Gluten sensitivity isn’t a fad

Posted on 07/10/2015 by wames

Gluten sensitivity isn’t a fad—it’s a real problem, say scientists, Tuesday, July 07, 2015 from What doctors don’t tell you

Not eating wheat is all the rage, and some sceptics regard it as a fashionable fad—but scientists have discovered that gluten sensitivity is a very real problem, and they’ve also figured out the biological mechanism behind it.

Eating wheat products such as bread or pasta releases molecules that can pass through the gut lining. The molecules include exorphins, which have been found in the spinal fluid of people with schizophrenia and autism.  They could also have an opioid-drug effect, which would explain the light-headedness that seems to affect some sufferers.

Researchers from Milan University have discovered that eating gluten releases these proteins and molecules, but say that more research is needed to find out what biological effect they may be having.

Although the mechanism around celiac disease and gluten intolerance is known, that of gluten sensitivity has not, until now, been established—partly because doctors and scientists just haven’t believed the problem exists.

The researchers made the discovery after they observed the biological processes that occurred after eating two kinds of sliced bread and four types of spaghetti.

Release of wheat gluten exorphins A5 and C5 during in vitro gastrointestinal digestion of bread and pasta and their absorption through an in vitro model of intestinal epithelium, by Milda Stuknytėa et al in Food Research International, June 2015; 72: 208)

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‘Internet of Things’ enabled devices could take pressure off GP services

Posted on 07/09/2015 by wames

Health and the ‘Internet of Things’ [from Independent living, July 2015]

72% of Britons believe using Internet of Things (IoT) enabled devices, like in-home monitors, would take pressure off the NHS.

It is difficult not to be aware of the increasing pressures on GP services, as fewer doctors are attracted to working in this area at the same time as demand increases, due to the ageing population and increase in people living with long-term health conditions.

According to a recent survey by YouGov for technology company Arqiva, nearly two thirds of people worry about the level of GP care that will be available in older age, and more than 70 percent of adults in Britain think that using internet-connected in-home technology – so called telehealth – could relieve some of the pressure on GP services, and help them to prioritise their time more effectively.

Majority of adults surveyed would be willing to monitor basic vitals at home

More than 90 percent of us would be ready to monitor basic health indicators, such as blood pressure, heart-rate and weight at home, which could be achieved via Internet of Things (IoT) enabled devices. Though perhaps not surprisingly, monitoring things that sound a bit more complicated, insulin levels, for example, or mental well-being, did not appeal to so many people, just 44 percent and 29 percent, respectively.

Key findings from the research include:

  • Over 70% of UK adults believe using in-home care technologies to monitor health would take the pressure off patients and the NHS (72%) and enable local GPs to prioritise patient treatment (71%)
  • 91% of people say they would be prepared to monitor basic vitals – such as blood pressure, heart rate and weight – at home
  • 64% of people are concerned about the level of GP care available in older age
  • Almost three quarters (72%) agree that the presence of monitoring technology in an elderly relative’s home would give them greater peace of mind and 70% said it would allow their relative to live independently for longer

Concerns regarding self-managed healthcare in terms of cost and technology

While there seems to be widespread agreement about the possibility of future self-management of healthcare, and a recognition that it could do a great deal to relieve some of the pressure on the NHS, there are some cautionary notes:

  • More than a quarter of those surveyed confessed that they already struggled with current levels of technology in their home
  • Almost a third thought that trying to manage technology in the home of an elderly relative would create more worries
  • A quarter believed that using telemedicine technology would be more trouble than going to the surgery

And some interesting ideas about where the money should be coming from, to pay for this brave new world of connected devices:

• 50% thought the government should pay
• 42% gave a share of the responsibility to NHS trusts
• 37% believed that the person concerned or their family should pay
• 32% saw a financial role for the local council…

Share your thoughts about self-managed healthcare!

What do you think? Would you be ready to keep a check on your own vital health stats at home? Or do you prefer the reassurance of a face-to-face meeting with your GP or practice nurse? Do you think we can continue to expect such a level of service from local doctors?

The downside of advancing technology: The Internet of Things: Your worst nightmare

The Internet of Things Council

NHS Wales & telehealth

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The Kynurenine Pathway in FM and ME/CFS

Posted on 07/08/2015 by wames

Cort Johnson explores the kynurenine pathway at Health Rising June 28 2015

The next couple of years may indicate that neuroinflammation and microglial activation play key roles in fibromyalgia and chronic fatigue syndrome. If that turns out to be true, the attention will probably quickly shift to something called the kynurenine pathway.

