The causal role of circulating immunity‐inflammation in preeclampsia: A Mendelian randomization

Xiaolei Xue; Chuanhui Guo; Cuifang Fan; Di Lei

doi:10.1111/jch.14775

The Journal of Clinical Hypertension (May 2024)

The causal role of circulating immunity‐inflammation in preeclampsia: A Mendelian randomization

Xiaolei Xue,
Chuanhui Guo,
Cuifang Fan,
Di Lei

Affiliations

Xiaolei Xue: Department of Obstetrics The Fifth Affiliated Hospital of Xinjiang Medical University Urumqi China
Chuanhui Guo: State Key Laboratory of Animal Biotech Breeding College of Biological Sciences China Agricultural University Beijing China
Cuifang Fan: Department of Obstetrics Renmin Hospital of Wuhan University Wuhan China
Di Lei: Department of Obstetrics Renmin Hospital of Wuhan University Wuhan China

DOI: https://doi.org/10.1111/jch.14775
Journal volume & issue: Vol. 26, no. 5
pp. 474 – 482

Abstract

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Abstract Patients with systemic autoimmune diseases, such as systemic lupus erythematosus, were at a higher risk for preeclampsia. The causal relationship between immunological inflammation and preeclampsia (PE) remains uncertain. We aimed to investigate the causal relationship between circulating immune inflammation and PE. Genetically predicted blood immune cells and circulating inflammatory proteins were identified using two genome‐wide association studies (GWAS). We used a two‐sample Mendelian randomization (MR) method to determine whether circulating immunological inflammation causes PE. Our findings indicated that ten immunophenotypes were identified to be significantly associated with PE risk: CD62L‐ Dendritic Cell Absolute Count, CD86+ myeloid Dendritic Cell %Dendritic Cell, CD62L‐ myeloid Dendritic Cell Absolute Count, CD86+ myeloid Dendritic Cell Absolute Count, CD62L‐ myeloid Dendritic Cell %Dendritic Cell, CD62L‐ CD86+ myeloid Dendritic Cell %Dendritic Cell, CD62L‐ CD86+ myeloid Dendritic Cell Absolute Count, CD16 on CD14+ CD16+ monocyte, HLA DR+ Natural Killer Absolute Count, and T cell Absolute Count. Ninety‐one inflammation‐related proteins had no statistically significant effect on PE following false discovery rate (FDR) correction. Certain proteins exhibited unadjusted low p‐values that merited mention. These proteins include interleukin‐10 (OR = 0.76, 95%CI = 0.63–0.93, p = .006), fibroblast growth factor 21 (OR = 1.23, 95%CI = 1.01–1.47, p = .035), and Caspase 8 (OR = 0.65, 95%CI = 0.50–0.85, p = .001). The ELISA analysis demonstrated elevated levels of FGF‐21 and decreased levels of IL‐10 and Caspase‐8 in the plasma of patients with PE. These findings reveal that immunophenotypes and circulating inflammatory proteins may induce PE, confirming the importance of peripheral Immunity‐Inflammation in PE. The discovery has the potential to lead to earlier detection and more effective treatment techniques.

Published in The Journal of Clinical Hypertension

ISSN: 1524-6175 (Print); 1751-7176 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the circulatory (Cardiovascular) system
Website: https://onlinelibrary.wiley.com/journal/17517176

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