Fetal Presentation of MYRF-Related Cardiac Urogenital Syndrome: An Emerging and Challenging Prenatal Diagnosis.

IF 2.7 2区 医学 Q2 GENETICS & HEREDITY
Prenatal Diagnosis Pub Date : 2024-11-14 DOI:10.1002/pd.6700
Maud Favier, Elise Brischoux-Boucher, Louise C Pyle, Nicolas Mottet, Marion Auber-Lenoir, Julie Cattin, Eric Dahlen, Christelle Cabrol, Francine Arbez-Gindre, Tania Attié-Bitach, Odile Boute, Louise Devisme, Detlef Trost, Aicha Boughalem, David Chitayat, Lev Prasov, Odelia Chorin, Annick Rein-Rothschild, Eran Kassif, Tal Weissbach, Laura Godfrey Hendon, Margaret P Adam, Chloé Quelin, Sylvie Jaillard, Laura Mary, Sietse M Aukema, Malou Heijligers, Christine de Die-Smulders, Sander Stegmann, Lauren Badalato, Adi Ben-Yehuda, Claire Beneteau, Pierre-Louis Forey, Paul Kuentz, Juliette Piard
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引用次数: 0

Abstract

Purpose: MYRF-related cardiac-urogenital syndrome (MYRF-CUGS) is a rare condition associated with heterozygous MYRF variants. The description of MYRF-CUGS phenotype is mostly based on postnatal cases and 36 affected individuals have been published so far. We aim now to delineate the prenatal phenotype of MYRF-CUGS by reporting clinical data from fetuses and neonates with a pathogenic MYRF variant.

Methods: Detailed radiographic, pathological, clinical, and molecular data from 12 prenatal cases were collected through an international collaborative study. Adding the five fetuses previously published, we were able to study a cohort of 17 cases.

Results: Main ultrasound-accessible manifestations of MYRF-CUGS include congenital heart defects (13/17, 76%), congenital diaphragmatic hernia (10/17, 59%) and disorders of sexual differentiation in 46, XY fetuses (7/14; 50%). Postnatal examination and/or autopsy data highlighted additional birth defects and neurological findings with a large spectrum of severity. Molecular results revealed ten previously unpublished variants, one missense and nine predicted truncating variants (three frameshift, three nonsense and three splice site variants).

Conclusion: We report the first prenatal cohort of MYRF-CUGS, allowing us to further characterize the variable expressivity of this rare disorder in fetuses. Severe congenital anomalies with a poor prognosis are more frequent than previously described in postnatal cases. Our data suggest that MYRF-CUGS is characterized by a recurrent recognizable malformative association, accessible to prenatal diagnosis, with a significant intrafamilial phenotypic variability making genetic counseling challenging.

与 MYRF 相关的心脏泌尿系统综合征的胎儿表现:一种新出现且极具挑战性的产前诊断。
目的:MYRF相关心脏-先天性综合征(MYRF-CUGS)是一种与杂合子MYRF变异相关的罕见病。对 MYRF-CUGS 表型的描述大多基于出生后的病例,迄今为止已发表了 36 例受影响的个体。现在,我们旨在通过报告具有致病性MYRF变异体的胎儿和新生儿的临床数据,描述MYRF-CUGS的产前表型:方法:我们通过一项国际合作研究收集了12例产前病例的详细放射学、病理学、临床和分子数据。加上之前发表的 5 个胎儿,我们共研究了 17 个病例:结果:MYRF-CUGS 的主要超声表现包括先天性心脏缺陷(13/17,76%)、先天性膈疝(10/17,59%)和 46 XY 胎儿的性分化障碍(7/14;50%)。产后检查和/或尸检数据突出显示了严重程度不一的其他先天缺陷和神经系统发现。分子研究结果显示了 10 个以前未发表的变异,1 个错义变异和 9 个预测的截断变异(3 个移帧变异、3 个无义变异和 3 个剪接位点变异):结论:我们报告了首例MYRF-CUGS产前队列,使我们能够进一步确定这种罕见疾病在胎儿中的不同表达特性。在产后病例中,预后不良的严重先天畸形比以往描述的更为常见。我们的数据表明,MYRF-CUGS 的特点是反复出现可识别的畸形关联,可进行产前诊断,但家族内的表型变异很大,这给遗传咨询带来了挑战。
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来源期刊
Prenatal Diagnosis
Prenatal Diagnosis 医学-妇产科学
CiteScore
5.80
自引率
13.30%
发文量
204
审稿时长
2 months
期刊介绍: Prenatal Diagnosis welcomes submissions in all aspects of prenatal diagnosis with a particular focus on areas in which molecular biology and genetics interface with prenatal care and therapy, encompassing: all aspects of fetal imaging, including sonography and magnetic resonance imaging; prenatal cytogenetics, including molecular studies and array CGH; prenatal screening studies; fetal cells and cell-free nucleic acids in maternal blood and other fluids; preimplantation genetic diagnosis (PGD); prenatal diagnosis of single gene disorders, including metabolic disorders; fetal therapy; fetal and placental development and pathology; development and evaluation of laboratory services for prenatal diagnosis; psychosocial, legal, ethical and economic aspects of prenatal diagnosis; prenatal genetic counseling
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