Your search keyword '"Genes, Modifier"' showing total 199 results

1. Variants in Genes of Calpain System as Modifiers of Spinocerebellar Ataxia Type 3 Phenotype

Author

Maria Luiza Saraiva-Pereira, Ana Carolina Martins, Mariana Rieck, Laura Bannach Jardim, and Vanessa Bielefeldt Leotti

Subjects

Adult, Male, 0301 basic medicine, Heterozygote, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Genotype, medicine, Humans, Allele, Calpastatin, Genetics, Genes, Modifier, Calpain, Calcium-Binding Proteins, Haplotype, Machado-Joseph Disease, General Medicine, Middle Aged, medicine.disease, Pedigree, Phenotype, 030104 developmental biology, Mutation, Spinocerebellar ataxia, Female, Trinucleotide Repeat Expansion, Trinucleotide repeat expansion, Machado–Joseph disease, 030217 neurology & neurosurgery

Abstract

Calpain-mediated proteolysis has been proposed to modulate the pathogenesis of spinocerebellar ataxia type 3, also known as Machado-Joseph disease (SCA3/MJD), a disorder due to a CAG repeat expansion (CAGexp) at ATXN3. We aimed to investigate if single-nucleotide polymorphisms (SNPs) at calpain gene CAPN2 and at calpastatin gene CAST modulate the age at onset (AO) and disease progression in SCA3/MJD. A total of 287 SCA3/MJD symptomatic subjects (151 families) were included. AO was analyzed and controlled by the CAG repeat length of expanded allele and family. Candidate polymorphisms were chosen based on the literature and on a priori criteria. The CAG repeat length and SNPs were genotyped according to standard methods. AO of carriers of AA and AG + GGrs1559085 genotypes in CAST and with the median value of 75 repeats at the expanded allele were 34.23 (33.07–35.38) and 36.42 years (34.50–38.34), respectively (p = 0.049, mixed model treating the expanded CAG repeat size as fixed effect and family as random effect). Carriers of haplotype Crs27852/Grs1559085 had mean AO of 37.23 (12.76) and 33.42 years (12.20) (p = 0.047, Student’s t test). Our data suggest an association between allele Grs1559085 and haplotype Crs27852/Grs1559085 at CAST and variations in the AO of SCA3/MJD subjects, independent from the effects of the CAGexp and family. The present results support the potential role of calpain cleavage pathway over modulation of SCA3/MJD phenotype.

Published

2021

2. Genetic modifiers regulating DNA replication and double strand break repair are associated with differences in mammary tumors in mouse models of Li-Fraumeni Syndrome

Author

Amy L. Roberts, Kim Joana Maurus, Jacob A. Mayfield, D. Joseph Jerry, Divyen H. Patel, Sallie S. Schneider, Evan Savage, Nicholas B. Griner, Lisa Wiesmüller, Trevor A Baptiste, Shannon Compton, Prabin Dhangada Majhi, Anneke C. Blackburn, Jeffrey J. Kane, and Karen A. Dunphy

Subjects

0301 basic medicine, Genetic modifiers, DNA Replication, Cancer Research, DNA Repair, DNA repair, DNA damage, Genetic Linkage, animal diseases, Congenic, Locus (genetics), Genetic mapping, Breast Neoplasms, Biology, Polymorphism, Single Nucleotide, Article, Li-Fraumeni Syndrome, 03 medical and health sciences, Mice, 0302 clinical medicine, Breast cancer, Replication-associated repair, Genetics, Animals, DNA Breaks, Double-Stranded, TP53, Allele, Molecular Biology, Gene, Chromosome 7 (human), Mice, Knockout, Genes, Modifier, DNA replication, Chromosome Mapping, Recombinational DNA Repair, Molecular biology, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, Genetic Loci, 030220 oncology & carcinogenesis, Female, Disease Susceptibility, Tumor Suppressor Protein p53

