Eyes with Fuchs endothelial corneal dystrophy (FECD) are known to have reduced contrast vision from increased glare even if high-contrast acuity is not affected.1 In a retrospective study, Augustin and colleagues suggested that corneal guttae without edema contribute to decreased contrast sensitivity, and that such eyes would benefit from Descemet membrane endothelial keratoplasty (DMEK).2 The topic is important because it is unknown whether guttae in the absence of any corneal edema affect vision and therefore whether such eyes truly benefit from DMEK. The authors enrolled eyes with >5 mm of confluent guttae and without edema (modified Krachmer grade 5); however, they did not state their definition of “edema”. In FECD, when corneal edema is not clinically detectable by slit-lamp examination, it can be detected by Scheimpflug tomography.3 A recent study found evidence of subclinical corneal edema in 88% of eyes with FECD grade 5 and almost 40% of eyes with lesser grades of FECD.4 It is therefore highly likely that many of the FECD eyes examined by Augustin and colleagues did in fact have subclinical corneal edema, so can the authors examine the Scheimpflug tomograms of these eyes and report the contrast sensitivity results based on the presence or absence of subclinical edema? This is important because reduced contrast sensitivity might be caused by subclinical edema and not simply by “guttae without edema”, and cornea surgeons should not conclude that it is appropriate to offer DMEK for any eye with guttae. Surgeons and clinicians should recognize that Scheimpflug tomography patterns, which are easily acquired and repeatable,5 are more helpful than guttae assessment for guiding clinical decision-making in FECD.4

References

1. van der Meulen IJ, Patel SV, Lapid-Gortzak R, Nieuwendaal CP, McLaren JW, van den Berg TJ. Quality of vision in patients with Fuchs endothelial dystrophy and after Descemet stripping endothelial keratoplasty. Arch Ophthalmol 2011;129:1537-1542.
2. Augustin VA, Weller JM, Kruse FE, Tourtas T. Influence of corneal guttae and nuclear cataract on contrast sensitivity. Br J Ophthalmol 2020.
3. Sun SY, Wacker K, Baratz KH, Patel SV. Determining Subclinical Edema in Fuchs Endothelial Corneal Dystrophy. Revised Classification using Scheimpflug Tomography for Preoperative Assessment. Ophthalmology 2019;126:195-204.
4. Patel SV, Hodge DO, Treichel EJ, Spiegel MR, Baratz KH. Predicting the Prognosis of Fuchs Endothelial Corneal Dystrophy by using Scheimpflug Tomography. Ophthalmology 2020;127:315-323.
5. Patel SV, Hodge DO, Treichel EJ, Spiegel MR, Baratz KH. Repeatability of Scheimpflug Tomography for Assessing Fuchs Endothelial Corneal Dystrophy. Am J Ophthalmol 2020;215:91-103.

We thank Dr. Shukla for his interest in our article and his comments 1, 2.
In our study all consecutive cases of rhegmatogenous retinal detachment (RD) that underwent pars plana vitrectomy (PPV) were included in the study regardless of complexity, type of tear, lens or refractive status, or use of supplemental buckle in order to reduce selection bias and to allow study of various subgroups of patients. For the same reason the 13 cases with silicone oil present at the time of last follow-up were not excluded. The paper referenced by Dr. Shukla reports a retinal re-detachment rate of 13.2% after removal of silicone oil (ROSO), with many of the cases performed prior to the era of small gauge vitrectomy and wide-angle viewing systems (WAVS) 3. Encircling endolaser photocoagulation further reduces the re-detachment rate to 8.6% 4. More recent surgical techniques are likely associated with a lower retinal re-detachment rate. Nevertheless, a presumed retinal re-detachment of 13.2% following ROSO corresponds to an estimated 1.7 eyes with recurrent RD out of the 13 eyes with residual silicone oil in our series 3. This in turn corresponds to a 0.5% difference in the overall single surgery success rate (SSSR) in 312 eyes. It could therefore be safely assumed that inclusion of the small group with silicone oil at the last follow-up visit did not affect the overall success rate significantly, but reduced chances of introducing a selection bias.

