Abstract
Background: Lipid metabolite dysfunction makes a substantial contribution to the clinical signs and pathophysiology of Alzheimer’s disease (AD). It is unclear that the role of dyslipidemia in the promotion of neuropathological processes and brain functional impairment that subsequently facilitates the progression of AD.Methods: Lipid pathway-based polygenic scores and large-scale resting-state networks (RSNs), was constructed. Together with canonical correlation analysis (CCA) and support vector machine (SVM) model, to explore the effects of lipid-related polygenic scores and blood lipoproteins on the molecular biomarkers, cognitive function, as well as large-scale RSNs. Associations between lipid-related genetic scores, serum lipoproteins, cognitive function, CSF biomarkers and RSNs were examined.Results: Dynamic trajectory of large-scale RSNs was exhibited significantly differential connectivity within-network, one-versus-all-others-network, and pairwise between networks across the AD spectrum (ADS). Importantly, the summative effects of lipid-pathway genetic variants and lipoproteins significantly promoted the process of β-amyloid and Tau levels and cognitive decline, and preferentially targeted functional couplings within- and between RSNs in the ADS, supporting the hypothesis that abnormal lipid profiles in the AD pathogenesis via disrupting large-scale RSNs and accelerating molecular pathological processes, consequently exacerbating cognitive decline.Conclusions: Our findings reveal the importance of lipids in the pathogenesis of AD via disruption of RSNs and acceleration of molecular pathological processes, consequently exacerbating cognitive decline. These findings provide the potential lipid-associated neuroimaging biomarkers for ADS.
Identification of Abnormal Lipid Profiles Promote Cognitive Decline in Alzheimer's Disease Spectrum via Large-Scale Brain Connectivity