Abstract

Breast cancer is the most common tumor among women with inherited variants in the TP53 tumor suppressor, but onset varies widely suggesting interactions with genetic or environmental factors. Rodent models haploinsufficent for Trp53 also develop a wide variety of malignancies associated with Li-Fraumeni Syndrome, but BALB/c mice are uniquely susceptible to mammary tumors and is genetically linked to the Suprmam1 locus on chromosome 7. To define mechanisms that interact with deficiencies in p53 to alter susceptibility to mammary tumors, we fine-mapped the Suprmam1 locus in females from an N2 backcross of BALB/cMed and C57BL/6J mice. A major modifier was localized within a 10 cM interval on chromosome 7. The effect of the locus on DNA damage responses was examined in the parental strains and mice that are congenic for C57BL/6J alleles on the BALB/cMed background (SM1-Trp53+/−). The mammary epithelium of C57BL/6J-Trp53+/− females exhibited little radiation-induced apoptosis compared to BALB/cMed-Trp53+/− and SM1-Trp53+/− females indicating that the Suprmam1B6/B6 alleles could not rescue repair of radiation-induced DNA double-strand breaks mostly relying on non-homologous end joining. In contrast, the Suprmam1B6/B6 alleles in SM1-Trp53+/− mice were sufficient to confer the C57BL/6J-Trp53+/− phenotypes in homology-directed repair and replication fork progression. The Suprmam1B6/B6 alleles in SM1-Trp53+/− mice appear to act in trans to regulate a panel of DNA repair and replication genes which lie outside the locus. Significance: Genetic variation in replication-associated DNA repair can modify consequences of heterozygous mutations in Trp53 and contribute to susceptibility to mammary tumors in mouse models of Li-Fraumeni syndrome.

Published

2021

3. FAN1, a DNA Repair Nuclease, as a Modifier of Repeat Expansion Disorders

Author

Gagan B. Panigrahi, Jean-Yves Masson, Amit Laxmikant Deshmukh, Antonio Porro, Mohiuddin Mohiuddin, Stella Lanni, Christopher E. Pearson, Alessandro A. Sartori, Marie-Christine Caron, University of Zurich, Jones, Lesley, Pearson, Christopher E, and Wheeler, Vanessa

Subjects

0301 basic medicine, DNA Repair, DNA repair, 2804 Cellular and Molecular Neuroscience, Clinical Neurology, 610 Medicine & health, Review, Biology, Genomic Instability, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Huntington's disease, FAN1, medicine, Animals, Humans, Spinocerebellar Ataxias, Copy-number variation, nuclease, Gene, repeat instability, Genetics, modifier, Endodeoxyribonucleases, Genes, Modifier, 10061 Institute of Molecular Cancer Research, medicine.disease, Multifunctional Enzymes, FMR1, karyomegalic interstitial nephritis, Exodeoxyribonucleases, Huntington Disease, 2728 Neurology (clinical), 030104 developmental biology, Spinocerebellar ataxia, 570 Life sciences, biology, Neurology (clinical), Trinucleotide Repeat Expansion, Trinucleotide repeat expansion, 030217 neurology & neurosurgery, Huntington’s disease

Abstract

FAN1 encodes a DNA repair nuclease. Genetic deficiencies, copy number variants, and single nucleotide variants of FAN1 have been linked to karyomegalic interstitial nephritis, 15q13.3 microdeletion/microduplication syndrome (autism, schizophrenia, and epilepsy), cancer, and most recently repeat expansion diseases. For seven CAG repeat expansion diseases (Huntington’s disease (HD) and certain spinocerebellar ataxias), modification of age of onset is linked to variants of specific DNA repair proteins. FAN1 variants are the strongest modifiers. Non-coding disease-delaying FAN1 variants and coding disease-hastening variants (p.R507H and p.R377W) are known, where the former may lead to increased FAN1 levels and the latter have unknown effects upon FAN1 functions. Current thoughts are that ongoing repeat expansions in disease-vulnerable tissues, as individuals age, promote disease onset. Fan1 is required to suppress against high levels of ongoing somatic CAG and CGG repeat expansions in tissues of HD and FMR1 transgenic mice respectively, in addition to participating in DNA interstrand crosslink repair. FAN1 is also a modifier of autism, schizophrenia, and epilepsy. Coupled with the association of these diseases with repeat expansions, this suggests a common mechanism, by which FAN1 modifies repeat diseases. Yet how any of the FAN1 variants modify disease is unknown. Here, we review FAN1 variants, associated clinical effects, protein structure, and the enzyme’s attributed functional roles. We highlight how variants may alter its activities in DNA damage response and/or repeat instability. A thorough awareness of the FAN1 gene and FAN1 protein functions will reveal if and how it may be targeted for clinical benefit.

