I few months ago this study was kicking around the Forum. I was asked for my take and never came up with anything to my own satisfaction. I now have a decent explanation, which may or may not turn out to be correct. It seems to shed some light on the benefits of C60. Turns out there is precedent for an antioxidant to have effects long beyond its last dose.
Dietary lipoic acid supplementation can mimic or block the effect of dietary restriction on life span
https://www.scienced...000961?via=ihub
Dietary restriction feeding extends survival in a range of species but a detailed understanding of the underlying mechanism is lacking. There is interest therefore in identifying a more targeted approach to replicate this effect on survival. We report that in rats dietary supplementation with alpha-lipoic acid, has markedly differing effects on lifetime survival depending upon the dietary history of the animal. When animals are switched from DR feeding to ad libitum feeding with a diet supplemented with alpha-lipoic acid, the extended survival characteristic of DR feeding is maintained, even though the animals show accelerated growth. Conversely, switching from ad libitum feeding a diet supplemented with alpha-lipoic acid to DR feeding of the non-supplemented diet, blocks the normal effect of DR to extend survival, even after cessation of lipoic acid supplementation. Unlike the dynamic effect of switching between DR and ad libitum feeding with a non-supplemented diet where the subsequent survival trajectory is determined by the new feeding regime, lipoic acid fixes the survival trajectory to that established by the initial feeding regime. Ad libitum feeding a diet supplemented with lipoic acid can therefore act as mimetic of DR to extend survival.
Could ALA be affecting stem cell proliferation? Check this out:
Influence of alpha-lipoic acid on survival and proliferation of mesenchymal stem cells
http://feyz.kaums.ac...d=1&slc_lang=en
Background: Mesenchymal stem cells (MSCs) contribute to tissue repair in vivo and form an attractive cell source for tissue engineering. The regenerative potential of MSCs is impaired by oxidative stress-induced cellular senescence. Alpha-lipoic acid (ALA) is well-known for its antioxidant properties. The Ki-67 antigen is expressed during all phases of cell cycle (G1, S, G2 and M phase) except for G0 phase and is commonly used as a proliferation marker. Herein, the aim of the present study was to investigate the impact of ALA on rat MSCs survival and proliferative potential in vitro.
Materials and Methods: Isolated rat bone marrow and derived mesenchymal stem cells were synchronized by serum starvation for 24h and the addition of hydroxyurea (2µM). Afterwards, the cells were cultured in the presence of ALA (1µM) for 48h. An MTT assay was used to investigate cell survival and proliferation. The expression of Ki-67, a proliferation marker, was also evaluated.
Results: The MMT assay showed a statistically significant increase in proliferation of MSCs in ALA-treated groups for 48 hours. Immunoctytochemistry of Ki-67 revealed significant differences between ALA- treated and Control groups.
Conclusion: In conclusion, ALA is effective in increasing the survival and cell proliferation of isolated rat bone marrow and derived mesenchymal stem cells.
Here is a finger-in-the-air hypothesis. Ad lib feeding results in greater use of stem cells; DR preserves stem cells. ALA increases stem cell use even more when combined with ad lib feeding to the extent that subsequent DR could not extend life.
But it appears that late in life increasing proliferation of stem cells can trump their preservation if they have been saved for the occasion; ALA added to an ad lib diet preserves the lifespan benefits of a prior DR diet.
ALA added to Ad lib alone does not increase lifespan; perhaps increased stem cell proliferation, which is beneficial to failing health in old age, is offset by their profligate use in early life.
Effect of Alpha-Lipoic Acid on Memory, Oxidation, and Lifespan in SAMP8 Mice
This study used old SAMP8 (senescence-accelerated) mice and ALA and showed an improvement on learning and memory but a reduction in remaining lifespan, which supports the using up of stem cells as beneficial to health in the short term, but detrimental to long term survival.
https://www.research...lipoic-acid.cfm
https://pubmed.ncbi....-in-samp8-mice/
Mice tend to spend more time exploring new objects than familiar ones, so the mice in the behavior study were exposed to two similar objects (plastic frogs) for five minutes. Twenty-four hours later, one of the frogs was replaced with a novel object (a plastic bird). The 10 mice that had been given alpha-lipoic acid before the test spent more time exploring the new object than 10 others who had not been given the drug.
These mice also were given a test using a maze, to see if the mice could learn the location of an escape chamber. In this test, the mice that were administered alpha-lipoic acid learned the location of the "target area" more quickly than those who had not received the acid, especially during the first few days of testing. Since all 20 of the mice in the study were extremely old for the species (18 months), the study indicated that even more advanced dementia can be reversed by alpha-lipoic acid…..The lifespan study, however, provided less encouraging results. In this study, 50 11-month old SAMP8 mice were given alpha-lipoic acid every day until the day they died. Their longevity was compared with a control group of 50 SAMP8 mice that were not given the drug. The team found that mice receiving the drug lived for an average of 20 weeks after the drug was first administered, and those who did not receive the drug lived an average of 34 weeks from the beginning of the test—a significant difference.
What does this mean for C60 use? C60 fullerene added at 10 months of age for 7 months allowed rats to live to 50 months + (normal max lifespan ~35). This suggests that stem cell stimulation is beneficial if used in youth to middle age. My research above suggests however that the benefits seen in the Baati study will be hard to replicate if the study design is significantly deviated from.
For us self-experimenters it suggests stem cell stimulation should be used with caution, and mitigation for loss of stem cells should be accounted for. See for example, Turnbuckle’s Stem Cell Protocol that uses supplements to encourage self-renewal or my approach using telomerase.
It also begs the question - for any intervention that appears to be healthy in the short run, is it depleting stem cells?
Edited by Mind, 29 September 2020 - 09:26 AM.