In our series a supplemental encircling scleral buckle (SB) (42 silicone band) was used in 34% of the eyes. Throughout the study there was a decreasing trend in the use of supplemental SB while the outcomes remained stable. This has been discussed in detail in a sequel publication5. Dr. Shukla comments, “the optional use of scleral buckle in this study is confusing”. It is clear from the data that good anatomic outcomes may be achieved with PPV without vitreous base (VB) shaving in both PPV and PPV+SB groups. The author further states “the vitreous base-shaving is critical to anatomical success when no encirclage is used”. This is an assumption that is not supported by the findings of our study: 195 (94.7%) of 206 eyes without SB had reattachment of the retina with a single surgery. The reference that is provided is a retrospective series of RDs that underwent PPV and silicone oil between 2000 and 2012, many of which were presumably performed without the use of small gauge vitrectomy or WAVS3. The study retrospectively identified vitreous remnants during retinal re-detachment surgery and equated this finding to inadequate VB shaving rather than inadequate vitreous removal. Using WAVS, it is possible to visualize the retina periphery to the vicinity of the VB and remove the peripheral vitreous effectively without a need for scleral depressed shaving of the VB6. Removal of clinically significant peripheral vitreous without VB shaving avoids leaving significant amounts of vitreous remnant and is compatible with good anatomic success rate. Dr. Shukla states “the authors reported no additional benefit from buckling”. We reported, “the single-surgery success rate was similar in eyes with and without SB (95.2% and 94.7%)” and cautioned against comparative interpretation of these findings as eyes with SB likely had more complex retinal detachments. Dr. Shukla further comments “We therefore do not have clarity about the one moot issue this study could settle: whether vitrectomy sans base-shaving is good enough for simple RD at least”. The answer to this comment-question is clear: Using WAVS and small gauge vitrectomy systems, vitrectomy without routine prophylactic scleral depressed shaving of VB may be associated with good anatomic outcomes (95% SSSR) for retinal detachments with a range of complexities including simple RDs2.

A recent report by Sohn and colleagues detailed the characteristics and outcomes of retinal detachment surgery for eyes with posteriorly inserted vitreous base (PIVB)7. The authors suggested encircling endolaser photocoagulation or supplemental scleral buckle in these cases. In our series, PIVB was noted in a minority of cases. In these cases encircling endolaser photocoagulation was performed posterior to the insertion of the vitreous base with additional septate pattern in each quadrant. Supplemental SB was considered if retinal detachment with multiple tears was present inferiorly. While a thorough removal of peripheral vitreous makes clinical sense, there is no evidence in the literature that shaving of the vitreous base improves anatomic outcomes in cases with PIVB.

In our series, GRTs measured from 3 to 11 clock hours, with the majority measuring between 4-6 clock hours. Proliferative vitreoretinopathy ranged from none to funnel retinal detachment. Seven (50%) of 14 eyes with GRT had supplemental SB, 11 (79%) eyes had silicone oil tamponade, and 2 of the 8 phakic eyes had removal of cataractous lens in order to improve visualization. At the last follow-up, silicone oil was present in 3 eyes. Dr. Shukla comments that vitreous base shaving is considered non-negotiable in a GRT and references a review article on GRT by Shunmugam and colleagues 8. The article cites 2 studies published in 1981 and 1992 in support of shaving of the vitreous base in the management of RD associated with GRT9, 10. Interestingly, within the same section, it is stated “opposite the GRT, however, because of the adherence of the vitreous base, limited vitrectomy is advisable to avoid circumferential extension of the GRT or the formation of further retinal breaks”. It appears that shaving of the vitreous base has uncertain merit for these cases. In the area corresponding to GRT, the VB is partly removed during removal of the anterior flap of the GRT and the remainder covers the surface of pars plana. In the area outside of the GRT, retinal laser photocoagulation applied posterior to the VB margin reduces risk of retinal detachment originating from this area.

