A comparison of cytokine profiles of CFS/ME and MS patients

Posted on 11/16/2015 by wames

Research abstract:

Background: Chronic Fatigue Syndrome, also known as Myalgic Encephalomyelitis (CFS/ME), is a debilitating condition that presents with a range of symptoms, including fatigue, cognitive dysfunction, muscular and joint pain, and may be immune-mediated. In particular, patients exhibit abnormal cytokine expression.

Similarly, in Multiple Sclerosis (MS), patients display neuroimmunological symptoms, and abnormal cytokine expression, with some overlap in symptomology with CFS/ME. The purpose of this study was to compare Th1, Th2, Th17 cytokines, inflammatory cytokines and chemokines, in healthy controls, CFS/ME and MS patients.

Methods: Serum samples were collected from healthy controls (n = 16, mean age = 50 ± 11.85 years), CFS/ME patients (n = 16, mean age = 49.88 ± 9.54 years) and MS patients (n = 11, mean age = 52.75 ± 12.81 years). The concentrations of 27 cytokines (IFN-γ, TNF-α, IL-12, IL-2, IL-1β, IL-4, IL-6, IL-10, IL-13, IL-5, IL-17, IL-1ra, IL-7, IL-8, IL-9, eotaxin, IP-10, MCP-1, MIP1α, MIP1β, PDGF-bb, RANTES, basic FGF, GCSF, GMCSF, VEGF and IL-15) were measured using a Bio-Plex Pro™ kit.

Results: IFN-γ, IL-10 and IL-5 were significantly higher in the serum of both CFS/ME and MS patients compared to the healthy controls (p ≤ 0.041). However, only the MS patients had significantly elevated levels of IL-12, IL-1β, IL-4, IL-13, IL-6, IL-17, IL-1ra, IL-7, IL-9, eotaxin, IL-10, MIP1α, basic FGF, GCSF and VEGF compared to the CFS/ME patients and controls (p ≤ 0.04). There were no significant differences between groups for IL-8, MCP-1, MIP1β, RANTES, GMCSF, TNF-α, and IL-2.

Conclusion: CFS/ME and MS patients both displayed abnormal cytokine levels, with dual expression of Th1 and Th2 cytokines. Further research into cytokines such as IFN-γ, IL-10 and IL-5, with the use of a specific CFS/ME case definition and sensitive cytokine assays, is required to improve the understanding of the pathophysiology of CFS/ME.

Conclusion to paper:
In conclusion, this study has reported expression of Th1 and Th2 cytokines in CFS/ME and MS patients. Elevated levels of IFN-γ, IL-10 and IL-5 were found in both CFS/ME and MS. In the MS cohort, the results were consistent with the majority of findings from previous studies, where general elevation of pro-inflammatory, some anti-inflammatory, Th1 and Th2 cytokines has been observed [102].

However, results for CFS/ME cytokine levels, including IFN-γ [37] [103], IL-10 [6] [10], IL-17 [8], and IL-12 [6] [8], conflicted with previous findings. This is likely due to the heterogeneity of CFS/ME [102]. Additionally the use of the ICC [1] as opposed to the more commonly used 1994 CDC definition [104], may have played a role in differential results.

A study comparing the results of cytokines across differing definitions could help resolve conflicting findings of previous studies. Additionally different subgroups of CFS/ME, based on symptomology and severity, may present with differing cytokine profiles, and this may be an area for future research.

A longitudinal study with multiple time points would be more suitable to assess cytokine profiles. Furthermore isolation of immune cells to determine specific cytokine secretion from different cell types may provide more detailed insight into CFS/ME pathophysiology.

Lastly CFS/ME patients are known to administer multiple medications, which may affect cytokine secretion. Analysis of these interactions and effects could be an important area for further research.

A comparison of Cytokine profiles of Chronic Fatigue Syndrome/Myalgic Encephalomyelitis and Multiple Sclerosis patients, by N Wong, T Nguyen, E Brenu, S Broadley, D Staines and S Marshall-Gradisnik in International Journal of Clinical Medicine vol 6, pp 769-783.

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Psychological factors associated with sleep disturbance in CFS & insomnia

Posted on 11/13/2015 by wames

Research abstract:

Objectives:
Reports of tiredness and poor quality sleep are common to both Chronic Fatigue Syndrome (CFS) and insomnia, despite evidence that sleep structure is not objectively impaired in these groups. Similar vulnerability and maintenance factors have been identified in both conditions, such as perfectionism, unhelpful beliefs and misattributions
about symptoms. The aim of this study was to compare CFS and insomnia groups in terms of subjective sleep and fatigue symptoms and associated cognitive factors.

Method:
Using a cross-sectional design, CFS patients (n=18), community insomnia participants (n=18) and healthy community controls (n=19) were compared on a range of self-report questionnaires, including measures of psychological wellbeing (depression, anxiety, worry), insomnia, sleepiness and fatigue severity, cognitions about sleep and fatigue, and
other cognitive variables associated with CFS and insomnia.

Results:
Between-group analyses identified that CFS and Insomnia participants did not differ significantly on the majority of variables. Compared to controls, both groups reported poorer psychological wellbeing and higher levels of insomnia, sleepiness, and sleep-related cognitions. Both groups also reported elevated perfectionism and unhelpful beliefs about
emotions. Compared to the Insomnia group, CFS participants reported higher levels of fatigue, fatigue-related cognitions, and pre-sleep somatic experiences.