Kynurenines in CNS disease: regulation by inflammatory cytokines, by Brian M. Campbell, Erik Charych, Anna W. Lee and Thomas Moller in Frontiers in Neuroscience February 2014, Volume 8, Article12

The story starts with the metabolism of a single substance – tryptophan (TRP).  Tryptophan is an essential amino acid that forms the basis for some central nervous system heavyweights. Serotonin and melatonin are both derived from it and other tryptophan metabolites have significant functions.

Tryptophan is usually metabolized into serotonin and other factors but in the presence of inflammation, whether in the body or the brain, things change. It turns out that immune activation, in particular interferon-y, a key player in the antiviral response causes an enzyme called indole-2,3-dioxygenase (IDO) to transform tryptophan into kynurenine.

That has the unhappy result of depleting the brain of serotonin but that’s just the beginning of the problem.

The Road Not Taken

Kynurenine metabolism is complex but for our purposes the key fact is that at one point kynurenine metabolism splits into the two pathways – a neurotoxic (bad) pathway powered by an enzyme called KMO, and a neuroprotective (good) pathway powered by the KATS enzyme. Inflammation triggered tryptophan metabolism always sends kynurenine metabolism whizzing down the neurotoxic pathway.  A recent review of the kynurenine’s pathway effects in HIV/AIDS called it “An Immune Checkpoint at the Crossroads of Metabolism and Inflammation“. (HIV proteins activate the kynurenine pathway)

Activation of this pathway prods the microglia to produce substances like QUIN, an excitatory agent that sends the NMDA-type glutamate receptors into a glutamate producing frenzy. QUIN also teams up with a substance called 3-HK to produce oxidative stress.

The list of central nervous system disorders associated with increased kynurenines is a long one,  and includes neurodegenerative disorders like Parkinson’s disease and Alzheimer’s, autoimmune disorders (multiple sclerosis), psychiatric disorders (major depression, ADHD, schizophrenia) and infectious diseases (HIV-associated cognitive disorder).  The kynurenine triggered excitatory outburst may get so intense that it actually starts destroying neurons in Parkinson’s and ALS.  It may also contribute to the reduced dopamine levels (and reduced reward) present in ME/CFS and fibromyalgia.

Insights into how the kynurenine pathway may figure in chronic fatigue syndrome and fibromyalgia may be seen in interferon-alpha (IFN-a) trials in hepatitis and cancer.  Hepatitis C patients getting this intense immune booster experience similar symptoms (fatigue, depression, pain) and central nervous findings as ME/CFS patients.

Studies suggest increased kynurenine levels in hepatitis and breast cancer patients are associated with increased anxiety.

Another link with possible implications for ME/CFS and FM concerns Epstein-barr virus (EBV). Chronic active EBV infection  is present when antibody test results indicate an active infection is present.  Most people with ME/CFS do not have that kind of EBV infection, but it’s intriguing that chronic EBV  activation – which occurs in many cases of mononucleosis – triggers IDO to degrade tryptophan to kynurenine. Given kynurenine’s ability to sensitize the microglia kynurenine pathway upregulation, could be the straw that breaks the camel’s back for many.

Chronic Fatigue Syndrome and Fibromyalgia

Several studies suggest tryptophan levels may be lowered in fibromyalgia and/or ME/CFS. One study suggested an aberrant tryptophan – kynurenine pathway was operating in FM patients.  Blankfield asserts the reduced tryptophan levels could reflect malabsorption in the gastrointestinal tract or a chronic infection (or presumably chronic inflammation).  The fact that tryptophan degrading bacteria may help produce leaky gut syndrome as well suggests an inflammatory loop beginning at the gut and ending at kynurenine production in the central nervous system could occur.  On top of all this kynurenines have profound T-cell depleting properties.

Treatment Implications

The KP is an important target for the development of new therapies against neurodegenerative disorders, as it is comprised of compounds influencing processes related to excitotoxicity, oxidative damage and inflammation. [Bohar et.al 2015]

If inflammation either inside or outside the central nervous is triggering the neurotoxic arm of the kynurenine pathway, what can be done about it?  Not a lot right now, but the discovery that the kynurenine pathway upregulation is present in virtually every central nervous system disorder is spurring research.

Numerous targets on kynurenine activating enzymes have been identified that could be used to knock the neurotoxic portion of the pathway down.  Several compounds have been developed, one of which may be able to stop the production of the neurotoxic metabolite QUIN in its tracks. Other compounds have been developed to turn the neuroprotective side of the kynurenine pathway on.

