REPLY TO ADRION ET AL. ON PATEL ET AL. Letter to the Editor, British Medical Journal

Patel, M., Arshad, Q., Seemungal, B.M., Harcourt, J.P., Golding, J.F. and Bronstein, A.M. 2018. REPLY TO ADRION ET AL. ON PATEL ET AL. Letter to the Editor, British Medical Journal . British Medical Journal.

TitleREPLY TO ADRION ET AL. ON PATEL ET AL. Letter to the Editor, British Medical Journal
AuthorsPatel, M., Arshad, Q., Seemungal, B.M., Harcourt, J.P., Golding, J.F. and Bronstein, A.M.
Description

We apologise for not having noticed earlier Adrion and colleagues’ comments on our study comparing the effectiveness of intratympanic Methylprednisolone to Gentamicin in refractory Ménière’s disease [1], covered by the BMJ [2]. Contrary to our expectations, both drugs were equally effective in controlling vertigo (primary outcome).
Adrion’s main concerns were, (i) that negative studies pose the problem of “not knowing how to interpret the non-significant results in a clinically relevant way” and, (ii) the lack of a power calculation for the primary outcome.
Regarding (i), our interpretation is that given the known ototoxic effects of gentamicin, ascertaining any minuscule difference between the two drugs is not justified and, very likely, unethical. A further comment was that “transforming the data to achieve a more symmetric distribution may have resulted in more power when an ANOVA or t-test is applied”. We agree that some of the data deviated from strict normality. There is always debate about the robustness of ANOVA in these cases, however this was addressed in the paper - non-parametric tests confirmed that there were no significant differences between Methylprednisolone and Gentamicin for vertigo outcomes ([1] Appendix, page 6).
Adrion also recommended adjustment for baseline differences, but a crucial strength of our study was adherence to the CONSORT 2010 guidelines for transparent reporting of trials [3], which states that “Although proper random assignment prevents selection bias, it does not guarantee that the groups are equivalent at baseline. Any differences in baseline characteristics are, however, the result of chance rather than bias. The study groups should be compared at baseline for important demographic and clinical characteristics so that readers can assess how similar they were…….Adjustment for variables because they differ significantly at baseline is likely to bias the estimated treatment effect.” Nevertheless, to satisfy Adrion and colleagues’ concerns and for the benefit of readers, we reanalysed our primary outcome data with ANCOVA using baseline vertigo attack frequency over 6 months as covariate. As with ANOVAs and non-parametric tests, the re-analysis showed no difference between drugs (F=.527 df=1,57 p=.471). In other words, performing the ANCOVA does not change our results nor add any further information for the reader.
Regarding (ii) the reason for the lack of power calculation for the primary outcome was clearly stated in our paper: “At the time of planning of our study, there were few published data on intratympanic gentamicin versus steroid treatment for Ménière’s disease”. Hence sample-size calculations were based on hearing outcomes where drug differences were better established [4]. However, we are now able to back-calculate our data. Depending on which outcome metric is chosen to resolve the small effects observed (vertigo attacks at 2 years, percentage reduction in vertigo attacks, absolute reduction in number of vertigo attacks, using intention to treat or per protocol), for conventional 80% power with p=.05 2-tailed the numbers of patients required is between 150 to over 400 per group, thus illustrating the minute differences, if any, for the primary outcome (vertigo).
Finally, the comment “the primary endpoint may be biased since it was assessed by retrospective face-to-face interviews instead of event-oriented or daily symptom diaries”, was also addressed in the paper. It would be unethical to recruit patients with refractory Meniere’s disease experiencing more than one attack per week (Table 1,[1]) and require that they fill up a diary for the next 6 months before receiving treatment. Further, all the validated vestibular questionnaires used showed no differences between Methylprednisolone and Gentamicin either. In the same vein, it would be unethical to give patients a placebo when gentamicin is more effective than placebo for vertigo control (for Cochrane Review, see [5]) and it should be emphasised that a comparison between Gentamicin and Placebo led to the early termination of a randomised, double-blind, controlled trial in 2014 [6]. In view of our data [1], we believe that the initial treatment choice between an ototoxic drug (Gentamicin) and one that it is not (Methylprednisolone), will be simplified for most patients and doctors.
References
[1] Patel M, Agarwal K, Arshad Q et al. Intratympanic methylprednisolone versus gentamicin in patients with unilateral Meniere's disease: a randomised, double-blind, comparative effectiveness trial. Lancet 2016; 388(10061): 2753-62.
[2]. Mayor S. Steroid injections through the eardrum reduce dizziness in Meniere’s disease, study finds. BMJ 2016; 355:i6185.
[3] Schulz KF, Altman DG, Moher D, for the CONSORT Group. CONSORT 2010 Statement: updated guidelines for reporting parallel group randomised trials. BMJ 2010;340:c332.
[4] Sennaroglu L, Sennaroglu G, Gursel B et al. Intratympanic dexamethasone, intratympanic gentamicin, and endolymphatic sac surgery for intractable vertigo in Meniere's disease. Otolaryngology--head and neck surgery: official journal of American Academy of Otolaryngology-Head and Neck Surgery 2001; 125(5): 537-43.
[5] Pullens B, van Benthem PP. Intratympanic gentamicin for Ménière's disease or syndrome. Cochrane Database Syst Rev. 2011;(3):CD008234.
[6] Bremer HG, van Rooy I, Pullens B, et al. Intratympanic gentamicin treatment for Ménière's disease: a randomized, double-blind, placebo-controlled trial on dose efficacy - results of a prematurely ended study. Trials 2014;15:328.
Competing Interests: None
Competing interests: No competing interests

