Seroxat study under-reported harmful effects on young people

Posted on 09/24/2015 by wames

Seroxat study under-reported harmful effects on young people, say scientists, by Sarah Boseley Health editor in Guardian online, Wednesday 16 September 2015

Experts who re-analysed data say study is still referred to in medical literature and needs to be retracted.

An influential study which claimed that an antidepressant drug was safe for children and adolescents failed to report the true numbers of young people who thought of killing themselves while on it, re-analysis of the trial has found

Study 329, into the effects of GlaxoSmithKline’s drug paroxetine on under-18s, was published in 2001 and later found to be flawed. In 2003, the UK drug regulator instructed doctors not to prescribe paroxetine – sold as Seroxat in the UK and Paxil in the US – to adolescents.

But experts who have obtained the original data say the study is still referred to in the medical literature and needs to be retracted.

In their re-analysis of the trial, published in the British Medical Journal, they say the beneficial effects of paroxetine on young people were far less and the harmful effects far greater than the study suggested.

Out of 275 children and adolescents in the trial, 11 taking the drug and one in the group given a placebo developed suicidal or self-harming behaviour. The original publication of the study reported five on the drug and one on placebo. There were no reports of suicidality on a second drug, imipramine, which was also tested in study 329.

David Healy, professor of psychiatry at Bangor University in Wales, said it was hard to see how so many suicidal children could have been overlooked. “We think if you were to go in and look at this data, anyone without training will find there are at least of the order of 12 children becoming suicidal on this drug out of about 93 [who were given it],” he said.

“This is a very high rate of kids going on to become suicidal. It doesn’t take expertise to find this. It takes extraordinary expertise to avoid finding it.”

In an article published with the re-analysis, Peter Doshi, associate editor of the BMJ, said the new paper “has reignited calls for retraction of the original study, putting additional pressure on academic and professional institutions to publicly address the many allegations of wrongdoing.”

He said few trials had been as controversial as study 329, whose lead author was Martin Keller from Brown University. In 2002, the year after its publication, the US Food and Drug Administration said it should be considered a failed trial because the depressed adolescents taking the drug did no better than those on placebo.

In that same year, more than two million prescriptions for paroxetine were written for adolescents and children in the United States, on the back of an advertising campaign which claimed the trial had shown “remarkable efficacy and safety”. GSK was fined $3bn in 2012 for fraudulently promoting the drug.

“It is often said that science self-corrects. But for those who have been calling for a retraction of the Keller paper for many years, the system has failed,” Doshi writes. “None of the paper’s 22 mostly academic university authors, nor the journal’s editors, nor the academic and professional institutions they belong to, have intervened to correct the record. The paper remains without so much as an erratum, and none of its authors – many of whom are educators and prominent members of their respective professional societies – have been disciplined.”

The BMJ authors, led by Prof Jon Jureidini at the University of Adelaide, wrote to GSK in 2013 asking whether the company intended to re-analyse the data itself. They say GSK declined.

However, GSK did co-operate with the re-analysis by agreeing to post 77,000 pages of de-identified case reports from the adolescents in the trial on a website.

The BMJ paper is the first re-analysis of a drug study under a new initiative called Riat (Restoring Invisible and Abandoned Trials). Dr Fiona Godlee, BMJ editor-in-chief, said publication of the reanalysed data from study 329 “sets the record straight” and “shows the extent to which drug regulation is failing us”. She said it also showed that the public and clinicians did not have the unbiased information they needed to make informed decisions.

She called for independent clinical trials rather than trials funded and managed by industry, as well as legislation “to ensure that the results of all clinical trials are made fully available and the individual patient data are available for legitimate independent third-party scrutiny.”

GSK stressed its commitment to transparency and its help for the researchers who re-analysed study 329. “Importantly, the findings from this team’s analysis appear to be in line with the longstanding view that there is an increased risk of suicidality in paediatric and adolescent patients given antidepressants like paroxetine,” it said.

“This is widely known and clear warnings have been in place on the product label for more than a decade. As such we don’t believe this reanalysis affects patient safety.”

