Dysregulated metabolites and lipids in serum of patients with acute hepatitis E: A longitudinal study

Author:

Khan Shaheen1,Kumar Yashwant2,Sharma Charu3,Gupta Sonu Kumar2,Goel Amit4ORCID,Aggarwal Rakesh4ORCID,Veerapu Naga Suresh1ORCID

Affiliation:

1. Virology Section, Department of Life Sciences Shiv Nadar Institution of Eminence Gautam Buddha Nagar India

2. Translational Health Science and Technology Institute NCR Biotech Science Cluster Faridabad India

3. Department of Mathematics Shiv Nadar Institution of Eminence Gautam Buddha Nagar India

4. Department of Gastroenterology Sanjay Gandhi Postgraduate Institute of Medical Sciences Lucknow India

Abstract

AbstractHepatitis E is a disease associated with acute inflammation of the liver. It is related to several dysregulated metabolic pathways and alterations in the concentration of several metabolites. However, longitudinal analysis of the alterations in metabolites and lipids is generally lacking. This study investigated the changes in levels of metabolites and lipids over time in sera from men with acute hepatitis E compared to healthy controls similar in age and gender. Untargeted measurement of levels of various metabolites and lipids was done using mass spectrometry on 65 sera sequentially sampled from 14 patients with acute hepatitis E and 25 serum samples from five controls. Temporal changes in intensities of metabolites and lipids were determined over different times at 3‐day periods for the hepatitis E virus (HEV) group. In carbohydrate metabolism, glucose levels, fructose 1‐6‐bisphosphate and ribulose‐5‐phosphate were increased in the HEV‐infected persons compared to the healthy controls. HEV infection is significantly associated with decreased levels of inosine, guanosine, adenosine and urate in purine metabolism and thymine, uracil and β‐aminoisobutyrate in pyrimidine metabolism. Glutamate, alanine and valine levels were significantly lower in the HEV group than in healthy individuals. Homogentisate of tyrosine metabolism and cystathionine of serine metabolism were increased, whereas kynurenate of tryptophan metabolism decreased in the HEV group. Metabolites of the bile acid biosynthesis, urea cycle (arginine and citrulline) and ammonia recycling (urocanate) were significantly altered. Co‐enzymes, pantothenate and pyridoxal, and co‐factors, lipoamide and FAD, were elevated in the HEV group. The acylcarnitines, sphingomyelins, phosphatidylcholine (PC), phosphatidylethanolamine (PE), lysoPC and lysoPE tended to be lower in the HEV group. In conclusion, acute hepatitis E is associated with altered metabolite and lipid profiles, significantly increased catabolism of carbohydrates, purines/pyrimidines and amino acids, and decreased levels of several glycerophospholipids.

Funder

Indian Council of Medical Research

Publisher

Wiley

Subject

Virology,Infectious Diseases,Hepatology

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