Harold Katcher’s Last Rat

Experience tells us that it is much easier to extend median lifespan than maximum lifespan. Katcher’s trial of E5 in 8 rats breaks this expectation. The last of Harold Katcher’s rats has died, and she outlived her sisters by 7 months. Compared to controls, the average lifespan of treated rats increased 9.6%, while the maximum lifespan increased 22.0%. (For reasons unknown, the control rats lived longer than most Sprague-Dawley rats.)

When I last wrote about Katcher’s rats, there were just two left alive, and the survival curve conformed well to the Gompertz rule, which says that mortality rates increase exponentially with age. (There is no theoretical basis for the Gompertz rule, but it has been found to be a good empirical model for aging in many species.) From a Gompertz fit to the first 6 rats, I was projecting a maximum lifespan of 1250 days. The 7th rat wasn’t far off from that estimate, but the last of the 8 has lived just over 4 years (1464 days), breaking the record for lab rats. “Sima” lived 5% longer than the previous  longest-lived Sprague-Dawley rat.

Write-up in The Guardian

Sima received five infusions during her lifetime at intervals of 3 months. A sixth scheduled treatment was held on the judgment of the experimenters, so that at Sima’s death she was more than six months out from her last infusion. The fact that one rat lived longer than the rest is an invitation to experiment with optimization of the E5 protocol. All the rats were genetically identical and raised in the same lab. All received their first treatment around 2 years of age. Perhaps there are physiological tests that would offer suggestions why Sima responded better to the treatment.

Where does this project need to go?

It has been almost three years since I wrote up (breathlessly) the results of Katcher’s first study. I called it an Age Reduction Breakthrough. I still believe that plasma transfusions are the most promising path toward real, practical rejuvenation in the near-term. It is frustrating how little has happened in the intervening years. This should be a crash project for laboratories around the world, and instead it is being confined to a small group of scientists in Mumbai and Baltimore who are holding the IP.

Edison invented the lightbulb in 1879, and the first commercial units went on sale to the public in 1880.

We all should be demanding of Katcher and Sanghavi and our funding agencies a full-scale research program.

  • Determining what are the essential ingredients in E5 (Our patent system provides perverse incentives NOT to do this.)
  • Developing synthetic methods for creating these proteins (perhaps with vats of genetically modified E coli, a method which provides insulin and other human proteins in bulk at extremely low cost).
  • Adding plasma dilution to the protocol of infusions
  • Experimenting with different schedules and dosages, using Horvath clocks for feedback
  • Following all this up with lifespan studies in several mammalian species
  • Simultaneously offering E5 in combination with plasma dilution to human volunteers who are eager to be experimental subjects in exchange for probability of substantial health benefits.

Katcher and Sanghavi have a company called Yuvan Research, and they have connections with a laboratory at Johns Hopkins University in Baltimore. But this program is moving much more slowly than I would like (perhaps you concur) because the resources they have available are limited and Yuvan is jealously guarding its intellectual property. It didn’t help that Yuvan’s working capital was parked with Silicon Valley Bank, which went belly-up on Friday.

I suspect that many partners for Yuvan are available worldwide if suitable legal agreements can be reached.

43 thoughts on “Harold Katcher’s Last Rat

  1. Well done to Yuvan and Sima! Let’s hope Yuvan are not too adversely affected by SVB. Biophysical therapeutics have turned to crowd funding and the cosmetics route to introduce and fund their new product (works on reducing body temp btw). Are Yuvan still forging ahead with their cosmetic trials?

    • I certainly wouldn’t hope for adverse effects from the bank fallout. But if they happen I would hope they prove to be a blessing in disguise. Perhaps Yuvan would seek other partners; partners with deeper pockets who could bring about Josh’s 6 bullet points.

    • Last I heard the treasury in collaboration with the FDIC is going to make all depositors whole, meaning no losses of deposits > $250k will be incurred. It seems shareholders and bondholders will be wiped out.

