Efficacy of a Novel Herbal Formulation (F2) on the Management of Obesity: In Vitro and In Vivo Study

Background. Currently, obesity and its comorbidities have become a serious threat to human health necessitating urgent development of safe and effective therapy for their management. Materials and Methods. In this research, a novel polyherbal formulation (F2) was prepared by mixing specific proporti...

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Published in:Evidence-based complementary and alternative medicine 2021, Vol.2021 (NA), p.8854915-14
Main Authors: Pandeya, Prakash Raj, Lamichhane, Ramakanta, Lee, Kyung-Hee, Lamichhane, Gopal, Kim, Se-Gun, Jung, Hyun-Ju
Format: Article
Language:English
Subjects:
Acids
Adipocytes
Adipose tissue
Antioxidants
Body mass index
Body weight gain
Cancer
Ethanol
Fatty acids
Fruit juices
Garcinia gummi-gutta
Gene expression
Geranium thunbergii
Herbal medicine
High fat diet
Nutrition research
Obesity
Orostachys japonica
Overweight
Phytochemicals
Rhus verniciflua
Royal jelly
Transcription factors
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Summary:Background. Currently, obesity and its comorbidities have become a serious threat to human health necessitating urgent development of safe and effective therapy for their management. Materials and Methods. In this research, a novel polyherbal formulation (F2) was prepared by mixing specific proportions of royal jelly and lemon juice with ethanol extracts of Orostachys japonicus, Rhus verniciflua, and Geranium thunbergii. The antioxidant activity was assessed using DPPH and ABTS assay methods. The antiobesity potential of the F2 was assessed in vitro using 3T3-L1 fibroblast and in vivo using a high-fat diet (HFD) fed C57BL/6J mice model. F2 was administered in mice at the dose of 23 mg/kg and 46 mg/kg, twice daily by oral gavage. A well-accepted antiobesity agent, Garcinia cambogia (GC), at 200 mg/kg was used as a positive control. Results. F2 was observed to exhibit synergistic antiadipogenic activity in 3T3-L1 cells. This inhibition was reinforced by the downregulation of specific adipogenic transcription factors. Furthermore, F2 was also found to reduce mice body weight gain, food efficiency ratio, fasting blood glucose level, fat deposition into the liver, and mass of white adipose tissue. F2 also played a role in the excretion of fat consumed by the mice. For most of the assays performed, the F2 (46 mg/kg) was comparable to the positive control GC (200 mg/kg). In addition, potential and synergistic antioxidant activity was observed on F2. Conclusion. The results revealed that the formulation F2 exhibited potential antiobesity activity through the inhibition of adipocyte differentiation, dietary fat absorption, and reduction of free fatty acids deposition in tissues.
ISSN:1741-427X
1741-4288
DOI:10.1155/2021/8854915