Pages

Thursday, 28 February 2019

Who lives in Libya? And Raising the level of BHB in your blood.



Today’s post is mainly about some “home-research” that was sent to me by a company that sold me C8 oil (caprylic acid MCT oil).
It is not peer-reviewed research, but it is a well thought out home experiment measuring the level of the ketone BHB in the blood of two healthy young adults testing a range of commercially available products. It is important to note that BHB was measured in blood and not urine, which is a big plus for the experiment.

Dr D’Agostino’s starting dose
First, a recap of where we started a few months ago in this blog.
One of the leading ketone researchers is Dr D’Agostino and his suggested starting dose on ketone supplements is 10 ml of Ketoforce and 10ml of C8/caprylic acid.
We saw in earlier posts that the amount of BHB produced by taking C8 is highly dependent on whether it is taken with food. Taken on an empty stomach resulted in more BHB in the bloodstream.
10 ml of KetoForce contains 4g of BHB along with 500mg of sodium and 500mg of potassium.

BHB salts and BHB esters
Until recently BHB supplements were all salts, so the BHB was combined with sodium, potassium, calcium or magnesium.
Taking large amounts of sodium, calcium, potassium or magnesium will likely disturb the electrolytes in your body and may cause you problems.
Ketone esters are composed of a ketone molecule like BHB bound to a ketone precursor using an ester bond (butanediol or glycerol).
Ketone esters are commercially available, but very expensive.  They are currently used by athletes and the US military.
The first commercial product was developed based on the work of researchers at Oxford University in the UK, but the resulting product cannot legally be sold in the UK. HVMN, a company in the US, are currently selling it as a supplement for athletes. I wonder if it has been declared a banned substance by sports doping agencies.
Some of the research:-

Ketone bodies are the most energy-efficient fuel and yield more ATP per mole of substrate than pyruvate and increase the free energy released from ATP hydrolysis. Elevation of circulating ketones via high-fat, low-carbohydrate diets has been used for the treatment of drug-refractory epilepsy and for neurodegenerative diseases, such as Parkinson’s disease. Ketones may also be beneficial for muscle and brain in times of stress, such as endurance exercise. The challenge has been to raise circulating ketone levels by using a palatable diet without altering lipid levels. We found that blood ketone levels can be increased and cholesterol and triglycerides decreased by feeding rats a novel ketone ester diet: chow that is supplemented with (R)-3-hydroxybutyl (R)-3-hydroxybutyrate as 30% of calories. For 5 d, rats on the ketone diet ran 32% further on a treadmill than did control rats that ate an isocaloric diet that was supplemented with either corn starch or palm oil (P < 0.05). Ketone-fed rats completed an 8-arm radial maze test 38% faster than did those on the other diets, making more correct decisions before making a mistake (P < 0.05). Isolated, perfused hearts from rats that were fed the ketone diet had greater free energy available from ATP hydrolysis during increased work than did hearts from rats on the other diets as shown by using [31P]-NMR spectroscopy. The novel ketone diet, therefore, improved physical performance and cognitive function in rats, and its energy-sparing properties suggest that it may help to treat a range of human conditions with metabolic abnormalities.






The Military as Early Adopters
For centuries military forces have sought to gain a competitive advantage using drugs, so it is not surprising that the current US military are interested in ways to increase physical endurance.

Survival rations for downed airmen, or just reducing the weight of food rations for Special Forces, would be obvious applications for BHB esters.
In modern times it was the Germans who made the greatest military use of drugs with their Pervitin tablets that enabled their soldiers and airmen to fight for days without sleep. Pervitin turned out to be Methamphetamine. Such drugs are used today by irregular forces.
Extensive use was made of drugs to counter altitude sickness in Afghanistan, first by the Russians and later by the Americans. Diamox/Acetazolamide is the Western drug and this same drug has application in some channelopathies and some types of autism.
Drugs that improve exercise endurance, and so are likely banned for use in sport, are potentially interesting for people with mitochondrial disease, vascular abnormalities and even glucose transporter dysfunctions. In short if you have restricted ATP production in your brain, anything that can overcome whatever the route problem is, should improve brain function. Alzheimer’s disease is a good example where apparently quite different reasons result in reduced power output within the brain. 
I thought it was encouraging to see that military funding is being used to develop medical therapies for PTSD and suicide prevention. The latter was the application for the hormone TRH, which I suggested as a possible autism treatment, since it affects a chain reaction of important hormones affecting mood.

