Ovarian stimulation with follitropin delta for in vitro fertilization: a multicentre, randomized, assessor-blind comparison with follitropin alfa using conventional dosing regimens (ADAPT-1 trial)

IF 6 1区医学 Q1 OBSTETRICS & GYNECOLOGY

Human reproduction Pub Date : 2025-07-09 DOI:10.1093/humrep/deaf119

Andrea Bernabeu, Philipp Zajc, Marta García Sánchez, Rina Agrawal, Enrico Papaleo, Stefan Jirecek, Signe Møgelmose, Ida Engberg Jepsen, Rita Lobo

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WHAT IS KNOWN ALREADY Follitropin delta, a recombinant FSH (rFSH), is currently approved for ovarian stimulation using an individualized fixed daily dose based on serum anti-Müllerian hormone (AMH) and bodyweight (maximum 12 µg/day for first cycle and 24 µg/day in subsequent cycles). Other rFSHs, such as follitropin alfa, conventionally apply a starting dose of 150–225 IU, fixed for the initial days of stimulation, after which dose adjustments can be made (maximum 450 IU/day). Ovarian stimulation with follitropin delta 10 µg/day provides a similar ovarian response to follitropin alfa 150 IU/day for serum concentration and number of follicles ≥12 mm. STUDY DESIGN, SIZE, DURATION ADAPT-1 was a randomized, accessor-blinded, multicentre trial comparing efficacy and safety of a starting dose of follitropin delta 15 µg/day with follitropin alfa 225 IU/day in conventional dosing regimens. The primary endpoint was the number of oocytes retrieved; mean difference between treatment groups was estimated using a negative binomial regression model (treatment and serum AMH level as factors). During the follow-up period, clinical pregnancies resulting from the first fresh/frozen transfers within 3 months of the start of stimulation, and ovarian hyperstimulation syndrome (OHSS) rates were assessed. PARTICIPANTS/MATERIALS, SETTING, METHODS Participants, 18–40 years, undergoing IVF/ICSI could enrol at specialist reproductive clinics in Austria, France, Italy, Spain, and the United Kingdom for ovarian stimulation if they had no contraindications for treatment with a starting gonadotropin dose of 225 IU/day. Patients could enrol if they reported infertility for at least 1 year if ≤37 years and at least 6 months for those &gt;37 years, and regular menstrual cycles (21–35 days). All cycles used a GnRH antagonist protocol. MAIN RESULTS AND THE ROLE OF CHANCE Between 1 August 2022 and 16 April 2024, 300 of 337 screened patients were randomized to, and received, follitropin delta (n = 200) or follitropin alfa (n = 100). The two treatment groups were comparable in terms of demographics, baseline characteristics, and duration of infertility. The mean duration of treatment was ∼9 days in both groups. The mean total dose of follitropin delta was 143.7 ± 33.6 µg and 154.3 ± 23.1 µg (2105 ± 315 IU) for follitropin alfa. Three-quarters (226/300) used an human Chorionic Gonadotropin trigger for final follicular maturation. A mean of 9.9 oocytes was retrieved for both groups (estimated difference: 0.0 oocytes; 95% CI −1.3, 1.2). The category of 8–14 oocytes retrieved was the most common ovarian response (follitropin delta: 45.5%; follitropin alfa: 50.0%). Clinical pregnancy rates were comparable (31.6% and 31.0%; estimated difference 0.6 (95% CI −10.6, 11.8)). Early OHSS (≤9 days after triggering) occurred in 2.5% and 3.0%, and all cases were Grade 3 (moderate) or lower. No participant had the stimulation cycle cancelled due to excessive ovarian response. LIMITATIONS, REASONS FOR CAUTION Only pregnancies from the first fresh or cryopreserved transfer within 3 months of oocyte retrieval were recorded. Cumulative pregnancy rates after the first transfer were not followed up. All analyses are of descriptive nature and no formal hypothesis testing or multiplicity adjustment was applied. WIDER IMPLICATIONS OF THE FINDINGS Treatment groups had similar ovarian responses, supporting equivalence for starting doses follitropin delta 15 µg and follitropin alfa 225 IU, with low rates of early OHSS. Ovarian stimulation cycles with follitropin delta in µg can be planned and adjusted, leveraging the established IU dose equivalence to follitropin alfa. STUDY FUNDING/COMPETING INTEREST(S) This trial was funded by Ferring Pharmaceuticals A/S, Kastrup, Denmark. Medical writing support for manuscript development was provided by Celia J. Parkyn, PhD, and was funded by Ferring Pharmaceuticals A/S, Kastrup, Denmark. P.Z. and R.A. have none. A.B. has received grants from Gedeon Richter, IBSA, GP Pharm & Seid, Miguel Hernandez University, Centre for Technological Development and Innovation, Valencian Innovation Agency, Regional Secretary for Industry, Trade and Consumption, and the Government Ministry of Industry and Tourism; payments from University Complutense of Madrid, Ferring Pharmaceuticals, Fentypharm, Miguel Hernandez University, Gedeon Richter, & Vall d’Hebron Hospital; travel support from Ferring Pharmaceuticals, Fentypharm, Gedeon Richter, International ESHRE Congress Organising Committee, Spanish Society of Gynaecology and Obstetrics, CROG Congress Organising Committee, & Vall d’Hebron Hospital; has a patent pending for Sperm plate (U202431456); and is Chair of the Organising Committee of the Infertility and Sterility Section of the Spanish Society of Gynaecologist (non-paid role) and equipment from Obstetrics; & equipment from Cook Medical. J.S. has received consulting fees from Ferring Pharmaceuticals. 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引用次数: 0

