Joint association of diabetes mellitus and inflammation status with biological ageing acceleration and premature mortality

IF 4.3 Q1 ENDOCRINOLOGY & METABOLISM

Diabetes & Metabolic Syndrome-Clinical Research & Reviews Pub Date : 2024-06-01 DOI:10.1016/j.dsx.2024.103050

Fan Tang , Shuang Yang , Hongbin Qiu , Yan Liu , Shaohong Fang , Yiying Zhang , Shanjie Wang

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引用次数: 0

Abstract

Background

We aimed to investigate the associations of diabetes mellitus (DM) and C-reactive protein (CRP) with biological ageing acceleration and mortality risk.

Methods

We analyzed data from 41,634 adults with CRP and DM at baseline. Subjects were categorized into high CRP (>3 mg/L) and low CRP (≤3 mg/L) groups. The cross-sectional endpoints of the study were biological ageing indicators Klemera-Doubal method BioAge acceleration (KDMAccel) and Phenotypic age acceleration (PhenoAgeAccel), and the follow-up endpoints were all-cause mortality and cardiovascular mortality.

Results

In adults with high CRP, compared with those without DM, PhenoAgeAccel increased by 1.66 years (95 % CI: 1.38–1.93), and 8.74 years (95 % CI: 8.25–9.22) in adults with prediabetes and DM, respectively (p for interaction <0.001). Using the CRP_low/non-DM group as a reference, adults in the CRP_high/non-DM, CRP_low/DM, and CRP_high/DM groups had significantly advanced biological ageing. Compared to adults without DM, low CRP, and no ageing acceleration, the multivariable-adjusted HRs (95%CIs) of all-cause and cardiovascular mortality in those with DM, CRP, and ageing acceleration were 3.22 (2.79–3.72), and 3.57 (2.81–4.54), respectively.

Conclusions

These findings suggest that the joint presence of low-grade inflammation and DM might be associated with higher odds of biological ageing acceleration and premature mortality.

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糖尿病和炎症状态与生物老化加速和过早死亡的联合关联

背景我们旨在研究糖尿病（DM）和C反应蛋白（CRP）与生物老化加速和死亡风险之间的关系。方法我们分析了41,634名基线CRP和DM的成年人的数据。受试者被分为高 CRP 组（3 毫克/升）和低 CRP 组（≤3 毫克/升）。研究的横断面终点是生物老化指标克莱默拉-杜巴法生物年龄加速度（KDMAccel）和表型年龄加速度（PhenoAgeAccel），随访终点是全因死亡率和心血管死亡率。结果在 CRP 偏高的成人中，与非 DM 患者相比，PhenoAgeAccel 在糖尿病前期和 DM 患者中分别增加了 1.66 年（95 % CI：1.38-1.93）和 8.74 年（95 % CI：8.25-9.22）（交互作用 p <0.001）。以CRP低/非DM组为参照，CRP高/非DM组、CRP低/DM组和CRP高/DM组的成年人的生物衰老明显提前。与无DM、低CRP和无老化加速的成年人相比，有DM、CRP和老化加速的成年人的全因死亡率和心血管死亡率的多变量调整HRs（95%CIs）分别为3.22（2.79-3.72）和3.57（2.81-4.54）。

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

Diabetes & Metabolic Syndrome-Clinical Research & Reviews ENDOCRINOLOGY & METABOLISM-

CiteScore

22.90

自引率

2.00%

发文量

248

审稿时长

51 days

期刊介绍： Diabetes and Metabolic Syndrome: Clinical Research and Reviews is the official journal of DiabetesIndia. It aims to provide a global platform for healthcare professionals, diabetes educators, and other stakeholders to submit their research on diabetes care. Types of Publications: Diabetes and Metabolic Syndrome: Clinical Research and Reviews publishes peer-reviewed original articles, reviews, short communications, case reports, letters to the Editor, and expert comments. Reviews and mini-reviews are particularly welcomed for areas within endocrinology undergoing rapid changes.