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肿瘤突变负担与肺癌中的抑郁:与炎症的关联。

Tumor Mutation Burden and Depression in Lung Cancer: Association With Inflammation.

机构信息

Department of Psychiatry and Behavioral Sciences, Memorial Sloan Kettering Cancer Center, New York, New York.

Department of Psychiatry and Behavioral Sciences, Emory University School of Medicine, Atlanta, Georgia; and.

出版信息

J Natl Compr Canc Netw. 2020 Apr;18(4):434-442. doi: 10.6004/jnccn.2019.7374.

DOI:10.6004/jnccn.2019.7374
PMID:32259781
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7327956/
Abstract

BACKGROUND

Patients with lung cancer with greater systemic inflammation have higher rates of depression. Tumor mutation burden (TMB) predicts immunotherapy response in patients with lung cancer and is associated with intratumoral inflammation, which may contribute to systemic inflammation and depression. This study evaluated whether higher TMB was associated with increased depression and systemic inflammation in patients with lung cancer.

PATIENTS AND METHODS

Patients with metastatic lung cancers were evaluated for depression severity using the Hospital Anxiety and Depression Scale. TMB was measured using the Memorial Sloan Kettering-Integrated Mutation Profiling of Actionable Cancer Targets. Inflammation was evaluated using C-reactive protein (CRP) level and neutrophil-to-lymphocyte ratio (NLR).

RESULTS

A total of 96 patients with adequate TMB testing were evaluated. The average number of mutations (TMB) was 10.8 (SD, 10.9). A total of 19% of patients endorsed clinically significant depression symptoms. TMB was significantly correlated with depression severity (r = 0.34; P=.001) and NLR (r = 0.37; P=.002) but not CRP level (r = 0.19; P=.07). TMB was also higher in patients receiving chemotherapy (mean, 12.0) and immunotherapy (mean, 14.4) versus targeted therapy (mean, 4.8). A multivariate model found that TMB (β = 0.30; P=.01) and CRP level (β = 0.31; P=.01) were independently associated with depression; there was no significant interaction effect of TMB × CRP and depression. A similar multivariate model showed no independent effect for NLR and depression (β = 0.16; P=.17) after accounting for TMB.

CONCLUSIONS

These data provide evidence for biologic depression risk in patients with lung cancer who have high levels of TMB. The underlying mechanism of the association is not clearly related to inflammation but warrants further analysis to broadly elucidate the mechanism of biologically derived depression in cancer.

摘要

背景

患有全身性炎症的肺癌患者抑郁发生率更高。肿瘤突变负担(TMB)可预测肺癌患者的免疫治疗反应,并且与肿瘤内炎症相关,这可能导致全身性炎症和抑郁。本研究评估了 TMB 较高是否与肺癌患者的抑郁和全身性炎症增加有关。

患者和方法

使用医院焦虑和抑郁量表评估转移性肺癌患者的抑郁严重程度。使用纪念斯隆凯特琳综合行动癌症靶基因突变分析测定 TMB。使用 C 反应蛋白(CRP)水平和中性粒细胞与淋巴细胞比值(NLR)评估炎症。

结果

共评估了 96 例 TMB 检测充分的患者。平均突变数(TMB)为 10.8(标准差,10.9)。19%的患者有临床显著的抑郁症状。TMB 与抑郁严重程度(r = 0.34;P =.001)和 NLR(r = 0.37;P =.002)显著相关,但与 CRP 水平无关(r = 0.19;P =.07)。接受化疗(平均 12.0)和免疫治疗(平均 14.4)的患者的 TMB 高于接受靶向治疗(平均 4.8)的患者。多变量模型发现,TMB(β=0.30;P =.01)和 CRP 水平(β=0.31;P =.01)与抑郁独立相关;TMB 和 CRP 与抑郁之间无显著交互作用。在考虑 TMB 后,类似的多变量模型显示 NLR 与抑郁无独立影响(β=0.16;P =.17)。

结论

这些数据为 TMB 水平较高的肺癌患者存在生物学抑郁风险提供了证据。关联的潜在机制与炎症无明显关系,但需要进一步分析以广泛阐明癌症中生物学来源的抑郁的机制。