Imagine you are an epilepsy health professional seeing a patient with clinical symptoms of depression. What should you do? If you have read Noble et al.’s [1] recent JNNP review, entitled ‘Cognitive-behavioural therapy does not meaningfully reduce depression in most people with epilepsy…’ you may have become sceptical about the potential of CBT, or psychotherapy in general, to alleviate depression in people with epilepsy (PWE). This recent systematic review pooled data from five small randomised controlled trials (RCTs), with some elements of CBT for PWE, and performed an analysis of reliable change. ‘Pooled risk difference indicated likelihood of reliable improvement in depression symptoms was significantly higher for those randomised to CBT’, but the authors focused on the finding that ‘only’ 30% of patients receiving interventions, compared to 10% of controls, could be considered ‘reliably improved’. Emphasising the fact that over 2/3 of patients did not meet this criterion for improvement, the authors suggest CBT is ‘ineffective’, has ‘limited benefit’ and could even lead to lower ‘self–esteem’ and ‘helplessness’. Notably, the latter conclusions were based on hypothetical reactions to treatment, rather than empirically supported outcomes.

Therefore, the purpose of this letter, written by the Psychology Task Force of the International League Against Epilepsy (ILAE), is to argue that caution is needed when considering the authors’ conclusions and potential implications for the psychological care of PWE. Moreover, we offer alternative interpretations of the findings and raise the pertinent issue of how psychotherapy for PWE may continue to improve. Importantly, we hope to encourage health professionals to continue to refer patients for psychotherapy, which is an effective intervention for a substantial subgroup of PWE.
Consistent with Reuber’s [2] editorial commentary, Cognitive-behavioural therapy does meaningfully reduce depression in people with epilepsy, we would like to highlight the heterogeneity of the studies pooled and how this impacts the findings. First, the interventions were very diverse, and most would not be considered standardised CBT protocols for depression. Interestingly, one trial that utilised a standardised CBT protocol, resulted in 50% reliable change reductions in depressive symptoms, equivalent to CBT in the general population [3]. Second, over 10% of patients in the analyses had depressive symptoms within the non-clinical ranges. Further, unlike previous analysis of reliable change in depression [3], this review failed to control for baseline levels of depression severity. Third, Noble et al. collapsed data from four different self-report depression measures, only one designed for PWE. Depression in PWE can have distinct symptomatology, given the presence of seizures (peri-ictal depression) and anti-seizure medication effects, both of which can limit the validity of generic depression measures [4].
Noble et al. [1] describe their conclusion that 30% reliable improvements in depressive symptoms across trials is ‘ineffective’ as a ‘value judgement’, illustrating subjectivity, which Reuber’s [2] editorial commentary argued could be interpreted completely in reverse. That is, one could conclude from the data that the treatments are ‘effective’ for PWE. There is little consensus about what we expect a ‘reliable improvement’ to be in psychological distress for PWE, or for patients with a disabling neurological disorder in general. A stated goal of epilepsy treatment is “no seizures, no side-effects.” However, many PWE continue to have seizures, and all biological treatments have potential side-effects. 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. Arguments regarding quantifying ‘reliable improvement’ aside, we do agree with Noble et al.’s [1] conclusions that there is ‘substantial room for improvement’ in the treatment of depression for PWE.
One important limitation of previous trials is the relatively short duration of psychotherapy offered to PWE, a factor that Noble et al. [1] acknowledge. Across the five RCTs, there was only an average of 7 hours (8 sessions) of psychotherapy, the adherence of which is unclear [5]. Thus, it is very likely that participants did not receive a sufficient dosage of CBT, especially given a minimum of 12 sessions is indicated for depression in the general population [3]. In addition, many PWE experience cognitive difficulties, including memory impairment, which may require more intensive and tailored CBT [5]. These limitations need to be addressed and psychotherapy should be tailored to the unique needs of PWE. 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 (e.g. avoidance of seizure triggers), which Noble et al. did not consider.
Another critical area for improvement is the treatment of comorbid anxiety symptoms within psychotherapy for depression. Anxiety and depression are highly comorbid, and in clinical practice it is difficult to evaluate them separately [4]. As such, transdiagnostic treatments, which treat depression and anxiety in one protocol, are increasingly being adopted and proven to be effective in the general population. We disagree with Noble et al.’s [1] comments regarding the ‘disappointing’ evidence for the treatment of anxiety, as only one small trial is cited assessing the impact of CBT for depression (not anxiety), on a secondary anxiety measure. A conclusion of insufficient evidence would have been more accurate, given the state of the anxiety literature.
Depression in PWE remains underdiagnosed and treated, perhaps partially due to uncertainty about effective treatments [4]. At worse this results in poorer quality of life and higher suicide rates in PWE. Thus, the development of more effective psychotherapies, including alternatives to CBT, is warranted. However, the ILAE Psychology Task Force believes that it is inaccurate to label CBT as ‘ineffective’ based on the findings of Noble et al.’s [1] review. Instead, we encourage health professionals to interpret the Noble et al. [1] conclusions with caution, given the concerns raised with respect to depression outcome measures, dosage and quality of the psychotherapies, and interpretation of results. Further, even with a conservative estimate of 30% responders to the psychotherapies, we posit that CBT shows promise for treating depression in PWE and should remain a strong treatment consideration for the referring clinician.

