Research Question: To evaluate the immunogenicity of follitropin delta in repeated ovarian stimulation.
Design: Controlled, assessor-blind trial in IVF/intracytoplasmic sperm injection patients undergoing repeated cycles of ovarian stimulation (cycles 2 and 3), following initial stimulation with follitropin delta or follitropin alfa (cycle 1) in a preceding randomized trial. In cycles 2 and 3, 513 and 188 women, respectively, were treated as randomized in cycle 1, with dosing based on ovarian response in the previous cycle.
Results: The incidence of treatment-induced anti-FSH antibodies with follitropin delta was 0.8% and 1.1% in cycles 2 and 3, respectively, which was similar to the incidence in cycle 1 (1.1%). No antibodies were of neutralizing capacity. Women with pre-existing anti-FSH antibodies were safely treated with follitropin delta without boosting an immune response. Treatment with follitropin delta and follitropin alfa gave similar outcomes for mean number of oocytes retrieved (9.2 versus 8.6 [cycle 2]; 8.3 versus 8.9 [cycle 3]), ongoing pregnancy (27.8% versus 25.7%; 27.4% versus 28.0%) and live birth rates (27.4% versus 25.3%; 26.3% versus 26.9%). The presence of anti-FSH antibodies did not affect the ovarian response.
Conclusions: The trial demonstrated the low immunogenicity potential of follitropin delta in repeated ovarian stimulation, and confirmed the appropriateness of the follitropin delta dosing regimen in repeated cycles, with documented efficacy and safety.
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Article Synopsis
- - The study focused on optimising controlled ovarian stimulation (COS) for IVF by personalising treatment plans based on individual patient factors like medical history and ovarian reserve.
- - Researchers implemented a protocol using a novel hormone, follitropin delta, in combination with human menotrophin (HP-hMG) and tailored doses for 20 patients, evaluating outcomes such as clinical pregnancy rate (CPR).
- - Results showed a high CPR of 70% per started cycle, with no cycle cancellations or safety issues like ovarian hyperstimulation syndrome, indicating a promising risk-benefit balance for this mixed protocol in IVF.
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