The n=2 home trials of BHB-raising supplements

You can read the full report by clicking the link below


I have extracted some interesting highlights.

·      HVMN and KE4 are very expensive ketone esters (red and green lines)

·      C8 MCT oil is the product that I currently use (20ml a day) (purple line)

·      Keto Max and KETOCANA are ketone salts (blue and orange lines)































 Recall an earlier graphic of "the ketone zone" so you can put BHB levels into context.





Summary: The Takeaways

·       We confirmed that ketone supplements increase ketones: All of the ketone supplements tested resulted in an increase in ketones for a temporary time period.

·       Rapid 3-Hour Windows: Ketone esters and ketone salts rapidly increase ketones within 30 minutes. The effects last for a ~3 hour period.

·       Slow 5-Hour Window: C8 MCT oil increases ketones more slowly. However, the ketone increase lasts for a more prolonged period of ~5 hours (see C8 MCT Oil research review covering this).

·       What Does this Say About When to Use Which Supplement? This is a complex question that requires further investigation into the different applications. However, we have three hypotheses to start with based on these results.

1.     For higher ketone boosting needs: If you are looking to boost ketones into the therapeutic range of 2-4mmol, it is more cost effective to take KetoCaNa (Ketone Salts). But a more gut tolerable option would be a Ketone Ester – at a greater price. Both are able to boost ketones enough to meet this target.

2.     For lower ketone boosting needs: If you are looking for less than a 1 mmol boost in ketones, the most cost effective and convenient (longer duration) approach is via C8 MCT oil. This may be most relevant to A) People not on ketogenic diets who want some of the ‘satiation benefits’ of ketosis, and B) People on ketogenic diets who already have raised ketones and only want a small additional boost (e.g. you’re at 1 or 2 mmol, and want to increase to 2 or 3 mmol respectively).

3.     For the highest ketone boosting needs: Should you want a greater increase in ketones for any reason Ketone Esters are the best option (this article explores where and why this may be interesting)


My conclusions
The effect of C8 is slightly different to Ketone salts like Ketoforce and I think D’Agostino’s advice to combine them is wise.

A dose of 20ml of C8 appears a good upper limit, since its effect at producing BHB gradually fades. Better to make sure it is taken without food to maximize the effect. Even though it is the cheapest supplement there appears to be no point taking larger doses like 50ml.
Ketone salts are definitely limited by their composition of sodium, potassium, calcium or magnesium. I think high doses are extremely unwise. D’Agostino’s 10 ml of Ketoforce seems safe.
Ketone esters are very expensive, but do actually provide a genuine energy-boosting level of BHB, which will also trigger all the other suggested effects of BHB (summarized in the old post below), quite possible at increased levels.


So I suppose the ideal autism research study would be to use KetoneAid KE4 or the HVMN BHB Ester, as used by the US military.

I expect the BHB Ester would have a big effect on someone with Alzheimer’s disease. They have a problem with the glucose transporter at the blood brain barrier and with reduced insulin sensitivity. The large amount of BHB from the ester supplement would provide an alternative fuel for the mitochondria, which are not producing enough ATP from glucose to power the brain.
We saw that Nestle is investing in MCT as a nutraceutical for Alzheimer’s. Today’s home research suggests that high doses of MCT are not going to be effective at raising BHB levels in the blood to a very significant level. BHB esters look much more promising.

