Evaluating the Efficacy and Safety of Aflibercept Biosimilar (P041) Compared with Originator Product in Patients with Neovascular Age-Related Macular Degeneration

NCT05587062 | Not reported | Karkhaneh R et al. (2024)

Karkhaneh, R., Faghihi, H., Riazi-Esfahani, H., Abrishami, M., Bazvand, F., Ebrahimiadib, N., Johari, M., Akhlaghi, M., Shoeibi, N., Norouzzadeh, M. H., et al. Evaluating the Efficacy and Safety of Aflibercept Biosimilar (P041) Compared with Originator Product in Patients with Neovascular Age-Related Macular Degeneration. Ophthalmology Retina, 2024; 8:744-753.

Locations

12 medical centers in Iran

Study Period

October 2019 – July 2022

Study Design

Phase III, multicenter, randomized, double-masked, active control trial

Study Population

Characteristic:

Type of AMD:

2 (Wet AMD)

AMD Stage:

3 (Late)

Total Sample Size:

168 randomized (P041: 84, Aflibercept: 84)

Age:

Phase III, multicenter, randomized, double-masked, active control trial

Sex (Male) n%:

105 (62.5%)

Experimental Group

Intervention Therapy:

P041 (Aflibercept biosimilar) 2 mg

Dose & Frequency:

Three loading doses (Weeks 0, 4, 8), then every 8 weeks up to Week 48

Age (Years):

68.6 ± 6.9

Number of Patients:

Male N %:

58 (69.1%)

Patients Followed Up:

72 completed at 52 weeks

Control Group

Intervention Therapy:

Aflibercept (AFL) 2 mg

Dose & Frequency:

Three loading doses (Weeks 0, 4, 8), then every 8 weeks up to Week 48

Age (Years):

68.3 ± 6.2

Number of Patients:

Male N %:

47 (55.9%)

Patients Followed Up:

73 completed 52 weeks

Follow-up Time: 52 weeks

Outcomes

Durability

N/A

Vision

Maintaining Vision
Primary Outcome: the proportion of patients maintaining vision (a loss of < 15 letters) at week 52:
• 94.4% in the P041 group compared with 94.5% in the AFL group.
• The 95% confidence interval (CI) for the difference in maintaining vision from baseline did not exceed the predefined noninferiority margin of 10% (difference=-0.0008; 95% CI: 0.074 to 0.074; P = 0.98).
Mean Change in BCVA (ETDRS Letters)
The mean changes from baseline to week 52:
• P041: +7.95 (SD 17.61)
• AFL: +6.91 (SD 12.98)
• Difference = -0.13 (95% CI: -4.79 to 4.53, p = 0.96)
Proportion Gaining ≥15 Letters
The percentage of eyes with BCVA gain ≥15 letters from week 0 to week 52
• P041: 33.7% vs. AFL: 25.3% (p = 0.23)

Other

N/A

Immunognicity

One patient in P041 group tested positive for antidrug antibodies at Week 52 but maintained visual and anatomic response.

Pharmokinetics

Not reported

Anatomic

Change in Central Subfield Thickness (CST)
At week 52:
• P041: -167.3 µm (SD 189.1)
• Aflibercept: -148.4 µm (SD 109.6)
• Difference = -1.68 (95% CI: -40.4 to 37.0, p = 0.93).
Intraretinal fluid (IRF) and subretinal fluid (SRF)
• At the end of the study, the percentages of patients with no IRF or SRF were 63.75% and 54.88% in the P041 and Aflibercept patients, respectively (P = 0.25).
• In the P041 group, 61.25% exhibited the resolution of IRF at week 12 based on OCT, whereas in the Aflibercept group, 64.63% showed IRF resolution.
• SRF was resolved in 73.75% of patients in the P041 group and 69.51% in the Aflibercept group.

Safety

Patients experienced ≥ 1 AE
• P041= 47/84, 55.9%
• Aflibercept= 44/84, 52.4%
Any ocular AE
• P041= 38/84, 45.2%
• Aflibercept= 36/84, 42.8%
Any Nonocular AE
• P041= 30/84, 35.7%
• Aflibercept= 25/84, 29.8%
Serious AEs
Total event number:
• P041: 9 cases
• Aflibercep: 12 cases
Patients with ocular SAEs:
• P041= 2/84, 2.4%
• Aflibercept= 1/84, 1.2%
Patients with non-ocular SAEs:
• P041= 5/84, 6.0%
• Aflibercept= 5/84, 6.0%

Outcomes

Conclusion

P041 demonstrated non-inferiority to originator aflibercept, with similar efficacy, safety, and immunogenicity profiles at 52 weeks, supporting its use as a biosimilar treatment for nAMD.

Risk of Bias Assessment for Primary Outcome

Randomization Process

Low risk

Note: Randomization “using block randomization (with block sizes of 2 or 4) for generated by R-CRAN software version 3.2.3.” and baseline characteristics look balanced.

Missing Outcome Data

Low risk

Note: Evidence that the result was not biased by missing outcome data: “To conduct a sensitivity analysis for the primary end point, the primary analysis was performed using both per-protocol (PP) and intention-to-treat (ITT) sets.”

Selection of the Reported Results

Low risk Note: Registration with protocol

Deviations from Intended Observations

Low risk Note: “…all patients, clinical investigators, and data assessors were masked...”and ITT principle applied for the primary analysis.

Measurement of the Outcome

Some concerns Note: “…all patients, clinical investigators, and data assessors were masked...” As this is a multiple site study, the assessment for the primary outcome may exist difference. However, assessment of the outcome unlikely to be influenced by knowledge of intervention received

Overall

Some Concerns