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Study of Human Non-Shivering Thermogenesis and Basal Metabolic Rate

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ClinicalTrials.gov Identifier: NCT01950520
Recruitment Status : Recruiting
First Posted : September 25, 2013
Last Update Posted : December 4, 2019
Sponsor:
Information provided by (Responsible Party):
National Institutes of Health Clinical Center (CC) ( National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) )

Tracking Information
First Submitted Date September 21, 2013
First Posted Date September 25, 2013
Last Update Posted Date December 4, 2019
Actual Study Start Date February 15, 2014
Estimated Primary Completion Date February 2, 2021   (Final data collection date for primary outcome measure)
Current Primary Outcome Measures
 (submitted: November 23, 2019)
Pharmacological effects on non-shivering thermogenesis [ Time Frame: 12 months ]
It is envisioned that this study will further our knowledge of the mechanisms that regulate the acute adaptive changes in resting energy expenditure and the effects of drug therapy targeting obesity in humans. Since the principal physiologic stimulus to BAT (and possibly muscle for NST) is via the sympathetic nervous system (SNS), b-adrenergic receptors may hold key roles in regulating human EE. We hypothesize that, by careful measurements of NST (at an individually-titrated cool environmental temperature, between 18-21 C vs. at thermoneutrality of 27 C) and using b-adrenergic drugs that differ in receptor specificity and agonist/antagonist properties, we will gain better understanding of the regulation of human NST.
Original Primary Outcome Measures
 (submitted: September 21, 2013)
Pharmacological effects on non-shivering thermogenesis [ Time Frame: ongoing ]
Change History
Current Secondary Outcome Measures
 (submitted: November 23, 2019)
  • Shivering thresholds [ Time Frame: 12 months ]
    We hypothesize that, by careful measurements of NST (at an individually-titrated cool environmental temperature, between 18-21 C vs. at thermoneutrality of 27 C) and using b-adrenergic drugs that differ in receptor specificity and agonist/antagonist properties, we will gain better understanding of the regulation of human NST.
  • To compare the effects of mirabegron at 0mg, 50mg, and 200mg on BAT metabolic activity. [ Time Frame: 12 months ]
    Since the principal physiologic stimulus to BAT (and possibly muscle for NST) is via the sympathetic nervous system (SNS), beta adrenergic receptors may hold key roles in regulating human EE. We hypothesize that, by careful measurements of NST (at an individually-titrated cool environmental temperature, between 18-21 degrees C vs. at thermoneutrality of 27 degrees C) and using beta- adrenergic drugs that differ in receptor specificity and agonist/antagonist properties, we will gain better understanding of the regulation of human NST as well as further evaluation of the pharmacological activation of human BAT.
Original Secondary Outcome Measures Not Provided
Current Other Pre-specified Outcome Measures Not Provided
Original Other Pre-specified Outcome Measures Not Provided
 
Descriptive Information
Brief Title Study of Human Non-Shivering Thermogenesis and Basal Metabolic Rate
Official Title The Mechanism of Human Non-Shivering Thermogenesis and Basal Metabolic Rate
Brief Summary

Background:

- Changes in how a person s body burns energy or calories can affect their weight over time. The lowest level of energy the body needs to function is called basal metabolic rate. In the cold, we burn extra energy, even before we start to shiver. This is called non-shivering thermogenesis and it occurs in different types of tissue such as muscle and fat. Researchers want to learn more about this type of energy burning and how it is regulated. They hope this will help treat obesity in the future.

Objectives:

  • Sub-study 1: to better understand how non-shivering thermogenesis works.
  • Sub-study 2: to measure the effects of anti-obesity drugs on basal metabolic rate.
  • Sub-study 3: to better understand the effects of mirabegron, a beta-3 adrenergic receptor agonist, on brown fat activity.

Eligibility:

- Healthy, lean adult males ages 18 to 35.