In summary, introduction of 3-port pars plana vitrectomy in the 1970s transformed management of retinal detachment. Some of the early reports suggested that shaving of the VB may be associated with improved outcomes. Since the early days of PPV, many advances have been made including the introduction of endolaser photocoagulation, perfluorocarbon heavy liquid, WAVS, sclerotomy cannula systems, fast cutting small gauge vitrectomy systems, high precision microinstrumentation, chromophore-assisted visualization of the vitreous and preretinal membranes, and effective ocular anti-inflammatory pharmacotherapy. With continued advances in vitrectomy surgery, there is a need for reevaluation and modification of our surgical techniques.

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.

We read with interest the study by Özsaygili et al. in which the authors report that the presence or absence of posterior vitreous detachment (PVD) purportedly had no influence on the efficacy of aflibercept intravitreal injections in patients with diabetic macular oedema (DMO). We question the validity of this conclusion since it is known that eyes with attached vitreous require more injections to manage exudative age-related macular degeneration than eyes with PVD.1 This is presumed to be due to interference with macular access by anti-vascular endothelial growth factor (anti-VEGF) by the posterior vitreous cortex. The same mechanism of action could be expected in eyes with DMO. Thus, there may be alternative explanations for the observed lack of an effect of PVD status on the response to aflibercept. We hypothesize that the findings are due to both the unreliable diagnosis of PVD by spectral domain optical coherence tomography (SD-OCT) alone, and the possible presence of vitreoschisis.

Previous studies have shown that SD-OCT is not a robust way to diagnose PVD, since the positive predictive value is only approximately 50%.2, 3 Rather, ultrasound is the recommended way to detect complete PVD (Figure 1).2 Did Özsaygili et al. perform ultrasound in their patients? If not, they would be unable to determine true PVD status, and the validity of their conclusion needs to be called into question.

Additionally, it is unclear from the study by Özsaygili et al. whether vitreoschisis, defined as a split within the posterior vitreous cortex (Figure 2), was observed or documented. Although SD-OCT has the ability to detect vitreoschisis4–6, “what we see depends mainly on what we look for”, as Sir John William Lubbock once wrote. If there were cases in the series assembled by Özsaygili et al. with anomalous PVD and vitreoschisis, this could be incorrectly diagnosed as PVD, and the access of aflibercept into the macula may have been hindered by the outer wall of the vitreoschisis cavity (Figure 2), giving another reason for the false impression that PVD plays no role on aflibercept response in patients with diabetic macular oedema.

In conclusion, we agree with Sir Lubbock that we see what we seek and thus invite the authors to re-examine their data with the foregoing in mind.

References:
1. Sebag J. Vitreous in age-related macular degeneration therapy - The medium is the message. Retina. 2015;35(9):1715-1718. doi:10.1097/IAE.0000000000000718.
2. Hwang ES, Kraker JA, Griffin KJ, Sebag J, Weinberg D V, Kim JE. Accuracy of Spectral-Domain OCT of the Macula for Detection of Complete Posterior Vitreous Detachment. Ophthalmol Retin. 2020;4(2):148-153. doi:10.1016/j.oret.2019.10.013.
3. Abraham JR, Ehlers JP. Posterior Vitreous Detachment: Methods for Detection. Ophthalmol Retin. 2020;4(2):119-121. doi:10.1016/j.oret.2019.12.014.
4. Sebag J. Vitreoschisis. Graefe’s Arch Clin Exp Ophthalmol. 2008;246(3):329-332. doi:10.1007/s00417-007-0743-x.
5. Gupta P, Yee KMP, Garcia P, et al. Vitreoschisis in macular diseases. Br J Ophthalmol. 2011;95(3):376-380. doi:10.1136/bjo.2009.175109.
6. Sebag J. Vitreoschisis in diabetic macular edema. Invest Ophthalmol Vis Sci. 2011;52(11):8455-8456. doi:10.1167/iovs.11-8333.