N-acetylcarnosine attenuates age-associated declines in multi-organ systems to improve survival

  1. Edwin R. Miranda
  2. Justin L. Shahtout
  3. Shinya Watanabe
  4. Jan Spaas
  5. Norah Y. Milam
  6. Grace Neiswanger
  7. Benjamin Werbner
  8. Deborah Stuart
  9. Sohom Mookherjee
  10. Jack Wilson
  11. Michael Judge
  12. Isabella Y. Goh
  13. Tyler Slater
  14. Molly R. Gallop
  15. Guoli Hu
  16. Takuya Karasawa
  17. Jillian K. Landers
  18. Bryann Rainbow
  19. Kyle T. O’Connor
  20. Nicholas J. Black
  21. He Lan
  22. Linda S. Nikolova
  23. Ying Li
  24. Crystal F. Davey
  25. James E. Cox
  26. Sihem Boudina
  27. Courtney M. Karner
  28. Natalia S. Harasymowicz
  29. Nirupama Ramkumar
  30. J. David Symons
  31. Amandine Chaix
  32. Jonathan Z. Long
  33. Micah J. Drummond
  34. Katsuhiko Funai
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Abstract

Histidine containing dipeptides (HCDs) such as N-acetylcarnosine are endogenous metabolites that are ergogenic and mitigate metabolic dysfunction. We previously demonstrated that short-term N-acetylcarnosine treatment is highly efficacious in protecting muscle atrophy induced by disuse. Here we demonstrate that a 6-months treatment of N-acetylcarnosine attenuates a broad spectrum of age-associated maladies and improved survival by ∼50% in female mice. A comprehensive survey of organ systems revealed that N-acetylcarnosine prevents decline in adiposity, diastolic function, vasodilation, muscle strength, and bone density. Together, N-acetylcarnosine substantially delays the onset of system-wide end-stage pathology to prolong lifespan. As an endogenously present metabolite, treatment with N-acetylcarnosine may be a safe and promising intervention to promote healthy aging in humans.

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