Design:

  • Participants will be screened with medical history, physical exam, blood test, and EKG.
  • For sub-studies 1 and 2:

    • Participants will receive one X-ray scan.
    • Each day, all participants will:

<TAB>- Have height and weight measured, and have urine collected.

  • Spend 4 hours in a temperature-controlled room with furniture, toilet area, phone, and computer. They will wear small non-invasive devices to monitor activity, heart rate, temperature, and shivering.

<TAB>- Walk for 30 minutes.

-For sub-study 3:

  • Participants will receive one DXA scan and up to 4 PET/CT scans and 4 MRIs
  • Each stay, all participants will:

<TAB>- Have height and weight measured, and have urine collected.

  • Spend 6 hours in a temperature-controlled room with furniture, toilet area, phone, and computer. They will wear small non-invasive devices to monitor activity, heart rate, temperature, and shivering.
  • Participants will be compensated for their time and participation at the end of the study
Detailed Description

The balance between energy expenditure (EE) and energy intake ultimately determines body weight. Resting EE is the major component (60-75%) of total EE in an adult human being. Resting EE dynamically adapts to environmental changes such as ambient temperature. In our on-going study of environmental temperature changes within and around the thermoneutral zone, we observed that healthy young men can increase EE by 17 % of the basal metabolic rate through the process of non-shivering thermogenesis (NST). This capacity for NST is unexpectedly large as compared to prior reports of mild cold-induced thermogenesis (3 to 11%) and suggests that increasing NST could be explored as an intervention to combat obesity.

The aim of this study is to better understand the physiology of NST and to develop improved assays for evaluating the effect of drugs that alter EE. For example, only recently has it been realized that brown adipose tissue is functional in adult humans and that white adipose tissue can be converted to brown-adipose-like tissue to increase heat production during cold exposures. Moreover, skeletal muscle likely also plays a role in cold-induced thermogenesis even before overt shivering occurs. It is plausible that the mechanisms governing heat production for NST contribute to regulation of body weight and thus may be contributing to the current obesity epidemic: even small changes in EE, if not compensated by changes in food intake, can have long-term effects on body weight.

This protocol has two phases. The first uses a pharmacologic approach to investigate the mechanism of NST in young healthy lean males. Since the principal physiologic stimulus to BAT (and possibly muscle for NST) is via the sympathetic nervous system (SNS), b-adrenergic receptors may hold key roles in regulating human EE. We hypothesize that, by careful measurements of NST (at an individually-titrated cool environmental temperature, between 18-21 C vs. at thermoneutrality of 27 C) and using b-adrenergic drugs that differ in receptor specificity and agonist/antagonist properties, we will gain better understanding of the regulation of human NST.

The second phase of the study focuses on measuring of FDA-approved drugs (such as aitu-obesity drugs) potential effect on basal metabolic rate (BMR) under thermoneutral conditions. The rationale is that previous studies of drug effect on EE in humans have not always rigorously enforced the use of thermoneutral conditions, thus may have increased variability and underestimated the effect, contributing to inconclusive findings.

It is envisioned that this study will further our knowledge of the mechanisms that regulate the acute adaptive changes in resting energy expenditure and the effects of drug therapy targeting obesity in humans.

Study Type Observational
Study Design Observational Model: Cohort
Time Perspective: Prospective
Target Follow-Up Duration Not Provided
Biospecimen Not Provided
Sampling Method Non-Probability Sample
Study Population Healthy, lean adult males ages 18 to 35
Condition Healthy Volunteers
Intervention Not Provided
Study Groups/Cohorts
  • Sub-study 1
    to better understand how non-shivering thermogenesis works
  • Sub-study 2
    to measure the effects of anti-obesity drugs on basal metabolic rate
  • Sub-study 3
    to better understand the effects of mirabegron, a beta-3 adrenergic receptor agonist, on brown fat activity
Publications *

*   Includes publications given by the data provider as well as publications identified by ClinicalTrials.gov Identifier (NCT Number) in Medline.
 
