A treat and extend protocol with Aflibercept for cystoid macular oedema secondary to central retinal vein occlusion – an 18-month prospective cohort study

Treatment consisted of intravitreal injections of 2 mg of aflibercept (Eylea; Bayer Healthcare, Leverkusen, Germany) using a treat-and-extend protocol. An intravitreal injection of aflibercept was given at each study visit. All patients received three loading doses at 4-week intervals. After the loading period, the interval between study visits could be extended by 2 weeks at each visit, to a maximum of 12 weeks, if there was no clinical activity (see below for definition). If clinical activity was present at the end of the loading period, the interval between study visits was kept at 4 weeks until there was no clinical activity and then an attempt to extend the interval was made. Clinical activity was defined as any of:

The primary outcome measures were the change in BCVA from baseline and the proportion of patients gaining 15 or more ETDRS letters at 6, 12 and 18 months. Data was presented as the mean ± standard deviation (SD) when normally distributed or as median [interquartile range] (IQR) if not. Normality was assessed using the Shapiro-Wilks test. Descriptive statistics were performed of the baseline characteristics, visual and anatomical outcomes, treatment experience and venous closing pressure. The visual and anatomical outcomes were compared to the COPERNICUS and GALILEO trials in line graphs. To assess the predictive value of baseline characteristics on visual outcomes, a linear regression was applied. The dependent variable was change in ETDRS letters at 18 months from baseline. The independent variables were the measured baseline characteristics. For the regression analysis, baseline CMT was divided by 10. The resulting odds ratios were per 10 μm difference in baseline CMT. The difference in visual and anatomical outcomes at 18 months between patients that required a short or long interval between injections and less or more injections was assessed. For these analyses, patients were stratified into groups of less than the median, or, the median or more injection interval and number of injections. The homogeneity of variances between two groups was assessed using Levene’s test. Differences in continuous variables were compared using a student’s t-test or the Mann-Whitney U test for normally and not normally distributed data, respectively. Differences in proportions were analysed using Fisher’s exact test. All analyses were performed on a ‘per-protocol’ basis: patients lost to follow up were excluded from analyses at time points after they left the study.

The mean BCVA was 73.7 ± 9.6 letters, 74.9 ± 8.9 letters and 74.7 ± 10.1 letters at 6, 12 and 18 months respectively. Thus, the mean gain in BCVA from baseline was 19.7 ± 13.8 ETDRS letters at 6 months, 22.2 ± 13.9 ETDRS letters at 12 months and 21.9 ± 15.8 ETDRS letters at 18 months.

Sixty-five percent of patients (13 of 20 patients) gained 15 or more ETDRS letters at 6 months, 70.6% (12 of 17 patients) at 12 months and 70.6% (12 of 17 patients) at 18 months. The mean change in the CMT was − 476 ± 312 μm at 6 months, − 542 ± 277 μm at 12 months and – 534 ± 300 μm at 18 months.

Patients received on average 5.0 [4.0 to 6.0] injections by 6 months (range 4 to 6), 8.5 [8.0 to 10.3] injections by 12 months (range 7 to 13) and 11.0 [9.0 to 12.5] injections by 18 months (range 8 to 16) in the study, Fig. 1. The minimum number of injections possible during the 18-month period of the trial was 7 and the maximum was 19. The median injection interval was 7.0 [6.0 to 8.0] weeks, 8.0 [6.0 to 12.0] weeks and 10.0 [6.0 to 12.0] weeks at 6, 12 and 18 months, respectively. The percentages of patients at each injection interval at 6, 12 and 18 months are shown in Table 3. During the first year, an attempt to extend the interval between injections was made in all patients. The median time from baseline at which patients first met criteria for the interval between injections to be extended was 12.0 [8.0 to 20.0] weeks (range 8 to 28). Seventeen of 20 (85%) patients were extended at or before the sixth study visit. In those that were extended, the median time at which first recurrence occurred was 30.0 [22.0 to 38.0] weeks (range 14 to 68), with the median interval being 8.0 [6.0 to 10.0] weeks (range 6 to 12).