Miller reports that recent advances provide “great promise” for the development of IDO inhibitors that stop tryptophan from being degraded to kynurenine in the first place.  An IDO inhibitor called 1-methyltryptophan (1-MT) is being tested in mice and in human trials of advanced cancer.  IDO is a tricky substance: while it’s upregulating tryptophan metabolism it’s also helping to tamp down autoimmune responses and it’s knocking down natural killer cells. IDO inhibitors may not be useful in those with autoimmune disorders.

They may be useful in depression, however. A recent review suggests further research into the intersection between tryptophan degradation, inflammation and depression will likely “provide many targets for novel antidepressant therapies.”

The key factor with the kynurenine pathway is that it’s a growth field.  Any disorder from HIV/AIDS, to cancer, to depression, to cardiovascular disease, that is associated with inflammation, has a stake in learning more about the kynurenine pathway.  If the trends hold, the number of PubMed studies published on the pathway will almost double from last year.  We should learn much more about this intriguing central nervous system pathway in the coming years.

 

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Adolescents with CFS have poor quality of life

Posted on 07/06/2015 by wames

Research abstract:

AIM: To study health related quality of life (HRQOL) and depressive symptoms in adolescents with chronic fatigue syndrome (CFS) and to investigate in which domains their HRQOL and depressive symptoms differ from those of healthy adolescents.

BACKGROUND AND OBJECTIVE: Several symptoms such as disabling fatigue, pain and depressive symptoms affect different life domains of adolescents with CFS. Compared to adolescents with other chronic diseases, young people with CFS are reported to be severely impaired, both physiologically and mentally. Despite this, few have investigated the HRQOL in this group.

METHODS: This is a cross-sectional study on HRQOL including 120 adolescents with CFS and 39 healthy controls (HC), between 12 and 18 years. The Pediatric Quality of Life Inventory™, 4.0 (PedsQL) was used to assess HRQOL. The Mood and Feelings Questionnaire assessed depressive symptoms.

Data were collected between March 2010 and October 2012 as part of the NorCAPITAL project (Norwegian Study of Chronic Fatigue Syndrome in Adolescents: Pathophysiology and Intervention Trial). Linear and logistic regression models were used in analysis, and all tests were two-sided.

RESULTS: Adolescents with CFS reported significantly lower overall HRQOL compared to HCs. When controlling for gender differences, CFS patients scored 44 points lower overall HRQOL on a scale from 0–100 compared to HCs. The domains with the largest differences were interference with physical health (B = −59, 95 % CI −54 to −65) and school functioning (B = −52, 95 % CI −45 to −58). Both depressive symptoms and being a patient were independently associated with lower levels of HRQOL

CONCLUSION

The difference in HRQOL between CFS patients and healthy adolescents was even larger than we expected. The large sample of adolescents with CFS in our study confirms previous findings from smaller studies, and emphasizes that CFS is a seriously disabling condition that has a strong impact on their HRQOL. Even though depressive symptoms were found in the group of patients, they could not statistically explain the poor HRQOL.

Health related quality of life in adolescents with chronic fatigue syndrome: a cross-sectional study, by Anette Winger et al in Health and Quality of Life Outcomes, 3 July 2015

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Noncoeliac gluten sensitivity

Posted on 07/06/2015 by wames

Research abstract:

The past 5 years have seen an increase in the use of a gluten-free diet outside a diagnosis of coeliac disease or IgE-mediated wheat allergy. This trend has led to the identification of a new clinical entity termed noncoeliac gluten sensitivity (NCGS).

In this Review, we discuss the evidence for NCGS as demonstrated by the results of double-blind, placebo-controlled dietary rechallenge studies. Furthermore, the characteristic phenotype of individuals with NCGS is described as well as the symptom manifestations commonly reported after gluten exposure, which include intestinal symptoms consistent with IBS, and extraintestinal symptoms such as neurological dysfunction, psychological disturbances, fibromyalgia and skin rash.

Moreover, emerging evidence suggests that NCGS can be associated with organic gastrointestinal pathologies, such as IBD, in which its presence might be a reflection of severe or stricturing disease.

However, NCGS is not without its controversies and uncertainties, in particular pertaining to whether it is gluten or nongluten components of the grain evoking symptoms; evidence suggests that fermentable carbohydrates, amylase trypsin inhibitors and wheat-germ agglutinin can also be responsible culprits. Finally, we discuss the novel techniques that might help diagnose NCGS in the future.