Conclusions:
This study found similarities between CFS and insomnia participants in terms of cognitive processes known to maintain insomnia. This indicates that it may be appropriate to use a transdiagnostic cognitive-behavioural approach to treating sleep disturbance in CFS. The
results also indicate the importance of assessing for unhelpful fatigue-related beliefs and pre-sleep somatic complaints when working with the CFS population. Implications for further research are discussed.

Doctorate in Clinical Psychology: Main Research Portfolio:Psychological factors associated with self-reported sleep disturbance in Chronic Fatigue Syndrome and insomnia, by Wilson, F., 2015. Thesis (Doctoral) University of Bath

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Physiological post-exertional abnormalities in ME & CFS

Posted on 11/13/2015 by wames

Review article extracts:

Abstract: Post-exertional “malaise” is a hallmark symptom of Myalgic Encephalomyelitis (ME) and Chronic Fatigue Syndrome (CFS). Various abnormalities, including abnormal physiological responses to exertion, can account for post-exertional “malaise” and “exercise avoidance”. Since these abnormalities are not observed in sedentary healthy controls, the abnormalities and deviant responses cannot be explained by “exercise avoidance” and subsequent deconditioning, nor by  psychogenic factors.

Abnormalities relating to exercise and its effect:

  • Energetic abnormalities and reduced oxygen uptake amplified by exertion
  • Muscular abnormalities related to exercise
  • Long-lasting oxidative stress in response to exercise
  • Increased pain sensitivity and lower pain thresholds during and after exercise
  • Immunologic abnormalities in response to exertion
  • Cardiovascular dysfunction related to exertion and orthostasis
  • Autonomic abnormalities associated with exercise and orthostatic stress
  • Neurologic abnormalities in relation to physical and mental exertion

Conclusion: Post-exertional “malaise” and “exercise intolerance” are hallmark symptoms [80] of Myalgic Encephalomyelitis (ME) [1-3] and Chronic Fatigue Syndrome (CFS) [4].

This article reviews observations which support the position that post-exertional “malaise” in ME/CFS may be linked to a number of observable deviant physiological responses to exercise, including muscle weakness and myalgia, a substantial fall of oxygen uptake after exercise, an increase in metabolite-detecting (pain) receptors, increased acidosis, abnormal immune responses, and orthostatic intolerance.

Such findings go some way to explain why many ME/CFS sufferers either avoid exercise or report negative effects of exercised-based rehabilitation protocols, such as graded exercise therapy (GET). The physiological abnormalities induced by ME/CFS cannot be simply explained by a sedentary life style and deconditioning [81], or psychogenic factors
[82]. While we acknowledge the importance of physical activity in illness rehabilitation, our findings cast doubt on the efficacy of exercise protocols as a therapeutic approach.

More research into exercise-induced cellular and physiological abnormalities in ME/CFS is needed to better understanding the illness and its impact on patients, and to develop appropriate treatments.

Deviant Cellular and Physiological Responses to Exercise in Myalgic Encephalomyelitis and Chronic Fatigue Syndrome, by Frank N.M. Twisk, Keith J. Geraghty in Jacobs Journal of Physiology 11-07-2015

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Pattern-related visual stress found in ME/CFS

Posted on 11/13/2015 by wames

Research abstract:

The objective of this study was to determine vulnerability to pattern-related visual stress in Myalgic Encephalomyelitis/Chronic Fatigue Syndrome (ME/CFS).

A total of 20 ME/CFS patients and 20 matched (age, gender) controls were recruited to the study. Pattern-related visual stress was determined using the Pattern Glare Test. Participants viewed three patterns, the spatial frequencies (SF) of which were 0.3 (low-SF), 2.3 (mid-SF), and 9.4 (high-SF) cycles per degree (c/deg). They reported the number of distortions they experienced when viewing each pattern.

ME/CFS patients exhibited significantly higher pattern glare scores than controls for the mid-SF pattern. Mid-high SF differences were also significantly higher in patients than controls. These findings provide evidence of altered visual perception in ME/CFS.

Pattern-related visual stress may represent an identifiable clinical feature of ME/CFS that will prove useful in its diagnosis. However, further research is required to establish if these symptoms reflect ME/CFS-related changes in the functioning of sensory neural pathways.

Increased Vulnerability to Pattern-Related Visual Stress in Myalgic Encephalomyelitis by Rachel L. Wilson, Kevin B. Paterson, Claire V. Hutchinson in Perception November 3, 2015 [Published online before print]

 

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Body-mind therapies for IBS

Posted on 11/12/2015 by wames

Research abstract:

Irritable bowel syndrome (IBS) is one of the most commonly diagnosed gastrointestinal conditions. It represents a significant healthcare burden and remains a clinical challenge.

Over the years IBS has been described from a variety of different perspectives; from a strict illness of the gastrointestinal tract (medical model) to a more complex multi-symptomatic disorder of the brain-gut axis (biopsychosocial/psychosomatic model).

In this article we present aspects of the pathophysiology and the non-pharmacological treatment of IBS based on current knowledge. Effects of conditioned stress and/or traumatic influences on the emotional system (top-down) as well as effects on the intestine through stressors, infection, inflammation, food and dysbiosis (bottom-up) can affect brain-gut communication and result in dysregulation of the autonomic nervous system (ANS), playing an important role in the pathophysiology of IBS.

Conditioned stress together with dysregulation of the autonomic nervous system and the emotional system may involve reactions in which the distress inside the body is not recognized due to low body awareness. This may explain why patients have difficulty identifying their symptoms despite dysfunction in muscle tension, movement patterns, and posture and biochemical functions in addition to gastrointestinal symptoms.

