Cortical thickness is differently associated with ALDH2 rs671 polymorphism according to level of amyloid deposition

Author:

Cho Yong Hyuk,Lee Heirim,Kim Na-Rae,Choi Jin Wook,Roh Hyun Woong,Ha Jae Ho,Hong Chang Hyung,Seo Sang Won,Choi Seong Hye,Kim Eun-Joo,Kim Byeong C.,Kim Seong Yoon,Cheong Jaeyoun,Park Bumhee,Son Sang Joon

Abstract

AbstractAccumulating evidence indicates that amyloid-beta (Aβ) deposition and biogenic aldehyde accumulation contribute to the pathogenesis of neurodegenerative diseases. Human aldehyde dehydrogenase 2 (ALDH2) metabolizes biogenic aldehydes produced in the brain to prevent damage. However, r671G>A, a single nucleotide polymorphism of ALDH2, causes aldehyde accumulation and decreased ALDH2 activity. We aimed to investigate whether Aβ deposition and rs671 polymorphism have an interaction effect on cortical thickness (CTh). We grouped 179 participants in the Biobank Innovations for chronic Cerebrovascular disease With ALZheimer's disease Study as follows: amyloid (–) [A(–)] and amyloid (+) [A(+)] groups based on the Aβ deposition degree; A-carrier (AC) and GG (GG) groups based on the presence/absence of the rs671 A allele; and their combinations, i.e., A(–)AC, A(–)GG, A(+)AC, and A(+)GG groups. A multiple regression analysis identified nine regions of interest. Compared with the A(–)GG group, the A(–)AC group showed thinner CTh in all regions. There were no significant differences between the A(+)AC and A(+)GG groups. We observed an interaction effect of amyloid deposition and rs671 polymorphism on CTh. The CTh in the A(–) group appeared to be strongly influenced by rs671 polymorphism, which could have contributed to cortical thinning and biogenic aldehyde accumulation in the AC group. Additionally, CTh in the A(+) group appeared to be strongly influenced by amyloid deposition.

Funder

Biobank of Chronic Cerebrovascular Disease Consortium and biobank of Ajou University Hospital, a member of Korea Biobank Network

National Research Foundation of Korea

MD-Phd/Medical Scientist Training Program

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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1. Intracellular effects of lithium in aging neurons;Ageing Research Reviews;2024-08

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