Reply

To the Editor:
We appreciate the comments by Wei Gui and J. Sebag about Ozsaygili Cemal’s article titled ‘The effect of posterior vitreous detachment on aflibercept response in diabetic macular oedema.’1 In our study, we used the video display mode to obtain more reliable results while evaluating the posterior vitreous detachment (PVD) status with spectral-domain optical coherence tomography (SD-OCT). In a recent clinical study comparing the PVD status with ocular ultrasonography (US) and SD-OCT in patients with diabetic macular oedema (DMO), it was reported that video display mode SD-OCT showed total agreement (100% in video display mode) with US.2 We used the video display mode in all patients instead of a single cross-sectional view and excluded patients with poor image quality. Since it was a retrospective study, we could not have the chance to perform US, but excluding these patients from the study in patients where any of the 2 independent retina specialists (CO, BK) disagreed on the PVD status draws attention as factors that increase the validity of our data. In addition, the International Vitreomacular Traction Study Group, including doctor J. Sebag, has classified the posterior vitreous-macular relationship based on OCT and has mostly replaced USG with OCT in our current clinical practice.3
All eyes in our study were examined for vitreoschisis and similar anomalous PVD using SD-OCT video display mode. As you mentioned, SD-OCT has the ability to detect vitreoschisis.4,5 However, we had the chance to observe that the SD-OCT video display mode can make the fine distinction between vitreoschisis and artefact more reliably than single-section images and thanks to J. Sebag's letter for the opportunity to emphasize this once again. We think that the SD-OCT video imaging mode should be kept in mind by clinicians as it provides dynamic evaluation like USG and increases the reliability of static cross-sectional images which can rarely lead to erroneous interpretations.
We have applied the same number of injections to all eyes in our study and evaluated the short-term treatment response. However, as we mentioned in our study, further studies with longer follow-up are needed regarding the effects of PVD status on injection requirement. After intravitreal injection, larger molecules may be more exposed to the molecular sieve effect of Balaz’s in the posterior vitreous cortex6, but aflibercept also may be too small to be affected by the molecular sieve effect. Not only the presence of the attached posterior vitreous cortex but also vitreous glycation and different amounts of vitreous that had glycated cross-links and hyaluronan can also affect the permeability coefficient for diffusion7 and treatment response. The answer to whether the effect of the posterior vitreous on the treatment response is more than a mechanical barrier will be elucidated by future studies. We thank Dr. Wei Gui and J. Sebag for the interest in our study and we welcome further comments, questions, and suggestions.

Cemal OZSAYGILI, Bekir KUCUK, Yener YILDIRIM

None of the authors has any financial/conflicting interests to disclose.

References
1. Özsaygili C, Küçük B, Yildirim Y. The effect of posterior vitreous detachment on aflibercept response in diabetic macular oedema [published online ahead of print, 2020 Jul 29]. Br J Ophthalmol. 2020;bjophthalmol-2020-316155. doi:10.1136/bjophthalmol-2020-316155
2. Pessoa B, Coelho J, Malheiro L, et al. Comparison of Ocular Ultrasound Versus SD-OCT for Imaging of the Posterior Vitreous Status in Patients With DME. Ophthalmic Surg Lasers Imaging Retina. 2020;51(4):S50-S53. doi:10.3928/23258160-20200401-07
3. Duker, J. S., Kaiser, P. K., Binder, S., de Smet, M. D., Gaudric, A., Reichel, E., Sadda, S. R., Sebag, J., Spaide, R. F., & Stalmans, P. (2013). The International Vitreomacular Traction Study Group classification of vitreomacular adhesion, traction, and macular hole. Ophthalmology, 120(12), 2611–2619. https://doi.org/10.1016/j.ophtha.2013.07.042
4. Gupta, P., Yee, K. M., Garcia, P., Rosen, R. B., Parikh, J., Hageman, G. S., Sadun, A. A., & Sebag, J. (2011). Vitreoschisis in macular diseases. The British journal of ophthalmology, 95(3), 376–380. https://doi.org/10.1136/bjo.2009.175109
5. Sebag J. Vitreoschisis in diabetic macular edema. Invest Ophthalmol Vis Sci. 2011;52(11):8455-8456. doi:10.1167/iovs.11-8333.
6. Balazs EA. Die Mikrostruktur und Chemie des Glaskörpers [Microstructure and chemistry of the vitreous body]. Ber Zusammenkunft Dtsch Ophthalmol Ges. 1968;68:536-572.
7. Lee O-T, Good SD, Lamy R, et al. Advanced glycation end product accumulation reduces vitreous permeability. Invest Ophthalmol Vis Sci 2015;56:2892–2897.

