Borax-boron how to detox and heal yourself inexpensively / Arthritis

Johnno

The Living Force
I heard this interview on Australian ABC radio last week. It's an alternative treatment known as minocycline thath is usually used for acne treatment which is proving sometimes effective for rheumatoid arthritis. I was under the impression rheumatoid arthritis was genetic or a result of "over-use" of the joint but found out it was an immunity disorder.

My left hand fingers have been starting to ache a bit and I've been using glucosamine which seems to also be effective.

In any case, here a transcript of the interview on the ABC

http://www.abc.net.au/rn/healthreport/stories/2008/2260412.htm#



Health controversies often start with impressions, anecdotes, push back and then some clarity one way or the other eventually. So when the smoke clears, arguments like mumps vaccine causing autism prove to have no foundation and the A1/A2 milk story while sounding off beat may indeed have something going for it. So let's stay in the smoke and move from one auto immune disease, type 1 diabetes, to another, rheumatoid arthritis which is a destructive arthritis that can cripple people and be hard to treat. The newer medications for rheumatoid can cost tens of thousands of dollars a year.

There seems however to be growing enthusiasm outside orthodox specialist rheumatology practice for an inexpensive antibiotic which some people with rheumatoid arthritis swear by. And as you'll hear there are suggestions it may work in osteoarthritis as well.

One strong proponent is a former colleague of mine from the ABC who has rheumatoid arthritis, he's Peter Wall.

Peter Wall: I was playing golf and I actually had a pain in my jaw and I thought what is this and on the way there for the first time ever I've pulled over and fell asleep twice. I didn't know it had anything to do with it until later on that inflammation made you tired.

Norman Swan: Were you getting pains in other joints as well?

Peter Wall: Yeah, then they came in a whole lot of joints, I remember the ankle, the wrist, the fingers. With this rheumatoid arthritis I was diagnosed as having you actually get this sort of brain fog which is a dreadful thing, it's almost like have vaseline on the lens the whole time. It's a dreadful way to live and so I then progressed to the stage where I couldn't get up and go to the toilet without crutches, I was really in a bad way, I couldn't turn the tap on properly, I had to hold my right wrist with my left hand to shave.

Norman Swan: And this was because of pain in your joints?

Peter Wall: Because of pain, straight pain.

Norman Swan: What medications did they have you on?

Peter Wall: Well I did the normal run of things, I had Gold shots, I had a thing called Arava, I didn't do the Methotrexate route because -

Norman Swan: To explain to listeners Methotrexate is a cancer drug but it also affects the immune system and is quite effective in rheumatoid arthritis for some people and other auto immune diseases.

Peter Wall: But Arava I believe has given me what you guys call peripheral neuropathy in my feet.

Norman Swan: So you've got numbness and tingling in your feet?

Peter Wall: I have numbness from the middle of my foot to my toes, probably about 50% of the feeling that I used to have. I then had Gold shots and it made my skin go like shark's skin and it gave me ulcers in the mouth and on the lips. It was dreadful.

Norman Swan: So you were having a lot of fun?

Peter Wall: I wasn't having a lot of fun at all, I was managing a radio station and I used to have to go to the car at lunchtime and sleep every lunchtime without telling people where I was going because I needed the actual sleep to get through the day. Every Saturday I'd sleep for three or four hours and then it was at that radio station I was talking to one of the board members and I apologised for not being very focused on the job and he said to me you should speak to my wife. And I said why's that? And he said because she's discovered something in America and she has rheumatoid arthritis and it's worked well for her. So I said OK, you'll do anything, you'll stand on one leg and whistle Dixie if you've got to. So I rang her and she said that she took this thing called Minomycine which is a drug basically that children take for acne in Australia. And I said how does that work? And she said you must read this book and the book was called The New Arthritis Breakthrough by a guy called Henry Scammell and she said you must look up a website which is called The Road Back and I discovered this group of people and yes, some of them are whackers and dare I say, this is the saddest thing to say Norman, that most of the wackiest ones are the Australians on there. But the theory is, and you'll need to ask somebody who knows a lot more about it than me, that tetracycline somehow gets into enzymes in micro plasma which is a cell that knows no boundaries or something, I don't know, and that it actually works on those and it gets in prior to the auto immune problem kicking in.

Anyhow I took it and after about five days the brain fog started lifting and after about ten days the brain fog had gone and then when you do this there's a thing called the Herxheimer effect which some people know of, but I'd never heard of it.

Norman Swan: This traditionally occurs with penicillin which is a reaction to taking an antibiotic.

Peter Wall: Yeah and in layman's language it means that you feel really dreadful before you get better and so I'm reading this book and it says if you have this reaction it's the best sign you've got that the tetracycline, which is what Minomycine is, is reaching its target. Literally I was in bed for a week, knocked around, I could hardly get out. That's the problem with this treatment. The joints that have been hurting really hurt and then they stopped hurting. Other joints that hadn't hurt hitherto were starting to hurt but the brain fog had gone so I was thinking clearly.

Norman Swan: So it's a very mixed picture, the joints that were sore were getting better but other joints were starting to flare up.

Peter Wall: And then went away so they didn't actually get as bad as the ones that had been really painful were.

Norman Swan: How many weeks into treatment are we now?

Peter Wall: I think after about six or seven weeks I was tiggety boo.

Norman Swan: So you really had to dig in and stick with it?

Peter Wall: Absolutely, and I think that this is probably not something that most rheumatologists want to go through with most patients, I think it's a hard road.

Norman Swan: Obviously this is not a normal sort of Health Report story where we're dealing with a randomised controlled trial with control populations and all that sort of thing, we're talking about Peter Wall and his experience. But has your rheumatoid come back on the minocycline?

Peter Wall: I've been on it now for about three years and on about four or five occasions I've had pain in a joint in three years that's probably about one tenth of what it used to be and it's always lasted a day or two. Every time I've tried to change the dosage, for the first year I had monthly blood tests, when I went on this they all went to normal.

Norman Swan: So when you try to change your dose does the disease come back?

Peter Wall: I've done it twice and it does seem to come back.

Norman Swan: And have you had to increase your dose at all because it was wearing off?

Peter Wall: No, the only side effect is that I'm as brown as a berry because tetracycline does make you go brown so you've got to really watch that.

