Abstract
BackgroundIn Morocco, consanguinity rate is very high; which lead to an increase in the birth prevalence of infants with autosomal recessive disorders. Previously, it was difficult to diagnose rare autosomal recessive diseases. Next Generation Sequencing (NGS) techniques have considerably improved clinical diagnostics. A genetic diagnosis showing biallelic causative mutations is the requirement for targeted carrier testing in parents, prenatal and preimplantation genetic diagnosis in further pregnancies, and also for targeted premarital testing in future couples at risk of producing affected children by a known autosomal recessive disease.MethodsIn this report, we present our strategy to advise a future couple of first cousins, whose descendants would risk cystinosis; an autosomal recessive lysosomal disease caused by mutations in the CTNS gene. Indeed, our future husband’s sister is clinically and biochemically diagnosed with cystinosis in early childhood. First, we opted to identify the patient’s CTNS gene abnormality by using (NGS), then we searched for heterozygosity in the couple’s DNA, which allows us to predict the exact risk of this familial disease in the future couple’s offspring.ResultsWe have shown that the future husband, brother of the patient is heterozygous for the familial mutation. On the other hand, his future wife did not inherit the familial mutation. Therefore, genetic counseling was reassuring for the risk of familial cystinosis in this couple’s offspring.ConclusionsWe report in this study, one of the major applications of (NGS), an effective tool to improve clinical diagnosis and to provide the possibility of targeted premarital carrier testing in couples at risk.
Highlights
In Morocco, consanguinity rate is very high; which lead to an increase in the birth prevalence of infants with autosomal recessive disorders
The sequence data analysis detected a potential deletion spanning exons 4 and 5 (no reads are generated for these tow exons (Fig. 2a)) and no other pathogenic variant is detected in CTNS gene
We performed RTPCR and Complementary Deoxyribonucleic Acid (cDNA) Sanger sequencing, which confirmed the Next Generation Sequencing (NGS) suspected deletion (Fig. 2b). This result allows us to identify the causal mutation of cystinosis in this family: homozygous deletions carrying both exons 4 and 5 [c.(61 + 1_62–1)_(225 + 1_226–1); NM_004937.3] of the CTNS gene, according to the HGVS format (Fig. 2a)
Summary
In Morocco, consanguinity rate is very high; which lead to an increase in the birth prevalence of infants with autosomal recessive disorders. A genetic diagnosis showing biallelic causative mutations is the requirement for targeted carrier testing in parents, prenatal and preimplantation genetic diagnosis in further pregnancies, and for targeted premarital testing in future couples at risk of producing affected children by a known autosomal recessive disease. The large number of potential genes and the phenotypic variability associated with many known genetic causes, have made the diagnosis of rare autosomal recessive disorders very difficult. Significant advances are achieved using generation sequencing (NGS) technology in medical practice especially in the diagnosis of children with autosomal recessive diseases. Ouhenach et al BMC Medical Genetics (2020) 21:240 counseling and targeted parental carrier testing, prenatal and preimplantation genetic diagnosis in subsequent pregnancies, and targeted premarital genetic testing in at-risk couples.
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