To the Editor,
We read with interest the work from Licher et al. [1] in which the authors tried to quantify the burden of common neurological diseases (i.e. dementia, stroke and parkinsonism) in 12 102 individuals (6 982 women and 5 120 men) aged ≥ 45 years and free from these diseases at baseline. All these individuals were recruited between 1990 and 2016 into the prospective population-based Rotterdam Study. At the end of their analyzes, the authors concluded that one in two women and one in three men will develop dementia, stroke or parkinsonism during their lifetime, and that the risk for women to develop both stroke and dementia during their life is almost twice that of men [1].
By reading the article from Licher et al. [1], we were extremely surprised by the fact that the authors did not consider the impact of the difference in life expectancies between men and women on their results and conclusions. This is particularly well underlined by the fact that the authors did not clearly precise the age structures of the two populations they studied [1]. In our view, this information is critical as, although the reasons for this difference are still debated and may probably be multi-factorial [2], it is well known that women live longer than men. This trend is confirmed by the 2018 World Health Statistics report [3] that estimates that in 2016, the life expectancies of men and women at birth were respectively 69.8 and 74.2 years at the international level. Therefore, knowing that stroke, dementia and parkinsonism are more prevalent in the elderly than in younger people [4], it is clear for us that what the authors attributed to sex is in fact the direct consequence of ageing, an aspect that was not studied by the authors. By not highlighting this factor, they led readers to misinterpretations, including general newspapers journalists that assume that this difference is a gender gap that should be filled.
To conclude, by not considering the impact of the difference in life expectancies between men and women on their study, the authors introduced an important bias in their study, leading them to draw erroneous conclusions. Age is the real culprit, not gender!
 
References
1 Licher S, Darweesh SKL, Wolters FJ, et al. Lifetime risk of common neurological diseases in the elderly population. J Neurol Neurosurg Psychiatry 2018;:jnnp-2018-318650.
2 Marais GAB, Gaillard J-M, Vieira C, et al. Sex gap in aging and longevity: can sex chromosomes play a role? Biol Sex Differ 2018;9:33.
3 World Health Organization. World Health Statistics 2018- Monitoring health for the Sustainable Development Goals. Available from http://apps.who.int/iris/bitstream/handle/10665/272596/9789241565585-eng.... Accessed on 2018/10/22.
4 GBD 2015 Neurological Disorders Collaborator Group. Global, regional, and national
burden of neurological disorders during 1990-2015: a systematic analysis for the
Global Burden of Disease Study 2015. Lancet Neurol 2017;16:877–97.

We read with interest the description of the movement disorder manifestations in patients with N-methyl-D-aspartate receptor antibody mediated encephalitis (NMDAR-AbE) by a panel of movement disorders experts (1). The authors conclude that the co-existence of dystonia, chorea and stereotypies within the same patient, variability in phenomenology within the course of a single day and evolution over time, are helpful pointers to the diagnosis of NMDAR-AbE and therefore early treatment. We agree with this conclusion. However, this analysis overlooks consideration of the distinctive, if not unique, phenomenology of the “classical” movement disorder of NMDAR-AbE (2).

In our earlier description of this complex movement disorder we reported the presence of variable, complex, jerky semi-rhythmic bulbar and limb movements, associated with posturing and oculogyric crises, but in summarising the overall clinical syndrome we deliberately avoided conventional movement disorder terms because none captured the entire clinical picture (2). Classification of a movement disorder, particularly when complex, is guided by the most obvious, dominant or overwhelming clinical feature. The ‘classical’ movement disorder in NMDAR-AbE is complex but as acknowledged by the expert reviewers, is not typical of any of the movement disorder categories (1). Stereotypies are purposeless repetitive motor behaviours that occur when awake and are interrupted by a shift in attention or distraction. Dystonia and chorea characteristically accompany voluntary or postural movements, subsiding with rest and disappearing during sleep. We drew attention to the occurrence of the movement disorder in the obtunded state, ‘awake unresponsiveness’ or coma, the disappearance of the movements following recovery of consciousness, and highlighted the modulation of movements with sensory stimuli. These features are not typical of stereotypies, dystonia or chorea. Mutism, waxy flexibility, catatonia, oculogyric crises, opisthotonus and other signs occur as elements of the clinical picture but are not dominant features of the syndrome.

