A Combination of Rapamycin and Trametinib Extended Maximum Lifespan by up to 35%

RapAdmin · 2024-07-29T02:22:24.091Z

Some very good results (significant reduction of side effects) from intermittent dosing of trametinib:

Intermittent dosing in these examples is defined as: a five-week-on and three-week-off schedule.

In February 2016, after almost a full year of continuous daily dosing, she started a 3-week drug holiday before resuming treatment using an intermittent schedule of 5 weeks of treatment followed by a 3-week break, per 8-week cycle. This approach was associated with a considerable reduction in her fatigue and an improvement of her well-being.

Like patient 2, this patient noted considerable improvement in her sense of well-being after converting to an intermittent therapy regimen. On treatment for now 18 months (13 months on intermittent drug administration), this patient continues to tolerate dabrafenib and trametinib at full dose on the five-week-on, three-week-off schedule and has resumed work unencumbered by symptoms from her disease or from the treatment.

Both patients experienced considerably fewer adverse events and no cumulative toxicity with intermittent dosing, permitting them to resume active lifestyles largely unencumbered by the anticancer treatment.

Results: Both patients showed rapid clinical improvement upon starting the regimen. They also noted improved tolerance of treatment upon transitioning to the intermittent dosing schedule. They continue to show evidence of antitumor activity 27 and 18 months respectively from the start of treatment and 15 and 13 months respectively from the start of the first break using intermittent dosing.

Intermittent Dosing of Dabrafenib and Trametinib in Metastatic BRAFV600E Mutated Papillary Thyroid Cancer: Two Case Reports

PubMed Central (PMC)

Intermittent Dosing of Dabrafenib and Trametinib in Metastatic BRAFV600E...

Background: A multi-institutional, randomized phase II trial of continuous dosing of dabrafenib with or without trametinib is ongoing in metastatic thyroid cancer. Preclinical evidence and emerging clinical experience in other cancers support...

RapAdmin · 2024-07-29T04:13:56.981Z

Here is a phase 2 clinical trial looking at intermittent dosing with trametinib:

Continuous versus intermittent BRAF and MEK inhibition in patients with BRAF-mutated melanoma: a randomized phase 2 trial

PubMed Central (PMC)

Continuous versus intermittent BRAF and MEK inhibition in patients with BRAF...

Preclinical modeling suggests that intermittent BRAF inhibitor therapy may delay acquired resistance when blocking oncogenic BRAF[V600] in melanoma[,] . We conducted S1320, a randomized, open-label, phase 2 clinical trial () evaluating whether...

The intermittent dosing arm used the same doses during weeks 1 and 5–8 of each 8-week cycle (5 weeks on). No therapy was given during weeks 2–4 on the intermittent therapy arm (3 weeks off).

Adverse events.

All adverse events assessed as possibly, probably, and definitely related to study treatment. On the continuous therapy arm, 38 patients (36%) experienced grade 3 adverse events, and 7 (7%) experienced grade 4 events, while on the intermittent therapy arm, 31 patients (31%) experienced grade 3 adverse events, and 3 (3%) experienced grade 4 events (p=0.46 for grade 3, p=0.33 for grade 4). The most common grade 3–4 adverse event across both arms was fatigue. There was a significant difference in the incidence of grade 3 and 4 pyrexia, (6 patients on continuous dosing vs 1 patient on intermittent dosing, p<0.001).

There has been at least one additional (2024) clinical study using intermittent dosing schedules, and larger numbers of patients, for trametinib, but it is behind a paywall. If anyone can access and post it please do, as it would give us more information on the side effect reduction from continuous to intermittent dosing schedules.

PubMed

A randomised phase 2 study of intermittent versus continuous dosing of...

INTERIM findings are consistent with other recent clinical trials reporting that intermittent dosing does not improve efficacy of BRAF+MEK inhibitors.

RapAdmin · 2024-07-29T07:44:46.359Z

I don’t think there is any hurry… we’re all going to get some extra time from the rapamycin, and it seems some de-risking could and should be done by longevity researchers on trametinib before even periodic dosing is tested by biohackers:

Anyone taking Trametinib?

Do not take trametinib for longevity purposes. I worked on synthetic lethal chemo combinations in cancer at a startup for years. We tested this compound and it is not a good idea. The Erk pathway is very important for most epithelial cells. Stick to low risk acarbose and rapamycin combinations and do not consider trametinib. If you have melanoma or another type of solid tumor type then you could consider trametinib. Just trying to prevent you from causing long term damage.

Anyone taking Trametinib?

