You mentioned one of the effects you experienced with this protocol was reduced appetite.
Why is this? What's it doing to the body to cause that?
Posted 19 July 2021 - 03:16 AM
You mentioned one of the effects you experienced with this protocol was reduced appetite.
Why is this? What's it doing to the body to cause that?
Posted 21 July 2021 - 04:41 PM
I have a question: Is there any relationship between fusion/fission and body temperature?
If this is so, we might use individual variations in body temperature to roughly understand whether a certain protocol is successful in inducing fusion/fission.
Posted 21 July 2021 - 06:24 PM
You mentioned one of the effects you experienced with this protocol was reduced appetite.
Why is this? What's it doing to the body to cause that?
It's just an observation, but certainly if you are producing ATP more efficiently, you should require less fuel, and thus will experience less hunger. Hunger is moderated by the hypothalamus, so increased ATP production with the same fuel availability may result in a reduced hunger signal. See Increased ATP content/production in the hypothalamus may be a signal for energy-sensing of satiety.
I have a question: Is there any relationship between fusion/fission and body temperature?
If this is so, we might use individual variations in body temperature to roughly understand whether a certain protocol is successful in inducing fusion/fission.
I've not seen anything on the effects of body temperature on mito morphology in humans, but it can make a considerable difference in hibernators vs non-hibernators in hypothermic situations. See this paper.
Also, there seems to be some dispute about the operating temperature of mitochondria. Since most of the heat of endotherms is due to the activity of mitochondria, it is expected that they will run hotter than the rest of the cell. Due to their small size, however, it was expected that this would be a tiny fraction of one degree. However, the following paper suggests it might be very large -- on the order of 10 degrees C.
we found that the rise in mitochondrial temperature due to full activation of respiration is as high as about 10 °C (n = 10, range 7–12 °C, compared to 38 °C, the temperature of the cell suspension medium). We also showed that respiratory chain (RC) activities measured in intact mitochondria can be increased up to threefold when assayed at the inferred mitochondrial temperature of intact cells.
https://www.ncbi.nlm...les/PMC5784887/
The activity going up with temperature is not surprising, as the rule of thumb in chemical reactions is a doubling of the rate with each 10 °C rise in temperature. So what effect will this have on defective mitochondria in the fissioned state, say during exercise? Myocyte mitochondria should run even hotter with exercise, but as mito membrane potential drops, the heat production should also drop. Thus the ATP output between mitochondria with good and bad mtDNA should be accentuated. But will that make any difference to PINK1/Parkin, giving that labeling for mitophagy requires zero membrane potential?
As for knowing whether you are in fission or fusion, the bicep curls to failure technique should be a good indicator, as long as you have defective mitochondria.
Edited by Turnbuckle, 21 July 2021 - 06:40 PM.
Posted 21 July 2021 - 06:39 PM
I've not seen anything on the effects of body temperature on mito morphology in humans, but it can make a considerable difference in hibernators vs non-hibernators in hypothermic situations. See this paper.
Also, there seems to be some dispute about the operating temperature of mitochondria. Since most of the heat of endotherms is due to the activity of mitochondria, it is expected that they will run hotter than the rest of the cell. Due to their small size, however, it was expected that this would be a tiny fraction of one degree. However, the following paper suggests it might be very large -- on the order of 10 degrees C.
The activity going up with temperature is not surprising, as the rule of thumb in chemical reactions is a doubling of the rate with each 10 °C rise in temperature. So what effect will this have on defective mitochondria in the fissioned state, say during exercise? Myocyte mitochondria should run even hotter with exercise, but as mito membrane potential drops, the heat production should also drop. Thus the ATP output between mitochondria with good and bad mtDNA should be accentuated. But will that make any difference to PINK1/Parkin, giving that labeling for mitophagy requires zero membrane potential?
Thanks for the answer. I understand that, theoretically, the issue is not easy to solve.
Those following the fission/fusion protocol might record their body temperature in fission and fusion days. This would empirically suggest an answer.
