The usefulness of the retinal sensitivity measurement with a microperimetry for predicting the visual prognosis of branch retinal vein occlusion with macular edema

Retinal vein occlusions (RVOs) are one of the most common retinal vascular diseases [1]. In RVOs, such as branch RVO (BVO), patient’s sights are threatened by various associated complications, including macular edema (ME). ME in RVOs is usually treated with the intravitreal injection of anti-vascular endothelial growth factor (anti-VEGF) agents as the first-line therapy [2‐6]. The identification and quantitative evaluation of ME have been greatly enhanced with the development of optical coherence tomography (OCT) [2], and the treatment strategies are usually decided basing on both of visual acuity (VA) and OCT-measured ME thickness after the anti-VEGF treatment. It should be noted that BCVA mainly reflects visual function only around fovea, whereas ME impairs visual function not only at fovea but also in a surrounding area. Agreeing with this, previous studies suggested that retinal sensitivity measured with perimetry is associated with OCT-measured macular structural change, using the Humphrey Field Analyzer (HFA, Carl-Zeiss Meditec AG, Dublin, CA, USA) [3] and the MP1 Microperimeter (Nidek CO., LTD, Aichi, Japan) [7] in eyes with RVO with ME. In addition, the improvement of visual functional (BCVA and retinal sensitivity) is significantly associated with morphological (OCT-measured retinal thickness) improvement in RVO and ME eyes after the intravitreal anti-VEGF treatment [7]. Moreover, a recent study suggested that the retinal sensitivity measured with a microperimetry of MAIA (Center Vue, Padova, Italy) 1 day after the anti-VEGF treatment was significantly related with BCVA at 1 month in eyes with BVO with ME, suggesting the potential usefulness of retinal sensitivity in predicting the BCVA prognosis [8], although it was not investigated whether it is useful to measure retinal sensitivity, in addition to BCVA.

The MP-3 microperimeter (Nidek CO., LTD, Aichi, Japan) is a relatively new perimetry instrument. In contrast to its predecessor of the MP-1, the MP-3 has a wide dynamic range (between 0 and 34 dB) on the background luminance of 31.5 ASB which is identical to that with the HFA. Furthermore, in this microperimeter, the target light is projected onto the retina directly, rather than on a screen like in the HFA, which enables automatic tracking of retina. As a result, the exact same location can be stimulated in repeated target presentations. We previously reported visual retinal sensitivity measured with MP-3 has a better test-retest reproducibility than HFA in patients with retinitis pigmentosa (RP) [9] and glaucoma [10]. This advantage of MP-3 would be more pronounced in the eyes with ME, because the damage in central retina would hamper the fixation of an eye during the VF measurement. Thus, the purpose of the current study was to investigate whether it is advantageous to measure the retinal sensitivity using MP-3, in addition to BCVA, to predict the prognosis of BCVA, in eyes with BVO with ME following the anti-VEGF treatment.

This was a retrospective study and the procedures were approved by the Research Ethics Committee of the Graduate School of Medicine and Faculty of Medicine at The University of Tokyo (#3770). Written consent was given by patients for their information to be stored in the hospital database and used for research. This study was performed according to the tenets of the Declaration of Helsinki.

Table 1 shows the subjects’ demographics. The mean (± standard deviation: SD) age was 68.9 ± 7.2 (range 52 to 79) years, and 9 patients were male and 11 patients were female. BCVAbase was 0.13 ± 0.21 (− 0.079 to 0.7), MSbase was 22.7 ± 2.2 (17.2 to 26.7) dB, and MVbase was 2.8 ± 0.37 (2.3 to 3.7) mm³. CRTbase was 330.6 ± 135.2 (164 to 622) μm. qMSbase was 19.6 ± 3.3 (12.8 to 26) dB. qMVbase was 1.0 ± 0.24 (0.73 to 1.6) mm³. Among 20 eyes, qMV was in the superior quadrant in 8 eyes, whereas it was in the inferior quadrant in 12 eyes.

