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S100A8/A9 and Innate Immunity in Liver Disease

S

St George's, University of London

Status

Enrolling

Conditions

Cirrhosis, Liver
Infections
Liver Failure, Acute on Chronic
Ascites Hepatic
Immune Suppression

Study type

Observational

Funder types

Other

Identifiers

NCT05793983
285573 (Other Identifier)
2021.0073

Details and patient eligibility

About

This observational study evaluates the concentration of immune protein S100A8/A9 in different liver failure syndromes, its interaction with the immune system and validity as an immunotherapeutic target to improve survival in patients with advanced cirrhosis and/or acute on chronic liver failure.

Full description

A paradox exists in chronic liver disease whereby there is a general recognition that chronic inflammation is part of the pathophysiology, heightened when there is an acute deterioration and organ failure (acute-on-chronic liver failure), yet there is an increased susceptibility to infection due to a dysfunctional immune system, which is often the trigger for organ failure and the reason for death in these patients.

A danger signal reported in other inflammatory conditions called S100A8/A9 (calprotectin) is known to activate the immune system by production of pro-inflammatory cytokines but has also been observed to promote the development immunosuppressive signals (e.g. IL-10 and MDSCs).

In an attempt to explain this paradox in liver disease, this study proposes to identify at the cellular and molecular level, the triggers for S100A8/A9 production, how it varies with time in stable patients and those that have acute deteriorations including the development of organ failure, and its interaction with innate immune cells in the circulation and at tissue level.

By studying this, the Investigators hope to be able to identify immunotherapeutic targets and understand whether potential immunotherapy could be applied locally or systemically. The Investigators' observations in this study could provide the basis for the future development of clinical immunomodulating agents, which may ameliorate immunopathology, reduce susceptibility to infection and could reduce mortality in critically ill patients with liver disease. Findings in this study may also have more generalizable impact especially with the recent recognition in the COVID-19 pandemic that immunomodulatory therapies may improve the clinical outcomes of inflammatory phenotypes in virus-induced severe sepsis.

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Enrollment

100 estimated patients

Sex

All

Ages

18 to 80 years old

Volunteers

Accepts Healthy Volunteers

Inclusion criteria

A) Patients with acute or chronic liver disease:

  1. Presence of chronic liver disease, or cirrhosis due to any aetiology (latter based upon a histopathological diagnosis or compatible laboratory data and radiological findings)
  2. Acute alcoholic hepatitis (definition as per Crabb et al, 2016)35
  3. Acute liver failure due to any aetiology
  4. Acute-on-chronic liver failure (defined as per EASL-CLIF definition)17

B) Patients undergoing diagnostic or therapeutic abdominal paracentesis Patients with acute or chronic liver disease of any aetiology undergoing clinically-indicated paracentesis for ascites

C) Patients undergoing broncho-alveolar lavage

  1. Intubated patients with liver disease in intensive care
  2. Undergoing a bronchoscopy or a non-directed broncho-alveolar lavage as part of their routine clinical care

D) Patients with acute or chronic liver disease undergoing liver biopsy (percutaneous or transjugular) as routine part of their clinical care

E) Patients with portal hypertension (cirrhotic or non-cirrhotic) undergoing transjugular intrahepatic shunt (TIPSS) placement as part of their routine care

F) Patients with acute or chronic liver disease undergoing orthoptic liver transplantation

G) Patients undergoing surgical liver resection or hepatectomy for liver-related diseases

Control groups:

A) Patients with ascites without chronic liver disease:

  1. Absence of cirrhosis based on clinical, radiological or histopathological features, including patients with non-cirrhotic portal hypertension, cardiac ascites (ascites due to heart failure) or patients with chronic kidney disease undergoing continuous ambulatory peritoneal dialysis (CAPD)
  2. Presence of clinically significant ascites
  3. Undergoing diagnostic or therapeutic paracentesis

B) Patients with sepsis without acute or chronic liver disease

C) Patients with haemochromatosis without liver disease or end-organ damage who undergo regular venesection

D) Healthy subjects

Exclusion criteria

Age under 18 or over 80 Evidence of disseminated malignancy (isolated cancers including hepatocellular carcinoma are not an exclusion criteria) Patients with known immunodeficiency syndromes (e.g. HIV infection)

Trial design

100 participants in 11 patient groups

Patients with acute or chronic liver disease
Description:
1. Presence of chronic liver disease, or cirrhosis due to any aetiology (latter based upon a histopathological diagnosis or compatible laboratory data and radiological findings) 2. Acute alcoholic hepatitis 3. Acute liver failure due to any aetiology 4. Acute-on-chronic liver failure
Patients undergoing diagnostic or therapeutic abdominal paracentesis
Description:
Patients with acute or chronic liver disease of any aetiology undergoing clinically-indicated paracentesis for ascites
Patients undergoing broncho-alveolar lavage
Description:
1. Intubated patients with liver disease in intensive care 2. Undergoing a bronchoscopy or a non-directed broncho-alveolar lavage as part of their routine clinical care
Patients with acute or chronic liver disease undergoing liver biopsy
Patients with undergoing transjugular intrahepatic shunt (TIPSS) placement
Patients with acute or chronic liver disease undergoing orthoptic liver transplantation
Patients undergoing surgical liver resection or hepatectomy for liver-related diseases
Patients with ascites without chronic liver disease
Description:
1. Absence of cirrhosis based on clinical, radiological or histopathological features, including patients with non-cirrhotic portal hypertension, cardiac ascites (ascites due to heart failure) or patients with chronic kidney disease undergoing continuous ambulatory peritoneal dialysis (CAPD) 2. Presence of clinically significant ascites 3. Undergoing diagnostic or therapeutic paracentesis
Patients with sepsis without acute or chronic liver disease
Patients with haemochromatosis who undergo regular venesection
Healthy subjects

Trial contacts and locations

1

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Central trial contact

Arjuna Singanayagam, MBBS; PhD

Data sourced from clinicaltrials.gov

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