Serum keratin-18 detects hepatic inflammation and predicts progression in compensated alcohol-associated liver disease

Katrine Holtz Thorhauge; Maja Thiele; Sönke Detlefsen; Ditlev Nytoft Rasmussen; Stine Johansen; Bjørn Staehr Madsen; Steen Antonsen; Lars Melholt Rasmussen; Katrine Prier Lindvig; Aleksander Krag

doi:10.1002/hep4.2075

Serum keratin-18 detects hepatic inflammation and predicts progression in compensated alcohol-associated liver disease

Hepatol Commun. 2022 Dec;6(12):3421-3432. doi: 10.1002/hep4.2075. Epub 2022 Oct 20.

Authors

Katrine Holtz Thorhauge^{1

2}, Maja Thiele^{1

2

3}, Sönke Detlefsen^{2

4}, Ditlev Nytoft Rasmussen^{1

2}, Stine Johansen^{1

2}, Bjørn Staehr Madsen^{1

2}, Steen Antonsen⁵, Lars Melholt Rasmussen^{2

6}, Katrine Prier Lindvig^{1

2}, Aleksander Krag^{1

2}

Affiliations

¹ Department of Gastroenterology and Hepatology, Odense University Hospital, Odense, Denmark.
² Institute for Clinical Research, University of Southern Denmark, Odense, Denmark.
³ Odense Patient data Exploratory Network, Odense University Hospital, Odense, Denmark.
⁴ Department of Pathology, Odense University Hospital, Odense, Denmark.
⁵ Department of Clinical Biochemistry, Odense University Hospital, Svendborg, Denmark.
⁶ Department of Clinical Biochemistry and Pharmacology, Odense University Hospital, Odense, Denmark.

Abstract

Alcohol-associated liver fibrosis accumulates over decades, driven by hepatic inflammation and cell death. We investigated the diagnostic accuracy of keratin-18 degradation, measured using serum M30 and M65 levels, and the ActiTest for hepatic inflammatory activity in patients with compensated alcohol-associated liver disease (ALD). Furthermore, we evaluated the prognostic accuracy of markers for liver-related events and all-cause mortality. All findings were compared with routine liver function tests: Aspartate aminotransferase (AST), alanine aminotransferase (ALT), and gamma-glutamyltransferase. Our prospective, biopsy-controlled, single-center study included 265 patients with ongoing or prior excessive alcohol intake, representing the full spectrum of compensated ALD. We defined hepatic inflammatory activity as a combined score of lobular inflammation and ballooning. For severe hepatic inflammatory activity (n = 40), we found excellent diagnostic accuracy for M30 (area under the receiver operating characteristics curve [AUROC] = 0.90), M65 (AUROC = 0.86), and AST (AUROC = 0.86). Elevated M30 (M30 > 240 U/L) had the highest positive predictive value (PPV) and specificity, significantly higher than M65, ActiTest and ALT, but not AST (M30: sensitivity = 83%, specificity = 82%, positive predictive value = 45%, negative predictive value = 95%). Patients were followed up for 1445 patient-years. All markers, except for ALT, significantly predicted liver-related events and all-cause mortality. After adjusting for advanced fibrosis, drinking behavior and body mass index, M30 and M65 remained significant predictors of liver-related events, whereas M30 and AST were significant predictors of all-cause mortality. Conclusion: M30 and AST accurately detect severe hepatic inflammatory activity in patients with compensated ALD. M30 was the only significant predictor of both liver-related events and all-cause mortality after adjusting for advanced fibrosis, body mass index, and drinking behavior at inclusion.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Biomarkers / blood
Ethanol
Humans
Inflammation / diagnosis
Keratin-18* / blood
Liver Cirrhosis / diagnosis
Liver Diseases, Alcoholic* / diagnosis
Prospective Studies

Substances

Biomarkers
Ethanol
Keratin-18