An Expert Consensus Delphi Panel in Metabolic Dysfunction- and Alcohol-associated Liver Disease: Opportunities and Challenges in Clinical Practice

Authors

Luis Antonio Diaz
Veeral Ajmera
Juan Pablo Arab
Daniel Q Huang
Cynthia Hsu
Brian P Lee
Alexandre Louvet
Maja Thiele
Federica Tavaglione
Monica Tincopa
Elisa Pose
Leon A Adams
William Alazawi
Marco Arrese
Ramon Bataller
Ajay Duseja
Suthat Liangpunsakul
Michael R Lucey
Philippe Mathurin
Jessica L. Mellinger, Henry Ford HealthFollow
Atsushi Nakajima
Vlad Ratziu
Nancy Reau
Mary E Rinella
Mark Thursz
Vincent Wai-Sun Wong
Patrick S Kamath
Rohit Loomba

Recommended Citation

Diaz LA, Ajmera V, Arab JP, Huang DQ, Hsu C, Lee BP, Louvet A, Thiele M, Tavaglione F, Tincopa M, Pose E, Adams LA, Alazawi W, Arrese M, Bataller R, Duseja A, Liangpunsakul S, Lucey MR, Mathurin P, Mellinger J, Nakajima A, Ratziu V, Reau N, Rinella ME, Thursz M, Wai-Sun Wong V, Kamath PS, and Loomba R. An Expert Consensus Delphi Panel in Metabolic Dysfunction- and Alcohol-associated Liver Disease: Opportunities and Challenges in Clinical Practice. Clin Gastroenterol Hepatol 2025.

Document Type

Article

Publication Date

4-30-2025

Publication Title

Clinical gastroenterology and hepatology

Abstract

BACKGROUND & AIMS: Metabolic dysfunction- and alcohol-associated liver disease (MetALD) is a recently defined entity for individuals with liver steatosis, metabolic dysfunction, and increased alcohol intake. However, the current definition of MetALD poses multiple challenges in clinical practice and research. In this Delphi consensus, we provide practical recommendations for the clinical assessment and management of MetALD to address current clinical challenges in MetALD.

METHODS: We used a modified Delphi process, including 2 surveys involving a panel of 28 experts from 10 countries spanning 4 continents. We predefined consensus as requiring an ≥80% agreement.

RESULTS: The panel reached consensus on 28 statements. Recommendations emphasize the importance of a comprehensive assessment of patients with presumed MetALD, including the quantification of alcohol intake using validated questionnaires and the use of objective biomarkers of alcohol use, such as phosphatidylethanol. The need to reassess metabolic risk factors and liver disease after a period of alcohol abstinence was highlighted to distinguish the primary driver of liver injury. Noninvasive tests were recommended to assess liver disease severity, whereas routine liver biopsy was deemed unnecessary unless other diagnoses were suspected. Comprehensive management strategies should involve multidisciplinary care focusing on lifestyle modifications, alcohol reduction or cessation, weight loss, and exercise. Finally, the panel identified significant gaps in knowledge, advocating for standardized research protocols, longitudinal studies, exploration of pathophysiological mechanisms to inform precision medicine approaches, and the validation of quantitative alcohol biomarkers for identifying MetALD.

CONCLUSIONS: This Delphi consensus provides clear recommendations for the clinical assessment and management of MetALD, addressing the unique challenges posed by this condition.

PubMed ID

40315973

ePublication

ePub ahead of print