Biosimilar SB11 versus reference ranibizumab in neovascular age‑related macular degeneration: 1‑year phase III randomised clinical trial outcomes

• NCT03150589 • EudraCT: 2017 000422 36 | Biosimilar SB11 versus reference ranibizumab in nAMD: 1‑year phase III randomised clinical trial outcomes | Bressler NM et al. (2023)

Bressler NM, Veith M, Hamouz J, et al. Biosimilar SB11 versus reference ranibizumab in neovascular age‑related macular degeneration: 1‑year phase III randomised clinical trial outcomes. Br J Ophthalmol 2023; 107:384–391. doi:10.1136/bjophthalmol-2021-319637

Locations

75 centres in 9 countries

Study Period

March 2018 to December 2019

Study Design

Randomised, double‑masked, parallel‑group, multicentre, 52‑week phase III clinical trial

Study Population

Characteristic:

Type of AMD:

2 (Wet AMD)

AMD Stage:

Neovascular AMD (advanced); specific staging not provided

Total Sample Size:

705 randomized

Age:

Randomised, double‑masked, parallel‑group, multicentre, 52‑week phase III clinical trial

Sex (Male) n%:

Not reported

Experimental Group

Intervention Therapy:

SB11 (ranibizumab biosimilar)

Dose & Frequency:

0.5 mg intravitreal injection every 4 weeks from baseline to week 48

Age (Years):

307

Number of Patients:

Approximately 351 in the full analysis set

Male N %:

74.4±8.0

Patients Followed Up:

149 (42.5%)

Control Group

Intervention Therapy:

Reference ranibizumab (RBZ, Lucentis)

Dose & Frequency:

0.5 mg intravitreal injection every 4 weeks from baseline to week 48

Age (Years):

327

Number of Patients:

Approximately 354 in the full analysis set

Male N %:

73.8±8.9

Patients Followed Up:

153 (43.2%)

Follow-up Time: 52 Weeks

Outcomes

Durability

Not reported

Vision

Best-corrected visual acuity (BCVA)
The least-squares mean (SE) changes in BCVA from baseline at week 8 (Primary Outcome):
• SB11: +6.2 letters (SE 0.5)
• RBZ: +7.0 letters (SE 0.5)
• The adjusted treatment difference between groups was −0.8 letters (90%CI, −1.8 to 0.2) letters

Changes in BCVA in the FAS at all times to week 24 were comparable between treatment groups:
• SB11: +9.8 letters (SE 0.8)
• RBZ: +10.4 letters (SE 0.7)
• Adjusted treatment difference: –0.6 letters (90% CI: –2.1 to 0.9) letters.

Vision Maintaining
Patients with <15 Letter Loss:
• SB11: 96.8%
• RBZ: 97.9%
• Adjusted difference: –1.2% (95% CI: –3.8 to 1.3)
Patients with ≥15 Letter Gain:
• SB11: 34.6%
• RBZ: 37.6%
• Adjusted difference: –3.2% (95% CI: –10.5 to 4.2)

Other

Quality of Life (QoL)
NEI VFQ- 25 Score
The mean change from baseline to week 52:
• SB11: 4.54
• RBZ: 6.47

Immunognicity

• The cumulative incidence of ADAs up to week 24 was low and similar between treatment groups (SB11, 10 of 330 [3.0%]; ranibizumab, 10 of 327 [3.1%]).
• A minority of ADA-positive participants had neutralizing antibodies.
• The incidence of ADAs and neutralizing antibodies by visit to week 24 was similar between treatment groups.

Pharmokinetics

Serum concentration profiles up to week 52 were comparable between SB11 and RBZ, with levels below the 11–27 ng/mL threshold required for 50% inhibition of VEGF‑A

Anatomic

Central Retinal Lesion Thickness (CRLT)
The least-squares mean (SE) changes in CRLT from baseline at week 52:
• SB11: –161 (5.1) μm
• RBZ: –149.5 (4.9) μm
• Difference: –11.5 μm (95% CI: –23.2 to 0.1)

Central Subfield Thickness (CST)
The least-squares mean (SE) changes in CST from baseline at week 52:
• SB11: –140.0 μm (SE 4.5)
• RBZ: –125.1 μm (SE 4.3)
• Adjusted treatment difference: –14.9 μm (95% CI: –25.3 to –4.5)

Choroidal Neovascularisation (CNV)
The least-squares mean (SE) changes in NV size from baseline at week 52:
• SB11: –5.2 mm² (SE 0.3
• RBZ: –4.6 mm² (SE 0.3)
• Difference: –0.6 mm² (95% CI: –1.2 to 0.1)

Patients with active CNV leakage:
• SB11: 158 (52.1%)
• RBZ: 185 (59.1%)
• Adjusted difference: –7.4% (95% CI: –15.0 to 0.2)

