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Comments on Lombardi, et al in Science

Otis

Señor Mumbler
Messages
1,117
Location
USA
If someone lets me know how to do it in idiot proof language that my legendary computer skills can cope with i will try when I have led the oppositions drivel in more detail.

Gerwyn,

Here's one thought. If you can write a rough draft (with references as appropriate) we can try to fix up the typos, readability, footnotes, etc. I would likely request some clarifications/elaborations.

If we get it to the point where I understand it the language will idiot proof by definition. :^)

Otis
 
G

Gerwyn

Guest
sorry this is the letter

Well-conducted case-control studies provide important insights into disease pathogenesis. Lombardi et al. (1) demonstrated an apparent association between chronic fatigue syndrome (CFS) and the presence, infectivity of, and immune response to the human gammaretrovirus, xenotropic murine leukemia virus–related virus (XMRV).

I am surprised that Sudlow begins with such loose terminology.Lobardi et al reported a statistically significant correlation beween patients who fulfilled the Canadian Consensus criteria for diagnosing a person as suffering from ME,cfs defined as a neurological disorder by the world health authority and the presence of XMRV.

First, although the CFS cases studied fulfilled broadly accepted diagnostic criteria,

Again I am surprised by this comment. The CCC diagnostic criteria are the only clinical diagnostic guidelines in the world.All others are research guidelines.The FUKUDA guidelines are internationally agreed and recognised.The research guidelines(The Oxford criteria) used to diagnose people in the European studies are not. The Oxford criteria has fatigue as the only mandatory diagnostic criteria(sharpe et al 1991).This a strange way of diagnosing a neurological disorder.The CCC guidelines on the other hand have neuroimmunoendocrine symptoms as mandatory.

Sudlow also seems to be unaware of the fact that CFS is not an objective diagnosis.

It is a socially constructed label driven by the diagnostic criteria applied by the diagnoser.Different doctors apply different diagnostic criteria and thus produce objectively different patient cohorts which are unfortunately given the same label.
I am astonished that someone who purports to be an epidemiologist does not seem to realise this.

Second, to avoid selection bias, the CFS-free controls should have been drawn from the same background population as the cases and selected independent of the exposure (in this case, a viral infection) under study (2, 3). Put simply, the controls should ideally have been people who would have been cases in the study if they had CFS.

Sudlow is assuming that XMRV is not causative.Put simply if XMRV is causative then Sudlows design would leave us with no way of telling XMRV levels in patients with CFS compared to controls.They would all have equal levels of the virus .Selection bias is all to obvious in the Imperial college study because all the patients were supplied by one psychiatrist using diagnostic critera constructed by himself and his colleagues which are not internationally recognised.Sudlow is completely silent on this subject.

However, the control subjects are not described in (1) beyond a mention that they were healthy donors. Third, the lack of clinical data for cases and controls makes it impossible to assess the potential for confounding by numerous other characteristics that may independently influence XMRV status, including age, sex, social deprivation status, medical history (e.g., of prostate cancer), and area of residence.

None of these parameters are described in the European studies.She seems to be accepting,albeit tacitly, that there is a link between XMRV and prostate cancer while questioning the link between XMRV and ME/cfs which is in statistical terms about a hundred times stronger.There is no clinical data supplied in the European studies for any of the patients control groups or otherwise.

Fourth, Lombardi et al. do not explain whether identical and contemporaneous laboratory sample storage, handling, and analysis procedures were used for both cases and controls. Differences in these could be another potentially important source of confounding. Fifth, even if identical laboratory procedures for cases and controls were intended, researchers exploring an exciting new hypothesis of a viral cause for CFS in a laboratory established to explore biological causes of CFS will be understandably eager for positive results. This so-called "expectation bias" may lead to completely unconscious and nondeliberate differences in sample handling and data interpretation between cases and controls; it can be avoided only if researchers are blinded to the case-control status of the samples. However, this is not described in (1).

