Incidence and risk factors of monozygotic twinning following ART: analysis of 154 671 live births resulting from single embryo transfer.

IF 6 1区 医学 Q1 OBSTETRICS & GYNECOLOGY
Repon C Paul,Christos A Venetis,Oisin Fitzgerald,Georgina M Chambers
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Previous studies have suggested younger maternal age, blastocyst culture, fresh embryo transfer, and certain ART techniques, such as assisted hatching and preimplantation genetic testing may elevate MZT risk. However, findings have been inconsistent, and with many prior studies underpowered and few reflecting contemporary ART practices.\r\n\r\nSTUDY DESIGN, SIZE, DURATION\r\nThis retrospective cohort study analyzed data from 590 441 SET cycles conducted between 2009 and 2021 in Australia and New Zealand. The analysis included 154 671 live births following autologous SET cycles recorded in the Australian and New Zealand Assisted Reproductive Technology Database (ANZARD).\r\n\r\nPARTICIPANTS/MATERIALS, SETTING, METHODS\r\nThe study focused on autologous fresh and thawed SET cycles. MZT incidence was estimated by applying Weinberg's differential rule, which assumes a 1:1 ratio of sex-concordant and sex-discordant dizygotic twins in the population of twins born following SET cycles. A multivariable logistic regression model with generalized estimating equations was used to identify risk factors for MZT, adjusting for potential misclassification of zygosity due to the absence of DNA confirmation.\r\n\r\nMAIN RESULTS AND THE ROLE OF CHANCE\r\nThe MZT rate was 1.5% among live births following SET. Blastocyst transfer was associated with a nearly 2-fold increase in MZT risk compared to cleavage-stage transfer (adjusted odds ratio [aOR] = 1.99, 95% CI: 1.71-2.31), and vitrified-thaw transfers had a lower MZT risk than fresh transfers (aOR = 0.87, 95% CI: 0.79-0.95). Sensitivity analyses supported these findings, with consistent MZT risk patterns across subgroups by maternal age, fertilization technique, and embryo transfer type (fresh/frozen).\r\n\r\nLIMITATIONS, REASONS FOR CAUTION\r\nZygosity estimation was based on Weinberg's differential rule rather than DNA testing, which could lead to some misclassification. Additionally, the study lacked data on embryo quality, a variable with potential influence on MZT risk, and was limited to a retrospective design, potentially introducing treatment and information biases.\r\n\r\nWIDER IMPLICATIONS OF THE FINDINGS\r\nThis large-scale study identifies blastocyst transfer and fresh embryo transfer as significant MZT risk factor in ART, with potential implications for patient counseling and obstetric care. Future research should further investigate the mechanisms underlying these associations.\r\n\r\nSTUDY FUNDING/COMPETING INTEREST(S)\r\nFunding was received from the Ferring Pharmaceuticals Pty Ltd as part of the Ferring FSANZ Leaders in Fertility Research and Education grant (to R.C.P.). The sponsors had no role in the design and conduct of the study; data collection, management, analysis, and interpretation; manuscript preparation, review, or approval; or the decision to submit for publication. FSANZ contracts National Perinatal Epidemiology and Statistics Unit (NPESU) of the University of New South Wales (UNSW) to prepare annual reports and benchmarking reports from the ANZARD: one of those datasets is used in this study. R.C.P. is a Research Fellow of the NPESU, UNSW; C.A.V. is affiliated with the NPESU, UNSW; G.M.C. is an employee of the UNSW and is the Director of the NPESU, UNSW. C.A.V., based at Aristotle University of Thessaloniki (Greece), is a member of the Executive Board of the Hellenic Society of Fertility and Sterility and serves as Senior Deputy of the Steering Committee for the SIG Reproductive Endocrinology of ESHRE. C.A.V. also reports lecture and advisory roles from Merck Ltd, Merck Sharpe & Dohme, Ferring, Organon, Gedeon-Richter, IBSA, Vianex, and Sonapharm; travel support from Merck Ltd, Merck Sharpe & Dohme, Ferring, Organon, Gedeon-Richter, and Vianex; and holds stock or stock options in Virtus Health Ltd, all outside the submitted work. O.F. reports funding from Ferring Pharmaceuticals Pty Ltd, unrelated to this study.\r\n\r\nTRIAL REGISTRATION NUMBER\r\nN/A.","PeriodicalId":13003,"journal":{"name":"Human reproduction","volume":"51 1","pages":""},"PeriodicalIF":6.0000,"publicationDate":"2025-06-30","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Human reproduction","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.1093/humrep/deaf121","RegionNum":1,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"OBSTETRICS & GYNECOLOGY","Score":null,"Total":0}