Dear Editor,

In their review and meta-analysis, Hedengran and coworkers1 report no relative therapeutic benefit of preservative-free (PF) therapies over benzalkonium chloride (BAK)-preserved ones. Should the costlier PF medications therefore be abandoned, or should we question this conclusion?
Ten of the 16 comparative trials analysed were of short duration, (between 15 and 90 days), the longest taking 6 months. Once-a-day medication was used in each trial, yet the dose response curve for BAK toxicity shows that each additional drop of BAK-containing medication doubles the likelihood of lissamine green corneal staining2 and increases the risk of early failure of glaucoma surgery.3 BAK toxicity is slow in onset increasing over time, due to its continual accumulation within ocular tissues.3 Thus, inconsistencies between experimental studies, which document the harmful effects of BAK and clinical trials, which do not, likely relate to the timing, dosing and duration of glaucoma therapy.4 Two to 12 week trials comparing BAK with alternatively preserved eyedrops, or PF formulations have shown no convincing differences in ocular tolerability, yet the benefits from switching from once-a-day preserved to PF therapy, accrue several months later.4 Longer term transition to alternatively preserved, or PF formulations improves tolerability, and there is good evidence that substituting PF tafluprost for BAK-containing latanoprost significantly improves tolerability.3 So short duration studies are unlikely to reveal substantive differences.4
Several methodological issues within this systematic review merit consideration. First, there is no protocol registration, which questions its transparency. Such protocols safeguard against biased post hoc decisions in review methods, such as selective outcome reporting. Second, there is no flow diagram presenting the process of report selection. Third, cross-over trials were considered as parallel in this meta-analysis, leading to a unit-of-analysis error, which should be avoided. Appropriate unbiased methodology does exist to impute within-patient differences to incorporate cross-over trials into a meta-analysis.5 Fourth, there was no risk-of-bias assessment across studies, such as a funnel plot and an asymmetry test, to elicit evidence of publication bias. A risk-of-bias in individual studies’ evaluation was performed utilizing an old Cochrane tool. Recently, a revised Cochrane risk-of-bias tool (the RoB 2.0) for randomized trials has been introduced, and is now the preferred option.6 Last but not least every meta-analysis should include the GRADE approach for grading the strength and quality of evidence.
Unfortunately, this review and most published literature focus on mild glaucoma therapy-related ocular surface disease (GTR-OSD). The dosing and number of IOP-lowering medications needed for glaucoma control increase with disease duration so studies to determine the optimal formulations needed to avert longer term moderate/severe GTR-OSD are sorely needed.3 We agree with the authors’ statement that the “study lengths are short, especially in the context of BAK-preserved eyedrop use often being lifelong”, but are unable to accept the conclusion that BAK-containing and PF medications do not differ with respect to tolerability and therapy outcome.

Anastasios G. Konstas1, Gábor Holló2, Andreas Katsanos3, Konstadinos G. Boboridis1, Anna-Bettina Haidich4, Gordon N. Dutton5.

1: 1st and 3rd University Departments of Ophthalmology, Aristotle University of Thessaloniki, Thessaloniki, Greece;
2: Tutkimusz Ltd and Eye Center, Prima Medica Health Centers, Budapest, Hungary;
3: Ophthalmology Department, University of Ioannina, Ioannina, Greece;
4: Department of Hygiene, Social-Preventive Medicine & Medical Statistics, School of Medicine, Faculty of Health Sciences, Aristotle University of Thessaloniki, Thessaloniki, Greece;
5: Department of Ophthalmology, Caledonian University, Glasgow, UK.

