Metabolomic Analysis Identifies Alterations of Amino Acid Metabolome Signatures in the Postmortem Brain of Alzheimer's Disease

Yoon Hwan Kim; Hyun Soo Shim; Kyoung Heon Kim; Junghee Lee; Bong Chul Chung; Neil W Kowall; Hoon Ryu; Jeongae Lee

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Metabolomic Analysis Identifies Alterations of Amino Acid Metabolome Signatures in the Postmortem Brain of Alzheimer's Disease

Author: Yoon Hwan KIM ¹ ; Hyun Soo SHIM ; Kyoung Heon KIM ; Junghee LEE ; Bong Chul CHUNG ; Neil W KOWALL ; Hoon RYU ; Jeongae LEE
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1. MolecularRecognition Research Center, Korea Institute of Science and Technology, Seoul 02792, Korea. frans@kist.re.kr
Publication Type:Original Article
Keywords: Alzheimer's disease; Metabolomics; Liquid chromatography mass spectrometry; Biomarkers; amino acid metabolism
MeSH: Alzheimer Disease; Amyloid; Biomarkers; Brain; Chromatography, Liquid; Humans; Hydrocortisone; Metabolism; Metabolome; Metabolomics; Models, Statistical; Neurosciences
From:Experimental Neurobiology 2019;28(3):376-389
CountryRepublic of Korea
Language:English
Abstract: Despite significant advances in neuroscience research over the past several decades, the exact cause of AD has not yet fully understood. The metabolic hypothesis as well as the amyloid and tau hypotheses have been proposed to be associated with AD pathogenesis. In order to identify metabolome signatures from the postmortem brains of sporadic AD patients and control subjects, we performed ultra performance liquid chromatography coupled with linear ion trap-Orbitrap mass spectrometer (UPLC-LTQ–Orbitrap-MS). Not only our study identified new metabolome signatures but also verified previously known metabolome profiles in the brain. Statistical modeling of the analytical data and validation of the structural assignments discovered metabolic biomarkers associated with the AD pathogenesis. Interestingly, hypotaurin, myo-inositol and oxo-proline levels were markedly elevated in AD while lutamate and N-acetyl-aspartate were decreased in the postmortem brain tissue of AD patients. In addition, neurosteroid level such as cortisol was significantly increased in AD. Together, our data indicate that impaired amino acid metabolism is associated with AD pathogenesis and the altered amino acid signatures can be useful diagnostic biomarkers of AD. Thus, modulation of amino acid metabolism may be a possible therapeutic approach to treat AD.