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英国生物银行队列中的长期病症、多病共存与结直肠癌风险

Long-term conditions, multimorbidity and colorectal cancer risk in the UK Biobank cohort.

作者信息

Corcoran Neave Me, Mair Frances S, Nicholl Barbara, Macdonald Sara, Jani Bhautesh Dinesh

机构信息

General Practice and Primary Care, Institute of Health and Wellbeing, University of Glasgow, Glasgow, UK.

出版信息

J Multimorb Comorb. 2022 Sep 15;12:26335565221110123. doi: 10.1177/26335565221110123. eCollection 2022 Jan-Dec.

Abstract

PURPOSE

Early identification of colorectal cancer (CRC) is an international priority. Multimorbidity (presence of ≥2 long-term conditions (LTCs)) is increasing and the relationship between CRC and LTCs is little-understood. This study explores the relationship between individual LTCs, multimorbidity and CRC incidence and mortality.

METHODS

Longitudinal analysis of the UK Biobank cohort, participants recruited 2006-2010; = 500,195; excluding previous CRC at baseline. Baseline data was linked with cancer/mortality registers. Demographic characteristics, lifestyle factors, 43 LTCs, CRC family history, non-CRC cancers, and multimorbidity count were recorded. Variable selection models identified candidate LTCs potentially predictive of CRC outcomes and Cox regression models tested for significance of associations between selected LTCs and outcomes.

RESULTS

Participants' age range: 37-73 (mean age 56.5; 54.5% female). CRC was diagnosed in 3669 (0.73%) participants, and 916 (0.18%) died from CRC during follow-up (median follow-up 7 years). CRC incidence was higher in the presence of heart failure (Hazard Ratio (HR) 1.96, 95% Confidence Interval (CI) 1.13-3.40), diabetes (HR 1.15, CI 1.01-1.32), glaucoma (HR 1.36, CI 1.06-1.74), male cancers (HR 1.44, CI 1.01-2.08). CRC mortality was higher in presence of epilepsy (HR 1.83, CI 1.03-3.26), diabetes (HR 1.32, CI 1.02-1.72), osteoporosis (HR 1.67, CI 1.12-2.58). No significant association was found between multimorbidity (≥2 LTCs) and CRC outcomes.

CONCLUSIONS

The associations of certain LTCs with CRC incidence and mortality has implications for clinical practice: presence of certain LTCs in patients presenting with CRC symptoms could trigger early investigation and diagnosis. Future research should explore causative mechanisms and patient perspectives.

摘要

目的

早期识别结直肠癌(CRC)是一项国际重点工作。多重疾病(存在≥2种长期病症(LTCs))的情况日益增多,而CRC与LTCs之间的关系却鲜为人知。本研究探讨个体LTCs、多重疾病与CRC发病率和死亡率之间的关系。

方法

对英国生物银行队列进行纵向分析,研究对象为2006年至2010年招募的参与者;n = 500,195;排除基线时已患CRC的患者。将基线数据与癌症/死亡率登记册相链接。记录人口统计学特征、生活方式因素、43种LTCs、CRC家族史、非CRC癌症以及多重疾病计数。变量选择模型确定了可能预测CRC结局的候选LTCs,Cox回归模型检验所选LTCs与结局之间关联的显著性。

结果

参与者年龄范围为37 - 73岁(平均年龄56.5岁;54.5%为女性)。在随访期间,3669名(0.73%)参与者被诊断出患有CRC,916名(0.18%)死于CRC(中位随访时间7年)。存在心力衰竭(风险比(HR)1.96,95%置信区间(CI)1.13 - 3.40)、糖尿病(HR 1.15,CI 1.01 - 1.32)、青光眼(HR 1.36,CI 1.06 - 1.74)、男性癌症(HR 1.44,CI 1.01 - 2.08)时,CRC发病率较高。存在癫痫(HR 1.83,CI 1.03 - 3.26)、糖尿病(HR 1.32,CI 1.02 - 1.72)、骨质疏松症(HR 1.67,CI 1.12 - 2.58)时,CRC死亡率较高。未发现多重疾病(≥2种LTCs)与CRC结局之间存在显著关联。

结论

某些LTCs与CRC发病率和死亡率之间的关联对临床实践具有启示意义:出现CRC症状的患者若存在某些LTCs,可能会促使早期检查和诊断。未来的研究应探索因果机制以及患者的观点。

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