Hyperlipidemia Clinical Trial
Official title:
A Randomized, Double-Blind, 3-Period Crossover Study to Evaluate the Effects of a Dietary Supplement Containing Botanical Extracts on Fasting and Postprandial Lipid Metabolism in Apparently Healthy, Overweight and Obese Individuals
This study will evaluate the effects of encapsulated botanical extracts, previously shown to inhibit the enzyme diacylglycerol-acyltransferase-1 (DGAT-1) in vitro, on fasting and postprandial lipid metabolism during an oral fat tolerance test (OFTT) in apparently healthy, overweight and obese adult men and women.
Medications currently approved for the treatment of obesity act primarily to promote a state
of energy balance - by either suppressing appetite or interfering with lipid absorption in
the small intestine. Similarly, it may be possible to reduce or inhibit the synthesis of
triglycerides (TG) from dietary fat by targeting the activity of
diacylglycerol-acyltransferase-1 (DGAT-1) in the enterocytes of the small intestine.
DGAT-1 catalyzes the final step in the biosynthesis of TG and is most abundantly expressed
in the small intestine and adipose tissue. DGAT-1 in enterocytes is critical for assembly of
TG from fatty acids derived from food intake. Ingested dietary fat is cleaved to
monoacylglycerol and free fatty acids by lipases in the gut lumen and these are next taken
up by the enterocytes, where they are re-esterified to TG in the postprandial period. TG is
eventually released into circulation, primarily transported by chylomicrons. Thus, DGAT-1
plays a critical role in the absorption of dietary fat and inhibition of DGAT-1 has been
shown to delay and decrease re-esterification of dietary fats into circulating TG. It is
hypothesized that this effect may lead to decreased deposition of excess dietary fat as
adipose tissue, perhaps due to increased fatty acid oxidation in the enterocytes.
The potential physiological benefits of DGAT-1 inhibition lead to the development of the
potent, selective DGAT-1 inhibitor, AZD7687. Human clinical trials of AZD7687 demonstrated
attenuation of postprandial TG excursions, consistent with inhibition of gut DGAT-1.
However, this compound has limited, if any, therapeutic potential due to profound
gastrointestinal (GI) side effects, particularly diarrhea, nausea, and abdominal cramping
which were deemed intolerable. Moreover, no consistent dose-related treatment effects on
body weight, glucose or lipid metabolism were found in the small trials which were deemed to
be non-representative of the target therapeutic population.
Both cell-free and cellular in vitro models have been used to identify botanical extracts
that have potential to inhibit DGAT-1. In a follow-up 7-d parallel arm proof-of-mechanism
human clinical trial, each of four lead ingredients (2 g/d) were evaluated for the ability
to inhibit the intestinal release of dietary fat into circulation following a high-fat meal
challenge using post-prandial TG response as a surrogate marker. Of the four lead botanical
ingredients, whole grape extract (WGE) reduced fasting and postprandial TG levels (total
area under the curve from 0 to 6 h) by ~ 7% to 8% following a high-fat meal challenge. This
demonstration of efficacy, albeit modest, was sufficient to warrant continued exploration.
Importantly, only a few subjects reported very mild GI side effects, primarily bloating, in
this trial.
Combinations of WGE with other botanical extracts possessing biological activity against
supportive secondary mechanisms that might strengthen the overall inhibition of dietary fat
release into circulation and fat deposition were then explored. To examine potential
synergistic interactions, WGE was combined with other ingredients known to act on
complementary biological pathways that converge into a single efficacy outcome; in this
case, cellular TG levels. Ingredients that had effects on both glucose and fatty acid
metabolism that could ultimately synergize with the DGAT-1 pathway were chosen. The
complementary pathway targets chosen for these experiments were
Peroxisome-Proliferator-Activated Receptor-gamma Coactivator 1-alpha (PGC1-α) and Sterol
Regulatory Element Binding Protein 1c (SREBP1c).
In the cellular DGAT-1 model, grape seed extract (GSE) resulted in a significant inhibition
of DGAT-1 activity when combined with WGE. The combination index (CI), a quantitative
measure of synergy, indicated a strong synergistic effect (CI = 0.61). Synergy occurred at a
1:1 ratio of WGE to GSE, and at ratios that induced no effect on DGAT-1 activity when either
was used alone. The synergy data, together with the proof of mechanism clinical data, forms
the basis for conducting the presently proposed clinical trial at a WGE level below that
used in the previous study.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Basic Science
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