Norman Swan: So has your rheumatologist's scepticism diminished?

Peter Wall: They all think I'm basically lucky. I said to my wife I'm going to talk to Norman Swan about this thing, you know a lot of people don't believe in this and she said well I've seen how bad you were and I've seen how you are now, you should go and tell people.

Norman Swan: Peter Wall. We'll go to a rheumatologist in a moment but before that to a general practitioner who uses minocycline a lot in people with rheumatoid arthritis.

As I said to Peter a moment ago, this isn't a regular Health Report story where we try to stick to the evidence from placebo controlled randomised trials. This is to a large extent anecdotal but the stories do impress. Richard Schloeffel is a GP who's a tetracycline enthusiast for rheumatoid arthritis and subscribes to the theory that an infection lies at the heart of this autoimmune disease. And in fact this isn't a million miles away from mainstream immunological opinion about what triggers autoimmunity.

Richard Schloeffel: We believe that rheumatoid arthritis is activated by an infection called mycoplasma but I started initially with a drug called Doxycycline which is another sort of tetracycline antibiotic and we know these drugs are relatively safe and very inexpensive.

Norman Swan: Not a good idea for children though?

Richard Schloeffel: Under the age of 8 you shouldn't use it because it can damage your teeth and minocycline you shouldn't use either for younger children but over 100 patients now or more that I've treated with minocycline for rheumatoid arthritis stabilising their inflammation, reducing their blood tests down to normal and as Peter was saying there's a marked reduction in pain and stiffness.

Norman Swan: So tell me what happens, because Peter has described his course there where it seems to get worse for a while before it gets better?

Richard Schloeffel: Yes, there's a type of reaction that people get when you start antibiotics, it happens with lots of infection called a Herxheimer reaction. If you start killing organisms with an antibiotic that releases a lot of toxins from those particular organisms but when you're treating a long term infection such as rheumatoid arthritis and I know I'm stretching the boundaries there, you get worse because you release a lot of -

Norman Swan: It's classic with penicillin rather than tetracycline.

Richard Schloeffel: Yes it is, the second or third week into treatment with minocycline up to about six weeks they get worse, more pain, more swelling, more stiffness, ESR C-reactive protein measures of inflammation go up and then gradually it improves and over a three to six month period you'll notice a gradual reduction of symptoms.

Norman Swan: What proportion of people that you treat actually get a response because no drug works on 100% of people?

Richard Schloeffel: Well some of the studies that have been done in the States looks around 60%65% of people will benefit from antibiotics, particularly minocycline and I think I'm getting around about the same numbers. Most patients see me twice a year for scripts for minocycline which is working out a few dollars a week as compared to some of the newer treatments the TNF drugs, anti TNF drugs Enbrel and whatever.

Norman Swan: They are the new monoclonal antibody drugs that can cost $60,000 per year.

Richard Schloeffel: That's right. I still have patients on them, in patients who have failed but I'm seeing patients who have failed the traditional treatments, Methotrexate, Prednisone, other anti-inflammatory drugs and then putting them on minocycline and as Peter says they start to look like they are going into remission, then their blood tests normalise, their movement improves but if you stop the medication they start to get it back.

Norman Swan: There haven't really been randomised controlled trials which is the gold standard evidence here to show that this works. When you talk to specialists, when you talk to rheumatologists what do they say?

Richard Schloeffel: Several of them are actually starting their patients on minocycline, especially the milder patients or the patients with what we call sero-negative rheumatoid arthritis where they don't have any blood tests positive, we know they're sick and often if they've got evidence that they've had mycoplasma they may well give this a trial to start with but they don't talk about it and they wouldn't offer it unless the patient asks for it.

Norman Swan: Because to be fair it is off label, it's not -

Richard Schloeffel: Oh absolutely and I think part of the reason is that there is not much money in prescribing or studying minocycline for the use of rheumatoid arthritis. I think the side effects are twofold - problems of photo sensitivity and with minocycline you can get hyper-pigmentation of the skin, you may get gut disturbance and you have to watch for this.

Norman Swan: Richard Schloeffel. One of Australia's most respected rheumatologists and someone who's been on the Health Report several times in the past is Associate Professor Lyn March who's based at Royal North Shore Hospital in Sydney.

Lyn March: Rheumatoid arthritis is a chronic inflammatory condition of the joints that ultimately if not treated leads to destruction of the joints. It is an auto immune disease in that the body's immune system is being over-active and essentially attacking its own joints. We don't know what causes it but clearly there are strong genetic elements and environmental triggers that add to that.

Norman Swan: Which is where this tetracycline treatment comes in presumably if indeed it works because some people have suggested that an infection can be the trigger because it can mimic the lining of the joints and the immune system gets confused.

Lyn March: Yes the international community has been searching for years for the infective agent that starts rheumatoid arthritis and clearly that hasn't been found yet. Something has triggered the immune system but it just keeps going but very close looks have not been able to find infective agents in the majority of rheumatoid arthritis patients.

Norman Swan: So what do you think of this tetracycline story?

Lyn March: It's not a new story.The trials done some years ago would suggest in rheumatoid arthritis, compared to a placebo treatment the tetracycline antibiotics particularly minocycline can reduce joint pain and joint swelling and also induce the inflammation levels that we can measure in the blood. What these studies haven't been able to show us though is whether that actually switches off the erosive damage and actually prevents progression of the disease. So there seems to be evidence that it does modify symptoms and some of the signs of inflammation but we don't know and maybe it's just because we haven't studied enough people over a long enough time period to see if it classifies as one of those disease modifying agents.

Norman Swan: And what do you think of this flare that people describe a week or so after starting it, in other words you get worse before you get better?

Lyn March: Yes I'm not sure exactly what's going on there because I mean the tetracycline seems to do an enormous number of things at a different cellular level in the body as well as the anti-bacterial effect.

Norman Swan: It seems to have an effect on tissue glue because some people are using it for aortic aneurisms to stop them growing because it has an effect on the way tissues hold together.

Lyn March: Yes it's to do with the collagen as you know which is one of the main components of all tissues in our body and the tetracyclines probably block a particular group of enzymes called the matrix metalloproteinases and what's happening in things like aortic aneurisms but also what's happening in the joints in rheumatoid arthritis and in osteoarthritis, the cartilage has been broken down by a lot of inflammatory markers and the tetracyclines can block some of that collagen breakdown and perhaps protect the joint.