Expectation bias arises as a result of the self biasing nature of mental representations.This leads us to interpret things according to the nature of our beliefs world views and expectations.In neurocognitive terms it is called top down processing. This is one of the main reasons why the scientific method is constructed in such a way that to test a hypothesis is to actively try to disprove it. Lombardi et al far from displaying expectation bias challenged their hypothesis by attempting to find XMRV using 4 different methods.Had any one of their approaches failed then their hypothesis would have been invalidated.That is robust science.Contrast that to the approach used in the imperial; college study when the author of the study on the basis of one study claimed that”there is no XMRV in the UK.That in objective terms corresponds to the scientific definition of expectation bias.By not extending the scope of her analysis to the other studies in this area Sudlow appears to be displaying cognitive biases of her own.

Aside from these crucial methodological issues, other plausible alternative explanations for the findings are not explicitly discussed. Foremost among these is reverse causality: Patients with poor general health because of CFS may be more susceptible to viral and other infections.

The conclusion in the study by Lombardi et al was that there was a statistically significant correlation between the presence of XMRV and peopled diagnosed with ME,cfs according to the CCC criteria. There were a myriad of counfounding vatiables in the design of the European studies which made the results impossible to interpret and the conclusions reached unfalsifyable. Surely an epidemiologist would note that point.

Finally it is extremely common that people in very poor health because of a retroviral infection fall prey to secondary pathogens.This is what happens in patients suffering from Aids.So it is far more likely that a retroviral infection accounts for the poor health seen in patients with ME,cfs.I feel that a scientist should offer that as an alternative explanation especially as she is so keen on plausible alternative explanations been put forward Sudlows explanation that people with CFS are in such poor health because that they are susceptible to XMRV infection is rather like saying that people with AIDS are in such poor health that they are susceptible to HIV infection.It is a totally circular argument and not one I would expect from someone who purports to comment on technical issues
 

oerganix

Senior Member
Messages
611
I agree - I missed that - and later included it in my post. I think that was an area where answering the question allowed the WPI to further strengthen their case. It sounds like both groups had 'blinding procedures' in place. Its unfortunate they didn't spell them out in the paper.

I think its unfortunate that this red herring has grown all out of proportion. Anyone, retrovirologist or not, upon reading the paper, would know it was a blinded study. Why do it any other way? No researcher would. Cleveland Clinic, NCI and Science magazine would not have gone along with a study that wasn't blinded, and blinded properly, so they all knew it was. Bringing it up in the comments is just more smoke, mud in the water and BS.
 

oerganix

Senior Member
Messages
611
XMRV's fate does not hang on these questions and answers; most of the questions were presumably admitted some time ago - at least a month and a half ago - and the WPI has answered most of them. Science, however, wanted the answers in print. Its not usual to see something like this and Science would not publish questions it did not consider relevant. And several of the questions were relevant at least at one time. I see them as an opportunity for the WPI to buttress its case.

Regardless of whoever made them or what their background is - there were relevant questions about the study. For instance this



WPI admitted they made a mistake by stating the patients had reproducible immune abnormalities, VO2 max problems, etc in the Science paper. That statement lead to statements like this:



Based on what was reported in the Science paper that's a perfectly legitimate statement. They also made a mistake by stating the patients came from areas where 'outbreaks' had occurred; - both those statements threw alot of people off. They lead some researchers to believe that all the patients came from outbreaks and we know that's not true. That lead to this comment



The WPI later cleared up these questions on their website but we don't know when the comments to Science were written and it may have been that Science wanted the answers down in the Journal anyway. No papers are perfect - mistakes can probably be found in most papers and these did create questions in the research community. Dr. Vernon was clearly worried about the cohort as were other researchers; it came up again and again.

Dr. Mikovits recently stated in the IACFS/ME Q&A that the only immune abnormality that correlated iwth XMRV infection was Interferon alpha. The authors are correct that that abnormality is NOT typically associated with CFS. On the other hand none of the immune abnormalities associated with CFS (RNase L, Natural killer cell problems, and some of the cytokines (although watch out for that)) were associated with XMRV infection. Now to be very objective that has really got to give you pause. If XMRV is a major factor in CFS then it's affecting the immune system in a unCFS-like way. Its obviously a complicated situation.



Based on my reading of the Science this is absolutely true - cytokine profiles in studies are generally all over the map.

"The WPI later cleared up these questions on their website but we don't know when the comments to Science were written and it may have been that Science wanted the answers down in the Journal anyway. No papers are perfect - mistakes can probably be found in most papers and these did create questions in the research community. Dr. Vernon was clearly worried about the cohort as were other researchers; it came up again and again."

