亨廷顿病的提前护理计划和健康相关生活质量:来自一项多中心国家研究的结果

IF 1.1 Q4 HEALTH CARE SCIENCES & SERVICES
Leonard L Sokol, Jonathan P Troost, Danny Bega, Benzi M Kluger, Holly G Prigerson, Martha Nance, Samuel Frank, Joel S Perlmutter, Praveen Dayalu, David Cella, Noelle E Carlozzi
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引用次数: 1

摘要

目的:亨廷顿病(HD)是一种致命的神经退行性疾病,与其他神经系统疾病相比,其自杀念头和行为(STB)的患病率仍然较高,目前尚不清楚STB和健康相关生活质量(HRQoL)是否会影响临终计划或更广泛地影响提前护理计划(ACP)。相反,ACP是否会引起未来STB和HRQoL的变化是未知的。因此,我们试图评估STB和HRQoL患者报告的结果(PROs)是否与ACP有关,以及ACP是否与24个月时STB和HRQoL的变化有关。方法:通过我们的多中心研究(HDQLIFE™),在基线入组、12个月和24个月时获得经HD验证的临床和患者评估(即HRQoL pro),该研究在美国范围内对表现为HD的前期、早期和晚期患者进行了研究。我们使用线性混合效应模型来确定基线时STB与HRQoL和随访时HDQLIFE生命末期计划之间的关系。使用单独的线性混合效应模型来评估基线时HDQLIFE生命终点计划与12个月和24个月时HRQoL和STB之间的关系。错误发现率调整用于解释多重比较。结果:在基线入组时,STB和HRQoL在12个月或24个月时与HDQLIFE生命终点计划无关。同样,在基线时,HDQLIFE临终计划显示与STB或HRQoL在12个月或24个月时没有关联。解释:STB和HRQoL的PROs对ACP的患者参与没有显著影响。最重要的是,参与ACP不会对这种罕见的神经退行性疾病的HRQoL或STB造成不良影响,其中STB的终生患病率接近30%。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Advance Care Planning and Health-Related Quality of Life in Huntington Disease: Results from a Multicenter National Study.

Objective: With Huntington disease (HD), a fatal neurodegenerative disease where the prevalence of suicidal thoughts and behavior (STB) remains elevated as compared to other neurological disorders, it is unknown whether STB and health-related quality of life (HRQoL) affect plans for the end of life or more broadly, advance care planning (ACP). Conversely, it is unknown whether ACP would provoke future changes to STB and HRQoL. Therefore, we sought to evaluate whether STB and HRQoL patient-reported outcomes (PROs) contribute to ACP and whether ACP relates to changes in STB and HRQoL at 24 months.

Methods: HD-validated clinician- and patient-assessments (i.e., HRQoL PROs) were obtained at baseline enrollment, 12 and 24 months through our multi-center study (HDQLIFE™) throughout the United States among people with premanifest, early-stage, and late-stage manifest HD. We used linear mixed-effects models to determine the relationships between STB and HRQoL at baseline and HDQLIFE End of Life Planning at follow-up. Separate linear mixed-effects models were used to assess the relationship between HDQLIFE End of Life Planning at baseline, and HRQoL and STB at 12 and 24 months. False discovery rate adjustments were used to account for multiple comparisons.

Results: At baseline enrollment, STB and HRQoL were not related to HDQLIFE End of Life Planning at 12 or 24 months. Similarly, at baseline, HDQLIFE End of Life Planning demonstrated no association with STB or HRQoL at 12 or 24 months.

Interpretation: STB and HRQoL PROs do not significantly affect patient engagement with ACP. Most importantly, engaging in ACP does not cause untoward effects on HRQoL or STB for this rare neurodegenerative disease where the lifetime prevalence of STB approaches 30%.

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