IBS shares many features with other idiopathic conditions, such as fibromyalgia, chronic fatigue syndrome and somatoform disorders. The key to effective treatment is a thorough examination, including a gastroenterological examination to exclude other diseases along with an assessment of body awareness by a body-mind therapist.

The literature suggests that early interdisciplinary diagnostic co-operation between gastroenterologists and body-mind therapists is necessary. Re-establishing balance in the ANS is an important component of IBS treatment. This article discusses the current knowledge of body-mind treatment, addressing the topic from a practical point of view.

Core tip: Due to the complex nature of irritable bowel syndrome (IBS), no long-lasting generally accepted therapies are available. Different lines of research have been developed to address this issue. One line focuses on identifying intestinal mechanisms that may be affected by pharmacologic intervention. The understanding of IBS, especially the interactions between the central and enteric nervous systems, has grown considerably in recent years. Because recent research has focused more on the body-mind aspect of the disease, body-mind remedies such as hypnotherapy, psychotherapy and body awareness therapy have been applied. In highlighting this topic we discuss non-pharmacological methods and practical guidelines for the treatment of IBS.

Aspects of the non-pharmacological treatment of irritable bowel syndrome, by Elsa Maria Eriksson, Kristina Ingrid Andrén, Göran Karl Kurlberg, and Henry Ture Eriksson in
World J Gastroenterol. 2015 Oct 28; 21(40): 11439–11449.

Published online 2015 Oct 28.  doi:  10.3748/wjg.v21.i40.11439

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Uses of vagal nerve stimulation for chronic pain

Posted on 11/12/2015 by wames

Review abstract:

Recent human and animal studies provide growing evidence that vagal nerve stimulation (VNS) can deliver strong analgesic effects in addition to providing therapeutic efficacy in the treatment of refractory epilepsy and depression.

Analgesia is potentially mediated by vagal afferents that inhibit spinal nociceptive reflexes and transmission and have strong anti-inflammatory properties. The purpose of this review is to provide pain practitioners with an overview of VNS technology and limitations. It specifically focuses on clinical indications of VNS for various chronic pain syndromes, including fibromyalgia, pelvic pain, and headaches.

We also present potential mechanisms for VNS modulation of chronic pain by reviewing both animal and human studies.

Review of the Uses of Vagal Nerve Stimulation in Chronic Pain Management, by K Chakravarthy, H Chaudhry, K Williams, PJ Christo  in Curr Pain Headache Rep. 2015 Dec;19(12):54
KEYWORDS:

Chronic pain; Fibromyalgia; Headache; Inflammation; Pelvic pain; Vagal nerve stimulation

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It’s too good to be true that exercise can help CFS sufferers

Posted on 11/12/2015 by wames

In medicine, as in life, it is sensible to be cautious about claims that seem too good to be true. Daily Telegraph’s Doctor’s Diary: It’s too good to be true that exercise can help Chronic Fatigue Syndrome sufferers  [James Le Fanu,  9 Nov 2015]:

Back in 1999, software engineer Ollie Cornes contracted a throat infection that transmuted into a state of “unbelievable exhaustion, with an intense flu-like malaise”, leading to him eventually being diagnosed as having postviral fatigue syndrome.

Since then, the severity of his fatigue has waxed and waned, but is invariably exacerbated by doing more than his usual level of activity allows – leaving him “bedridden for weeks with muscle weakness, dizziness and loss of appetite”. This phenomenon of fatigue following minimal physical or mental exertion is a well recognised feature of many neurological disorders, affecting two thirds of those with multiple sclerosis and being almost universal in the Post Polio Syndrome (PPS) that afflicts the survivors of the polio epidemics of the 40s and 50s. The precise mechanism remains obscure, but is obviously related to disturbed functioning of the relevant parts of the brain.

First biological proof that ME is real found by scientists

By contrast, the mainstream medical explanation for those like Mr Cornes with post-viral fatigue – otherwise known as chronic fatigue syndrome, or, even more commonly, ME (myalgic encephalomyelitis) – is very different, being attributed to the “unhelpful belief they have some persistent medical condition” that is exacerbated on exertion. This results, it is claimed, in a “chronic fatigue state in which symptoms are perpetuated by a cycle of inactivity and deconditioning with further deterioration in exercise tolerance”.

Hence the proposal that breaking this cycle with a combination of cognitive behavioural therapy together with a regime of graded exercise should promote recovery. And, indeed, as reported in this paper last week, researchers at Oxford University who have evaluated this approach found that, two years later, “most” patients had benefitted feeling less tired and being able to complete most tasks more easily”.

The researchers may be persuaded by their optimistic conclusions, but Telegraph readers certainly are not, as is clear from the impressive number (more than 1,200) of highly critical comments posted online, drawing attention to, for example, the remarkable absence of any measurable criteria for assessing what “recovery” entailed. It is far too good to be true to suppose that positive thinking and graded exercise should reverse a debilitating illness that, as with Mr Cornes, can last for decades – and it would be good to think the sheer implausibility of asserting otherwise could be the last hurrah for the psychological explanation for post-viral fatigue.

Earlier this year, the Institute of Medicine in the United States, having reviewed all the medical evidence on chronic fatigue over the past 50 years, advised it be classified as a physical brain disorder, which in view of its “complexity and severity” should be redesignated Systemic Exertion Intolerance Disease, the better to reflect its defining feature: that “physical and cognitive exertion adversely affect these patients in many aspects of their lives”.

