Details on the LEV Foundation's First Study of Combined Interventions in Mice
The recently launched Longevity Escape Velocity (LEV) Foundation will, initially at least, focus on testing combinations of interventions. This work is informed by the SENS view of aging, in that degenerative aging is produced by a limited number of forms of cell and tissue damage that result from the normal operation of metabolism. These include the accumulation of senescent cells, cross-linking of the extracellular matrix, mitochondrial DNA damage, and so forth. Each form of damage produces its own contribution to a complex web of interacting downstream consequences, so while repairing any one form of damage should be beneficial, repairing more than one should be better.
Unfortunately the research and development communities operate under incentives that strongly discourage earnest work on combinations of therapies, these incentives largely resulting from the way in which intellectual property and regulation of medical development interact. Research into combined therapies is necessary to achieve the end goal of a comprehensive toolkit of rejuvenation therapies, but it is near entirely ignored as an aspect of this area of medical research. Thus philanthropic efforts are required to fill in the gap and light the way. Combined interventions are on the roadmap of the rejuvenome project, for example. And now they are a focus at the LEV Foundation.
Robust Mouse Rejuvenation - Study 1
LEV Foundation's flagship research program is a sequence of large mouse lifespan studies, each involving the administration of (various subsets of) at least four interventions that have, individually, shown promise in others' hands in extending mean and maximum mouse lifespan and healthspan. We focus on interventions that have shown efficacy when begun only after the mice have reached half their typical life expectancy, and mostly on those that specifically repair some category of accumulating, eventually pathogenic, molecular or cellular damage. The first study in this program is starting in January 2023.
Our ultimate goal in this program is to achieve "Robust Mouse Rejuvenation". We define this as an intervention, almost certainly multi-component, that: (a) is applied to mice of a strain with a historic mean lifespan of at least 30 months; (b) is initiated at an age of at least 18 months; (c) increases both mean and maximum lifespan by at least 12 months.
In each study in this program, we will examine the synergy of (typically at least four) interventions already known individually to extend mouse lifespan when started in mid-life. We will determine not only the ultimate readout of lifespan, but also the interactions between the various interventions, as revealed by the differences between the treatment groups (receiving different subsets of the interventions) in respect of the trajectories with age of cause of death, decline in different functions, etc. In this way we will add greatly to the understanding of which benefits these interventions confer and how they synergize, or possibly antagonize.
There are two key motivations for this program. One is purely biomedical: as with all mouse work with a biomedical end goal, we hope to generate data that will inform the development of therapies to let humans live longer in good health. The other could be called rhetorical, societal, political - it is to demonstrate a definitive proof of concept that aging is much more malleable than society currently insists on thinking it is, and thus must be viewed as a tractable medical problem, rather than a fact of life.
Interventions are chosen on the basis that they 1) act systemically and 2) have individually shown some lifespan-extending effect in naturally aged mice. In this way, we are specifically selecting rejuvenation therapeutics, as opposed to those which are purely preventative and/or require early life intervention. Therapies are also selected to have minimal mechanistic overlap, based on our current understanding of their mechanisms of action. The first four interventions selected for the initial study are rapamycin, hematopoietic stem cell transplant, telomerase upregulation via TERT gene therapy, and senolytic treatment.
I wish work on the Lifespan machine 2.0 using Daphina (water fleas) would progress. It could provide a much faster readout on whether multiple interventions synergise, and could be a good sanity test. With limited dollars to invest, a predictive tool of how mouse studies might go could be valuable.
That should be Longevity Escape Velocity (LEV) Foundation, right?
@Jay Roesch: Thanks. Typing on automatic some days.
pretty exciting! It looks like they will give updates as it goes on
Wonderful to think of the progress that will be made.
For the future, what about social support?
Colonies of mice living together?
"...and senolytic treatment". Inquiring minds want to know which ones. Fasting? DQ? Fisetine?
Everyone - just to say, please ask any questions you have - I will follow the comment feed and respond. In response to those I see so far:
@jimofoz - I like Daphnia as a model, but (a) it is phylogenetically distant from us and has very different aging (try searching 'daphnia AND "senescent cells"' in PubMed), and (b) it is structurally different and some therapies are impossible (such as stem cell treatments). I believe we are now at the point where only mammalian studies will get us to LEV fast.
@Jeremy Waletzky - we are indeed considering ways to make mice happier. More on that in due course.
@Thomas Schaefer - the choice of senolytic will be announced as soon as possible.
Hello, Dr de Grey. Are you planning some kind of special fundraiser for the next phase of the project? (With a fixed monetary goal, a time limit, etc.)
@ Antonio - no special fundraiser, no - we will start the next round as soon as we raise another $3M (or in six months or so, whichever is the later, since we need to design it and liaise with reagent suppliers etc). I will be continuously beating the bushes!
@ AdG, I been using SEN for donations from.my Amazon purchases. Your new longevity name is LEVF. But I believe someone ( maybe you) said to use a different name that would benefit your new organization since LEVF doesn't come up.
Could you or someone advise?
Thanks and Merry Christmas all.
@Robert - thanks for asking. LEV Foundation obtained 501c3 status quickly by being given a pre-existing one named Ichor Research Institute. (We are of course changing the legal name, but that takes time.) If you go to levf.org/donate and select the Smile option it will all work. Thank you so much in advance!!
@ Audrey, Awesome, thx so much. Been following your work for about 2 decades. Hope to eventually meet you.
@aubrey - Any thoughts on testing gut microbiome treatments (fecal transplantation, flagella injections? etc) in combination with other therapies? These are things that Reason has definitely spoken up for in his blog.
@AdG
Why do you believe that (transgenic) mouse models/studies translate in any meaningful way to humans? Big effects in short lived species are easy to achieve, in long lived species not so much.
A nice recent interview of Aubrey looking back to historic of this space and his approach, LEVF non-mainstream combination approach, industry/academia grant biases, the 4x Round 1 interventions etc .. Great to see Aubrey energetic as usual and going public again (did he ever stop?). I might go to Dublin this year....
https://www.youtube.com/watch?v=KEdRTzl2DgY