Your search keyword '"Monogenic disorder"' showing total 134 results

1. The clinical application of affected-embryo-based SNP haplotype analysis for patients with de novo pathogenic mutations in PGT-M cycles.

Author

Wang, Jie, Xing, Jun, Chen, Linjun, Diao, Zhenyu, He, Linlin, Wang, Shanshan, Lin, Fei, and Zhang, Ningyuan

Abstract

Purpose: In preimplantation genetic testing for monogenic/single gene disorders (PGT-M) cycles, direct detection of the pathogenic mutation combined with indirect haplotype analysis are recommended to achieve accurate diagnosis. However, it poses a challenge to conduct haplotype analysis for patients carried de novo pathogenetic mutations or without no identified haplotype in families. Herein, the strategy of affected-embryo-based haplotype analysis was implemented in clinical practice to provide a convenient, economical and effective way for such patients. Materials and methods: Eight cases with de novo mutations were recruited. Six cases found the embryo-proband from biopsied blastocysts, and two case (case5 and 6) found them from developmental arrested embryos. A total of thirty-seven biopsied blastocysts from eight PGT-M cycles were performed direct detection and affected-embryo-based single nucleotide polymorphism (SNP) haplotype analyses. Results: Till now, five cases (case 1, 2, 3, 7, 8) had delivered healthy babies and one case (case6) achieved successful ongoing pregnancy. We reported for the first time to find proband from developmental arrested embryos to complete haplotype analyses when no carriers were found in biopsied ones in clinical practice. Conclusion: Our study further proves and expands the application of the double-checking strategy based on affected-embryo proband and allows patients with de novo mutations or lack positive family members to benefit from the strategy. [ABSTRACT FROM AUTHOR]

Published

2024

2. Beta Thalassemia in Children: Established Approaches, Old Issues, New Non-Curative Therapies, and Perspectives on Healing.

Author

Origa, Raffaella and Issa, Layal

Subjects

*BETA-Thalassemia, *CHELATION therapy, *CHILD patients, *GENE therapy, *GENOME editing

Abstract

Despite a decrease in prevalence and incidence rates, beta thalassemia continues to represent a significant public health challenge worldwide. In high-resource settings, children with thalassemia have an open prognosis, with a high chance of reaching adulthood and old age with a good quality of life. This is achievable if transfusion therapy is properly managed, effectively mitigating ineffective erythropoiesis and its associated complications while also minimizing excessive iron accumulation. Adequate iron chelation is essential to maintain reactive forms of iron within the normal range throughout life, thus preventing organ damage caused by hemosiderosis, which inevitably results from a regular transfusion regimen. New therapies, both curative, such as gene therapy, and non-curative, such as modulators of erythropoiesis, are becoming available for patients with transfusion-dependent beta thalassemia. Two curative approaches based on gene therapy have been investigated in both adults and children with thalassemia. The first approach uses a lentivirus to correct the genetic defect, delivering a functional gene copy to the patient's cells. The second approach employs CRISPR/Cas9 gene editing to directly modify the defective gene at the molecular level. No non-curative therapies have received approval for pediatric use. Among adults, the only available drug is luspatercept, which is currently undergoing clinical trials in pediatric populations. However, in many countries around the world, the new therapeutic options remain a mirage, and even transfusion therapy itself is not guaranteed for most patients, while the choice of iron chelation therapy depends on drug availability and affordability. [ABSTRACT FROM AUTHOR]

Published

2024

3. A monoallelic UXS1 variant associated with short‐limbed short stature.

Author

Rustad, Cecilie F., Backe, Paul Hoff, Jin, Chunsheng, Merckoll, Else, Tveten, Kristian, Maciej‐Hulme, Marissa Lucy, Karlsson, Niclas, Prescott, Trine, Sand, Elise Sandås, Woldseth, Berit, Elgstøen, Katja Benedikte Prestø, and Holla, Øystein L.

Subjects

*SHORT stature, *SKELETAL dysplasia, *BONE density, *DYSPLASIA, *GENETIC variation, *GLYCOSAMINOGLYCANS, *EPIPHYSIS

Abstract

Background: Serine residues in the protein backbone of heavily glycosylated proteoglycans are bound to glycosaminoglycans through a tetrasaccharide linker. UXS1 encodes UDP‐glucuronate decarboxylase 1, which catalyzes synthesis of UDP‐xylose, the donor of the first building block in the linker. Defects in other enzymes involved in formation of the tetrasaccharide linker cause so‐called linkeropathies, characterized by short stature, radio‐ulnar synostosis, decreased bone density, congenital contractures, dislocations, and more. Methods: Whole exome sequencing was performed in a father and son who presented with a mild skeletal dysplasia, as well as the father's unaffected parents. Wild‐type and mutant UXS1 were recombinantly expressed in Escherichia coli and purified. Enzyme activity was evaluated by LC–MS/MS. In vivo effects were studied using HeparinRed assay and metabolomics. Results: The son had short long bones, normal epiphysis, and subtle metaphyseal changes especially in his legs. The likely pathogenic heterozygous variant NM_001253875.1(UXS1):c.557T>A p.(Ile186Asn) detected in the son was de novo in the father. Purified Ile186Asn‐UXS1, in contrast to the wild‐type, was not able to convert UDP‐glucuronic acid to UDP‐xylose. Plasma glycosaminoglycan levels were decreased in both son and father. Conclusion: This is the first report linking UXS1 to short‐limbed short stature in humans. [ABSTRACT FROM AUTHOR]

Published

2024

4. Monogenic Disorders of ROS Production and the Primary Anti-Oxidative Defense.

Author

Grüning, Nana-Maria and Ralser, Markus

Subjects

*HOMEOSTASIS, *HEART block, *REACTIVE oxygen species, *NICOTINAMIDE adenine dinucleotide phosphate, *DEFENSE mechanisms (Psychology), *OXIDATIVE stress, *METABOLIC disorders

Abstract

Oxidative stress, characterized by an imbalance between the production of reactive oxygen species (ROS) and the cellular anti-oxidant defense mechanisms, plays a critical role in the pathogenesis of various human diseases. Redox metabolism, comprising a network of enzymes and genes, serves as a crucial regulator of ROS levels and maintains cellular homeostasis. This review provides an overview of the most important human genes encoding for proteins involved in ROS generation, ROS detoxification, and production of reduced nicotinamide adenine dinucleotide phosphate (NADPH), and the genetic disorders that lead to dysregulation of these vital processes. Insights gained from studies on inherited monogenic metabolic diseases provide valuable basic understanding of redox metabolism and signaling, and they also help to unravel the underlying pathomechanisms that contribute to prevalent chronic disorders like cardiovascular disease, neurodegeneration, and cancer. [ABSTRACT FROM AUTHOR]

Published

2024

5. A monoallelic UXS1 variant associated with short‐limbed short stature

Author

Cecilie F. Rustad, Paul Hoff Backe, Chunsheng Jin, Else Merckoll, Kristian Tveten, Marissa Lucy Maciej‐Hulme, Niclas Karlsson, Trine Prescott, Elise Sandås Sand, Berit Woldseth, Katja Benedikte Prestø Elgstøen, and Øystein L. Holla

Subjects

medical genetics, monogenic disorder, skeletal dysplasia, Genetics, QH426-470

Abstract

Abstract Background Serine residues in the protein backbone of heavily glycosylated proteoglycans are bound to glycosaminoglycans through a tetrasaccharide linker. UXS1 encodes UDP‐glucuronate decarboxylase 1, which catalyzes synthesis of UDP‐xylose, the donor of the first building block in the linker. Defects in other enzymes involved in formation of the tetrasaccharide linker cause so‐called linkeropathies, characterized by short stature, radio‐ulnar synostosis, decreased bone density, congenital contractures, dislocations, and more. Methods Whole exome sequencing was performed in a father and son who presented with a mild skeletal dysplasia, as well as the father's unaffected parents. Wild‐type and mutant UXS1 were recombinantly expressed in Escherichia coli and purified. Enzyme activity was evaluated by LC–MS/MS. In vivo effects were studied using HeparinRed assay and metabolomics. Results The son had short long bones, normal epiphysis, and subtle metaphyseal changes especially in his legs. The likely pathogenic heterozygous variant NM_001253875.1(UXS1):c.557T>A p.(Ile186Asn) detected in the son was de novo in the father. Purified Ile186Asn‐UXS1, in contrast to the wild‐type, was not able to convert UDP‐glucuronic acid to UDP‐xylose. Plasma glycosaminoglycan levels were decreased in both son and father. Conclusion This is the first report linking UXS1 to short‐limbed short stature in humans.

Published

2024

6. Preimplantation Genetic Testing (PGT)

Author

Morales, Carmen, González, Daniel, Bautista-Llacer, Rosa, Velilla, Esther, and Ghumman, Surveen, editor

Published

2023

7. Assessing whole-exome sequencing data from undiagnosed Brazilian patients to improve the diagnostic yield of inborn errors of immunity

Author

Cristina Santos Ferreira, Ronaldo da Silva Francisco Junior, Alexandra Lehmkuhl Gerber, Ana Paula de Campos Guimarães, Flávia Anisio Amendola, Fernanda Pinto-Mariz, Monica Soares de Souza, Patrícia Carvalho Batista Miranda, Zilton Farias Meira de Vasconcelos, Ekaterini Simões Goudouris, and Ana Tereza Ribeiro Vasconcelos

Subjects

Whole exome sequencing, Single nucleotide variants, Monogenic disorder, Inborn errors of immunity, Genetics, QH426-470

Abstract

Abstract Objectives Inborn error of immunity (IEI) comprises a broad group of inherited immunological disorders that usually display an overlap in many clinical manifestations challenging their diagnosis. The identification of disease-causing variants from whole-exome sequencing (WES) data comprises the gold-standard approach to ascertain IEI diagnosis. The efforts to increase the availability of clinically relevant genomic data for these disorders constitute an important improvement in the study of rare genetic disorders. This work aims to make available WES data of Brazilian patients’ suspicion of IEI without a genetic diagnosis. We foresee a broad use of this dataset by the scientific community in order to provide a more accurate diagnosis of IEI disorders. Data description Twenty singleton unrelated patients treated at four different hospitals in the state of Rio de Janeiro, Brazil were enrolled in our study. Half of the patients were male with mean ages of 9 ± 3, while females were 12 ± 10 years old. The WES was performed in the Illumina NextSeq platform with at least 90% of sequenced bases with a minimum of 30 reads depth. Each sample had an average of 20,274 variants, comprising 116 classified as rare pathogenic or likely pathogenic according to American College of Medical Genetics and Genomics and the Association (ACMG) guidelines. The genotype-phenotype association was impaired by the lack of detailed clinical and laboratory information, besides the unavailability of molecular and functional studies which, comprise the limitations of this study. Overall, the access to clinical exome sequencing data is limited, challenging exploratory analyses and the understanding of genetic mechanisms underlying disorders. Therefore, by making these data available, we aim to increase the number of WES data from Brazilian samples despite contributing to the study of monogenic IEI-disorders.

