Pro-atherogenic medical conditions are associated with widespread regional brain metabolite abnormalities in those with alcohol use disorder

Author:

Durazzo Timothy C12ORCID,Kraybill Eric P1,Stephens Lauren H2,May April C12,Meyerhoff Dieter J34

Affiliation:

1. Mental Illness Research and Education Clinical Centers, VA Palo Alto Health Care System , 3801 Miranda Ave. (151Y), Palo Alto, CA 94304 , United States

2. Department of Psychiatry and Behavioral Sciences, Stanford University School of Medicine , 401 Quarry Road, Stanford, CA 94305 , United States

3. Center for Imaging of Neurodegenerative Diseases (CIND), San Francisco VA Medical Center , 4150 Clement St. (114M) San Francisco, CA 94121 , United States

4. Department of Radiology and Biomedical Imaging, University of California , 505 Parnassus St., San Francisco, CA 94143 , United States

Abstract

Abstract Aims Widespread brain metabolite abnormalities in those with alcohol use disorder (AUD) were reported in numerous studies, but the effects of the pro-atherogenic conditions of hypertension, type 2 diabetes mellitus, hepatitis C seropositivity, and hyperlipidemia on metabolite levels were not considered. These conditions were associated with brain metabolite abnormalities in those without AUD. We predicted treatment-seeking individuals with AUD and pro-atherogenic conditions (Atherogenic+) demonstrate lower regional metabolite markers of neuronal viability [N-acetylaspartate (NAA)] and cell membrane turnover/synthesis [choline-containing compounds (Cho)], compared with those with AUD without pro-atherogenic conditions (Atherogenic−) and healthy controls (CON). Methods Atherogenic+ (n = 59) and Atherogenic− (n = 51) and CON (n = 49) completed a 1.5 T proton magnetic resonance spectroscopic imaging study. Groups were compared on NAA, Cho, total creatine, and myoinositol in cortical gray matter (GM), white matter (WM), and select subcortical regions. Results Atherogenic+ had lower frontal GM and temporal WM NAA than CON. Atherogenic+ showed lower parietal GM, frontal, parietal and occipital WM and lenticular nuclei NAA level than Atherogenic− and CON. Atherogenic− showed lower frontal GM and WM NAA than CON. Atherogenic+ had lower Cho level than CON in the frontal GM, parietal WM, and thalamus. Atherogenic+ showed lower frontal WM and cerebellar vermis Cho than Atherogenic− and CON. Conclusions Findings suggest proatherogenic conditions in those with AUD were associated with increased compromise of neuronal integrity and cell membrane turnover/synthesis. The greater metabolite abnormalities observed in Atherogenic+ may relate to increased oxidative stress-related compromise of neuronal and glial cell structure and/or impaired arterial vasoreactivity/lumen viability.

Funder

National Institute of Drug Abuse

National Institute on Alcohol Abuse and Alcoholism

National Institutes of Health

Northern California Institute for Research and Education

San Francisco Veterans Administration (VA) Medical Center

VA Palo Alto Health Care System

Publisher

Oxford University Press (OUP)

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