1) Those comments could have been modified or withdrawn up until the date they were accepted for publication: April 16, 2010. That they didn't do anything to modify their comments just shows they were trying to trash it in the guise of legitimate scientific criticism. And during all this, the Dutch researchers knew XMRV had been found in their own samples, but didn't reveal that.

2) Oh yes, we remember how Vernon went on and on about cohort, just like the psych lobby did. Thanks for reminding us of how she was willing to support the "it's all in your head" guys' agenda and couldn't be bothered to pick up the phone or email and ask Lombardi, Mikovits or Peterson these questions before publishing her "worries". Funny how she's willing to cut slack to those slackers overseas, but can't do the same for WPI. If she were just to be honestly impartial, I'd accept that, but that she has to go so far as to snipe at WPI without even communicating her concerns to them beforehand is just disgusting. She willingly participated in the disinformation campaign of Wessely and clones and that is unforgiveable. She should have been in there fighting for the truth about this illness, but when the bullies piled on, she joined them.

Cort, your comments seem to indicate that you believe those critical comments published in Science are coming from scientists who sincerely want to find the physical cause of ME/CFS, and to save us from the likes of WPI/Cleveland Clinic/NCI/Peterson/Lombardi/Moskovits; that they have no hidden agenda, contrary to what their history indicates. Is this really what you think is going on?
 

Orla

Senior Member
Messages
708
Location
Ireland
for gerwyn

I am v brainfogged and too wrecked to check this, but I think the groom et all paper and the McCLure one used Fukuda not Oxford. The Dutch one used Oxford. But I have not double checked this.

Orla
 

starryeyes

Senior Member
Messages
1,558
Location
Bay Area, California
The questions asked in this latest Science article show that these authors have no understanding of the pathology of ME/CFS:
Comment on "Detection of an Infectious Retrovirus, XMRV, in Blood Cells of Patients with Chronic Fatigue Syndrome"
Cathie Sudlow,1,2,* Malcolm Macleod,1,3 Rustam Al-Shahi Salman,1 Jon Stone1

They write: Although this cytokine profile may be associated with a possible viral infection (while by no means being necessarily specific), it has not been reported previously as such in patients with CFS. The cytokine abnormalities in CFS patients are notoriously inconsistent (9), with some studies reporting increased (10), not different (11), or even lower (12) cytokine responses. Thus it is not possible to use "immunological abnormalities" as a selection criterion.

I think they missed the boat on understanding CFS here. In CFS cytokine production as well as many other chemical processes in our bodies, are either running too high or too low.


Based on my reading of the Science this is absolutely true - cytokine profiles in studies are generally all over the map. - Cort Johnson

Yes they are all over the map:
Results
We clustered the results of the cytokine assays into 5 groups according to the cytokine literature.

The results of the individual Kruskal-Wallis analyses are shown in Table 1.

Table 1. Cytokines in Plasma of Female CFS Patients Compared to Female Healthy Controls.

Pro- inflammatory Cytokines:
A significant elevation in the relative amounts of 4 of 5 pro-inflammatory cytokines in peripheral blood plasma of patients with CFS was found when compared with the controls

Only tumor necrosis factor (TNF)α was unchanged.

In cases, lymphotoxin (LT)α was elevated by 257% and IL-6 by 100% over the controls.

TH2 cytokines:
Both interleukin (IL)-4 and IL-5 were elevated in CFS, with the median of IL-4 240% and of IL-5 95% higher in cases over controls.

Anti-inflammatory cytokines:
IL-13 was significantly lower (!5%) in CFS patients while IL-10 was not different.

TH1 cytokines:
Median plasma levels of IL-2 and IFNγ in CFS were similar to those in controls. However, IL-12 was significantly elevated (120%) and IL-15 decreased 15% in cases compared to controls.

IL-8 (CXCL8):
This chemokine was 42% lower in the CFS patients.

TH17 cytokines:
IL-17 and IL-23 were not significantly different in CFS cases compared to controls.

