We warmly thank Calugaru D and associates for their correspondence regarding our article entitled " Early response to ranibizumab predictive of functional outcome after dexamethasone for unresponsive diabetic macular oedema".1
We agree with them about some of the challenges concerning our study. As we have acknowledged in the limitation section of our article, our study is limited by several biases, as its design was retrospective. In particular, patients selection and follow-up represented some of the major flaws in our study. We collected data about patients switched to dexamethasone for different reasons; some patients were treatment-naïve, other had already undergone treatments for diabetic macular edema (DME). No one disclosed any feature of chronic long-standing DME; all of them received prompt therapy after DME diagnosis.
Some of them showed a good response to ranibizumab loading-dose, with satisfying reduction of macular thickness after the injections. Nevertheless, no patient disclosed a completely dry macula after the anti-vascular endothelial growth factor (VEGF) loading-dose.
As far as it regards the final functional and anatomical gain at the end of the follow-up, the Authors state that the outcomes of this series were unsatisfactory. However, in the non-responders group, despite initial poor results, the best-corrected visual acuity (BCVA) had improved significantly (p<0.05) and clinically (> 5 letters), as highlighted in the text.
The analysis of central macular thickness (CMT) at 12 months on optical coherence tomography disclosed that the poor and good responders reached CMT of 363 microns and of 359 microns, respectively. Despite being more than the cutoff for the upper level of normal CMT, as suggested by the Authors, for DME eyes a CMT of ~350um should be considered as a good outcome, as values inferior to this cut-off would indicate impending atrophy of the neurovascular tissue. As a validation of our approach, we referred to the latest Diabetic Retinopathy Clinical Research Network (DRCR.net) guidelines about persistent macular thickening after ranibizumab treatment, according to which CMT appeared to be a less important prognostic factor in DME outcomes. In fact, persistent macular edema was associated with similar long-term improvement in visual acuity showed by patients in which DME did not persist.2 Finally, we would like to specify that we analyzed data of included patients until 12-months follow-up; these patients did not conclude treatment for DME, and most of them continued to receive injections for their condition.
We perfectly agree that, along with CMT, other OCT biomarkers (as disorganization of the retinal inner layers, integrity of the ellipsoid zone and of the cone outer segment tips, presence of taut internal limiting membrane or epiretinal membrane, and vitreomacular traction) should be analyzed in order to predict the prognostic outcome of diabetic patients.3-4 A specific analysis of these parameters was beyond our purposes, but we will include them in a future more complete stepwise linear regression analysis of the data presented in the present study.
We listed the complications of treatment experienced by patients who underwent dexamethasone (DEX) implant, with particular attention to intraocular pressure increase as well as cataract worsening. These two are well-known side-effects of dexamethasone implant and their rate did not exceed the expectations in our study.5 Despite these complications, intravitreal steroids have shown a good safety profile in long-term prospective studies, especially in those cases when anti-VEGF are contraindicated, or fewer intravitreal injections regimen is required.
In conclusion, we kindly disagree with the conclusion of the Authors and we further demonstrated the usefulness of switching the therapeutic drug in diabetic patients non-responders to anti-VEGF the by replying to this letter.

References:

1. Cicinelli MV, Cavalleri M, Querques L, et al. Early response to ranibizumab predictive of functional outcome after dexamethasone for unresponsive diabetic macular oedema. Br J Ophthalmol 2017; http:/ dx. doi. org/ 10.1136/bjophthalmol-2017-310242.

2. Bressler SB, Ayala AR, Bressler NM, Melia M, Qin H, Ferris FL 3rd, Flaxel CJ, Friedman SM, Glassman AR, Jampol LM, Rauser ME; Diabetic Retinopathy Clinical Research Network. Persistent Macular Thickening After Ranibizumab Treatment for Diabetic Macular Edema With Vision Impairment. JAMA Ophthalmol. 2016 Mar;134(3):278-85. doi: 10.1001/jamaophthalmol.2015.5346.

3. Sun JK, Lin MM, Lammer J, Prager S, Sarangi R, Silva PS, Aiello LP. Disorganization of the retinal inner layers as a predictor of visual acuity in eyes with center-involved diabetic macular edema. JAMA Ophthalmol. 2014 Nov;132(11):1309-16.

4. Iacono P, Parodi MB, Scaramuzzi M, Bandello F. Morphological and functional changes in recalcitrant diabetic macular oedema after intravitreal dexamethasone implant. Br J Ophthalmol. 2016 Sep 13. pii: bjophthalmol-2016-308726. doi: 10.1136/bjophthalmol-2016-308726.

5. Boyer DS, Yoon YH, Belfort R Jr, et al; Ozurdex MEAD Study Group. Three-year, randomized, sham-controlled trial of dexamethasone intravitreal implant in patients with diabetic macular edema. 2014;121:1904-1914.

Thank you for your interest in our publication entitled "Preoperative aqueous humour flare values do not predict proliferative vitreoretinopathy in patients with rhegmatogenous retinal detachment".

