My thoughts on the 3 hr. dosing sche... 
Tizona
13 y
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this is my long-winded take on the three hour dosing schedule that Andy Cutler recommends
after extensive research into ALA and mercury chelation, I've come to conclude that ALA most definitely is a mercury chelator and helps to heal the body of the effects of mercury
However!
I'm seriously questioning the concept that unless one sticks to the every three hour chelation dosing schedule, that you are at risk of making yourself (in the words of Andy) "permanently and irreversibly worse"
every single study that I've looked at that uses ALA to treat mercury toxic rats and/or mice concludes that the ALA significantly reduce the effects of mercury on the rats. Not one single study showed that the rats became "permanently worse" because the ALA was not given on a three hour dosing cycle
in fact several of those studies had the rats receiving just one large intravenous dosage of ALA per day. This is anathema according to Andy, and theoretically should have resulted in Mercury redistribution and saw the rats get permanently worse. But they didn't. In fact they got better by quite a bit
please note these are the EXACT SAME studies that Andy used to originate his chelation theory in the first place.
Furthermore, the half-life of ALA in the body is about 30 minutes. So let's say you take 100 mg of ALA. After 30 minutes only 50 mg is left in your body, after one hour 25 mg, after two hours only 6 mg is left, after three hours just 1.5 mg is still active in your body.
Now, according to Andy the reason you need to take it every three hours is to prevent mercury redistribution. But at the end of three hours about 98% of the ALA is already gone. By following his logic that means 98% of the mercury redistributes after three hours.
is he claiming that that 2% of ALA that remains after three hours somehow prevents all of that mercury that has been chelated from redistributing? I find that to be preposterous
If ALA is a strong chelator of mercury, and if it forms an irreversible bond with the mercury ion (as Andy claims and as the Science seems to suggest), then once it gloms on to the mercury atom it should hold onto that atom until it is escorted out of the body, regardless of if more ALA is introduced into your body or not
don't get me wrong, low dose frequent chelation is almost certainly the most effective and most efficient means of chelation therapy. on this point I do agree with Andy
However, I can find no evidence whatsoever that if you don't stick to a three hour dosing schedule you'll make yourself "permanently and irreversibly worse". I just don't see it. It's not logical, nor does the scientific evidence support this conclusion
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- Re: My thoughts on the 3 hr. dosing ... maiaeutic
13 y
4,331
This is a reply to # 1,848,027What I still don't understand from a theoretical point of view regarding the Cutler protocol, is why you can't just take chlorella (or pehaps, some combination of cilantro, chlorella, and garlic, as each has the ability to vaccum up mercury that may be circulating in the body) and just toss the whole three hour dosing schedule, and dose whenever its convenient.
I'm NOT telling anyone to go do this, I'm not an expert or a clinician, etc. etc....But my own experience supports this, a least to a certain degree.
About a couple of weeks after I began taking phosphlipid exchange (whose primary constituents are EDTA and ALA), I ran out of chlorella, and without even thinking about it continued to take the phospholipid exchange for a couple of days while I waited for more chlorella to come in the mail. Well, at the end of the second day I started to feel like hell and really have a sense of the horror stories people relate about redistribution. So I went and got some more chlorella, and within hours of taking a large dose I was fine again, no problem.
The other thing I've never quite grasped about the Cutler protocol, is since redistribution can happen at any point upon cessation of the ALA, then why the hell can't it happen at the end of the 3-day dosing cycle?
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- Re: My thoughts on the 3 hr. dosing ... Michael B
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This is a reply to # 1,848,075It DOES happen at the end of the 3 day closing cycle. That is exactly what makes so many people report feeling miserable in between rounds but great while on them. That is also why Dr. Cutler recommends taking DMSA or oral DMPS along with the ALA, because they have a stronger bond to mercury and can "mop up" what ALA leaves behind. It is also why some people recommend taking the DMSA or DMPS for a day or more after ceasing the ALA.- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
4,208
This is a reply to # 1,848,096but nothing you wrote there has anything to do with feeling better while taking chlorella, and feeling worse not taking it
- Re: My thoughts on the 3 hr. dosing ... Michael B
13 y
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This is a reply to # 1,848,107Are you kidding me? Wow tizona. The Chlorella story is actually testifying AGAINST your post's reasoning...he took large dose infrequent ALA and experienced redistribution as soon as stopping another known chelator which he had already been taking prior. It's obvious that if you are taking more than one chelator and stop one of them, mercury is going to be redistributed, and so of course taking the chlorella once again restablised the redistributed mercury.