 

Posted in News | Tagged , , | Comments Off on Seroxat study under-reported harmful effects on young people

SSRI combined with Dengzhanshengmai improves fatigue

Posted on 09/24/2015 by wames

Research abstract:

OBJECTIVE:

This study was to assess the efficacy and safety of selective serotonin reuptake inhibitor (SSRI) plus Dengzhanshengmai capsule in patients with chronic fatigue syndrome (CFS).

METHODS:

SSRI at a moderate dose plus Dengzhanshengmai (n = 134) with SSRI alone (n = 134) were compared for the efficacy and safety in the treatment of CFS. The therapeutic efficacy and safety were evaluated.

RESULTS:

As compared to monotherapy group, the efficacy in combined therapy group was better and characterized by the improvement of general fatigue (0.8±0.6 vs. 1.3±0.7), physical fatigue (0.6±0.3 vs. 1.0±0.4) and reduced activity (1.0±0.5 vs. 1.3±0.6) since the 2nd week (P<0.01) and in reduced motivation (2.1±0.8 vs. 2.4±1.0) since the 8th week (P<0.01) and the improvement continued thereafter. The mental fatigue score and HAD score were comparable between two groups (P>0.05). No significant difference was found in the drop-out rate between SSRI group (15.7%) and SSRI plus Dengzhanshengmai group (18.0%). The reasons for drop out were adverse events (7.5% vs. 9.7%), requests of the patients or career requirement (3.7% vs. 4.5%), loss to follow-up and others (2.2% vs. 3.0%) and lack of efficacy (2.2% vs. 0.7%). Although the patients in combined therapy group experienced a higher rate of hypertension than (5.8% vs. 1.5%), no significant difference was observed (P = 0.08).

CONCLUSION:

SSRI combined with Dengzhanshengmai capsule may significantly improve the general fatigue, physical fatigue, reduced activity and reduced motivation of CFS patients as compared to monotherapy with SSRI. Furthermore, this combined therapy is safe and tolerable.

Selective serotonin reuptake inhibitor combined with dengzhanshengmai capsule improves the fatigue symptoms: a 12-week open-label pilot study, by De-Qiang Li, Zhong-Chun Li and Zhi-Yuan Dai  in Int J Clin Exp Med, 2015 Jul 15; 8(7): 11811-11817.

 

 

Posted in News | Tagged , , , | Comments Off on SSRI combined with Dengzhanshengmai improves fatigue

Clonidine has little effect on autonomic cardiovascular & orthostatic symptoms in adolescents with CFS

Posted on 09/23/2015 by wames

Research abstract:

Background:

Chronic Fatigue Syndrome (CFS) is a common and disabling condition in adolescence with few treatment options. A central feature of CFS is orthostatic intolerance and abnormal autonomic cardiovascular control characterized by sympathetic predominance. We hypothesized that symptoms as well as the underlying pathophysiology might improve by treatment with the alpha2A–adrenoceptor agonist clonidine.

Methods:

A total of 176 adolescent CFS patients (12–18 years) were assessed for eligibility at a single referral center recruiting nation-wide. Patients were randomized 1:1 by a computer system and started treatment with clonidine capsules (25 μg or 50 μg twice daily, respectively, for body weight below/above 35 kg) or placebo capsules for 9 weeks. Double-blinding was provided. Data were collected from March 2010 until October 2012 as part of The Norwegian Study of Chronic Fatigue Syndrome in Adolescents: Pathophysiology and Intervention Trial (NorCAPITAL). Effect of clonidine intervention was assessed by general linear models in intention-to-treat analyses, including baseline values as covariates in the model.

Results:

A total of 120 patients (clonidine group n = 60, placebo group n = 60) were enrolled and started treatment. There were 14 drop-outs (5 in the clonidine group, 9 in the placebo group) during the intervention period. At 8 weeks, the clonidine group had lower plasma norepinephrine (difference = 205 pmol/L, p = 0.05) and urine norepinephrine/creatinine ratio (difference = 3.9 nmol/mmol, p = 0.002). During supine rest, the clonidine group had higher heart rate variability in the low-frequency range (LF-HRV, absolute units) (ratio = 1.4, p = 0.007) as well as higher standard deviation of all RR-intervals (SDNN) (difference = 12.0 ms, p = 0.05); during 20° head-up tilt there were no statistical differences in any cardiovascular variable. Symptoms of orthostatic intolerance did not change during the intervention period.

