Suppressed Inventions and Other Discoveries (17 page)

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GN: Describe what the treatment consisted of.

SAT: The polyatomic apheresis looks like the following: a patient sits in a chair that looks a little like a dentist's chair. It's a comfortable chair. There are intravenous needles inserted in both of their arms, the blood coming out of the left arm is pulled through a pump that is in synch with the heart rate, and a circuit of blood is created between the left arm coming out and the right arm coming in. The blood goes through a series of tubes, goes down through a cascade tube where it is met with ozone under pressure, and at that point that's where the viral kill happens. The blood continues down through an escape tube, through a filter, back into their right arm. What you see visually is the blood exiting the left arm is a very black colour; it is black. It goes down through this cascade tube, which is a wide bore cascade tube, about an inch in diameter, and it goes back into the arm, the right arm, a bright cherry-red colour. It comes out looking alarmingly different—this is with the HIV patients—alarmingly different from what you would expect.

Now, the first patient I saw on the machine was a person without HIV. She was a normal prison who had an infected foot, and her blood came out looking like yours and mine would, and went back in only slightly differently than it came out; so what I witnessed was that the HIV patients' blood was considerably blacker than a normal person's and went back considerably lighter. That's, in a nutshell, what it is.

GN: Alright, now, what other parts of the therapy were included with this ozone treatment, and how does this ozone treatment differ from, let's say, one which would be done in New York where you pull out about, oh, a half pint of blood, ozonate it and put it back in the arm over a fifteen- to twenty-minute period?

SAT: I've never witnessed any of the other treatments that you're talking about. The only two ozone treatments that I've seen actually operate are the polyatomic apheresis and, using the same equipment, a process called rectal insufflation where the ozone gas is put in through a catheter into the rectum, which becomes an ozone enema, so to speak. Those two were used at the clinic and in conjunction with one another. Some of the participants in the study had experienced the treatment that you are talking about and had some success with it. What they believe from their own experience, what they told me, is that it was the difference between a Volkswagen and a Rolls Royce, from what they felt with the treatment, you're talking about getting in New York versus what they got in the Philippines.

GN: So, it was far more productive in the Philippines?

SAT: Correct.

GN: Now, what happened to these twenty patients? Where are they at now and have there been any additional protocols for these people to follow?

SAT: The turning point of everything was on March 19. The youngest participant was a 23-year-old woman named Jodi, and she had full-blown AIDS. It was a real tragedy because she really kind of represented all of our daughters, and her courage was phenomenal. She died in the clinic and that's when things started to tumble very quickly. She died from a series of complications. I'm not a medical expert but I believe she received two insufflations too close together and her body had trouble coping with the amount of ozone that she had taken in. She also received those against doctor's orders, so I guess it would have to be chalked up to human error rather than anything to do with the equipment. She received the ozone via the rectal insufflation.
GN: You mean the Philippine doctors had suggested she not take those?

SAT: Actually, it was the American doctor, the expert on the ozone, who had said this girl shouldn't have another until she recovers a little bit. She had remarkable success on the equipment, though. When I first arrived I was afraid Jodi was not going to make it until the equipment arrived. There were all kinds of customs hangups that prevented the equipment from getting into the country and getting set up on time. So the patients arrived ahead of the equipment, which was a real management error because it just added too much stress to the patients.

GN: By the way, who raided the clinic?

SAT: It was raided by the Department of Immigration.

GN: Was there any evidence the FDA had been involved in the raid?

SAT: There wasn't any evidence that the FDA had been involved; but what I was told was that the story really got underway when Australia's version of A Current Affair did a scathing story on the clinic and what the patients were about to experience, just as they were getting on the plane. I was told by another journalist in Australia whom I trust, that ACA is the one who went in to the Department of Immigration and tipped them off. I was also told that the producers were directed by their upper management to do a 'chuck job' on the ozone therapy. And no matter what they were told, no matter how much positive information they were given, it never aired; and I watched this happen time after time.

GN: So, in other words, there was a gross bias in the media, from your interpretation, to prevent positive stories about the success of ozone from getting back to the general population?

SAT: It's not even a question of interpretation. I watched it happen; I watched the participants give interviews; I gave interviews myself. We would turn on the TV and we would be shocked at what actually would show up. Paul, whom I was telling you about, would tell his entire story; he would show his feet, all of those things; and he made a comment in one of the television interviews where he said, "After I got going I could just feel it in my heart that this was working." That little snippet is the only thing that they would use, and then they would cut to the doctor saying, "Well, you know, there's a certain amount of mind over matter," and all that kind of stuff. So they were completely dismissing the science of it and trying to make it sound like their improvements were all in their own minds; but fifteen patients had improved T-cell counts, one as high as a 70-percent increase.

GN: I would like to shift gears, now, and bring in another individual to share a different perspective on this, and one that we haven't talked about in the past. Basil Wainwright, welcome to our programme.

BW: Thank you very much, Gary. I must congratulate you on running a super programme, and a very courageous one too.

GN: Basil, you are now incarcerated in Florida?

BW: That's right, so if any of your listeners hear any background effects, I must apologise for that. I am currently incarcerated down here in Miami.

GN: From what I understand, you are a scientist and you are the inventor of this polyatomic machine, this ozone machine, and that you have been incarcerated without trial for three years. Is that correct?

BW: Yes, I'm now well into my third year without trial and some seven violations of my basic human rights.

GN: What are those violations?

BW: Well, there's the 4th amendment and the 5th amendment, the 6th amendment has been violated, and the 8th, and 14th. So . . .