We suggested the occurrence of these movements in obtunded states provided an important clue to the pathophysiology (2) and drew attention to similar movements in phencyclidine and ketamine intoxication associated with “dissociative anaesthesia” (ie, loss of responsiveness to external stimuli, also referred to as akinetic mutism, coma vigil or wakeful unresponsiveness in the neurological literature), stupor or coma. The initial neuropsychiatric and behavioural abnormalities suggest frontal-limbic involvement but this does not account for the altered conscious state and movement disorder. In order to explain this we postulated progression to diffuse cortical NMDA receptor blockade, interrupting glutamate transmission and suspending or “silencing” supratentorial descending tonic GABAergic inhibitory input to brainstem reticular systems, releasing patterned rhythmic movements such as chewing, bruxism, facial grimacing, frowning, lip smacking, tongue movements and rudimentary limb movements from pattern generators within pontomesencephalic locomotor regions or the pontomedullary reticular formation. These movements are analogous to primitive motor synergies such as undulatory gill and fin motion in fish, chewing and stepping. Decerebrate posturing, opisthotonus and oculogyric crises may be generated by similar mechanisms releasing the brainstem reticular systems from supratentorial control. As conscious state, awareness and responsiveness improve the movements subside, indicating return of the normal hierarchical descending hemispheric control over the brainstem centres. This model therefore explains the observed correlation between level of consciousness and movement severity.

References
1. Varley JA, Webb AJS, Balint B, et al. The movement disorder associated with NMDAR antibody encephalitis is complex and characteristic: an expert video rating study. J Neurol Neurosurg Psychiatry doi:10.1136/jnnp-2018-318584.
2. Kleinig TJ, Thompson PD, Matar W, et al. The distinctive movement disorder of ovarian teratoma associated encephalitis. Mov Disord 2008, 23: 1256-1261.

Dear Editor,
Re: A response from Noble et al. to e-letter by Psychology Task Force of the International League Against Epilepsy
Cognitive behavioural therapy (CBT) has been recommended for treating depression in people with epilepsy (PWE).[1, 2] The clinical significance of the effects of CBT for PWE has though, not been considered. We therefore systematically searched the literature for randomised controlled trials of CBT for PWE [3] and used Jacobson’s criteria [4] to empirically determine whether PWE made clinically reliable improvement. We compared this to that seen in the control arms of these trials.
Our main findings were that the likelihood of statistically reliable improvement in symptoms of depression was significantly higher for those PWE randomised to CBT compared to control conditions. The overall proportion of PWE achieving reliable improvement was low – 30% compared to 10% in the control arms. For most PWE, symptoms were unchanged.
The proportion of PWE who improve following CBT is limited. It should serve as a clarion call for the development of more effective treatments. Indeed, our review may have inflated CBT’s benefit since some trials included PWE without clinical distress at baseline and so it was not possible to apply Jacobson’s second, more stringent criterion and calculate for what proportion CBT also resulted in recovery.
The Psychology Task Force of the International League Against Epilepsy submitted a response to our article. [5] We are pleased that our article has drawn attention to the issue of what currently available treatments are able to offer PWE and that is has stimulated a needed discussion on the topic. Our paper agreed with many of the points raised by the Task Force:
1. More well conducted trials of psychological interventions are needed. Methodologically weak trials are known to overestimate treatment effects;
2. CBT can alleviate depression for some PWE in clinical practice, but substantial room for improvement exists;
3. Participant samples need to be better described and standardised criteria should be used to do this. Evaluations of sample representativeness can then be made, and potential treatment moderators identified;
4. Trials need to test the benefit of treatments for the full range of clinical depression. Trials have so far tended to exclude those with severe levels of depression, and some have included PWE without depression at baseline;
5. Trials should use measures of depression that are valid and reliable for the epilepsy population and for the context in which they are used.
However, there were several comments in the Task Force’s response which misrepresented our position. The Task Force also presented some reasons that they felt might explain the low rate of improvement in depression detected by our review. Below we clarify our position and address the explanations forwarded by the Task Force.
MISREPRESENTATIONS
Comment 1 by Task Force: “...we hope to encourage health professionals to continue to refer patients for psychotherapy... We argue that if just under 1 in 3 PWE reliably improve with CBT, which has no known side-effects, this is better than a possible alternative of unmanaged depression... the ILAE Psychology Task Force believes that it is inaccurate to label CBT as ‘ineffective’.”