Norman Swan: Do you have many patients on it?

Lyn March: No I don't because as I said it's not mainstream, it's not at this stage recommended and not actually listed for that use. With rheumatoid we really should be aiming to get the patients into remission and that is achievable now with the drugs that we have available so we can actually switch off the erosions and I guess clearly there are potentials for harms and benefits in every drug and there certainly are potential harms for the tetracycline usage long term as well. And you want your benefits to far outweigh those harms so I'm not convinced with the evidence that that's where we are with the tetracyclines.

Norman Swan: And what are the downsides?

Lyn March: Because it's affecting the immune system, it can actually tip it over the other way sometimes and there are numerous case reports of the tetracycline derivatives, particularly minocycline, actually causing some autoimmune diseases so it can induce the anti-nuclear antibodies that we see in systemic lupus erythematosus and cause evasculitis, it can cause acute renal failure or liver failure.

Norman Swan: You mentioned osteoarthritis in passing is there any evidence for these tetracyclines in osteo?

Lyn March: It might well be Norman that it may be more useful in osteoarthritis because one of the key pathology that's occurring in osteoarthritis is in the articular cartilage and in the underlying bone and by inhibiting those metalloproteinases and reducing collagen destruction it might actually protect the cartilage and there has been quite a reasonably done randomised trial that showed that the joint space narrowing that we see on X-ray was reduced in the people taking the minocycline but interestingly pain wasn't particularly influenced. So it's clearly not straightforward.

Norman Swan: Associate Professor Lyn March who is based at Royal North Shore Hospital in Sydney. I'm Norman Swan and you've been listening to the Health Report.
 
Hi Johnno, it might be worth really examining your diet as well - especially since you eat vegemite, which is a glutamate (as in msg - an 'excitotoxin' - and have you eliminated gluten? ) - I've recently learned that most of my considerable joint pain was due to my diet - (in my case a lifelong dairy allergy - and I ate dairy at every meal) - so I can't stress enough the fact that what we consume very often turns our body against itself - which is rather the definition of autoimmune disorder - especially when we're no longer in our twenties.

So - perhaps before taking a pharmaceutical - the first step should be a brutal investigation of everything that is consumed. fwiw,
 
I rarely have Vegemite anymore after your last bit of advice which was about vitamin B I think.

And yes, it's now time to get off of the gluten. How did you find out about your milk allergy?
 
Johnno said:
I rarely have Vegemite anymore after your last bit of advice which was about vitamin B I think.
:lol: :lol: Sorry for badgering... heheheh.

Johnno said:
And yes, it's now time to get off of the gluten. How did you find out about your milk allergy?
Well, a good friend of mine kept recommending her kinesiologist - so I finally 'tried it' (quite frankly, I was thinking that he was likely a 'voodoo' doctor and wouldn't do much good - yep, that's me being so 'opened minded'.)

Turns out, he nailed it, plus a few other things and after following his directions for a month or so - I feel ten years younger - there is no comparison. So no matter my continuing suspicions about his subjectivity ( ;) ) - there is no arguing with success. It was really interesting to observe myself while removing all dairy though - cheese was one of my staples, so, boy, oh boy did 'i' push back.

There is more to work on though, with my diet - but a step at a time.
 
anart said:
Hi Johnno, it might be worth really examining your diet as well - especially since you eat vegemite, which is a glutamate (as in msg - an 'excitotoxin' - and have you eliminated gluten? ) - I've recently learned that most of my considerable joint pain was due to my diet - (in my case a lifelong dairy allergy - and I ate dairy at every meal) - so I can't stress enough the fact that what we consume very often turns our body against itself - which is rather the definition of autoimmune disorder - especially when we're no longer in our twenties.

So - perhaps before taking a pharmaceutical - the first step should be a brutal investigation of everything that is consumed. fwiw,
Hi Anart,

I've been reading a bit about digestive enzymes lately. One thing I recall reading was that a dairy allergy could actually be caused by a deficiency in the digestive enzymes amylase, lipase, and protease. So you may want to give pancreatic enzymes, or food enzymes a try. FWIW.

Here is some general information.
http://www.netnutritionist.com/qa.htm
 
Hi Johnno, FWIW here is my recent experience with a naturopath/kinesiologist.

Around last November, I started experiencing what seemed like asthma. Well it got so bad that I had no choice but to see a conventional doctor not only to get some medicine but mainly to get an M.C. since the company that I work for will only recognise a medical certificate from conventional doctors. Now this particular doctor after having described my symptoms to him, concluded that I had asthma although up to that point in time, I've never suffered from asthma ever. He prescribed Ventolin inhaler and Flixotide (steroid) inhaler. The Ventolin was to help me breathe easier but the Flixotide was to suppress the asthma! I didn't like the idea of suppressing symptoms since to me it was the body's way of telling me something was wrong and I had to figure a way to heal it rather than suppress it. So I started using the Ventolin whenever I needed it but initially avoided the Flixotide.

After awhile, the symptoms got really bad. Just standing up would cause me to start panting, gasping for air. So just to get some relieve I started using the Flixotide and sure enough, all the symptoms disappeared and I was almost back to normal but somehow I was not very comfortable using the steroid inhaler knowing full well that all it was doing was suppressing symptoms and not actually curing anything. So, I stopped using the steroid inhaler and within a day or so the asthma like attacks would return and I was basically backed to where I started. So it went on. On many occasions I had to go overseas and each time that I left this country, I was completely back to normal without any medication. And when I revisited the doctor again after about 2 months or so, he concluded that perhaps it was something in the air that was causing me to have all this breathing problems and apparently a very common problem for people arriving from overseas to live here.

Well after another few months or so with the problem not going away, I finally decided to try some alternative remedies. It was a toss up between doing Reiki or going to a naturopath. I eventually settled on visiting the naturopath first and if that didn't solve my breathing problems, I would give Reiki a try. I made the necessary appointment and had my first meeting with her about a month ago.

The first appointment started with the naturopath listening to my problems and then with checking for any allergies that I might have. She did that by me holding a metal rod and touching vials of liquids of various substances while she kept pulling apart my thumb and third finger on my left hand gently apart. From that it was concluded that I didn't have any sort of significant allergy. The next step was what she called _http://www.bodytalksystem.com/bodytalk/ body talk.

