Nonalcoholic steatohepatitis (or NASH) is known to be caused by deposition of fat in the liver and development of scarring. This condition occurs more frequently in overweight and obese persons. It is often associated with resistance to the actions of insulin hormone. Fat cells secrete a hormone called leptin. Recently, we have learned that obese or overweight persons make too much leptin, which may contribute to insulin resistance. Paradoxically, patients who do not have any fat cells, also have insulin resistance. In these patients, insulin resistance is caused by the absence of leptin and leptin replacement significantly improves insulin resistance and fat deposition in the liver. In an earlier study, we determined the leptin levels in patients with NASH and how these levels are related to body fat levels as well as responsiveness to insulin. We saw that a subgroup of patients with NASH have relatively low levels of leptin in contrast to the amount of body fat they had. We now would like to see if restoring leptin levels to normal will improve the disease process in these patients. Our study patients will be male patients, aged between 18 and 65 (inclusive), who do not have any other cause for their liver disease. We have put some restrictions in body size such that a spectrum of patients from normal weight to obese range would be included. They will also demonstrate low leptin levels (levels similar to only 25% of normal population). We will use a genetically engineered form of leptin manufactured by Amylin Inc. given via injections under the skin. We plan to continue therapy for a period of one year and evaluate the change in liver disease by a liver biopsy. We will also follow the metabolic parameters and body composition characteristics that we examined in our earlier study. We expect that patients with low blood leptin levels will show improvement in their liver disease and insulin resistance when their blood leptin levels are restored to normal.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
TREATMENT
Masking
NONE
Enrollment
9
0.1 mg/kg/day once a day via subcutaneous injections
University of Michigan
Ann Arbor, Michigan, United States
Non-alcoholic Steatohepatitis Score as Determined by Liver Histopathology at 12 Months
Non-alcoholic steatohepatitis (NASH) score after approximately one year of treatment with metreleptin. Total NASH scores can range from 0 to 14. The higher the NASH score the more severe the liver disease.
Time frame: 1 year
Body Weight at 12 Months
Body weight (kg) after one year of treatment on metreleptin for patients that completed 12 months of metreleptin treatment.
Time frame: 1 year
Liver Fat Percentage by Magnetic Resonance Imaging (MRI - Dixon Method) at 12 Months
For determination of hepatic fat content by MRI and MR spectroscopy in patients, a series of out-phase and in-phase MRI at multiple flip angles are used. By combination of out-phase and in-phase MRI at multiple flip-angles and TE times, relaxation-time effects can be removed to yield quantitative intra-hepatic (and other organs') fractional fat content throughout the liver in a few breath-hold intervals.
Time frame: 1 year
Liver Function Test: Alanine Aminotransferase (ALT) Values at 12 Months
ALT value in subjects that completed 12 months of metreleptin treatment.
Time frame: 1 year
Liver Function Test: Aspartate Aminotransferase (AST) Values at 12 Months
AST value in subjects that completed 12 months of metreleptin treatment.
Time frame: 1 year
Fasting Glucose Value at 12 Months
Fasting glucose value in subjects that completed 12 months of metreleptin treatment.
Time frame: 1 year
Fasting Triglycerides Value at 12 Months
Fasting triglyceride value in subjects that completed 12 months of metreleptin treatment.
Time frame: 1 year
Insulin Resistance: Homeostatic Model Assessment (HOMA) at 12 Months
HOMA values in subjects that completed 12 months of metreleptin treatment.
Time frame: 1 year
This platform is for informational purposes only and does not constitute medical advice. Always consult a qualified healthcare professional.