Conclusions:

Low-dose clonidine reduces catecholamine levels in adolescent CFS, but the effects on autonomic cardiovascular control are sparse. Clonidine does not improve symptoms of orthostatic intolerance.

Effects of low-dose clonidine on cardiovascular and autonomic variables in adolescents with chronic fatigue: a randomized controlled trial, by Even Fagermoen et al in BMC Pediatr, 2015 Sep 10; 15(1): 117 [Published online 2015 Sep 10]

Clinical Trials ID: NCT01040429, date of registration 12/28/2009.

Posted in News | Tagged , , , , , , , | Comments Off on Clonidine has little effect on autonomic cardiovascular & orthostatic symptoms in adolescents with CFS

Measuring post exertional fatigue

Posted on 09/23/2015 by wames

Research abstract:

OBJECTIVE:

To design and validate an instrument to capture the characteristic post-exertional exacerbation of fatigue in patients with chronic fatigue syndrome (CFS).

HIGHLIGHTS:

  • Provides a new self-report measure of fatigue in patients with chronic fatigue syndrome
  • Uniquely captures fatigue in real time with descriptive anchors derived from focus groups
  • Captures exacerbations following challenge tasks in the laboratory and in daily living
  • Distinct scale domains capture exacerbations following physical and cognitive tasks.

METHODS:

Firstly, patients with CFS (N=19) participated in five focus group discussions to jointly explore the nature of fatigue and dynamic changes after activity, and inform development of a self-report instrument – the Fatigue and Energy Scale (FES).

The psychometric properties of the FES were then examined in two case-control challenge studies: a physically-demanding challenge (moderate-intensity aerobic exercise; N=10 patients), and a cognitively-demanding challenge (simulated driving; N=11 patients). Finally, ecological validity was evaluated by recording in association with tasks of daily living (N=9).

RESULTS:

Common descriptors for fatigue included ‘exhaustion’, ’tiredness’, ‘drained of energy’, ‘heaviness in the limbs’, and ‘foggy in the head’. Based on the qualitative data, fatigue was
conceptualised as consisting of ‘physical’ and ‘cognitive’ dimensions.

Analysis of the psychometric properties of the FES showed good sensitivity to the changing symptoms during a post-exertional exacerbation of fatigue following both physical exercise and driving simulation challenges, as well as tasks of daily living.

CONCLUSION:

The ‘fatigue’ experienced by patients with CFS covers both physical and cognitive components. The FES captured the phenomenon of a post-exertional exacerbation of fatigue commonly reported by patients with CFS.

The characteristics of the symptom response to physical and cognitive challenges were similar. Both the FES and the challenge paradigms offer key tools to reliably investigate biological correlates of the dynamic changes in fatigue.

Capturing the post-exertional exacerbation of fatigue following physical and cognitive challenge in patients with chronic fatigue syndrome, by A Keech et al in Journal of Psychosomatic Research, 2 September 2015 [Epub ahead of print]

Simon McGrath from Phoenix rising comments:

There are a number of things I really like about this study:

  • Focus on post-exertional, not general fatigue, and ‘challenge’ tests of both moderate exercise and a driving simulator a cognitive challenge. I’d like to see a lot more studies using this approach
  • Involvement of patients in discussing what should be  in the fatigue scale (by contrast, Simon Wessley said he came up with the fatigue questions for the Chalder Fatigue scale all by himself).
  • The descriptors for post-exertional fatigue seem – from memory- similar to those that came up in studies by Lennny Jason and colleagues.

I wish they’d looked at post-exertional malaise more generally, rather than just focusing on fatigue. And while this study seems like a good start I don’t think you can validate any questionnaire on such a small sample. Added: the authors acknowledge this: “While the analysis of the psychometric properties of the FES was conducted across several patient groups and assessment conditions, each analysis involved only small samples of patients with CFS; investigation of the validity and reliability of the instrument in larger samples, and especially in patients with more severe symptomology, is required”.

This paper is part of a series using the challenge tests (another one here), and I know of two others that sound pretty interesting, including one that aims to replicate work done elsewhere.