ROC curve analyses
Results for those cytokines that were significantly higher in the case/control comparison are shown in Figure 1 and Table 2.
Those for cytokines that were lower in CFS than controls are shown in Figure 2 and Table 3.


Area under the curve (AUC) for IL-5 (0. 84), LTα (0.77), IL-4 (0.77), IL-12 (0.76) indicated good biomarker potential.


Coordinates of the curves for these 4 cytokines are in Additional File 1. The AUC of IL-6 (0.73), IL-15 (0.73), IL-8 (0.69), IL-13 (0.68) IL-1α (0.62), IL-1β (0.62) showed fair potential as biomarkers (Tables 2 and 3).

Additional file 1. Coordinates of the curves for those cytokines with AUC that indicated good biomarker material.

Format: DOC Size: 667KB Download file
This file can be viewed with: Microsoft Word Viewer

Table 2. AUC for Plasma Cytokines Significantly Higher in CFS Cases vs. Controls

Table 3. AUC for Plasma Cytokines Significantly Lower in CFS Cases vs. Controls

Figure 1. ROC curves shows the classification performance of plasma cytokines from CFS cases and healthy controls. Curves are for the 7 cytokines significantly elevated (p < .05) in cases compared to controls (IL-4, IL-5, IL-12, LTα, IL-1α, IL-1β, and IL-6).

Figure 2. ROC curves show the classification performance of plasma cytokines from CFS cases and healthy controls. Curves are for the 3 cytokines significantly lower (p < .05) in cases compared to controls (IL-8, IL-13 and IL-15).

http://www.translational-medicine.com/content/7/1/96

Cort wrote: WPI admitted they made a mistake by stating the patients had reproducible immune abnormalities, VO2 max problems, etc in the Science paper.

That's because our immune system abnormalities are not reproducible. Our immune systems are dysfunctional but not consistent when tested. This is one of the reasons many doctors believe CFS is a waste basket disease. Do we the patients, know better? Heck yeah! Does the WPI know better? You know it does! There is a lot of literature out there showing that there are major immune system abnormalities in CFS and many of us know this intrinsically because we catch everything that comes around.

Here's an article put out by Klimas et al. that highlights immune system abnormalities in CFS:

http://www.ncbi.nlm.nih.gov/pmc/articles/PMC267940/pdf/jcm00054-0338.pdf

Cathie Sudlow,1,2,* Malcolm Macleod,1,3 Rustam Al-Shahi Salman,1 Jon Stone1 wrote: As a consequence, it is surprising that no independent cohort of patients with sporadic CFS was investigated by Lombardi et al., as these CFS cases represent the majority of patients. Investigation of such an independent cohort is necessary before a claim regarding the presence of the XMRV retrovirus in CFS patients is justified.

They don't believe there have been outbreaks of CFS. Even Dr. Yes's doctor threw that one in his face the other day, just like a lot of our doctors do. But we know differently.

Here's a list of epidemics in ME/CFS:

http://www.evri.com/media/article;j...;jsessionid=gzwkv1m8acax&referring_title=Evri
 

Orla

Senior Member
Messages
708
Location
Ireland
Jon Stone background

Too wiped to participate properly in the discussions, but I thought people would be interested in this little bit of background on Jon Stone, who co-authored one of the letters.

It concerns a case where a patient with CJD, Creutzfeldt‐Jakob disease, (a serious, progressive and fatal neurological disorder) was misdiagnosed with Conversion disorder (new name for Hysteria). Stone was not involved in this patient's "care" or the misdiagnosis, but his response to the case was interesting.

An article was written by the people involved in the patients care, basically trying to justify their misdiagnosis and make out that some of her symptoms were psychiatric. Stone et al sent in a letter in response.

This article I quote below quotes some of Stone et al's letter (I have put a few things in bold text). It is worth reading the full article by Webster which includes more information on the case of the woman with CJD misdiagnosed as being hysterical. It is shocking and sad.