This would be an expensive Alzheimer’s therapy, but still much cheaper than relocating to a care home. 

I did check and there actually is a case history; it is a physician wife treating her own husband who has early onset Alzheimer's. She read the research and translated it into a novel therapy for him. Nice work! This would of course be frowned upon in most countries as treating hubby like a guinea pig and doctors are not meant to treat family members, but to me it looks like the most caring thing she could do.  The good thing is that she published the result. Mainstream doctors treating their own children with autism, or even sometimes others, rarely seek to publish/share their results, so helping to maintain the convenient false perception that all autism treatments are just quackery (some are, while some clearly are not).
  • After six to eight weeks of taking 28.7g of the KME thrice daily, he began to exhibit improvement in memory retrieval, spontaneously discussing events that occurred up to a week earlier. He was again able to perform more complex tasks, such as vacuuming, washing dishes by hand, and yard work.
  • Plasma βHB levels were measured occasionally to assess KME-plasma βHB dose-response relationships (Fig. 2). Noticeable improvements in performance (conversation, interaction) were observed at higher, post-dose βHB levels, compared to pre-dose values.

  • In treatment of TP’s long-standing AD dementia, KME-produced repeated diurnal elevations of circulating βHB levels were clearly effective, during the 20-month study, in improving behavior, and cognitive and daily-activity performance. The physician-caregiver noted that performance seemed to track plasma ketone concentrations, with conversation and interaction declining as levels fell toward baseline. From requiring almost constant supervision, TP became much more self-sufficient on KME

The question in autism is what level of BHB do you need to maximize the effect and how long does this spike in blood BHB produce its beneficial effect. Do you need a constant level for 24 hours (I think not)? Do you need one BHB elevation/spike a day? Does a second daily dose have any benefit?
The BHB ester would be a good research tool, since it should not disturb electrolyte levels.


Who does live in Libya?
Anecdotal evidence has always got to be taken with a large pinch of salt, but if all you are doing is an N=1 trial that is often all you have got.

From more than half a year of experimenting with the combination BHB salts and C8 oil, the effect is clear. It causes an increase in relevant speech, directly related to current activities. You could call this unprompted commenting.
Monty will now answer the phone at home, rather than just hanging up to stop the annoying ringing noise, or having an ultra-trivial conversation. He will have a functional conversation in either of his two languages. This was particularly noted by his Grandmother as an improvement.

The good thing is the increased conversation fades when BHB/C8 is paused and returns when re-started.
Along the way we have discovered that not all BHB salts are equal. The Ketoforce liquid is the best, because it has most effect and does not disturb electrolytes, as Primaforce BHB powder appeared to, not by much, but enough to have an impact.

Using a mixture of C8 + C10 oil, produced a negative effect (aggression) after a few weeks. So while C10 may have a unique effect on mitochondria, beneficial to some, it was not tolerated.
10ml of Ketoforce and 20ml of C8 a day means one bottle of Ketoforce and one litre of C8 lasts 50 days.

The beneficial effect is not on the magnitude of bumetanide. The Ketoforce/C8 therapy costs 15 times more than bumetanide, but I think that really just means that generic bumetanide is extremely cheap.
Adding the small 0.5mg dose of Clemastine in the evening does seem to have an incremental effect after a few weeks.

It does appear to manifest itself again in improved speech. Now the comments are not related to current activities, but also past events and making connections.
“Colin has a moustache, like Poirot”
Colin is a friend of mine who Monty last saw a few months ago. He does have a moustache and so does Hercule Poirot.
The strangest recent “conversation” started with:-

“Who lives in Libya?    Do Indians live in Libya?” asked Monty
“No, Indians do not live in Libya, Arabs live in Libya”, I replied.
“Indians live in London” he countered
            “Yes, some Indians do live in London, but a lot more live in India”
“Who lives in Israel?” he asked    (We did recently visit Jerusalem)
            “Jewish people and Arabs live in Israel”, I replied
            “Who lives in France?” I asked
“Leopoldine” (a former classmate from school) he answered
            “Who lives in Italy?” and so it continued.