It does not prove that the chlorella was a 1 time fix, as you so seem to suggest with your response....
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- Re: My thoughts on the 3 hr. dosing ... Michael B
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- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
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- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
4,478
This is a reply to # 1,848,075it's clear to me there's a lot we don't know about chelation
chlorella is the perfect example. It seems SOME people react very poorly to using it as a chelator, and yet SOME people react to it quite well such as yourself
Why?
I don't know! And furthermore, I'm not sure anybody else knows either. It's possible that different people detox from mercury differently. There may be different liver heavy metal detox pathways that are open in some people and closed in other people. any depending on which pathways is open and/or closed in any one individual will determine how that person reacts to chlorella
But that's just a theory.
- Re: My thoughts on the 3 hr. dosing ... Michael B
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- Re: My thoughts on the 3 hr. dosing ... Michael B
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This is a reply to # 1,848,027The bond of ALA is not as strong as DMSA or DMPS. I've read posts from users on this site saying they used supplements in the past containing large dose ALA and got redistribution syndromes without knowing what was going on or what caused it.
If the study with the rats was from acute mercury poisoning it cannot apply to a long term exposure such as Amalgam poisoning because the mercury did not have enough time to lodge itself in the body as well as cross the blood/brain barrier then convert into inorganic mercury. Inorganic mercury cannot pass the blood brain barrier. In such an occurence as with the rat experiment, of course a single dose of ALA can prove to chelate mercury effectively; it is essential still floating around in their systems.
The brain is constantly letting organic mercury in through the blood/brain barrier and then back out the barrier at a certain rate. If sufficient mercury in either inorganic or organic form is present in the body, mercury is no longer released from the brain at the same rate. What ALA essentially does in the context of a chelation protocol is hold the blood brain barrier open and allow the brain to detox mercury. However, the body MUST have a lower concentration of mercury in it for this natural chelation to work. This is where dmsa and dmps come into play.
The danger is when methylmercury readily enters the brain but does not leave it due to higher concentrations in the body, where it then converts to inorganic mercury and cannot pass the blood brain barrier.
Once again, what ALA really serves in this purpose is holding the blood brain barrier open long enough for the brains natural chelation mechanisms to escort the inorganic mercury through the barrier. It does have the ability to bond to mercury, but given the duration of time it takes for the brain to rid itself of inorganic mercury poisoning (3 years or so) it is evident that ALA is not a magical brain chelator that simply goes in, picks up some mercury, and leaves. It is evident rather that the brain chelates, at its own rate, what it could not due to the inorganic mercury being unable to leave the brain without the help of ALA.
Thanks for sharing, though :)- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
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This is a reply to # 1,848,089you claim that because somebody took the extra large dose of ALA and then felt bad afterwards, that proves that redistribution happened
It doesn't prove anything of the sort. It just proves they had a bad reaction to a large dose of ALA. Like I said LOW DOSE frequent chelation is almost always the best approach. Taking large doses of any chelator is likely to whack out any mercury toxic person. But that has nothing to do with redistribution, it has to do with the fact that your body simply isn't able to handle that amount of mercury being dislodged and move through its system
As for the rest of your post, it's almost entirely off topic to what I posted
You're discussing the specific actions of ALA versus DMSA etc.
Okay fine, if you think ALA is a weaker chelator than DMSA, they just substitute DMSA in my post everywhere you see ALA. The logic regarding the three hour dosing schedule still holds up.- Re: My thoughts on the 3 hr. dosing ... Michael B
13 y
4,153
This is a reply to # 1,848,106"But that has nothing to do with redistribution, it has to do with the fact that your body simply isn't able to handle that amount of mercury being dislodged and move through its system"
And just what do you think the reason is why "your body simply isn't able to handle that amount of mercury being dislodged and move through its system"? do you think the cells look at the mercury and get scared? Do you think a mercury atom can affect a cell psychologically? It's common sense: If a mercury atom is not bound by a chelator, it's redistributing in your body.