Hysteria
Medicine, psychiatry and misdiagnosis

RICHARD WEBSTER
2007
http://www.richardwebster.net/000HysteriaOpening.pdf (ME is mentioned briefly in this article in a sympathetic way, it is worth a look)

....This attempt to rationalise a medical mistake and to present error as insight is not the end of the story. Soon after the ‘case‐conference’ paper describing Ms A’s case was published in the American Journal of Psychiatry two English [Ed - they are in Scotland strictly speaking] physicians began to prepare a response to it which would eventually appear in the journal in February 2003. The physicians in question were Jon Stone, a neurologist at the University of Edinburgh, and Michael Sharpe, Professor of Psychiatry at the University of Edinburgh. The letter which they submitted to the journal also carried the name of Martin Zeidler, a specialist in Creutzfeldt‐Jakob disease

When their letter is read carefully it is not clear that they accept that the diagnosis of conversion disorder which had been given to Ms A was a mistake at all. The mistake, it would seem, was the failure to recognise the presence of neurological disease as an aspect of her condition: ‘Clinical vigilance for a missed diagnosis of neurological disease,’ they write ‘in cases of conversion disorder is essential’[italics added]. This reading of their position is reinforced by what they say elsewhere:

The authors [of the paper about Ms A] usefully highlighted how organic disease may be important in generating symptoms that are medically unexplained, either directly by effects on brain function or because of more complex behavioral responses to illness. They also showed how our current somatoform classification leaves little room for a dual diagnosis of organic and functional disorder. This unsatisfactory either/or philosophy is perhaps one reason why doctors are reluctant to diagnose conversion disorder in the first place.

Their closing words do appear to concede that Ms A’s psychiatrists made a mistake. But the thought that this mistake might actually lead to physicians exercising more caution about making the diagnosis of conversion disorder is clearly one which Stone, Sharpe and Zeidler find unacceptable:

It would be a shame, however, if this case conference reinforced the erroneous idea that the development of neurological disease in such cases is the norm. Failure to make a positive diagnosis of conversion disorder can have serious adverse consequences. The patient may be denied appropriate treatment management that vitally depends on persuading him or her that the symptoms are reversible and not due to disease. We should not withhold the diagnosis simply because we occasionally get it wrong.

The fact that this letter was written at all is testimony to the continuing prestige and apparent usefulness of the diagnosis of hysteria – in some quarters at least. Yet it leaves unaddressed the most disturbing aspects of the original article.

What ought to be recognised as one of the most shocking features of the case history of Ms A is the inability of her original physician, and the psychiatrists to whom she was subsequently referred, to ‘see’ their patient, or the symptoms from which she suffered, in any but the most perfunctory sense of the word. Instead of relying on their own eyes and their own observations to register the reality of her illness, they evidently chose to place all their faith in the results of technologically sophisticated tests. When the machines they were relying on failed to show that their patient was ill, they concluded that she was physically well and that her symptoms were the product of some occult process taking place mysteriously somewhere inside her. Their belief that her various, increasingly acute physical symptoms could all somehow be ‘produced’ by the process of somatization or conversion was not a rationally tested belief, nor was it empirically verifiable. It depended entirely on their faith in an article of medical ‘knowledge’ which they had apparently accepted on trust from their elders.

It is this same article of received medical wisdom which informs the letter submitted by the three Edinburgh‐based physicians in response to the case history.
 
G

Gerwyn

Guest
I am v brainfogged and too wrecked to check this, but I think the groom et all paper and the McCLure one used Fukuda not Oxford. The Dutch one used Oxford. But I have not double checked this.

Orla


No Orla the patients were diagnosed according to the criterea set out by Sharpe et al.

The way it was put in the studies was confusing

If you read it closely the patients were assessed by a semi structured interview designed by sharpe et al 1991.This semi structured interview establishes CFS according to the Oxford criteria.

They then stated that the patients complied with the CDC criteria.They did not specify which presentation or whether it was FUkuda or the 2003 version.Oxford can be made to look like Fukuda:

Fatigue difficulty in concentrating,sore throat, headache joint pain

Now is that ME/cfs? It does comply with FUKUDA but it also rrepresents the symptoms of patients with clinical depression.

The only symptom which is mandatory under Oxford is fatigue.

"other symptoms MAY be recorded" (sharpe et al 1991)

Funnily enough the Oxford permutations match the 2003 criteria almost exactly strange is it not?
 
G

Gerwyn

Guest
"The WPI later cleared up these questions on their website but we don't know when the comments to Science were written and it may have been that Science wanted the answers down in the Journal anyway. No papers are perfect - mistakes can probably be found in most papers and these did create questions in the research community. Dr. Vernon was clearly worried about the cohort as were other researchers; it came up again and again."