FACT BOX
Symptoms of Chronic Fatigue Syndrome

The main symptom of CFS is persistent physical and mental fatigue (exhaustion). This does not go away with sleep or rest and limits your usual activities.  Most people with CFS describe this fatigue as overwhelming, and a different type of tiredness from what they have experienced before.

Other symptoms include:

  • Muscular pain, joint pain and severe headaches
  • Poor short-term memory and concentration, and difficulty organising thoughts and finding the right words (‘brain fog’)
  • Painful lymph nodes (small glands of the immune system)
  • Stomach pain and other problems similar to irritable bowel syndrome, such as bloating, constipation, diarrhoea and nausea
  • Sore throat
  • Sleeping problems, such as insomnia and feeling that sleep is not refreshing
  • Sensitivity or intolerance to light, loud noise, alcohol and certain foods
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Why has the PACE Study’s “Sister Trial” been “Disappeared” and Forgotten?

Posted on 11/11/2015 by wames

David Tuller continues his analysis of research about treatments for CFS with an examination of the FINE trial.  A summary has been compiled by MEAction.

Virology blog: Trial By Error, Continued: Why has the PACE Study’s “Sister Trial”been “Disappeared” and Forgotten? [9 November 2015]:

In 2010, the BMJ published the results of the Fatigue Intervention by Nurses Evaluation, or FINE. The investigators for this companion trial to PACE, also funded by the Medical Research Council, reported no benefits to ME/CFS patients from the interventions tested.

In medical research, null findings often get ignored in favor or more exciting “positive” results. In this vein, the FINE trial seems to have vanished from the public discussion over the controversial findings from the PACE study. I thought it was important to re-focus some attention on this related effort to prove that “deconditioning” is the cause of the devastating symptoms of ME/CFS. (This piece is also too long but hopefully not quite as dense.)

An update on something else: I want to thank the public relations manager from Queen Mary University of London for clarifying his previous assertion that I did not seek comment from the PACE investigators before Virology Blog posted my story. In an e-mail, he explained that he did not mean to suggest that I hadn’t contacted them for interviews. He only meant, he wrote, that I hadn’t sent them my draft posts for comment before publication. He apologized for the misunderstanding.

I accept his apology, so that’s the end of the matter. In my return e-mail, however, I did let him know I was surprised at the expectation that I might have shared the draft with the PACE investigators before publication. I would not have done that whether or not they had granted me interviews. This is journalism, not peer-review. Different rules.

************************************************************************

In 2003, with much fanfare, the U.K. Medical Research Council announced that it would fund two major studies of non-pharmacological treatments for chronic fatigue syndrome. In addition to PACE, the agency decided to back a second, smaller study called “Fatigue Intervention by Nurses Evaluation,” or FINE. Because the PACE trial was targeting patients well enough to attend sessions at a medical clinic, the complementary FINE study was designed to test treatments for more severely ill patients.

(Chronic fatigue syndrome is also known as myalgic encephalomyelitis, CFS/ME, and ME/CFS, which has now been adopted by U.S. government agencies. The British investigators of FINE and PACE prefer to call it chronic fatigue syndrome, or sometimes CFS/ME.)

Alison Wearden, a psychologist at the University of Manchester, was the lead FINE investigator. She also sat on the PACE Trial Steering Committee and wrote an article about FINE for one of the PACE trial’s participant newsletters. The Medical Research Council and the PACE team referred to FINE as PACE’s “sister” trial. The two studies included the same two primary outcome measures, self-reported fatigue and physical function, and used the same scales to assess them.

The FINE results were published in BMJ in April, 2010. Yet when the first PACE results were published in The Lancet the following year, the investigators did not mention the FINE trial in the text. The trial has also been virtually ignored in the subsequent public debate over the results of the PACE trial and the effectiveness, or lack thereof, of the PACE approach.

What happened? Why has the FINE trial been “disappeared”?

*****

The main goal of the FINE trial was to test a treatment for homebound patients that adapted and combined elements of cognitive behavior therapy and graded exercise therapy, the two rehabilitative therapies being tested in PACE. The approach, called “pragmatic rehabilitation,” had been successfully tested in a small previous study. In FINE, the investigators planned to compare “pragmatic rehabilitation” with another intervention and with standard care from a general practitioner.

Here’s what the Medical Research Council wrote about the main intervention in an article in its newsletter, MRC Network, in the summer of 2003: “Pragmatic rehabilitation…is delivered by specially trained nurses, who give patients a detailed physiological explanation of symptom patterns. This is followed by a treatment programme focussing on graded exercise, sleep and relaxation.”

The second intervention arm featured a treatment called “supportive listening,” a patient-centered and non-directive counseling approach.  This treatment presumed that patients might improve if they felt that the therapist empathized with them, took their concerns seriously, and allowed them to find their own approach to addressing the illness.

The Medical Research Council committed 1.3 million pounds to the FINE trial. The study was conducted in northwest England, with 296 patients recruited from primary care. Each intervention took place over 18 weeks and consisted of ten sessions–five home visits lasting up to 90 minutes alternating with five telephone conversations of up to 30 minutes.

As in the PACE trial, patients were selected using the Oxford criteria for chronic fatigue syndrome, defined as the presence of six months of medically unexplained fatigue, with no other symptoms required. The Oxford criteria have been widely criticized for yielding heterogeneous samples, and a report commissioned by the National Institutes of Health this year recommended by the case definition be “retired” for that reason.