This document was written by experts selected by the International League Against Epilepsy (ILAE) and was approved for publication by the ILAE. Opinions expressed by the authors, however, do not necessarily represent the policy or position of the ILAE.

References:
1. Noble AJ, Reilly J, Temple J, et al. 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: doi: 10.1136/jnnp-2018-317997
2. Reuber M. Cognitive-behavioural therapy does meaningfully reduce depression in people with epilepsy. Journal of Neurology, Neurosurgery and Psychiatry 2018 doi: 10.1136/jnnp-2018-318743
3. Ogles BM, Lambert MJ, Sawyer JD. Clinical Significance of the National Institute of Mental Health Treatment of Depression Collaborative Research Program Data. Journal of Consulting and Clinical Psychology 1995;63(2):321-26. doi: 10.1037/0022-006X.63.2.321
4. Kwon O-Y, Park S-P. Depression and Anxiety in People with Epilepsy. Journal of Clinical Neurology (Seoul, Korea) 2014;10(3):175-88. doi: 10.3988/jcn.2014.10.3.175
5. Modi AC, Wagner J, Smith AW, et al. Implementation of psychological clinical trials in epilepsy: Review and guide. Epilepsy and Behavior 2017;74:104-13. doi: 10.1016/j.yebeh.2017.06.016

In my view the data presented in this study (1) which are interpreted as indicating a high prevalence of functional movement disorders (FMD) in PD might also be interpreted as suggesting that diagnostic delay is common in PD, particularly among women patients who present as "high maintenance" patients. The diagnosis of functional movement disorders is a matter of expert opinion and in my view problems with study design and interpretation support rather than minimize cognitive and confirmation bias in this study.
Subjects all met UK brain bank criteria for PD. Subjects diagnosed with FND in this study had high rates of family history of PD. They had depression, anxiety, cognitive symptoms, pain, nausea, fatigue all common complaints among the population in general and most particularly in PD. The presence of these symptoms before or after diagnosis of PD is considered by the authors as supportive for a diagnosis of FMD. However, these same symptoms are known to be associated with PD and might be considered supportive of a PD diagnosis.
Disparities in healthcare for women are well established (2). Neurology has a long history of mistakes distinguishing the "functional" from the "organic" (e.g.3). To choose one example people with blepharospasm, mostly women, were institutionalized long-term as the disease was not recognized as neurologic. Women commonly encounter dismissal in the medical context and this can occasion missed opportunities for established clinical interventions (e.g. 4, 5, 6)
Study subjects were selected for assessment for FMD on the basis of their doctors having used language suggesting a suspicion of an FMD in the chart. It sounds as if investigators were reviewing records of colleagues at their own institution. How many, if any, neurologists were considered to have made diagnostic error?
Evidence for the effects of cognitive bias in clinical medicine overshadows evidence for the reliability and validity of expert evaluation of functional movement disorders (4, 7 8).
In the 19th century there was debate over whether Parkinson's disease itself was functional or organic (9). While some cases are clear cut, an old saw I use in teaching is that the proper movement disorder diagnosis is the one offered by the most senior professor in the vicinity.