She basically had my left wrist under her right hand fingers and her left hand fingers over the top of my left wrist and as she mumble questions, she kept moving my left wrist up and down (feeling the muscles I guess). After a minute or so, she would then start tapping very gently the top of the front part of my head followed by tapping in the region of where the sternum, collarbone and the first rib meet.

What she explained to me was that she first “talked to my body” via the questioning and then getting a response through the muscles of my wrist and finally followed by telling the body to heal via the tapping. You can imagine that I was not very sure of what to expect.

After the first visit, I actually got worst which she did explain could happen as the body re-adjusted. Second visit was schedule for two weeks after the first visit and the third visit was a week after the second. She stated that the visits were scheduled based on what my body was telling her. On both the second and third visits, she only did the questioning, response and tapping lasting for about 30 to 40 minutes or so. So in a month, I've seen her 3 times. Guess what? My symptoms are all gone! And that without any medication, supplements, etc whatsoever. Infact after every visit with her, there were changes in symptoms. For example, after my first visit, I stopped coughing up dark greenish phlegm. I would still cough but the phlegm was clear in colour. I've got another visit in about middle of July just to see how's everything going on. I did ask her about using the Ventolin and Flixotide inhalers and basically she told me to use it with no restrictions stating that the body will tell me when it didn't need it anymore. I did use the the Ventolin inhaler during the 2 weeks after my first visit but I did not use the steroid inhaler at all.

To help things along I also started a sort of raw diet. I basically eliminated all bread, pasta, cereals, pastry, etc but only for about week or so. Breakfast started with 2 or 3 squeezed lemon juice followed by a fruit and some plain yoghurt. Lunch was again just plain yoghurt and fruits and at times a boiled egg and dinner was salad with pieces of fried chicken meat. I only started all this about two weeks after my first visit.

Right now, I am symptom free and more or less back to my my normal eating routine although I do try and avoid pastry, cakes, biscuits, cereals, etc. I must say I am impressed by naturopathic methods and kinesiology.
 
I'm thinking that I must have some kind of arthritis in my right hand. Just about every day I will experience pain in my middle and ring fingers, around the middle and upper joints. I'm thinking that it might have been exacerbated by years of using a computer mouse with that hand. But since I'm 28, I wouldn't have expected this kind of pain until I was a bit older. I have a definite suspicion that I am lactose or perhaps even gluten intolerant (my mother is a coeliac). Perhaps now is the time to see what a change in diet regime might do?
 
As ya'll know, I'm always experimenting with new things to try and find the magic bullet against this evil rheumatoid arthritis thing that has me in its grip. I've made tremendous progress and control my pain with diet and have been detoxing for over a year and a half. I've lost weight, look and feel about 10 years younger, but I still have flare-ups if there is something really toxic in the environment. Yesterday, I had a horrible dental experience because I was already in a state of mild inflammation possibly due to pollen in the air or EM changes on the planet, whatever. So, after a HUGE amount of novocaine, injected into five or six separate sites in my mouth, the tooth that was acting up (it was supposed to get a root canal because it has been a problem for several months now), just simply would not calm down. The dentist wouldn't work on me unless the tooth was deadened, so I was sent home to wait a couple weeks before we try again.

As a result of the invasion of the novocaine, the multiple injections, the whole autoimmune response just went crazy. My face swelled up, hurt, I felt like I'd been hit with the flat side of a shovel. All that pain and misery and nothing to show for it!

Some weeks back, I read a comment in an article about arthritis about Cetyl Myristoleate. As it happens, they arrived in today's mail (thank you Anart!) So, today I begin this experiment along with low dose doxycycline (20 mg 2X daily) and will increase my dose on the low-dose hydrocortisone therapy from 2.5 mg to 5 mg per day. I'll let ya'll know how it goes.

Anyway, here's an article about Cetyl Myristoleate for those of you who have arthritis related conditions:

Cetyl Myristoleate: A Unique Natural Compound, Valuable in Arthritis Conditions

by Dr. Charles Cochran and Dr. Raymond Dent

Introduction

Arthritis is a disease of epidemic proportions, but it has been around for so many centuries that it is considered by most people as a part of growing old or a consequence of physical injury. Arthritis is in fact a far more complex disease than is generally known. For instance, Dorland's Medical Dictionary describes 27 different types of arthritis, and that does not include such diverse conditions as systemic lupus erythematosus, scleroderma, fibromyalgia, and numerous other conditions which some authorities consider to be types of arthritis.1 One authority states that there are approximately 100 causes for arthritis.2

Arthritis is thought to affect more than 50 million Americans, and is generally accepted to be the leading cause of movement limitation and disability. It deserves and receives a great deal of research and medical attention. There are hundreds of drugs, procedures, and medical aids and devices directed at coping with the many manifestations of the disease. Given this degree of complexity, certainly no one agent alone could ever be expected to manage or cure "arthritis" in its entirety. New agents take their place in the spectrum and make a contribution. Now there is a relatively new discovery of a natural substance, cetyl myristoleate, which shows promise of making a great contribution in non-infective types of arthritis.

Cetyl Myristoleate

Cetyl myristoleate was discovered and isolated by one person, working alone, on a quest to find a cure for arthritis. Harry W. Diehl, while employed by the National Institute of Arthritis, Metabolism, and Digestive Diseases, specialized in sugar chemistry. He used his chemical knowledge and research instincts to great advantage, identifying and characterizing over 500 compounds, several of which were patented by the National Institutes of Health (NIH). His most significant discovery before cetyl myristoleate was a method of synthesizing 2-deoxydextroribose, a sugar used in the preparation of oral polio vaccine by Dr. Jonas Salk.3

Diehl's interest in discovering a way to help victims of arthritis began over 40 years ago when his friend and next door neighbor, a carpenter, developed severe rheumatoid arthritis. His condition deteriorated over time until he became disabled. The neighbor had a family to support, but his arthritis made that impossible. Diehl is a deeply religious man whose feelings overwhelmed him as his friend's condition worsened. Harry thought, "Here I am working at the National Institutes of Health, and I have never seen anything that was good for curing arthritis."4 He decided to establish a laboratory in his home and embark on a search for something to relieve the pain and disability of his neighbor and the millions of people who suffer from arthritis. Unfortunately, he was too late to help the neighbor, but Diehl's research did lead to the discovery of cetyl myristoleate, which may someday be hailed as one of the significant nutritional discoveries of the 20th century.