This is not the sort of “conversation” you normally have with Monty. This was the longest ever "conversation".
You would not expect him to recall that London has a large population of Asian descent. He lives far away.

Is this the cumulative effect of BHB/C8, or an emerging benefit of a quarter dose of an OTC hay fever drug?

Clemastine, taken in the evening, has had no negative side effects and is not expensive. $10 buys 60 pills that will last 4 months. Daniel Kerlinsky, the enlightened US psychiatrist we encountered in a post a while back, was keen to point out that it takes months for low dose Clemastine to show its effect (myelin, microglia or both).
In our case BHB/C8 looks like it is heading towards being included in the PolyPill. The only side effect is feeling thirsty, which is manageable. I am surprised to be considering adding what is a Californian diet therapy to my son’s autism therapy. Incidentally he has not lost any weight, he continues to gain it.

The jury is still out on Clemastine. Due to the onset of its potential benefit being very slow, it is not so easy to make a withdrawal trial (stopping a therapy, seeing if the believed effect is lost and then restarting to see if that effect returns). I will wait to see the feedback of other readers of this blog.




34 comments:

  1. Hi Ling,

    Hope all is well!

    Ling, I've been super busy with work and my personal project over the last couple of months, so I haven't had time to post much, but I just saw the following paper today and wanted to make sure you saw it:

    https://www.frontiersin.org/articles/10.3389/fnmol.2019.00033/full

    Just in case you hadn't seen it yet (but knowing you, you've probably been all over this for a while ;-)), I also ran into the following one after reading the one above:

    https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6364870/

    Ling, I hope the above is helpful!

    Your friend in snowy Canada,

    AJ

    ReplyDelete
    Replies
    1. AJ, you were actually in my thoughts. :-)
      Thanks for spotting those articles, to my surprise I had not seen either of them before. Highly interesting!
      I've been superbusy myself, documenting all my findings from last year, and I thought I was as up to date with the research as possible. Documentation has been a crazy amount of work, but now I see more clearly what pathways I need to patch treatmentwise. Anyway, my efforts now will be more towards testing stuff and perhaps networking as well. Or, ahem, maybe spend more time with my family and less with PubMed...

      /Ling

      Delete
    2. Hi Ling!

      I'm so glad you hadn't seen them yet. I really hope there is at least one useful nugget of information there for you.

      Yes, I know exactly what you mean about PubMed :-) I have spent many a night (where I probably should have been sleeping …) on PubMed going from rabbit hole to rabbit hole...

      I am so impressed by what you are doing - I think SATB2 researchers would benefit from your documentation as a resource.

      I'm looking forward to the day that both of our kids are significantly improved … I suspect that will be the day that the folks running PubMed ask their IT department why there are so many fewer hits on their site ;-)

      Have a wonderful day Ling!

      AJ

      Delete
    3. I did like the quote "only the genes encoding adult but not those encoding neonatal cortex SATB2 protein interactors contribute to human cognitive function", which at least in my mind says that there is a great chance for improvements even postnatally. Yay for that!
      It's also interesting that the strongest genetic association found was with "intelligence" and not any of the big brain pathologies (scz, asd, bp, ad...)
      The other take-away here was that there is a Chinese research group working with mice, so maybe an opportunity to reach out?

      Thanks anyway for the nice words, and yes, you are right about PubMed. They should pay us for keeping their visitor statistics look so nice!

      Keeping my fingers super-crossed for your next venture on ketone esters.

      /Ling, wishing you the same.