Correspondence to: Anastasios G. Konstas, 1st and 3rd University Departments of Ophthalmology, Aristotle University of Thessaloniki, Thessaloniki, Greece; email: agkonstas@gmail.com

References
1. Hedengran A, Steensberg AT, Virgili G, Azuara-Blanco A, Kolko M. Efficacy and safety evaluation of benzalkonium chloride preserved eye-drops compared with alternatively preserved and preservative-free eye-drops in the treatment of glaucoma: a systematic review and meta-analysis. Br J Ophthalmol 2020;104:1512-18.
2. Leung EW, Medeiros FA, Weinreb RN. Prevalence of ocular surface disease in glaucoma patients. J Glaucoma 2008;17:350–5.
3. Konstas AGP, Labbe A, Katsanos A et al. The treatment of glaucoma using topical preservative-free agents: an evaluation of safety and tolerability. Expert Opin Drug Saf 2021;20:453-66.
4. Rasmussen CA, Kaufman PL, Kiland JA. Benzalkonium chloride and glaucoma. J Ocul Pharmacol Ther 2014;30:163–9.
5. Elbourne DR, Altman DG, Higgins JP et al. Meta-analyses involving cross-over trials: methodological issues. Int J Epidemiol 2002;31:140-9.
6. Sterne JAC, Savović J, Page MJ et al. RoB 2: a revised tool for assessing risk of bias in randomised trials. BMJ 2019;366:l4898.

We read with interest the recent article by Evans et al regarding outcomes in randomised control trial of multifocal lenses in cataract surgery, and their case for development of a core outcome set.1 We wholeheartedly agree that a set of core outcomes would be hugely beneficial to multifocal intraocular lens (MIOL) studies, as there is such variation in multifocal studies currently. This has been commented on by previous Cochrane reviews2 yet there remains no consensus. Such variability makes meaningful comparison between studies difficult.
Evans’ suggests that the minimum data collected in MIOL studies should be unaided and corrected distance and near LogMAR acuity and contrast sensitivity. Also, the use of a questionnaire for patient reported outcomes that must include questions relating to spectacle independence and halos/glare.
Whilst we agree with the above measures, we feel that perhaps such a minimum data set may be insufficient particularly as it fails to address intermediate vision. We would recommend the inclusion of a defocus profile that covers distance, intermediate and near ranges. In addition, a standardised method of defocus measurement3 and analysis.4 This could be used as an adjunct to conventional visual acuity testing or indeed as a replacement. MIOLs have different add powers and light distribution profiles; consequently the choice of testing distance for near and intermediate acuity measures has a profound impact on results and hence may not reflect visual function accurately. The use of a defocus curve is more robust to the variations between lenses and provides vital information for clinicians looking to assess the performance of the MIOL.
Finally, Evans suggests a post-operative interval of 6-18 months, and we entirely support the need for a long-term follow-up interval, yet feel it is beneficial to include a short-term follow-up also (<6 months) to allow for comparison and documentation of changes to measures, such as contrast sensitivity, which have been shown to improve with time5

References
1. Evans JR, de Silva SR, Ziaei M, Kirthi V, Leyland MD. Outcomes in randomised controlled trials of multifocal lenses in cataract surgery: the case for development of a core outcome set. Br J Ophthalmol. 2020;104(10):1345-1349.
2. de Silva SR, Evans JR, Kirthi V, Ziaei M, Leyland M. Multifocal versus monofocal intraocular lenses after cataract extraction. Cochrane Database Syst Rev. 2016;12:CD003169.
3. Gupta N, Wolffsohn JS, Naroo SA. Optimizing measurement of subjective amplitude of accommodation with defocus curves. J Cataract Refract Surg. 2008;34(8):1329-1338.
4. Buckhurst PJ, Wolffsohn JS, Naroo SA, et al. Multifocal intraocular lens differentiation using defocus curves. Invest Ophthalmol Vis Sci. 2012;53(7):3920-3926.
5. Law EM, Aggarwal RK, Buckhurst H, et al. Visual function and subjective perception of vision after bilateral implantation of monofocal and multifocal IOLs: a randomized controlled trial. J Cataract Refract Surg. 2020;46(7):1020-1029.