More specific case definitions for the illness require the presence of core symptoms like post-exertional malaise, cognitive problems and sleep disorders, rather than just fatigue per se. Because the symptom called post-exertional malaise means that patients can suffer severe relapses after minimal exertion, many patients and advocacy organizations consider increases in activity to be potentially dangerous.

To be eligible for the FINE trial, participants needed to score 70 or less out of 100 on the physical function scale, the Medical Outcomes Study 36-Item Short Form Health Survey, known as the SF-36. They also needed to score a 4 or more out of 11 on the 11-item Chalder Fatigue Scale, with each item scored as either 0 or 1. On the fatigue scale, a higher score indicated greater fatigue.

Among other measures, the trial also included a key objective outcome–the “time to take 20 steps, (or number of steps taken, if this is not achieved) and maximum heart rate reached on a step-test.”

Participants were to be assessed on these measures at 20 weeks, which as right after the end of the treatment period, and again at 70 weeks, which was one year after the end of treatment. According to the FINE trial protocol, published in the journal BMC Medicine in 2006, “short-term assessments of outcome in a chronic health condition such as CFS/ME can be misleading” and declared the 70-week assessment to be the “primary outcome point.”

*****

The theoretical model behind the FINE trial and pragmatic rehabilitation paralleled the PACE concept. The physical symptoms were presumed to be the result not of a pathological disease process but of “deconditioning” or “dysregulation” caused by sedentary behavior, accompanied by disrupted sleep cycles and stress. The sedentary behavior was itself presumed to be triggered by patients’ “unhelpful’  conviction that they suffered from a progressive medical illness.  Counteracting the deconditioning involved re-establishing normal sleep cycles, reducing anxiety levels and gently increasing physical exertion, even if patients remained homebound.

“The treatment [pragmatic rehabilitation] is based on a model proposing that CFS/ME is best understood as a consequence of physiological dysregulation associated with inactivity and disturbance of sleep and circadian rhythms,” stated the FINE trial protocol. “We have argued that these conditions…are often maintained by illness beliefs that lead to exercise-avoidance. The essential feature of the treatment is the provision of a detailed explanation for patients’  symptoms, couched in terms of the physiological dysregulation model, from which flows the rationale for a graded return to activity.”

On the FINE trial website, a 2004 presentation about pragmatic rehabilitation explained the illness in somewhat simpler terms, comparing it to “very severe jetlag.” After explaining how and why pragmatic rehabilitation led to physical improvement, the presentation offered this hopeful message, in boldface: “There is no disease–you have a right to full health. This is a good news diagnosis. Carefully built up exercise can reverse the condition. Go for 100% recovery.”

In contrast, patients, advcoates and many leading scientists have completely rejected the PACE and FINE approach. They believe the evidence overwhelmingly points to an immunological and neurological disorder triggered by an initial infection or some other physiological insult. Last month, the National Institutes of Health ratified this perspective when it announced a major new push to seek biomedical answers to the disease, which it refers to as ME/CFS.

As in PACE, patients in the FINE trial were issued different treatment manuals depending upon their assigned study arm. The treatment manual for pragmatic rehabilitation repeatedly informed participants that the therapy could help them get better—even though the trial itself was designed to test the effectiveness of the therapy. (In the PACE trial, the manuals for the cognitive behavior and graded therapy arms also included many statements promoting the idea that the therapies could successfully treat the illness.)

“This booklet has been written with the help of patients who have made a full recovery from Chronic Fatigue Syndrome,” stated the FINE pragmatic rehabilitation manual on its second page. “Facts and information which were important to them in making this recovery have been included.” The manual noted that the patients who helped write it had been treated at the Royal Liverpool University Hospital but did not include more specific details about their “full recovery” from the illness.

Among the “facts and information” included in the manual were assertions that the trial participants, contrary to what they might themselves believe, had no persistent viral infection and “no underlying serious disease.” The manual promised them that pragmatic rehabilitation could help them overcome the illness and the deconditioning perpetuating it. “Instead of CFS controlling you, you can start to regain control of your body and your life,” stated the manual.

Finally, as in PACE, participants were encouraged to change their beliefs about their condition by “building the right thoughts for your recovery.” Participants were warned that “unhelpful thoughts”—such as the idea that continued symptoms indicated the presence of an organic disease and could not be attributed to deconditioning—“can put you off parts of the treatment programme and so delay or prevent recovery.”

The supportive listening manual did not similarly promote the idea that “recovery” from the illness was possible. During the sessions, the manual explained, “The listener, your therapist, will provide support and encourage you to find ways to cope by using your own resources to change, manage or adapt to difficulties…She will not tell you what to do, advise, coach or direct you.”

*****

A qualitative study about the challenges of the FINE research process, published by the investigators in the journal Implementation Science in 2011, shed light on how much the theoretical framework and the treatment approaches frustrated and angered trial participants.

According to the interviews with some of the nurses, nurse supervisors, and participants involved in FINE, the home visits often bristled with tension over the different perceptions of what caused the illness and which interventions could help.

“At times, this lack of agreement over the nature of the condition and lack of acceptance as to the rationale behind the treatment led to conflict,” noted the FINE investigators in the qualitative paper. “A particularly difficult challenge of interacting with patients for the nurses and their supervisors was managing patients’ resistance to the treatment.”

