Immunotherapy targeting plasma ASM is protective in a mouse model of Alzheimer’s disease

Author:

Choi Byung Jo,Park Min Hee,Park Kang Ho,Han Wan Hui,Yoon Hee Ji,Jung Hye Yoon,Hong Ju Yeon,Chowdhury Md Riad,Kim Kyung Yeol,Lee Jihoon,Song Im-Sook,Pang Minyeong,Choi Min-Koo,Gulbins ErichORCID,Reichel Martin,Kornhuber JohannesORCID,Hong Chang-WonORCID,Kim Changho,Kim Seung HyunORCID,Schuchman Edward H.,Jin Hee KyungORCID,Bae Jae-sungORCID

Abstract

AbstractAcid sphingomyelinase (ASM) has been implicated in neurodegenerative disease pathology, including Alzheimer’s disease (AD). However, the specific role of plasma ASM in promoting these pathologies is poorly understood. Herein, we explore plasma ASM as a circulating factor that accelerates neuropathological features in AD by exposing young APP/PS1 mice to the blood of mice overexpressing ASM, through parabiotic surgery. Elevated plasma ASM was found to enhance several neuropathological features in the young APP/PS1 mice by mediating the differentiation of blood-derived, pathogenic Th17 cells. Antibody-based immunotherapy targeting plasma ASM showed efficient inhibition of ASM activity in the blood of APP/PS1 mice and, interestingly, led to prophylactic effects on neuropathological features by suppressing pathogenic Th17 cells. Our data reveals insights into the potential pathogenic mechanisms underlying AD and highlights ASM-targeting immunotherapy as a potential strategy for further investigation.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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