The spectrum of noncoeliac gluten sensitivity, by I Aziz, M Hadjivassiliou, DS Sanders in Nat Rev Gastroenterol Hepatol. 2015  Jun 30 [Epub ahead of print]

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IL-1 inhibition improves fatigue in CAPS

Posted on 07/03/2015 by wames

Research abstract:

Cryopyrin associated periodic syndromes (CAPS) is a rare group of autoinflammatory disorders that includes familial cold autoinflammatory syndrome (FCAS), Muckle-wells syndrome (MWS), and Neonatal onset multisystemic inflammatory disease (NOMID) .

CAPS is caused by a mutation in the NLRP3 (NOD like receptor family, pyrin domain containing 3) gene. This ultimately leads to increased production of IL-1β. IL-1β is a biologically active member of the IL-1 family. It is not only a pro-inflammatory cytokine responsible for features such as fever, rash, arthritis, but is also a major mediator in the central pathways of fatigue.

Fatigue is a major component of CAPS and is associated with severely compromised quality of life . In clinical studies, fatigue was measured using FACIT-F (functional assessment of chronic illness therapy-fatigue) and SF-36 (short form-36, physical component score) instruments.

These questionnaires can also be used to monitor improvement of fatigue following initiation of therapy. IL-1 inhibitors block the IL-1 signaling cascade, thereby preventing systemic inflammation in CAPS. The decrease in systemic inflammation is accompanied by improvement in fatigue .

Impact of IL-1 inhibition on fatigue associated with autoinflammatory syndromes, by P Efthimiou & SYadlapati in Mod Rheumatol, 2015 Jul 3: 1-22

 

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Immune and inflammation related genes in CFS

Posted on 07/03/2015 by wames

Research abstract:

Recent evidence suggests immune and inflammatory alterations are important in chronic fatigue syndrome (CFS). This study was done to explore the association of functionally important genetic variants in inflammation and immune pathways with CFS.

Peripheral blood DNA was isolated from 50 CFS and 121 non-fatigued (NF) control participants in a population-based study. Genotyping was performed with the Affymetrix Immune and Inflammation Chip that covers 11 K single nucleotide polymorphisms (SNPs) following the manufacturer’s protocol. Genotyping accuracy for specific genes was validated by pyrosequencing.

Golden Helix SVS software was used for genetic analysis. SNP functional annotation was done using SPOT and GenomePipe programs.

CFS was associated with 32 functionally important SNPs: 11 missense variants, 4 synonymous variants, 11 untranslated regulatory region (UTR) variants and 6 intronic variants. Some of these SNPs were in genes within pathways related to complement cascade (SERPINA5, CFB, CFH, MASP1 and C6), chemokines (CXCL16, CCR4, CCL27), cytokine signaling (IL18, IL17B, IL2RB), and toll-like receptor signaling (TIRAP, IRAK4).

Of particular interest is association of CFS with two missense variants in genes of complement activation, rs4151667 (L9H) in CFB and rs1061170 (Y402H) in CFH. A 5′ UTR polymorphism (rs11214105) in IL18 also associated with physical fatigue, body pain and score for CFS case defining symptoms.

This study identified new associations of CFS with genetic variants in pathways including complement activation providing additional support for altered innate immune response in CFS. Additional studies are needed to validate the findings of this exploratory study.

Pathway-focused genetic evaluation of immune and inflammation related genes with chronic fatigue syndrome, by Mangalathu S Rajeevan, Irina Dimulescu, Janna Murray, Virginia R. Falkenberg, Elizabeth R. Unger in Human Immunology,  24 June 2015

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ME/CFS: a real illness

Posted on 07/03/2015 by wames

Comment on the US Institute of Medicine’s report and choice of new name SEID by Prof Anthony Komaroff:

Chronic fatigue syndrome (named by some as myalgic encephalomyelitis/chronic fatigue syndrome [ME/CFS]) frustrates many physicians. That is understandable because there are no diagnostic tests or proven treatments. Some physicians even insist that the illness has no biological basis. Patients who seek help from such physicians are unlikely to have a satisfying therapeutic experience.

Fortunately, ME/CFS has recently received some welcome attention from the Institute of Medicine (IOM), Agency for Healthcare Research and Quality (AHRQ), and National Institutes of Health (NIH). Four articles in Annals address their findings. I will recap their answers to important questions.