There was not a significant difference in BCVAbase and BCVA1m (p = 0.058, paired Wilcoxon test). However, significant differences were observed between BCVAbase and BCVA3m (p = 0.033) and between BCVAbase and BCVA12m (p = 0.002). On the other hand, there was a significant difference between MSbase and MS1m, MVbase and MV1m, CRTbase and CRT1m, qMSbase and qMS1m, and qMVbase and qMV1m (paired Wilcoxon test, p = 0.0017, < 0.001, < 0.001, < 0.001 and < 0.001, respectively).

There was a significant negative relationship between BCVAbase and MSbase (coefficient = − 0.050, p = 0.014, linear regression) and between BCVAbase and qMSbase (coefficient = − 0.032, p = 0.021, linear regression). Although a significant correlation was not observed between BCVA1m and MS1m (p = 0.10, linear regression), there was a significant relationship between ΔBCVA1m and ΔMS1m (coefficient = − 0.038, p = 0.048, linear regression) and ΔBCVA1m and ΔqMS1m (coefficient = − 0.028, p = 0.048, linear regression).

Table 2 shows the relationships between the values of CRT and MV and the variables of BCVAbase, MSbase, qMSbase, and age. qMSbase was significantly related to CRTbase (coefficient = − 52.7, p = 0.014, linear regression). The relationships between CRT1m and the variables of BCVA1m, MS1m, qMS1m, and age are also shown in Table 2. There was no parameter significantly related to CRT1m. qMSbase was significantly related to MVbase (coefficient = − 0.14, p = 0.0093, linear regression). There was no parameter significantly related to MV1m.

As shown in Table 3, qMSbase was significantly related to qMVbase (coefficient = − 0.077, p = 0.033, linear regression). There was no parameter significantly related to qMV1m.

Figure 3 shows the relationships between ΔBCVA1m and ΔMV1m, and between ΔBCVA1m and ΔCRT1m; significant relationship was not observed (p = 0.053 and 0.17, linear regression, respectively). Similar result was obtained with the multivariable regression analysis (Table 4).

As shown in Fig. 4, there was no significant relationship between ΔMS1m and ΔMV1m, and between ΔMS1m and ΔCRT1m (p = 0.067 and 0.22, respectively, linear regression). Similar result was obtained with the multivariable regression analysis (Table 4). In contrast, as shown in Fig. 5, significant relationship was observed between ΔqMS1m and ΔMV1m (ΔqMS = 0.85–4.7 x ΔMV, p = 0.0024), between ΔqMS1m and ΔCRT 1 m (ΔqMS = 1.76–0.01 x ΔCRT, p = 0.015), and between ΔqMS1m and ΔqMV1m (ΔqMS = 1.13–6.72 x ΔqMV, p = 0.0047). Similar result was obtained with the multivariable regression analysis (Table 4).

As a result of AICc model selection for BCVA3m using the variables of BCVAbase, ΔBCVA1m, MSbase, ΔMS1m, integrity of EZ, the frequency of the injection of anti-VEGF, and age, only BCVAbase, ΔBCVA1m, and ΔMS1m were selected in the optimal model for BCVA3m: BCVA3m = 0.036 + 0.88 x BCVAbase (standard error: SE = 0.085, p < 0.001) + 0.76 x ΔBCVA1m (SE = 0.13, p < 0.001) − 0.022 x ΔMS1m (SE = 0.0095, p = 0.032): AICc = − 42.1. Removing ΔMS1m from this optimal model resulted in a significant decrease of the loglikelihood (AICc = − 39.8, p = 0.033, ANOVA).

As a result of AICc model selection for BCVA3m using the variables of BCVAbase, ΔBCVA1m, qMSbase (instead of MSbase), ΔqMS1m (instead of ΔMS1m), integrity of EZ, the frequency of the injection of anti-VEGF and age, only the optimal model was BCVA3m = 0.041 + 0.90 x BCVAbase (SE = 0.086, p < 0.001) + 0.79 x ΔBCVA1m (SE = 0.13, p < 0.001) − 0.014 x ΔqMS1m (SE = 0.0070, p = 0.053): AICc = − 41.0. Removing ΔqMS1m from this model did not result in a significantly decreased log-likelihood, although it approached a significance (AICc = − 39.8, p = 0.053, ANOVA).

