Glycon
World's Most Dangerous Hand Puppet
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ME/CFS ≠ CFS/ME, @AndyPR . Surely you know that! 
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Why arepsychiatristsresearchers who promote a failed behavioural model of the disease involved?
The MEGA consortium has brought together many experts from a wide range of different disciplines from across genetics, genomics, metabolomics, pain research, proteomics,psychiatry,sleep research and transcriptomics.Psychiatry needs to be there to complete the big picture yet it is just one minor aspect.We had originally included psychiatry, as a courtesy because of the naive view held by some that they're doing their best to help patients (even if they fail miserably at it and have a long history of produce low-grade research and ignoring patients). However, after listening to patients, we accept there is no actual good evidence that there is a psychiatric element to the disease and we agree that their research is junk, patients do not consider them experts in anything but spin, and they would bring nothing to the MEGA table. Therefore, following discussions, certain relevant individuals have decided to remove themselves from the project. We wish them the best. MEGA will always be a Big Data ‘omics study, and is committed to delivering the high quality research of the sort patients have waited decades for. In order to achieve hat aim we recognise the importance of working in genuine partnership with patients, and not associating ourselves with those who do not work in patients' best interests.will never be a psychiatric study.
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I think this is a step change in the UK.MEGA Q&A said:setting up the world’s largest Bioresource of data and samples from CFS/ME patients.
Will the data be open access?
Yes. Subject to individuals’ consent, the data and the samples will be available for researchers to use. We want to rapidly increase effective research (by us, by anyone) to understand the biology, causes and different types of CFS/ME.
It would be unethical, if not illegal, to share data without consent, especially when it includes things like DNA profiles which are very personal. I would consent to having my data shared, but I'd want the choice.They say each patient will have to consent for data release and then data will only be released to 'researchers'.
How is this going to link in with the UK Biobank started at the London School of Tropical Medicine?
Charles Shepherd or the Prof will know more re this, sorry don't seem to be able to get the right tags.
To do the genetic studies that we want to do, we think we need to recruit at least 10 thousand adults and 2 thousand children. The only way to do this is to recruit patients through NHS clinics throughout England. England is the only place in the world that can collect this large number of patients in a short time frame.
Patients with CFS/ME will be identified by clinicians in the NHS clinics. The clinicians will be asked to identify patients they judge from NICE criteria to have CFS/ME. This means patients with other causes of fatigue will not be recruited including (for example): those with thyroid disease, diabetes or depression that is sufficiently severe to explain their fatigue. Patients will have been examined, a full history taken and they will have had screening blood tests (to ensure other causes of fatigue have been excluded).
We will collect sufficient information on each patient to be able to say whether they have CFS/ME using other research diagnoses (for example, the CDC [Fukuda 1994] diagnostic criteria, the IACFS criteria, Canadian criteria and so on). This is in addition to the diagnoses of CFS/ME that patients will get following NICE guidance. We will listen to our patient advisory group in terms of how much data we can collect on different diagnostic criteria. Our patients advisory groups may recommend collecting less data as patients are so ill.
I am not suggesting that they do anything illegal to satisfy my desire for freedom of data. It, in the main, is the vagueness of the words that they use here. Why can they not just say that every patient involved would have to agree to data sharing at sign up? It may be what they intend to say but it's not what they actually say.It would be unethical, if not illegal, to share data without consent, especially when it includes things like DNA profiles which are very personal. I would consent to having my data shared, but I'd want the choice.
Fantastic point!Doesn't it strike them as odd that they are using NICE diagnostic criteria for a biomedical research study into a disease that NICE considers treatable with psychological interventions ?
From the link:
"Petition update
MEGA Questions and Answers
M.E./CFS Epidemiology and Genomics Alliance (MEGA)
United Kingdom
Oct 5, 2016 — Many of you have asked us questions about MEGA. We have not yet applied for funding and the patient advisory groups have not yet met to provide advice. So these are our preliminary thoughts at the moment. Some of this will change as we work on the first application (see below) and during consultations prior to future applications. We want to engage with as many people as possible especially in the current planning phase."
https://www.change.org/p/support-th...k&utm_source=petition_update&utm_medium=email
I think the norm is not to make data sharing mandatory, but to give every patient an opt out. I'd be unhappy if patients had to agree to open data to be accepted (while I'd hope they'd all agree) - ultimately I think this has to be patient choice. And AFAIK, MEGA are not proposing anything unusual here.Why can they not just say that every patient involved would have to agree to data sharing at sign up? It may be what they intend to say but it's not what they actually say.
Because patients have rights: the right to share and the right not to share (I hope they all will) but of course the data can still be used by the main MEGA omics study. I don't know what opt-out figures are but suspect it's pretty low.Why would they bother to take samples from someone who did not consent to data being shared? Why go to the cost of taking samples and analysing them?
I didn't say their definition was vague - the were clear on what a researcher was, but only wanted to share with friendly ones. The MEGA statement commits them to sharing with any researcher.As you acknowledge, the PACE definition of researcher was extremely limited. So who will count as a researcher and who wont for this study?