Posted 21 July 2021 - 06:42 PM
Thanks for the answer. I understand that, theoretically, the issue is not easy to solve.
Those following the fission/fusion protocol might record their body temperature in fission and fusion days. This would empirically suggest an answer.
I doubt body temp would be a good indicator, as that is kept in close control, whereas curls to failure shows a big difference.
Posted 21 July 2021 - 07:03 PM
I started the mitochondrial protocol in July of last year at a weight of 161 lbs. I also experienced reduced appetite. Without doing much I lost 10 pounds at a regular weight.
Posted 22 July 2021 - 03:42 PM
I doubt body temp would be a good indicator, as that is kept in close control, whereas curls to failure shows a big difference.
I hope not to bother you insisting on a similar point.
I understand that Turnbuckle sees no compelling argument for an appreciable effect of mito morphology on body temperature.
My question now is: can we say anything on the relation between fission/fusion and heart rate?
Posted 30 July 2021 - 04:23 AM
There are many drugs that can damage mitochondria, but certainly the most pervasive is sodium fluoride. A paper published this year examined the effect of fluoride levels on child intelligence in China and found —
Ug. I have been guzzling San Pellegrino by the 1L bottle. It has nearly 0.5 ppm of fluoride which approaches the "minimum recommended fluoridation level" for the US tap water which was lowered to 0.7 in 2015.
Posted 30 July 2021 - 04:29 AM
The problem for us following a carnivore diet is that if it doesn't work we don't know whether it's because our mitochondria are optimized or because we eat so much stearic acid that the N+R combo does not kick us into Fission.
For example, I followed the protocol doing the "push-ups to failure" bit and did not see the pattern at all. Control, Fusion and Fission days I did the same number of repetitions. And I don't believe that my mitochondria are already optimized.
Since I am doing Carnivore as an elimination diet it comes with a cost for me to substitute beef for something else to avoid nutritional Fusion. Nevertheless, I am planning on doing a chicken+fisk week and see if I can get in and out of Fission/Fusion.
Will post if anything interesting happens.
Saludos,
S.
I follow a carnivore diet (mostly beef) and my tracked progress on the current mitochondria protocol seemed consistent with Turnbuckle's experience.
Posted 07 September 2021 - 10:24 AM
I adjusted my weekly diet to enhance the effect of this great protocol, as stearic acid inhibits Fission and has a half-life of 17h
Thursday: Fruits only
Friday: Carb refeed (fasting till evening Fission dose)
Saturday: Fish with carrots and celery (fasting till evening Fusion dose)
Sun-Wed: Bulletproof Diet meals
Noticed reduced resting HR, better sleep, less hunger, faster recovery, better memory - all after 3cycles already.
Thank you for sharing this Protocol Turnbuckle
Posted 08 September 2021 - 01:58 PM
I adjusted my weekly diet to enhance the effect of this great protocol, as stearic acid inhibits Fission and has a half-life of 17h
How long fusion lasts will be greatly dependent on the source and dose. Ten grams of stearic acid triglyceride in a brownie will produce a much longer period of fusion than one gram of GMS. And there are alternatives for fusion, like sulforaphane, which has a half life of around two hours. The minimum cycle time will likely be dependent of the rate of mitophagy and biogenesis, and will vary with tissue type. Biogenesis is relatively fast while mitophagy (with the fission half cycle) is substantially slower.
Damaged mitochondria were efficiently sequestered within autophagosomes, but lysosomal fusion or acidification was significantly delayed. Surprisingly, engulfed mitochondria persisted in non-acidified vesicular compartments for hours to days after initial damage.
https://www.ncbi.nlm...les/PMC7144876/
From the experiment I reported a while back, 24 hours seems both sufficient and convenient for a half-cycle, either fission or fusion.
Edited by Turnbuckle, 08 September 2021 - 02:05 PM.
Posted 22 September 2021 - 12:06 AM
Posted 22 September 2021 - 10:18 PM
Any thoughts on whether taking betaine (trimethylglycine TMG) will impact the mitochondrial protocol?
