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炎症相关蛋白作为治疗相关行为症状的生物标志物:一项针对乳腺癌患者及年龄匹配对照的纵向研究

Inflammation-related proteins as biomarkers of treatment-related behavioral symptoms: A longitudinal study of breast cancer patients and age-matched controls.

作者信息

Patel Sunita K, Breen Elizabeth C, Paz I Benjamin, Kruper Laura, Mortimer Joanne, Wong F Lennie, Bhatia Smita, Irwin Michael R, Behrendt Carolyn E

机构信息

Department of Population Sciences, City of Hope Comprehensive Cancer Center, USA.

Department of Supportive Care Medicine, City of Hope Comprehensive Cancer Center, USA.

出版信息

Brain Behav Immun Health. 2023 Jul 31;32:100670. doi: 10.1016/j.bbih.2023.100670. eCollection 2023 Oct.

Abstract

BACKGROUND

Behavioral symptoms in breast cancer (BC) survivors have been attributed to cancer treatment and resulting inflammation. However, studies linking behavioral symptoms to BC treatment have observed patients only after some treatment. Our prospective study with pre-treatment baseline investigates post-treatment changes in inflammation-related biomarkers and whether those changes correlate with changes in symptoms.

METHODS

Participants were postmenopausal women, newly-diagnosed with stage 0-3 BC before any treatment (n = 173 "patients"), and age-matched women without cancer (n = 77 "controls"), who were assessed on plasma markers [soluble tumor necrosis factor receptor type 2 (sTNF-RII), interleukin (IL)-6, IL-1 receptor antagonist (IL-1RA), C-reactive protein (CRP)]) and symptoms (Physical Functioning, Pain, Attention/concentration, Perceived Cognitive Problems, Fatigue, Sleep Insufficiency, Depression). Participants were assessed again 1 month, 1 year, and 2 years after completing primary treatment or similar interval in controls. Generalized linear mixed models tested 4 treatments (surgery alone or with chemotherapy, radiation, or both) for association with change per marker. Joint models tested change per marker for association with change per symptom. Models considered demographic, socioeconomic, and clinical covariates. False Discovery Rate method controlled risk of error from multiple hypotheses.

RESULTS

At one month post-completion of treatment, sTNF-RII and IL-6 were elevated by all BC treatments, as were IL-1RA and CRP after surgery alone (all, p < 0.05). By 1 year, markers' average values returned to baseline. Throughout 2-year follow-up, increase-from-baseline in sTNF-RII, IL-1RA, and IL-6 coincided with worsened Physical Functioning, and increase-from-baseline in sTNF-RII coincided with increased Pain (all, p < 0.01). These biomarker-symptom associations (excepting IL-6) were exclusive to patients. No other symptoms worsened, and baseline Fatigue and Depression improved in all participants.

CONCLUSIONS

BC treatment, even surgery, is associated with transient elevation in inflammatory markers. In patients post-treatment, increase-from-baseline in sTNF-RII accompanies increased Pain and decreased Physical Functioning, suggesting that sTNF-RII merits development as a clinical biomarker in BC patients.

摘要

背景

乳腺癌(BC)幸存者的行为症状被认为与癌症治疗及由此产生的炎症有关。然而,将行为症状与BC治疗联系起来的研究仅在患者接受部分治疗后对其进行观察。我们的前瞻性研究在治疗前设立基线,旨在调查治疗后炎症相关生物标志物的变化,以及这些变化是否与症状变化相关。

方法

参与者为绝经后女性,其中新诊断为0 - 3期BC且尚未接受任何治疗的患者有173名(“患者组”),年龄匹配的无癌女性有77名(“对照组”)。对这些参与者进行血浆标志物[可溶性肿瘤坏死因子受体2型(sTNF - RII)、白细胞介素(IL)- 6、IL - 1受体拮抗剂(IL - 1RA)、C反应蛋白(CRP)]和症状(身体功能、疼痛、注意力/集中力、认知问题感知、疲劳、睡眠不足、抑郁)的评估。在完成初始治疗后1个月、1年和2年对参与者进行再次评估,对照组则在相似时间间隔后进行评估。使用广义线性混合模型测试4种治疗方法(单纯手术或联合化疗、放疗或两者)与每个标志物变化的关联。联合模型测试每个标志物的变化与每个症状变化的关联。模型考虑了人口统计学、社会经济和临床协变量。错误发现率方法控制了多重假设产生的错误风险。

结果

在完成治疗后的1个月,所有BC治疗均使sTNF - RII和IL - 6升高,单纯手术后IL - 1RA和CRP也升高(均p < 0.05)。到1年时,标志物的平均值恢复到基线水平。在整个2年的随访中,sTNF - RII、IL - 1RA和IL - 6相对于基线的升高与身体功能恶化同时出现,sTNF - RII相对于基线的升高与疼痛增加同时出现(均p < 0.01)。这些生物标志物与症状的关联(IL - 6除外)仅在患者中存在。没有其他症状恶化,所有参与者的基线疲劳和抑郁症状有所改善。

结论

BC治疗,即使是手术,也与炎症标志物的短暂升高有关。在治疗后的患者中,sTNF - RII相对于基线的升高伴随着疼痛增加和身体功能下降,这表明sTNF - RII值得作为BC患者的临床生物标志物进行开发。

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