Posted in News | Tagged , , , | Comments Off on Measuring post exertional fatigue

Low NK cell activity differs in ME/CFS & MS

Posted on 09/22/2015 by wames

Research abstract:

Chronic Fatigue Syndrome/Myalgic Encephalomyelitis (CFS/ME) and Multiple Sclerosis (MS) patients suffer from debilitating fatigue which is not alleviated by rest. In addition to the fatigue related symptoms suffered by CFS/ME and MS patients, dysfunction of the immune system and in particular, reduced Natural Killer (NK) cell cytotoxic activity has also been reported in CFS/ME and MS.

The purpose of this pilot study was to compare NK cellular mechanisms in CFS/ME and MS patients to investigate potential dysfunctions in the NK cell activity pathway. Flow cytometry protocols assessed CD56dim CD16+ and CD56bright CD16+/- NK cell expression of adhesion molecules, NK activating and inhibiting receptors, NK cell maturation and lytic proteins.

All participants in this study were female and included 14 CFS/ME patients, 9 MS patients and 19 non-fatigued controls. The patient groups and the non-fatigued controls were not taking any immunosuppressive or immune enhancing medications.

In the MS cohort, KIR2DL5 was significantly increased on CD56bright CD16+/- NK cells and expression of CD94 was significantly increased on CD56dim CD16+ NK cells in comparison to the controls. Co-expression of CD57 and perforin was significantly increased on CD56dim CD16+ NK cells from CFS/ME patients compared to the MS and non-fatigued control participants.

The results from this pilot study suggest that NK cells from CFS/ME and MS patients may have undergone increased differentiation in response to external stimuli which may affect different mechanisms in the NK cell cytotoxic activity pathway.

Pilot Study of Natural Killer Cells in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis and Multiple Sclerosis, by TK Huth, EW Brenu , S Ramos, T Nguyen, S Broadley, D Staines, S Marshall-Gradisnik in Scand J Immunol. 2015 Sep 18.  [Epub ahead of print]

Posted in News | Tagged , , , , , | Comments Off on Low NK cell activity differs in ME/CFS & MS

Children with CFS use more of their brain to concentrate

Posted on 09/22/2015 by wames

Research abstract:

The ability to divide one’s attention deteriorates in patients with childhood chronic fatigue syndrome (CCFS).

We conducted a study using a dual verbal task to assess allocation of attentional resources to two simultaneous activities (picking out vowels and reading for story comprehension) and functional magnetic resonance imaging.

Patients exhibited a much larger area of activation, recruiting additional frontal areas: 1) The right middle frontal gyrus (MFG), which is included in the dorsolateral prefrontal cortex, of CCFS patients was specifically activated in both the single and dual tasks; this activation level was positively correlated with motivation scores for the tasks and accuracy of story comprehension;

and 2) In patients, the dorsal anterior cingulate gyrus (dACC) and left MFG were activated only in the dual task, and activation levels of the dACC and left MFG were positively associated with the motivation and fatigue scores, respectively.

Patients with CCFS exhibited a wider area of activated frontal regions related to attentional resources in order to increase their poorer task performance with massive mental effort. This is likely to be less efficient and costly in terms of energy requirements. It seems to be related to the pathophysiology of patients with CCFS and to cause a vicious cycle of further increases in fatigue.

Highlights:

  • Decrease in divided attention was related to fatigue in childhood and adolescence.
  • Left frontal cortex of healthy students activated in verbal divided attention task
  • Right MFG and ACG were additionally activated in CCFS patients.
  • CCFS is characterized as an energy-inefficient process in frontal cortex.

Less efficient and costly processes of frontal cortex in childhood chronic fatigue syndrome, by K Mizuno K et al. in NeuroImage: Clinical, 2015 Sep 10.

Posted in News | Tagged , , , , , , , , , | Comments Off on Children with CFS use more of their brain to concentrate

Low NK Cell activity in CFS and is related to severity

Posted on 09/21/2015 by wames

Review abstract:

Background: Natural killer (NK) cells act as an immune surveillance against invading pathogens and tumors. NK cell cytotoxicity (NKCC) has been reported to be decreased in patients with CFS.