Even though I've done many cycles in the past, I did mito1 and mito2 days both with 1g betaine, this time doing the dumbbell test. I got 50 reps on the mito1 day and 76 on the mito2.
I'm wondering either if I need betaine to get the most out of this protocol (I'm heterozygous for MTHFR), or whether betaine benefits everyone regardless of status.
Posted 27 September 2021 - 01:21 AM
I had a minor scare a couple of nights ago. I was putting the D-Ribose into my glass and managed to spill much more than 1 gram (maybe 5-10 grams) into the water. I figured what the heck it's only sugar so I mixed it in and drank it with the AKG and went to bed. About an hour later I woke up and my body was vibrating. It was like shivers from being cold but I was actually warm. This lasted maybe 10 minutes before I fell asleep again. When I got up in the morning I felt fine. Also, I use 1 gram of niacin (flushing) and not niacinamide for this protocol.
Posted 28 September 2021 - 04:25 PM
I had a minor scare a couple of nights ago. I was putting the D-Ribose into my glass and managed to spill much more than 1 gram (maybe 5-10 grams) into the water. I figured what the heck it's only sugar so I mixed it in and drank it with the AKG and went to bed. About an hour later I woke up and my body was vibrating. It was like shivers from being cold but I was actually warm. This lasted maybe 10 minutes before I fell asleep again. When I got up in the morning I felt fine. Also, I use 1 gram of niacin (flushing) and not niacinamide for this protocol.
10g of D-Ribose is A LOT all at once. It sounds like you had a hypoglycemic shock as D-ribose is known to reduce blood sugar levels.
Posted 28 September 2021 - 08:07 PM
An updated Mito protocol
The previous protocol can be found at post #1366
So I say get rid of them all, mutations and methylation alike.
The new protocol:
This new procedure is much simplified. It requires only two doses, Mito1 and Mito2, which are alternated on a daily basis.
Mito1 (fission)
● NAM+R, 1 g of each
● AKG, 1 g
● PQQ, 20 mg
Mito2 (fusion)
● GMS, 1 g
● AKG, 1 g
● PQQ, 20 mg
NAM+R (nicotinamide plus ribose) is a fission promoter, GMS (glycerol monostearate) is a fusion promoter, AKG (alpha-ketoglutarate) is a demethylase promoter, and PQQ is a biogenesis promoter. All of these are fast acting.
Hello to all the mito folks out there!
I am writing with a very important comment regarding the new protocol, as well as soliciting Turnbuckle and the community-at-large for a solution.
I first want to thank Turnbuckle for all his work on this topic and also on stem cell renewal. I learned a lot and benefited from both the knowledge and use of the protocols. Thanks to all of the other contributors as well.
My comment to everyone is to be very careful with AKG/AAKG if you have any type of depression or anxiety, or in my case low-level bipolar.
Background:
I began the new protocol a few weeks ago. During that time I started to feel very tired and out of it. Also very irritable, according to other. Of course, like usual, it took a while to put all the pieces of the puzzle together and didn't make the connection to AKG right away - and hence continued the protocol. It turns out that many (but not all) people who have depression or anxiety related conditions have very high levels of glutamate. The connection is well established, I have linked some articles below. More than that, once I stopped the AKG my own symptoms abated. Nothing like first-hand experience to validate.
It seems that at least one reason for elevated glutamate is that many people with depression/anxiety conditions have trouble converting glutamate to GABA, so glutamate builds up. There's probably more to it.
If you suffer from a condition and have noticed changes since starting this protocol - AKG may be why.
So that's a cautionary tell for everyone. It leaves me (and others if they head this warning) with a problem - is there a good alternative that will have a similar effect to AKG in this protocol? Obviously there is no perfect replacement, but we if consider the action of AKG in the protocol there may be a "next best" that doesn't increase glutamate. It's my understanding that AKG is converted into GABA, is that right? Is that the mechanism that drives the benefit in this protocol?