The Quest

As a researcher, Diehl knew that finding a cure for arthritis first meant inducing the disease experimentally in research animals. He started with mice, and quickly realized that he was unable to induce arthritis in them. Diehl said he tried every way he could to give those mice arthritis, but they just would not get it. Then, he contacted a researcher in California who wrote to him, "If you or anyone else can give mice arthritis, I want to know about it, because mice are 100% immune to arthritis."5 At that moment, Diehl's research instincts told him that what he wanted was already somewhere in those mice.

It was a long, tedious job, working on his own in his spare time, but Diehl finally found the factor - cetyl myristoleate - that protected mice from arthritis. As Diehl said, "It didn't come on a silver platter to me, but after years of chemical sleuthing and just old-fashioned chemical cooking, I found it!" On thin layer chromatography of methylene chloride extract from macerated mice, Diehl noticed a mysterious compound, which was subsequently identified as cetyl myristoleate. As Diehl was to prove, cetyl myristoleate circulates in the blood of mice and makes them immune to arthritis.

Cetyl myristoleate is now known to exist in sperm whale oil and in a small gland in the male beaver. At this time no other sources in nature are known to contain cetyl myristoleate. While the first amounts of cetyl myristoleate for experimentation were extracted from mice, Diehl quickly developed a method for making cetyl myristoleate in the lab by the esterification of myristoleic acid.

Chemistry

Cetyl myristoleate, an oil, is the hexadecyl ester of the unsaturated fatty acid cis-9-tetradecenoic acid. The common name for the acid is myristoleic acid. Myristoleic acid is found commonly in fish oils, whale oils, dairy butter, and kombo butter. The chemical formula for cetyl myristoleate is (Z)-ROCO(CH2)7CH=CH(CH2)3CH3. Cetyl myristoleate was unrecorded in chemical literature until Diehl's discovery was reported. The current Merck Index of Chemicals does not list cetyl myristoleate. A search of Chemical Abstracts lists Diehl's method of extracting cetyl myristoleate from mice but contains no reference to cetyl myristoleate prior to his 1977 patent.

Experimentation

To test his theory that mice are immune to arthritis because of cetyl myristoleate, Diehl began to experiment on laboratory rats. This research was reported in an article written in conjunction with one of his colleagues at NIH in the Journal of Pharmaceutical Sciences.6 In summary, this paper reports that ten normal mice were injected in the tail with Freund's Adjuvant (heat-killed desiccated Mycobacterium butyricum) to which rats and certain other rodents are susceptible. In a period of 10-20 days, no noticeable swelling developed in the legs or paws. Mice in a second group were injected in the left hind paw. Again, after 10-20 days, no swelling was detected as determined by comparison of the measurements of paws at the time of injection.

Then, a group of rats was injected with cetyl myristoleate, and 48 hours later, they were given the arthritis-inducing Freund's adjuvant. A control group of rats was given Freund's adjuvant only. Both groups of rats were observed for a total of 58 days with respect to weight change, hind and front leg swelling, and general well-being. All rats receiving only Freund's adjuvant developed severe swelling of the front and hind legs, lagged in weight gain, and were lethargic and morbid. Those receiving cetyl myristoleate before receiving Freund's adjuvant grew an average of 5.7 times as much as the control group and had little if any evidence of swelling or other symptoms of polyarthritis.

The authors concluded that it was apparent that cetyl myristoleate gave virtually complete protection against adjuvant-induced arthritis in rats. Furthermore, a 1:1 mixture of cetyl myristoleate and a homologue, cetyl oleate, gave results not significantly different from administering cetyl myristoleate alone.

A Hiatus

Diehl patented his discovery in 1977, receiving a use patent for rheumatoid arthritis. He then sought pharmaceutical companies to conduct human trials with cetyl myristoleate, but none were interested in his discovery. Perhaps the lack of interest was because cetyl myristoleate was a natural substance and could not be granted a product patent, or maybe because drug companies know they will have to run through 25,000 to 35,000 substances before they find one that makes it to market. Diehl had made a major nutritional discovery, and no one was interested! Being a scientist, not a marketing expert, Diehl let his discovery lay dormant for about 15 years.

Cetyl Myristoleate Cures Diehl's Arthritis

As Diehl got older, he began to experience some osteoarthritis in his hands, his knees, and his heels. His family physician tried the usual regimen of cortisone and non-steroidal anti-inflammatory drugs without much effect on the course of the disease. Finally his physician told Harry he could not have any more cortisone. "So," Diehl said, "I thought about my discovery, and I decided to make a batch and use it on myself." He did, and successfully cured himself of his osteoarthritis.

Many of his family members and friends became aware of the relief Diehl got from his discovery, and they wanted to try it too. Time after time, people with both rheumatoid and osteoarthritis received astounding relief with cetyl myristoleate. Before long, family members and friends grew into customers, and cetyl myristoleate appeared on the market as a dietary supplement in 1991.

Clinical Observations and Usage

In common with many other natural substances and drugs, the exact mechanism of cetyl myristoleate's physiologic activity is unclear. As a fatty acid ester, it appears to have the same characteristics as the essential fatty acids, linoleic and alpha linolenic acids, except stronger and longer lasting. These fatty acids are referred to as "essential fatty acids" because the human body cannot make them and we must ingest them in our diets. These EFA's truly are essential to normal cell structure and body function and function as components of nerve cells, cell membranes, and hormone-like substances known as prostaglandins. Many of the beneficial effects of a diet rich in plant foods is a result of the low levels of saturated fat and the relatively higher levels of EFA's. While a diet high in saturated fat has been linked to many chronic diseases, a diet low in saturated fat but high in EFA's prevents these very same diseases.7 The use of EFA's over an extended period of time has been shown to decrease the pain, inflammation, and limitation of motion of arthritis.8

The difference between the activity of EFA's and cetyl myristoleate is that the quantity required and the period of time over which EFA's are taken are markedly longer. Cetyl myristoleate is taken in a one month course of about 13 grams, while EFA's must be taken over extended periods, sometimes many years, and intake varies widely from hundreds to thousands of grams. Cetyl myristoleate seems to have properties in common with EFA's, but it acts faster and lasts longer.

