Your search keyword '"Alcoholic hepatitis"' showing total 3 results

1. Model of disease severity in alcoholic hepatitis and novel prognostic insights.

Author

Enciu, Vlad-Teodor, Ologeanu, Priscila Mădălina, Călin-Necula, Ana-Maria, Moldoveanu, Alexandru Constantin, Oprea-Călin, Gabriela, and Fierbinţeanu-Braticevici, Carmen

Subjects

DISEASE risk factors, ESOPHAGEAL varices, ALCOHOL drinking, HEPATITIS, LIVER failure

Abstract

Harmful alcohol consumption is one of the leading risk factors for global disease burden and injury condition, causing death and disability early in life, with over 3 million deaths worldwide every year. Alcoholic hepatitis (AH) is a clinical syndrome characterized by hepatic failure with recent onset of jaundice, consequence of a heavy chronic alcohol drinking. The disease severity ranges from mild to severe cases, with high short-term mortality. Individual variety regarding disease outcome and therapeutic response complicates the prognosis stratification. Thus, novel parameters and continuously sought for a better disease outcome assessment. To highlight new parameters that accurately assess 30-day mortality (short-term) in patients with AH and to develop a new severity score that uses readily available parameters accessible to any clinician. This is a prospective study on patients diagnosed with AH between 2022-2023. We identified 70 patients with AH who met the National Institute on Alcohol Abuse and Alcoholism (NIAAA) criteria for diagnosis after exclusion of patients with severe comorbidities that could influence disease outcome. Clinical and paraclinical parameters were assessed at least on admission and day 7. Mortality at 30-day was considered the endpoint. The database was composed using Microsoft Excel (Microsoft Corporation) and the data was analyzed using SPSS Statistics version 26 (IBM Corporation). A total of 70 patients were included in the study with a mortality at 30-days of 22.9% (n=16). The independent variables associated with increased short-term mortality identified using the univariate analysis were: fever, infection, esophageal varices, prothrombin time PT, INR, total bilirubin, CRP, LDH and CHI (creatinine height index). Using multivariate regression we determined a novel prognostic score, with criterion for retaining variable being p<0.05. Total bilirubin day 7, CRP, PT, fever and CHI resulted after the analysis and were included into a new mortality score. Our Prognostic Model Score obtained an area under the ROC of 0.950 (95% CI: 0.890-0.980, p<0.001), with a cut-off value of 13.75 (Sn=87.5%, Sp=91%). Regarding the consecrated prognostic scores, MDF and Lille score obtained good AUROCs=0.839 and 0.881, respectively (p<0.000), with cut-off values comparable with literature (MDF=34.35 vs 32) and (Lille=0.475 vs 0.450). The discriminatory power for ABIC (p=0.58), GAHS (p=0.16), MELD-Na (p=0.61) was not significant. We obtained a new prognostic score for the assessment of 30-day mortality in AH that includes markers of inflammation (CRP, fever) and markers of sarcopenia (CHI) along parameters of hepatic disfunction (total bilirubin and PT). Amongst consecrated prognostic models, MDF and Lille scores were representative for our study, while ABIC, GAHS and MELD-Na did not attain statistical significance. Our score is unique by the addition of CRP and this could prove to be a useful tool in AH severity stratification. [ABSTRACT FROM AUTHOR]

Published

2024

2. Hospital General de Mexico Researchers Report on Findings in Alcoholic Hepatitis (LILLE-4 vs. LILLE-7 to predict short-term mortality in patients with severe alcoholic hepatitis).

Subjects

HEPATITIS, RESEARCH personnel, DIGESTIVE system diseases, PEOPLE with alcoholism

Abstract

A recent study conducted at the Hospital General de Mexico aimed to determine if the Lille-4 model is equivalent to the Lille-7 model in predicting 28-day mortality in patients with severe alcoholic hepatitis. The study collected data from 327 patients and found that the Lille-7 model had the highest accuracy in predicting early mortality, with a sensitivity of 78% and specificity of 45%. The researchers concluded that total bilirubin should not be measured prematurely and that steroid therapy should be provided for up to 7 days to assess treatment response. This information may be useful for researchers and medical professionals studying and treating alcoholic hepatitis. [Extracted from the article]

Published

2024

3. IL-33/ST2 pathway regulates neutrophil migration and predicts outcome in patients with severe alcoholic hepatitis.

Author

Artru, Florent, Bou Saleh, Mohamed, Maggiotto, François, Lassailly, Guillaume, Ningarhari, Massih, Demaret, Julie, Ntandja-Wandji, Line-Carolle, Pais de Barros, Jean-Paul, Labreuche, Julien, Drumez, Elodie, Helou, Doumet Georges, Dharancy, Sébastien, Gantier, Emilie, Périanin, Axel, Chollet-Martin, Sylvie, Bataller, Ramon, Mathurin, Philippe, Dubuquoy, Laurent, and Louvet, Alexandre

Subjects

*HEPATITIS, *LIVER diseases, *ALCOHOL-induced disorders, *NEUTROPHILS, *CIRRHOSIS of the liver

Abstract

Severe alcoholic hepatitis (SAH) is associated with a high risk of infection. The IL-33/ST2 pathway is involved in sepsis control but data regarding its role in alcohol-related liver disease (ALD) are lacking. We aimed to characterize the role of IL-33/ST2 in the polymorphonuclear neutrophils (PMNs) of patients with ALD and SAH. Serum and circulating neutrophils were collected from patients with SAH, alcoholic cirrhosis and healthy controls. We quantified IL-33/ST2 pathway activity and CXCR2 at baseline and after exposure to IL-33. We also determined the migration capacity of PMNs. The decoy receptor of IL-33 (soluble ST2 [sST2]) was increased in SAH vs. cirrhosis and controls, demonstrating the defect in this pathway during ALD. The sST2 level was associated with response to treatment, 2-month survival, infection-free survival and probability of infection in SAH. Endotoxemia was weakly correlated with sST2. GRK2, a negative regulator of CXCR2, was overexpressed in PMNs of patients with SAH and cirrhosis and was decreased by IL-33. CXCR2 levels on PMNs were lower in SAH vs. cirrhosis and controls. Treatment with IL-33 partially restored CXCR2 expression in SAH and cirrhosis. PMN migration upon IL-8 was lower in patients with SAH and cirrhosis vs. controls. Treatment with IL-33 partially restored migration in those with SAH and cirrhosis. Interestingly, the migration capacity of PMNs and the response to IL-33 were enhanced in responders to corticosteroids (Lille <0.45) compared to non-responders. The IL33/ST2 pathway is defective in SAH and predicts outcome. This defect is associated with decreased CXCR2 expression on the surface of PMNs and lower migration capacity, which can be corrected by IL-33, especially in patients responding to steroids. These results suggest that IL-33 has therapeutic potential for SAH and its infectious complications. The neutrophils of patients with severe alcoholic hepatitis are associated with a defect in the IL-33/ST2 pathway. This defect is associated with lower migration capacities in neutrophils and a higher probability of getting infected. Administration of IL-33 to the neutrophils at least partly restores this defect and may be effective at reducing the risk of infection in patients with severe alcoholic hepatitis. • The IL-33/ST2 pathway is defective in the neutrophils of patients with severe alcoholic hepatitis. • This defect is associated with a higher risk of developing infection. • Dosage of the decoy receptor sST2 helps identify patients at risk of death and/or infection. • The defect in IL-33/ST2 in neutrophils is responsible for lower migration capacities. • Treating neutrophils with recombinant IL-33 restores, at least in part, their migration capacities. [ABSTRACT FROM AUTHOR]

Published

2020