Literature DB >> 19463739

(-)-Ternatin inhibits adipogenesis and lipid metabolism in 3T3-L1 cells.

Masahiko Ito1, Junko Ito, Hidefumi Kitazawa, Ken Shimamura, Takehiro Fukami, Shigeru Tokita, Kenichiro Shimokawa, Kaoru Yamada, Akio Kanatani, Daisuke Uemura.   

Abstract

(-)-Ternatin, a highly N-methylated cyclic peptide, inhibits fat accumulation in 3T3-L1 cells and reduces fat mass in mice. However, the mechanism for its anti-adipogenic effect has remained unknown. To examine the mechanism used by (-)-ternatin to inhibit adipocyte differentiation, we examined the effects of (-)-ternatin and [l-Ala(4)]ternatin, an inactive analog of (-)-ternatin, on the expression of adipocyte markers and lipogenic enzymes. We found that (-)-ternatin potently reduced mRNA expression of several adipocyte markers in a dose-dependent manner, whereas [l-Ala(4)]ternatin showed no effects. At the immediate early phase, (-)-ternatin, but not [l-Ala(4)]ternatin, reduced the expression of Srebp1c, Fas, Acc2 and C/EBP-alpha while showing no effects on C/EBP-beta and C/EBP-delta. These results suggest that (-)-ternatin affects the mid-to late differentiation stages of adipocytes. Consistent with the decreased expression of lipogenic enzymes, (-)-ternatin potently inhibited triglyceride synthesis. Intriguingly, (-)-ternatin also inhibited triglyceride synthesis in rat primary hepatocytes, suggesting that the potential action sites for (-)-ternatin are shared by adipocytes and liver. Although the target molecule of (-)-ternatin remains unknown, our data suggest that (-)-ternatin and its potential target might provide a new therapeutic approach to metabolic disorders.

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Year:  2009        PMID: 19463739     DOI: 10.1016/j.peptides.2009.02.008

Source DB:  PubMed          Journal:  Peptides        ISSN: 0196-9781            Impact factor:   3.750


  2 in total

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Authors:  Manuel F Juette; Jordan D Carelli; Emily J Rundlet; Alan Brown; Sichen Shao; Angelica Ferguson; Michael R Wasserman; Mikael Holm; Jack Taunton; Scott C Blanchard
Journal:  Elife       Date:  2022-10-20       Impact factor: 8.713

2.  Plitidepsin has potent preclinical efficacy against SARS-CoV-2 by targeting the host protein eEF1A.

Authors:  Kris M White; Romel Rosales; Soner Yildiz; Thomas Kehrer; Lisa Miorin; Elena Moreno; Sonia Jangra; Melissa B Uccellini; Raveen Rathnasinghe; Lynda Coughlan; Carles Martinez-Romero; Jyoti Batra; Ajda Rojc; Mehdi Bouhaddou; Jacqueline M Fabius; Kirsten Obernier; Marion Dejosez; María José Guillén; Alejandro Losada; Pablo Avilés; Michael Schotsaert; Thomas Zwaka; Marco Vignuzzi; Kevan M Shokat; Nevan J Krogan; Adolfo García-Sastre
Journal:  Science       Date:  2021-01-25       Impact factor: 47.728

  2 in total

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