Nowhere in our article did we recommend not referring PWE who are distressed for CBT or psychotherapy. Our review explicitly states that CBT does lead to statistically reliable improvement for some PWE and is preferable to offering no treatment. Depression has many deleterious effects and should not be left unmanaged.
Our review indicates that substantial room for treatment improvement exists. Consequently, we said “that it seems reasonable to conclude that when only 30% of treated patients make an improvement that highly effective CBT treatments for distress in epilepsy do not exist.” We did not, as asserted, label CBT as ineffective. Rather, we said the approach was “largely ineffective”.
Comment 2 by Task Force: “the authors suggest CBT... could even lead to lower ‘self–esteem’ and ‘helplessness’... the latter conclusions were based on hypothetical reactions to treatment, rather than empirically supported outcomes.”
Here a discussion point is mistaken for a conclusion. In our discussion we appropriately considered what implications our results have for what therapists should tell PWE considering CBT and related this to ethical and professional guidelines. We questioned how patients might feel if they were not informed about likely treatment response and went on to experience no benefit. Based on clinical experience amongst our team, and evidence from the literature,[6] we suggested possible reactions might include increased feelings of helplessness and hopelessness and lower expectations of therapy being successful in the future.
REASONS PRESENTED BY TASK FORCE TO ACCOUNT FOR LOW RATE OF IMPROVEMENT:
Comment 3 by Task Force: “we offer alternative interpretations of the findings...we would like to highlight the heterogeneity of the studies pooled and how this impacts the findings... First, the interventions were very diverse... Interestingly, one trial that utilised a standardised CBT protocol, resulted in 50% reliable change reductions in depressive symptoms... Second, over 10% of patients in the analyses had depressive symptoms within the non-clinical ranges.”
The pooled risk difference (RD) across the trials in our review was 0.20 – meaning 20% more PWE randomised to the CBT treatment arms reliably improved compared to the control arms. The trials in our review used different modes of treatment delivery and had samples with different levels of pre-treatment distress. We acknowledged this in our article and to explore whether this heterogeneity obscured higher rates of improvement in some trials, we presented RDs for the individual trials and also pooled RDs for trials using similar treatments and/or samples.
Unfortunately, regardless of how one approached the dataset (i.e., just looking at change in individuals who received face to face treatments or focusing on change in just participants who were distressed at baseline) only around 20% more patients in the CBT groups reliably improved compared to the control arms (see supplementary Figures 1-2 of our review [3]).
The Task Force highlighted the rate of reliable change reported by one trial in our review and implied that it’s results better reflect the potential of CBT for PWE. The trial in question was by Ciechanowski et al.[7]. Unfortunately, the benefit of CBT in that trial was actually not much better than indicated by the pooled RD. The Task Force correctly point out that the proportion of reliable change in the treatment arm of Ciechanowski et al.’s trial was 50%. They neglected to consider though that the proportion who reliably improved in that trial’s (treatment as usual) control arm was 24%. Thus, the RD for Ciechanowski et al.’s trial is 0.26 – not that much different to the pooled RD of 0.20.
Comment 4 by Task Force: “One important limitation of previous trials is the relatively short duration of psychotherapy offered to PWE, a factor that Noble et al. [1] acknowledge... it is very likely that participants did not receive a sufficient dosage of CBT... many PWE experience cognitive difficulties, including memory impairment, which may require more intensive and tailored CBT [5].”
Our review could only comment on the extent of change elicited by CBT treatments so far evaluated for PWE by trials. On average, the treatments offered by the trials in our review lasted 8.8 sessions. The Task Force suggest more treatment sessions may be required for PWE due to the presence of cognitive impairment. Whilst some PWE do experience such difficulties, this explanation does not appear to be able to account for the low rate of improvement seen in the trials in our review since most of them excluded patients with such difficulties.
Comment 5 by Task Force: “One advantage of CBT is that many of the behavioural skills; such as problem solving, sleep hygiene and controlled relaxation can also be tailored to assist with the self-management of epilepsy... which Noble et al. did not consider.”
We focused on trials for which the primary outcome measure was depression and examined the degree of change achieved