Those are the questions I pose to the community. I'd like to find an alternative to AKG if that is at all possible.
Thanks!
Links to AKG and bipolar/depression/anxiety (there are endless articles):
https://www.frontier...021.640977/full
https://psychnews.ps...pi.pn.2014.7a17
https://www.karger.c...Fulltext/496294
https://grantome.com...R21-MH110850-02
https://www.nature.c...icles/tp2017141
https://www.medscape...ressive-illness
Glutamate --> GABA:
https://bebrainfit.c...urotransmitter/
https://www.geneticl...urotransmitter/
Glutamate - GABA problem, genetic?:
https://drkirshner.c...ety-be-genetic/
https://www.holistic...nxiety-genetic/
Posted 28 September 2021 - 08:32 PM
Those are the questions I pose to the community. I'd like to find an alternative to AKG if that is at all possible.
If you have a problem with AKG, you could eliminate it from the fusion part, and if you still have a problem, you could eliminate it from the fission side as well. Most of the work in removing defective and methylated mtDNA is done by combining fission and biogenesis. I expect it will take longer, but it doesn't take that long to begin with.
Edited by Turnbuckle, 28 September 2021 - 08:35 PM.
Posted 28 September 2021 - 11:26 PM
10g of D-Ribose is A LOT all at once. It sounds like you had a hypoglycemic shock as D-ribose is known to reduce blood sugar levels.
Thanks, I was wondering what it could be. It seems D-Ribose stimulates an insulin release. I was afraid the combination with niacin might have nuked my mitos.
Posted 29 September 2021 - 04:20 PM
Posted 29 September 2021 - 06:02 PM
Just in case you will find something interesting here:
AMPK activator is available from LEF. I found a reaction path diagram that showed that AMPK is essentially "exercise in a pill". So I ordered a bunch of it up during the lockdowns last year when I could not go to the gym. It worked for me.
Posted 29 September 2021 - 10:14 PM
If you have a problem with AKG, you could eliminate it from the fusion part, and if you still have a problem, you could eliminate it from the fission side as well. Most of the work in removing defective and methylated mtDNA is done by combining fission and biogenesis. I expect it will take longer, but it doesn't take that long to begin with.
Turnbuckle - thanks for the quick response.
Yeah, there's no way it's worth messing with brain chemistry on this one. So, just to clarify, you think that by doing the rest of the protocol: D1 NAD+R, PPQ; D2 GMS, PPQ will still work just not as effectively?
Any sense in trying to add GABA?
Thanks!
Posted 02 October 2021 - 06:49 PM
Turnbuckle - thanks for the quick response.
Yeah, there's no way it's worth messing with brain chemistry on this one. So, just to clarify, you think that by doing the rest of the protocol: D1 NAD+R, PPQ; D2 GMS, PPQ will still work just not as effectively?
Any sense in trying to add GABA?
Thanks!
You could also space out the treatments, and you might look at adding theanine and/or taurine.
Edited by Turnbuckle, 02 October 2021 - 06:50 PM.
Posted 31 December 2021 - 07:28 PM
Posted 31 December 2021 - 11:47 PM
Vit C will stop fission, so skip it on the fission day. I believe the same it true with the olive leaf extract. You can take both with fusion.
You may want to start fission off at half a dose. For many, the first few fission cycles give flu like symptoms. If that happens, you can give the body a few days to recover and/or cut it short with a dose of vitamin C.
Posted 31 December 2021 - 11:55 PM
Posted 02 January 2022 - 04:05 AM
Edited by Old grandpa, 02 January 2022 - 04:06 AM.
Posted 02 January 2022 - 07:58 AM
I sometimes would take a gram of taurine with the GMS.
Posted 05 January 2022 - 05:30 PM
Do PQQ and CoQ10 promote mito fission or mito fusion?
Same question about ALCAR - fission or fusion or neither? although I think there may not be enough data out there to make that determination.
thanks
Edited by Phoebus, 05 January 2022 - 05:35 PM.
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