引用次数: 0

Abstract

STUDY QUESTION What is the incidence of and risk factors for monozygotic twinning (MZT) following single embryo transfer (SET) in ART cycles in Australia and New Zealand? SUMMARY ANSWER MZT occurred in 1.5% of live births following SET, with blastocyst transfer and fresh embryo transfer identified as key risk factors, while vitrified-thaw transfers were associated with a lower MZT risk. WHAT IS KNOWN ALREADY ART has been associated with a higher incidence of MZT compared to natural conception. Previous studies have suggested younger maternal age, blastocyst culture, fresh embryo transfer, and certain ART techniques, such as assisted hatching and preimplantation genetic testing may elevate MZT risk. However, findings have been inconsistent, and with many prior studies underpowered and few reflecting contemporary ART practices. STUDY DESIGN, SIZE, DURATION This retrospective cohort study analyzed data from 590 441 SET cycles conducted between 2009 and 2021 in Australia and New Zealand. The analysis included 154 671 live births following autologous SET cycles recorded in the Australian and New Zealand Assisted Reproductive Technology Database (ANZARD). PARTICIPANTS/MATERIALS, SETTING, METHODS The study focused on autologous fresh and thawed SET cycles. MZT incidence was estimated by applying Weinberg's differential rule, which assumes a 1:1 ratio of sex-concordant and sex-discordant dizygotic twins in the population of twins born following SET cycles. A multivariable logistic regression model with generalized estimating equations was used to identify risk factors for MZT, adjusting for potential misclassification of zygosity due to the absence of DNA confirmation. MAIN RESULTS AND THE ROLE OF CHANCE The MZT rate was 1.5% among live births following SET. Blastocyst transfer was associated with a nearly 2-fold increase in MZT risk compared to cleavage-stage transfer (adjusted odds ratio [aOR] = 1.99, 95% CI: 1.71-2.31), and vitrified-thaw transfers had a lower MZT risk than fresh transfers (aOR = 0.87, 95% CI: 0.79-0.95). Sensitivity analyses supported these findings, with consistent MZT risk patterns across subgroups by maternal age, fertilization technique, and embryo transfer type (fresh/frozen). LIMITATIONS, REASONS FOR CAUTION Zygosity estimation was based on Weinberg's differential rule rather than DNA testing, which could lead to some misclassification. Additionally, the study lacked data on embryo quality, a variable with potential influence on MZT risk, and was limited to a retrospective design, potentially introducing treatment and information biases. WIDER IMPLICATIONS OF THE FINDINGS This large-scale study identifies blastocyst transfer and fresh embryo transfer as significant MZT risk factor in ART, with potential implications for patient counseling and obstetric care. Future research should further investigate the mechanisms underlying these associations. STUDY FUNDING/COMPETING INTEREST(S) Funding was received from the Ferring Pharmaceuticals Pty Ltd as part of the Ferring FSANZ Leaders in Fertility Research and Education grant (to R.C.P.). The sponsors had no role in the design and conduct of the study; data collection, management, analysis, and interpretation; manuscript preparation, review, or approval; or the decision to submit for publication. FSANZ contracts National Perinatal Epidemiology and Statistics Unit (NPESU) of the University of New South Wales (UNSW) to prepare annual reports and benchmarking reports from the ANZARD: one of those datasets is used in this study. R.C.P. is a Research Fellow of the NPESU, UNSW; C.A.V. is affiliated with the NPESU, UNSW; G.M.C. is an employee of the UNSW and is the Director of the NPESU, UNSW. C.A.V., based at Aristotle University of Thessaloniki (Greece), is a member of the Executive Board of the Hellenic Society of Fertility and Sterility and serves as Senior Deputy of the Steering Committee for the SIG Reproductive Endocrinology of ESHRE. C.A.V. also reports lecture and advisory roles from Merck Ltd, Merck Sharpe & Dohme, Ferring, Organon, Gedeon-Richter, IBSA, Vianex, and Sonapharm; travel support from Merck Ltd, Merck Sharpe & Dohme, Ferring, Organon, Gedeon-Richter, and Vianex; and holds stock or stock options in Virtus Health Ltd, all outside the submitted work. O.F. reports funding from Ferring Pharmaceuticals Pty Ltd, unrelated to this study. TRIAL REGISTRATION NUMBER N/A.