In the current study, retinal sensitivity measurement with MP-3 microperimetry was performed in patients with BVO and ME before and after the anti-VEGF treatment, along with OCT measurement. As a result, the change of retinal sensitivity was correlated with retinal volume especially in the affected quadrant; on the other hand, visual acuity was not correlated with retinal structure. Moreover, retinal sensitivity change at 1 month was significantly related to BCVA at 3 months after anti-VEGF treatment, indicating the usefulness of the measurement of retinal sensitivity to predict visual acuity.

This usefulness of the measurement of retinal sensitivity would be further validated by the association with OCT-measured retinal thicknesses; significant relationships were observed between ΔqMS1m and ΔMV1m, ΔqMV1m, and ΔCRT1m whereas this was not the case between ΔBCVA1m and any OCT parameter. Kriechbaum et al. also investigated BCVA, mean retinal sensitivity using MP-1, and OCT-measured retinal volume at 12 months after anti-VEGF treatments in patients with macular edema secondary to retinal vein occlusion [7]. These values were significantly improved compared with baseline, and moreover, BCVA and mean retinal sensitivity were significantly correlated with mean central retinal thickness, but not with retinal volume.

There have been many studies which suggested the usefulness of the anti-VEGF therapy in eyes with BVO with ME [5‐8, 15‐19]. For instance, Mylonas et al. have reported that BCVA improved significantly at 3 months and 12 months after the anti-VEGF therapy in patients with BVO [15]. Fujihara-Mino et al. also suggested that BCVA significantly improved 1 month after the anti-VEGF therapy in patients with BVO [16]. However, in contrast to these previous studies, in the current study, BCVA did not significantly improve 1 month after anti-VEGF treatment, although the difference approached a significance (p = 0.058). This reason for the contradicting result is entirely unknown, but in the current study, BVO patients were consecutively recruited and the majority of patients had already received anti-VEGF treatments prior to the initiation of the study. In contrast to BCVA, MS and qMS significantly improved at 1 month after anti-VEGF treatment, suggesting retinal sensitivity might improve earlier than BCVA.

Sugimoto et al. [8] suggested retinal sensitivity using MAIA at 1 day after the intravitreal bevacizumab was correlated with BCVA at 1 month in patients with BVO. Agreeing with this report [8], our results suggested that the retinal sensitivity at 1 month is a useful predictive factor of BCVA at 3 months, which was consistent with the previous report. More specifically, as a result of model selection, the optimal model for BCVA3m included BCVAbase, ΔBCVA1m, and ΔMS1m or ΔqMS1m. Thus, retinal sensitivity measurement using the MP-3 was useful to precisely predict the prognosis of BCVA.

One of the possible limitations of the current study was that the onset of BVO was not known in all patients, and the period from onset was not included in the analysis. The second limitation of the current study was the exclusion of the eyes with ischemic cases. Manabe et al. reported the association between parafoveal capillary nonperfusion and retinal sensitivity in eyes with resolved BVO patients. They concluded mean retinal sensitivity at the capillary non-perfusion area was significantly lower than that at the capillary perfusion area [20]. It would be of interest that whether retinal sensitivity measurement is also useful in such cases; however, the purpose of the current study was to investigate the usefulness of measuring retinal sensitivity in eyes with BVO and ME, and it was beyond the purpose of the current study. Also, BCVA prognosis was observed up to 3 months, and a longer observation would be needed in a future study.

In conclusion, there was a significant improvement in retinal sensitivity measured with MP-3 microperimetry in BVO patients with ME, whereas no improvement was observed in BCVA at 1 month after anti-VEGF injection. Retinal sensitivity measured with MP-3 was closely related to the OCT-measured structural change after the anti-VEGF treatment, whereas this was not the case with BCVA. The current results suggest the usefulness of the evaluation of the retinal sensitivity in eyes with BVO and ME.