As per request, we would like to provide more details on our protocol.

As described in our discussion, centre 1 used the mean of ten correct measurements making sure these measurements did not differ more than 2 standard deviations from each other. In centre 2, seven correct measurements were recorded of which the highest and lowest value were discarded leaving an average of five measurements. A correct measurement meant that the background readings did not differ more than 15% (indicated by the code ‘BG’ on the output) and that single “cell/C” measurements were replaced by an additional measurement. In addition, measurements with a small signal to noise ratio (indicated by the code ‘s/n’) were avoided as much as possible. However, with low flare values this was not always feasible. The flare meters were located in a room with blinds (centre 1) and a room without windows (centre 2); computer screens and lights were turned off during measurements. Both flare meters were calibrated monthly to assure correct readings. We therefore believe that the included mean values are artefact free.

Despite the exclusion of patients with additional conditions such as AMD, CRVO and preoperative PVR grade C or higher, we did end up with patients with a preoperative flare value above 100 pc/ms. These measurements were accurate because they showed small SD’s (e.g. mean 263.8± SD 2.8; mean 196.5±SD 3.5; mean 162.0±SD 6.0) and flare was also visible upon slit lamp examination. Therefore, because these values do occur in patients with a rhegmatogenous retinal detachment we feel that inclusion of these measurements is mandatory.

However, excluding patients with a preoperative flare value above 100 pc/ms from our regression and ROC analyses – as is suggested by dr. Schaub and colleagues – did not significantly improve the results from either centre 1 or centre 2. Logistic regression centre 1: OR 1.013; p = 0.446, centre 2: OR 1.035; p = 0.028. Sensitivity and specificity at a cut-off of 15 pc/ms dropped to 78 and 39% in centre 1, and 36% and 77% in centre 2 (p = 0.051).

A possible explanation for the discrepancy with the previous reports is our low prevalence of postoperative PVR (7.5% and 6.2% respectively) compared to the previous reports. All previous reports included consecutive patients and found prevalences of 10.3%(1), 14.9%(2) and 20% (3). Both the positive predictive value (PPV) and the odds ratio (OR) are affected by the prevalence. This means that even with comparable sensitivity and specificity the PPV and the OR will be lower when the prevalence is lower. In addition, different reports used different definitions of postoperative PVR. We used reoperation due to epiretinal membranes and/or subretinal strands within six months of initial surgery, as did Schröder et al.(1) Hoerster et al. based their findings on PVR grade C at 3 months postoperatively. While ten patients developed PVR only four (6%) needed a reoperation.(2) It is unclear from the report whether all four patients had a flare value > 15 pc/ms but if this were the case this would give a PPV of 20% and OR of 8 instead of the reported 40% and 30. Conart et al. used PVR grade B and C at 6 months as the outcome. Moreover, they included 20% patients with preoperative PVR grade C which influenced the postoperative number of patients with PVR. Both studies included flare values > 100 pc/ms which confirms that high values are not uncommon.(2,3)

The predictive value of the flare value thus depends on the patient group that is targeted. Our results indicate that there is a large overlap in flare values which makes selecting those patient at high risk for developing postoperative PVR (according to our definition) inaccurate.(4) Dependent on the implications of a positive test result (flare value > 15pc/ms) we should decide whether a false discovery rate of 60-90% is acceptable.

We agree with dr. Schaub and collegues that identifying patients with an increased risk of PVR would be of great benefit in studies of the treatment of PVR by “enriching” the study population. Unfortunately, in our study, we have not been able to validate preoperative flare measurements for this purpose.
Recently, however, we have shown that postoperative flare measurements may have that potential (Mulder et al, non published data, presented at the NOG Maastricht, March 29 2017), and we encourage other groups to validate these findings.

References
1 Schroder S, Muether PS, Caramoy A, et al. Anterior chamber aqueous flare is a strong predictor for proliferative vitreoretinopathy in patients with rhegmatogenous retinal detachment. Retina 2012;32(1):38-42.
2 Hoerster R, Hermann MM, Rosentreter A, et al. Profibrotic cytokines in aqueous humour correlate with aqueous flare in patients with rhegmatogenous retinal detachment. Br.J.Ophthalmol. 2013;97(4):450-453.
3 Conart JB, Kurun S, Ameloot F, et al. Validity of aqueous flare measurement in predicting proliferative vitreoretinopathy in patients with rhegmatogenous retinal detachment. Acta Ophthalmol. 2016;.
4 Mulder VC, Kluft C, van Etten PG, et al. Higher vitreous concentrations of dabigatran after repeated oral administration. Acta Ophthalmol. 2017;.

Early response to ranibizumab predictive of functional outcome after dexamethasone for unresponsive diabetic macular oedema
Dan Calugaru, Mihai Calugaru
Department of Ophthalmology, Univ of Medicine Cluj-Napoca/Romania

Re: Early response to ranibizumab predictive of functional outcome after dexamethasone for unresponsive diabetic macular oedema. Cicinelli et al. Br J Ophthalmol 2017; http: /dx.doi. org/ 10.1136/bjophthalmol-2017-310242.

