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691.
Greenway FL Liu Z Yu Y Caruso MK Roberts AT Lyons J Schwimer JE Gupta AK Bellanger DE Guillot TS Woltering EA 《Obesity surgery》2007,17(4):510-515
Background Inhibition of angiogenesis reverses rodent obesity. A validated assay in human fat tissue is needed to study the role of angiogenesis
in human obesity.
Methods Human fat tissue fragments from surgery were placed in 96-well plates, embedded in fibrin thrombin clot and overlaid with
cell culture media containing 20% fetal bovine serum. After 15 days, the clots were examined by histology and electron microscopy.
The effect of taxol, cobalt chloride and a heparin-steroid combination was tested in the fat tissue assay and compared to
the validated human placental vein angiogenesis model (HPVAM).
Results Blood vessels initiated growth and elongated from the fat tissue fragments over 15 days. Presence of blood vessels was confirmed
with histology and electron microscopy. Taxol at 10−6 and 10−7 M completely inhibited angiogenesis, while Taxol 10−8 and 10−9 M and the heparin-steroid partially inhibited angiogenesis.The response to taxol and heparin-steroid was similar to that
of the HPVAM, a validated angiogenesis assay. Cobalt chloride, a stimulator of vascular endothelial growth factor (VEGF) stimulated
angiogenesis initiation at 10−9 M in fat tissue and the HPVAM, but at 10−10 M blood vessel growth was stimulated only in the fat assay.
Conclusion This angiogenesis assay based on human fat tissue uses three-dimensionally intact human tissue. The vessels are derived from
quiescient vessels within the fat. These properties allow the angiogenic switch to be evaluated in an in vitro setting. The
angiogenic response of fat tissue is not identical to placental tissue. This assay allows exploration of angiogenesis in fat
tissue. 相似文献
692.
Greenway FL Liu Z Martin CK Kai-yuan W Nofziger J Rood JC Yu Y Amen RJ 《International journal of obesity (2005)》2006,30(12):1737-1741
OBJECTIVE: A human pilot study testing the safety and effectiveness of NT (Number Ten), a dietary herbal supplement made from rhubarb, ginger, astragulus, red sage and turmeric, to reduce food intake and cause weight loss. RESEARCH METHODS AND PROCEDURES: A total of 24 healthy women, 18-60 years, body mass index 25-35 kg/m(2) on no chronic medication were randomized to four groups of six: (1) oral freeze-dried NT 6 gm/day, (2) bed-dried NT 6 gm/day, (3) freeze-dried NT 12 gm/day or (4) placebo. Number Ten dose was escalated over 3 weeks and maintained for 8 weeks on a 700 kcal/day diet below maintenance. Food intake was measured at baseline and 4 weeks. Safety parameters were monitored weekly during dose escalation, week 6 and week 12. RESULTS: Weight loss was 1.8 kg for placebo and 0.4 kg for 500 mg NT whereas the 250 mg bed- and freeze-dried NT gained 0.43 and 0.87 kg, respectively (P=NS). The food intake increased 74 kcal with 250 mg freeze-dried NT and decreased 193.7 kcal with 500 mg freeze-dried NT (P<0.01). There was a dose-related incidence of loose stools in the NT groups, but no other toxicity was seen. Number Ten was found to contain sennosides, known laxatives and gallic acid, which is known to give weight loss in rodents. DISCUSSION: The human dose equivalent of NT used in this study was & frac16; and & frac112; of that shown to give well-tolerated weight loss in rodents. Number Ten will not be an effective dietary herbal supplement for the treatment of obesity owing to dose-limiting gastrointestinal toxicity. 相似文献
693.
694.
Candida J. Rebello Tyler S. Morales Katsya Chuon Shu Dong V. Tyrone Lam Dan Purner Stanley Lewis Jonathan Lakey Robbie A. Beyl Frank L. Greenway 《Obesity reviews》2023,24(12):e13625
Insulin is secreted in pulses from pancreatic beta-cells, and these oscillations maintain fasting plasma glucose levels within a narrow normal range. Within islets, beta-cells exhibit tight synchronization of regular oscillations. This control circuit is disrupted in type 2 diabetes, and irregularities in pulse frequency and amplitude occur. The prevalence of type 2 diabetes is three times higher in American Indian and Native Alaskans compared to Whites, and their genetic ancestry is associated with low beta-cell function. Obesity in this population compounds their vulnerability to adverse outcomes. The purpose of this article is to review insulin secretion and action and its interaction with race. We also present the results from a 6-month retrospective chart review of metabolic outcomes following intravenous physiologic hormone administration to 10 Native Americans. We found reductions in hemoglobin A1C (baseline: 9.03% ± 2.08%, 6 months: 7.03% ± 0.73%, p = 0.008), fasting glucose (baseline: 176.0 ± 42.85 mg/dL, 6 months: 137.11 ± 17.05 mg/dL, p = 0.02), homeostatic model assessment of insulin resistance (baseline: 10.39 ± 4.66, 6 months: 7.74 ± 4.22, p = 0.008), and triglycerides (baseline: 212.20 ± 101.44, 6 months: 165.50 ± 76.48 mg/dL, p = 0.02). Physiologic hormone administration may improve components of the metabolic syndrome. The therapy warrants investigation in randomized controlled trials. 相似文献