Abstract

STUDY QUESTION How do ovarian responses using conventional dosing for follitropin delta 15 µg/day compare with follitropin alfa 225 IU/day in women undergoing ovarian stimulation? SUMMARY ANSWER The ADAPT-1 trial demonstrates similar ovarian responses with follitropin delta 15 µg/day and follitropin alfa 225 IU/day starting doses in a conventional dosing regimen. WHAT IS KNOWN ALREADY Follitropin delta, a recombinant FSH (rFSH), is currently approved for ovarian stimulation using an individualized fixed daily dose based on serum anti-Müllerian hormone (AMH) and bodyweight (maximum 12 µg/day for first cycle and 24 µg/day in subsequent cycles). Other rFSHs, such as follitropin alfa, conventionally apply a starting dose of 150–225 IU, fixed for the initial days of stimulation, after which dose adjustments can be made (maximum 450 IU/day). Ovarian stimulation with follitropin delta 10 µg/day provides a similar ovarian response to follitropin alfa 150 IU/day for serum concentration and number of follicles ≥12 mm. STUDY DESIGN, SIZE, DURATION ADAPT-1 was a randomized, accessor-blinded, multicentre trial comparing efficacy and safety of a starting dose of follitropin delta 15 µg/day with follitropin alfa 225 IU/day in conventional dosing regimens. The primary endpoint was the number of oocytes retrieved; mean difference between treatment groups was estimated using a negative binomial regression model (treatment and serum AMH level as factors). During the follow-up period, clinical pregnancies resulting from the first fresh/frozen transfers within 3 months of the start of stimulation, and ovarian hyperstimulation syndrome (OHSS) rates were assessed. PARTICIPANTS/MATERIALS, SETTING, METHODS Participants, 18–40 years, undergoing IVF/ICSI could enrol at specialist reproductive clinics in Austria, France, Italy, Spain, and the United Kingdom for ovarian stimulation if they had no contraindications for treatment with a starting gonadotropin dose of 225 IU/day. Patients could enrol if they reported infertility for at least 1 year if ≤37 years and at least 6 months for those >37 years, and regular menstrual cycles (21–35 days). All cycles used a GnRH antagonist protocol. MAIN RESULTS AND THE ROLE OF CHANCE Between 1 August 2022 and 16 April 2024, 300 of 337 screened patients were randomized to, and received, follitropin delta (n = 200) or follitropin alfa (n = 100). The two treatment groups were comparable in terms of demographics, baseline characteristics, and duration of infertility. The mean duration of treatment was ∼9 days in both groups. The mean total dose of follitropin delta was 143.7 ± 33.6 µg and 154.3 ± 23.1 µg (2105 ± 315 IU) for follitropin alfa. Three-quarters (226/300) used an human Chorionic Gonadotropin trigger for final follicular maturation. A mean of 9.9 oocytes was retrieved for both groups (estimated difference: 0.0 oocytes; 95% CI −1.3, 1.2). The category of 8–14 oocytes retrieved was the most common ovarian response (follitropin delta: 45.5%; follitropin alfa: 50.0%). Clinical pregnancy