1) Those comments could have been modified or withdrawn up until the date they were accepted for publication: April 16, 2010. That they didn't do anything to modify their comments just shows they were trying to trash it in the guise of legitimate scientific criticism. And during all this, the Dutch researchers knew XMRV had been found in their own samples, but didn't reveal that.

2) Oh yes, we remember how Vernon went on and on about cohort, just like the psych lobby did. Thanks for reminding us of how she was willing to support the "it's all in your head" guys' agenda and couldn't be bothered to pick up the phone or email and ask Lombardi, Mikovits or Peterson these questions before publishing her "worries". Funny how she's willing to cut slack to those slackers overseas, but can't do the same for WPI. If she were just to be honestly impartial, I'd accept that, but that she has to go so far as to snipe at WPI without even communicating her concerns to them beforehand is just disgusting. She willingly participated in the disinformation campaign of Wessely and clones and that is unforgiveable. She should have been in there fighting for the truth about this illness, but when the bullies piled on, she joined them.

Cort, your comments seem to indicate that you believe those critical comments published in Science are coming from scientists who sincerely want to find the physical cause of ME/CFS, and to save us from the likes of WPI/Cleveland Clinic/NCI/Peterson/Lombardi/Moskovits; that they have no hidden agenda, contrary to what their history indicates. Is this really what you think is going on?

what really gets me is that vernon knows that different diagnostic criteria produce different patient groups.She co authored a paper on the very subject!
 

Impish

Senior Member
Messages
101
Location
Victoria, BC
Look... I hate to say this as it is going to get me flamed I am sure but if you stand back there are starting to be some real warning signs from WPI.

They in effect own VipDX who are making money selling XMRV tests. Judy is now running all over the place linking XMRV with other diseases (Autism, Lyme Disease) with no published research backing it up. The fact that they are finding XMRV all over the place and no one else ever has at some point has to start to raise some red flags.

They are now associated with BioRay who is selling basically the modern version of snake oil. Look at the list of products they sell. They are a company that is clearly trying to prey on peoples fears and concerns. Parents of autistic children, people who are worried about fillings, people who think eating silver is a good idea, etc. I mean a product called "Loving Energy" that contains 18% alcohol that they are suggesting giving to children "regularly"... WTF?

The letters that were published as critical responses in Science are very poor, of that there is no doubt and drafting a response is a good idea. On the other hand I think one should also turn a critical eye towards what WPI are doing. In effect they are lying in their response. WPI says that " At no time have we wished to raise false hopes among a group of patients who, in general, have not been treated well by the medical research community." This is simply an untrue statement. The WPI are all over the place inferring that XMRV = CFS and now are suggesting that XMRV might equal autism and lyme disease. We all including me really hope that in fact they have identified the cause but in the meantime we need to make sure that we also hold them to some sort of standard.

If the WPI is out representing CFS patients is everyone happy with them inferring XMRV = Autism and working with snake oil salesman? I think it is worth a series of tough questions to them before everyone starts to throw their time and effort into helping them.
 
G

Gerwyn

Guest
Summary

I thought the following points would be useful

Wesselly and co have no knowledge of virology or epidemiology.

They are not qualified to comment on technical matters in any way

They view ME ,cfs classified by the World Health organisation as a neurological disease as entirely psychological.

They diagnose people according to their own home made criteria and think they know better than the World Health Organisation.

They clearly appear to hold erroneous beliefs about the cause of ME,cfs and the level of their own expertise.

Sudlow is an epidemiologist who thinks that people who have AIDS are poorly and that fact makes them more susceptible to infection by the HIV virus.

What she actually said is that people with CFS are so unwell that they are more susceptible to XMRV infection.I,ve applied that line of reasoning to people labelled as having AIDS just to expose the flaws in the reasoning!

As to our Friends from the netherlands. They thought they could find high levels of XMRV in patients with fatigue caused entirely by psychological factors in 20 year old blood.

Their study failed the peer review process of the lancet and according to Godleewould not have passed the peer review process of the BMJ either.

It was published because the BMJ controllers were so concerned about us.