Published

2023

8. Genetics in reproductive endocrinology and infertility.

Author

Lee, Iris T., Kappy, Michelle, Forman, Eric J., and Dokras, Anuja

Subjects

*ENDOCRINOLOGY of human reproduction, *GENETICS, *GENETIC testing, *INFERTILITY, *FERTILIZATION in vitro

Abstract

Tremendous advances in genetics have transformed the field of reproductive endocrinology and infertility over the last few decades. One of the most prominent advances is preimplantation genetic testing (PGT), which allows for the screening of embryos obtained during in vitro fertilization before transfer. Moreover, PGT can be performed for aneuploidy screening, detection of monogenic disorders, or exclusion of structural rearrangements. Refinement of biopsy techniques, such as obtaining samples at the blastocyst rather than the cleavage stage, has helped optimize results from PGT, and technological advances, including next-generation sequencing, have made PGT more efficient and accurate. The continued evolution of the approach to PGT has the potential to further enhance the accuracy of results, expand the application to other conditions, and increase access by reducing cost and improving efficiency. [ABSTRACT FROM AUTHOR]

Published

2023

9. Assessing whole-exome sequencing data from undiagnosed Brazilian patients to improve the diagnostic yield of inborn errors of immunity.

Author

Ferreira, Cristina Santos, da Silva Francisco Junior, Ronaldo, Gerber, Alexandra Lehmkuhl, Guimarães, Ana Paula de Campos, Amendola, Flávia Anisio, Pinto-Mariz, Fernanda, de Souza, Monica Soares, Miranda, Patrícia Carvalho Batista, de Vasconcelos, Zilton Farias Meira, Goudouris, Ekaterini Simões, and Vasconcelos, Ana Tereza Ribeiro

Subjects

*EXOMES, *MEDICAL genomics, *MEDICAL genetics, *GENETIC disorder diagnosis, *SINGLE nucleotide polymorphisms, *IMMUNITY

Abstract

Objectives: Inborn error of immunity (IEI) comprises a broad group of inherited immunological disorders that usually display an overlap in many clinical manifestations challenging their diagnosis. The identification of disease-causing variants from whole-exome sequencing (WES) data comprises the gold-standard approach to ascertain IEI diagnosis. The efforts to increase the availability of clinically relevant genomic data for these disorders constitute an important improvement in the study of rare genetic disorders. This work aims to make available WES data of Brazilian patients' suspicion of IEI without a genetic diagnosis. We foresee a broad use of this dataset by the scientific community in order to provide a more accurate diagnosis of IEI disorders. Data description: Twenty singleton unrelated patients treated at four different hospitals in the state of Rio de Janeiro, Brazil were enrolled in our study. Half of the patients were male with mean ages of 9 ± 3, while females were 12 ± 10 years old. The WES was performed in the Illumina NextSeq platform with at least 90% of sequenced bases with a minimum of 30 reads depth. Each sample had an average of 20,274 variants, comprising 116 classified as rare pathogenic or likely pathogenic according to American College of Medical Genetics and Genomics and the Association (ACMG) guidelines. The genotype-phenotype association was impaired by the lack of detailed clinical and laboratory information, besides the unavailability of molecular and functional studies which, comprise the limitations of this study. Overall, the access to clinical exome sequencing data is limited, challenging exploratory analyses and the understanding of genetic mechanisms underlying disorders. Therefore, by making these data available, we aim to increase the number of WES data from Brazilian samples despite contributing to the study of monogenic IEI-disorders. [ABSTRACT FROM AUTHOR]

Published

2023

10. Monogenic Disorders of ROS Production and the Primary Anti-Oxidative Defense

Author

Nana-Maria Grüning and Markus Ralser

Subjects

oxidative stress, reactive oxygen species (ROS), cellular redox balance, monogenic disorder, inherited disease, Microbiology, QR1-502

Abstract

Oxidative stress, characterized by an imbalance between the production of reactive oxygen species (ROS) and the cellular anti-oxidant defense mechanisms, plays a critical role in the pathogenesis of various human diseases. Redox metabolism, comprising a network of enzymes and genes, serves as a crucial regulator of ROS levels and maintains cellular homeostasis. This review provides an overview of the most important human genes encoding for proteins involved in ROS generation, ROS detoxification, and production of reduced nicotinamide adenine dinucleotide phosphate (NADPH), and the genetic disorders that lead to dysregulation of these vital processes. Insights gained from studies on inherited monogenic metabolic diseases provide valuable basic understanding of redox metabolism and signaling, and they also help to unravel the underlying pathomechanisms that contribute to prevalent chronic disorders like cardiovascular disease, neurodegeneration, and cancer.

Published

2024

11. A mathematical modelling to detect sickle cell anemia using Quantum graph theory and Aquila optimization classifier

Author

P. Balamanikandan and S. Jeya Bharathi

Subjects

monogenic disorder, genetic disorder, sickle cell anemia, red blood cells, hemoglobin, aquila optimization based cascaded lstm classifier, elasticity property features, quantum graph theory model, Biotechnology, TP248.13-248.65, Mathematics, QA1-939

Abstract

Recently genetic disorders are the most common reason for human fatality. Sickle Cell anemia is a monogenic disorder caused by A-to-T point mutations in the β-globin gene which produces abnormal hemoglobin S (Hgb S) that polymerizes at the state of deoxygenation thus resulting in the physical deformation or erythrocytes sickling. This shortens the expectancy of human life. Thus, the early diagnosis and identification of sickle cell will aid the people in recognizing signs and to take treatments. The manual identification is a time consuming one and might outcome in the misclassification of count as there is millions of red blood cells in one spell. So as to overcome this, data mining approaches like Quantum graph theory model and classifier is effective in detecting sickle cell anemia with high precision rate. The proposed work aims at presenting a mathematical modeling using Quantum graph theory to extract elasticity properties and to distinguish them as normal cells and sickle cell anemia (SCA) in red blood cells. Initially, input DNA sequence is taken and the elasticity property features are extracted by using Quantum graph theory model at which the formation of spanning tree is made followed by graph construction and Hemoglobin quantization. After which, the extracted properties are optimized using Aquila optimization and classified using cascaded Long Short-Term memory (LSTM) to attain the classified outcome of sickle cell and normal cells. Finally, the performance assessment is made and the outcomes attained in terms of accuracy, precision, sensitivity, specificity, and AUC are compared with existing classifier to validate the proposed system effectiveness.

Published

2022

12. Noninvasive fetal genotyping of single nucleotide variants and linkage analysis for prenatal diagnosis of monogenic disorders

Author

Wenman Wu, Xuanyou Zhou, Zhengwen Jiang, Dazhi Zhang, Feng Yu, Lanlan Zhang, Xuefeng Wang, Songchang Chen, and Chenming Xu

Subjects

Cell-free DNA, Fetal genotyping, Prenatal diagnosis, Massively parallel sequencing, Monogenic disorder, Medicine, Genetics, QH426-470

Abstract

Abstract Background High-cost, time-consuming and complex processes of several current approaches limit the use of noninvasive prenatal diagnosis (NIPD) for monogenic disorders in clinical application. Thus, a more cost-effective and easily implementable approach is required. Methods We established a low-cost and convenient test to noninvasively deduce fetal genotypes of the mutation and single nucleotide polymorphisms (SNPs) loci by means of targeted amplification combined with deep sequencing of maternal genomic and plasma DNA. The sequential probability ratio test was performed to detect the allelic imbalance in maternal plasma. This method can be employed to directly examine familial pathogenic mutations in the fetal genome, as well as infer the inheritance of parental haplotypes through a group of selected SNPs linked to the pathogenic mutation. Results The fetal mutations in 17 families with different types of monogenic disorders including hemophilia A, von Willebrand disease type 3, Duchenne muscular dystrophy, hyper-IgM type 1, glutaric acidemia type I, Nagashima-type palmoplantar keratosis, and familial exudative vitreoretinopathy were identified in the study. The mutations included various forms: point mutations, gene inversion, deletions/insertions and duplication. The results of 12 families were verified by sequencing of amniotic fluid samples, the accuracy of the approach in fetal genotyping at the mutation and SNPs loci was 98.85% (172/174 loci), and the no-call rate was 28.98% (71/245 loci). The overall accuracy was 12/12 (100%). Moreover, the approach was successfully applied in plasma samples with a fetal fraction as low as 2.3%. Conclusions We have shown in this study that the approach is a cost-effective, less time consuming and accurate method for NIPD of monogenic disorders.

Published

2022

13. Assessment of an automated approach for variant interpretation in screening for monogenic disorders: A single‐center study.

Author

Gall, Bryan J., Smart, Trevor B., Munch, Robin, Kolluri, Supraja, Tadepally, Hamsa, Lim, Karen Phaik Har, Demko, Zachary P., Benn, Peter, Souter, Vivienne, Sanapareddy, Nina, and Keen‐Kim, Dianne

Subjects

*MEDICAL screening, *GENETIC variation, *GENETIC testing, *AUTOMATION

Abstract

Background: Automation has been introduced into variant interpretation, but it is not known how automated variant interpretation performs on a stand‐alone basis. The purpose of this study was to evaluate a fully automated computerized approach. Method: We reviewed all variants encountered in a set of carrier screening panels over a 1‐year interval. Observed variants with high‐confidence ClinVar interpretations were included in the analysis; those without high‐confidence ClinVar entries were excluded. Results: Discrepancy rates between automated interpretations and high‐confidence ClinVar entries were analyzed. Of the variants interpreted as positive (likely pathogenic or pathogenic) based on ClinVar information, 22.6% were classified as negative (variants of uncertain significance, likely benign or benign) variants by the automated method. Of the ClinVar negative variants, 1.7% were classified as positive by the automated software. On a per‐case basis, which accounts for variant frequency, 63.4% of cases with a ClinVar high‐confidence positive variant were classified as negative by the automated method. Conclusion: While automation in genetic variant interpretation holds promise, there is still a need for manual review of the output. Additional validation of automated variant interpretation methods should be conducted. [ABSTRACT FROM AUTHOR]

Published

2022

14. Clinical outcomes following preimplantation genetic testing for monogenic conditions: a systematic review of observational studies.