Dear Editor
We would like to address several challenges that have arisen from the study by Cicinelli et al (1), which can be specifically summarized below.
1. The study was retrospectively conducted, with a selection bias attributable to the heterogeneity of the patients included, for example, six patients were affected by the type 1 diabetes mellitus; eighteen eyes were phakic; twenty seven eyes underwent cataract extraction and intraocular lens implant; and thirteen eyes received grid macular photocoagulation for diabetic macular oedema (DME) prior to ranibizumab (RNB).
2. After undergoing three loading-dose intravitreal injections of RNB performed at fixed 4-week intervals for the first 12 weeks, all the patients regardless of functional and anatomical characteristics, were shifted to dexamethasone implant (DEX implant 0.7 mg; Ozurdex; Allergan, Irvine, California, USA) continued at 4-month intervals until stable best-corrected visual acuity (BCVA) was reached. However, nothing was stated as to whether there were patients with complete retinal dryness at week 12 and if so, why they were switched to dexamethasone implant.
3. In the assessment of the final results of this study we considered the current assertion that evaluation of outcomes has to be guided by anatomical measure data with visual changes as a secondary guide [2]. Accordingly, the final outcomes of this series were unsatisfactory. Specifically, despite a significant mean gain of 5.6 Early Treatment Diabetic Retinopathy Study (ETDRS) letters in BCVA score in poorly responding patients and an insignificant improvement of 2.1 ETDRS letters in patients with good visual response, the central macular thickness (CMT) decreased significantly to 363.6 microns and reduced insignificantly to 359 microns, in the poor and good responders, respectively. Of note, the both CMT values were more than the cutoff for the upper level of normal CMT [3], highlighting unresolved DME. Moreover, seven eyes developed intraocular pressure =/> 20 mm Hg, cataract progression was observed in nine among the phakic eyes (50%) during the study period, and two patients underwent cataract extraction after the dexamethasone implant. Importantly, persistence of unresolved macular oedema can permanently damage the outer retinal layers, leading to retinal fibrosis and macular atrophy, indicating that the disease process is still active and progressive, requiring further treatment with antiangiogenic agents.
4. As far as the potential prognosticatours of clinical outcome after dexamethasone implant are concerned, the following baseline characteristics should have been considered and included in a stepwise linear regression analysis along with those already presented, namely the subfoveal choroidal thickness, the qualitative status of the 4 outer retinal layers, the vitreoretinal interface abnormalities (vitreomacular adhesion/traction and epiretinal membrane), the diabetic retinopathy severity, the presence of macular ischemia on fluorescein angiography, and the duration of DME prior to therapy.
5. The specific anti-VEGF drugs (bevacizumab [Avastin; Genentech, South San Francisco, California, USA)/ranibizumab [Lucentis, Genentech]/aflibercept [Eylea; Regeneron Pharmaceuticals Inc, Tarrytown, New York, USA]) represent the front-line therapy for the treatment of DME but only the VEGF inhibition may not be sufficient to decrease inflammatory response. Therefore, addition of a non-specific anti-VEGF substance, ie. a corticosteroid implant, is mandatory. Both groups of anti-VEGF substances provide similar rates of vision improvement but with superior anatomic outcomes and fewer injections in the corticosteroid implant-treated eyes. However, more patients receiving the corticosteroid implant lose vision mainly due to cataract [4].
Altogether, the results of this study can not be validated and extrapolated because a stepwise linear regression analysis of the potential predictors of functional outcome was not carried out. Regardless of the anti-VEGF agents employed (bevacizumab/ranibizumab/aflibercept/ corticosteroid), the efficacy of therapy depends primarily on the promptness of the therapy after DME diagnosis [4,5].

References
1. Cicinelli MV, Cavalleri M, Querques L, et al. Early response to ranibizumab predictive of functional outcome after dexamethasone for unresponsive diabetic macular oedema. Br J Ophthalmol 2017; http:/ dx. doi. org/ 10.1136/bjophthalmol-2017-310242.
2. Freund KB, Korobelnik JF, Devenyi R, et al. Treat-and-extend regimens with anti-VEGF agents in retinal diseases. Retina 2015;35(8):1489-1506.
3. Gover S, Murthy RK, Brar VS, Chalam KV.Normative data for macular thickness by high-definition spectral-domain optical coherence tomography (spectralis). Am J Ophthalmol 2009;148(2):266-271.
4. Calugaru D, Calugaru M. Real-world outcomes of ranibizumab treatment for diabetic macular edema in a United Kingdom National Health Service setting. Am J Ophthalmol 2017;174(2):175-176.
5. Calugaru D, Calugaru M. Comments to: Long-term efficacy and safety of intravitreal dexamethasone implant for the treatment of diabetic macular edema. Eur J Ophthalmol 2016;26(6):171-172.

Conflict of interest:
None declared