UG0712, A Ginsenoside Complex, Improved Endurance Performance and Changed Hepatic and Muscular Transcriptomic Signatures in C57BL/6N Male Mice
- Authors
- Yu, Su Hyun; Oh, Hea Ry; Park, Yong Hyun; Hong, Hye Ryeong; Kim, Hyun Jin; Park, Jinbong; Han, Yohan; Ko, Seong-Gyu; Shin, Eui Cheol; Kim, Tae Gyun; Cho, Hyung Taek; Pan, Jeong Hoon; Shim, Youn Young; Reaney, Martin J. T.; Cho, Tae Jin; Hong, Ji Youn; Kim, Young Jun; Han, Bok Kyung; Lee, Geung-Joo; Lee, Kangwook; Do, Seon Gil; Kim, Jae Kyeom
- Issue Date
- Feb-2025
- Publisher
- 한국식품영양과학회
- Keywords
- endurance performance; ginsenoside complex; liver; muscle; transcriptomics; UG0712
- Citation
- Journal of Medicinal Food, v.28, no.2, pp 127 - 143
- Pages
- 17
- Indexed
- SCIE
SCOPUS
KCI
- Journal Title
- Journal of Medicinal Food
- Volume
- 28
- Number
- 2
- Start Page
- 127
- End Page
- 143
- URI
- https://scholarworks.gnu.ac.kr/handle/sw.gnu/74864
- DOI
- 10.1089/jmf.2024.k.0089
- ISSN
- 1096-620X
1557-7600
- Abstract
- Ginsenosides, active compounds derived from Panax ginseng, exhibit promising potential in enhancing physical performance. This study investigates the impact of UG0712 (UG), a novel ginsenoside compound, on endurance capacity, body weight, organ weights, blood parameters, and specific transcriptomic changes in liver and muscle tissues using a C57BL/6N mouse model. The mice received UGs orally at three doses: UG50 (50 mg/kg), UG100 (100 mg/kg), and UG200 (200 mg/kg) for a specified duration. Endurance capacity, physiological parameters, and transcriptome signatures in liver and muscle tissues were assessed. UG administration significantly improved time to exhaustion, with UG50 and UG200 showing substantial enhancements. Body and organ weights exhibited no notable differences, suggesting a lack of adverse effects. Biochemical markers, except for decreased creatine kinase levels in the UG100 group, showed no significant variations. Transcriptome analysis revealed limited group separation and dose-dependent patterns. The UG100 group displayed significant enrichment in lipid metabolism and muscle-related terms. Identified dose-dependent improvements in endurance capacity highlight UGs' potential as supplements. The absence of adverse effects on body and organ weights, along with positive effects on biochemical markers, supports their safety. Despite limited dose-dependent patterns in transcriptomic analyses, the UG100 group showcased significant enrichment in pathways related to muscle and lipid metabolism. These findings offer valuable insights for athletes and aging individuals seeking to enhance physical performance, warranting further exploration into UG effects' on molecular mechanisms.
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