Author

Poulton A, Menezes M, Hardy T, Lewis S, and Hui L

Abstract

Objective: We aimed to report a summary of clinical outcomes following preimplantation genetic testing for monogenic conditions, by performing a systematic review of published literature on clinical pregnancy and live birth rates following preimplantation genetic testing due to a monogenic indication. Additionally, we aimed to undertake a subgroup analysis of clinical outcomes of concurrent monogenic and aneuploidy screening., Data Sources: Three electronic databases (MEDLINE, EMBASE, and PubMed) were searched from inception to May 2024., Study Eligibility Criteria: Quantitative data audits, observational studies, and case series reporting clinical outcomes for individuals undergoing preimplantation genetic testing for a monogenic indication were included. Only studies using blastocyst biopsies with polymerase chain reaction-based or genome-wide haplotyping methods for molecular analysis were eligible to reflect current laboratory practice., Methods: Quality assessment was performed following data extraction using an adaptation of the Joanna Briggs critical appraisal tool for case series. Results were extracted, and pooled mean clinical pregnancy rates and birth rates were calculated with 95% confidence intervals (95% CI). We compared outcomes between those with and without concurrent preimplantation genetic testing for aneuploidy., Results: Our search identified 1372 publications; 51 were eligible for inclusion. Pooled data on 5305 cycles and 5229 embryo transfers yielded 1806 clinical pregnancies and 1577 births. This translated to clinical pregnancy and birth rates of 34.0% [95% CI: 32.8%-35.3%] and 29.7% [95% CI: 28.5%-31.0%] per cycle and 24.8% [95% CI: 23.6%-26.0%] and 21.7% [95% CI: 20.8%-23.1%] per embryo transfer. In studies with concurrent aneuploidy screening, clinical pregnancy and birth rates were 43.3% [95% CI: 40.2%-46.5%] and 37.6% [95% CI: 34.6%-40.8%] per cycle and 37.0% [95% CI: 33.9%-40.3%] and 31.8% [95% CI: 28.8%-35.0%] per embryo transfer. Studies without aneuploidy screening reported clinical pregnancy and birth rates of 32.5% [95% CI: 31.0%-34.1%] and 28.1% [95% CI: 26.6%-29.7%] per cycle and 21.2% [95% CI: 19.8%-22.6%] and 18.6% [95% CI: 17.3%-20.0%] per embryo transfer., Conclusion: This systematic review reveals promising clinical outcome figures for this indication group. Additionally, synthesizing the published scientific literature on clinical outcomes from preimplantation genetic testing for monogenic conditions provides a rigorous, noncommercial evidence base for counseling., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

15. A brief clinical genetics review: stepwise diagnostic processes of a monogenic disorder-hypertriglyceridemia.

Author

Ueda M

Abstract

The completion of the Human Genome Project and tremendous advances in automated high-throughput genetic analysis technologies have enabled explosive progress in the field of genetics, which resulted in countless discoveries of novel genes and pathways. Many phenotype- or disease-associated single nucleotide polymorphisms (SNPs) with a high statistical significance have been identified through numerous genome-wide association studies (GWAS), and various polygenic risk scoring (PRS) schemes have been proposed to identify individuals with a high risk for a certain trait or disorder. Meanwhile, medical education in genetics has lagged far behind, leaving many physicians and healthcare providers unprepared in the genomic era. Thus, there is an urgent need to educate physicians and healthcare providers with basic knowledge and skills in genetics. To facilitate this, some basic terminologies and concepts are discussed in this review. In addition, some important considerations in delineating and incorporating clinical genetic testing in the diagnosis and management of a monogenic disorder are illustrated in a stepwise fashion. Furthermore, the effects of disease-associated SNPs represented by a PRS scheme clearly demonstrated that even the phenotypes of a monogenic disorder due to the same pathogenic variant in family members are modulated by the polygenic background. In human genetics, despite these explosive advancements, we are still far from clearly deciphering the interplay of gene variants to effect unique characteristics in an individual. In addition, sophisticated genome or gene directed therapies are being investigated for numerous disorders. Therefore, evolution in the field of genetics is likely to continue into the foreseeable future. In the meantime, much emphasis should be placed on educating physicians and healthcare professionals to be well-versed and skillful in the clinical use of genetics so that they can fully embrace the new era of precision medicine., Competing Interests: Conflicts of Interest: The author has completed the ICMJE uniform disclosure form (available at https://tp.amegroups.com/article/view/10.21037/tp-24-131/coif). The author has no conflicts of interest to declare., (2024 AME Publishing Company. All rights reserved.)

Published

2024

16. Assessment of an automated approach for variant interpretation in screening for monogenic disorders: A single‐center study

Author

Bryan J. Gall, Trevor B. Smart, Robin Munch, Supraja Kolluri, Hamsa Tadepally, Karen Phaik Har Lim, Zachary P. Demko, Peter Benn, Vivienne Souter, Nina Sanapareddy, and Dianne Keen‐Kim

Subjects

automated variant classification, genetic testing, manual curation, monogenic disorder, variant classification, variant interpretation, Genetics, QH426-470

Abstract

Abstract Background Automation has been introduced into variant interpretation, but it is not known how automated variant interpretation performs on a stand‐alone basis. The purpose of this study was to evaluate a fully automated computerized approach. Method We reviewed all variants encountered in a set of carrier screening panels over a 1‐year interval. Observed variants with high‐confidence ClinVar interpretations were included in the analysis; those without high‐confidence ClinVar entries were excluded. Results Discrepancy rates between automated interpretations and high‐confidence ClinVar entries were analyzed. Of the variants interpreted as positive (likely pathogenic or pathogenic) based on ClinVar information, 22.6% were classified as negative (variants of uncertain significance, likely benign or benign) variants by the automated method. Of the ClinVar negative variants, 1.7% were classified as positive by the automated software. On a per‐case basis, which accounts for variant frequency, 63.4% of cases with a ClinVar high‐confidence positive variant were classified as negative by the automated method. Conclusion While automation in genetic variant interpretation holds promise, there is still a need for manual review of the output. Additional validation of automated variant interpretation methods should be conducted.

Published

2022

17. Noninvasive fetal genotyping of single nucleotide variants and linkage analysis for prenatal diagnosis of monogenic disorders.

Author

Wu, Wenman, Zhou, Xuanyou, Jiang, Zhengwen, Zhang, Dazhi, Yu, Feng, Zhang, Lanlan, Wang, Xuefeng, Chen, Songchang, and Xu, Chenming

Abstract

Background: High-cost, time-consuming and complex processes of several current approaches limit the use of noninvasive prenatal diagnosis (NIPD) for monogenic disorders in clinical application. Thus, a more cost-effective and easily implementable approach is required. Methods: We established a low-cost and convenient test to noninvasively deduce fetal genotypes of the mutation and single nucleotide polymorphisms (SNPs) loci by means of targeted amplification combined with deep sequencing of maternal genomic and plasma DNA. The sequential probability ratio test was performed to detect the allelic imbalance in maternal plasma. This method can be employed to directly examine familial pathogenic mutations in the fetal genome, as well as infer the inheritance of parental haplotypes through a group of selected SNPs linked to the pathogenic mutation. Results: The fetal mutations in 17 families with different types of monogenic disorders including hemophilia A, von Willebrand disease type 3, Duchenne muscular dystrophy, hyper-IgM type 1, glutaric acidemia type I, Nagashima-type palmoplantar keratosis, and familial exudative vitreoretinopathy were identified in the study. The mutations included various forms: point mutations, gene inversion, deletions/insertions and duplication. The results of 12 families were verified by sequencing of amniotic fluid samples, the accuracy of the approach in fetal genotyping at the mutation and SNPs loci was 98.85% (172/174 loci), and the no-call rate was 28.98% (71/245 loci). The overall accuracy was 12/12 (100%). Moreover, the approach was successfully applied in plasma samples with a fetal fraction as low as 2.3%. Conclusions: We have shown in this study that the approach is a cost-effective, less time consuming and accurate method for NIPD of monogenic disorders. [ABSTRACT FROM AUTHOR]

Published

2022

18. Noninvasive prenatal diagnosis based on cell‐free DNA for tuberous sclerosis: A pilot study.

Author

Yang, Xiao‐Yan, Meng, Yan, Wang, Yang‐Yang, Lu, Yan‐Ping, Wang, Qiu‐Hong, You, Yan‐Qin, Xie, Xiao‐Xiao, Bai, Ling, Fang, Nan, and Zou, Li‐Ping

Subjects

*CELL-free DNA, *TUBEROUS sclerosis, *NONINVASIVE diagnostic tests, *PRENATAL diagnosis, *LEUCOCYTES, *CIRCULATING tumor DNA

Abstract

Background: Noninvasive prenatal diagnosis (NIPD) based on cell‐free DNA (cfDNA) has been introduced into the clinical application for some monogenic disorders but not for tuberous sclerosis (TSC) yet, which is an autosomal dominant disease caused by various variations in TSC1 or TSC2 gene. We aimed to explore the feasibility of NIPD on TSC. Methods: We recruited singleton pregnancies at risk of TSC from 14 families with a proband child. Definitive NIPD for TSC was performed using targeted next‐generation sequencing of cfDNA in parallel with maternal white blood cell DNA (wbcDNA). The NIPD results were validated by amniocentesis or postnatal gene testing and follow‐up of the born children. Results: Missense mutations, nonsense mutations, frameshift mutations, and splice‐site variants which were obtained through de‐novo, maternal, or paternal inheritance were included. The mean and minimum gestational weeks of NIPD were 17.18 ± 5.83 and 8 weeks, respectively. The NIPD results were 100% consistent with the amniocentesis or postnatal gene testing and follow‐up of the born children. Conclusion: This study demonstrates that NIPD based on cfDNA is feasible for TSC, but required to be confirmed with more samples. Studies on TSC can contribute to the application and promotion of NIPD for monogenic disorders. [ABSTRACT FROM AUTHOR]

Published

2022

19. Genetic Diagnostics in Routine Osteological Assessment of Adult Low Bone Mass Disorders.

Author

Oheim, Ralf, Tsourdi, Elena, Seefried, Lothar, Beller, Gisela, Schubach, Max, Vettorazzi, Eik, Stürznickel, Julian, Rolvien, Tim, Ehmke, Nadja, Delsmann, Alena, Genest, Franca, Krüger, Ulrike, Zemojtel, Tomasz, Barvencik, Florian, Schinke, Thorsten, Jakob, Franz, Hofbauer, Lorenz C., Mundlos, Stefan, and Kornak, Uwe