We thank you for the opportunity to respond to the Task Force’s letter. We trust that we have clarified our position on a range of points, including the need at present to continue to refer PWE who are distressed for CBT. We stand by our position though that there remains an urgent need for more effective treatments to be developed.

Yours sincerely,
Adam J. Noble
James Temple
James Reilly
Peter L. Fisher.

REFERENCES
[1] Kerr MP, Mensah S, Besag F, de Toffol B, Ettinger A, Kanemoto K, Kanner A, Kemp S, Krishnamoorthy E, LaFrance WJ, Mula M, Schmitz B, van Elst LT, Trollor J, Wilson SJ. International consensus clinical practice statements for the treatment of neuropsychiatric conditions associated with epilepsy. Epilepsia 2011;52: 2133-2138.
[2] Barry JJ, Ettinger AB, Friel P, Gilliam FG, Harden CL, Hermann B, Kanner AM, Caplan R, Plioplys S, Salpekar J, Dunn D, Austin J, Jones J, Advisory Group of the Epilepsy Foundation as part of its Mood Disorder. Consensus statement: the evaluation and treatment of people with epilepsy and affective disorders. Epilepsy & Behavior 2008 13: S1-29.
[3] Noble AJ, Reilly J, Temple J, Fisher PL. Cognitive-behavioural therapy does not meaningfully reduce depression in most people with epilepsy: a systematic review of clinically reliable improvement. Journal of Neurology, Neurosurgery & Psychiatry 2018; doi: 10.1136/jnnp-2018-317997.
[4] Jacobson NS, Truax P. Clinical significance: a statistical approach to defining meaningful change in psychotherapy research. Journal of Consulting and Clinical Psychology 1991;59: 12-19.
[5] Gandy M, Reuber M, LaFrance Jr WC, Modi A, Wagner JL, Goldstein LH, Tang V, Donald KA, Valente KD, Michaelis R. Why it’s still important to consider referring patients with epilepsy (PWE) with depression for psychotherapy – including Cognitive Behaviour Therapy. Response from the Psychology Task Force of the International League Against Epilepsy. Journal of Neurology, Neurosurgery & Psychiatry 2018; Published on: 11 July 2018.
[6] Crawford MJ, Thana L, Farquharson L, Palmer L, Hancock E, Bassett P, Clarke J, Parry GD. Patient experience of negative effects of psychological treatment: results of a national survey. The British Journal of Psychiatry 2016;208: 260-265.
[7] Ciechanowski P, Chaytor N, Miller J, Fraser R, Russo J, Unutzer J, Gilliam F. PEARLS depression treatment for individuals with epilepsy: a randomized controlled trial. Epilepsy & Behavior 2010;19: 225-231.

Dear Editor,

We read with great interest the recent paper of Sechi et al. that describes 13 patients with anti-GFAP related myelitis and compares them with 41 patients with anti-AQP4 related myelitis.1 To date, very little data is available about anti-GFAP related disorders.2-3 Sechi et al. highlight some differences between the two entities to help clinicians differentiate them.1 One of these clinical differences relates to area postrema syndrome (APS). Indeed, it is well known that APS is a classical feature of neuromyelitis optica spectrum disorders, particularly among anti-AQP4 positive patients.4 Sechi et al. report this syndrome as a prodromal event in 20% of anti-AQP4 related myelitis. Conversely, the authors do not report any case of APS preceding or accompanying myelitis related to anti-GFAP.1 Given these data, APS could be an indicator for ruling out anti-GFAP encephalomyelitis, particularly useful for centers that do not yet have access to biological testing for anti-GFAP Abs.
However, we report the case of a 41-year-old woman who in April 2016 developed intractable nausea and vomiting lasting for five weeks and leading to 35 kilograms in weight loss. An extensive search for a digestive disease was negative, and no neurological explorations were performed. One month following the resolution of digestive symptoms, she developed mental confusion, diplopia, dysarthria, dizziness, bilateral blurred vision (with optic disc edema) and paraparesis. Brain MRI was highly suggestive of anti-GFAP encephalomyelitis, notably with the presence of diffuse T2 abnormalities in periventricular white matter, with linear perivascular enhancement oriented radially to the ventricles.Spinal cord MRI revealed longitudinally extensive T2 hyperintensity (extended to the brainstem, with an upper limit involving the area postrema), with ill-defined margins, as described by Sechi et al.1. Anti-AQP4 and anti-MOG IgG were negative in the serum. Anti-GFAP IgG were detected in the serum (by cell-based assay and tissue-based assay). Lumbar puncture was performed before the patient was referred to our department, and was not repeated given the dramatic clinical improvement rapidly achieved with intravenous steroids. Among the 13 patients reported by Sechi et al., anti-GFAP IgG were detected only in the serum for two patients for which no CSF was available, like for our patient.
The patient gave written informed consent for information and images to be published
Our case underlines that the clinical spectrum of anti-GFAP encephalomyelitis is not fully described and understood yet and that clinical features of this syndrome may overlap with those of neuromyelitis optica spectrum disorders (related to anti-AQP4 IgG, to anti-MOG IgG or negative for both antibodies). As such, combining clinical data with radiological and biological data remains essential in order to properly classify patients with such rare central nervous system inflammatory disorders.

References
1 Sechi E, Morris PP, McKeon A et al. Glial fibrillary acidic protein IgG related myelitis: characterisation and comparison with aquaporin-4-IgG myelitis. J Neurol Neurosurg Neuropsychiatry 2018 (in press).
2 Fang B, McKeon A, Hinson SR et al. Autoimmune glial fibrillary acidic protein astrocytopathy: a novel meningoencephalomyelitis. JAMA Neurol 2016;73(11):1297-1307.
3 Flanagan EP, Hinson SR, Lennon VA et al. Glial fibrillary acidic protein immunoglobulin G as biomarker of autoimmune astrocytopathy: analysis of 102 patients. Ann Neurol 2017;81:298-309.
4 Wingerchuk DM, Banwell B, Bennett JL et al. International consensus diagnostic criteria for neuromyelitis optica spectrum disorders. Neurology 2015;85:177-189.