Safety

TEAEs
Patients with any TEAE:
• SB11: 72% vs RBZ: 72.3%
Ocular TEAEs in the study eye:
• SB11: 32% vs RBZ: 29.7%
Ocular TEAEs in the fellow eye:
• SB11: 26.3% vs RBZ: 21.8%
Non-ocular TEAEs:
• SB11: 55.4% vs RBZ: 57.9%
Patients with any serious TEAE:
• SB11: 14.3% vs RBZ: 14.4%

Serious AEs (SAEs)
Patients with any SAE
• SB11: 14.9% vs RBZ: 14.7%

Serious ocular AE (Study Eye)
Patients with any ocular SAE:
• SB11: 2.9% vs RBZ: 2.3%
Visual acuity reduced:
• SB11: 0.6% vs RBZ: 0.3%
Endophthalmitis:
• SB11: 0.6% vs RBZ: 0
Cataract:
• SB11: 0.6% vs RBZ: 0
Iridocyclitis:
• SB11: 0.3% vs RBZ: 0
Macular oedema:
• SB11: 0.3% vs RBZ: 0.3%
Retinal haemorrhage:
• SB11: 0.3% vs RBZ: 0.3%
Retinal pigment epithelial tear:
• SB11: 0.3% vs RBZ: 0
Subretinal fluid:
• SB11: 0.3% vs RBZ: 0.3%
Uveitis:
• SB11: 0.3% vs RBZ: 0
Vitritis:
• SB11: 0.3% vs RBZ: 0
Cataract subcapsular:
• SB11: 0 vs RBZ: 0.3%
Macular degeneration:
• SB11: 0.3% vs RBZ: 0.6%
Retinal artery occlusion:
• SB11: 0.3% vs RBZ: 0.3%

Serious ocular AE (Fellow eye)
Patients with any ocular SAE:
• SB11: 0.9% vs RBZ: 0.6%
Retinal haemorrhage:
• SB11: 0.6% vs RBZ: 0
Age- related macular degeneration:
• SB11: 0.3% vs RBZ: 0
Vitreous haemorrhage:
• SB11: 0.3% vs RBZ: 0
Choroidal neovascularisation:
• SB11: 0 vs RBZ :0.3%
Retinal artery occlusion:
• SB11: 0 vs RBZ: 02.3%

Serious non-ocular AE
Patients with any non-ocular SAE:
• SB11: 11.7% vs RBZ: 11.9%
Atrial fibrillation:
• SB11: 1.1% vs RBZ: 0.8%
Cardiac failure congestive:
• SB11: 0.6% vs RBZ: 0.6%
Pancreatitis acute:
• SB11: 0% vs RBZ: 0.6%
Cystitis:
• SB11: 0% vs RBZ: 0.6%
Femoral neck fracture:
• SB11: 0.3% vs RBZ: 0.6%
Acute kidney injury:
• SB11: 0.9% vs RBZ: 0.3%
Chronic obstructive pulmonary disease:
• SB11: 0.6% vs RBZ: 0
Hypertension:
• SB11: 0.9% vs RBZ: 0

TEAEs leading to IP discontinuation
Patients with any TEAEs leading to investigation production (IP) discontinuation:
• SB11: 2.6% vs RBZ: 1.4%
Ocular TEAEs in the study eye leading to IP discontinuation:
• SB11: 2.0% vs RBZ: 1.0%
Ocular TEAEs in the fellow eye leading to IP discontinuation:
• SB11: 0 vs RBZ: 0
Non-ocular TEAEs leading to IP discontinuation:
• SB11: 0.6% vs RBZ: 0.3%

Death
• SB11: 0.6% vs RBZ: 1.1%

Outcomes

Conclusion

The 52‑week outcomes demonstrate that SB11 and RBZ have comparable efficacy, safety, immunogenicity, and pharmacokinetics profiles in patients with nAMD, thereby supporting the biosimilarity of SB11 to the reference ranibizumab product.

Risk of Bias Assessment for Primary Outcome

Randomization Process

Low risk

Note: “… participants were randomized in a 1:1 ratio (randomization blocks of fixed size=4) by the Interactive Web Response System (IWRS)…” “Baseline demographic and disease characteristics appeared comparable between the treatment groups”.

Missing Outcome Data

Low risk

Note: The evidence that the result was not biased by missing outcome data (sensitivity analysis): “The PK analysis set (PKS) included participants who had at least one PK sample analyzed”

Selection of the Reported Results

Low risk Note: registration with protocol.

Deviations from Intended Observations

Low risk Note: This is a double-masked study. mITT principle was applied as the primary outcome analysis using “the full analysis set (FAS)”.

Measurement of the Outcome

Some concerns Note: this is a double-masked study. However, as an international multiple-site study, the measurement of primary outcome may be inconsistent.

Overall

Some concerns