Obesity Clinical Trial
Official title:
Pilot Study of the Effects of Colchicine in Non-Diabetic Adults With Metabolic Syndrome
Background:
- Being overweight may cause low-level inflammation. This inflammation may cause some of the
medical problems of obesity, like high blood sugar (diabetes) and heart disease. This study
will test whether a medication called colchicine can improve metabolism in adults who are
overweight but have not yet developed diabetes.
Objectives:
- To learn whether colchicine improves sugar regulation and metabolism.
Eligibility:
- Healthy overweight adults18 to 100 years old.
Design:
- Participants must fast before each visit, including the screening visit.
- Participants will be screened with blood tests,urine tests, medical history, and
physical exam. They will have to drink sugar water, and have blood drawn to find out if
they are healthy.
- For visit 1, participants will have a medical history and physical exam and answer
questions. They will have blood taken with an intravenous (IV) line, give urine sample,
and give 2 stool samples..
- Also, subjects will get sugar water through one IV. Blood will be drawn from the other.
This measures sugar and insulin levels. During this, participants will lie in a bed and
can watch TV.
- Participants will have a full-body X-ray, lying on a table while a camera passes over
them. They will also have an abdominal CT scan, lying on a table that moves through a
ring that takes pictures.
- Participants will have a small fat tissue sample taken from their abdomen. It is like
getting a mini-liposuction.
- Participants will be given the study drug or placebo. They will take it twice daily for
3 months.
- For visit 2, participants will have blood tests, urine tests, medical history, and
physical exam.
- For visit 3, participants will repeat the tests in visit 1.
Obesity affects one-third of the adult U.S. population and is a major risk factor for the
development of type 2 diabetes and cardiovascular disease. Mouse models and human data
suggest that obesity-induced chronic inflammation is one mechanism promoting
obesity-associated comorbid conditions. In obesity, innate immunity is activated by
circulating molecules such as fatty acids and cholesterol crystals bind to nucleotide-binding
oligomerization (NOD)-like receptor family, pyrin domain containing 3 (NLRP3) receptors in
adipocyte tissue macrophages (ATMs). This binding stimulates NLRP3 oligomerization,
inflammasome formation, and proinflammatory cytokine activation. The resultant inflammatory
cascade leads to insulin resistance and decreased pancreatic beta-cell reserve. It has been
proposed that the suppression of this chronic low-level inflammatory state may impede the
onset of diabetes and cardiovascular disease.
Recent studies have shown colchicine, a potent microtubule inhibitor commonly used for the
treatment of gout and some rare inflammatory conditions, disrupts intracellular localization
of NLRP3, thereby blocking inflammasome assembly. As there are limited medical therapies
proven effective to improve obesity-related metabolic dysregulation, we propose to determine
the efficacy of colchicine 0.6 mg twice daily in non-diabetic obese adults with metabolic
syndrome. We will conduct a randomized, double-blinded, placebo-controlled pilot trial of
colchicine in forty subjects. We will study changes in insulin resistance, beta-cell reserve,
and systemic inflammation. Using adipose tissue obtained from biopsies, we will also study
colchicine s local effects on inflammation and insulin resistance. Should results prove
promising, this pilot study will allow determination of the sample size needed for an
adequately powered study of the effects of colchicine in obese adults with metabolic
syndrome.
Seven patients with diet-controlled type 2 diabetes will be given open-label colchicine and
followed as described above. We also plan to perform baseline evaluations on 40 subjects who
are not eligible for the treatment protocol. This group will consist of non-obese adults,
obese adults who are not insulin-resistant, and adults with diet-controlled type 2 diabetes.
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