One participant in the pragmatic rehabilitation arm, who apparently found it difficult to do what was apparently expected, attributed this resistance to the insistence that deconditioning caused the symptoms and that activity would reverse them. “If all that was standing between me and recovery was the reconditioning I could work it out and do it, but what I have got is not just a reconditioning problem,” the participant said. “I have got something where there is damage and a complete lack of strength actually getting into the muscles and you can’t work with what you haven’t got in terms of energy.”

Another participant in the pragmatic rehabilitation arm was more blunt. “I kept arguing with her [the nurse administering the treatment] all the time because I didn’t agree with what she said,”  said the participant, who ended up dropping out of the trial.

Some participants in the supportive listening arm also questioned the value of the treatment they were receiving, according to the study. “I mostly believe it was more physical than anything else, and I didn’t see how talking could truthfully, you know, if it was physical, do anything,” said one.

In fact, the theoretical orientation also alienated some prospective participants as well, according to interviews the investigators conducted with some patients who declined to enter the trial. ‘It [the PR intervention] insisted that physiologically there was nothing wrong,” said one such patient. “There was nothing wrong with my glands, there was nothing wrong, that it was just deconditioned muscles. And I didn’t believe that…I can’t get well with treatment you don’t believe in.”

When patients challenged or criticized the therapeutic interventions, the study found, nurses sometimes felt their authority and expertise to be under threat. “They are testing you all the time,” said one nurse. Another reported: “That anger…it’s very wearing and demoralizing.”

One nurse remembered the difficulties she faced with a particular participant. “I used to go there and she would totally block me, she would sit with her arms folded, total silence in the house,” said the nurse. “It was tortuous for both of us.”

At times, nurses themselves responded to these difficult interactions with bouts of anger directed at the participants, according to a supervisor.

“Their frustration has reached the point where they sort of boiled over,” said the supervisor. “There is sort of feeling that the patient should be grateful and follow your advice, and in actual fact, what happens is the patient is quite resistant and there is this thing like you know, ‘The bastards don’t want to get better.’”

*****

BMJ published the FINE results in 2010. The FINE investigators found no statistically significant benefits to either pragmatic rehabilitation or supportive listening at 70 weeks. Despite these null findings one year after the end of the 18-week course of treatment, the mean scores of those in the pragmatic rehabilitative arm demonstrated at 20 weeks a “clinically modest” but statistically significant reduction in fatigue—a drop of one point (plus a little) on the 11-point fatigue scale. The slight improvement still meant that participants were much more fatigued than the initial entry threshold for disability, and any benefits were no longer statistically significant by the final assessment.

Despite the null findings at 70 weeks, the authors put a positive gloss on the results, reporting first in the abstract that fatigue was “significantly improved” at 20 weeks. Given the very modest one-point change in average fatigue scores, perhaps the FINE investigators intended to report instead that there was a “statistically significant improvement” at 20 weeks—an accurate phrase with a somewhat different meaning.

The abstract included another interesting linguistic element. While the trial protocol had designated the 70-week assessment as “the primary outcome point,” the abstract of the paper itself now stated that “the primary clinical outcomes were fatigue and physical functioning at the end of treatment (20 weeks) and 70 weeks from recruitment.”

After redefining their primary outcome points to include the 20-week as well as the 70-week assessment, the abstract promoted the positive effects found at the earlier point as the study’s main finding. Only after communicating the initial benefits did they note that these advantages for pragmatic rehabilitation later wore off. The FINE paper cited no oversight committee approval for this expanded interpretation of the trial’s primary outcome points to include the 20-week assessment, nor did it mention the protocol’s caveat about the “misleading” nature of short-term assessments in chronic health conditions.

In fact, within the text of the paper, the investigators noted that the “pre-designated outcome point” was 70 weeks. But they did not explain why they then decided to highlight most in the abstract what was not the pre-designated but instead a post-hoc “primary” outcome point—the 20-week assessment.

A BMJ editorial that accompanied the FINE trial also accentuated the positive results at 20 weeks rather than the bad news at 70 weeks.
According to the editorial’s subhead, pragmatic rehabilitation “has a short term benefit, but supportive listening does not.” The editorial did not note that this was not the pre-designated primary outcome point. The null results for that outcome point—the 70-week assessment—were not mentioned until later in the editorial.

*****

Patients and advocates soon began criticizing the study in the “rapid response” section of the BMJ website, citing its theoretical framework, the use of the broad Oxford criteria as a case definition, and the failure to provide the step-test outcomes, among other issues.

“The data provide strong evidence that the anxiety and deconditioning model of CFS/ME on which the trial is predicated is either wrong or, at best, incomplete,” wrote one patient. “These results are immensely important because they demonstrate that if a cure for CFS/ME is to be found, one must look beyond the psycho-behavioural paradigm.”

Another patient wrote that the study was “a wake-up call to the whole of the medical establishment” to take the illness seriously. One predicted “that there will those who say that the this trial failed because the patients were not trying hard enough.”

A physician from Australia sought to defend the interests not of patients but of the English language, decrying the lack of hyphens in the paper’s full title: “Nurse led, home based self help treatment for patients in primary care with chronic fatigue syndrome: randomised controlled trial.”

“The hyphen is a coupling between carriages of words to ensure unambiguous  transmission of thought,” wrote the doctor. “Surely this should read ‘Nurse-led, home-based, self- help…’

“Lest English sink further into the Great Despond of ambiguity and non-sense [hyphen included in the original comment], may I implore the co-editors of the BMJ to be the vigilant watchdogs of our mother tongue which at the hands of a younger ‘texting’ generation is heading towards anarchy.” [The original comment did not include the expected comma between ‘tongue’ and ‘which.’]

