MedPath

Hepatic Encephalopathy and Albumin Lasting Cognitive Improvement

Phase 2
Recruiting
Conditions
Hepatic Encephalopathy
Cirrhosis
Interventions
Drug: Albumin Infusion
Registration Number
NCT06052176
Lead Sponsor
Hunter Holmes Mcguire Veteran Affairs Medical Center
Brief Summary

Hypothesis: Improvement in cognitive dysfunction with IV albumin in patients with cirrhosis with prior HE and MHE lasts for several weeks after albumin infusion has ended, and is due to persistent improvement in inflammatory markers, endothelial dysfunction, albumin function and gut microbial changes.

This will be a single-arm, single-blind sequential trial of IV 25% albumin and IV saline over 8 weeks with biological sampling and cognitive and health related quality of life (HRQOL) testing with each subject acting as their own control.

Detailed Description

In outpatients with cirrhosis with prior HE who have cognitive impairment despite adequate therapy, how long the impact of albumin lasts and through which potential mechanism(s) needs to be determined.

A prior recent HEAL trial showed that patients with prior HE and current minimal hepatic encephalopathy (MHE) randomized to albumin experienced significant improvement in cognitive dysfunction and psychosocial quality of life. Moreover, these improvements persisted a week after the last albumin infusion, which was not seen in the placebo group. This was accompanied by an improvement in endothelial dysfunction, ischemia-modified albumin levels and inflammatory markers that persisted one week even after albumin discontinuation. The reported half-life of IV albumin is 2 weeks, but the function and the length of time of albumin's action in decompensated cirrhosis is lower, and further details surrounding albumin pharmacokinetics in this population remain unelucidated. The mechanisms and length of time albumin's potential improvement for patients with MHE after treatment discontinuation also require continued study.

Study design:

This will be a single-arm, single-blind sequential trial of IV 25% albumin and IV saline over 8 weeks with biological sampling and cognitive and health related quality of life (HRQOL) testing with each subject acting as their own control.

Th order of the albumin and placebo infusion and blind the infusions from the subjects and the assessors of the outcomes will be changed.

Recruitment & Eligibility

Status
RECRUITING
Sex
All
Target Recruitment
30
Inclusion Criteria
  • Age >18 years
  • Cirrhosis diagnosed using either (a) liver biopsy, (b) transient wave elastography (>20 KPa) (c) radiological evidence consistent with cirrhosis, (d) in a patient with chronic liver disease endoscopic or radiological evidence of varices (e), in a patient with chronic liver disease, platelet count <150,000/mm3 and AST/ALT ratio >1.
  • Cognitive impairment defined by MHE on psychometric hepatic encephalopathy score (PHES), critical flicker frequency (CFF), or EncephalApp Stroop
  • Prior HE controlled by lactulose or rifaximin for at least one month
  • Serum albumin <4gm/dl
Exclusion Criteria
  • Unclear diagnosis of cirrhosis
  • No prior overt HE
  • No cognitive impairment on the tests noted
  • Requiring regular albumin infusions within 3 months or anticipated during the study visit
  • Infection within a month
  • Allergies to albumin
  • Unlikely to be adherent to the study
  • Unable or unwilling to consent
  • West Haven Criteria>2
  • Alcohol abuse within 1 month
  • Serum albumin >4gm/dl
  • Congestive heart failure

Study & Design

Study Type
INTERVENTIONAL
Study Design
SEQUENTIAL
Arm && Interventions
GroupInterventionDescription
AlbuminAlbumin InfusionIV Albumin at 1.5g/kg ideal body weight
PlaceboAlbumin InfusionSaline given at the same volume as the albumin on visits the patients are assigned to it
Primary Outcome Measures
NameTimeMethod
Delta change in Psychometric Hepatic Encephalopathy Score (PHES) in Placebo phase vs Albumin phase4 weeks each

cognitive improvement (PHES score ranges from -15 to 5), higher is good

Secondary Outcome Measures
NameTimeMethod
Change in PROMIS-29 Placebo phase vs Albumin phase4 weeks each

Health-related quality of life change (Total PROMIS-29 score will be evaluated)

Change in endotoxin binding protein Placebo phase vs Albumin phase4 weeks each

Change in endotoxin binding protein will be recorded in the serum; higher is worse

Change in serum Short-chain fatty acids Placebo phase vs Albumin phase4 weeks each

Change in serum Short-chain fatty acids (acetate, propionate, butyrate will be recorded

Change in stool Short-chain fatty acids Placebo phase vs Albumin phase4 weeks each

Change in stool Short-chain fatty acids (acetate, propionate, butyrate will be recorded

Critical Flicker Frequency change in Placebo phase vs Albumin phase4 weeks each

cognitive improvement (Hz at which CFF is reached will be evaluated), higher is good

Change in stool bile acids Placebo phase vs Albumin phase4 weeks each

Change in stool bile acids (total, primary, secondary, conjugated/deconjugated) will be recorded

Change in serum bile acids Placebo phase vs Albumin phase4 weeks each

Change in serum bile acids (total, primary, secondary, conjugated/deconjugated) will be recorded

Change in stool bacterial alpha diversity Placebo phase vs Albumin phase4 weeks each

Change in Shannon diversity of stool bacteria

Change in serum inflammatory cytokines Placebo phase vs Albumin phase4 weeks each

Change in IL-6, TNF-α, IL-10, IL-1β in serum

EncephalApp Stroop change in Placebo phase vs Albumin phase4 weeks each

cognitive improvement (Stroop OffTime+OnTime in seconds will be evaluated); higher is worse

Change in MELD-Na score Placebo phase vs Albumin phase4 weeks each

Liver disease severity change using MELD-Na; higher is worse

Change in oxidized albumin Placebo phase vs Albumin phase4 weeks each

Change in oxidized albumin will be recorded in the serum ; higher is worse

Change in Sickness Impact Profile Placebo phase vs Albumin phase4 weeks each

Health-related quality of life change (SIP total, psychosocial and physical scores where a higher score indicates poor HRQOL willl be evaluated)

Change in ischemia modified albumin Placebo phase vs Albumin phase4 weeks each

Change in ischemia modified albumin will be recorded in the serum

Trial Locations

Locations (1)

Hunter Holmes McGuire VA Medical Center

🇺🇸

Richmond, Virginia, United States

Related Trials

HEAL STUDY (Hepatic Encephalopathy and Albumin Study)

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Posted 7/12/2018
Updated 5/31/2022

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