Because EFA's are necessary for normal functioning of all tissue, it is not surprising that the list of symptoms of EFA deficiency is a long one. In chronic inflammatory processes, the supply of EFA's is depleted. Cetyl myristoleate appears to have the ability to correct the imbalance created by chronic inflammation. Like EFA's, maybe cetyl myristoleate turns off the fires of chronic inflammation by serving as a mediator of prostaglandin formation and metabolism.

Venous blood from the gastrointestinal tract is carried to the liver via the portal vein. With the exception of intestinal chylomicrons that enter the lymphatics, all absorbed products pass initially through the liver, and in most instances are extracted or modified before passage into systemic circulation.9 Since all fatty acids enter systemic circulation through the liver, an oil like cetyl myristoleate would begin its systemic circulation from the liver also. It is speculated that cetyl myristoleate stimulates the production of immunoglobulins and series 1 and 3 prostaglandins, which could be one explanation for why cetyl myristoleate has such potent effect in auto-immune and inflammatory conditions.

Cases

Here are some cases involving the use of cetyl myristoleate from the author's practice.

Leona - She is a 64 year old mother of five who has been developing degenerative changes in her fingers over the last 15 years. She plays the piano frequently and had to reduce the amount of playing time as a result of the arthritis pain in her fingers. ANA titers have been mildly elevated over the years and rheumatoid disease has been diagnosed in several of her ancestors and one sibling. Leona's other medical problems are mild hypertension and chronic sacro-lumbar pain which appears to be attributable both to sciatic damage sustained in a water skiing accident 24 years ago and Shunerman's disease as teenager. Demonstrating both rheumatoid and osteoarthritis changes in her fingers, she has a mild nodular deformity at the terminal joints of the 3rd and 4th fingers on the left hand and fusiform swelling in the medial and distal joints of most of her fingers. Her thumbs were intermittently painful and swollen. She first took cetyl myristoleate in mid-January, 1997. There is now increased range of motion in all of the finger joints and visible reduction of the rheumatoid-like swelling. The nodular deformities have not changed noticeably. Her back problems demonstrated no improvement. Her sedimentation rate has run from 15 to 35, and is currently 16, with her ANA <1:360. Leona is now able to play the piano all she wants to without pain or swelling of her fingers.

Joyce - She is a 42 year old mother of three and a court reporter in good general health, suffering only from moderate hayfever in the spring. Recently Joyce developed a generalized stiffness and soreness in her fingers, which was worse on her right hand. The condition became so bad over a couple of weeks that she began making numerous mistakes in her court reporting and her speed was significantly reduced. She was diagnosed with tenosynovitis. Joyce shows no deformities of her hands associated with arthritis. She began a course of cetyl myristoleate during the last week of February and finished the last week of March, 1997. She reports complete restoration of her dexterity with return of her normal accuracy and speed, along with elimination of the associated pain.

Bob - He is a 67 year-old retired politician who suffered lumbar and pelvic fractures in WWII when his jeep struck a land mine. Over the years, these injuries produced increasing pain, which seriously affected routine daily activities like getting out of bed in the morning and his ability to play golf. X-rays demonstrate degenerative arthritic changes in the lumbar articulations and the right sacroiliac joint. At 6 feet tall and 185 pounds, he is otherwise in good health. Bob has been using anti-inflammatory drugs for over 20 years, including Voltaren, ibuprofen, Tylenol, and aspirin. He took a one-half course of 7.6 grams of cetyl myristoleate in September, 1996. He experienced moderately severe inflammation (breakthrough pain) on day two which lasted for three days. On the 4th day, the pain began to subside and was completely gone by the 5th day. He has been virtually pain-free since and is very happy with the increased comfort with which he can begin each day. He can now comfortably walk the golf course whereas before he was limited to a golf cart. In February, 1997, he perceived a slight return of his low back pain and decided to take another one-half course. He experienced no breakthrough pain this time and is currently pain-free. He has not taken any other medication for his back pain since taking cetyl myristoleate initially.

Virginia - She is an 85 year-old lady who still works part-time at the family-owned business and cares for her husband who has cancer. Virginia was diagnosed ten years ago with diabetes, and elevated triglycerides and cholesterol. Overweight all her life, she is now stable at 265 pounds. She suffers from long-standing osteoarthritis in her knees and ankles, for which she was placed on cetyl myristoleate. No other agents have been used by her for arthritis except for non-steroidal anti-inflammatory drugs, both OTC and prescription. After about 7.6 grams of cetyl myristoleate, she was able to walk without limping or experiencing significant pain. About three months following the initial course, some pain returned, but she has retained what she estimates to be 50% improvement. She also has gallstones and a recurrent problem with gout, both of which have been symptomless since her cetyl myristoleate course. She evidently did not receive enough cetyl myristoleate for her body weight and will be given another course of 13.25 grams.

Rose - Rose is a 46 year old mother of four who works as a legal secretary. She was diagnosed five years ago as having an atypical form of multiple sclerosis. She had MRI exams of the skull and spinal cord, which demonstrated several areas of non-specific degenerative changes in the brain with several "bright spots" in the cervical spinal cord. She had periodic visual aberrations as well as constant fatigue and fibromyalgia-like pains focused in her trapezius (bilaterally), and in her upper arms and legs below the knees. She also complained of burning sensations in her hands and feet. All of the symptoms worsened with elevated stress. There was no sign of pernicious anemia or diabetes. She was receiving chiropractic therapy. Joyce was started on numerous naturopathic therapies in March, 1996 without significant benefit over an eight month period. In November, 1996, she started on cetyl myristoleate and indicated that she felt more fatigued for the first three days but that the pain in her upper back and extremities was completely gone. She further reported that the tingling/burning sensation in her feet and hands was also gone. Rose felt this was the most striking aspect of the treatment as those areas were the ones most constantly affected. This improvement lasted until she had to travel out of state to tend to her mother who was diagnosed with a rapidly advancing malignancy. Over the next three weeks, her symptoms began to reappear. After the death of her mother, she returned home in as bad shape as before first taking cetyl myristoleate. She decided that she wanted to take another half course of cetyl myristoleate, which completely duplicated the relief from the initial dosage with the exception that she feels slightly less relief from her tendencies to fatigue than she did after the first course. Rose will be taking another half course to see if she can improve her stamina.

