Clinical Utility and Yield of Carrier Exome Sequencing in High-Risk Indian Couples.

IF 2.7 2区医学 Q2 GENETICS & HEREDITY

Prenatal Diagnosis Pub Date : 2025-05-28 DOI:10.1002/pd.6830

Mounika Endrakanti, Sarath R S, Neerja Gupta, Madhulika Kabra

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Abstract

Objective: To evaluate the diagnostic yield and spectrum of monogenic disorders identified through exome sequencing (ES) based couple carrier screening in high-risk couples.

Methods: We retrospectively reviewed the results of carrier screening by ES conducted between 2016 and 2023 at a tertiary care center in India for couples at increased risk of inherited genetic disease in their children. After pre-test genetic counseling, all couples underwent carrier screening through ES. We defined high-risk couples as those at an increased risk of inherited genetic disease in their children, and classified them as Category I (couples with a significant obstetric history, such as a previous fetus or child with a suspected genetic disorder), Category II (couples with a family history of a suspected genetic disorder in a parent or close relative) and Category III (couples opting for expanded carrier screening without any significant contributory history). Category I was further subcategorized based on the phenotype of the affected fetus, neonate, or child into: Ia - multiple malformations including non-immune hydrops and skeletal dysplasia; Ib - features suggestive of other system involvement; Ic - neurological phenotype with or without intellectual disability; and Id - unexplained intrauterine/neonatal death or stillbirth.

Results: Of the 137 couples evaluated, 130 (95%) belonged to category I, of which 48/130 (37%) were subcategorised as Ia, 61/130 (47%) as Ib, 8/130 (6%) as Ic and 24/130 (18.5%) as Id. Nine couples had more than one subcategory indication for ES. Four couples (3%) belonged to category II, and three (2%) belonged to category III. Consanguinity was noted in 23.4% (32/137). The overall diagnostic yield in the cohort was 38.7% (53/137), mainly contributed by category I (52/130, 40%), with the highest yield in subcategory Ib (39/61, 64%).

Conclusion: Carrier screening by ES is useful for identifying couples at high risk of having an offspring with genetic disorders. The yield is higher in couples with an affected previous pregnancy. ES allows comprehensive carrier screening in genetically diverse populations.

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携带者外显子组测序在高危印度夫妇中的临床应用和产量。

目的：评价基于外显子组测序（ES）的高危夫妇单基因疾病筛查的诊断率和谱。方法：我们回顾性回顾了2016年至2023年在印度一家三级医疗中心对子女遗传遗传病风险增加的夫妇进行ES携带者筛查的结果。在测试前遗传咨询后，所有夫妇都通过ES进行了携带者筛查。我们将高风险夫妇定义为其子女遗传遗传病风险增加的夫妇，并将其分类为第一类（有重大产科病史的夫妇，如先前有疑似遗传疾病的胎儿或儿童），第二类（父母或近亲有疑似遗传疾病家族史的夫妇）和第三类（选择扩大携带者筛查但没有任何重大贡献史的夫妇）。根据受影响的胎儿、新生儿或儿童的表型，第一类进一步细分为：Ia -多种畸形，包括非免疫性水肿和骨骼发育不良；b -提示其他系统参与的特征；有或没有智力障碍的神经表型；不明原因的宫内/新生儿死亡或死产。结果：137对夫妇中有130对（95%）属于I类，其中48/130对（37%）为Ia类，61/130对（47%）为Ib类，8/130对（6%）为Ic类，24/130对（18.5%）为Id类。9对夫妇有一个以上的ES亚类指征。4对（3%）属于第二类，3对（2%）属于第三类。有血缘关系的占23.4%（32/137）。该队列的总诊断率为38.7%(53/137)，主要为I类（52/130,40%），其中Ib亚类诊断率最高（39/61,64%）。结论：ES基因携带者筛查有助于鉴别后代遗传疾病的高危夫妇。怀孕前受影响的夫妇的产出率更高。ES允许在基因多样化的人群中进行全面的携带者筛查。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

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