Exploring Age and Gender Disparities in Cardiometabolic Phenotypes and Lipidomic Signatures Among Chinese Adults: A Nationwide Cohort Study

Authors

Xiaojing Jia
Hong Lin
Ruizhi Zheng
Shuangyuan Wang
Yilan Ding
Chunyan Hu
Mian Li
Yu Xu
Min Xu
Guixia Wang
Lulu Chen
Tianshu Zeng
Ruying Hu
Zhen Ye
Lixin Shi
Qing Su
Yuhong Chen
Xuefeng Yu
Li Yan
Tiange Wang
Zhiyun Zhao
Guijun Qin
Qin Wan
Gang Chen
Meng Dai
Di Zhang
Bihan Qiu
Xiaoyan Zhu
Jie Zheng
Xulei Tang
Zhengnan Gao
Feixia Shen
Xuejiang Gu
Zuojie Luo
Yingfen Qin
Li Chen
Xinguo Hou
Yanan Huo
Qiang Li
Yinfei Zhang
Chao Liu
Youmin Wang
Shengli Wu
Tao Yang
Huacong Deng
Jiajun Zhao
Yiming Mu
Shenghan Lai
Donghui Li
Weiguo Hu
Guang Ning
Weiqing Wang
Yufang Bi
Jieli Lu
4C Study Group

Publication Date

10-1-2024

Journal

Life Metabolism

Abstract

Understanding sex disparities in modifiable risk factors across the lifespan is essential for crafting individualized intervention strategies. We aim to investigate age-related sex disparity in cardiometabolic phenotypes in a large nationwide Chinese cohort. A total of 254,670 adults aged 40 years or older were selected from a population-based cohort in China. Substantial sex disparities in the prevalence of metabolic diseases were observed across different age strata, particularly for dyslipidemia and its components. Generalized additive models were employed to characterize phenotype features, elucidating how gender differences evolve with advancing age. Half of the 16 phenotypes consistently exhibited no sex differences, while four (high-density lipoprotein [HDL] cholesterol, apolipoprotein A1, diastolic blood pressure, and fasting insulin) displayed significant sex differences across all age groups. Triglycerides, apolipoprotein B, non-HDL cholesterol, and total cholesterol demonstrated significant age-dependent sex disparities. Notably, premenopausal females exhibited significant age-related differences in lipid levels around the age of 40-50 years, contrasting with the relatively stable associations observed in males and postmenopausal females. Menopause played an important but not sole role in age-related sex differences in blood lipids. Sleep duration also had an age- and sex-dependent impact on lipids. Lipidomic analysis and K-means clustering further revealed that 58.6% of the 263 measured lipids varied with sex and age, with sphingomyelins, cholesteryl esters, and triacylglycerols being the most profoundly influenced lipid species by the combined effects of age, sex, and their interaction. These findings underscore the importance of age consideration when addressing gender disparities in metabolic diseases and advocate for personalized, age-specific prevention and management.

Keywords

aging, lipidomics, metabolic diseases, modifiable risk factors, sex difference

DOI

10.1093/lifemeta/loae032

PMID

39872143

PMCID

PMC11749084

PubMedCentral® Posted Date

8-2-2024

PubMedCentral® Full Text Version

Post-print

Published Open-Access

yes