The cohort used is now under official investigation.

They also failed to notify the BMJ that samples that they had found negative had tested positive elsewhere.

They are hardly in a position to talk about technical matters,cohort selection,ethics or anything else even remotely connected with the scientific method

Finally we have the study by Lombardi et al which passed the most ardous peer review system in the world.

This study was described by John coffin to be "as good as it gets" and found XMRV using 4 different methods.
I am astonished that Dr Vernon when faced with the failed European efforts directed her fire towards the Science study rather than towards the obvious flaws in the European work latterly described by John Coffin as "thin".

I really cant understand why an advocate would do that when her queries could have been addressed by a couple of simple e mails. If someone can explain it please let me know
 
G

Gerwyn

Guest
Look... I hate to say this as it is going to get me flamed I am sure but if you stand back there are starting to be some real warning signs from WPI.

They in effect own VipDX who are making money selling XMRV tests. Judy is now running all over the place linking XMRV with other diseases (Autism, Lyme Disease) with no published research backing it up. The fact that they are finding XMRV all over the place and no one else ever has at some point has to start to raise some red flags.

They are now associated with BioRay who is selling basically the modern version of snake oil. Look at the list of products they sell. They are a company that is clearly trying to prey on peoples fears and concerns. Parents of autistic children, people who are worried about fillings, people who think eating silver is a good idea, etc. I mean a product called "Loving Energy" that contains 18% alcohol that they are suggesting giving to children "regularly"... WTF?

The letters that were published as critical responses in Science are very poor, of that there is no doubt and drafting a response is a good idea. On the other hand I think one should also turn a critical eye towards what WPI are doing. In effect they are lying in their response. WPI says that " At no time have we wished to raise false hopes among a group of patients who, in general, have not been treated well by the medical research community." This is simply an untrue statement. The WPI are all over the place inferring that XMRV = CFS and now are suggesting that XMRV might equal autism and lyme disease. We all including me really hope that in fact they have identified the cause but in the meantime we need to make sure that we also hold them to some sort of standard.

If the WPI is out representing CFS patients is everyone happy with them inferring XMRV = Autism and working with snake oil salesman? I think it is worth a series of tough questions to them before everyone starts to throw their time and effort into helping them.

The only snake oil salespeople I,m aware of are certain psychiatrists and members of the BS forum.In fact you could say that members of the BS forum are purveyors of BS.The first word is Bull I will leave the other word to the readers imagination bearing in mind that the word starts with s followed by H and ending in T
 

flybro

Senior Member
Messages
706
Location
pluto
Functional Symptoms = Psychiatric, for anyone who hasn't come across this term before

and an early hysterectomy is considered a functional symptom,

the info was in a PDf to help neurologists diagnos functional neurologic symptoms.

it appears as the wider patient community start to get to grips with the linguistic mechanisms of diagnosi, the 'THEY' start a new ELITE dictionary.

I really don't see how this much mud got in the water by accident.


Sorry..in ramble blah mode
 

Otis

Señor Mumbler
Messages
1,117
Location
USA
The only snake oil salespeople I,m aware of are certain psychiatrists and members of the BS forum.In fact you could say that members of the BS forum are purveyors of BS.The first word is Bull I will leave the other word to the readers imagination bearing in mind that the word starts with s followed by H and ending in T

Yes, I'd like to buy a vowel please. :D;):D;)
 

dannybex

Senior Member
Messages
3,561
Location
Seattle
Dedra Buchwald is head of the CFS Clinic here in Seattle at Harborview hospital. Whenever we've had a newcomer to our support group ask about the clinic, eyes roll in unison. It's a monumental joke, where one fills out reems of paperwork, then waits six months for their scheduled appointment, where they then run a few standard blood samples and then tell you to go home and rest.

Dedra, if you ever read this, you should know that no one in the community has any respect for you whatsover, and your 'clinic' is a joke. It's also a monumental insult to thousands of patients desperately looking for help.

Now I better go and rest.
 
R

Robin

Guest
Look... I hate to say this as it is going to get me flamed I am sure but if you stand back there are starting to be some real warning signs from WPI.