rates were comparable (31.6% and 31.0%; estimated difference 0.6 (95% CI −10.6, 11.8)). Early OHSS (≤9 days after triggering) occurred in 2.5% and 3.0%, and all cases were Grade 3 (moderate) or lower. No participant had the stimulation cycle cancelled due to excessive ovarian response. LIMITATIONS, REASONS FOR CAUTION Only pregnancies from the first fresh or cryopreserved transfer within 3 months of oocyte retrieval were recorded. Cumulative pregnancy rates after the first transfer were not followed up. All analyses are of descriptive nature and no formal hypothesis testing or multiplicity adjustment was applied. WIDER IMPLICATIONS OF THE FINDINGS Treatment groups had similar ovarian responses, supporting equivalence for starting doses follitropin delta 15 µg and follitropin alfa 225 IU, with low rates of early OHSS. Ovarian stimulation cycles with follitropin delta in µg can be planned and adjusted, leveraging the established IU dose equivalence to follitropin alfa. STUDY FUNDING/COMPETING INTEREST(S) This trial was funded by Ferring Pharmaceuticals A/S, Kastrup, Denmark. Medical writing support for manuscript development was provided by Celia J. Parkyn, PhD, and was funded by Ferring Pharmaceuticals A/S, Kastrup, Denmark. P.Z. and R.A. have none. A.B. has received grants from Gedeon Richter, IBSA, GP Pharm & Seid, Miguel Hernandez University, Centre for Technological Development and Innovation, Valencian Innovation Agency, Regional Secretary for Industry, Trade and Consumption, and the Government Ministry of Industry and Tourism; payments from University Complutense of Madrid, Ferring Pharmaceuticals, Fentypharm, Miguel Hernandez University, Gedeon Richter, & Vall d’Hebron Hospital; travel support from Ferring Pharmaceuticals, Fentypharm, Gedeon Richter, International ESHRE Congress Organising Committee, Spanish Society of Gynaecology and Obstetrics, CROG Congress Organising Committee, & Vall d’Hebron Hospital; has a patent pending for Sperm plate (U202431456); and is Chair of the Organising Committee of the Infertility and Sterility Section of the Spanish Society of Gynaecologist (non-paid role) and equipment from Obstetrics; & equipment from Cook Medical. J.S. has received consulting fees from Ferring Pharmaceuticals. E.P. has received grants from Merck, Ferring, Theramex, Gedeon Richter, IBSA, and Organon; payments from Merck, Ferring, IBSA, and Organon; travel support from Merck, IBSA, Organon, Theramex, and Ferring; and participated in a Safety Monitoring Board or Advisory Board for Merck. M.G.S. has received patient medication from Ferring; payments from Ferring, Merck for educational events; and travel support from Ferring, Merck, Theramex, and IBSA. R.L. and S.M. are employees of Ferring Pharmaceuticals. I.E.J. was an employee of Ferring Pharmaceuticals at the time of the trial conduct. TRIAL REGISTRATION NUMBER clinicaltrials.gov NCT05263388; Eudract 2021-001785-38 TRIAL REGISTRATION DATE 16 November 2021 (clinicaltrials.gov); 5 August 2021 (Eudract) DATE OF FIRST PATIENT’S ENROLMENT 1 August 2022