GN: What has happened to your attorney filing proper motions to get a fair and speedy trial? That's one of the constitutional provisions for people who are incarcerated. I haven't heard of people waiting three years except this particular political detainee who was here in New York, the IRA supporter who was held for some seven years.

BW: That is absolutely right. Well, it all started that—really, I suppose I should give you and your listeners a brief synopsis. I was working with Dr. Viebahn in Germany and I was brought into this project along with Medizone, and then got very much involved in the process. And I was somewhat intrigued to find that nobody had really done any specific testing i.e., looking at the cytotoxic levels or, that is, the concentration of ozone, looking at the specific atomic structures of that, and also the contacting time; so there were an awful lot of areas that particularly interested me. I worked with the University of Medicine and Dentistry and also the Mt. Sinai Hospital with Dr. Weinburg and with Dr. Michael Carpendale, and started to get very, very involved in the course.

It was very evident there were some phenomenal results being seen in the AIDS area and I started to look at it more in-depth. There were several controversies going on as to whether it was a function of free radical reaction or oxidation—but of course both of those functions occur extensively—and also this ionisation; and I wanted to determine the specific parameters of that, because when people refer to ozone you might just as well refer to a vehicle being involved in a collision because you're not really defining the atomic structure of ozone which can be multifold. There can be many aggregate combinations of molecules which can have very specifically different responses, and I wanted to determine this.

GN: Since 1985 you have been working with some German doctors including Dr. Viebahn that you talked about. Now, you had a way of determining that the ozone being used back then was not as effective as the way you could create a better ozone; they were using O
2
but you also saw O
3
and O
4
.

BW: Yes.

GN: Now tell us about what you found with what you created concerning viral inactivation.

BW: Well, of course, I think it's very important for your listeners to know that the reason scientists refer to retroviruses' inactivation as opposed to being killed is because normal micro-organisms have metabolic mechanisms, whereas a retrovirus could almost be considered a piece of genetic material drifting around in the bloodstream. And so, it's rather difficult to kill a non-living thing, hence scientists refer to inactivation. We looked at these various techniques and procedures, including the study which we did with Biotest in worked but wouldn't treating high enough volumes of blood. We wanted to see that once someone had been taken back to HIV negative using polyatomic oxygen or ozone, they indeed remained negative. I think there is only one case that actually went back to positive so that was rather unique because all the doctors were saying, Okay, so what? You get somebody to negative, but in a couple of months' time they're going to go back to positive. Well, that was proven not to be the case, which I think even surprised the Germans. And it might well be that the immune system k i c k s back in, and when we

Miami. We determined that the German process be dramatically effective because they were not say negative we're looking at nucleic acid response or PCR work to determine that; but certainly the patients were not going back to positive—that was very interesting.

So we thought, okay, if these patients are going to use autohemotherapy which you referred to earlier, Gary, where you take out half a pint of blood, treat it with ozone, and then reinfuse it back into the patient, that was taking typically eleven months, of course combined with a very rigid nutritional control as well. But using that process it was very evident that it's like chipping away at a mountain with an ice pick when you're looking at the view of this pandemic facing mankind; and it became very apparent in 1987 that the best way to go was with dialysis or a dialysistype procedure. So I worked with dialysis equipment and in fact filed my first dialysis patents using ozone in 1988.

However, using ordinary dialysis equipment which is a hollow fibre membrane, we discovered there was too much homolysis occurring as a result of that; also, the thing that we refer to as mechanical shear. The very fact of pumping the blood round outside the body can cause all sorts of trauma to cells—there are thermal reactions, there are pressure zones, the pumping head itself can actually crush cells—so we had to look at a number of factors. And then, when we did more research, we found that O
4
in particular had some very unique responses. It has a phenomenal amount of electrons; as a matter of interest, in O
4
you have 40 electrons, and that makes it a very powerful negative ionising platform drifting around in your bloodstream. It was also far more stable than O
3
which again was completely the reverse of what everyone was projecting.

It was very evident that O
3
had a better oxidative effect, and that was very effective in eliminating infected cells, but O
4
had the ability because of its ionisation to break down, we believe, the RNA, and of course uracil, which is a very important sugar combination—the 5-carbon sugar in the virus RNA—was actually being broken down. Well, when we actually achieved this, we did our first study down at Biotest Laboratories here in Miami—hence my incarceration down here. We did this study and as far as I know, for the first time in history, using apheresis we successfully converted HIV-positive to negative, and we could do this time and time again using PCR. That's the reason we came here, actually, because Biotest Laboratories in conjunction with Miami University had this latest state-of-the-art equipment; and from that very moment, the FDA witch hunt started.

We tried to keep a relatively low profile but of course the word soon got around the system, and then one night I came home and the SWAT team descended, guns drawn, and eight of them sort of crashed in the front door. I was arrested and charged with practicing medicine without a license, which of course is complete nonsense. But the SWAT team, instead of looking for anything that might indeed have been relevant to my practising medicine without a licence, all they did was dig out all my patent specifications, technical data and intellectual mechanisms. So they came with a very specific directive from the FDA, to seize all my intellectual property rights. From there I was thrown into prison. Eventually I had charges from the FDA which boil down to sending and selling ozone generators from interstate—interstate trading laws, etc. Unfortunately, a couple of months after I was in prison, it was discovered that I had a very severe heart condition. In fact, if this radio show had been yesterday I doubt very much if I could have done it. It's progressed to a point now where I'm collapsing and having blackouts and stuff, but still hanging in there. I've just recently done a technical paper.

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