They in effect own VipDX who are making money selling XMRV tests. Judy is now running all over the place linking XMRV with other diseases (Autism, Lyme Disease) with no published research backing it up. The fact that they are finding XMRV all over the place and no one else ever has at some point has to start to raise some red flags.

They are now associated with BioRay who is selling basically the modern version of snake oil. Look at the list of products they sell. They are a company that is clearly trying to prey on peoples fears and concerns. Parents of autistic children, people who are worried about fillings, people who think eating silver is a good idea, etc. I mean a product called "Loving Energy" that contains 18% alcohol that they are suggesting giving to children "regularly"... WTF?

<<snip>>

If the WPI is out representing CFS patients is everyone happy with them inferring XMRV = Autism and working with snake oil salesman? I think it is worth a series of tough questions to them before everyone starts to throw their time and effort into helping them.

The association of CFS with XMRV is currently being studied by the HHS group; the results of the WPI Science study will either be verified or not verified. That is sufficient for me. It deserves more than a cursory glance that was given by the European studies or snarky sideline analysis written on various blogs.

I think they're looking into other illnesses which have either related symptoms or unknown causes. Whether you like it or not, according to the CDC the rise in autism may be due to more than just increased awareness and diagnosis. Some infections that occur during pregnancy can cause neurological damage in developing fetus: CMV infection can cause congenital disease and it's speculated that influenza can cause shizophrenia. If someone has a hypothesis through observation that autism and CFS are in the same families, why not investigate if perhaps an XMRV infection in utero could cause a child on autism spectrum? Does an autism association automatically make something suspect?

As far as VIPdx, the money from the tests goes back into research at the WPI. It's hardly a fortune they're making compared to the cost of the research they're doing. Do you know how little funding goes into CFS research? We get like $3 per person. We get funded less than erectile dysfunction (and yet cost the government and the economy far far far more.) The WPI works on a shoestring -- I hardly think selling test kits is a huge ethical violation.

I don't know about the bioray stuff, would you care to link to it? Are they receiving money from bioray? Endorsing their products? Please, share.
 

Impish

Senior Member
Messages
101
Location
Victoria, BC
The only snake oil salespeople I,m aware of are certain psychiatrists and members of the BS forum.In fact you could say that members of the BS forum are purveyors of BS.The first word is Bull I will leave the other word to the readers imagination bearing in mind that the word starts with s followed by H and ending in T

What are you talking about? Here is the link to the press release from VipDX which is owned by the Whittmores http://www.vipdx.com/press/. They are working with BioRay. Here is a link to BioRay's web site. http://www.bioraynaturaldetox.com

They have one product that contains 18% alcohol that they suggest for kids. They have another one with recommended dosing levels for kids under 1 year old that contains silver as well as wormwood. Wormwood is the active ingredent in absinthe. Whether or not is actually causes one to see green fairies is up for debate but again not something I would be giving my children.

Selling unproven herbal formulas to vulnerable people looking for a cure for something is the very definition of a snake oil salesmen.

I agree with everything Robin said but in the meantime, assuming that WPI is right and not scamming us, they are doing HUGE damage to their credibility by associating themselves with such people. Since they are acting as the face of CFS (or trying to) and getting us to rally to their cause they ABSOLUTELY need to act in an ethical and responsible manner. Associating with BioRay is not how to do this. The more I think about it the more angry I get.

I would love it if someone who is in direct contact with them here would ask them that the heck they are thinking doing this?
 

Lesley

Senior Member
Messages
188
Location
Southeastern US
Impish,

I don't have the time or energy to respond to this in detail, so I'll just make a few points:

1. The products with alcohol as a preservative are dosed in DROPS. The entire 2 oz bottle contains about 1/3 oz of alcohol. The bottle will last for many weeks. Using a form of alcohol as a preservative is common in homeopathics.

2. The Whittemores' stock in VIP Dx is in trust. They have no way to gain financially from VIP Dx.

3. WPI needs funds to continue research. A preliminary connection to autism has been found. The autism community is probably a much richer source of contributions than the CFS community. I'm guessing that the talks Dr. M is giving are intended to generate funds for more thorough research.

4. The Science paper included authors from the Cleveland Clinic and the National Cancer Institute, and was subject to rigorous peer review. Are CC, NCI, and the Science editors also scamming us?