How Prevalent and Important Is the Illness?
The IOM estimates that 836 000 to 2.5 million Americans have ME/CFS. The direct and indirect economic costs of the illness to society are estimated to be between $17 billion and $24 billion annually.

Is ME/CFS Real?
According to the most widely used case definition, the illness is characterized exclusively by symptoms; therefore, physicians have understandably wondered whether there are “real” underlying biological abnormalities. The IOM, AHRQ, and NIH panels concluded that there are such biological abnormalities. After evaluating thousands of published articles, the IOM committee stated that “ME/CFS is a serious, chronic, complex systemic disease that often can profoundly affect the lives of patients”. Summarizing the committee’s deliberations, Ganiats said that the illness “is not, as many clinicians believe, a psychological problem,” while emphasizing that psychiatric comorbid conditions occur in some patients with ME/CFS and need to be diagnosed and treated.

The IOM committee concluded that there is evidence of various neurologic abnormalities in patients with ME/CFS. Formal studies of cognition show slowed information processing, potentially related to problems with white matter integrity. A positron emission tomography study demonstrated neuroinflammation (activated microglia or astrocytes), functional magnetic resonance imaging studies found distinctive abnormalities when patients were challenged with working memory tasks, and the NIH report found “strong evidence of neurotransmitter signaling disruption.”

Studies summarized in the IOM report showed that some patients had reduced overnight cortisol, 24-hour urinary cortisol, and adrenocorticotropic hormone levels compared with healthy control participants, suggesting a secondary (brain) rather than a primary (adrenal) cause of reduced cortisol production. Many patients have orthostatic intolerance, manifested by objective heart rate and blood pressure abnormalities during standing or head-up tilt testing.

The IOM report also concluded that several immunologic abnormalities have been demonstrated in ME/CFS. Patients may have poor natural killer cell cytotoxicity that correlates with illness severity, although the IOM report noted that this abnormality was not specific to ME/CFS. There may be increased cytokine levels in the blood (or increased production of cytokines by leukocytes in the culture), suggesting a state of immune activation, although not all studies agreed on this point.

A recently published study—the largest of its type (298 case participants, 348 healthy control participants, and 51 cytokines measured in each blood sample)—found strikingly increased cytokine levels in the first 3 years of illness, which decreased thereafter (7). This suggests that heterogeneity in illness duration across studies may explain discrepant results.

Finally, the IOM assessed the possible role of infection in ME/CFS. It found “sufficient evidence suggesting that ME/CFS follows infection with EBV [Epstein–Barr virus] and possibly other specific infections—viral, bacterial and possibly protozoal.” The NIH report called especially for research on herpesviruses.

Is There a Biological Diagnostic Test?
As summarized previously, the IOM and NIH reports cited several objective biological abnormalities that help distinguish persons with ME/CFS from healthy control participants and, in some instances, from control participants with other fatiguing diseases, such as depression and multiple sclerosis. However, neither report found conclusive evidence that any particular biomarker was sufficiently sensitive or specific to serve as a diagnostic test.

Are There Proven Treatments?
The AHRQ-commissioned review of treatment trials, published in this issue, finds that counseling therapies and graded exercise therapy might help improve fatigue and function in some, but not all, patients; that not all trials show a benefit for the average patient; and that neither treatment is curative. Authors of the review warn that exercise therapy must be pursued very cautiously because several trials show that exercise leads to more adverse events and withdrawals. This is not surprising, given that postexertional malaise is a cardinal feature of the illness. The review notes that trials of drug treatments typically are of fair or poor quality, that no drug treatments are of proven value, and that some treatments—particularly corticosteroids and galantamine—cause important adverse events.

What Should Be the Case Definition?
The IOM committee proposes a new clinical case definition that is simpler than the most widely used research case definition. It will likely encompass a more homogeneous and sicker group of persons than the past case definitions and may help discriminate persons with this illness from those with other illnesses associated with fatigue, such as depression. However, as Haney and colleagues caution in their AHRQ-commissioned review of diagnostic methods, the proposed new case definition needs thorough testing in many patients with other fatiguing illnesses to ascertain its specificity.

What Should the Illness Be Named?
The IOM committee also proposes a new name for ME/CFS: systemic exertion intolerance disease. The reason to consider a new name is clear: The name “chronic fatigue syndrome” trivializes this often devastating illness. The U.S. Department of Health and Human Services commissioned the IOM report, and its agencies and advisory bodies will consider the proposed new name and case definition. This includes the Centers for Disease Control and Prevention, which sponsored the IOM’s effort as well as earlier efforts that had resulted in 2 previous case definitions.

