1. Sign our petition calling on Cochrane to withdraw their review of Exercise Therapy for CFS here.
    Dismiss Notice
  2. Guest, the 'News in Brief' for the week beginning 18th March 2024 is here.
    Dismiss Notice
  3. Welcome! To read the Core Purpose and Values of our forum, click here.
    Dismiss Notice

USA: National Institutes of Health (NIH) intramural ME/CFS study

Discussion in 'ME/CFS research news' started by Simon M, Mar 15, 2018.

Thread Status:
Not open for further replies.
  1. adambeyoncelowe

    adambeyoncelowe Senior Member (Voting Rights)

    Messages:
    2,731
    Yes. NICE has flagged '40% misdiagnosis' from one UK study.
     
    MSEsperanza, Binkie4, ukxmrv and 10 others like this.
  2. Sid

    Sid Senior Member (Voting Rights)

    Messages:
    1,051
    That (entirely bogus in my view) claim comes from a crappy study by Newton which classified someone as misdiagnosed with ME/CFS if the person was found to have a sleep disorder, POTS, nutritional deficiency, depression/anxiety and such common ME/CFS comorbidities. None of those things explain ME/CFS symptoms and treating them in most cases makes little difference to core ME/CFS symptoms.

    I remember the huge media blitz in the UK newspapers a few years ago when she claimed a third of ME/CFS patients actually have POTS. Apparently it has never occurred to her that POTS is just another symptom for these people and that jacking up their BP or suppressing heart rate with meds does not cure them.

    The sleep stuff is just a money racket for sleep doctors. I can't tell you how many times they tried to get me to have a useless 'sleep study' (pay out of pocket of course) and how many other patients with ME/CFS I know who went along with it and treated their 'sleep disorder' and found that they are still disabled by ME/CFS.

    Same goes for nutritional deficiencies... can't tell you how many times a doctor will confidently assert that because they found iron deficiency or low B12 status this explains your symptoms. Naturally it doesn't but it sounds so similar on paper, right? "Tiredness", exhaustion, weakness etc.

    Same with psych comorbidities. I don't know of a single person who cured their ME with antidepressants or benzos.
     
  3. adambeyoncelowe

    adambeyoncelowe Senior Member (Voting Rights)

    Messages:
    2,731
    That may well be true too. That's the main study I remember because it was in the scoping responses especially (and this info is in the public domain so I can discuss it), but I know that other studies looking at misdiagnosis have been considered too.
     
  4. Forbin

    Forbin Senior Member (Voting Rights)

    Messages:
    1,581
    Location:
    USA
    Dr. Nath understandably does not want to discuss any findings yet. My impression is that they don't even want to analyze the data at this stage. Still, I'd love to ask him, "So, given what you've seen so far, what do you think of the deconditioning hypothesis?"
     
    feeb, Webdog, DokaGirl and 5 others like this.
  5. wigglethemouse

    wigglethemouse Senior Member (Voting Rights)

    Messages:
    954
    I think a lot of tests are subject to processing variables - Cytokines are one that come to mind immediately that can vary a lot. So good study design involves minimizing variables and as such perhaps they will process all samples together in one batch.
     
    andypants, Milo, Hutan and 1 other person like this.
  6. Ravn

    Ravn Senior Member (Voting Rights)

    Messages:
    2,042
    Location:
    Aotearoa New Zealand
    There was also an Australian study that looked at how many doctor-diagnosed patients met either Fukuda or ICC. And the results were impressive for all the wrong reasons.
    https://meaustralia.net/2016/05/26/australia-2-in-5-cfsme-diagnoses-wrong/

    Clearly misdiagnosis is a major problem.

    However, I think the most likely explanation for all the other conditions found in the Nath study is that the patients in question had both a correct ME diagnosis plus something else. And they're excluding all those with something else to get the cleanest data they can.
     
  7. Milo

    Milo Senior Member (Voting Rights)

    Messages:
    2,107
    Perhaps yes, and perhaps no. I am unsure whether these patients were excluded from the study (I would assume they were, considering the low number of patients that were admitted.

    We are missing large pieces of the puzzle. We are heterogenous. We are stigmatized and neglected. Patients give up seeing a doctor all together and veer on to treating themselves instead.

    There are so many things we do not understand about ME quite yet. We have been in this ‘perfect storm’ for decades now, hidden in plain sight.
     
    WillowJ, Ravn, Snowdrop and 7 others like this.
  8. DokaGirl

    DokaGirl Senior Member (Voting Rights)

    Messages:
    3,664
    Thank you to Dr. Nath for recognizing and stating pwME he has seen are devastated. He has not spent his career studying this illness. And yet it seems some mental health workers who have had a career focus in this area question whether ME is disabling. (As per deleted tweet noted in another thread.)
     
    andypants, WillowJ, Ravn and 3 others like this.
  9. DokaGirl

    DokaGirl Senior Member (Voting Rights)

    Messages:
    3,664
    Could someone tell me if the initial diagnosis for these patients, that which was given to them originally, before any contact with NIH, was provided by a ME specialist? I looked at the NIH requirements for participant entry in the study, and did not find this as a prerequisite - that participants' ME must first be confirmed by a ME specialist.

    My understanding is these people were more likely first diagnosed by their GPs. Which then explains the almost 30 percent misdiagnosis rate.

    Thank you.