Year2018
Output mediaOnline
PublisherBritish Medical Journal
Publication dates
Published28 Feb 2018
ISSN0959-8138
Web address (URL)http://www.bmj.com/content/355/bmj.i6185/rr-0

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Nauseogenicity of off-vertical axis rotation vs. equivalent visual motion
Bijveld, M.M.C., Bronstein, A.M., Golding, J.F. and Gresty, M.A. 2008. Nauseogenicity of off-vertical axis rotation vs. equivalent visual motion. Aviation, Space, and Environmental Medicine. 79 (7), pp. 661-665. https://doi.org/10.3357/ASEM.2241.2008

Cognitive impairment by spatial disorientation
Gresty, M.A., Golding, J.F., Le, H. and Nightingale, K. 2008. Cognitive impairment by spatial disorientation. Aviation, Space, and Environmental Medicine. 79 (2), pp. 105-111. https://doi.org/10.3357/ASEM.2143.2008

[18F]2-fluoro-2-deoxy-D-glucose positron emission tomography (FDG PET) as a diagnostic tool for neurofibromatosis 1 (NF1) associated malignant peripheral nerve sheath tumours (MPNSTs): a long-term clinical study
Ferner, R.E., Golding, J.F., Smith, M., Calonje, E., Jan, W., Sanjayanathan, V. and O'Doherty, M. 2008. [18F]2-fluoro-2-deoxy-D-glucose positron emission tomography (FDG PET) as a diagnostic tool for neurofibromatosis 1 (NF1) associated malignant peripheral nerve sheath tumours (MPNSTs): a long-term clinical study. Annals of Oncology. 19 (2), pp. 390-394. https://doi.org/10.1093/annonc/mdm450

Visuo-vestibular influences on the moving platform locomotor aftereffect.
Bunday, K.L. and Bronstein, A.M. 2008. Visuo-vestibular influences on the moving platform locomotor aftereffect. Journal of Neurophysiology. 99 (3), pp. 1354-1365. https://doi.org/10.1152/jn.01214.2007

Cognitive performance in light current users and ex-users of ecstasy (MDMA) and controls
Golding, J.F., Groome, D.H., Rycroft, N. and Denton, Z. 2007. Cognitive performance in light current users and ex-users of ecstasy (MDMA) and controls. American Journal of Drug and Alcohol Abuse. 33 (2), pp. 301-307. https://doi.org/10.1080/00952990601175052

Genetic influences on motion sickness susceptibility in adult women: a classical twin study
Reavley, C.M., Golding, J.F., Cherkas, L.F., Spector, T.D. and MacGregor, A.J. 2006. Genetic influences on motion sickness susceptibility in adult women: a classical twin study. Aviation, Space, and Environmental Medicine. 77 (11), pp. 1148-1152.

Motion sickness susceptibility
Golding, J.F. 2006. Motion sickness susceptibility. Autonomic Neuroscience. 129 (1-2), pp. 67-76. https://doi.org/10.1016/j.autneu.2006.07.019

Increasing cognitive load with increasing balance challenge: recipe for catastrophe
Barra, J., Bray, A., Vishal, S., Golding, J.F. and Gresty, M.A. 2006. Increasing cognitive load with increasing balance challenge: recipe for catastrophe. Experimental Brain Research. 174 (4), pp. 734-745. https://doi.org/10.1007/s00221-006-0519-2

Tachypnea and hypocapnia are induced by 'buffeting' in vehicles
Green, D.A., Bray, A., Golding, J.F., Bronstein, A.M. and Gresty, M.A. 2006. Tachypnea and hypocapnia are induced by 'buffeting' in vehicles. Clinical Autonomic Research. 16 (4), pp. 281-285. https://doi.org/10.1007/s10286-006-0360-5

Predicting individual differences in motion sickness susceptibility by questionnaire
Golding, J.F. 2006. Predicting individual differences in motion sickness susceptibility by questionnaire. Personality and Individual Differences. 41 (2), pp. 237-248. https://doi.org/10.1016/j.paid.2006.01.012

Motion sickness susceptibility fluctuates through the menstrual cycle
Golding, J.F., Kadzere, P. and Gresty, M.A. 2005. Motion sickness susceptibility fluctuates through the menstrual cycle. Aviation, Space, and Environmental Medicine. 76 (10), pp. 970-973.

