Prenatal diagnosis of SLC25A24 Fontaine progeroid syndrome: description of the fetal phenotype, genotype and detection of parental mosaicism

IF 1.6 4区 医学 Q4 DEVELOPMENTAL BIOLOGY
Emmanuelle Pannier, Abel Sekri, Nathalie Roux, Alexandre Vasiljevic, Laïla El Khattabi, Nicolas Chatron, Sarah Grotto, Delphine Menzella, Gilles Grangé, Florent Thébault, Jérôme Massardier, Cécile Fourrage, Laurence Lohmann, Vassilis Tsatsaris, Audrey Putoux, Lucile Boutaud, Tania Attié-Bitach
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Abstract

Background

Fontaine progeroid syndrome (FPS, OMIM 612289) is a recently identified genetic disorder stemming from pathogenic variants in the SLC25A24 gene, encoding a mitochondrial carrier protein. It encompasses Gorlin–Chaudry–Moss syndrome and Fontaine–Farriaux syndrome, primarily manifesting as craniosynostosis with brachycephaly, distinctive dysmorphic facial features, hypertrichosis, severe prenatal and postnatal growth restriction, limb shortening, and early aging with characteristic skin changes, phalangeal anomalies, and genital malformations.

Cases

All known occurrences of FPS have been postnatally observed until now. Here, we present the first two prenatal cases identified during the second trimester of pregnancy. While affirming the presence of most postnatal abnormalities in prenatal cases, we note the absence of a progeroid appearance in young fetuses. Notably, our reports introduce new phenotypic features like encephalocele and nephromegaly, which were previously unseen postnatally. Moreover, paternal SLC25A24 mosaicism was detected in one case.

Conclusions

We present the initial two fetal instances of FPS, complemented by thorough phenotypic and genetic assessments. Our findings expand the phenotypical spectrum of FPS, unveiling new fetal phenotypic characteristics. Furthermore, one case underscores a potential novel inheritance pattern in this disorder. Lastly, our observations emphasize the efficacy of exome/genome sequencing in both prenatal and postmortem diagnosis of rare polymalformative syndromes with a normal karyotype and array-based comparative genomic hybridization (CGH).

Abstract Image

SLC25A24 方丹早衰综合征的产前诊断:描述胎儿表型、基因型和检测亲本嵌合。
背景:方丹早衰综合征(FPS,OMIM 612289)是最近发现的一种遗传性疾病,源于编码线粒体载体蛋白的 SLC25A24 基因的致病变异。它包括戈林-考德里-莫斯综合征(Gorlin-Chaudry-Moss Syndrome)和方丹-法瑞奥综合征(Fontaine-Farriaux Syndrome),主要表现为颅骨发育不良伴颅骨畸形、明显的面部畸形、多毛症、严重的产前和产后生长受限、肢体短小、早衰并伴有特征性皮肤改变、趾骨异常和生殖器畸形:迄今为止,所有已知的 FPS 病例都是在出生后观察到的。在此,我们介绍了在妊娠后三个月发现的首两例产前病例。在肯定产前病例存在大多数产后畸形的同时,我们注意到在年幼胎儿中没有出现早衰表现。值得注意的是,我们的报告引入了新的表型特征,如颅脑和肾脏畸形,这在以前的产后病例中是从未见过的。此外,在一个病例中还检测到父系SLC25A24嵌合:结论:我们首次发现了两例 FPS 胎儿病例,并对其进行了全面的表型和遗传评估。我们的研究结果扩展了FPS的表型谱,揭示了新的胎儿表型特征。此外,其中一个病例强调了这种疾病潜在的新型遗传模式。最后,我们的观察结果强调了外显子组/基因组测序在产前和死后诊断具有正常核型和基于阵列的比较基因组杂交(CGH)的罕见多畸形综合征中的有效性。
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来源期刊
Birth Defects Research
Birth Defects Research Medicine-Embryology
CiteScore
3.60
自引率
9.50%
发文量
153
期刊介绍: The journal Birth Defects Research publishes original research and reviews in areas related to the etiology of adverse developmental and reproductive outcome. In particular the journal is devoted to the publication of original scientific research that contributes to the understanding of the biology of embryonic development and the prenatal causative factors and mechanisms leading to adverse pregnancy outcomes, namely structural and functional birth defects, pregnancy loss, postnatal functional defects in the human population, and to the identification of prenatal factors and biological mechanisms that reduce these risks. Adverse reproductive and developmental outcomes may have genetic, environmental, nutritional or epigenetic causes. Accordingly, the journal Birth Defects Research takes an integrated, multidisciplinary approach in its organization and publication strategy. The journal Birth Defects Research contains separate sections for clinical and molecular teratology, developmental and reproductive toxicology, and reviews in developmental biology to acknowledge and accommodate the integrative nature of research in this field. Each section has a dedicated editor who is a leader in his/her field and who has full editorial authority in his/her area.
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