Three of 17 (17.6%) were successfully extended to a 12-week interval between injections without recurrence of disease activity by 12 months and thus it was possible to cease injections. These patients were followed and none experienced recurrent disease activity by 18 months. Of the patients who were unable to be extended without the development of recurrent CMO and reduction in BCVA during the first 12 months, 13 patients met the criteria for a second attempt to extend the interval between injections at the 12 month visit. In nine of these (69%), it was possible to extend the interval between injections, including 6 (46%) that did not have a further recurrence by 18 months.

In comparison with the COPERNICUS and GALILEO pivotal trials, the baseline characteristics of the patients in our study were well matched to the patients in those studies (Supplementary Table 1), although our patients had a higher baseline CMT and a smaller proportion of patients were considered to be perfused. Fig. 2 depicts the mean BCVA gain and the mean change in CMT in our patients as compared to COPERNICUS and GALILEO patients at month 6, 12 and 18 [3, 6‐8, 10, 11]. The visual and anatomical results in this cohort appears to be similar to those of COPERNICUS and GALILEO during the monthly dosing period (6 months) of those studies and may be superior in the PRN periods (12 and 18 months). (Fig. 2) The number of injections patients received in our study was similar to those of COPERNICUS and GALILEO. In COPERNICUS, patients in the initial aflibercept arm received 6 loading doses and then 6.0 ± 3.4 injections from weeks 24 to 100 [7]. In GALILEO, patients in the initial aflibercept arm received 5.7 ± 0.9 injections between baseline and 24 weeks, 2.5 ± 1.7 injections between weeks 24 and 52 and 1.3 ± 1.1 injections between weeks 52 and 78 [10].

Eyes with poor baseline visual acuity (20/200 or less) had a greater proportion with a 15-letter gain and a similar rate achieving driving vision (20/40) at 18 months as compared to eyes with good baseline vision (20/80 or more). Four of 4 (100%) patients with baseline visual acuity of 20/200 or less had a 15-letter gain at 18 months versus 4 of 9 (44%) with a baseline visual acuity of 20/80 or more. Three of 4 (75%) patients with baseline visual acuity of 20/200 or less achieved driving vision (20/40) at 18 months versus 6 of 9 (66%) with a baseline visual acuity of 20/80 or more. Similarly, patients with worse baseline visual acuity had a greater improvement in vision at 18 months in the linear regression model. None of the other measured baseline characteristics, including perfusion status, was correlated to improvement in vision. (Supplementary Table 2).

The visual and anatomical outcomes after 18 months of treatment with aflibercept when stratified by the interval between injections is shown in Table 4.

Regardless of the injection interval or the number of injections required by 18 months visual and anatomical outcomes were similar in patients who required more intensive treatment (8 weeks) compared to those who needed less intensive treatment (≥10 weeks). Similarly, the number of injections given by 18 months also had no influence on visual or anatomical outcomes.

CVP was measured in 15 patients at the visit at which they first met the criteria to be extended; it was high in 9 (60%), medium in 1 (7%) and low in 5 (33%) patients. A reduction in CVP from the highest recorded prior to the time of first extension occurred in only 3 (20%) patients. At the visit at which clinical activity recurred, CVP was measured in 14 patients; it was high in 7 (50%), medium in 2 (17%) and low in 5 (33%). There had been an increase in CVP from the study visit prior to recurrence in 1 (7%) patient.

There were no events of endophthalmitis, retinal tears or retinal detachments during the study period. Four serious adverse events (SAEs) occurred, none were related to study treatment. Two SAEs were reported in a 77 year-old female patient; a lumbar spine compression fracture 5 weeks after her 7th injection and an exacerbation of bronchiectasis 2 weeks after her 10th injection. A 72 year-old female developed microbial keratitis in the non-study eye 4 weeks after her 12th injection. A 57 year-old male patient had abdominal pain requiring admission 4 days after his 4th injection.