References:
(1) Wissel BD, Dwivedi AK, Merola A, et al. Functional neurological disorders in Parkinson disease. J Neurol Neurosurg Psychiatry. 2018 Jun;89(6):566-571.
(2) Hornbuckle LM, Amutah-Onukagha N, Bryan A, et al. Health Disparities in Women. Clinical Medicine Insights Women’s Health. 2017.
(3) Hamill EB, Yen MT. The History of Blepharospasm in Medicine. Int Ophthalmol
Clin. 2018 Winter;58(1):3-10.
(4) Schulman KA, Berlin JA, Harless W, et al. The effect of race and sex on physicians' recommendations for cardiac catheterization. N Engl J Med. 1999 Feb 25;340(8):618-26.
(5) Faigle R, Urrutia VC, Cooper LA, Gottesman RF. Individual and System
Contributions to Race and Sex Disparities in Thrombolysis Use for Stroke Patients in the United States. Stroke. 2017 Apr;48(4):990-997
(6) Dusenbery M. Doing harm. Harper Collins 2018.
(7) Vickrey BG, Samuels MA, Ropper AH. How neurologists think: A cognitive psychology perspective on missed diagnoses. Ann Neurol. 2010 Apr;67(4):425-33.
(8) Saposnik G, Redelmeier D, Ruff CC, Tobler PN. Cognitive biases associated with medical decisions: a systematic review. BMC Med Inform Decis Mak. 2016 Nov 3;16(1):138.
(9) Bechet E. Contribution a l'etude clinique des formes de la maladie de parkinson. Paris. Ancienne Maison Delahaye. 1892.

Conflict of Interest

Dr. Laura Boylan does medicolegal consulting work.

Dear Editor,

I read the article entitled "Patients with Parkinson disease are prone to functional neurological disorders" by Hallett M published in the Journal of Neurology, Neurosurgery and Psychiatry (Published Online First: 16 March 2018. doi: 10.1136/jnnp-2017-317684). I want to congratulate the author for this successful article, and make some contributions.

The article particularly mentions certain aspects of the clinical presentation, medical history and examination of patients, which should raise the suspicion of a functional disorder (1). I think it is important to remember patients with functional disorders will not always adhere to these criteria and clinicians should perhaps consider trialling suspected patients on either cognitive behavioural therapy (CBT) or physiotherapy to assess if they experience any improvement with these strategies. There is increasing evidence to show CBT and physiotherapy are beneficial for patients with functional disorders, hence they may be useful in confirming the diagnosis (2)(3).

Furthermore, the author suggests patients with functional symptoms and no sign of Parkinson's Disease should not be pursued further for a diagnosis of Parkinson's Disease. I think a difficulty is often deciding what classifies as a sign of Parkinson's Disease. The cardinal symptoms of bradykinesia, resting tremor, muscular rigidity and postural instability are commonly subtle within patients, making them a challenge to distinguish from normal limits. This is made even more difficult if a functional disorder is also suspected. Clinicians should therefore consider demonstrating reduced levels of the presynaptic dopamine active transporter (DAT) using a DaTscan, if available, to aid their diagnosis of Parkinson's Disease as the author suggests in another of their articles (4). Guidance surrounding the use of a DaTscan from the National Institute for Health and Care Excellence (NICE) does not currently account for this indication, however it may be worth considering for future recommendations (5).