Subjects

GENETIC disorder diagnosis, BONE density

Abstract

Context: Many different inherited and acquired conditions can result in premature bone fragility/low bone mass disorders (LBMDs). Objective: We aimed to elucidate the impact of genetic testing on differential diagnosis of adult LBMDs and at defining clinical criteria for predicting monogenic forms. Methods: Four clinical centers broadly recruited a cohort of 394 unrelated adult women before menopause and men younger than 55 years with a bone mineral density (BMD) Z-score < -2.0 and/or pathological fractures. After exclusion of secondary causes or unequivocal clinical/biochemical hallmarks of monogenic LBMDs, all participants were genotyped by targeted next-generation sequencing. Results: In total, 20.8% of the participants carried rare disease-causing variants (DCVs) in genes known to cause osteogenesis imperfecta (COL1A1, COL1A2), hypophosphatasia (ALPL), and early-onset osteoporosis (LRP5, PLS3, and WNT1). In addition, we identified rare DCVs in ENPP1, LMNA, NOTCH2, and ZNF469. Three individuals had autosomal recessive, 75 autosomal dominant, and 4 X-linked disorders. A total of 9.7% of the participants harbored variants of unknown significance. A regression analysis revealed that the likelihood of detecting a DCV correlated with a positive family history of osteoporosis, peripheral fractures (> 2), and a high normal body mass index (BMI). In contrast, mutation frequencies did not correlate with age, prevalent vertebral fractures, BMD, or biochemical parameters. In individuals without monogenic disease-causing rare variants, common variants predisposing for low BMD (eg, in LRP5) were overrepresented. Conclusion: The overlapping spectra of monogenic adult LBMD can be easily disentangled by genetic testing and the proposed clinical criteria can help to maximize the diagnostic yield. [ABSTRACT FROM AUTHOR]

Published

2022

20. Noninvasive prenatal diagnosis based on cell‐free DNA for tuberous sclerosis: A pilot study

Author

Xiao‐Yan Yang, Yan Meng, Yang‐Yang Wang, Yan‐Ping Lu, Qiu‐Hong Wang, Yan‐Qin You, Xiao‐Xiao Xie, Ling Bai, Nan Fang, and Li‐Ping Zou

Subjects

autosomal dominant disease, cell‐free DNA, monogenic disorder, noninvasive prenatal diagnosis, tuberous sclerosis, Genetics, QH426-470

Abstract

Abstract Background Noninvasive prenatal diagnosis (NIPD) based on cell‐free DNA (cfDNA) has been introduced into the clinical application for some monogenic disorders but not for tuberous sclerosis (TSC) yet, which is an autosomal dominant disease caused by various variations in TSC1 or TSC2 gene. We aimed to explore the feasibility of NIPD on TSC. Methods We recruited singleton pregnancies at risk of TSC from 14 families with a proband child. Definitive NIPD for TSC was performed using targeted next‐generation sequencing of cfDNA in parallel with maternal white blood cell DNA (wbcDNA). The NIPD results were validated by amniocentesis or postnatal gene testing and follow‐up of the born children. Results Missense mutations, nonsense mutations, frameshift mutations, and splice‐site variants which were obtained through de‐novo, maternal, or paternal inheritance were included. The mean and minimum gestational weeks of NIPD were 17.18 ± 5.83 and 8 weeks, respectively. The NIPD results were 100% consistent with the amniocentesis or postnatal gene testing and follow‐up of the born children. Conclusion This study demonstrates that NIPD based on cfDNA is feasible for TSC, but required to be confirmed with more samples. Studies on TSC can contribute to the application and promotion of NIPD for monogenic disorders.

Published

2022

21. A Systematic Review of Monogenic Inflammatory Bowel Disease.

Author

Nambu, Ryusuke, Warner, Neil, Mulder, Daniel J., Kotlarz, Daniel, McGovern, Dermot P.B., Cho, Judy, Klein, Christoph, Snapper, Scott B., Griffiths, Anne M., Iwama, Itaru, and Muise, Aleixo M.

Abstract

Advances in genomic technologies have led to increasing reports of monogenic inflammatory bowel disease (IBD). Here, we systematically review the literature to determine the clinical features, genetic profile, and previously used treatment strategies in monogenic IBD. A systematic review of MEDLINE articles published between January 2000 and December 2020 was conducted. A total of 750 individual monogenic IBD cases were identified from 303 eligible articles. The most frequently reported monogenic IBD genes were IL10RA / B , XIAP , CYBB , LRBA , and TTC7A. In total, 63.4% of patients developed IBD before 6 years of age, 17.4% developed IBD between ages 10 and 17.9 years, and 10.9% developed IBD after age 18. There was a substantial difference between these age groups and the underlying monogenic disorders. Only 31.7% had any history of extraintestinal comorbidity (EIC) before IBD onset, but 76.0% developed at least 1 EIC during their clinical course. The most common EICs were atypical infection (44.7%), dermatologic abnormality (38.4%), and autoimmunity (21.9%). Bowel surgery, biologic therapy, and hematopoietic stem cell transplantation were performed in 27.1%, 32.9%, and 23.1% of patients, respectively. Monogenic IBD cases, although rare, have varied extraintestinal comorbidities and limited treatment options including surgery and transplant. Early identification and improved understanding of the characteristics of the genes and underlying disease processes in monogenic IBD is important for effective management. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

22. Myopia-26, the female-limited form of early-onset high myopia, occurring in a European family

Author

Noémi Széll, Tamás Fehér, Zoltán Maróti, Tibor Kalmár, Dóra Latinovics, István Nagy, Zsuzsanna Z. Orosz, Márta Janáky, Andrea Facskó, and Zoltán Sohajda

Subjects

Early onset high myopia, X-linked female-limited high myopia, Intrinsically photosensitive retinal ganglion cell, Monogenic disorder, Mendelian inheritance, X-arrestin, Medicine

Abstract

Abstract Background Female-limited early-onset high myopia, also called Myopia-26 is a rare monogenic disorder characterized by severe short sightedness starting in early childhood and progressing to blindness potentially by the middle ages. Despite the X-linked locus of the mutated ARR3 gene, the disease paradoxically affects females only, with males being asymptomatic carriers. Previously, this disease has only been observed in Asian families and has not gone through detailed investigation concerning collateral symptoms or pathogenesis. Results We found a large Hungarian family displaying female-limited early-onset high myopia. Whole exome sequencing of two individuals identified a novel nonsense mutation (c.214C>T, p.Arg72*) in the ARR3 gene. We carried out basic ophthalmological testing for 18 family members, as well as detailed ophthalmological examination (intraocular pressure, axial length, fundus appearance, optical coherence tomography, visual field- testing) as well as colour vision- and electrophysiology tests (standard and multifocal electroretinography, pattern electroretinography and visual evoked potentials) for eight individuals. Ophthalmological examinations did not reveal any signs of cone dystrophy as opposed to animal models. Electrophysiology and colour vision tests similarly did not evidence a general cone system alteration, rather a central macular dysfunction affecting both the inner and outer (postreceptoral and receptoral) retinal structures in all patients with ARR3 mutation. Conclusions This is the first description of a Caucasian family displaying Myopia-26. We present two hypotheses that could potentially explain the pathomechanism of this disease.

Published

2021

23. Noninvasive Prenatal Testing of Methylmalonic Acidemia cblC Type Using the cSMART Assay for MMACHC Gene Mutations.

Author

Lv, Weigang, Liang, Lili, Chen, Xin, Li, Zhuo, Liang, Desheng, Zhu, Huimin, Teng, Yanling, Wu, Weijuan, Wu, Lingqian, and Han, Lianshu

Subjects

PRENATAL diagnosis, GENETIC mutation, ACIDOSIS, MOLECULAR diagnosis, INVASIVE diagnosis, METHYL methacrylate

Abstract

Noninvasive prenatal testing (NIPT) for monogenic disorders has been developed in recent years; however, there are still significant technical and analytical challenges for clinical use. The clinical feasibility of NIPT for methylmalonic acidemia cblC type (cblC type MMA) was investigated using our circulating single-molecule amplification and re-sequencing technology (cSMART). Trios molecular diagnosis was performed in 29 cblC type MMA-affected children and their parents by traditional Sanger sequencing. In the second pregnancy, invasive prenatal diagnosis (IPD) of the pathogenic MMACHC gene was used to determine fetal genotypes, and NIPT was performed using a novel MMACHC gene–specific cSMART assay. Maternal–fetal genotypes were deduced based on the mutation ratio in maternal plasma DNA. Concordance of fetal genotypes between IPD and NIPT, and the sensitivity and specificity of NIPT were determined. After removing two cases with a low P value or reads, the concordance ratio for NIPT and IPD was 100.00% (27/27), and the sensitivity and specificity were 100.00% (54.07–100.00%) and 100.00% (83.89–100.00%), respectively. This study demonstrates that NIPT using the cSMART assay for cblC type MMA was accurate in detecting fetal genotypes. cSMART has a potential clinical application as a prenatal diagnosis and screening tool for carrier and low-risk genotypes of cblC type MMA and other monogenic diseases. [ABSTRACT FROM AUTHOR]

Published

2022

24. Noninvasive Prenatal Testing of Methylmalonic Acidemia cblC Type Using the cSMART Assay for MMACHC Gene Mutations

Author

Weigang Lv, Lili Liang, Xin Chen, Zhuo Li, Desheng Liang, Huimin Zhu, Yanling Teng, Weijuan Wu, Lingqian Wu, and Lianshu Han

Subjects

noninvasive prenatal testing, methylmalonic acidemia cblC type, circulating single molecule amplification and re-sequencing technology, monogenic disorder, next-generation sequencing, cell-free DNA, Genetics, QH426-470

Abstract

Noninvasive prenatal testing (NIPT) for monogenic disorders has been developed in recent years; however, there are still significant technical and analytical challenges for clinical use. The clinical feasibility of NIPT for methylmalonic acidemia cblC type (cblC type MMA) was investigated using our circulating single-molecule amplification and re-sequencing technology (cSMART). Trios molecular diagnosis was performed in 29 cblC type MMA-affected children and their parents by traditional Sanger sequencing. In the second pregnancy, invasive prenatal diagnosis (IPD) of the pathogenic MMACHC gene was used to determine fetal genotypes, and NIPT was performed using a novel MMACHC gene–specific cSMART assay. Maternal–fetal genotypes were deduced based on the mutation ratio in maternal plasma DNA. Concordance of fetal genotypes between IPD and NIPT, and the sensitivity and specificity of NIPT were determined. After removing two cases with a low P value or reads, the concordance ratio for NIPT and IPD was 100.00% (27/27), and the sensitivity and specificity were 100.00% (54.07–100.00%) and 100.00% (83.89–100.00%), respectively. This study demonstrates that NIPT using the cSMART assay for cblC type MMA was accurate in detecting fetal genotypes. cSMART has a potential clinical application as a prenatal diagnosis and screening tool for carrier and low-risk genotypes of cblC type MMA and other monogenic diseases.

Published

2022

25. Prevalence of severe hypertriglyceridemia and pancreatitis in familial partial lipodystrophy type 2.

Author

Lazarte, Julieta, Wang, Jian, McIntyre, Adam D., and Hegele, Robert A.