Methods: The objective of this review was to conduct an analysis of available publications that reported NKCC data in CFS in order to evaluate any relationships to case definitions used to define CFS and symptom severity.

Results: Of 17 studies that evaluated NKCC in patients with CFS, defined using the CDC 1988 and/or 1994 case definition (CD), 88% (15/17) concluded that NKCC was decreased in CFS patients compared to normal controls. The NKCC decrease was seen using two established methods, 51Cr release (11/13) and flow cytometry (4/4). The mean percent decrease in NKCC using the CDC 1988 CD (66.3%) was significantly greater than that using the CDC 1994 CD (49.7%) (p<0.01).

This result is consistent with that of six publications showing a greater decrease in NKCC associated with increased CFS symptom severity based on the lower symptom requirement for the CDC 1994 vs. 1988 CD. In contrast, there was no significant difference in the mean percent decrease in NKCC seen comparing the CDC 1994 CD defined population using the 51Cr release (48.3%) vs. flow cytometry (50.7%) assays (p>0.5).

Finally, seven studies investigating the ability of various agents to augment NKCC in patients with CFS showed increases of NKCC with both in vitro exposure (4/5) and in vivo exposure using randomized trials (2/2).

Conclusions: Low NKCC is commonly seen in CFS and is associated with increase symptom severity.

Low NK Cell Activity in Chronic Fatigue Syndrome (CFS) and Relationship to Symptom Severity, by  David Strayer, Victoria Scott and William Carter in J Clin Cell Immunol 6:348. [Published: July 29, 2015]

Posted in News | Tagged , , , | Comments Off on Low NK Cell activity in CFS and is related to severity

Immune dysfunction differs in moderate and severe CFS/ME over time

Posted on 09/21/2015 by wames

Research abstract:

Background:
Research has identified immunological abnormalities in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis (CFS/ME), a heterogeneous illness with an unknown cause and absence of diagnostic test. There have been no CFS/ME studies examining innate and adaptive immune cells longitudinally in patients with varying severities. This is the first study to investigate immune cells over 6 months while also examining CFS/ME patients of varying symptom severity.

Methods
Participants were grouped into 18 healthy controls, 12 moderate and 12 severe CFS/ME patients and flow cytometry was used to examine cell parameters at 0 and 6 months.

Results
Over time, iNKT CD62L expression significantly increased in moderate CFS/ME patients and CD56 bright NK receptors differed in severe CFS/ME. Naïve CD8 + T cells, CD8 − CD4 − and CD56 − CD16 − iNKT phenotypes, γδ2T cells and effector memory subsets were significantly increased in severe CFS/ME patients at 6 months. Severe CFS/ME patients were significantly reduced in CD56 bright CD16 dim NKG2D, CD56 dim CD16 − KIR2DL2/DL3, CD94 − CD11a − γδ1T cells and CD62L + CD11a − γδ1T cells at 6 months.

Conclusions
Severe CFS/ME patients differed from controls and moderate CFS/ME patients over time and expressed significant alterations in iNKT cell phenotypes, CD8 + T cell markers, NK cell receptors and γδT cells at 6 months. This highlights the importance of further assessing these potential immune biomarkers longitudinally in both moderate and severe CFS/ME patients.

Longitudinal analysis of immune abnormalities in varying severities of Chronic Fatigue Syndrome/Myalgic Encephalomyelitis patients, by Sharni Lee Hardcastle, Ekua Weba Brenu, Samantha Johnston, Thao Nguyen, Teilah Huth, Sandra Ramos, Donald Staines and Sonya Marshall-Gradisnik in Journal of Translational Medicine 2015, 13:299  [Published: 14 September 2015]

ME Research UK article: Immune changes in severe ME/CFS

Posted in News | Tagged , , , , , , | Comments Off on Immune dysfunction differs in moderate and severe CFS/ME over time

Childhood trauma in CFS: personality disorders & psychopathology

Posted on 09/18/2015 by wames

Research abstract:

INTRODUCTION:

Personality Disorders (PDs) and childhood traumatic experiences have been considered risk factors for Chronic Fatigue Syndrome (CFS). However, the relationship between these factors and their associated psychopathological impact has not been explored in this population. This study was designed to evaluate the association between different childhood traumas and the presence and number of PDs and current psychopathology in a sample of CFS patients.