      Delete
    4. I had been wondering about keto ester /HVMN
      --------------------
      If I understand correctly, I realized that the advantage of keto ester /HVMN is that it could be administered in large quantity, rather than it has other advantages over Ketoforce (KF).
      If 20g * 2 BHB/day is needed for an adult, then maybe 20g BHB/day is sufficient for a child (depending on the body weight).
      KF marks that 3 caps (= 7.5 ml*3, this is the recommended serving ) has 11.5 g BHB, then 20g BHB/day can be approximately achieved by 3 caps KF + 5g BHB of keto ester + > 20ml C8 oil.
      Thus 20g BHB/day is achievable.
      On the other hand, it occurs to me that keto ester /HVMN may not be very cost-effective if the goal is 20g BHB/day for a long duration.

      Delete
  2. Hi Peter,

    Thanks so much for this additional info on Ketones!

    And congratulations on the conversation with Monty! That is great, it was a back and forth conversation, which is something many can only dream of.

    As I had mentioned to you some time ago, we saw the best improvement we have ever seen with BHB + C8, and we have been titrating up slowly, and I think we are still at a super low dose (which I would think bodes well for potential improvement) as the test sticks you had suggested don't even register ketones in her urine.

    I think we're around 2.5 grams of BHB per day, split between 2 doses (1.25mg each) + 1 teaspoon of C8 X2 per day, which I know is very low. My daughter is ~42 pounds. And yet, her speech improved with this so I'm looking to see continued improvement as we titrate up.

    The additional info on BHB Esters is fascinating. I'm considering trialing one at a small dose (e.g. 10ml). The comments from the two taste testers in the relevant videos have me concerned. "Jet Fuel" has never been used positively when describing a flavor. But this does seem to be the best way to increase ketone levels based on the charts shown, and if our very modest level of ketone salts is showing some improvement, it may worth a single purchase of ketone esters to test to see if increased BHB levels do show continued improvement. If so, that will be a big wow for us. I will do some more reading and will let you and the board know if I pursue the ketone esters.

    Have a great day Peter!

    AJ

    ReplyDelete
    Replies
    1. AJ, keep us all posted. The US/Canada is the place to buy these products.

      Delete
    2. Hi Peter, absolutely will do! I ordered the KE4 over the weekend, and we are very excited to see if this makes an impact. As I had noted, a tiny dosage of Ketone salts seemed to make a noticeable improvement, so if there is a linear dose relationship (or any real impact from ketones), we will hopefully see soon after started on ketone esters. I think I will look at using 10ml / day to start, maybe titrated up to 15ml depending on the dipstick readings. Fingers tightly crossed!

      AJ

      Delete
    3. AJ, I am eager to hear your results. I am sure you can mask the taste.

      Delete
  3. Hi Peter, what dose of Clemastine you would suggest for 4 years old. The same for Bumetanide if possible.
    Many thanks , Ella
    How do you split the intake of Bumex and Cl

    ReplyDelete
    Replies
    1. Ella, the important thing to note is that 1 mg of the active clemastine substance is contained in 1.34mg of clemastine hydrogen fumerate. They are not labelled the same way by different producers. Sometimes the tablet is labelled 1mg and the same tablet can also be labelled 1.34mg.

      My 1mg tablets (called Tavegil made by GSK) give a standard allergy dose for 3-6 years of ½ tablet night and morning. I would use a much lower dose than this. For example, 1/8 or ¼ of a tablet just once a day at bed time. This low dose is even safer than the allergy dose, which has been thoroughly tested for safety.

      The current bumetanide study for 200 kids aged 2 to 7 years old has a dose of (0.5mg Twice a Day).

      https://clinicaltrials.gov/ct2/show/NCT03715153

      You do need to add potassium in diet and as a supplement and I would continue for a month before deciding if your child is a bumetanide responder.

      Delete
  4. Peter, many thanks for the thorough explanation .

    ReplyDelete
  5. Two very interesting papers about AHr signalling (and science is finally also backing up that its implicated in autism and asd!)