J.P. - He is a 60 year old male who has been a farmer his entire life. Diagnosed with rheumatoid arthritis 15 years ago, he has been on various pharmacologic protocols during that time. The most recent includes Plaquenil, methotrexate, and prednisone, with daily non-steroidal anti-inflammatory drug dosing. J.P. has fusiform swelling involving most of the joints of his fingers and moderate ulnar deviation of both hands. He suffered severe pain most of the time which limited the labor he could perform. He began cetyl myristoleate during the last week of February, 1997, at which time he terminated his methotrexate and Plaquenil (not recommended except in consultation with a qualified physician). He has also reduced his prednisone from 15 milligrams per day to 5 mg, but he still maintains his NSAID dosing on a daily basis. J.P. experienced a mild increase in pain during the first four days of taking cetyl myristoleate, but since then he has been pain free and the swelling in his hands is reducing. J.P. will be monitored over the next month to determine his stability, with checking of his serum parameters by an MD. If he continues to remain symptom-free, his steroid and NSAID therapies will be terminated. J.P. does not smoke, eat chocolate, nor drink alcohol or caffeinated beverages. He was advised at the onset of his cetyl myristoleate dosage to avoid sugar. He is also taking Glucosaplex (a mix of glucosamines) and Lyprinol (fatty acid extract of green lipped mussel) as an additional natural anti-inflammatory agent.

Optimizing the Effects of Cetyl Myristoleate

Since the days of Paracelsus, physicians have been combining therapeutic agents for synergistic effects, or to achieve potentiation of several compounds. As powerful a nutrient as it is, the effects of cetyl myristoleate can be helped by combining it with other natural substances. Two or three grams daily of omega-3 fish oil or two tablespoonfulls of flaxseed oil during the month-long course of cetyl myristoleate can help its effects. This should be accompanied by 300-500 mg of Vitamin E daily. A minimum of 1,500 mg of glucosamine sulfate should be taken daily for at least three months to assist in rebuilding cartilage damaged by degenerative arthritis. In severe cases, three to six grams of glucosamine daily for one month and reduced to 1,500 mg daily for three months has been found to be very effective. Afterwards, a daily maintenance of 500 mg of glucosamine should be used for healthy cartilage. If stomach upset occurs, glucosamine should be taken with meals.

Clinical experience has shown that glucosamine sulfate is far superior when compared to cartilage extracts, such as sea cucumber, hydrolyzed bovine cartilage, and shark cartilage. This is due to the increased absorption and utilization of glucosamine sulfate compared to these sources of chrondroitin sulfates, which are very large molecules and difficult to digest. Animal and human studies have shown up to 98% absorption of glucosamine,10,11 compared to only 8% absorption of chrondroitin sulfate.12

One of the reasons that glucosamine sulfate is more effective in rebuilding cartilage when compared to other sources of glucosamine, including the N-acetyl and hydrochloride forms, is that it provides bioavailable dietary sulfur. Sulfur helps provide the protein links necessary for cartilage matrix repair. Another source of sulfur is methylsulfonylmethane (MSM), which has been used historically to treat a wide variety of conditions including allergies, emphysema, arthritis, gastrointestinal upset, and some vascular conditions. MSM is a metabolite of dimethylsulfoxide (DMSO) and provides many similar good effects. MSM is found in most natural unprocessed foods. Because of its volatility, MSM is lost when fresh food is cooked, processed, or stored. The richest source of MSM is mother's milk; consequently, very few nursing infants are deficient in dietary sulfur.

As with any oil, cetyl myristoleate requires lipase to be digested. Lipases are pancreatic enzymes that play a key role in the digestion of fats and fat soluble vitamins. If lipase is absent or deficient, cetyl myristoleate will be poorly absorbed, if at all. As many arthritis patients are of the age when lipase production decreases, approximately 100 mg of lipase enzyme should be taken with each cetyl myristoleate capsule. In addition to taking lipase, cholecystectomy patients will need lecithin or ox bile extract to assure absorption.

Diet can play a role in optimizing the benefits of cetyl myristoleate. Carbonated cola beverages and citrus juices may block the absorption of cetyl myristoleate and should be avoided on the days cetyl myristoleate is taken. Sugar intake should be minimized when taking cetyl myristoleate, and adding refined sugar to liquids like coffee and tea should be avoided altogether. Alcohol and caffeine intake should be very limited or eliminated altogether while combating arthritis and chronic inflammatory conditions.

Reported Results

Both osteoarthritis and rheumatoid arthritis sufferers report striking improvement with cetyl myristoleate. Numerous private correspondence describes decreased stiffness and pain, and increased flexibility and range of motion with cetyl myristoleate. Swelling and redness is reduced in rheumatoid arthritis. Writers describe other health benefits, including positive effect of cetyl myristoleate on emphysema, hepatitis, hypertension, diabetes, eczema, psoriasis, colds, allergies, low back pain, and headaches. These reported improvements in general health status are not surprising since each of these conditions could be associated with deficiency in the balance of EFA's.

Like everything else, cetyl myristoleate does not work 100% of the time. Failure to work can be associated with failure to follow the dietary recommendations; failure to use lipase in conjunction with each capsule of cetyl myristoleate; failure to take a sufficient amount of cetyl myristoleate; failure of the liver to uptake and respond to the cetyl myristoleate; and, misdiagnosis in which the condition is not really an arthritis-type condition.

Dosage

Cetyl myristoleate is taken in a one month course. A total dose of 12 to 15 grams appears to be indicated. This is usually enough for most people, but for osteoarthritis sufferers, the dose appears to be related to the number of sites in which cartilage has worn away. For example, a patient with osteoarthritis of the knees could expect 10 to 15 grams to be sufficient in most cases, while a patient with osteoarthritis of 5 or 6 spinal discs, both hips, and both knees may require an additional 5 to 10 grams, or even a full second course. Some of the patients treated by the author would likely have benefited even more from their cetyl myristoleate usage with the larger doses now recommended.

