Actively Recruiting

Phase Not Applicable
Age: 21Years - 65Years
All Genders
NCT05166499

HMB Enriched Amino Acids to Reverse Muscle Loss in Cirrhosis

Led by The Cleveland Clinic · Updated on 2025-11-25

24

Participants Needed

1

Research Sites

265 weeks

Total Duration

On this page

AI-Summary

What this Trial Is About

Loss of skeletal muscle mass or sarcopenia is the most common and potentially reversible complication in cirrhosis that increases morbidity and mortality before, during and after liver transplantation. No proven treatments exist for the prevention or reversal of sarcopenia in cirrhosis, primarily because the mechanisms responsible for this are unknown. Based on compelling preliminary studies and those of the co investigator, investigators hypothesize that the mechanism of reduced skeletal muscle mass in cirrhosis is due to a myostatin mediated impaired mTOR (mechanistic target of rapamycin) signaling resulting in reduced protein synthesis and increased autophagy. Investigators further postulate that leucine, a direct stimulant of mTOR, will reverse the impaired mTOR phosphorylation in the skeletal muscle of cirrhotics. The consequent increase in protein synthesis reduced autophagy will result in an increase in skeletal muscle mass. Investigators will test these hypotheses by quantifying the response to acute and long term (3 month) administration of hydroxymethyl butyrate (HMB) enriched essential amino acid compared with an isonitrogenous isocaloric non-essential balanced amino acid mixture (does not stimulate protein synthesis) in cirrhotic patients. Fractional protein synthesis rate (FSR) in skeletal muscle, responses of the molecular regulatory pathways of skeletal muscle protein synthesis, and autophagy flux will be quantified in the acute and long term protocols. Tracer studies using L-\[D5\]-phenylalanine (Phe) as a primed constant infusion (prime 2µmol.kg-1.hr-1; constant 0.05 µmol.kg-1.hr-1) with and L \[ring-D2\] tyrosine, forearm plethysmography, and sequential skeletal muscle biopsies (total of 3 per study subject) will be used to quantify these outcomes. Anthropometric, clinical and body composition measures will be additional outcome measures for the long term intervention. Expression of regulatory signaling proteins, myostatin, IGF-1 (insulin like growth factor) , phospho-Akt, phospho-AMPK (activated protein kinase), phospho-mTOR and phospho-p70s6k will be quantified by Western immunoblots. Autophagy flux will be measured by quantifying expression of the autophagosome proteins.

CONDITIONS

Official Title

HMB Enriched Amino Acids to Reverse Muscle Loss in Cirrhosis

Who Can Participate

Age: 21Years - 65Years
All Genders

Eligibility Criteria

Eligible

You may qualify if you...

  • Diagnosis of cirrhosis of the liver
  • Child-Pugh score of 5-8
  • Age between 21 and 65 years
Not Eligible

You will not qualify if you...

  • Recent gastrointestinal bleeding (less than 3 months)
  • Active infection
  • Overt encephalopathy
  • Renal failure on dialysis
  • Pedal edema
  • Uncontrolled diabetes (HbA1C greater than 7.9 mg/dL)
  • Advanced cardiac, lung, or kidney disease
  • Metastatic cancer
  • Use of medications that alter muscle protein metabolism
  • Pregnancy
  • Recent bowel resection or gastric bypass surgery
  • INR greater than 1.7, platelets less than 60,000/ml, serum creatinine greater than 2 mg/dL
  • Use of medications that interfere with blood clotting

AI-Screening

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Trial Site Locations

Total: 1 location

1

Cleveland Clinic

Cleveland, Ohio, United States, 44195

Actively Recruiting

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Research Team

A

Annette Bellar

CONTACT

How is the study designed?

Study Type

INTERVENTIONAL

Masking

NONE

Allocation

RANDOMIZED

Model

PARALLEL

Primary Purpose

OTHER

Number of Arms

2

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HMB Enriched Amino Acids to Reverse Muscle Loss in Cirrhosis | DecenTrialz