    Host-microbiome interactions: the aryl hydrocarbon receptor and the central nervous system
    https://link.springer.com/article/10.1007/s00109-016-1486-0

    "The aryl hydrocarbon receptor is an evolutionarily conserved receptor recognizing environmental compounds, including a number of ligands produced directly and indirectly by the microbiome. This review focuses on the microbiome-gut-brain axis in regard to the aryl hydrocarbon receptor signaling pathway and its impact on underlying mechanisms in neurodegeneration."

    "Short chain fatty acids, such as propionic acid and butyrate, from the microbiome are not direct ligands for AHR, but our recent data suggest that they stabilize AHR, increasing its activity in the presence of true ligands (Fig. 2)."

    "In functional experiments, the AHR was shown to alter hippocampal neurogenesis and contextual fear memory in mice [66], as well as aggression behavior in C. elegans [67]. Latchney et al. demonstrated that adult AHR-KO mice and TCDD-exposed mice hippocampal-dependent memory impairment. AHR-deficient mice and TCDD-exposed mice also exhibited reduced cell proliferation, survival, and differentiation in the adult dentate gyrus [66]. The often conflicting data demonstrating both the KO and activation of AHR lead to similar outcomes, suggesting that the AHR plays a vital role in CNS homeostasis."

    "A recent study demonstrated that, in an animal model of ASD, correction of the microbiota with probiotic administration of Bacteroides fragilis corrected biochemical and behavioral abnormalities associated with ASD [70]. In this ASD mouse model, the key effector in the microbiota-gut-brain axis was the metabolome; a number of specific metabolites altered in the ASD mouse model were normalized by the treatment. Indolepyruvate, a microbially controlled molecule that is metabolized into an AHR agonist, was significantly regulated in the ASD model and by B. fragilis treatment [70]. This metabolite is an interesting corollary to indolyl-3-acryloylglycine, which has been shown to be elevated in the urine of humans with ASD [71]."


    The Aryl Hydrocarbon Receptor and the Nervous System
    https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6163841/

    Talks about how AHr antagonism/agonism can modulate NMDA/GABA and AMPA signalling.

    Lets hope this *ahummm* finally sparks some interest and that people and scientists are starting to wake up. Hell it might even explain why keto diets achieve their results.

    ReplyDelete
  6. Hi Peter,

    did you ever look into HRV measuring ( with like a Polar monitor) so you could see changes in the Para and Sympathetic Systems?
    It would be interesting to see the stats and how supplements balance those out.:)
    thanks

    ReplyDelete
    Replies
    1. There are some cool looking gadgets like the Polar monitors, that many fitness people clearly love. 24 hour heart rate monitoring is used as a mainstream diagnostic tool.

      I think some people might just get obsessed with it, for no good reason. It is like measuring your blood pressure every day; if you are 75 years old, had a heart attack and take a shoe box full of pills, it is very prudent; for most people there is no point.

      Delete
    2. its not the Heart Rate I meant- its HRV heart rate variability- 2-3 min measurement which breaks down HF and LF stats- so you can see- ok too much stress, too much relaxation, balance, imbalance..

      Delete
    3. of the Nervous system- excellent measurement especially for products and such- to see response

      Delete
    4. Yes, I know you mean heart rate variability, but I am not sure what you would do with this data.

      Delete
    5. It looks like measuring heart rate variability (HRV) is one element being used to identify/measure autism. The paper below on JAKE uses a whole series of inputs including HRV.

      If you only have one person to treat with autism, you do not need JAKE (yet). If you want to study large populations with autism, find sub-groups and objectively measure the effects of therapies then JAKE makes a lot of sense. If this proves to work then using N=1 JAKE/HRV might avoid some trial and error in treating autism.