*****

In a response on the BMJ website a month after publishing the study, the FINE investigators reported that they had conducted a post-hoc analysis with a different kind of scoring for the Chalder Fatigue Scale.

Instead of scoring the answers as 0 or 1 using what was called a bimodal scale, they rescored them using what was called a continuous scale, with values ranging from 0 to 3. The full range of possible scores now ran from 0 to 33, rather than 0 to 11. (As collected, the data for the Chalder Fatigue Scale allowed for either scoring system; however, the original entry criteria of 4 on the bimodal scale would translate into a range from 4 to as high as 19 on the revised scale.)

With the revised scoring, they now reported a “clinically modest, but statistically significant effect” of pragmatic rehabilitation at 70 weeks—a reduction from baseline of about 2.5 points on the 0 to 33 scale. This final score represented some increase in fatigue from the 20-week interim assessment point.

In their comment on the website, the FINE investigators now reaffirmed that the 70-week assessment was “our primary outcome point.” This statement conformed to the protocol but differed from the suggestion in the BMJ paper that the 20-week results also represented “primary” outcomes. Given that the post-hoc rescoring allowed the investigators to report statistically significant results at the 70-week endpoint, this zig-zag back to the protocol language was perhaps not surprising.

In their comment, the FINE investigators also explained that they did not report their step-test results—their one objective measure of physical capacity–“due to a significant amount of missing data.” They did not provide an explanation for the missing data. (One obvious possible reason for missing data on an objective fitness test is that participants were too disabled to perform it at all.)

The FINE investigators did not address the question of whether the title of their paper should have included hyphens.

In the rapid comments, Tom Kindlon, a patient and advocate from a Dublin suburb, responded to the FINE investigators’ decision to report their new post-hoc analysis of the fatigue scale. He noted that the investigators themselves had chosen the bimodal scoring system for their study rather than the continuous method.

“I’m sure many pharmacological and non-pharmacological studies could look different if investigators decided to use a different scoring method or scale at the end, if the results weren’t as impressive as they’d hoped,” he wrote. “But that is not normally how medicine works. So, while it is interesting that the researchers have shared this data, I think the data in the main paper should be seen as the main data.”

*****

The FINE investigators have published a number of other papers arising from their study. In a 2013 paper on mediators of the effects of pragmatic rehabilitation, they reported that there were no differences between the three groups on the objective measure of physical capacity, the step test, despite their earlier decision not to publish the data in the BMJ paper.

Wearden herself presented the trial as a high point of her professional career in a 2013 interview for the website of the University of Manchester’s School of Psychological Sciences. “I suppose the thing I did that I’m most proud of is I ran a large treatment trial of pragmatic rehabilitation treatment for patients with chronic fatigue syndrome,” she said in the interview. “We successfully carried that trial out and found a treatment that improved patients’ fatigue, so that’s probably the thing that I’m most proud of.”

The interview did not mention that the improvement at 20 weeks was transient until the investigators performed a post-hoc-analysis and rescored the fatigue scale.

*****

The Science Media Centre, a self-styled “independent” purveyor of information about science and scientific research to journalists, has consistently shown an interest in research on what it calls CFS/ME. It held a press briefing for the first PACE results published in The Lancet in 2011, and has helped publicize the release of subsequent studies from the PACE team.

However, the Science Media Centre does not appear to have done anything to publicize the 2010 release of the FINE trial, despite its interest in the topic. A search of the center’s website for the lead FINE investigator, Alison Wearden, yielded no results. And a search for CFS/ME indicated that the first study embraced by the center’s publicity machine was the 2011 Lancet paper.

That might help explain why the FINE trial was virtually ignored by the media. A search on the LexisNexis database for “PACE trial” and “chronic fatigue syndrome” yielded 21 “newspaper” articles (I use the “apostrophes” here because I don’t know if that number includes articles on newspaper websites that did not appear in the print product; the accuracy of the number is also in question because the list did not include two PACE-related articles that I wrote for The New York Times).

Searches on the database combining “chronic fatigue syndrome” with either “FINE trial” or “pragmatic rehabilitation” yielded no results.
(I used the version of LexisNexis Academic available to me through the University of California library system.)

Other researchers have also paid scant attention to the FINE trial, especially when compared to the PACE study. According to Google Scholar, the 2011 PACE paper in The Lancet has been cited 355 times.  In contrast, the 2010 FINE paper in BMJ has only been cited 39 times.

*****

The PACE investigators likely exacerbated this virtual disappearance of the FINE trial by their decision not to mention it in their Lancet paper, despite its longstanding status as a “sister trial” and the relevance of the findings to their own study of cognitive behavior therapy and graded exercise therapy. The PACE investigators have not explained their reasons for ignoring the FINE trial. (I wrote about this lapse in my Virology Blog story, but in their response the PACE investigators did not mention it.)

This absence is particularly striking in light of the decision made by the PACE investigators to drop their protocol method of assessing the Chalder Fatigue Scale. In the protocol, their primary fatigue outcome was based on bimodal scoring on the 11-item fatigue scale. The protocol included continuous scoring on the fatigue scale, with the 0 to 33 scale, as a secondary outcome.

In the PACE paper itself, the investigators announced that they had dropped the bimodal scoring in favor of the continuous scoring “to more sensitively test our hypotheses of effectiveness.” They did not explain why they simply didn’t provide the findings under both scoring methods, since the data as collected allowed for both analyses. They also did not cite any references to support this mid-trial decision, nor did they explain what prompted it.

