A proteomic approach of biomarker candidate discovery for alcoholic liver cirrhosis

Krishna Sumanth Nallagangula; V Lakshmaiah; C Muninarayana; KV Deepa; KN Shashidhar

doi:10.33393/jcb.2018.2092

Authors

Krishna Sumanth Nallagangula Department of Biochemistry, Sri Devaraj Urs Medical College, SDUAHER, Kolar, Karnataka, India
V Lakshmaiah Department of Medicine, Sri Devaraj Urs Medical College, SDUAHER, Kolar, Karnataka, India
C Muninarayana Department of Community Medicine, Sri Devaraj Urs Medical College, SDUAHER, Kolar, Karnataka, India
KV Deepa Centre for Cellular and Molecular Platforms, GKVK Campus, Bengaluru, Karnataka, India
KN Shashidhar Department of Biochemistry, Sri Devaraj Urs Medical College, SDUAHER, Kolar, Karnataka, India

DOI:

https://doi.org/10.33393/jcb.2018.2092

Keywords:

Alcoholic liver cirrhosis, protein biomarker candidates, albumin depletion, two-dimensional electrophoresis, liquid chromatography–mass spectrometry

Abstract

Alcoholic liver disease (ALD) progresses from steatosis to alcoholic hepatitis to fibrosis and cirrhosis. Liver biopsy is considered as the gold standard method for diagnosis of liver cirrhosis and provides useful information about damaging process which is an invasive procedure with complications. Existing biomarkers in clinical practice have narrow applicability due to lack of specificity and lack of sensitivity. The objective of this article is to identify proteomic biomarker candidates for alcoholic liver cirrhosis by differential expression analysis between alcoholic liver cirrhotic and healthy subjects. Blood samples were collected from 20 subjects (10 alcoholic liver cirrhosis and 10 healthy) from R. L. Jalapa Hospital and Research Centre, Kolar, Karnataka, India. Differential protein analysis was carried out by two-dimensional electrophoresis after albumin depletion, followed by liquid chromatography–mass spectrometry. The image analysis found 46 spots in cirrhotic gel and 69 spots in healthy gel, of which 14 spots were identified with significant altered expression levels. Based on the protein score and clinical significance, among 14 spots, a total of 28 protein biomarker candidates were identified: 13 with increased expression and 15 with decreased expression were categorized in alcoholic liver cirrhosis compared to healthy subjects. Protein biomarker candidates identified by “-omics” approach based on differential expression between alcoholic liver cirrhotic subjects and healthy subjects may give better insights for diagnosis of ALD. Prioritization of candidates identified is a prerequisite for validation regimen. Biomarker candidates require verification that demonstrates the differential expression will remain detectable by assay to be used for validation.