      An Observational Study With the Janssen Autism Knowledge Engine (JAKE®) in Individuals With Autism Spectrum Disorder
      https://www.frontiersin.org/articles/10.3389/fnins.2019.00111/full


      Improving Anxiety Assessment in Autism: A Potential Use for Heart Rate Variability and Heart Rate
      https://pdfs.semanticscholar.org/4fc8/32037a479c090996b5ccf653785c09ad285a.pdf

      Sympathetic, Metabolic Adaptations, and Oxidative Stress in Autism Spectrum Disorders: How Far From Physiology?
      https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5874307/

      Delete
  7. https://arxiv.org/ftp/arxiv/papers/1808/1808.08306.pdf

    ReplyDelete
  8. hrv study
    small but still

    ReplyDelete
  9. Maybe someone mentioned this before, but in case not:

    https://www.researchgate.net/publication/310837290_Caffeine_intake_increases_plasma_ketones_An_acute_metabolic_study_in_humans

    /Ling

    ReplyDelete
    Replies
    1. Ling, coffee is a big part of some adult's ketogenic diet. They put MCT oil and even butter in their morning coffee.

      Delete
  10. Hi Peter, I started to give to my daughter ketoforce (ketosport) 6ml (3ml first thing in the morning and 3 ml in the afternoon) and C8 mct oil 10 ml (5ml in the morning 5 ml in the afternoon) a week ago without any effect. My daughter is 7y and has 21kg. Should I increase to 10ml Ketoforce and 20ml C8? How long will take to see an effect? I give a try to keto supplements because she tested low in pyruvic acid.

    ReplyDelete
    Replies
    1. Prada, you can safely increase Ketoforce and C8 if your daughter had no GI side effects so far. The effect in many people is on speech.

      Delete
    2. Thank you Peter for the prompt answer. Today I gave her another form of NAC Designs for Health. I opened a capsule and mixed with her juice and gave her by syringe on empty stomach. She had a few reprises of diarrhea. I gave her 1800mg NAC in two dose. I intend to increase to 2400 mg. Usually she is very constipated so we did have same reaction as Laxaday. Is this a normal reaction? We did not have any success with PharmaNAC because she did not accepted because of the taste.

      Delete
    3. Prada, 6 years ago I was giving NAC by emptying capsules into water. It did not taste good, but it worked and we had no side effects at all. If you have GI problems then try giving with/after food. I think some people mix the powder into apple sauce.

      The NAC in capsules degrades quickly since it reacts with the air inside them. So either the NAC or what it degrades into may irritate your daughter's stomach. When she is older you can give the hard NAC tablets, which are less degraded.

      Delete
  11. Hi Peter. Do you think that I can crush a Jarrow NAC sustain tablet to give her by syringe?

    ReplyDelete
    Replies
    1. Prada, you can try. I think it actually has a membrane inside it as part of the sustained release mechanism. You could put the pills inside a kitchen grinding machine/liquidizer.

      Delete
  12. Peter, I stopped NAC after 3 weeks trial. We did 900 mg, 1800 mg, 2250 and finally 2700 mg without any effect. I tried the brand Design for Health (did not have a smell after 1 month). I got Jarrow Sustain but during the time we started ENDURACELL. I intend to try another trial of NAC after a while.
    We also almost have finished the Ketoforce (12 ml) and MCT oil (15-20ml) trails without any effect (we have only 2-3 days doses left). I will give you feedback on broccoli sprout on the comments of appropriate article.

    ReplyDelete
  13. Hi Peter (or anyone else that has tried KetoneAid KE4) - what dosage and times/day do you recommend for a 10 year-old boy who weighs 34.5 kg?
    Many thanks in advance!
    Molara

    ReplyDelete
  14. Hi Peter (and anyone else who has tried KetoneAid KE4) - please what is your recommended dose for a 10-year-old boy weighing 34.5 kg.
    Many thanks in advance!
    Mo

    ReplyDelete
    Replies
    1. The standard dose is 60ml taken on an empty stomache before breakfast.

      There are several different protocols on their website. Clearly some people benefit from a much lower dose.

      I suggest you start at 5ml, observe the effect, and if necessary increase the dose gradually.

      There are multiple potential modes of action, so there will not be a one size fits all dosage.

      Delete
    2. Got it. Thanks!

      Delete

Post a comment