They certainly did not mention that PACE’s “sister” study, the FINE trial, had reported null results at the 70-week endpoint—that is, until the investigators rescored the data using a continuous scale rather than the bimodal scale used in the original paper.

The three main PACE investigators—psychiatrist Peter White and Michael Sharpe, and behavioral psychologist Trudie Chalder—did not respond to an e-mail request for comment on why their Lancet paper did not mention the FINE study, especially in reference to their post-hoc decision to change the method of scoring the fatigue scale. Lancet editor Richard Horton also did not respond to an e-mail request for an interview on whether he believed the Lancet paper should have included information about the FINE trial and its results.

Update 11/9/15 10:46 PM: According to a list of published and in-process papers on the FINE trial website, the main FINE study was rejected by The Lancet before being accepted by BMJ, suggesting that the journal was at least aware of the trial well before it published the PACE study. That raises further questions about the absence of any mention of FINE and its null findings in the text of the PACE paper.

David Tuller is academic coordinator of the concurrent masters degree program in public health and journalism at the University of California, Berkeley.

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Nature of fatigue in POTS

Posted on 11/11/2015 by wames

Research Abstract:

Individuals with postural orthostatic tachycardia syndrome share many symptoms with those who have chronic fatigue syndrome; one of which is severe fatigue. Previous literature found that those with chronic fatigue syndrome experience many forms of fatigue.

The goal of this study was to investigate whether individuals with postural orthostatic tachycardia syndrome also experience multidimensional fatigue and whether these individuals can be clustered into subgroups based on the types of fatigue they endorse.

A convenience sample of 138 participants (aged 14-29) with postural orthostatic tachycardia syndrome completed questionnaires that assessed fatigue, brain fog symptom severity, activities that improve brain fog, and brain fog-related disability. An exploratory factor analysis was conducted on the Fatigue Types Questionnaire, and a three-factor solution was produced. Factor scores were then used to cluster the patients into groups using a TwoStep cluster analysis.

This resulted in two clusters, a high severity group and a low severity group. The clusters were then compared on a number of items related to symptom expression. Individuals within the more severe cluster had significantly more brain fog at the beginning and end of the survey when compared to cluster two. Those in the more severe cluster also described more activity impairment as well as more frequent, more severe, and more debilitation from postural orthostatic tachycardia syndrome and brain fog.

The findings of the factor analysis suggest that patients with postural orthostatic tachycardia syndrome experience fatigue as a multidimensional construct and they also can be subgrouped based on symptom severity.

An assessment of fatigue in patients with postural orthostatic tachycardia syndrome, by S Wise, A Ross, A Brown, M Evans, L Jason in J Health Psychol. 2015 Nov 4. pii: 1359105315613624. [Epub ahead of print]

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Insomnia common in chronic diseases

Posted on 11/10/2015 by wames

Research abstract:

Highlights

  • Seventy-eight percent of US-based PatientsLikeMe respondents were at risk for National Sleep Foundation (NSF)-defined insomnia.
  • Trouble falling asleep was the sleep symptom most likely to result in self-reporting insomnia.
  • Forty-four percent awaken during the night and 42% awake unrefreshed, but these symptoms receive less attention.
  • Insomnia was worse in fibromyalgia (92%), Crohn’s disease (88%), depression (85%), and rheumatoid arthritis (RA) (85%).
  • Only 34% of patients reporting severe insomnia had ever received an insomnia diagnosis.

Background

Insomnia is increasingly recognized to be comorbid with one or more medical conditions. This study used an online research platform to characterize insomnia across different mental and physical conditions.

Methods

A custom cross-sectional survey was fielded online to 31,208 users of the patient community PatientsLikeMe. The survey queried members on National Sleep Foundation-defined insomnia risk (waking up feeling unrefreshed, difficulty falling asleep, waking in the middle of the night, or waking too early).

Results

Complete results were obtained from 5256 patients with 11 comorbid conditions. Seventy-six percent of US-based respondents were at risk for insomnia. Patients who reported difficulty falling asleep were found to have nearly twice the odds of self-reporting insomnia (odds ratio [OR]: 1.84; 95% confidence interval [CI]: 1.5–2.1) when compared to those who do not have difficulty falling asleep, whereas those who reported waking during the night or waking up unrefreshed were no more likely (OR: 1.025 and 1.032, respectively) to report that they suffered from insomnia than those who did not experience these issues. Although insomnia was self-reported as severe or very severe across most conditions, few respondents had actually been diagnosed with insomnia by a physician. After adjustment for age and gender, there was an independent and strong effect of primary condition severity on insomnia risk, and those with severe epilepsy (0.93), depressive disorders (0.92), and fibromyalgia (0.92) occupied the highest risk probabilities.

Conclusions

The high rate of severity and frequency of insomnia across a multitude of mental and physical conditions reveals an opportunity for better disease management through enhanced insomnia awareness.

New approach for analyzing self-reporting of insomnia symptoms reveals a high rate of comorbid insomnia across a wide spectrum of chronic diseases, by Bozena Katic, James Heywood, Fred Turek, Emil Chiauzzi, Timothy E. Vaughan, Kristina Simacek, Paul Wicks, Sachin Jain, Christopher Winrow, John J. Renger in Sleep journal Nov 2015 Vol 16, Issue 11, Pages 1332–1341

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