The problem is most targeted protein kinase inhibitor clinical trials are done in patients that failed first line chemo so this is a drug population that can’t be studied long term since they often have less than a year to live. I expect most long term side effects are not documented. The side effect profile does not look promising for a drug used for longevity purposes. The study of combination longevity effect also observed a significant reduction of fecundity so I hope you do not plan on having children. This is presumably also going to be combined with rapa which is also known to reduce fecundity. So I will restate that MEKi drugs all around are a bad class of drugs to consider for longevity based on my risk reward calculations.

Anyone taking Trametinib?

And I support the right of an individual to make his own choices regarding his personal health and the medications he buys. And if you decide to proceed, I hope it works out for you. With that said, this is a discussion forum. And I think most people here would agree that quality of evidence, cost, and risk/benefit ratios are all important considerations before adding a new compound to one’s antiaging regimen. For me, this medication wouldn’t satisfy any of these criteria. At standard dosages, almost half of patients become anemic. Elevated AST and hypoalbuminemia occur in 60 and 42%, respectively, suggesting liver toxicity. Neutropenia occurs in 44% of patients. And leukopenia occurs in 38%. And the list goes on. It’s one of those medications where, if you’re going to take it, you’d better have a damn good reason for doing so. And then careful monitoring and management of these adverse effects if they do occur. Additionally, the primary reason for considering it for longev…

DeStrider · 2024-07-29T07:47:38.225Z

Good points. Best to avoid for now.

Cohen · 2024-07-29T08:03:25.061Z

In patients, trametinib is used for the treatment of metastatic melanomas [76] and has also been used in clinical trials for the treatment of solid tumours [77] [78]. At a dose of 2 mg trametinib once a day, the drug was well tolerated with only small side effects including skin rash, diarrhoea, fatigue and retinopathy [77]. Average peak plasma levels in patients receiving 2mg trametinib daily were between 5.5 and 7.5ng/ml [77] [78], which is significantly higher than the 0.1ng/ml in mice fed with the lifespan extending dose of 1.44mg trametinib/kg food. In a mouse model of mucosal melanoma, administering trametinib via oral gavage resulted in an average peak concentration of 23.8ng/ml [79], which is more than 200-fold the concentration required for lifespan extension. Although trametinib plasma levels might not be directly comparable between chronic feeding and acute application, these results suggest that higher trametinib doses are required for its anti-cancer effect than for lifespan extension. Consistently, tumour progression or load were not significantly changed in long-lived mice treated with trametinib. The effect of trametinib at the chosen concentration of 1.44mg/kg on lifespan and health at old age was mild, indicating that we underdosed and that the optimal dose for lifespan extension might be higher. In the pre-test, a dose of 2.88 mg/kg trametinib did not cause detrimental side effects. Thus, this can be used as a guideline for future studies to optimize the dose of trametinib for maximal lifespan extension. Additionally, it would be interesting to determine whether late-onset or intermittent feeding recapitulates the effects of continuous trametinib treatment on mouse lifespan, as this would be key to enhance adherence and feasibility of trametinib treatment in humans.

Cohen · 2024-07-29T08:15:32.030Z

The half-life is also long, so you can take it once a week or every two weeks without any hassle.

nikney · 2024-07-29T19:58:22.616Z

The half-life of trametinib is 4-5 days, almost twice as long as rapamycin. If you take rapamycin every day, you may experience a lot of side effects. But once a week, it causes almost no side effects. Couldn’t a similar situation occur for trametinib taken once every two weeks? Since no one has tried it, we naturally have no information. But I think there is an unnecessary fear about this.

RapAdmin · 2024-07-29T20:21:02.694Z

There is definitely a reasonable argument that dosing once every week or two with trametinib could have very low or minimal side effects, but it would be good for a medical group to do such a test with regular blood and functional monitoring for the more serious potential risks; retinal issues, heart issues (ejection fraction), blood pressure, kidney function, anemia, etc… It would be very hard, if not impossible, for a biohacker to be able to do this type of monitoring over a period of many weeks or months, so I really think we need to lobby a longevity research group to start a small clinical study to do this, and publish the results.

@Livin and @Vlasko , given your experience with, and knowledge about, this drug what are you opinions? How would you design a study to test its safety in a pulsed once weekly or once every two week dosing schedule?

KarlT · 2024-07-29T20:53:20.706Z

nikney:

But I think there is an unnecessary fear about this.

We could use a few human test subjects if you’re volunteering?

Cohen · 2024-07-29T22:23:27.644Z

And who’s going to pay for the trial?

RapAdmin · 2024-07-29T22:28:32.464Z

I’m going to write up a proposal, try to get some researcher’s to partner with, then submit a the idea to Impetus Grants. I’ll post the proposal here to get people’s feedback on it before I approach the researchers.