抗逆转录病毒治疗后单卵双胞胎的发生率及危险因素:单胚胎移植的154 671例活产分析。
研究问题:在澳大利亚和新西兰的ART周期中,单胚胎移植(SET)后单卵双胞胎(MZT)的发生率和危险因素是什么?SET后活产的MZT发生率为1.5%,囊胚移植和新鲜胚胎移植被确定为关键危险因素,而玻璃化解冻移植与较低的MZT风险相关。已知的是,与自然受孕相比,人工受孕与更高的MZT发生率有关。先前的研究表明,较年轻的母亲年龄、囊胚培养、新鲜胚胎移植和某些ART技术(如辅助孵化和植入前基因检测)可能会增加MZT的风险。然而,研究结果并不一致,许多先前的研究都不够有力,很少反映当代艺术实践。研究设计、规模、持续时间本回顾性队列研究分析了2009年至2021年在澳大利亚和新西兰进行的590441个SET周期的数据。该分析包括记录在澳大利亚和新西兰辅助生殖技术数据库(ANZARD)中的154 671例自体SET周期的活产婴儿。参与者/材料,设置,方法本研究集中于自体新鲜和解冻的SET循环。MZT发病率是通过应用Weinberg微分规则来估计的,该规则假设在SET周期后出生的双胞胎群体中,性别一致和性别不一致的异卵双胞胎比例为1:1。使用多变量逻辑回归模型和广义估计方程来识别MZT的危险因素,并调整由于缺乏DNA确认而可能导致的合子性错误分类。主要结果及偶然性的作用:随访的活产婴儿中MZT率为1.5%。与卵裂期移植相比,囊胚移植的MZT风险增加了近2倍(调整优势比[aOR] = 1.99, 95% CI: 1.71-2.31),玻璃化解冻移植的MZT风险低于新鲜移植(aOR = 0.87, 95% CI: 0.79-0.95)。敏感性分析支持这些发现,不同亚组的MZT风险模式与母亲年龄、受精技术和胚胎移植类型(新鲜/冷冻)一致。局限性,谨慎的原因合子估计是基于Weinberg的微分规则,而不是DNA测试,这可能会导致一些错误分类。此外,该研究缺乏胚胎质量的数据,这是一个对MZT风险有潜在影响的变量,并且仅限于回顾性设计,可能会引入治疗和信息偏差。这项大规模研究确定囊胚移植和新鲜胚胎移植是抗逆转录病毒治疗中重要的MZT风险因素,对患者咨询和产科护理具有潜在意义。未来的研究应进一步调查这些关联的机制。研究资金/竞争利益(S) Ferring Pharmaceuticals Pty Ltd作为Ferring FSANZ Leaders in Fertility Research and Education grants(给R.C.P.)的一部分,收到了Ferring Pharmaceuticals Pty Ltd的资金。赞助方在研究的设计和实施中没有任何作用;数据收集、管理、分析和解释;手稿的准备、审查或批准;或者决定提交出版。FSANZ与新南威尔士大学(UNSW)的国家围产期流行病学和统计部门(NPESU)签订合同,准备来自ANZARD的年度报告和基准报告:本研究使用了其中一个数据集。R.C.P.是新南威尔士大学NPESU的研究员;C.A.V.隶属于新南威尔士大学NPESU;G.M.C.是新南威尔士大学的雇员,也是新南威尔士大学NPESU的主任。c.a.v.,总部设在塞萨洛尼基亚里士多德大学(希腊),是希腊生育和不育学会执行委员会的成员,并担任ESHRE SIG生殖内分泌学指导委员会的高级副主席。C.A.V.还报道了默克有限公司、默沙东、Ferring、Organon、Gedeon-Richter、IBSA、Vianex和Sonapharm的讲座和顾问职位;来自Merck Ltd, Merck Sharpe & Dohme, Ferring, Organon, Gedeon-Richter和Vianex的差旅支持;并持有Virtus Health Ltd的股票或股票期权,所有这些都在提交的工作之外。O.F.报告来自Ferring Pharmaceuticals Pty Ltd的资金,与本研究无关。试验注册号/ a。
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来源期刊
Human reproduction
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.
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