    ETA: for punctuation
     
    Last edited: Mar 28, 2019
    andypants, Amw66 and Hutan like this.
  10. Snow Leopard

    Snow Leopard Senior Member (Voting Rights)

    Messages:
    3,819
    Location:
    Australia
    I think that is the most likely scenario - selection bias... Chronic fatigue is a common long term consequence of certain autoimmune diseases, even once the primary symptoms are attenuated/improve.
     
    andypants likes this.
  11. ME/CFS Skeptic

    ME/CFS Skeptic Senior Member (Voting Rights)

    Messages:
    3,494
    Location:
    Belgium
    As far as I know, these studies like the one by Newton et al. looked at the diagnosis of patients who were referred to a ME/CFS centre. So the patients were suspected to have ME/CFS, probably by their GP, but turned out to have other conditions after examination by a ME/CFS specialist. Many of these were straightforward conditions such as sleep- or psychiatric conditions that were not excluded, as the Fukuda criteria prescribe. In other words: the misdiagnosis in these studies seems to be a fault of GP's who fail to consider all the exclusions, all the other diseases that can cause similar symptoms as ME/CFS, not a critique of diagnostic criteria.
     
  12. Milo

    Milo Senior Member (Voting Rights)

    Messages:
    2,107
    I agree with what you say Michiel, and i will add that there are guidelines once the patient has been diagnosed with ME/CFS to only do minimal work up and sleep study is not recommended. They will only do the regular blood work, CBC, liver, kidney, Hepatitis and HIV screen, CRP and a few more to rule out according to the symptomatology. ME and CFS are dead end diseases. The main message is “You have arrived to your destination, stop looking”
     
  13. FMMM1

    FMMM1 Senior Member (Voting Rights)

    Messages:
    2,595
    ME is a convenient disease i.e. if your patient has unexplained fatigue then they have ME. I wonder if autoimmune disease is a similarly convenient diagnosis e.g. you may not even need to have an identified autoimmune antibody to be classified as having an autoimmune disease. An added complication is that Phair's metabolic trap predicts low Kynurenine which predisposes you to autoimmune diseases. Your high titre for autoimmune disease X could potentially due to the fact that your intracellular Kynurenine is low.

    I wonder if methods like Mass Spectrometry could be applied to these "autoimmune diseases". E.g. NMDAR encephalitis has an autoimmune form (the autoantibody has been identified and patients respond to immuno-suppressants) and a non-autoimmune form. If you analysed enough cases of the autoimmune form then you may find a reliable biomarker/diagnostic test.

    I'm suspicious of these "autoimmune diseases". Thankfully we have folks like Ron Davis working on this i.e. people with a vested interest in understanding and treating ME.
     
    ScottTriGuy likes this.
  14. Trish

    Trish Moderator Staff Member

    Messages:
    51,871
    Location:
    UK
  15. B_V

    B_V Established Member (Voting Rights)

    Messages:
    87
    I was one of the six patients the NIH team excluded from the data analysis. My second diagnosis, made by the NIH team, is 'atypical myositis.' I have probably had the myositis for as long or even longer than the ME (which started suddenly in 2012). I had a droopy right eyelid pointed out to me by an eye doctor about six months earlier than the ME, and that can be an early sign of some types of myositis.

    I had been thoroughly evaluated by neurologists before getting an ME/CFS diagnosis by Susan Levine and Derek Enlander, and had several EMGs (electromyograms - used to diagnose muscle disorders). EMGs are usually - but not always - abnormal in myositis. The reason everyone else missed the myositis is because, a) My EMG's were read as normal, and b) whatever type of myositis I have does not neatly fit into current categories. It was diagnosed only after muscle biopsies were performed at Stanford and NIH. No one ordered a muscle biopsy earlier, because the EMGs were negative. Neurologists are not going to order expensive surgeries (that's what a muscle biopsy is) without supporting evidence.

    I do have both disorders. I definitely qualify as having ME/CFS under the most stringent criteria, as determined by the five-person expert adjudication committee adjourned by NIH. I also have some sort of myositis.

    Edit: Of course I do wonder if an astute neurologist might have suspected I had a muscle disorder in the absence of the ME/CFS symptoms and made a diagnosis much earlier. But I'll never have an answer.
     
    Last edited: Apr 29, 2019
    Sid, lunarainbows, Estherbot and 24 others like this.
  16. wingate

    wingate Senior Member (Voting Rights)

    Messages:
    135
    Thanks for sharing, @B_V . Very interesting.
     
    MSEsperanza, WillowJ, Binkie4 and 4 others like this.
  17. Sly Saint

    Sly Saint Senior Member (Voting Rights)

    Messages:
    9,574
    Location:
    UK
    Hutan, rvallee, Nellie and 2 others like this.
  18. Sanna

    Sanna Established Member

    Messages:
    8
    I am pretty sure Dr. Walitt goes over all of these numbers, including how many did not respond after being invited, in his talk at the ME/CFS conference at the NIH in April 2019. If someone was interested in those exact numbers, you could look up the video recording and Dr. Walitt's talk.
     
    Andy likes this.
  19. Sanna

    Sanna Established Member

    Messages:
    8
    The NIH is many people and many groups. I don't think we can lump them all together saying "they" want to or don't want to help. From my experience as a patient in this study, I felt that the people involved in the study that I met definitely wanted to move us forward and be as helpful as possible, but proper research requires certain steps and certain sequences to be followed, so it will not be as fast as most of us wish for.
     
    Last edited: Sep 14, 2019
  20. Sanna

    Sanna Established Member

    Messages:
    8
    This is only the first step. From my conversations while participating in the study as a patient, as long as they find useful data, they would try to study other sub-groups later on, such as more severe patients, etc.
     
    Amw66, Binkie4, Andy and 5 others like this.
Thread Status:
Not open for further replies.

Share This Page