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促卵泡素δ刺激卵巢用于体外受精：与常规给药方案促卵泡素α的多中心、随机、评估盲比较（ADAPT-1试验）

研究问题：在接受卵巢刺激的女性中，使用常规剂量的促卵泡素δ 15 μ g/天与使用常规剂量的促卵泡素α 225 IU/天相比，卵巢反应如何？ADAPT-1试验显示，在常规给药方案中，起始剂量为卵泡素δ 15 μ g/天和卵泡素α 225 IU/天的卵巢反应相似。Follitropin delta是一种重组卵泡刺激素（rFSH），目前已被批准用于卵巢刺激，使用基于血清抗<s:1>勒氏激素（AMH）和体重的个体化固定日剂量（第一个周期最大12 μ g/天，后续周期最大24 μ g/天）。其他rFSHs，如卵磷脂α，通常应用150-225 IU的起始剂量，在刺激的最初几天固定，之后可以进行剂量调整（最大450 IU/天）。在血清浓度和卵泡数量≥12 mm时，卵泡素δ 10µg/天的卵巢刺激与卵泡素α 150 IU/天的卵巢反应相似。ADAPT-1是一项随机、随机盲法、多中心试验，比较在常规给药方案中，起始剂量为15 μ g/天的卵泡素δ和起始剂量为225 IU/天的卵泡素α的疗效和安全性。主要终点是获得的卵母细胞数量；使用负二项回归模型（治疗和血清AMH水平为因素）估计治疗组之间的平均差异。在随访期间，评估了刺激开始后3个月内首次新鲜/冷冻移植导致的临床妊娠，以及卵巢过度刺激综合征（OHSS）的发生率。参与者/材料，环境，方法18-40岁，接受IVF/ICSI的参与者，如果他们没有起始剂量为225 IU/天的促性腺激素治疗禁忌症，可以在奥地利，法国，意大利，西班牙和英国的专业生殖诊所登记进行卵巢刺激。如果患者报告不孕至少1年（≤37年），至少6个月（≤37年），并且月经周期正常（21-35天），则可以入选。所有周期使用GnRH拮抗剂方案。在2022年8月1日至2024年4月16日期间，337名筛选的患者中有300名被随机分配并接受了卵泡素δ (n = 200)或卵泡素α (n = 100)。两个治疗组在人口统计学、基线特征和不孕症持续时间方面具有可比性。两组患者的平均治疗时间为~ 9天。α卵磷脂的平均总剂量为154.3±23.1µg(2105±315 IU)， δ卵磷脂为143.7±33.6µg。四分之三（226/300）使用人绒毛膜促性腺激素触发最终卵泡成熟。两组平均回收9.9个卵母细胞(估计差异：0.0个卵母细胞；95% ci−1.3,1.2)。8-14个卵母细胞是最常见的卵巢反应(卵泡素δ: 45.5%；卵泡素α: 50.0%)。临床妊娠率比较(31.6%和31.0%；估计差异0.6 (95% CI−10.6,11.8))。早期OHSS（触发后≤9天）发生率分别为2.5%和3.0%，所有病例均为3级（中度）及以下。没有参与者因卵巢反应过度而取消刺激周期。限制，注意原因仅记录了在卵母细胞取出后3个月内首次新鲜或冷冻移植的妊娠。第一次移植后的累积妊娠率没有随访。所有的分析都是描述性的，没有正式的假设检验或多重性调整。研究结果的更广泛意义治疗组具有相似的卵巢反应，支持起始剂量卵泡素δ 15 μ g和卵泡素α 225 IU的等效性，早期OHSS发生率低。卵泡素δ (μ g)刺激卵巢周期可以计划和调整，利用已建立的IU剂量与卵泡素α等效。研究经费/竞争利益(S)本试验由丹麦Kastrup的Ferring Pharmaceuticals A/S资助。手稿开发的医学写作支持由Celia J. Parkyn博士提供，由丹麦Kastrup的Ferring Pharmaceuticals A/S资助。P.Z.和R.A.没有。他还是曾获得Gedeon Richter、IBSA、GP Pharm &amp；Seid、米格尔·埃尔南德斯大学、技术发展和创新中心、巴伦西亚创新局、工业、贸易和消费区域秘书以及政府工业和旅游部；来自马德里康普顿斯大学、Ferring制药公司、Fentypharm公司、Miguel Hernandez大学、Gedeon Richter等的付款；瓦尔德希布伦医院；Ferring Pharmaceuticals, Fentypharm, Gedeon Richter，国际ESHRE大会组委会，西班牙妇产科学会，CROG大会组委会，&amp；瓦尔德希布伦医院；精子板专利申请（U202431456）；并担任西班牙妇科医生协会不孕不育科组织委员会主席（无薪角色）和产科设备；,库克医疗公司的设备J.S.已收到Ferring Pharmaceuticals的咨询费。E.P.获得了Merck、Ferring、Theramex、Gedeon Richter、IBSA和Organon的资助；默克、fering、IBSA和Organon的付款；Merck、IBSA、Organon、Theramex和Ferring的差旅支持；并参加了默克公司的安全监督委员会或咨询委员会。M.G.S.已经从费林那里接受了病人的药物治疗；默克公司为教育活动支付的费用；以及来自Ferring、Merck、Theramex和IBSA的差旅支持。R.L.和S.M.是Ferring制药公司的员工。在进行试验时，I.E.J.是费林制药公司的雇员。试验注册号：clinicaltrials.gov NCT05263388；试验注册日期2021年11月16日（clinicaltrials.gov）；第一位患者入组日期2022年8月1日

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来源期刊

Human reproduction 医学-妇产科学

CiteScore

10.90

自引率

6.60%

发文量

1369

审稿时长

1 months

期刊介绍： Human Reproduction features full-length, peer-reviewed papers reporting original research, concise clinical case reports, as well as opinions and debates on topical issues. Papers published cover the clinical science and medical aspects of reproductive physiology, pathology and endocrinology; including andrology, gonad function, gametogenesis, fertilization, embryo development, implantation, early pregnancy, genetics, genetic diagnosis, oncology, infectious disease, surgery, contraception, infertility treatment, psychology, ethics and social issues.