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Integrated multi-omics reveals population-specific mechanisms of cardiovascular disease in high-altitude environments

  • Weiyu Meng
  • , Jiajun Yang
  • , Xi Wang
  • , Xiaobing Zhai
  • , Gang Luo
  • , Yuyang Sha
  • , Hongxin Pan
  • , Wei Xu
  • , Henry H.Y. Tong
  • , Edmundo Patricio Lopes Lao
  • , Ci ren Zhong-ga
  • , Song Cui
  • , Xiantao Song
  • , Kefeng Li

Research output: Contribution to journalArticlepeer-review

Abstract

High-altitude populations exhibit lower cardiovascular disease incidence and mortality with significant differences between indigenous highlanders and migrants. However, related genetic adaptation and population-specific mechanisms remain underexplored. We conducted a comprehensive multi-omics investigation of three cardiovascular disease patient cohorts from distinct altitudes: indigenous high-altitude residents (IHA, n = 31), high-altitude migrants (HAM, n = 18), and low-altitude residents (LAR, n = 50). IHA cardiovascular patients exhibited distinctive genetic signatures with significant enrichment of UGT1A family gene variants. Lipidomic profiling identified 118 differential lipid species between IHA and HAM patients, with significant enrichment in sphingolipid metabolism pathways. Integration of genomic and lipidomic data identified 102 significant gene-metabolite associations in IHA patients, particularly between UGT1A variants and sphingomyelin species. Comparative analysis with LAR patients revealed both shared and population-specific metabolic signatures. Our findings offer unique perspectives on cardiovascular disease in high-altitude environments, revealing complex interactions between genetic adaptation, environmental exposure, and disease pathophysiology.

Original languageEnglish
Article number115109
JournaliScience
Volume29
Issue number3
DOIs
Publication statusPublished - 20 Mar 2026

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

  1. SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well-being

Keywords

  • human physiology
  • omics

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