Amelioration of systemic inflammation in advanced chronic liver disease upon beta-blocker therapy translates into improved clinical outcomes

Mathias Jachs; Lukas Hartl; Dunja Schaufler; Christopher Desbalmes; Benedikt Simbrunner; Ernst Eigenbauer; David Josef Maria Bauer; Rafael Paternostro; Philipp Schwabl; Bernhard Scheiner; Theresa Bucsics; Albert Friedrich Stättermayer; Matthias Pinter; Michael Trauner; Mattias Mandorfer; Thomas Reiberger

doi:10.1136/gutjnl-2020-322712

Amelioration of systemic inflammation in advanced chronic liver disease upon beta-blocker therapy translates into improved clinical outcomes

Gut. 2021 Sep;70(9):1758-1767. doi: 10.1136/gutjnl-2020-322712. Epub 2020 Nov 16.

Authors

Mathias Jachs^{1

2}, Lukas Hartl^{1

2}, Dunja Schaufler^{1

2}, Christopher Desbalmes^{1

2}, Benedikt Simbrunner^{1

2

3}, Ernst Eigenbauer⁴, David Josef Maria Bauer^{1

2}, Rafael Paternostro^{1

2}, Philipp Schwabl^{1

2

3}, Bernhard Scheiner^{1

2}, Theresa Bucsics^{1

2}, Albert Friedrich Stättermayer¹, Matthias Pinter¹, Michael Trauner¹, Mattias Mandorfer^{1

2}, Thomas Reiberger^{5

2

3}

Affiliations

¹ Internal Medicine III, Division of Gastroenterology and Hepatology, Medical University of Vienna, Vienna, Austria.
² Vienna Hepatic Hemodynamic Lab, Medical University of Vienna, Vienna, Austria.
³ Christian Doppler Laboratory for Portal Hypertension and Liver Fibrosis, Medical University of Vienna, Vienna, Austria.
⁴ IT4Science, Medical University of Vienna, Vienna, Austria.
⁵ Internal Medicine III, Division of Gastroenterology and Hepatology, Medical University of Vienna, Vienna, Austria thomas.reiberger@meduniwien.ac.at.

PMID: 33199442
DOI: 10.1136/gutjnl-2020-322712

Abstract

Objective: Systemic inflammation promotes the development of clinical events in patients with advanced chronic liver disease (ACLD). We assessed whether (1) non-selective beta blocker (NSBB) treatment initiation impacts biomarkers of systemic inflammation and (2) whether these changes in systemic inflammation predict complications and mortality.

Design: Biomarkers of systemic inflammation, that is, white blood cell count (WBC), C reactive protein (CRP), interleukin-6 (IL-6) and procalcitonin (PCT) were determined at sequential hepatic venous pressure gradient (HVPG) measurements without NSBB and under stable NSBB intake. The influence of NSBB-related changes in systemic inflammation on the risk of decompensation and liver-related death was analysed using competing risk regression.

Results: Our study comprised 307 stable patients with ACLD (Child-A: 77 (25.1%), Child-B: 161 (52.4%), Child-C: 69 (22.5%), median HVPG: 20 (IQR 17-24) mm Hg) including 231 (75.2%) with decompensated disease.WBC significantly decreased upon NSBB therapy initiation (median: -2 (IQR -19;+13)%, p=0.011) in the overall cohort. NSBB-related reductions of WBC (Child-C: -16 (-30;+3)% vs Child-B: -2 (-16;+16)% vs Child-A: +3 (-7;+13)%, p<0.001) and of CRP (Child-C: -26 (-56,+8)% vs Child-B: -16 (-46;+13)% vs Child-A: ±0 (-33;+33)%, p<0.001) were more pronounced in advanced stages of cirrhosis. The NSBB-associated changes in WBC correlated with changes in CRP (Spearman's ρ=0.228, p<0.001), PCT (ρ=0.470, p=0.002) and IL-6 (ρ=0.501, p=0.001), but not with changes in HVPG (ρ=0.097, p=0.088).An NSBB-related decrease in systemic inflammation (ie, WBC reduction ≥15%) was achieved by n=91 (29.6%) patients and was found to be an independent protective factor of further decompensation (subdistribution HR, sHR: 0.694 (0.49-0.98), p=0.038) in decompensated patients and of liver-related mortality in the overall patient cohort (sHR: 0.561 (0.356-0.883), p=0.013).

Conclusion: NSBB therapy seems to exert systemic anti-inflammatory activity as evidenced by reductions of WBC and CRP levels. Interestingly, this effect was most pronounced in Child-C and independent of HVPG response. An NSBB-related WBC reduction by ≥15% was associated with a decreased risk of further decompensation and death.

Keywords: cirrhosis; inflammation; portal hypertension.

Publication types

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

MeSH terms

Acute-On-Chronic Liver Failure / complications
Acute-On-Chronic Liver Failure / drug therapy*
Acute-On-Chronic Liver Failure / mortality
Adrenergic beta-Antagonists / therapeutic use*
C-Reactive Protein / analysis
Female
Humans
Inflammation / drug therapy*
Inflammation / etiology
Inflammation / mortality
Interleukin-6 / blood
Leukocyte Count
Male
Middle Aged
Procalcitonin / blood
Retrospective Studies

Substances

Adrenergic beta-Antagonists
IL6 protein, human
Interleukin-6
Procalcitonin
C-Reactive Protein