These reports from the IOM, AHRQ, and NIH demonstrate how much we have learned about ME/CFS and how much we still do not know. We do not understand its pathogenesis, and we do not have a diagnostic test or a cure. However, these recent reports, summarizing information from more than 9000 articles, should put the question of whether ME/CFS is a “real” illness to rest. When skeptical physicians, many of whom are unaware of this literature, tell patients with ME/CFS that “there is nothing wrong,” they not only commit a diagnostic error: They also compound the patients’ suffering.

Myalgic Encephalomyelitis/Chronic Fatigue Syndrome: A real illness, by Anthony L. Komaroff, MD in Ann Intern Med.  2015;162(12):871-872 [references included]

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Rituximab leads to B-cell depletion and remission in ME/CFS

Posted on 07/02/2015 by wames

Research abstract:

Background: Myalgic Encephalopathy/Chronic Fatigue Syndrome (ME/CFS) is a disease of unknown etiology. We previously reported a pilot case series followed by a small, randomized, placebo-controlled phase II study, suggesting that B-cell depletion using the monoclonal anti-CD20 antibody rituximab can yield clinical benefit in ME/CFS.

Methods: In this single-center, open-label, one-armed phase II study (NCT01156909), 29 patients were included for treatment with rituximab
(500 mg/m2) two infusions two weeks apart, followed by maintenance rituximab infusions after 3, 6, 10 and 15 months, and with follow-up for 36 months.

Findings: Major or moderate responses, predefined as lasting improvements in self-reported Fatigue score, were detected in 18 out of 29 patients (intention to treat). Clinically significant responses were seen in 18 out of 28 patients (64%) receiving rituximab maintenance treatment. For these 18 patients, the mean response durations within the 156 weeks study period were 105 weeks in 14 major responders, and 69 weeks in four moderate responders.

At end of follow-up (36 months), 11 out of 18 responding patients were still in ongoing clinical remission. For major responders, the mean lag time from first rituximab infusion until start of clinical response was 23 weeks (range 8–66). Among the nine patients from the placebo group in the previous randomized study with no significant improvement during 12 months follow-up after saline infusions, six achieved a clinical response before 12 months after rituximab maintenance infusions in the present study.

Two patients had an allergic reaction to rituximab and two had an episode of uncomplicated late-onset neutropenia. Eight patients experienced one or more transient symptom flares after rituximab infusions. There was no unexpected toxicity.

Conclusion: In a subgroup of ME/CFS patients, prolonged B-cell depletion with rituximab maintenance infusions was associated with sustained clinical responses. The observed patterns of delayed responses and relapse after B-cell depletion and regeneration, a three times higher disease prevalence in women than in men, and a previously demonstrated increase in B-cell lymphoma risk for elderly ME/CFS patients, suggest that ME/CFS may be a variant of an autoimmune disease.

B-Lymphocyte Depletion in Myalgic Encephalopathy/ Chronic Fatigue Syndrome. An Open-Label Phase II Study with Rituximab Maintenance Treatment, by Øystein Fluge, Olav Mella et al in Plos One, July 1, 2015

New Scientist article: Antibody wipeout found to relieve chronic fatigue syndrome

ME Research UK article: Rituximab – promising effects

Phoenix rising article: Fluge & Mella’s pre-trial study highlights life-changing potential of rituximab

 

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The need to list exclusionary illnesses for SEID

Posted on 06/30/2015 by wames

Research abstract:

The Institute of Medicine recently proposed a new case definition for chronic fatigue syndrome (CFS), as well as a new name, Systemic Exertion Intolerance Disease (SEID).

Contrary to the Fukuda et al.’s CFS case definition, there are few exclusionary illnesses specified for this new SEID case definition.

The current study explored this decision regarding exclusionary illnesses using the SEID criteria with four distinct data sets involving patients who had been identified as having CFS, as well as healthy controls, community controls, and other illness groups.

The findings indicate that many individuals from major depressive disorder illness groups as well as other medical illnesses were categorized as having SEID. The past CFS Fukuda et al. prevalence rate in a community based sample of 0.42 increased by 2.8 times with the new SEID criteria.

The consequences for this broadening of the case definition are discussed.

From Diagnostics, 23 June 2015

Unintended Consequences of not Specifying Exclusionary Illnesses for Systemic Exertion Intolerance Disease, by Leonard A. Jason, Madison Sunnquist, Bobby Kot and Abigail Brown in Diagnostics, 23 June 2015
 

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