Contraindications and Toxicity

With the tens of thousands of people who have taken cetyl myristoleate there have been no confirmed reports of adverse side effects. In common with fish oils, it may produce some mild burping in some people which passes within an hour. There have been no reported interactions with other medications or natural substances, and other substances (except those mentioned above as diet considerations) do not interfere with cetyl myristoleate.

While teratogenicity of cetyl myristoleate is probably the same as for EFA's, as a safety matter cetyl myristoleate should not be used by pregnant or lactating women until studies of cetyl myristoleate's effects on fetuses and infants have been done. As with any substance being added to the diet of anyone with asthma or a history of severe allergic reactions, caution is advised and cetyl myristoleate should be used in these cases under the direct supervision of a health care professional.

Toxicity studies have been performed on cetyl myristoleate and the lack of toxicity is evident. Test results deemed cetyl myristoleate a non-toxic material in accordance with Federal regulations. Mega-doses were given to test animals with no ill effects. Necropsy of test animals showed no ill effects on their internal organs.13 The LD50 of cetyl myristoleate was not established, but it can be presumed to far exceed 10 grams per kilogram of body weight.

Correspondence:

Dr. Charles L. Cochran
226 Lake Court
Aptos, California 95003 USA

Dr. Raymond Dent
RR 1, Box 169
Lymington Road
Limmerick, Maine 04048 USA

References

1. Dorland's Medical Dictionary, 25th Ed.

2. Shils, Olson, and Shike. Modern Nutrition in Health and Disease. Lea & Febigen, 1994. Philadelphia, PA. p. 1480

3. Diehl, H. W. and Fletcher, H. G., A Simplified Preparation of 2-Deoxy-D-ribose Based on Treatment of a-D- Glucose Monohydrate with Solid Calcium Hydroxide, Archives of Biochemistry and Biophysics, Vol. 78, No. 2, Dec. 1958

4. Wright, M.D., J., and Gaby, M.D., A, Nutrition and Healing, August, 1996, Vol.3, Issue 8, paraphrase from page 5.

5. Private correspondence to H. W. Diehl, Rockville, Md. from Dr. Fay Wood, Univ. of Cal., Berkeley, 1969

6. Diehl, H. W. and May, E. L., Cetyl Myristoleate Isolated from Swiss Albino Mice: An Apparent Protective Agent against Adjuvant Arthritis in Rats. Jour. of Pharmaceutical Sciences, Vol. 83, No. 3, Mar, 94 pp296-299.

7. Murray, M. T. Encyclopedia of Nutritional Supplements, Prima Publishing, Rocklin, CA 1996 p. 237

8. Sobel, D. and Klein, A. C.. Arthritis: What Works. St. Martins Press, New York, NY. pp. 221-225

9. Shils, Olson, and Shike. Ibid. pg. 550.

10. Setnikar, I., et al., Pharmacokinetics of glucosamine in man. Arztneim Forsch 43 (10), 1109-1113, 1993

11. Setnikar, I., et al., Pharmacokinetics of glucosamine in the dog and man. Arztneim Forsch 36(4), 729-735, 1986.

12. Morrison, M., Therapeutic applications of chrondroitin-4-sulfate, appraisal of biologic properties. Folia Angiol 25, 225-232, 1977.

13. Leberco Testing, Inc., Jan. 22, 1996, private correspondence to EHP Products, Inc.
 
As a result of the invasion of the novocaine, the multiple injections, the whole autoimmune response just went crazy. My face swelled up, hurt, I felt like I'd been hit with the flat side of a shovel. All that pain and misery and nothing to show for it!


Yeow! I'm with you there. Went through a similar experience a couple weeks ago, and am still not feeling very well. Got the new crown, but the tooth that was filled is still tender enough I might have to go back. (yuck)

((((hugs))))


Be gentle with yourself, it may take a week or two to get to feeling better, but it WILL get better. :)
 
I imagine you guys know that some percentage of root canals continue to have pain associated with them after the procedure. I think it wise to wait some period of time after having a root canal before having a crown put on. The root canal I had never stopped hurting and I choose to have it extracted as opposed to having a crown. Also Laura I imagine you are aware there is a school of thought that root canals become hosts to a great deal of bacteria in the small pockets in the tooth that are not filled by the dentist. The problem is that options other than a root canal are usually not very practical
 
Thanks Laura and looking forward to read your comments on this cetyl myristoleate substancce. My grandfather life is currently worsen by arthritis, so I will be more than happy to make the remaining days he has to live better.
 
Yes, I'm aware of all the issues surrounding root canals. I have two and one of them I've had for over 25 years with not a minute's trouble with it. The other one is only about 5 years old and it's fine also.

One thing I did to calm my mouth down pretty fast was to take a mouthful of 50% DMSO and just hold it for about five minutes. Then I spit it out. I'll do it again today. It's about 70% better this afternoon, by the way.
 
Laura said:
Yes, I'm aware of all the issues surrounding root canals. I have two and one of them I've had for over 25 years with not a minute's trouble with it. The other one is only about 5 years old and it's fine also.

One thing I did to calm my mouth down pretty fast was to take a mouthful of 50% DMSO and just hold it for about five minutes. Then I spit it out. I'll do it again today. It's about 70% better this afternoon, by the way.


Hmmm. I don't have DMSO, but I do have colloidal silver. It might be worth trying for the tooth still bothering me? I can't talk today in any case. :rolleyes:

Glad to hear you're feeling better! :D
 
Gimpy said:
Hmmm. I don't have DMSO, but I do have colloidal silver. It might be worth trying for the tooth still bothering me? I can't talk today in any case. :rolleyes:

Glad to hear you're feeling better! :D

Colloidal silver will be less than worthless for that. Get a big bottle of DMSO and have it on hand. Read up on it, too! It is AMAZING stuff! You can drink it, too! It can save a person's life!
 
My wife has rheumatoid arthritis as well as neuropathy, diabetes and osteoarthritis. I'm researching this area for as much info as I can get and collate in order to see what I can do for her. She is on a medicine therapy, but lately, the pain in her legs (she says it feels like bone pain) gets so bad she lays in bed and cries some time.

I feel really bad for her and have been doing everything I can do to make her life easier, so I'll be interested in how this Cetyl Myristoleate works for you.

I hope your mouth is feeling much better by now! :)
 
Back
Top Bottom