Subjects

LIPODYSTROPHY, DIFFERENTIAL diagnosis, HYPERLIPIDEMIA, SEVERITY of illness index, RISK assessment, DISEASE prevalence, DESCRIPTIVE statistics, HOSPITAL care, PANCREATITIS, LONGITUDINAL method, LIPIDS, DISEASE risk factors, DISEASE complications

Abstract

• FPLD2 patients without diabetes have mild hypertriglyceridemia with no pancreatitis. • About 1 in 7 FPLD2 patients with diabetes have severe hypertriglyceridemia. • About 1 in 10 FPLD2 patients with diabetes have had pancreatitis. • Once diabetes develops in FPLD2, patients' lipids must be carefully monitored. Familial partial lipodystrophy (FPLD) is a rare Mendelian condition listed in the differential diagnosis of severe hypertriglyceridemia (HTG) and pancreatitis. Here we determined the prevalence of severe HTG and pancreatitis among a cohort of 74 FPLD patients assessed in a lipid clinic. We studied lipid profiles from individuals with either of the two most common pathogenic monoallelic variants in LMNA , namely p.R482Q (N= 51) and p.R482W (N= 23). In total, 28 (37.8%) patients with a mean age of 41.8 ± 14.8 years had diabetes, while 46 (62.2%) patients with a mean age of 35.4 ± 19.4 years had no diabetes. Among patients with and without diabetes, median TG levels (interquartile range) were 2.73 (4.78) and 1.86 (1.66) mmol/L (242 [423] and 165 [147] mg/dL), respectively. Overall, 4 subjects (5.4%) had triglyceride levels > 10 mmol/L (> 885 mg/dL), of whom 3 (4.1%) had a history of hospitalization for acute pancreatitis. All 4 patients with severe HTG had diabetes, i.e. 14.3% of those with diabetes. In contrast, FPLD2 patients without diabetes had only mild HTG, with no instances of severe HTG or pancreatitis. Thus, among this selected lipid clinic cohort with lipodystrophy, severe HTG and pancreatitis in FPLD2 are relatively common when diabetes is present. [ABSTRACT FROM AUTHOR]

Published

2021

26. Remus: A Web Application for Prioritization of Regulatory Regions and Variants in Monogenic Diseases

Author

Paweł Sztromwasser, Damian Skrzypczak, Arkadiusz Michalak, and Wojciech Fendler

Subjects

regulatory variants, whole-genome sequencing, monogenic disorder, variant prioritization, web application, regulatory regions, Genetics, QH426-470

Abstract

BackgroundAnalysis of variants in distant regulatory elements could improve the current 25–50% yield of genetic testing for monogenic diseases. However, the vast size of the regulome, great number of variants, and the difficulty in predicting their phenotypic impact make searching for pathogenic variants in the regulatory genome challenging. New tools for the identification of regulatory variants based on their relevance to the phenotype are needed.MethodsWe used tissue-specific regulatory loci mapped by ENCODE and FANTOM, together with miRNA–gene interactions from miRTarBase and miRWalk, to develop Remus, a web application for the identification of tissue-specific regulatory regions. Remus searches for regulatory features linked to the known disease-associated genes and filters them using activity status in the target tissues relevant for the studied disorder. For user convenience, Remus provides a web interface and facilitates in-browser filtering of variant files suitable for sensitive patient data.ResultsTo evaluate our approach, we used a set of 146 regulatory mutations reported causative for 68 distinct monogenic disorders and a manually curated a list of tissues affected by these disorders. In 89.7% of cases, Remus identified the regulator containing the pathogenic mutation. The tissue-specific search limited the number of considered variants by 82.5% as compared to a tissue-agnostic search.ConclusionRemus facilitates the identification of regulatory regions potentially associated with a monogenic disease and can supplement classical analysis of coding variations with the aim of improving the diagnostic yield in whole-genome sequencing experiments.

Published

2021

27. Remus: A Web Application for Prioritization of Regulatory Regions and Variants in Monogenic Diseases.

Author

Sztromwasser, Paweł, Skrzypczak, Damian, Michalak, Arkadiusz, and Fendler, Wojciech

Subjects

GENETIC testing, PHENOTYPES, GENES, GENOMES, WEB-based user interfaces

Abstract

Background: Analysis of variants in distant regulatory elements could improve the current 25–50% yield of genetic testing for monogenic diseases. However, the vast size of the regulome, great number of variants, and the difficulty in predicting their phenotypic impact make searching for pathogenic variants in the regulatory genome challenging. New tools for the identification of regulatory variants based on their relevance to the phenotype are needed. Methods: We used tissue-specific regulatory loci mapped by ENCODE and FANTOM, together with miRNA–gene interactions from miRTarBase and miRWalk, to develop Remus, a web application for the identification of tissue-specific regulatory regions. Remus searches for regulatory features linked to the known disease-associated genes and filters them using activity status in the target tissues relevant for the studied disorder. For user convenience, Remus provides a web interface and facilitates in-browser filtering of variant files suitable for sensitive patient data. Results: To evaluate our approach, we used a set of 146 regulatory mutations reported causative for 68 distinct monogenic disorders and a manually curated a list of tissues affected by these disorders. In 89.7% of cases, Remus identified the regulator containing the pathogenic mutation. The tissue-specific search limited the number of considered variants by 82.5% as compared to a tissue-agnostic search. Conclusion: Remus facilitates the identification of regulatory regions potentially associated with a monogenic disease and can supplement classical analysis of coding variations with the aim of improving the diagnostic yield in whole-genome sequencing experiments. [ABSTRACT FROM AUTHOR]

Published

2021

28. Myopia-26, the female-limited form of early-onset high myopia, occurring in a European family.

Author

Széll, Noémi, Fehér, Tamás, Maróti, Zoltán, Kalmár, Tibor, Latinovics, Dóra, Nagy, István, Orosz, Zsuzsanna Z., Janáky, Márta, Facskó, Andrea, and Sohajda, Zoltán

Subjects

*DYSTROPHY, *MYOPIA, *VISUAL evoked potentials, *COLLATERAL circulation, *COLOR vision, *OPTICAL coherence tomography, *SYMPTOMS

Abstract

Background: Female-limited early-onset high myopia, also called Myopia-26 is a rare monogenic disorder characterized by severe short sightedness starting in early childhood and progressing to blindness potentially by the middle ages. Despite the X-linked locus of the mutated ARR3 gene, the disease paradoxically affects females only, with males being asymptomatic carriers. Previously, this disease has only been observed in Asian families and has not gone through detailed investigation concerning collateral symptoms or pathogenesis.Results: We found a large Hungarian family displaying female-limited early-onset high myopia. Whole exome sequencing of two individuals identified a novel nonsense mutation (c.214C>T, p.Arg72*) in the ARR3 gene. We carried out basic ophthalmological testing for 18 family members, as well as detailed ophthalmological examination (intraocular pressure, axial length, fundus appearance, optical coherence tomography, visual field- testing) as well as colour vision- and electrophysiology tests (standard and multifocal electroretinography, pattern electroretinography and visual evoked potentials) for eight individuals. Ophthalmological examinations did not reveal any signs of cone dystrophy as opposed to animal models. Electrophysiology and colour vision tests similarly did not evidence a general cone system alteration, rather a central macular dysfunction affecting both the inner and outer (postreceptoral and receptoral) retinal structures in all patients with ARR3 mutation.Conclusions: This is the first description of a Caucasian family displaying Myopia-26. We present two hypotheses that could potentially explain the pathomechanism of this disease. [ABSTRACT FROM AUTHOR]

Published

2021

29. Ultrarare heterozygous pathogenic variants of genes causing dominant forms of early-onset deafness underlie severe presbycusis.

Subjects

*PRESBYCUSIS, *HEARING disorders, *DOMINANCE (Genetics), *DEAFNESS, *INNER ear

Abstract

Presbycusis, or age-related hearing loss (ARHL), is a major public health issue. About half the phenotypic variance has been attributed to genetic factors. Here, we assessed the contribution to presbycusis of ultrarare pathogenic variants, considered indicative of Mendelian forms. We focused on severe presbycusis without environmental or comorbidity risk factors and studied multiplex family age-related hearing loss (mARHL) and simplex/sporadic age-related hearing loss (sARHL) cases and controls with normal hearing by whole-exome sequencing. Ultrarare variants (allele frequency [AF] < 0.0001) of 35 genes responsible for autosomal dominant early-onset forms of deafness, predicted to be pathogenic, were detected in 25.7% of mARHL and 22.7% of sARHL cases vs. 7.5% of controls (P = 0.001); half were previously unknown (AF < 0.000002). MYO6, MYO7A, PTPRQ, and TECTA variants were present in 8.9% of ARHL cases but less than 1% of controls. Evidence for a causal role of variants in presbycusis was provided by pathogenicity prediction programs, documented haploinsufficiency, three-dimensional structure/function analyses, cell biology experiments, and reported early effects. We also established Tmc1N321I/+ mice, carrying the TMC1:p.(Asn327Ile) variant detected in an mARHL case, as a mouse model for a monogenic form of presbycusis. Deafness gene variants can thus result in a continuum of auditory phenotypes. Our findings demonstrate that the genetics of presbycusis is shaped by not only well-studied polygenic risk factors of small effect size revealed by common variants but also, ultrarare variants likely resulting in monogenic forms, thereby paving the way for treatment with emerging inner ear gene therapy. [ABSTRACT FROM AUTHOR]

Published

2020

30. Monogenic etiologies of persistent human papillomavirus infections: A comprehensive systematic review.

Author

Biglari S, Moghaddam AS, Tabatabaiefar MA, Sherkat R, Youssefian L, Saeidian AH, Vahidnezhad F, Tsoi LC, Gudjonsson JE, Hakonarson H, Casanova JL, Béziat V, Jouanguy E, and Vahidnezhad H

Subjects

Humans, Child, Preschool, Child, Adolescent, Skin, Syndrome, Membrane Proteins genetics, Guanine Nucleotide Exchange Factors, Papillomavirus Infections complications, Papillomavirus Infections genetics, Warts genetics, Warts complications, Epidermodysplasia Verruciformis genetics, Epidermodysplasia Verruciformis complications

Abstract

Purpose: Persistent human papillomavirus infection (PHPVI) causes cutaneous, anogenital, and mucosal warts. Cutaneous warts include common warts, Treeman syndrome, and epidermodysplasia verruciformis, among others. Although more reports of monogenic predisposition to PHPVI have been published with the development of genomic technologies, genetic testing is rarely incorporated into clinical assessments. To encourage broader molecular testing, we compiled a list of the various monogenic etiologies of PHPVI., Methods: We conducted a systematic literature review to determine the genetic, immunological, and clinical characteristics of patients with PHPVI., Results: The inclusion criteria were met by 261 of 40,687 articles. In 842 patients, 83 PHPVI-associated genes were identified, including 42, 6, and 35 genes with strong, moderate, and weak evidence for causality, respectively. Autosomal recessive inheritance predominated (69%). PHPVI onset age was 10.8 ± 8.6 years, with an interquartile range of 5 to 14 years. GATA2,IL2RG,DOCK8, CXCR4, TMC6, TMC8, and CIB1 are the most frequently reported PHPVI-associated genes with strong causality. Most genes (74 out of 83) belong to a catalog of 485 inborn errors of immunity-related genes, and 40 genes (54%) are represented in the nonsyndromic and syndromic combined immunodeficiency categories., Conclusion: PHPVI has at least 83 monogenic etiologies and a genetic diagnosis is essential for effective management., Competing Interests: Conflict of Interest Jean-Laurent Casanova serves on the scientific advisory boards of ADMA Biologics Inc., Kymera Therapeutics, and Elixiron Immunotherapeutics., (Copyright © 2023 American College of Medical Genetics and Genomics. Published by Elsevier Inc. All rights reserved.)

