帕金森病组 = 54.35%;95%CI = 46.72-60.88;p < 0.001)。在 90 天(对照组 = 0.41%;95%CI = 0.00-0.98;帕金森病组 = 1.03%;95%CI = 0.13-1.92;p = 0.256)和 1 年(对照组 = 0.41%;95%CI = 0.00-0.98;帕金森病组 = 2.10%;95%CI = 0.80-3.38;p = 0.021)时,翻修率无差异。在 9 年时,帕金森病患者的翻修率更高(对照组 = 1.75%;95%CI = 0.11-3.36;帕金森病组 = 5.44%;95%CI = 2.89-7.91;p = 0.001),使用 Kaplan-Meier 方法时更为明显。在术后 1 年时,两组患者的疼痛缓解程度无差异(对照组疼痛 VAS 评分平均降低 48.85,标准差为 20.46;帕金森病组为 47.18,标准差为 23.96;p = 0.510)。与对照组相比,帕金森病组患者的生活质量和整体健康状况从术前到术后 1 年的平均变化较小(对照组 EQ-5D 评分平均变化 0.42,标准差为 0.32;帕金森病组为 0.30,标准差为 0.37;p < 0.003;对照组 EQ VAS 评分平均变化 20.94,标准差为 23.63;帕金森病组为 15.04,标准差为 23.00;p = 0.027)。

结论

帕金森病与翻修风险增加相关,但与 THR 前评估风险与获益相关的短期死亡率无关。由于更高的长期死亡风险更可能是由于进行性神经疾病而不是 THR 本身,而帕金森病患者报告的结果与对照组相似,因此对患有帕金森病等其他神经疾病的患者进行 THR 的结果进行进一步研究,以更好地解决这一传统教学背后的广泛假设。证据水平 III,治疗研究。

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