References:
1. Wissel BD, Dwivedi AK, Merola A, et al Functional neurological disorders in Parkinson disease J Neurol Neurosurg Psychiatry Published Online First: 16 March 2018. doi: 10.1136/jnnp-2017-317378.
2. Nielsen G, Stone J, Matthews A, et al Physiotherapy for functional motor disorders: a consensus recommendation J Neurol Neurosurg Psychiatry 2015;86:1113-1119.
3. Conwill M, Oakley L, Evans K, Cavanna A. CBT-based group therapy intervention for nonepileptic attacks and other functional neurological symptoms: A pilot study. Epilepsy & Behavior. 2014;34:68-72.
4. Hallett M. Psychogenic Parkinsonism. Journal of the neurological sciences. 2011;310(1-2):163-165. doi:10.1016/j.jns.2011.03.019.
5. National Institute for Health and Care Excellence. Parkinson’s disease in adults NICE guideline NG71 [Internet]. Nice.org.uk. 2017 [cited 12 April 2018]. Available from: https://www.nice.org.uk/guidance/ng71/chapter/Recommendations#diagnosing....

I read with great interest the paper by Jamjoom et al.[1] The authors have done commendable work in establishing a national external ventricular drain related infection (ERI) rate and elucidating the factors influencing it in the largest prospective multicentre study. However, some questions have been left unanswered in this respect.
One of the contributing factors to a low ERI rate in the study could have been the fact that majority (98.6%) of EVDs were inserted in the operating theatre. In their single centre retrospective study of 84 patients, Arabi et al[2] found that placement outside operating rooms was associated with a trend towards higher ERIs. Clark et al[3], in their retrospective review of complications of intracranial pressure monitoring in 140 trauma patients, noted that the incidence of major infectious complications (eg. clinical ventriculitis, subdural empyema, brain abscesses) was higher in the groups in which the catheter was placed in the intensive care unit. A randomised control trial would better examine the importance of this finding.
In this study by Jamjoom et al[1], the authors found no significant difference between infected and uninfected cases with regard to the length of tunnelling. However, recent evidence although weak, points towards a preventive benefit of long tunnel EVDs over short tunnel EVDs.[4,5] Hence, a discussion about the role of tunnelling length in ERIs is felt missing in the paper.
Korinek et al, in their study to test the effect of a strict protocol of care on ERI, have postulated that frequent manipulation of EVD increases the risk of related infections.[6] Since the study by Jamjoom et al[1] was a prospective study, this strength could have been utilised in determining the role of frequent manipulation of EVD (eg. dressing, flushing the system, administering intrathecal drugs) for purposes other than CSF sampling.
Lastly, an analysis of the role of perioperative systemic antibiotics as a preventive measure in ERI could have been done as the evidence is still controversial in this regard.[6]

REFERENCES
1 Jamjoom AAB, Joannides AJ, Poon MT-C, et al. Prospective, multicentre study of external ventricular drainage-related infections in the UK and Ireland. J Neurol Neurosurg Psychiatry 2018;89:120–6. doi:10.1136/jnnp-2017-316415
2 Arabi Y, Memish ZA, Balkhy HH, et al. Ventriculostomy-associated infections: incidence and risk factors. Am J Infect Control 2005;33:137–43. doi:10.1016/j.ajic.2004.11.008
3 Clark WC, Muhlbauer MS, Lowrey R, et al. Complications of intracranial pressure monitoring in trauma patients. Neurosurgery 1989;25:20-4.
4 Omar MA, Mohd Haspani MS. The Risk Factors of External Ventricular Drainage-Related Infection at Hospital Kuala Lumpur: An Observational Study. Malays J Med Sci MJMS 2010;17:48–54.
5 Rafiq MFA, Ahmed N, Ali S. Effect of tunnel length on infection rate in patients with external ventricular drain. J Ayub Med Coll Abbottabad JAMC 2011;23:106–7.
6 Korinek A-M, Reina M, Boch AL, et al. Prevention of external ventricular drain--related ventriculitis. Acta Neurochir (Wien) 2005;147:39-45; discussion 45-46. doi:10.1007/s00701-004-0416-z