      Of course retaining access to cash flow is tantamount, so I hope they don’t drag their feet on this. For a change I’m actually pretty optimistic on this. If the SVB debacle drags down an entire generation of tech startups and VCs then the entire US economy may just go t*ts up. There’s a lot more to lose here than just a few billion – this is about retaining confidence in the financial system. They lose that and they’re done.

  2. Congratulations Sima on shattering the Gompertz curve. If possible I would love to see a bottom line statistical assessment of exactly how well she did. By that I mean, what is the likelihood that Harold and Akshay’s regimen extended maximum (not average) lifespan? Sima did quite well, but she’s just one rat.

  3. Josh, would have median and maximal lifespan % increases?

    The Sprague-Dawley that was the previously longest lived was on to any intervention (CR, for instance)?

  4. Josh, could you elaborate a little on this: “Our patent system provides perverse incentives NOT to do this.” (“This” being determining the essential ingredients.) Don’t patents (at least in the USA) *require* publication of methods and ingredients. If an inventor doesn’t want to publish those details, they have to take the chance of relying on trade secrets.

    I think the patent system is far from optimal. It obviously is not tempered by the market since it sets the same term of protection regardless of the dynamics of the market in each industry. I see no reason for having the same length of protection for software and for pharmaceuticals (especially when the cost of developing the latter is driven so high by regulation).

    Your example of Edison is illuminating. Things have slowed way down. It reminds me of another historical fact I learned recently that blew my mind: The Empire State Building was constructed start to finish in 13 months! Not years, months.

    • Yuvan has a patent on the METHOD of extracting E5. But the ingredients in E5 are all natural proteins, and unpatentable for that reason. Once we know the chemical composition, the patent becomes worthless.

      • Although natural proteins cannot be patented, their combination can be, provided that their combination gives better results than each protein alone.

  5. Interesting she lived so long. With this study and some others I am convinced we aren’t that far away from being able to have real big youth/healthspan breakthroughs for humans. I think we are heading to where we can make humans age more like animals like a crocodile where senescence isn’t that bad until you are near the end. 80 year olds being more like in shape 50 year olds and actually look in their 50s if treatment started by that age. As far as lifespan that seems to be quite a ways away now at least.

    I am curious how Harold Katcher and his team’s skin treatment trial is coming along and if participants are seeing effects like he had from applying it to his hand.

  6. This is great work Harold and Josh! I can’t believe the big guns in anti-aging research like multi-billion-dollar Google Calico/ AbbVie are not following this sort of approach to the effect that aging is purposely caused by signals in blood because aging created an evolutionary advantage for mammal ancestors. Cynthia Kenyon’s prior work certainly suggests they would be following a programmed aging approach. So far, there is no indication that they are! Imagine what could be done if Harold had thousands of rats!

  7. Indeed, many of us older folks would be willing to serve as human volunteer experimental subjects. We are already “gambling” on any number of rather unproven supplements, but we realize that the alternative is to simply age and die at the same rate as our peers!

  8. Let’s expect that since human nature doesn’t change, self-interest will win out. Dr. Katcher in his late 70s will do his best to find a way for plasma fraction treatments to move forward.
    What does Dr. Katcher want his supporters to do to help?

  9. Hi All: Maybe there is more than one runner up in the talent section of this beauty pageant, but here is my candidate and it’s not CR.

    A rat treated with mesenchymal stem cells lives to 44 months of age; Rejuvenation Res 19:318-321 (2016). https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4971423/pdf/rej.2015.1777.pdf

    Hopefully achieving this crown will produce some publicity that will help assist Howard and Akshay in moving this forward.

    One way that recently occurred to me is this. Partner with Moderna. All of the target proteins, i.e., plasma fractions are expressed by cells. All of these can be generated exactly as the spike protein is in the mRNA COVID vaccines. The concept of a vaccine targeted against aging has multiple regulatory and marketing advantages over the xenotransplantation / biological products they are now perusing. Scale up would be limitless and not dependent on harvesting young blood from piglets, puppies or people.

    All of us don’t know what we don’t know regarding what is going on behind the scenes at Yuvan. Let hope that we will all be shocked by their progress in about 6 months.

