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老年癌症患者的能量消耗情况与早期限制性毒性风险:ELCAPA - 25前瞻性队列研究

Energy expenditure profiles and the risk of early limiting toxicity in older patients with cancer: The ELCAPA-25 prospective cohort survey.

作者信息

Boudou-Rouquette Pascaline, de Moura Alexandre, Martinez-Tapia Claudia, Serrano Adolfo Gonzalez, Chahwakilian Anne, Jouinot Anne, Ulmann Guillaume, Orvoën Galdric, Chambraud Clélia, Durand Jean-Philippe, Caillet Philippe, Goldwasser Francois, Paillaud Elena, Canouï-Poitrine Florence

机构信息

AP-HP, Cochin Hospital, Cancer Research for PErsonalized Medicine (CARPEM), Department of Medical Oncology, ARIANE Program, Paris, France; Paris Cité University, Institut Cochin, Inserm U1016, Paris, France.

AP-HP, Cochin Hospital, Cancer Research for PErsonalized Medicine (CARPEM), Department of Medical Oncology, ARIANE Program, Paris, France.

出版信息

Clin Nutr. 2022 May;41(5):1073-1082. doi: 10.1016/j.clnu.2022.02.016. Epub 2022 Mar 3.

Abstract

BACKGROUND & AIMS: Predicting the risk of early limiting toxicity (ELT) is major challenge for the clinician seeking an effective, safe treatment for older patients with cancer. The Cancer and Aging Research Group (CARG) and CRASH (Chemotherapy Risk Assessment Scale for High-Age Patients) toxicity scores were designed to predict chemotherapy-related toxicity. Elevated resting energy expenditure (REE) may predispose to cachexia and increase ELT and mortality in older patients with cancer. The primary objective was to assess the association between elevated REE and ELT in older patients with cancer. The secondary objectives were to assess the discriminant ability of a predictive model including REE (relative to the CARG and CRASH scores) and the prognostic value of elevated REE.

METHODS

We assessed patients aged 70 or over included in the prospective ELCAPA cohort between 2014 and 2018. The inclusion criteria were a solid tumour, a measurement of REE at baseline (mREE, by indirect calorimetry), and a geriatric assessment prior to cancer treatment in a teaching hospital (Paris, France). The mREE was compared with the predicted REE (pREE), as defined by the Harris-Benedict equation. Depending on the mREE/pREE ratio, study participants were classified as hypermetabolic, hypometabolic or normometabolic. The primary endpoint was 3-month ELT, defined as any unplanned hospitalization or any event leading to dose reduction, a treatment delay of more than 7 days, or treatment discontinuation within 3 months of initiation. The secondary endpoint was the 3-month mortality rate.

RESULTS

A total of 179 patients were included. The median age was 80 [interquartile range: 76-84] years, 37% of the patients were female, 81.8% had metastatic disease, 67.6% received chemotherapy, 20.7% received hormone therapy, and 11.7% received targeted therapies. According to the mREE/pREE ratio, 85 patients (47%) were hypermetabolic, 63 (35%) were normometabolic, and 31 (18%) were hypometabolic. Sixty patients (33.5%; 95% confidence interval (CI): 26.7-40.9) experienced ELT. The discriminant ability (as assessed by the C-index) of a multivariate model including REE and adjustment factors was 0.82 [95%CI: 0.73-0.91]. In comparison, the discriminant ability of the CARG and CRASH models was 0.57 [0.45-0.68] and 0.51 [0.40-0.62], respectively. In our model, hypermetabolism was an independent risk factor for ELT (adjusted odds ratio = 2.44; 95%CI: 1.02-5.80). Other risk factors were the cancer type and stage, the treatment protocol, a clinical diagnosis of depression, the presence of grade 3 or 4 comorbidities, and the serum lactate dehydrogenase level.

CONCLUSION

Hypermetabolism status is an independent predictor of ELT in older patients with cancer, relative to normometabolic status. Baseline REE measurement might improve the ELT risk assessment and decision-making process.

摘要

背景与目的

对于寻求为老年癌症患者提供有效、安全治疗方案的临床医生而言,预测早期限制性毒性(ELT)风险是一项重大挑战。癌症与衰老研究组(CARG)毒性评分及CRASH(高龄患者化疗风险评估量表)毒性评分旨在预测化疗相关毒性。静息能量消耗(REE)升高可能易导致恶病质,并增加老年癌症患者的ELT及死亡率。主要目的是评估老年癌症患者中REE升高与ELT之间的关联。次要目的是评估包含REE的预测模型(相对于CARG和CRASH评分)的判别能力以及REE升高的预后价值。

方法

我们评估了2014年至2018年间纳入前瞻性ELCAPA队列的70岁及以上患者。纳入标准为实体瘤、基线时的REE测量值(通过间接测热法测得的mREE)以及在一家教学医院(法国巴黎)进行癌症治疗前的老年评估。将mREE与哈里斯 - 本尼迪克特方程定义的预测REE(pREE)进行比较。根据mREE/pREE比值,研究参与者被分类为高代谢、低代谢或正常代谢。主要终点为3个月时的ELT,定义为任何非计划性住院或导致剂量减少、治疗延迟超过7天或在开始治疗后3个月内治疗中断的任何事件。次要终点为3个月死亡率。

结果

共纳入179例患者。中位年龄为80岁[四分位间距:76 - 84岁],37%的患者为女性,81.8%患有转移性疾病,67.6%接受化疗,20.7%接受激素治疗,11.7%接受靶向治疗。根据mREE/pREE比值,85例患者(47%)为高代谢,63例(35%)为正常代谢,31例(18%)为低代谢。60例患者(33.5%;95%置信区间(CI):26.7 - 40.9)发生ELT。包含REE和调整因素的多变量模型的判别能力(通过C指数评估)为0.82[95%CI:0.73 - 0.91]。相比之下,CARG模型和CRASH模型的判别能力分别为0.57[0.45 - 0.68]和0.51[0.40 - 0.62]。在我们的模型中,高代谢是ELT的独立危险因素(调整后比值比 = 2.44;95%CI:1.02 - 5.80)。其他危险因素包括癌症类型和分期、治疗方案、抑郁症临床诊断、3级或4级合并症的存在以及血清乳酸脱氢酶水平。

结论

相对于正常代谢状态,高代谢状态是老年癌症患者ELT的独立预测因素。基线REE测量可能会改善ELT风险评估及决策过程。

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