Published

2024

31. Therapy Development by Genome Editing of Hematopoietic Stem Cells

Author

Lola Koniali, Carsten W. Lederer, and Marina Kleanthous

Subjects

genome editing, hematopoietic stem cell, blood disorders, gene therapy (GT), monogenic disorder, TALEN, Cytology, QH573-671

Abstract

Accessibility of hematopoietic stem cells (HSCs) for the manipulation and repopulation of the blood and immune systems has placed them at the forefront of cell and gene therapy development. Recent advances in genome-editing tools, in particular for clustered regularly interspaced short palindromic repeats (CRISPR)/CRISPR-associated protein (Cas) and CRISPR/Cas-derived editing systems, have transformed the gene therapy landscape. Their versatility and the ability to edit genomic sequences and facilitate gene disruption, correction or insertion, have broadened the spectrum of potential gene therapy targets and accelerated the development of potential curative therapies for many rare diseases treatable by transplantation or modification of HSCs. Ongoing developments seek to address efficiency and precision of HSC modification, tolerability of treatment and the distribution and affordability of corresponding therapies. Here, we give an overview of recent progress in the field of HSC genome editing as treatment for inherited disorders and summarize the most significant findings from corresponding preclinical and clinical studies. With emphasis on HSC-based therapies, we also discuss technical hurdles that need to be overcome en route to clinical translation of genome editing and indicate advances that may facilitate routine application beyond the most common disorders.

Published

2021

32. Disorders of Lipoprotein Metabolism

Author

Hegele, Robert A., Tonstad, Serena, Blau, Nenad, editor, Duran, Marinus, editor, Gibson, K Michael, editor, and Dionisi Vici, Carlo, editor

Published

2014

33. Recent Advances and Future Opportunities to Diagnose Male Infertility.

Author

Schilit, Samantha L. P.

Abstract

Purpose of Review: Infertility affects 10–15% of couples, making it one of the most frequent health disorders for individuals of reproductive age. The state of childlessness and efforts to restore fertility cause substantial emotional, social, and financial stress on couples. Male factors contribute to about half of all infertility cases, and yet are understudied relative to female factors. The result is that the majority of men with infertility lack specific causal diagnoses, which serves as a missed opportunity to inform therapies for these couples. Recent Findings: In this review, we describe current standards for diagnosing male infertility and the various interventions offered to men in response to differential diagnoses. We then discuss recent advances in the field of genetics to identify novel etiologies for formerly unexplained infertility. Summary: With a specific genetic diagnosis, male factors can be addressed with appropriate reproductive counseling and with potential access to assisted reproductive technologies to improve chances of a healthy pregnancy. [ABSTRACT FROM AUTHOR]

Published

2019

34. Genetic Enhancement of Human Beings: Reality or Fiction?

Author

Nelis, Annemiek, Posthuma, Danielle, Koops, Bert Jaap, editor, Lüthy, Christoph H., editor, Nelis, Annemiek, editor, Sieburgh, Carla, editor, Jansen, J.P.M., editor, and Schmid, Monika S., editor

Published

2013

35. Genetic Analyses in Health Laboratories: Current Status and Expectations

Author

Finotti, Alessia, Breveglieri, Giulia, Borgatti, Monica, Gambari, Roberto, Spoto, Giuseppe, editor, and Corradini, Roberto, editor

Published

2012

36. Introduction to Molecular Genetics

Author

Mannens, M. M. A. M., Smeets, H. J. M., Baars, H.F., editor, Doevendans, P.A.F.M., editor, and van der Smagt, J.J., editor

Published

2011

37. Rare Inherited Diseases and Vitiligo

Author

Taïeb, Alain, Morice-Picard, Fanny, Picardo, Mauro, editor, and Taïeb, Alain, editor

Published

2010

38. Sollen die Indikationen für nichtinvasive Pränataltests erweitert werden?

Author

Stumm, M. and Schröer, A.

Abstract

Copyright of Der Gynäkologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

39. Molecular Genetics in Cardiology

Author

Mannens, M. M. A. M., Smeets, H. J. M., Doevendans, P. A., editor, and Wilde, A. A. M., editor

Published

2001

40. Preimplantation Genetic Diagnosis (PGD) for Monogenic Disorders: the Value of Concurrent Aneuploidy Screening.

Author

Goldman, Kara, Nazem, Taraneh, Berkeley, Alan, Palter, Steven, and Grifo, Jamie

Abstract

Pre-implantation genetic diagnosis (PGD) has changed the landscape of clinical genetics by helping families reduce the transmission of monogenic disorders. However, given the high prevalence of embryonic aneuploidy, particularly in patients of advanced reproductive age, unaffected embryos remain at high risk of implantation failure or pregnancy loss due to aneuploidy. 24-chromosome aneuploidy screening has become widely utilized in routine in vitro fertilization (IVF) to pre-select embryos with greater pregnancy potential, but concurrent 24-chromosome aneuploidy screening has not become standard practice in embryos biopsied for PGD. We performed a retrospective cohort study of patients who underwent PGD with or without 24-chromosome aneuploidy screening to explore the value of concurrent screening. Among the PGD + aneuploidy-screened group ( n = 355 blastocysts), only 25.6 % of embryos were both Single Gene Disorder (SGD)-negative (or carriers) and euploid; thus the majority of embryos were ineligible for transfer due to the high prevalence of aneuploidy. Despite a young mean age (32.4 ± 5.9y), 49.9 % of Blastocysts were aneuploid. The majority of patients (53.2 %) had ≥1 blastocyst that was Single Gene Disorder (SGD)-unaffected but aneuploid; without screening, these unaffected but aneuploid embryos would likely have been transferred resulting in implantation failure, pregnancy loss, or a pregnancy affected by chromosomal aneuploidy. Despite the transfer of nearly half the number of embryos in the aneuploidy-screened group (1.1 ± 0.3 vs. 1.9 ± 0.6, p < 0.0001), the implantation rate was higher (75 % vs. 53.3 %) and miscarriage rate lower (20 % vs. 40 %) (although not statistically significant). 24-chromosome aneuploidy screening when performed concurrently with PGD provides valuable information for embryo selection, and notably improves single embryo transfer rates. [ABSTRACT FROM AUTHOR]

Published

2016

41. Development and validation of concurrent preimplantation genetic diagnosis for single gene disorders and comprehensive chromosomal aneuploidy screening without whole genome amplification.

Author

Zimmerman, Rebekah S., Jalas, Chaim, Tao, Xin, Fedick, Anastasia M., Kim, Julia G., Pepe, Russell J., Northrop, Lesley E., Jr.Scott, Richard T., Treff, Nathan R., and Scott, Richard T Jr

Subjects

*PREIMPLANTATION genetic diagnosis, *ANEUPLOIDY, *GENE amplification, *POLYMERASE chain reaction, *FIBROBLASTS, *HEALTH outcome assessment

Abstract

Objective: To develop a novel and robust protocol for multifactorial preimplantation genetic testing of trophectoderm biopsies using quantitative polymerase chain reaction (qPCR).Design: Prospective and blinded.Setting: Not applicable.Patient(s): Couples indicated for preimplantation genetic diagnosis (PGD).Intervention(s): None.Main Outcome Measure(s): Allele dropout (ADO) and failed amplification rate, genotyping consistency, chromosome screening success rate, and clinical outcomes of qPCR-based screening.Result(s): The ADO frequency on a single cell from a fibroblast cell line was 1.64% (18/1,096). When two or more cells were tested, the ADO frequency dropped to 0.02% (1/4,426). The rate of amplification failure was 1.38% (55/4,000) overall, with 2.5% (20/800) for single cells and 1.09% (35/3,200) for samples that had two or more cells. Among 152 embryos tested in 17 cases by qPCR-based PGD and CCS, 100% were successfully given a diagnosis, with 0% ADO or amplification failure. Genotyping consistency with reference laboratory results was >99%. Another 304 embryos from 43 cases were included in the clinical application of qPCR-based PGD and CCS, for which 99.7% (303/304) of the embryos were given a definitive diagnosis, with only 0.3% (1/304) having an inconclusive result owing to recombination. In patients receiving a transfer with follow-up, the pregnancy rate was 82% (27/33).Conclusion(s): This study demonstrates that the use of qPCR for PGD testing delivers consistent and more reliable results than existing methods and that single gene disorder PGD can be run concurrently with CCS without the need for additional embryo biopsy or whole genome amplification. [ABSTRACT FROM AUTHOR]

Published

2016

42. Genetic Relationship Between the Psychoses — Implications for Genetic Modeling

Author

Propping, P., Marneros, Andreas, editor, and Tsuang, Ming T., editor

Published

1990

43. Novel personalized therapies for cystic fibrosis: treating the basic defect in all patients.

Author

Amaral, M. D.

Subjects

*CYSTIC fibrosis treatment, *CYSTIC fibrosis transmembrane conductance regulator, *ANTIBIOTICS, *GENETIC mutation, *CAUCASIAN race

Abstract

Cystic fibrosis ( CF) is the most common genetic life-shortening condition in Caucasians. Despite being a multi-organ disease, CF is classically diagnosed by symptoms of acute/chronic respiratory disease, with persistent pulmonary infections and mucus plugging of the airways and failure to thrive. These multiple symptoms originate from dysfunction of the CF transmembrane conductance regulator ( CFTR) protein, a channel that mediates anion transport across epithelia. Indeed, establishment of a definite CF diagnosis requires proof of CFTR dysfunction, commonly through the so-called sweat Cl− test. Many drug therapies, including mucolytics and antibiotics, aim to alleviate the symptoms of CF lung disease. However, new therapies to modulate defective CFTR, the basic defect underlying CF, have started to reach the clinic, and several others are in development or in clinical trials. The novelty of these therapies is that, besides targeting the basic defect underlying CF, they are mutation specific. Indeed, even this monogenic disease is influenced by a large number of different genes and biological pathways as well as by environmental factors that are difficult to assess. Accordingly, every person with CF is unique and so functional assessment of patients' tissues ex vivo is key for diagnosing and predicting the severity of this disease. Of note, such assessment will also be crucial to assess drug responses, in order to effectively treat all CF patients. It is not because it is a monogenic disorder that personalized treatment for CF is much easier than for complex disorders. [ABSTRACT FROM AUTHOR]

Published

2015

44. A cost-effectiveness analysis of genomic sequencing in a prospective versus historical cohort of complex pediatric patients.