READ: If you are experiencing negative side effects from a chelation protocol, it means you are experiencing REDISTRIBUTION. This is not a parasite clean with herxheimer reactions. This is heavy metal being lodged back into your cells.
It's not that my replies have no relevance to your post. It's that your post really had nothing relevant to proper chelation, and you stated a ton of erroneous and dangerous information in the process that needed addressing.- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
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This is a reply to # 1,848,541are you saying that if you stick to the three hour dosing schedule, and you use DMSA/DMPS, that redistribution will NOT occur?
If that's the case people could simply take 300 mg of DMSA every three hours right out the gate and have absolutely no problems
But of course we know that doesn't happen. Even when people stick to the three hour dosing schedule 300 mg of DMSA is way way too much for just about everybody. So is 200 mg. in fact, 100 mg every three hours is still too much for most people. Most have to start out at 50 mg, 25, 12 or even 5 mg.
besides, your logic is this - if a single large dose of any chelator (whether it be ALA/DMSA/DMPS) results in negative reactions, that proves redistribution happened.
Therefore, using your logic, a single small dose of any chelator that DOESN'T result in negative reactions proves that redistribution DIDN'T happen
Also, nobody can explain why none of the rats got "permanently worse" despite getting large doses of ALA once daily. in fact they only got better- Re: My thoughts on the 3 hr. dosing ... Michael B
13 y
4,108
This is a reply to # 1,848,587Don't get excited and start fighting against reasoning that isn't even mine, which you are projecting onto me.
You don't understand many variables and are advocating dangerous advice, then later saying the best approach is to do exactly what you are reasoning against to begin with.
Large doses of DMSA or DMPS can mobilize more mercury into the blood than it can bind.
There are many cases of people taking frequent, large doses who are fine while on the protocol. In fact they feel great. Then, as soon as stopping, they get serious redistribution problems. Who is to say some of the damage they are causing is not permanent?
The goal is always to avoid redistribution. READ AGAIN: if you are experiencing negative reactions from chelation, REDISTRIBUTION is occurring.
Sure, redistribution is bound to happen, but it certainly can be minimized. But NOT by what you are preaching.
You really don't seem to be proving anything with your posts. You say one thing then support the contrary. Please get your reasoning straightened out before someone reads your posts and damages themselves, permanently.
But of course I am not without compassion for you. You are not the first person with mercury in their brain to post on this forum.- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
4,146
This is a reply to # 1,849,764give me a break
Just because somebody disagrees with you they have "mercury on their brain"? and then of course you have compassion on me? Good grief
these kind of petty passive aggressive condescending insults don't fly with me. learn to address the issue at hand without being petty and personal and insulting. Thank you
now I'll address some of your points.
You said "READ AGAIN: if you are experiencing negative reactions from chelation, REDISTRIBUTION is occurring."
really? You do realize that some people have really terrible reactions to 100 mg of any chelator even taken on a three-hour dosing schedule, right? Some have negative reactions to 50 mg, some even have negative reactions to 10 mg! Are you saying redistribution happens with 10 mg of any chelator taken in the proper three-hour dosing schedule?
and you seem to be missing my main point which I made multiple times.
Frequent low-dose chelation (i.e. every three hours) is most likely the most effective and efficient method of chelation.
The only thing I am arguing against is the idea that if you don't stick to that schedule you'll make yourself PERMANENTLY WORSE. something that Andy loves to say over and over again. I don't buy it. And there's no logic and there's no scientific study that backs him up on this
Can you point to one single chelation study which shows any human being, any rat, any mouse got permanently worse because they didn't stick to a three hour dosing schedule?
