Association between systemic inflammation biomarkers and incident cardiovascular disease in 423,701 individuals: evidence from the UK biobank cohort.

IF 8.5 1区医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

Cardiovascular Diabetology Pub Date : 2025-04-15 DOI:10.1186/s12933-025-02721-9

Pei Qin, Frederick K Ho, Carlos A Celis-Morales, Jill P Pell

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引用次数: 0

Abstract

Background: The associations between systemic inflammation biomarkers and cardiovascular disease (CVD) remain not well explored. This study aimed to investigate associations between different systemic inflammation biomarkers and incident CVD and main CVD subtypes - ischaemic heart disease (IHD), stroke, and heart failure - explore dose-response relationships, and compare their predictive performance.

Methods: This prospective cohort study included 423,701 UK Biobank participants free of CVD at baseline. Baseline neutrophil-to-lymphocyte ratio (NLR), lymphocyte-to-monocyte ratio (LMR), platelet-to-lymphocyte ratio (PLR), systemic immune-inflammation index (SII), and system inflammation response index (SIRI) were derived. Cox-proportional regression models were used to investigate the associations.

Results: NLR, PLR, SII, and SIRI was positively and LMR was negatively associated with all four of the outcomes investigated. The relationships were non-linear for all biomarkers with CVD and were linear for NLR, SII, and SIRI and non-linear for LMR and PLR with IHD, stroke and heart failure. Compared with the more established biomarkers, all four of the novel biomarkers had statistically superior predictive performance for three of the outcomes investigated (CVD, IHD and heart failure) and three of them were superior at predicting stroke. Compared to a model of CVD prediction with classical risk factors (C-index = 0.702), discrimination was improved on the addition of inflammation markers for CVD (C-index change 0.0069, 95% CI 0.0033 to 0.0107), IHD (C-index change 0.0054, 95% CI 0.0013 to 0.0095), and heart failure (C-index change 0.0153, 95% CI 0.0089 to 0.0218).

Conclusions: There were independent and dose-response relationships between the novel systemic inflammation biomarkers and CVD outcomes. Addition of the inflammation biomarkers including novel inflammation biomarkers showed improved discrimination of the traditional risk prediction model. With accumulated evidence, these biomarkers should be considered for inclusion in risk tools and prevention.

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423,701人的全身性炎症生物标志物与心血管疾病事件之间的关联：来自英国生物银行队列的证据

背景：全身性炎症生物标志物与心血管疾病（CVD）之间的关系尚未得到很好的探讨。本研究旨在探讨不同全身性炎症生物标志物与CVD和主要CVD亚型（缺血性心脏病（IHD）、中风和心力衰竭）发生之间的关系，探讨剂量-反应关系，并比较它们的预测性能。方法：这项前瞻性队列研究包括423,701名基线时无心血管疾病的英国生物银行参与者。得出基线中性粒细胞与淋巴细胞比值（NLR）、淋巴细胞与单核细胞比值（LMR）、血小板与淋巴细胞比值（PLR）、全身免疫炎症指数（SII）和系统炎症反应指数（SIRI）。使用cox -比例回归模型来调查相关性。结果：NLR、PLR、SII和SIRI与所有四项结果呈正相关，LMR与所有四项结果呈负相关。所有生物标志物与CVD的关系均为非线性，NLR、SII和SIRI的关系为线性，LMR和PLR与IHD、中风和心力衰竭的关系为非线性。与更成熟的生物标志物相比，所有四种新型生物标志物在统计上对所调查的三种结果（CVD， IHD和心力衰竭）的预测性能优越，其中三种生物标志物在预测中风方面优于其他生物标志物。与具有经典危险因素（C-index = 0.702）的CVD预测模型相比，加入炎症标志物对CVD （C-index变化0.0069,95% CI 0.0033 ~ 0.0107）、IHD （C-index变化0.0054,95% CI 0.0013 ~ 0.0095）和心力衰竭（C-index变化0.0153,95% CI 0.0089 ~ 0.0218）的鉴别能力得到了提高。结论：新型全身炎症生物标志物与CVD结局之间存在独立的剂量反应关系。包括新型炎症生物标志物在内的炎症生物标志物的加入提高了传统风险预测模型的辨别能力。随着证据的积累，应考虑将这些生物标志物纳入风险工具和预防。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cardiovascular Diabetology 医学-内分泌学与代谢

CiteScore

12.30

自引率

15.10%

发文量

240

审稿时长

1 months

期刊介绍： Cardiovascular Diabetology is a journal that welcomes manuscripts exploring various aspects of the relationship between diabetes, cardiovascular health, and the metabolic syndrome. We invite submissions related to clinical studies, genetic investigations, experimental research, pharmacological studies, epidemiological analyses, and molecular biology research in this field.