Fisetin to Clear Senescent Cells

Florin I am not familiar with those studies. Would you please provide links to them? Also, most people here are following a conservative approach aligned with the Phase 2 trials being conducted by the Mayo Clinic. Those results are not yet published, so data on the effect on humans is still lacking. Also, one study indicated a toxic accumulation in the liver of mice at a high dose, which may have been a result of the DMSO delivery, but it is still unknown, so people are being conservative until more clear long term toxicity studies are conducted. Toxicity is being studied as part of one of the newer Phase 2 human trials, but we are still probably 2 years away from those results, and it is following the Mayo Clinic protocol, not the much more aggressive one you suggest.

As for myself, I have been very happy with the Mayo Clinic protocol. I have less arthritis symptoms and can see the moles and wrinkles in my skin lightening and diminishing. I have upped consumption to 2 days every 2 weeks because I was seeing a regression if I waited a full month. However, I am relatively young, so don't feel the need to be aggressive in my treatment. I also consider fisetin like weight lifting. A stimulus is good, but you need recovery time to allow the adaptation to occur. Off time is when the body regenerates and heals. Fisetin is causing a stress response and literally killing cells in the body, and that process takes its toll, so recovery is important. Senolytics cause a stress response. Your body needs to be able to adapt. Too much, and you get other negative side effects, like with the chemotherapy drugs. High doses kill the cancer, but they also begin to affect healthy cells and stress the body's ability to process and eliminate both the chemotherapeutic and the destroyed cells.

Fairy8i8 Very nice summary and thank you. Agree with what you said, and I have also gone to 2  Mayo  treatments/month ( 20mg/kg bodyweight for two consecutive days)

My own personnel experience is that there was initially an immediate response  to the Mayo protocol in that my endurance, strength and color vision were almost instantaneously enhanced. This immediate response did not increase after my first treatment, but it has not diminished either. Others on this forum have reported similar experiences.  It seems to me that there has to be more than removal of senescent cells and/or mTOR inhibition to explain the initial response.  I have done a minor literature search and have not found an explanation my initial response. I wonder if there is some sort of impact on mitochondria. It may be that my age  (80 yr old) has something to do with the initial response. 

Fairy8i8 Do you have a link to the study? Thank you

Fairy8i8 It's the same study that this entire discussion is based on. Here's the relevant info:

Ercc1−/∆;p16Ink4a-luciferase mice were fed a standard Teklad 2020 chow diet with or without supplementation with 500 ppm (500 mg/kg) of fisetin, ad libitum (approximately 60 mg/kg fisetin per day)

To determine if fisetin-mediated clearance of senescent cells impacts the health or lifespan of mice, WT f1 C57BL/6:FVB mice were fed a diet containing 500 ppm fisetin beginning at 85 wks of age, roughly equivalent to age 75 years in humans. This resulted in an extension of median as well as maximal lifespan (Fig. 5A-B).

So, 500 ppm = 60 mg/kg fisetin per day.

The WT (wild-type) mice were the only ones demonstrated to have any lifespan extension. You might think that this effect was probably all due to the elimination of senescent cells, but it might also have been caused by other factors such as chronic admin of fisetin affecting the microbiome which the paper also speculated about.

Regarding toxicity, I'm not sure what would be more toxic: acute, mega doses of (possibly contaminated) fisetin or lower chronic doses? Mega doses might be safer if heavy metal contamination would be the only concern, but what about stuff like hinokiflavon (where the dose might make the poison)? Although I'd like some human data (I did request blood test results for liver function in another thread), I'm not too concerned about fisetin accumulation in the liver; chronic administration in this study was beneficial, not harmful. The study which suggested liver toxicity used 223 mg/kg, whereas I'm referring to 60 mg/kg which apparently didn't have any toxicity. That same study also mentioned that there was no observed toxicity even at 112 mg/kg. And as for the Mayo Clinic's protocol, the reason it's going for acute admin rather than chronic is probably because it wants to avoid drug interactions (several drugs and substances were contraindicated) and perhaps hoping that acute admin would produce faster results than chronic.

Whatever happens with stress and recovery, the data we have suggests that chronic admin might be better than acute for lifespan extension. Isn't maximum efficacy what everyone wants, given the same level of safety?

Fisetin is a senotherapeutic that extends health and lifespan
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6197652/

Anti-cancer effects of fisetin on mammary carcinoma cells via regulation of the PI3K/Akt/mTOR pathway: In vitro and in vivo studies
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6034928/

Florin Thanks for clarifying. I'm really glad you commented! I always got so caught up with the initial groups, that I failed to contemplate the significance of the final group. Refreshing to see a decrease in oxidative stress in the liver. However, we do not know how the different methods compare to longevity because the first 3 groups of mice on various diets were sacrificed rather than allowed to live. Also, there is a standard chart for adjusting dosing of animal subjects to human subjects. I don't have it off hand, but it's not 1 to 1, so 60mg/kg for humans would not be the indicated amount from this study.

Also, I will add a third day to our dose round (today) because I just took doses the last 2 days, based on the Mayo Clinic update and see how it goes. I have wondered about increasing a high dose to more days as the group of mice that was given the higher dosage for 5 days had more senescent clearance than the group given the 500ppm chow ad libidum pulsed on and off.  I never liked how that group had an initial decrease in senescent cells, but then a slow increase thereafter, even when given the chow again. It's too bad they didn't do the same imaging on the other groups to see senescent accumulation over time. If only I had money to fund research!

I had discussed which way to take fisetin with my dad. The nice thing about intermittent doses is that it is cheaper as well. As I said, I am young (40) so I have time to wait and see what becomes of the research while having benefitted on the Mayo Clinic protocol. Also, I take Biotivia Pteromax and Jarrow Broccomax daily, so I do take things that stimulate the nrf2 pathway on a daily basis already. At this point, I am more concerned with healthspan rather than lifespan.

 Michael To which study are you referring?

Fairy8i8 The only empirically-proven endpoints is that the chronic group had increased longevity and health. So, there's going to be a risk in assuming that intermittent or acute admin will provide the same or better results.

Florin Because that would cost me $6,745 a year...

Dan Nave It should cost a few hundred per year, not thousands. Remember that 60 mg/kg = 5 mg/kg HED (human equivalent dose) per day.

Florin Dr. Green has always said 3 consecutive days of Dasatinib 100 mg and 3 consecutive days of Fistein 1500 mg "every month" for elderly people.  Every 3 months for younger.  He also preaches, Vitamin C with dosing to improve bioavailability.  He leaves it up to you on whether to take Quercetin.  Says Fistein is so superior it is not necessary.

Van Interesting. Do you know how much younger "younger" might happen to be?

Moustachiarty No

Moustachiarty  At least 45, and you won't be too much off.

Mel it appears FB removed  that  Study,  do  U  remember the name of  it?

Ross Barker https://www.sciencedaily.com/releases/2020/11/201120150728.htm

aribadabar Curious enough about it to have just scheduled my first session on Thursday for the second week of December. If I decide to try three/four, will report back.