Association between plasma proteome and pulmonary heart disease: A two‐stage Mendelian randomization analysis

Author:

Li Shiyang123ORCID,Ding Haifeng4,Li Qi1,Zeng Xiaobin1,Zhang Yanyu5,Lai Chengyi6,Xie Xiaoshuang1,Tang Yongjiang6,Lan Jianjun12

Affiliation:

1. Division of Cardiology Panzhihua Central Hospital Panzhihua China

2. Dali University Dali China

3. Department of Genealogy Panzhihua Central Hospital Panzhihua China

4. Division of Cardiology The First Affiliated Hospital of Shihezi University Shihezi China

5. Clinical Laboratory Center Panzhihua Central Hospital Panzhihua China

6. Department of Vascular Diseases Panzhihua Central Hospital Panzhihua China

Abstract

AbstractPulmonary heart disease (PHD) involves altered structure and function of the right ventricle caused by an abnormal respiratory system that causes pulmonary hypertension. However, the association between changes in plasma proteomics and PHD remains unclear. Hence, we aimed to identify causal associations between genetically predicted plasma protein levels and PHD. Mendelian randomization was performed to test the target proteins associated with PHD. Summary statistics for the human plasma proteome and pulmonary heart disease were acquired from the UK Biobank (6038 cases and 426 977 controls) and the FinnGen study (6753 cases and 302 401 controls). Publicly available pQTLs datasets for human plasma proteins were obtained from a largescale genome‐wide association study in the INTERVAL study. The results were validated using a case–control cohort. We first enrolled 3622 plasma proteins with conditionally independent genetic variants; three proteins (histo‐blood group ABO system transferase, activating signal cointegration 1 complex subunit 1, and calcium/calmodulin‐dependent protein kinase I [CAMK1]) were significantly associated with the risk of pulmonary heart disease in the UK Biobank cohort. Only CAMK1 was successfully replicated (odds ratio: 1.1056, 95% confidence interval: 1.019–1.095, p = 0.0029) in the FinnGen population. In addition, the level of CAMK1 in 40 patients with PHD was significantly higher (p = 0.023) than that in the control group. This work proposes that CAMK1 is associated with PHD, underscoring the importance of the calcium signaling pathway in the pathophysiology to improve therapies for PHD.

Publisher

Wiley

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