With data freely available to any researcher we wouldn't have had to wait so long, and Alem would not have had to go to such ridiculous lengths, to get the data. The recovery paper came out in 2013 and was criticised immediately - imagine the difference if any researcher could have accessed the data and done the analysis according to protocol straight after the recovery paper came out.As we know that the only way we have got to the truth with PACE is by having a patient relentlessly pursue the data
Doesn't it strike them as odd that they are using NICE diagnostic criteria for a biomedical research study into a disease that NICE considers treatable with psychological interventions ?
Its doesn't specifically say that though. ?The MEGA statement commits them to sharing with any researcher.
As MEGA are now talking about a biorepository,, which sounds a lot like a biobank to me, I'd hope the would consult with the UK mecfs biobank on how to go about this. But the mecfs biobank, like MEGA, draws from NHS clinics (I didnt spot anyone complaining about that, but maybe I missed it) and MEGA will define patients according to multiple criteria. All biobank samples meet Fukuda and most meet Canadian; for MEGA all will meet NICE (I'm not sure which is 'better' between Fukuda and NICE, neither are ideal in my book) and will also diagnose according to other criteria..My understanding, and I could be wrong, is that the London School of Tropical Med biobank contains both patients who meet CCC and Fukuda patients who do not meet CCC. But they use different names for the two groups so you can tell which is which. This is important because its separating the two groups right up front based on hallmarks like PEM. Maybe someone else who is more familiar with that effort can provide more information on what they do.
Worth mentioning that the uk biobank selected on Fukuda, but most of those still met Canadian. I think Lenny Jason has done a similar study finding the same. So I don't think there's any good evidence that using looser criteria (Fukuda or NICE) will exclude patients with a tighter criteria such as Canadian.I appreciate the value of a large cohort but a cohort of what? I am struggling to see how a big cohort will compensate for poorly characterized and selected patient cohorts. This sounds like it is essentially a cohort of medically unexplained fatigue.
Yes, we need more detail. Eg willl they use Lenny Jason's DePaul symptom questionnaire to diagnose Canadian, as several groups do. The biobank used its own unpublished questionnaire to categorise patients as meeting Canadian criteria (that's not ideal either - but then many of the issues raised about MEGA apply to many other studies).My understanding, and I could be wrong, is that the London School of Tropical Med biobank contains both patients who meet CCC and Fukuda patients who do not meet CCC. But they use different names for the two groups so you can tell which is which. This is important because its separating the two groups right up front based on hallmarks like PEM. Maybe someone else who is more familiar with that effort can provide more information on what they do.
As AndyPR posted, the response said
It sounds like the approach taken in PACE - first select with an overly broad definition and then characterize with other definitions. But as David Tuller said in his 2015 article about PACE:
Bruce Levin, the Columbia University biostatistician, said the PACE investigators should not have assumed that the experience of a subgroup within an already defined population would match the experience of a group that hadn’t been pre-screened. “I would not accept an extrapolation to people diagnosed with alternative criteria from a subgroup comprising people satisfying both sets of criteria rather than just the alternative set of criteria,” he said, adding that reviewers should catch such questionable assumptions before publication.Maybe I am wrong but it sounds like they are stepping into the same problem again.
I appreciate the value of a large cohort but a cohort of what? I am struggling to see how a big cohort will compensate for poorly characterized and selected patient cohorts. This sounds like it is essentially a cohort of medically unexplained fatigue. Will the man-made heterogeneity of such a cohort confound interpretation even with the big-data, genomics approach being taken?
Leaving aside the problem that Levin notes for the moment I'd want to know:
I'd like to see the group comment on the issue that Levin raised and also explicitly explain their methods for symptom characterization and patient selection and how they compare to those of e.g. the London School of Tropical Medicine, Naviaux, Davis, the Australians, and any number of other groups doing successful research on ME using ME definitions.
- what specific definitions and how they are being applied including what inclusion and what exclusion criteria. PACE claimed to characterize patients according to Fukuda but they only required symptoms to be present for 1 week and even their own publications acknowledged that that change could have resulted in diagnostic inaccuracy. Will they apply e.g. CCC's exclusion of all mental illness?
- What specific tools and methods they are using to qualify patients as having the hallmark criteria of ME, particularly PEM. Jason's written lots on the problems with identifying these symptoms depending on how the questions are asked and whether a certain level of severity and frequency is required
Reads that way to me:Its doesn't specifically say that though. ?
MEGA said:Will the data be open access?
Yes. Subject to individuals’ consent, the data and the samples will be available for researchers to use. We want to rapidly increase effective research (by us, by anyone) to understand the biology, causes and different types of CFS/ME.
Reads that way to me:
Because patients have rights: the right to share and the right not to share (I hope they all will) but of course the data can still be used by the main MEGA omics study. I don't know what opt-out figures are but suspect it's pretty low.