MATERIAL AND METHODS:

For this purpose, 166 CFS patients were evaluated with the Personality Diagnostic Questionnaire-4+ (PDQ-4+) and the Child Trauma Questionnaire. Other instruments were used to assess the associated psychopathology and the impact of fatigue.

RESULTS:

Of the total sample, 55 (33.1%) presented childhood trauma, the most frequent of which were emotional neglect (21.7%) and emotional abuse (18.1%). Considering PD presence, 79 (47.6%) patients presented some PD. There were no differences in frequency of physical childhood trauma in patients with and without PD. However, patients with PD had more frequently experienced emotional childhood trauma (OR=2.18, p=0.034). Severity of childhood trauma was related to a higher number of PDs, more severe depressive symptoms (p=0.025) and suicide risk (p=0.001). Patients with PD and any childhood trauma presented more severe depressive and irritable symptoms and a higher suicide risk than those without any PD and non-childhood traumatic event. These patients’ psychopathological symptoms were similar to those of patients with childhood trauma and without PD.

CONCLUSIONS:

These results suggest that emotional childhood trauma but not physical childhood trauma is related to higher frequency of PD presence. More severe childhood emotional and physical traumas are related to a higher number of PDs and to more severe psychopathological symptoms.

Childhood trauma in Chronic Fatigue Syndrome: focus on personality disorders and psychopathology, by N Sáez-Francàs, Calvo N, Alegre J, Castro-Marrero J, Ramírez N, Hernández-Vara J, Casas in Compr Psychiatry. 2015 Oct;62:13-9  [Epub 2015 Jun 17]

Posted in News | Tagged , | Comments Off on Childhood trauma in CFS: personality disorders & psychopathology

Orthostatic intolerance syndromes have different biochemical, autonomic and hemodynamic parameters

Posted on 09/17/2015 by wames

Research abstract:

INTRODUCTION AND OBJECTIVES:

Orthostatic intolerance (OI) syndromes are a confusing topic and determining a specific diagnosis to achieve optimal treatment can be troublesome. We sought to assess biomarker, hemodynamic and autonomic variables in OI patients (autonomic dysfunction [AD], postural orthostatic tachycardia syndrome [POTS] and neurally mediated syncope [NMS]) and healthy controls during supine and head-up tilt position in order to achieve a better diagnosis.

RESULTS:

In response to head-up tilt, patients with AD presented a marked decrease in systolic blood pressure (SBP) (p=0.002), and a blunted increase in heart rate (HR) (p=0.04). Baroreceptor gain was almost absent in supine position and did not change in response to tilt.

Patients with POTS had lower values of atrial natriuretic peptide (p=0.03) but similar neurohormonal biomarkers and hemodynamic and baroreceptor function in supine position compared to healthy subjects. However, in response to head-up tilting greater reductions in stroke volume (p=0.008) and baroreceptor gain (p=0.002) and greater rises in HR (p=0.001), total peripheral resistance (p=0.008), low frequency component of SBP variability (LF-SBP) (p=0.003) and plasma noradrenaline (p=0.03) were observed.

Patients with NCS had similar biomarkers and autonomic indices to healthy subjects in supine position, but a larger decrease in baroreceptor gain (p=0.007) and a greater rise in LF-SBP (p=0.004) and plasma adrenaline (p=0.003) response to head-up tilting.

CONCLUSION:

Although different OI syndromes share similar symptoms, including blurred vision, syncope and dizziness particularly during orthostatism, they differ markedly regarding biochemical, autonomic and hemodynamic parameters. Assessment of these differences may be helpful for better diagnosis and management.

Autonomic activity and biomarker behavior in supine position and after passive postural stress in different orthostatic intolerance syndromes, by J Freitas  et al. in Rev Port Cardiol. 2015 Aug 26 pii: S0870-2551(15)00182-1.  [Epub ahead of print]

 

Posted in News | Tagged , , , , , , | Comments Off on Orthostatic intolerance syndromes have different biochemical, autonomic and hemodynamic parameters