Mediating and Moderating Effects of Plasma Proteomic Biomarkers on the Association Between Poor Oral Health Problems and Brain White Matter Microstructural Integrity: the UK Biobank Study

Overview

Journal Mol Psychiatry

Specialties Molecular Biology
Psychiatry

Date 2024 Jul 30

PMID 39080466

Authors

May A Beydoun

Hind A Beydoun

Yi-Han Hu

Zhiguang Li

Michael F Georgescu

Nicole Noren Hooten

Mustapha Bouhrara

Jordan Weiss

Lenore J Launer

Michele K Evans

Alan B Zonderman

Affiliations

Soon will be listed here.

Abstract

The plasma proteome can mediate associations between periodontal disease (Pd) and brain white matter integrity (WMI). We screened 5089 UK Biobank participants aged 40-70 years for poor oral health problems (POHP). We examined the association between POHP and WMI (fractional anisotropy (FA), mean diffusivity (MD), Intracellular Volume Fraction (ICVF), Isotropic Volume Fraction (ISOVF) and Orientation Diffusion (OD)), decomposing the total effect through the plasma proteome of 1463 proteins into pure mediation, pure interaction, neither, while adjusting for socio-demographic and cardiovascular health factors. Similarly, structural equations modeling (SEM) was conducted. POHP was more prevalent among men (12.3% vs. 9.6%), and was associated with lower WMI on most metrics, in a sex-specific manner. Of 15 proteins strongly associated with POHP, growth differentiation factor 15 (GDF15) and WAP four-disulfide core domain 2 (WFDC2; also known as human epididymis protein 4; HE4) were consistent mediators. Both proteins mediated 7-8% of total POHP effect on FA. SEM yielded significant total effects for FA, MD and ISOVF in full models, with %mediated by common latent factor (GDF15 and WFDC2) ranging between 13% (FA) and 19% (ISOVF). For FA, mediation by this common factor was found for 16 of 49 tract-specific and global mean metrics. Protein metabolism, immune system, and signal transduction were the most common pathways for mediational effects. POHP was associated with poorer WMI, which was partially mediated by GDF15 and WFDC2.

Citing Articles

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