Recruitment Information
Recruitment Status Recruiting
Estimated Enrollment
 (submitted: May 20, 2015)
134
Original Estimated Enrollment
 (submitted: September 21, 2013)
50
Estimated Study Completion Date February 2, 2021
Estimated Primary Completion Date February 2, 2021   (Final data collection date for primary outcome measure)
Eligibility Criteria
  • INCLUSION CRITERIA:
  • Generally healthy
  • Males between the age 18-35 years
  • Written informed consent.

EXCLUSION CRITERIA:

  • BMI less than 18.5 or greater than 25.0 kg/M(2)
  • History of cardiovascular disease such as congestive heart failure, heart block, clinically abnormal EKG as determined by investigators
  • History of liver disease or ALT serum level greater than two times the laboratory upper limit of normal
  • History of kidney diseases or renal insufficiency or estimated creatinine clearance less than or equal to 50 mL/min (MDRD equation)
  • History of cancer or bariatric surgery
  • History of diabetes mellitus or fasting serum glucose > 126 mg/dL
  • History of hypo- or hyper-thyroid or abnormal TSH, except minor deviations deemed to be of no clinical significance by the investigator.
  • History of asthma, chronic obstructive pulmonary disease and glaucoma
  • Psychological conditions, such as (but not limited to) claustrophobia, clinical depression, bipolar disorders, that would be incompatible with safe and successful participation in this study
  • Weight change >5 percent in the past 6 months or a trained athlete
  • Blood pressure greater than 140/90 mmHg or current antihypertensive therapy
  • Iron deficiency (Hemoglobin <13.7 g/dL and Hematocrit <40.1%)
  • History of illicit drug, opioids, or alcohol abuse within the last 5 years; current use of drugs (by history) or alcohol (CAGE greater than or equal to 2) (95)
  • Current use of medications/dietary supplements/alternative therapies known to alter energy metabolism
  • Current medications that may have interactions with study drugs as determined by the investigators
  • History of adverse or allergic reactions to the study drugs
  • Daily caffeine intake >500 mg (about 4 cups) and have withdrawal symptoms
  • Current smoker or user of tobacco products
  • Cannot commit to the schedule of visits to the Clinical Research Center (CRC) as required by the study timeline
  • Have had previous radiation exposure within the last year (X-rays, PET scans, etc.) that would exceed research limits (please let us know if you have received radiation for research purposes)
  • Have inflexible dietary restrictions
  • Any other reason that the investigator thinks would make interpretation of the study results difficult.
  • For subjects having an MRD (cOHORT 3), history of pacemaker, metallic heart valves, aneurysm clip, pedicle screws, metallic foreign body in eye, or other metallic implant.
  • For subjects receiving mirabegron (Cohort 3), a diagnosis of bladder outlet obstruction or the use of antimuscarinic medications for the treatement of overactive bladder.
Sex/Gender
Sexes Eligible for Study: Male
Ages 18 Years to 35 Years   (Adult)
Accepts Healthy Volunteers Yes
Contacts
Contact: Margaret S McGehee, C.R.N.P. (301) 594-6799 mcgeheems@mail.nih.gov
Contact: Kong Y Chen, Ph.D. (301) 451-1636 chenkong@niddk.nih.gov
Listed Location Countries United States
Removed Location Countries  
 
Administrative Information
NCT Number NCT01950520
Other Study ID Numbers 130200
13-DK-0200
Has Data Monitoring Committee Not Provided
U.S. FDA-regulated Product
Studies a U.S. FDA-regulated Drug Product: No
Studies a U.S. FDA-regulated Device Product: No
IPD Sharing Statement Not Provided
Responsible Party National Institutes of Health Clinical Center (CC) ( National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) )
Study Sponsor National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Collaborators Not Provided
Investigators
Principal Investigator: Kong Y Chen, Ph.D. National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
PRS Account National Institutes of Health Clinical Center (CC)
Verification Date November 26, 2019