Proteomic signatures of pediatric cardiovascular and cardiometabolic traits demonstrate long-term modifiable drivers of adult disease

  1. Joshua M Landman
  2. Heather M Highland
  3. Andrew S Perry
  4. Annie G Howard
  5. Quanhu Sheng
  6. Anna Lorenz
  7. Alexandra B Palmer
  8. Shilin Zhao
  9. Wanying Zhu
  10. Xinruo Zhang
  11. Victoria L Buchanan
  12. Elizabeth G Frankel
  13. Rashedeh Roshani
  14. Alyssa Scartozzi
  15. Eric H Farber-Eger
  16. Mohammad Y Anwar
  17. Jessica K Sprinkles
  18. Ash Breidenbach
  19. Ting-Chen Wang
  20. Christine A Ballard
  21. Matthew Nayor
  22. Jaclyn Tamaroff
  23. Absalon Gutierrez
  24. Lauren E Petty
  25. Alexander S Petty
  26. Benjamin Lippi
  27. Lindsay Fernandez-Rhodes
  28. Hung-Hsin Chen
  29. Mohanraj Krishnan
  30. Mariaelisa Graff
  31. Katie A Meyer
  32. Miryoung Lee
  33. Kristin L Young
  34. Quinn Wells
  35. Jane E Freedman
  36. Eric R Gamazon
  37. Joseph B McCormick
  38. Susan P Fisher-Hoch
  39. Penny Gordon-Larsen
  40. Jennifer E Below
  41. Kari E North
  42. Ravi V Shah
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Abstract

While the earliest pathological signs of cardiovascular disease (CVD) emerge before age 20, current adult-based risk thresholds fail to identify a substantial fraction of high-risk children. With the rising prevalence of childhood obesity, the need for early and sensitive detection of cardiovascular-kidney-metabolic disease (CKMD) risk is paramount to enable timely intervention that can prevent the trajectory toward CVD in later life. To identify early accessible molecular biomarkers of CKMD in children, we measured 25 CKMD phenotypes, spanning liver, adipose, vascular, and dysglycemia traits, linked those to the circulating proteome and built a multi-protein signature of composite CKMD, leveraging data from 273 children and adolescents (13.1 ± 2.7 years; 53% females). We compared these results to the adult CKMD proteome, using data from 685 adults from the same community and 28,257 adults from the UK Biobank. The pediatric CKMD proteome was highly concordant with the adult CKMD proteome, reflecting known and novel mechanisms of pancreatic beta-cell health and insulin sensitivity, liver homeostasis, inflammation, and cholesterol metabolism. Similarly, multi-protein signatures of composite CKMD phenotypes in children were strongly associated with CKMD-related outcomes in both adult populations. Importantly, many proteins linked to pediatric CKMD were modifiable with GLP-1 receptor agonist therapy, associated with adult CKMD-related outcomes in a large-scale proteome-wide association study (PWAS), and exhibited significant variability during development (ages 4-24 years). These findings demonstrate that CKMD develops starting early in life-course continuum, with proteomic profiles linked to future irreversible CVD conditions emerging early in life when they may still be reversible. This highlights a critical opportunity to improve CVD-free longevity through precision medicine diagnosis and intervention in children and adolescents.

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  1. Version published to 10.1101/2025.10.27.25338754 on medRxiv