    Michael

    • If MSC’s worked so well in humans you would think the Riordan clinic in Panama would be pumping out success stories in the literature instead of selling supplements,

  10. Josh, could you confirm that the previous record holder was on 40% CR for most of his adult life please? (if E5 on a short of ideal protocol beats that kind of CR for maximal lifespan it would be sure nice to know).

      • Not sure when.
        But I was just joking, anyway 🙂
        Even if it becomes scientifically possible by 2030, by the time it gets FDA approvals and it reaches the general public, it will be 2040 or beyond. So, our best bet is still E5.

    • I guess you have seen Josh’s comment on the Lifeboat blog:
      “There are some things Kurzweil understands brilliantly. Aging is not one of them. Aging is not a cellular disease, it’s a systemic disease.”

      • Actually, I had not read the comments at Lifeboat, so I was not aware of Josh’s comment when I posted here. As I have been following this blog for a long time, I have been aware of Josh’s thinking, which makes a lot of sense of me. As a result, I consider E5 to be the “smart way” to address the aging problem.
        Of course, being able to solve the problem “smartly” does not preclude the possibility of addressing the same problem by “brute force” at the cellular level as Kurzweil suggests. Kurzweil has a good record with predicting future developments. His prediction that solving the problem of aging at the cellular level in the thirties might be possible at the lab. It is very unlikely that it will be available to the general public in that time frame.
        I strongly believe that “E5” is now the best bet. Hopefully it will be available much sooner.
        With my initial comment that we might no longer need “E5” I was trying to be funny.

  11. Great comments Josh. Its tragic that we likely stand on the threshold of a breakthrough which excites our imagination and would add hope to the lives of literally billions of people around the world, but are held back not by fundamental technology but by the nature of human society. Huge numbers of people are dying who very well might not need to.

    I suppose we need an angel investor who themselves want to bring this boon to humanity (and themselves) and are sufficiently willing to share the profits (and all of the credit) with Yuvan. It seems likely that there should be a large number of people with the kind of resources that could do this. Finding that person and convincing them has been achieved for lesser objectives in the past. It’s not clear to me why it’s not possible now.

  12. “…There is no theoretical basis for the Gompertz rule, but it has been found to be a good empirical model for aging in many species…”
    It looks like there might be theoretical basis to Gompertz, e.g. I found this, from Uri Alon and team, an interesting conjecture:
    “A causal factor in mammalian aging is the accumulation of senescent cells (SnCs). SnCs cause chronic inflammation, and removing SnCs decelerates aging in mice. Despite their importance, turnover rates of SnCs are unknown, and their connection to aging dynamics is unclear. Here we use longitudinal SnC measurements and induction experiments to show that SnCs turn over rapidly in young mice, with a half-life of days, but slow their own removal rate to a half-life of weeks in old mice. This leads to a critical-slowing-down that generates persistent SnC fluctuations. We further demonstrate that a mathematical model, in which death occurs when fluctuating SnCs cross a threshold, quantitatively recapitulates the Gompertz law of mortality in mice and humans. The model can go beyond SnCs to explain the
    effects of lifespan-modulating interventions in Drosophila and C. elegans, including scaling of survival-curves and rapid effects of dietary shifts on mortality.”

    • Nice draft, thanks for sharing.

      Anecdote: a friend of mine, a top-level professional football (soccer) athlete, suffered an ankle injury when he was 35, i.e. close to the end of his professional career. He decided to try a treatment with stem cells-derived extracellular vesicles that included liposuction and, after isolation/cultivation, re-infusion in his arm. This not only cured his ankle in a record time but also had an important systemic effect on his whole body that allowed him to compete a few more years at the top level.

  13. Thank you Josh for pointing out the obvious: this is a massively important area of research, and the lack of progress and funding here is frustrating.

  14. another view
    aging is caused by the imbalance in the number of differentiated cells VS stem cells. It is because of the fast growth of the differentiated cells during the growth phase, the epigenetic curve shows a vertical slope , which gradually changes as the differentiated cells numbers grow. eventually growth stops and aging commences as it is the property of the differentiated cells to age epigenetically. The mere presence of differentiated cells in sufficient numbers tamps down the activity of the stem cells.