Can tamoxifen relieve motion sickness?
Gianni, M.C., Golding, J.F. and Goldhirsch, A. 2005. Can tamoxifen relieve motion sickness? Annals of Oncology. 16 (10), pp. 1713-1714. https://doi.org/10.1093/annonc/mdi304

Motion sickness
Golding, J.F. and Gresty, M.A. 2005. Motion sickness. Current Opinion in Neurology. 18 (1), pp. 29-34.

Effect of a novel motion desensitization training regime and controlled breathing on habituation to motion sickness
Yen Pik Sang, F., Billar, J., Gresty, M.A. and Golding, J.F. 2005. Effect of a novel motion desensitization training regime and controlled breathing on habituation to motion sickness. Perceptual and Motor Skills. 18 (1), pp. 29-34.

Perceived control, locus of control and preparatory information: effects on the perception of an acute pain stimulus
Williams, D., Golding, J.F., Phillips, K. and Towell, A. 2004. Perceived control, locus of control and preparatory information: effects on the perception of an acute pain stimulus. Personality and Individual Differences. 36 (7), pp. 1681-1691. https://doi.org/10.1016/j.paid.2003.07.009

We are most aware of our place in the world when about to fall
Bray, A., Subanandan, A., Isableu, B., Ohlmann, T., Golding, J.F. and Gresty, M.A. 2004. We are most aware of our place in the world when about to fall. Current Biology. 14 (15), pp. R609-R610. https://doi.org/10.1016/j.cub.2004.07.040

Suppression of sickness by controlled breathing during mildly nauseogenic motion
Yen Pik Sang, F., Golding, J.F. and Gresty, M.A. 2003. Suppression of sickness by controlled breathing during mildly nauseogenic motion. Aviation, Space, and Environmental Medicine. 74 (9), pp. 998-1002.

Effect of breathing supplemental oxygen on motion sickness in healthy adults
Ziavra, N., Yen Pik Sang, F., Golding, J.F., Bronstein, A.M. and Gresty, M.A. 2003. Effect of breathing supplemental oxygen on motion sickness in healthy adults. Mayo Clinic Proceedings. 78 (5), pp. 574-578.

Behavioral methods of alleviating motion sickness: effectiveness of controlled breathing and a music audiotape
Yen Pik Sang, F., Billar, J., Golding, J.F. and Gresty, M.A. 2003. Behavioral methods of alleviating motion sickness: effectiveness of controlled breathing and a music audiotape. Journal of Travel Medicine. 10 (2), pp. 108-112.

Impairment of spatial cognitive function with preservation of verbal performance during spatial disorientation
Gresty, M.A., Waters, S., Bray, A., Bunday, K. and Golding, J.F. 2003. Impairment of spatial cognitive function with preservation of verbal performance during spatial disorientation. Current Biology. 13 (21), pp. R829-R830. https://doi.org/10.1016/j.cub.2003.10.013

Motion sickness and tilts of the inertial force environment: active suspension systems vs. active passengers
Golding, J.F., Bles, W., Bos, E., Haynes, T. and Gresty, M.A. 2003. Motion sickness and tilts of the inertial force environment: active suspension systems vs. active passengers. Aviation, Space, and Environmental Medicine. 74 (3), pp. 220-227.

Attentional demands of continuously monitoring orientation using vestibular information
Yardley, L., Papo, D., Bronstein, A.M., Gresty, M.A., Gardner, M., Lavie, N. and Luxon, L. 2002. Attentional demands of continuously monitoring orientation using vestibular information. Neuropsychologia. 40 (4), pp. 373-383. https://doi.org/10.1016/S0028-3932(01)00113-0

Interference between postural control and mental task performance in patients with vestibular disorder and healthy controls
Yardley, L., Gardner, M., Bronstein, A.M., Davies, R., Buckwell, D. and Luxon, L. 2001. Interference between postural control and mental task performance in patients with vestibular disorder and healthy controls. Journal of Neurology, Neurosurgery and Psychiatry. 71 (1), pp. 48-52. https://doi.org/10.1136/jnnp.71.1.48

A motion sickness maximum around the 0.2 Hz frequency range of horizontal translational oscillation
Golding, J.F., Mueller, A.G. and Gresty, M.A. 2001. A motion sickness maximum around the 0.2 Hz frequency range of horizontal translational oscillation. Aviation, Space, and Environmental Medicine. 72 (3), pp. 188-192.

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