What I’m proposing is effectively a new phase 1 clinical study (perhaps a dozen participants or so). I’d be following this type of guideline: A Comprehensive Guide to Phase 1 Clinical Trials

It seems like a small phase 1 clinical study like this with a commercially available, FDA-approved drug, might cost something like $200K to $300K; similar to the dental rapamycin study: New Study Funded: Towards reversing periodontal disease using Rapamycin

Longevity Impetus Grants

RapAdmin · 2024-07-30T03:15:03.577Z

And, more good news on trametinib; it appears it goes off patent in 2025, so at that point it becomes very inexpensive.

Trametinib (Mekinist)
Like dabrafenib, trametinib is used against melanomas containing the activating BRAF V600E or V600K point mutation [44]. It was authorized by EMA in June 2014 and the EU patent is expected to last until July 2029. However, trametinib was authorized by FDA in May 2013 and the patent is expected to expire in September 2025, resulting in three years less market exclusivity in the US.

Source: Overview of the patent expiry of (non-)tyrosine kinase inhibitors approved for clinical use in the EU and the US - GaBI Journal

DeStrider · 2024-07-30T03:23:10.735Z

Maybe it would be a good ITP candidate for verification?

Luminary · 2024-07-30T03:31:32.074Z

I don’t believe there is any evidence that low-dose Trametinib has a significant life extending effect which is the main issue for this. Would it be possible perhaps to try a low-dose Trametinib trial in the wormbot?

RapAdmin · 2024-07-30T03:46:49.598Z

Cohen:

Average peak plasma levels in patients receiving 2mg trametinib daily were between 5.5 and 7.5ng/ml [77] [78], which is significantly higher than the 0.1ng/ml in mice fed with the lifespan extending dose of 1.44mg trametinib/kg food.

See the earlier post by @Cohen

I also just realized I mis-interpreted the 1.44mg/kg as per kg of weight of the mouse, whereas its actually a measure of drug in the food.

Gokhan · 2024-07-30T14:09:14.474Z

Dosing to match mice plasma levels

The lifespan-extending dose of trametinib (1.44 mg/kg diet) resulted in plasma levels of ~0.1 ng/ml in mice. This is significantly lower than the 5.5-7.5 ng/ml peak levels observed in human patients receiving 2 mg daily doses for cancer treatment. [1]
Considering trametinib’s long elimination half-life of 3.9 to 4.8 days in humans, an appropriate starting dose for human longevity trials might be 0.25-0.5 mg taken orally once or twice weekly. This weekly dose, approximately 1/8th-1/4th of the standard 2 mg daily dose used in cancer treatment, aims to maintain plasma levels similar to those observed in the long-lived mice (around 0.1-0.2 ng/ml) while accounting for the drug’s extended presence in the body.
Trametinib is sold in 0.5mg tablets. A single 0.5mg tablet can be obtained for $21 in a country like Turkey. If one were to use 0.5mg weekly, the yearly cost of the drug would be $1100.
We can follow the same principle that Dr Blagosklonny has long proposed for Rapa: The optimal longevity dose is the highest dose without side effects.
As an experiment, Trametinib timing can be aligned with intermittent Rapamycin timing to maximize the “fasting-like” effects (two nutrient sensing pathways blocked simultaneously).

[1] A combination of the geroprotectors trametinib and rapamycin is more effective than either drug alone, Gkioni et al, 2024 (preprint)

Trametinib user experience (Link)

In 2020 I ran trametinib in 2 separate experiments. I was forced to discontinue quickly due to notable unpleasant side effects.
Dose: 1mg/day
This was based on studies showing triple combo of rapa lithium tranetinib extending life close to 50%. I had calculated 4mg/day [based on the fruit fly study] and started light to be safe. Maybe I got it wrong?? Took a few days to feel like shit.
What were the side effects? feeling poisoned. drained. off

(Not Mine – From another Rapamycin group. Sharing because it’s very interesting!)

Gokhan · 2024-07-30T14:21:20.493Z

Triple Drug Combination Targeting Nutrient-Sensing Network Dramatically Extends Lifespan in Fruit Flies (2019)

This study investigated the effects of combining three drugs that target different components of the nutrient-sensing network to extend lifespan in fruit flies. The researchers tested rapamycin (an mTOR inhibitor), trametinib (a MEK inhibitor), and lithium (a GSK-3 inhibitor) individually and in combination. They found that double combinations of these drugs produced greater lifespan extension (around 30% on average) compared to any single drug alone (11% on average). Most remarkably, the triple combination of all three drugs extended median lifespan by 48%. The drug combinations did not significantly alter feeding behavior or food intake, suggesting the lifespan effects were not due to dietary restriction.