Author

McEwan C., White S.M., Smagarinsky Y., Martyn M., Goranitis I., Gaff C., Yeung A., Tan N.B., Tan T.Y., Stark Z., Brown N., Hunter M.F., Delatycki M., Stutterd C., Savarirayan R., Mcgillivray G., Stapleton R., Kumble S., Downie L., Regan M., Lunke S., Chong B., Phelan D., Brett G.R., Jarmolowicz A., Prawer Y., Valente G., McEwan C., White S.M., Smagarinsky Y., Martyn M., Goranitis I., Gaff C., Yeung A., Tan N.B., Tan T.Y., Stark Z., Brown N., Hunter M.F., Delatycki M., Stutterd C., Savarirayan R., Mcgillivray G., Stapleton R., Kumble S., Downie L., Regan M., Lunke S., Chong B., Phelan D., Brett G.R., Jarmolowicz A., Prawer Y., and Valente G.

Abstract

Purpose: Cost-effectiveness evaluations of first-line genomic sequencing (GS) in the diagnosis of children with genetic conditions are limited by the lack of well-defined comparative cohorts. We sought to evaluate the cost-effectiveness of early GS in pediatric patients with complex monogenic conditions compared with a matched historical cohort. Method(s): Data, including investigation costs, were collected in a prospective cohort of 92 pediatric patients undergoing singleton GS over an 18-month period (2016-2017) with two of the following: a condition with high mortality, multisystem disease involving three or more organs, or severe limitation of daily function. Comparative data were collected in a matched historical cohort who underwent traditional investigations in the years 2012-2013. Result(s): GS yielded a diagnosis in 42% while traditional investigations yielded a diagnosis in 23% (p = 0.003). A change in management was experienced by 74% of patients diagnosed following GS, compared with 32% diagnosed following traditional investigations. Singleton GS at a cost of AU$3100 resulted in a mean saving per person of AU$3602 (95% confidence interval [CI] AU$2520-4685). Cost savings occurred across all investigation subtypes and were only minimally offset by clinical management costs. Conclusion(s): GS in complex pediatric patients saves significant costs and doubles the diagnostic yield of traditional approaches.Copyright © 2020, American College of Medical Genetics and Genomics.

Published

2020

45. A national approach to rapid genomic diagnosis in acute paediatrics.

Author

Tan N.B., Patel C., Wilson M., Pinner J., Sandaradura S.A., Mowat D., Kirk E., Hunter M.F., Krzesinski E.I., Barnett C., Akesson L.S., Richmond C.M., Kumble S., Hunt L., Eggers S., Riseley J., Chong B., Phelan D., Sadedin S., Martyn M., Goranitis I., Best S., Buckley M.F., Roscioli T., Christodoulou J., Stark Z., Lunke S., Fennell A., Rogers J., Higgins M., Vasudevan A., Howell K.B., White S.M., De Silva M.G., Brett G.R., Gallacher L., Ayres S., Boggs K., Bray A., Baxendale A., Borrie S., King-Smith S., Quinn M.C., Fowles L., Tan N.B., Patel C., Wilson M., Pinner J., Sandaradura S.A., Mowat D., Kirk E., Hunter M.F., Krzesinski E.I., Barnett C., Akesson L.S., Richmond C.M., Kumble S., Hunt L., Eggers S., Riseley J., Chong B., Phelan D., Sadedin S., Martyn M., Goranitis I., Best S., Buckley M.F., Roscioli T., Christodoulou J., Stark Z., Lunke S., Fennell A., Rogers J., Higgins M., Vasudevan A., Howell K.B., White S.M., De Silva M.G., Brett G.R., Gallacher L., Ayres S., Boggs K., Bray A., Baxendale A., Borrie S., King-Smith S., Quinn M.C., and Fowles L.

Abstract

Introduction: Implementation of rapid genomic testing in neonatal and paediatric intensive care units (NICUs/PICUs) is gathering momentum, and requires the development of systems capable of consistent delivery across multi-site networks. Method(s): We developed a rapid genomic diagnosis program involving 10 Australian hospitals and two laboratories with the aim of providing test results in <5 days for acutely unwell paediatric patients with suspected monogenic disorders. Rapid exome sequencing (rES) was performed as trios when possible, and analysis utilised multidisciplinary expertise. Experience was shared between clinical sites, laboratories, and professional groups to enable collective learning. Result(s): The program considered 123 patients for rES over 10 months, and approved 114 (93%). Five families declined testing (4.4%), and nine (7.9%) were withdrawn due to change in clinical circumstances. Of 100 patients tested, 51 received a diagnosis. Eleven of the diagnoses (21%) were made using approaches augmenting standard ES analysis: mitochondrial genome sequencing, ES-based copy number analysis, matchmaking of emerging genes, reverse phenotyping and RNA analysis. Median time from hospital admission to consent was 6 days (range 0-64 days); median time from sample receipt to clinical ES report was 3 days (range 2-7 days). The total cost of testing was AU$1,123,000/701,638 (AU$11,230/7,016 per case). Changes in management following a result occurred in 77% of diagnosed patients and 10% of undiagnosed patients. Conclusion(s): We demonstrate the feasibility of a national, highly integrated clinical-laboratory approach to rapid genomic diagnosis, which delivers results within a timeframe relevant to acute paediatrics, while optimising clinical utility and resource allocation.

Published

2020

46. Feasibility of Ultra-Rapid Exome Sequencing in Critically Ill Infants and Children with Suspected Monogenic Conditions in the Australian Public Health Care System.

Author

Tan T.Y., Springer A., Tan N.B., Temple S.L., Theda C., Vasudevan A., White S.M., Yeung A., Zhu Y., Martyn M., Best S., Roscioli T., Christodoulou J., Stark Z., Lunke S., Eggers S., Wilson M., Patel C., Barnett C.P., Pinner J., Sandaradura S.A., Buckley M.F., Krzesinski E.I., De Silva M.G., Brett G.R., Boggs K., Mowat D., Kirk E.P., Ades L.C., Akesson L.S., Amor D.J., Ayres S., Baxendale A., Borrie S., Bray A., Brown N.J., Chan C.Y., Chong B., Cliffe C., Delatycki M.B., Edwards M., Elakis G., Fahey M.C., Fennell A., Fowles L., Gallacher L., Higgins M., Howell K.B., Hunt L., Hunter M.F., Jones K.J., King S., Kumble S., Lang S., Le Moing M., Ma A., Phelan D., Quinn M.C.J., Richards A., Richmond C.M., Riseley J., Rodgers J., Sachdev R., Sadedin S., Schlapbach L.J., Smith J., Tan T.Y., Springer A., Tan N.B., Temple S.L., Theda C., Vasudevan A., White S.M., Yeung A., Zhu Y., Martyn M., Best S., Roscioli T., Christodoulou J., Stark Z., Lunke S., Eggers S., Wilson M., Patel C., Barnett C.P., Pinner J., Sandaradura S.A., Buckley M.F., Krzesinski E.I., De Silva M.G., Brett G.R., Boggs K., Mowat D., Kirk E.P., Ades L.C., Akesson L.S., Amor D.J., Ayres S., Baxendale A., Borrie S., Bray A., Brown N.J., Chan C.Y., Chong B., Cliffe C., Delatycki M.B., Edwards M., Elakis G., Fahey M.C., Fennell A., Fowles L., Gallacher L., Higgins M., Howell K.B., Hunt L., Hunter M.F., Jones K.J., King S., Kumble S., Lang S., Le Moing M., Ma A., Phelan D., Quinn M.C.J., Richards A., Richmond C.M., Riseley J., Rodgers J., Sachdev R., Sadedin S., Schlapbach L.J., and Smith J.

Abstract

Importance: Widespread adoption of rapid genomic testing in pediatric critical care requires robust clinical and laboratory pathways that provide equitable and consistent service across health care systems. Objective(s): To prospectively evaluate the performance of a multicenter network for ultra-rapid genomic diagnosis in a public health care system. Design, Setting, and Participant(s): Descriptive feasibility study of critically ill pediatric patients with suspected monogenic conditions treated at 12 Australian hospitals between March 2018 and February 2019, with data collected to May 2019. A formal implementation strategy emphasizing communication and feedback, standardized processes, coordination, distributed leadership, and collective learning was used to facilitate adoption. Exposures: Ultra-rapid exome sequencing. Main Outcomes and Measures: The primary outcome was time from sample receipt to ultra-rapid exome sequencing report. The secondary outcomes were the molecular diagnostic yield, the change in clinical management after the ultra-rapid exome sequencing report, the time from hospital admission to the laboratory report, and the proportion of laboratory reports returned prior to death or hospital discharge. Result(s): The study population included 108 patients with a median age of 28 days (range, 0 days to 17 years); 34% were female; and 57% were from neonatal intensive care units, 33% were from pediatric intensive care units, and 9% were from other hospital wards. The mean time from sample receipt to ultra-rapid exome sequencing report was 3.3 days (95% CI, 3.2-3.5 days) and the median time was 3 days (range, 2-7 days). The mean time from hospital admission to ultra-rapid exome sequencing report was 17.5 days (95% CI, 14.6-21.1 days) and 93 reports (86%) were issued prior to death or hospital discharge. A molecular diagnosis was established in 55 patients (51%). Eleven diagnoses (20%) resulted from using the following approaches to augment standard exome

Published

2020

47. Human induced pluripotent cells in personalized treatment of monogenic epilepsies

Author

Mohammadi, Nazanin A., Freude, Kristine, Haukedal, Henriette, Tümer, Zeynep, Møller, Rikke S., Mohammadi, Nazanin A., Freude, Kristine, Haukedal, Henriette, Tümer, Zeynep, and Møller, Rikke S.

Abstract

The broad application of next-generation sequencing in genetic diagnostics opens up vast possibilities for personalized treatment of patients with genetic disorders including monogenic epilepsies. To translate genetic findings into personalized medicine, mechanistic studies of the individual pathogenic variants and drug screening in patient-specificin vitro models are very crucial. Recently, human induced pluripotent stem cell (hiPSC) technologies have made it possible to generate patient-specific pluripotent cells, which can be directed to differentiate into any given cell type. These hiPSCs are ideal for generating neurons to investigate specific neurological/ neurodevelopmental disorders. While two-dimensional single-cell models of hiPSC-derived neurons provide reliable investigation of synaptic transmission and plasticity, cerebral organoids are superior in regard to functional characterization and the study of cell-cell interactions in three-dimensional structures. In this review, we focus on monogenic epilepsies and discuss the application of hiPSC models in personalized drug treatment based on the patient’s specific genetic variants.

