Metabolic or Bariatric surgery is an effective treatment for type 2 diabetes mellitus (T2DM) diabetes associated with obesity. There remain some questions about the biochemical mechanism that drive how these surgeries work to reverse hyperglycemia. In the proposed human studies, the investigators will test the hypothesis that the amino acid tyrosine is a key metabolite in regulating blood sugar levels and that manipulation of the amount tyrosine supplied by nutrition is able to achieve some of the metabolic benefits seen in the early post-surgical period following bariatric surgery. The central hypothesis is that that the tyrosine content of the meal challenge affects post-prandial intestinal and plasma dopamine and levodopa and L-3,4-dihydroxyphenylalanine (L-DOPA) levels, which, in turn, impact β-cell insulin secretion and glucose excursions. The investigators now propose to characterize the possible effects of manipulating dopamine and L-DOPA levels in the gut and plasma on glucose tolerance, insulin secretion, and insulin sensitivity in healthy volunteers with a range of body mass indexes (BMIs).
Several biochemical mechanisms explaining how Roux-en-Y Gastric Bypass (RYGB) provides an effective treatment for obesity associated type 2 diabetes mellitus (T2DM) and improves hyperglycemia independently of weight loss have been proposed. Two are of particular interest; a) the hindgut hypothesis suggesting that nutrient delivery to the distal intestine drives the production of "incretins" which enhance insulin secretion (e.g. glucagon-like peptide-1 (GLP-1)), and b) the foregut hypothesis, positing that foregut bypass reduces the secretion of factors (i.e. anti-incretins) that normally defend against hypoglycemia. The investigators have been actively investigating this topic and have developed a hypothesis based on past studies that they wish to test in a limited human clinical study. In addition, preclinical data suggest that there exists a gut-to-beta cell pathway, responsive to nutritional tyrosine, regulating insulin secretion, and this pathway provides a mechanism for the early postoperative improvements in hyperglycemia observed in RYGB.
Study Type
INTERVENTIONAL
Allocation
NON_RANDOMIZED
Purpose
BASIC_SCIENCE
Masking
NONE
Enrollment
10
L-Tyrosine dietary supplement will be provided as 500 mg capsules and 4 (four) 500 mg capsules are to be given before OGTT. The capsules are formed from animal gelatin, and the contents are formulated with magnesium stearate as a flow agent, but without binders, coatings or colorings and also have no added flavorings, sugars, salt, artificial sweeteners, preservatives or salicylates. The capsules are to be administered with less than eight ounces of water to minimize dilution of gastric acidity.
Columbia University Irving Medical Center
New York, New York, United States
Whole blood glucose level
Glucose concentration versus time profile following glucose challenge define glucose tolerance
Time frame: Up to 120 minutes from baseline
Plasma insulin concentration
Plasma insulin concentration versus time profile following glucose challenge define glucose tolerance
Time frame: Up to 120 minutes from baseline
Plasma dopamine concentration
Plasma dopamine concentration versus time profile following glucose challenge may affect glucose tolerance
Time frame: Up to 120 minutes from baseline
Plasma L-DOPA concentration
Plasma L-DOPA concentration versus time profile following glucose challenge may affect glucose tolerance
Time frame: Up to 120 minutes from baseline
L-tyrosine concentration
Plasma L-tyrosine concentration versus time profile following glucose challenge may affect glucose tolerance
Time frame: Up to 120 minutes from baseline
Plasma glucagon concentration
Plasma glucagon concentration versus time profile following glucose challenge impacts glucose tolerance
Time frame: Up to 120 minutes from baseline
Plasma GLP-1 concentration
Plasma GLP-1 concentration versus time profile following glucose challenge impacts glucose tolerance
Time frame: Up to 120 minutes from baseline
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