Purpose

Nonalcoholic fatty liver disease (NAFLD) is now the most common liver disease worldwide and affects nearly 40% of obese youth and up to 10% of the general pediatric population. Some features of NAFLD are similar in children and adults, yet fibrosis and inflammation are more common in the portal zone and occur earlier in pediatric NAFLD patients than adults. This portends a rapid progression to end-stage liver disease in early adulthood. For the majority of children with NAFLD, mechanisms driving the origin and rapid progression of disease remain unknown. Thus, there is a critical, unmet need to study the specific underlying patterns of metabolic and molecular changes in the liver underlying the development and progression unique to children with NAFLD. This proposal will test the hypotheses that children with NAFLD have excess glucose and lipid produced by the liver, that those events are regulated by specific variations in the amount and location of RNAs and proteins in liver, and that the concentration of specific micro-RNAs in the blood can be used as a biomarker for NAFLD in pediatric patients.

Conditions

Eligibility

Eligible Ages
Between 10 Years and 20 Years
Eligible Sex
All
Accepts Healthy Volunteers
Yes

Inclusion Criteria

  • Age: All participants must be 10.0 to 20.9 years old at the time of enrollment. - Sex: Male and Female participants are eligible. - Race/Ethnicity: Participants of all racial/ethnic identities will be recruited. - Body mass index (BMI): Participants must be either in the normal weight (NW control group) or obese [Ob control, nonalcoholic fatty liver disease (NALFD) groups] range for BMI percentile. BMI percentile will be calculated from age- and sex-specific growth charts for children. - NAFLD status: The NAFLD group participants will be eligible if they are scheduled for liver biopsy for clinical reasons and their histopathology report confirms a diagnosis of NAFLD. NW control, and Ob control, and Liver control participants must not have diagnosed NAFLD.

Exclusion Criteria

  • Chronic illness: Participants will not be able to participate if they have conditions that are likely to affect metabolic variables (either directly or due to required medications) or result in them being unable to complete the required tests. Such conditions could include, but are not limited to, untreated hypothyroidism or other endocrine disorders, rheumatoid arthritis requiring steroids or limiting mobility, cardiovascular disease, stroke, or cardiac failure, neurological disorders such as multiple sclerosis, cancer, liver diseases other than NAFLD (e.g., Wilson's disease), other organ disorders, or orthopedic conditions that limit physical activity. - Acute illness: Participants will not be able to participate if they develop acute conditions that are likely to affect metabolic outcomes (either directly or due to required medications) or result in them being unable to participate; e.g., respiratory illness, infectious disease, fever, accident resulting in bone fractures, myocardial infarction, major depression. If such conditions resolve and there are no longer risks or likelihood of adverse effect on the study outcomes, participants may be rescheduled for testing. - Medications and nutritional supplements: Medications, vitamins, or supplements that have known effects on the primary outcomes will be cause for exclusion. Examples include weight loss medications, glucocorticoids, or experimental medications used to correct a metabolic or hepatic condition. Medications used to control asthma, allergies, anxiety, depression, attention deficit disorder, menstrual cycle, hypothyroidism, gastric reflux, hypertension, and sleep will be allowed. Participants who are taking medications for treatment of acute illness or conditions such as cold, flu, injury, or infection will be rescheduled after they complete their treatment course. - Pregnancy: Evidence of pregnancy or intent to become pregnant during the study is cause for exclusion. - Smoking, alcohol abuse, or illicit drug abuse: Participants who smoke or have signs or symptoms of alcohol or substance abuse will be excluded.

Study Design

Phase
N/A
Study Type
Interventional
Allocation
Non-Randomized
Intervention Model
Parallel Assignment
Intervention Model Description
Cross-sectional design in which all participants receive all interventions in the form of short-term observations following oral consumption of test materials.
Primary Purpose
Basic Science
Masking
None (Open Label)

Arm Groups

ArmDescriptionAssigned Intervention
Experimental
NAFLD
Participants in the pediatric NAFLD clinic
  • Other: Oral sugar tolerance test
    Measurement of glucose and insulin for calculation of insulin sensitivity
  • Other: De novo lipogenesis test
    Oral consumption of deuterated water to measure incorporation of label into lipids
  • Other: Gluconeogenesis test
    Oral consumption of 13C-labeled glycerol to measure incorporation into glucose
Experimental
Ob control
Participants with obesity, without NAFLD
  • Other: Oral sugar tolerance test
    Measurement of glucose and insulin for calculation of insulin sensitivity
  • Other: De novo lipogenesis test
    Oral consumption of deuterated water to measure incorporation of label into lipids
  • Other: Gluconeogenesis test
    Oral consumption of 13C-labeled glycerol to measure incorporation into glucose
Experimental
NW control
Participants in the normal range for body weight, without NAFLD
  • Other: Oral sugar tolerance test
    Measurement of glucose and insulin for calculation of insulin sensitivity
  • Other: De novo lipogenesis test
    Oral consumption of deuterated water to measure incorporation of label into lipids
  • Other: Gluconeogenesis test
    Oral consumption of 13C-labeled glycerol to measure incorporation into glucose
Experimental
Liver control
Participants undergoing liver biopsy or liver surgery, without NAFLD
  • Other: Oral sugar tolerance test
    Measurement of glucose and insulin for calculation of insulin sensitivity
  • Other: De novo lipogenesis test
    Oral consumption of deuterated water to measure incorporation of label into lipids
  • Other: Gluconeogenesis test
    Oral consumption of 13C-labeled glycerol to measure incorporation into glucose

Recruiting Locations

University of Oklahoma Health Sciences Center
Oklahoma City, Oklahoma 73104
Contact:
Kevin Short, PhD
405-271-8001
kevin-short@ouhsc.edu

More Details

Status
Recruiting
Sponsor
University of Oklahoma

Study Contact

Kevin Short, PhD
405-271-8001
kevin-short@ouhsc.edu

Detailed Description

This project uses a cross-sectional design with a single testing period without a formal intervention (e.g., diet, drug, exercise) or natural follow-up period. Participants with nonalcoholic fatty liver disease (NAFLD), and age-matched control groups classified as either obese (Ob control) or normal weight (NW control) will complete all metabolic and descriptive tests, including blood analyses. The NAFLD group will also have a liver biopsy as part of their standard clinical care; a portion of the biopsy will be used for the research testing. The Ob and NW control groups will not undergo liver biopsy. To provide a set of reference liver samples to compare with the NAFLD group, we will enroll a "liver control" group, consisting of age-matched patients who are scheduled to have a cholecystectomy with liver biopsy or are undergoing liver resection for tumor removal.

Notice

Study information shown on this site is derived from ClinicalTrials.gov (a public registry operated by the National Institutes of Health). The listing of studies provided is not certain to be all studies for which you might be eligible. Furthermore, study eligibility requirements can be difficult to understand and may change over time, so it is wise to speak with your medical care provider and individual research study teams when making decisions related to participation.