Published

2020

48. Myopia-26, the female-limited form of early-onset high myopia, occurring in a European family

Author

Zsuzsanna Z. Orosz, Zoltán Sohajda, Tamás Fehér, Andrea Facskó, István Nagy, Zoltán Maróti, Márta Janáky, Noémi Széll, Dóra Latinovics, and Tibor Kalmár

Subjects

Male, 0301 basic medicine, Intraocular pressure, medicine.medical_specialty, genetic structures, DNA Mutational Analysis, Nonsense mutation, lcsh:Medicine, Monogenic disorder, Disease, Fundus (eye), 03 medical and health sciences, 0302 clinical medicine, Cone dystrophy, Ophthalmology, Electroretinography, Myopia, medicine, Humans, Pharmacology (medical), Genetics (clinical), Exome sequencing, Early onset high myopia, X-arrestin, business.industry, Research, lcsh:R, General Medicine, ARR3, Middle Aged, Mendelian inheritance, medicine.disease, eye diseases, X-linked female-limited high myopia, Pedigree, Visual field, 030104 developmental biology, Child, Preschool, G-protein coupled receptor, Mutation, 030221 ophthalmology & optometry, Evoked Potentials, Visual, Intrinsically photosensitive retinal ganglion cell, Female, business, Asymptomatic carrier, Tomography, Optical Coherence

Abstract

Background Female-limited early-onset high myopia, also called Myopia-26 is a rare monogenic disorder characterized by severe short sightedness starting in early childhood and progressing to blindness potentially by the middle ages. Despite the X-linked locus of the mutated ARR3 gene, the disease paradoxically affects females only, with males being asymptomatic carriers. Previously, this disease has only been observed in Asian families and has not gone through detailed investigation concerning collateral symptoms or pathogenesis. Results We found a large Hungarian family displaying female-limited early-onset high myopia. Whole exome sequencing of two individuals identified a novel nonsense mutation (c.214C>T, p.Arg72*) in the ARR3 gene. We carried out basic ophthalmological testing for 18 family members, as well as detailed ophthalmological examination (intraocular pressure, axial length, fundus appearance, optical coherence tomography, visual field- testing) as well as colour vision- and electrophysiology tests (standard and multifocal electroretinography, pattern electroretinography and visual evoked potentials) for eight individuals. Ophthalmological examinations did not reveal any signs of cone dystrophy as opposed to animal models. Electrophysiology and colour vision tests similarly did not evidence a general cone system alteration, rather a central macular dysfunction affecting both the inner and outer (postreceptoral and receptoral) retinal structures in all patients with ARR3 mutation. Conclusions This is the first description of a Caucasian family displaying Myopia-26. We present two hypotheses that could potentially explain the pathomechanism of this disease.

Published

2021

49. Ultrarare heterozygous pathogenic variants of genes causing dominant forms of early-onset deafness underlie severe presbycusis

Author

Christian Renard, Christine Petit, Yosra Bouyacoub, Sedigheh Delmaghani, Magali Niasme-Grare, Nicolas Michalski, Hung Thai-Van, Olivier Deguine, Anne Aubois, Arnaud Deveze, Jean-Pierre Lavieille, Valérie Franco-Vidal, Anne-Laure Roudevitch-Pujol, Amrit Singh-Estivalet, Arnaud Coez, Vincent Michel, Christophe Vincent, Hugues Aschard, Claire Thibult-Apt, Amel Bahloul, Sophie Boucher, E. Ionescu, Bernard Fraysse, Fabienne Wong Jun Tai, Fabrice Giraudet, Vincent Darrouzet, Typhaine Dupont, Nicolas Wolff, Didier Bouccara, Lionel Collet, Crystel Bonnet, Gaelle M. Lefèvre, Jean-Louis Kemeny, Andrea Lelli, Eric Bizaguet, Paul Avan, Institut de l'Audition [Paris] (IDA), Institut Pasteur [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), ED 515 - Complexité du vivant, Sorbonne Université (SU), Centre Hospitalier Universitaire d'Angers (CHU Angers), PRES Université Nantes Angers Le Mans (UNAM), Université d'Angers (UA), CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Récepteurs Canaux - Channel Receptors, Centre National de la Recherche Scientifique (CNRS)-Institut Pasteur [Paris], Hôpital Beaujon [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), CHU Toulouse [Toulouse], Centre Hospitalier Lyon Sud [CHU - HCL] (CHLS), Hospices Civils de Lyon (HCL), Hôpital Edouard Herriot [CHU - HCL], Université Claude Bernard Lyon 1 (UCBL), Université de Lyon, CHU Gabriel Montpied [Clermont-Ferrand], CHU Clermont-Ferrand, Université Clermont Auvergne (UCA), Hôpital Nord [CHU - APHM], Centre Hospitalier National d'Ophtalmologie des Quinze-Vingts (CHNO), Hôpital Roger Salengro [Lille], Laboratoire d’Audiologie Renard, Hôpital Pellegrin, CHU Bordeaux [Bordeaux]-Groupe hospitalier Pellegrin, Laboratoire de correction auditive Eric Bizaguet, CEA- Saclay (CEA), Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Centre de Bioinformatique, Biostatistique et Biologie Intégrative (C3BI), Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS), Centre Jean Perrin [Clermont-Ferrand] (UNICANCER/CJP), UNICANCER, Chaire Génétique et physiologie cellulaire, Collège de France (CdF (institution)), This work was supported by a grant from Fondation pour l’Audition (to C.P.), LabEx Lifesenses Grant ANR-10-LABX-65, and Light4deaf Grant ANR-15-RHUS-0001., We thank the patients for participating in this study and Céline Trébeau for technical assistance. S.B. received funding from the University of Angers (Medical School), the University Hospital of Angers, and the Collège Français d’oto-rhino-laryngologistes., ANR-10-LABX-0065,LIFESENSES,DES SENS POUR TOUTE LA VIE(2010), ANR-15-RHUS-0001,LIGHT4DEAF,ECLAIRER LA SURDITÉ : UNE APPROCHE HOLISTIQUE DU SYNDROME D'USHER(2015), Institut Pasteur [Paris] (IP)-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), Centre Hospitalier Universitaire de Toulouse (CHU Toulouse), Collège de France - Chaire Génétique et physiologie cellulaire, Bonnet, Crystel, DES SENS POUR TOUTE LA VIE - - LIFESENSES2010 - ANR-10-LABX-0065 - LABX - VALID, and ECLAIRER LA SURDITÉ : UNE APPROCHE HOLISTIQUE DU SYNDROME D'USHER - - LIGHT4DEAF2015 - ANR-15-RHUS-0001 - RHUS - VALID

Subjects

0301 basic medicine, Presbycusis, [SDV.GEN] Life Sciences [q-bio]/Genetics, Deafness, Cohort Studies, Mice, 0302 clinical medicine, MESH: Presbycusis, MESH: Animals, Age of Onset, MESH: Cohort Studies, Genes, Dominant, Early onset, MESH: Heterozygote, Genetics, Multidisciplinary, monogenic disorder, Age Factors, Biological Sciences, Phenotype, MESH: Case-Control Studies, Mitochondria, 3. Good health, age-related hearing loss, symbols, MESH: Membrane Proteins, medicine.symptom, Heterozygote, MESH: Mutation, Hearing loss, MESH: Mitochondria, MESH: Age of Onset, MESH: Deafness, Biology, 03 medical and health sciences, symbols.namesake, MESH: Whole Exome Sequencing, Exome Sequencing, medicine, Animals, Humans, Allele frequency, Gene, ultrarare variants, MESH: Mice, MESH: Age Factors, [SDV.GEN]Life Sciences [q-bio]/Genetics, MESH: Humans, Membrane Proteins, Tmc1, medicine.disease, Comorbidity, MicroRNAs, 030104 developmental biology, Case-Control Studies, Mutation, Mendelian inheritance, MESH: Genes, Dominant, presbycusis, MESH: MicroRNAs, 030217 neurology & neurosurgery

Abstract

International audience; Presbycusis, or age-related hearing loss (ARHL), is a major public health issue. About half the phenotypic variance has been attributed to genetic factors. Here, we assessed the contribution to presbycusis of ultrarare pathogenic variants, considered indicative of Mendelian forms. We focused on severe presbycusis without environmental or comorbidity risk factors and studied multiplex family age-related hearing loss (mARHL) and simplex/sporadic age-related hearing loss (sARHL) cases and controls with normal hearing by whole-exome sequencing. Ultrarare variants (allele frequency [AF] < 0.0001) of 35 genes responsible for autosomal dominant early-onset forms of deafness, predicted to be pathogenic, were detected in 25.7% of mARHL and 22.7% of sARHL cases vs. 7.5% of controls ( P = 0.001); half were previously unknown (AF < 0.000002). MYO6 , MYO7A , PTPRQ , and TECTA variants were present in 8.9% of ARHL cases but less than 1% of controls. Evidence for a causal role of variants in presbycusis was provided by pathogenicity prediction programs, documented haploinsufficiency, three-dimensional structure/function analyses, cell biology experiments, and reported early effects. We also established Tmc1 N321I/+ mice, carrying the TMC1 :p.(Asn327Ile) variant detected in an mARHL case, as a mouse model for a monogenic form of presbycusis. Deafness gene variants can thus result in a continuum of auditory phenotypes. Our findings demonstrate that the genetics of presbycusis is shaped by not only well-studied polygenic risk factors of small effect size revealed by common variants but also, ultrarare variants likely resulting in monogenic forms, thereby paving the way for treatment with emerging inner ear gene therapy.

Published

2020

50. Preimplantation Diagnosis for Single Gene Disorders.

Author

Berger, Victoria K. and Baker, Valerie L.

Subjects

*GENETIC disorder diagnosis, *HUMAN chromosome abnormality diagnosis, *EMBRYOLOGY, *PREGNANCY, *HUMAN embryo transfer

Abstract

Preimplantation genetic diagnosis (PGD) allows patients who are carriers or who are affected by genetic diseases to select unaffected embryos for transfer before becoming pregnant. The practice of PGD is evolving with rapid advances in technology and biopsy methods. Testing for a specific gene mutation can be performed in combination with 24-chromosome aneuploidy screening. Several unique applications of PGD are reviewed, including exclusion diagnosis for couples from Huntington disease families, testing for fragile X premutations, and human leukocyte antigen matching for stem cell donor siblings. Although PGD for single gene mutations allows patients to gain information about their embryos and perhaps avoid a difficult decision about whether or not to terminate an ongoing pregnancy, this technique also provides for much ethical debate encompassing the well-being of the prospective couple, embryo, child, and people in the community affected by the diseases being screened. [ABSTRACT FROM AUTHOR]

Published

2014