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老年综合评估发现 65 岁以下癌症成年人的功能损害和衰弱:优化肿瘤治疗的机会。

Geriatric assessment-identified impairments and frailty in adults with cancer younger than 65: An opportunity to optimize oncology care.

机构信息

ReVital Cancer Rehabilitation, Select Medical, Mechanicsburg, PA, United States of America; University of North Carolina at Chapel Hill, NC, United States of America.

ReVital Cancer Rehabilitation, Select Medical, Mechanicsburg, PA, United States of America.

出版信息

J Geriatr Oncol. 2024 May;15(4):101751. doi: 10.1016/j.jgo.2024.101751. Epub 2024 Apr 3.

Abstract

INTRODUCTION

Frailty, a state of increased vulnerability to stressors due to aging or treatment-related accelerated aging, is associated with declines in physical, cognitive and/or social functioning, and quality of life for cancer survivors. For survivors aged <65 years, little is known about frailty status and associated impairments to inform intervention. We aimed to evaluate the prevalence of frailty and contributing geriatric assessment (GA)-identified impairments in adults aged <65 versus ≥65 years with cancer.

MATERIALS AND METHODS

This study is a secondary analysis of clinical trial data (NCT04852575). Participants were starting a new line of systemic therapy at a community-based oncology private practice. Before starting treatment, participants completed an online patient-reported GA and the Physical Activity (PA) Vital Sign questionnaire. Frailty score and category were derived from GA using a validated deficit accumulation model: frail (>0.35), pre-frail (0.2-0.35), or robust (0-0.2). PA mins/week were calculated, and participants were coded as either meeting/not-meeting guidelines (≥90 min/week). We used Spearman (ρ) correlation to examine the association between age and frailty score and chi-squared/Fisher's-exact or ANOVA/Kruskal-Wallis statistic to compare frailty and PA outcomes between age groups.

RESULTS

Participants (n = 96) were predominantly female (62%), Caucasian (68%), beginning first-line systemic therapy (69%), and 1.75 months post-diagnosis (median). Most had stage III to IV disease (66%). Common cancer types included breast (34%), gastrointestinal (23%), and hematologic (15%). Among participants <65, 46.8% were frail or pre-frail compared to 38.7% of those ≥65. There was no association between age and frailty score (ρ = 0.01, p = 0.91). Between age groups, there was no significant difference in frailty score (p = 0.95), the prevalence of frailty (p = 0.68), number of GA impairments (p = 0.33), or the proportion meeting PA guidelines (p = 0.72). However, older adults had more comorbid conditions (p = 0.03) and younger adults had non-significant but clinically relevant differences in functional ability, falls, and PA level.

DISCUSSION

In our cohort, the prevalence of frailty was similar among adults with cancer <65 when compared to those older than 65, however, types of GA impairments differed. These results suggest GA and the associated frailty index could be useful to identify needs for intervention and inform clinical decisions during cancer treatment regardless of age. Additional research is needed to confirm our findings.

摘要

简介

衰弱是一种由于衰老或与治疗相关的加速衰老而导致对压力源的易感性增加的状态,与癌症幸存者的身体、认知和/或社会功能以及生活质量下降有关。对于<65 岁的幸存者,关于衰弱状态以及与之相关的功能障碍的信息很少,无法为干预措施提供信息。我们旨在评估<65 岁和≥65 岁癌症患者的衰弱状况和相关的老年综合评估(GA)确定的损伤的患病率。

材料和方法

本研究是一项临床试验数据的二次分析(NCT04852575)。参与者正在一家社区肿瘤私人诊所开始新的一线系统治疗。在开始治疗之前,参与者完成了在线患者报告的 GA 和体力活动(PA)生命体征问卷。衰弱评分和类别是通过使用经过验证的缺陷积累模型从 GA 中得出的:衰弱(>0.35)、虚弱前期(0.2-0.35)或健壮(0-0.2)。计算每周的 PA 分钟数,并根据每周≥90 分钟的指南对参与者进行编码(符合/不符合)。我们使用 Spearman(ρ)相关性来检查年龄和衰弱评分之间的关联,使用卡方/Fisher 精确检验或 ANOVA/Kruskal-Wallis 统计量来比较年龄组之间的衰弱和 PA 结果。

结果

参与者(n=96)主要为女性(62%)、白种人(68%)、开始一线系统治疗(69%)和诊断后 1.75 个月(中位数)。大多数患者处于 III 期至 IV 期疾病(66%)。常见的癌症类型包括乳腺癌(34%)、胃肠道癌(23%)和血液癌(15%)。在<65 岁的参与者中,46.8%为衰弱或虚弱前期,而≥65 岁的参与者中这一比例为 38.7%。年龄与衰弱评分之间没有关联(ρ=0.01,p=0.91)。在年龄组之间,衰弱评分(p=0.95)、衰弱的患病率(p=0.68)、GA 损伤的数量(p=0.33)或符合 PA 指南的比例(p=0.72)均无显著差异。然而,老年人有更多的合并症(p=0.03),而年轻人在功能能力、跌倒和 PA 水平方面存在非显著但具有临床意义的差异。

讨论

在我们的队列中,<65 岁的癌症患者与>65 岁的患者相比,衰弱的患病率相似,但 GA 损伤的类型不同。这些结果表明,GA 和相关的衰弱指数可以用于识别干预需求,并在癌症治疗期间为临床决策提供信息,无论年龄大小。需要进一步的研究来证实我们的发现。

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