I have searched high and low and I can find no such study. If you have one I would love to read it
I did however find plenty of studies which show that both people and animals get PERMANENTLY better despite not sticking to any kind of a three hour dosing schedule
- Re: My thoughts on the 3 hr. dosing ... Michael B
13 y
4,000
This is a reply to # 1,849,769Being petty, and personal, and insulting is exactly what you have been coming across as. And yes, I mirrored your behavior intentionally. If you had behaved rationally, respectfully, and kindly you most likely would have been treated the same by me.
"really? You do realize that some people have really terrible reactions to 100 mg of any chelator even taken on a three-hour dosing schedule, right? Some have negative reactions to 50 mg, some even have negative reactions to 10 mg! Are you saying redistribution happens with 10 mg of any chelator taken in the proper three-hour dosing schedule?"
Once again, you are arguing against a point I didn't even try to make. Nevertheless, your statement needs correction. If the mobilised mercury and other heavy metals are not able to exit the body during the chelation round, then obviously redistribution is going to happen, even with 10mg doses. It can and does happen. And obviously it is much MUCH more severe if a large dose is taken, and even more severe if done infrequently. People can and absolutely do make themselves worse. Some permanently. What is so hard to understand?
If you had a different experience with chelation, say, severe redistribution, you would probably be writing posts quite opposite to what you have been suggesting. You may even have started a website just like:
Dmpsbackfire.com
You thought you had a brilliant, unique thought contrary to "the masses" here on curezone; that infrequent dosing is effective and safe. Sorry, what you are saying is exactly what the masses have blindly been preaching and following, while poisoning people in the thousands. It is the reason Cutler suggested his protocol to begin with.
And contrary to your attitude that anyone who agrees with Cutler is "worshipping" him as "god", it is your own subconscious level of thinking you are projecting outward. Andy Cutler is simply a sound thinker with reasoning behind his statements. Do you believe you are somehow onto something revolutionary with what you are suggesting?
The entire purpose behind advocating frequent low dosage is for safety, not efficiency. It is not *efficient* to have to wake up in the middle of the night, and it is not efficient taking such a small dosage. But it is safe.
- Re: My thoughts on the 3 hr. dosing ... Michael B
13 y
4,000
- Edited #121206
13 y
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This is a reply to # 1,849,764NOTE - I'm going to post this message again, I tried to post it once and it didn't seem to show up. hopefully it works this time
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give me a break
Just because somebody disagrees with you they have "mercury on their brain"? and then of course you have compassion on me? Good grief
these kind of petty passive aggressive condescending insults don't fly with me. learn to address the issue at hand without being petty and personal and insulting. Thank you
now I'll address some of your points.
You said "READ AGAIN: if you are experiencing negative reactions from chelation, REDISTRIBUTION is occurring."
really? You do realize that some people have really terrible reactions to 100 mg of any chelator even taken on a three-hour dosing schedule, right? Some have negative reactions to 50 mg, some even have negative reactions to 10 mg! Are you saying redistribution happens with 10 mg of any chelator taken in the proper three-hour dosing schedule?
and you seem to be missing my main point which I made multiple times.
Frequent low-dose chelation (i.e. every three hours) is most likely the most effective and efficient method of chelation.
The only thing I am arguing against is the idea that if you don't stick to that schedule you'll make yourself PERMANENTLY WORSE. something that Andy loves to say over and over again. I don't buy it. And there's no logic and there's no scientific study that backs him up on this
Can you point to one single chelation study which shows any human being, any rat, any mouse got permanently worse because they didn't stick to a three hour dosing schedule?
I have searched high and low and I can find no such study. If you have one I would love to read it
I did however find one study which clearly shows that a real live human being with mercury poisoning got permanently BETTER on a six hour chelation dosing schedule. I linked that study. Anybody can read it. - You are being completely rude to Tiz... North
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- Re: My thoughts on the 3 hr. dosing ... Tizona
13 y
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- Re: My thoughts on the 3 hr. dosing ... Michael B
13 y
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- This study proves my point! (edit) Tizona
13 y
4,414
This is a reply to # 1,848,541this poor two-year-old girl was suffering extreme symptoms of mercury poisoning. After one month of DMSA treatment all of her systems resolved
There is no mention of an every three hour dosing protocol. And I sincerely doubt her parents were getting up in the middle of the night and giving her DMSA every three hours.