Importantly, the study also found that lithium was able to counteract some negative side effects of the other drugs. Specifically, lithium reversed the increased triglyceride levels and starvation resistance caused by rapamycin treatment. The researchers conclude that simultaneously targeting multiple nodes of the nutrient-sensing network with drug combinations may be an effective strategy to maximize longevity benefits while minimizing side effects. They suggest this “polypharmacology” approach of combining established pro-longevity drugs could potentially be developed into therapies to improve health in late life.

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Gokhan · 2024-07-30T14:25:16.859Z

Targeting RAS/MAPK Signaling: A Promising Approach for Extending Healthspan and Lifespan (2022)

This review examines evidence that inhibition of the RAS/MAPK signaling pathway can extend lifespan and improve healthspan across multiple model organisms. Genetic studies in yeast, worms, flies and mice have shown that reducing activity of various components of the RAS/MAPK pathway can increase lifespan and enhance resistance to age-related decline. The effects appear to be evolutionarily conserved, as variants in human RAS pathway genes have also been associated with longevity. The RAS/MAPK pathway integrates with insulin/IGF signaling, a well-established aging regulatory pathway, suggesting it may be a key node in controlling the aging process.

Based on these genetic findings, the authors discuss the potential for repurposing existing RAS/MAPK inhibitor drugs as “geroprotectors” to promote healthy aging in humans. Several compounds that directly or indirectly inhibit RAS/MAPK signaling, including trametinib, statins, acarbose, and metformin, have shown lifespan-extending and health-promoting effects in model organisms. However, challenges remain in translating these findings to humans, including potential side effects and the need to determine optimal dosing and timing of interventions. Nevertheless, the authors argue that pharmacological modulation of RAS/MAPK signaling represents a promising avenue for developing interventions to extend healthspan and lifespan in humans.

Trametinib: RAS/MAPK/ERK Signaling Pathways and Mechanism of Action

signaling pathways

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RapAdmin · 2024-07-30T19:39:49.435Z

I wanted to add this comment from @Ray1 here, as its relevant. Just as with rapamycin, the general perception of medical professionals (given the typical cancer dosing levels used with trametinib) is quite negative. This suggests that, just as with rapamycin, getting an IRB approval for study in healthy humans may be a challenge… but, we’ll see.

A Summary of the top Life Extension Approaches (by Krister Kauppi)

I had an interesting conversation with a woman who runs a foundation for research into gastric cancer. The foundation had helped find a study in South Korea to test an MEK inhibitor for precancerous lesions of the stomach. The Korean government decided not to authorize the study. It is one thing to give an MEK inhibitor to children with a deadly cancer who have no other hope. Giving a drug with dangerous side effects to people who may not have a terminal disease at all is a whole different matter. This is why we need testing in creatures other than mice and humans. Some very important questions cannot be answered until we have some other test subjects. I sure hope the dog aging project keeps going. On Trametinib Grant funds research for therapies to prevent stomach cancer - VUMC News

jnorm · 2024-07-30T20:05:59.876Z

Warning: mechanistic speculation ahead…

Chronic rapa (for 4 mo or 16mo) in male mice can oppose the increased ERK activation that normally occurs during that time frame in liver and kidney. So it’s not actually reducing ERK activation below the level present in young mice—just preventing the age-associated increase.

PubMed Central (PMC)

Rapamycin, Acarbose and 17α-estradiol share common mechanisms regulating the...

Rapamycin (Rapa), acarbose (ACA), and 17α-estradiol (17aE2, males only) have health benefits that increase lifespan of mice. Little is known about how these three agents alter the network of pathways downstream of insulin/IGF1 signals ...

Even if we can just maintain youthful levels of ERK activation, I think that is huge. Because ERK is one of the primary positive regulators of AP-1 activity. AP-1 is a transcription factor recently shown to be a master regulator of epigenetic remodeling in aging. Presumably more ERK activity->more AP-1 activity->more rapid loss of epigenetic information

PubMed

The activity of early-life gene regulatory elements is hijacked in aging...

A mechanistic connection between aging and development is largely unexplored. Through profiling age-related chromatin and transcriptional changes across 22 murine cell types, analyzed alongside previous mouse and human organismal maturation datasets,...

To get ERK below even youthful values, you could periodically pulse a bona fide MEK or ERK inhibitor.

Another alternative to trametinib would be function-selective (as opposed to ATP-competitive) ERK inhibitors like SF-3-030, which affects expression of fewer genes than ATP-competitive ERK inhibitors.

PubMed Central (PMC)

Effects of ATP-competitive and function-selective ERK inhibitors on airway...

Increased airway smooth muscle (ASM) cell mass and secretory functions are characteristics of airway inflammatory diseases, such as asthma. To date, there are no effective therapies to combat ASM cell proliferation, which contributes to...