Frontiers in Psychiatry (Apr 2023)

Serum metabolomics analysis in patients with alcohol dependence

  • Yanjie Zhang,
  • Yanjie Zhang,
  • Yajun Sun,
  • Yajun Sun,
  • Qin Miao,
  • Qin Miao,
  • Shilong Guo,
  • Qi Wang,
  • Qi Wang,
  • Tianyuan Shi,
  • Tianyuan Shi,
  • Xinsheng Guo,
  • Xinsheng Guo,
  • Shuai Liu,
  • Shuai Liu,
  • Guiding Cheng,
  • Guiding Cheng,
  • Chuansheng Wang,
  • Chuansheng Wang,
  • Ruiling Zhang,
  • Ruiling Zhang

DOI
https://doi.org/10.3389/fpsyt.2023.1151200
Journal volume & issue
Vol. 14

Abstract

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ObjectiveAlcohol dependence (AD) is a chronic recurrent mental disease caused by long-term drinking. It is one of the most prevalent public health problems. However, AD diagnosis lacks objective biomarkers. This study was aimed to shed some light on potential biomarkers of AD patients by investigating the serum metabolomics profiles of AD patients and the controls.MethodsLiquid chromatography-mass spectrometry (LC–MS) was used to detect the serum metabolites of 29 AD patients (AD) and 28 controls. Six samples were set aside as the validation set (Control: n = 3; AD group: n = 3), and the remaining were used as the training set (Control: n = 26; AD group: n = 25). Principal component analysis (PCA) and partial least squares discriminant analysis (PCA-DA) were performed to analyze the training set samples. The metabolic pathways were analyzed using the MetPA database. The signal pathways with pathway impact >0.2, value of p <0.05, and FDR < 0.05 were selected. From the screened pathways, the metabolites whose levels changed by at least 3-fold were screened. The metabolites with no numerical overlap in their concentrations in the AD and the control groups were screened out and verified with the validation set.ResultsThe serum metabolomic profiles of the control and the AD groups were significantly different. We identified six significantly altered metabolic signal pathways, including protein digestion and absorption; alanine, aspartate, and glutamate metabolism; arginine biosynthesis; linoleic acid metabolism; butanoate metabolism; and GABAergic synapse. In these six signal pathways, the levels of 28 metabolites were found to be significantly altered. Of these, the alterations of 11 metabolites changed by at least 3-fold compared to the control group. Of these 11 metabolites, those with no numerical overlap in their concentrations between the AD and the control groups were GABA, 4-hydroxybutanoic acid, L-glutamic acid, citric acid and L-glutamine.ConclusionThe metabolite profile of the AD group was significantly different from that of the control group. GABA, 4-hydroxybutanoic acid, L-glutamic acid, citric acid, and L-glutamine could be used as potential diagnostic markers for AD.

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