According to Andy, she should've got "permanently worse". But of course she didn't. in fact, she got permanently better.
Again, if you want to tell me that dosing every three hours is the most efficient method of chelating, then I just might agree with you
But if you want to tell me that if you don't follow the every three hours schedule you will get "permanently worse", I just don't see any evidence for that
please somebody show me one single study where humans, rats, or mice, got permanently worse because they didn't stick to a three hour dosing schedule of DMSA and/or DMPS and/or ALA
EDIT- I found the complete study. The child was injected every six hours with DMSA. According to Andy that should have resulted in redistribution and worsening of symptoms. But it didn't
http://medind.nic.in/icb/t10/i10/icbt10i10p1153.pdf
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Abstract
A 2-year-old girl presented with hypertension, anorexia and vomiting, restlessness, insomnia and acrodynia. Her blood pressure upon arrival was 145/98 mmHg. Ultrasound of the abdomen, CT scan of chest, abdomen and pelvis, and echocardiogram, were normal. Urinary levels of catecholamines were elevated, urine level of mercury was found to be high (33.2 μg/g creatinine), although blood level was normal (>0.5 μg/dl, reference value 0–4 μg/dl). Following a 1-month course of oral treatment with dimercaptosuccinic acid (DMSA) the child’s symptoms and signs resolved, and urinary mercury and catecholamines levels normalized. Mercury intoxication should be suspected in a patient with severe hypertension, personality changes and acrodynia. Normal blood levels of mercury do not exclude this diagnosis, and catecholamine levels may serve as a surrogate marker for confirmation of the diagnosis and to evaluate response to treatment.- Re: This study proves my point! powertool4
13 y
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This is a reply to # 1,848,596Andy Cutler is a perfectly sane but delusional character. Some of his claims are downright ridiculous..
- Re: This study proves my point! Tizona
13 y
4,241
This is a reply to # 1,848,597agree. He deserves tons of credit for bringing the mercury issue to the forefront. Also, he is one of the few people out there championing ALA as a mercury chelator, which the literature most definitely supports. I think he's the original person to popularize ALA as a Mercury treatment
But there are some things he claims that have no real scientific basis. Of course you can't discuss the matter with him or anybody on his forum because you will be instantly banned for the grand crime of actually challenging one of his assumptions- Re: This study proves my point! powertool4
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- My thoughts #68716
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This is a reply to # 1,848,640Actually I feel better on 3 hours dosing with ALA. If I wait even 20 minutes I feel effects of mercury.
I tried for 2 months to chelate with 4 hours dosing but it was awful - very low concentration due to broken methylation, blurry vision appears, week body, pains everywhere...
When I switched to 3 hours and everything went back to normal.
After 10 months doing 3h chelation and 2 months on 4h, I'm great with less mercury in the system and not permanently injured. But these 2 months were very hard for me just because I thought that i can cope with 4h dosing.
Although I did not read the whole studies I think in those studies that the rats receive just one large intravenous dosage of ALA per day are performed only to prove effectiveness for its ability to remove mercury. They prove it and stop the study. Nothing more...
Do you think about the possibility that some people have the ability to produce more glutathione(or other natural mercury binders) than others. In this situation stopping ALA will not redistribute mercury because glutathion will grab it and prevent redistribution. And taking ALA after 5 or 6 hours won't be a problem for them.
It's easy on theory but the reality is that mercury inhibits a lot of reactions in the body and most people are low in GSH.
Other possibility can be if some people transport so fast the ALA-mercury bond to liver and/or excrete some via kidneys and thereby avoid redistribution.
It's crezy but we don't know lot of things as you say.
Regards
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- My thoughts #68716
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- Re: This study proves my point! powertool4
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- Re: This study proves my point! Tizona
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- Re: This study proves my point! powertool4
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- Re: My thoughts on the 3 hr. dosing ... Tizona
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- Re: My thoughts on the 3 hr. dosing ... Michael B
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- Re: My thoughts on the 3 hr. dosing ... Tizona
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- Re: My thoughts on the 3 hr. dosing ... maiaeutic
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