    • The factors in the plasma which allow stem cells to be activated and increase in numbers are the ones which need to be identified and are probably the solution. The balance of stem cells and differentiated cells needs to be restored to reverse aging.
      dwarfism is a condition which bestows many benefits to an individual, such as decelerated pace of aging. IMO the condition of dwarfism allows the balance of stem cells and differentiated cells to be favorable for a longer period of time because of lesser number of differentiated cells.
      Also IMO human females who are smaller in size than the males have a lesser burden of disease because of this very reason.

      • autophagy-dependent cell death mechanism might be activated during starvation/calorie restriction as well as stem cell stimulation. both these mechanisms alter the balance of stem cell/differentiated cells.
        Whereas intake of HGH/testosterone in the aged might lead to extended division/survival of differentiated cells again altering the balance of stem cell/differentiated cells, which can be pro-aging.

    • At the end of that paper’s Discussion section is:
      “Due to the sequential and non-randomized participant assessment schedule, we were unable to assess the influence of brain aging on body systems.”

      From Dr. Katcher’s 2015 “Towards an Evidence-based Model of Aging”:
      “It was demonstrated that increased aging occurred as a result of lack of gonadotropin-releasing hormone, and that increased lifespan resulted from its provision during aging. In this manner:
      Aging of hypothalamic microglia leads to
      Aging of the hypothalamus, which leads to
      Aging elsewhere in the body.

      So here we have a multi-level interaction:
      Activation of NF-κB leads to
      Cellular aging, leading to
      Diminished production of GnRH, which then
      Acts (through cells with a receptor for it, or indirectly as a result of changes to GnRH-receptor-possessing cells) to decrease lifespan.

      So the age state of hypothalamic cells, at least with respect to NF-κB activation, is communicated to other cells via the reduced output of GnRH.”

      Not using the same frameworks/paradigms, are they? But maybe through their limitations statements, those researchers at least know what’s the way forward.

      • @PRice, My comment was intentionally short to make it easier to deal with and more likely I would get a reply, but I think I should be more specific. I’ll preface this by saying I think both of your points are good and I really appreciated the time you spent responding to my comment. I was mainly concerned with a third thing.

        When validating a scientific hypothesis like Dr.Katcher’s theory of aging we’re talking about reproducibility of all of it’s elements and also how the body of supporting evidence from independent experiments effects the status quo. Namely, that even though it only serves to validate a relatively small proportion of the relevant facts, that aging of different organs are connected instead of merely coinciding in some sense, it happens that this is a particularly useful fact to validate.

        It’s particularly useful because of the mechanisms and status quo of the politics of science and to some extent public opinion. As Harold and Akshay continue to do research and to give their research the best chance of making an impact on human health there are a range of scenarios that they could face, ranging from incredible funding and public support to great resistance and even legal, financial and for Harold potentially even longevity barriers if those obstacles take too long to traverse. There is also the matter of some people who may end up dying or suffering other serious consequences waiting for it. Of course, the reality will probably be somewhere in the middle, and since his work isn’t that well known yet we don’t know how much support and opposition he’ll really get.

        In my view, at least on the opposition side of the ledger the biggest risk comes from substantially different opinions in certain parts of the scientific community. I’m not talking about constructive criticism or pointing out a few things that can be addressed in the existing experiments or published theory and methods, I’m talking about opposition, not simple concerns, on the basis of things that no one has tested yet. Some of it may come from scientists with a competing theory, but I think the strongest opposition would likely come from people who don’t think science has advanced enough to even have a theory of aging. If we think of these opinions on aging roughly fitting into distinct categories, I would suppose that the opposition would come less from people in the same category and more from people with highly differentiated categories of opinions.

        That’s why I think it’s particularly useful to validate this particular fact, since this research weighs in favor of the fact that is part of the 10,000 foot view of Harold’s work. I think fewer people from other categories will feel confident to criticize the details of Harold’s proposed mechanism and so this type of research can make a bigger impact on E5 research at this stage than many other things.

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