Myokines are associated with progression, course and mortality in alcohol‐associated liver disease

Author:

Kaur Parminder1,Verma Nipun1ORCID,Garg Pratibha1,Ralmilay Samonee1,Wadhawan Aishani1,Nadda Rohit1,Prajapati Jiya1,Sharma Gaurav2,Rathi Sahaj1ORCID,De Arka1ORCID,Premkumar Madhumita1ORCID,Taneja Sunil1ORCID,Singal Ashwani K.3ORCID,Duseja Ajay1ORCID

Affiliation:

1. Department of Hepatology Post Graduate Institute of Medical Education and Research Chandigarh India

2. Department of Translational and Regenerative Medicine Post Graduate Institute of Medical Education and Research Chandigarh India

3. University of Louisville School of Medicine Louisville Kentucky USA

Abstract

SummaryBackground and AimsMyokines are the muscle‐derived hormones orchestrating muscle and systemic health. Their role in the progression of alcohol‐associated liver disease (ALD) remains elusive.MethodsThree‐hundred‐one patients across the spectrum of ALD including fatty liver (FL, N = 13), compensated cirrhosis (CC, N = 17), non‐acute decompensation (NAD, N = 95), acute decompensation (AD, N = 51) and acute‐on‐chronic liver failure (ACLF, N = 125) were recruited between 2021 and 2023. Plasma myostatin, decorin levels, nutritional status, handgrip strength (HGS), systemic inflammation, infection, ammonia, disease course and 30‐day mortality were recorded.ResultsPatients aged 48 years (IQR: 38–52) and 97.7% of males were enrolled. Myostatin was elevated while decorin was reduced in cirrhosis compared to without cirrhosis, and further in DC compared to CC (p < 0.001). A step‐wise increase in myostatin and reduction in decorin was observed transitioning from NAD to AD to ACLF (p < 0.001). Myostatin was further increased and decorin was reduced along with the grades and organ failures in AD and ACLF (p < 0.001, each). Baseline decorin (AUC: 0.797) and its combination with MELD (AUC: 0.814) predicted disease resolution in AD and ACLF. Although, both myostatin (aOR: 18.96) and decorin (aOR: 0.02) could predict mortality, decorin was independent (aOR: 0.04) and additive to MELD (AUC of MELD+logDecorin + logTLC + HE‐grade:0.815); p < 0.05 each. Myostatin increased and decorin reduced with inflammation, hyperammonaemia, malnutrition and HGS in AD and ACLF (p < 0.05, each).ConclusionMyokines are linked with malnutrition, fibrosis, systemic inflammation, organ failures, disease course and mortality in ALD. Decorin enhances the risk estimation of mortality of MELD in AD and ACLF. Therapeutic modulation of myokines is a potentially disease‐modifying target in ALD.

Funder

Indian Council of Medical Research

Publisher

Wiley

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