Published

2021

4. Huntington’s Disease Pathogenesis: Two Sequential Components

Author

Marcy E. MacDonald, Darren G. Monckton, Lesley Jones, Vanessa C. Wheeler, Michael Orth, Eun Pyo Hong, Seung Kwak, Peter Holmans, Jong-Min Lee, James F. Gusella, and Jeffrey D. Long

Subjects

0301 basic medicine, genetic association, Locus (genetics), Disease, Review, Biology, genotype-phenotype correlation, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Huntington's disease, medicine, Humans, genetics, Cognitive decline, Genetic Association Studies, Genetic association, Genetics, modifier gene, Huntingtin Protein, Genes, Modifier, medicine.disease, Human genetics, 030104 developmental biology, Huntington Disease, Human genome, Neurology (clinical), trinucleotide repeat expansion, Trinucleotide repeat expansion, 030217 neurology & neurosurgery

Abstract

Historically, Huntington’s disease (HD; OMIM #143100) has played an important role in the enormous advances in human genetics seen over the past four decades. This familial neurodegenerative disorder involves variable onset followed by consistent worsening of characteristic abnormal movements along with cognitive decline and psychiatric disturbances. HD was the first autosomal disease for which the genetic defect was assigned to a position on the human chromosomes using only genetic linkage analysis with common DNA polymorphisms. This discovery set off a multitude of similar studies in other diseases, while the HD gene, later renamed HTT, and its vicinity in chromosome 4p16.3 then acted as a proving ground for development of technologies to clone and sequence genes based upon their genomic location, with the growing momentum of such advances fueling the Human Genome Project. The identification of the HD gene has not yet led to an effective treatment, but continued human genetic analysis of genotype-phenotype relationships in large HD subject populations, first at the HTT locus and subsequently genome-wide, has provided insights into pathogenesis that divide the course of the disease into two sequential, mechanistically distinct components.

Published

2021

5. Modifiers of Somatic Repeat Instability in Mouse Models of Friedreich Ataxia and the Fragile X-Related Disorders: Implications for the Mechanism of Somatic Expansion in Huntington’s Disease

Author

Daman Kumari, Bruce E. Hayward, Karen Usdin, Antonia G. Vitalo, Ricardo Mouro Pinto, Xiao-Nan Zhao, Geum-Yi Kim, and Carson J. Miller

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Huntingtin, Ataxia, Somatic cell, Review, Biology, base excision repair, DNA Mismatch Repair, non-homologous end-joining, Genomic Instability, 03 medical and health sciences, Cellular and Molecular Neuroscience, Exon, FMR1-associated disorders, Mice, 0302 clinical medicine, Huntington's disease, medicine, Huntingtin Protein, trinucleotide repeat instability, Animals, Humans, Genetics, Genes, Modifier, Fragile X-related disorders, Polyglutamine tract, medicine.disease, mismatch repair, 030104 developmental biology, Huntington Disease, Friedreich ataxia, Fragile X Syndrome, double-strand break repair, Neurology (clinical), medicine.symptom, Trinucleotide repeat expansion, Trinucleotide Repeat Expansion, 030217 neurology & neurosurgery, Huntington’s disease

Abstract

Huntington’s disease (HD) is one of a large group of human disorders that are caused by expanded DNA repeats. These repeat expansion disorders can have repeat units of different size and sequence that can be located in any part of the gene and, while the pathological consequences of the expansion can differ widely, there is evidence to suggest that the underlying mutational mechanism may be similar. In the case of HD, the expanded repeat unit is a CAG trinucleotide located in exon 1 of the huntingtin (HTT) gene, resulting in an expanded polyglutamine tract in the huntingtin protein. Expansion results in neuronal cell death, particularly in the striatum. Emerging evidence suggests that somatic CAG expansion, specifically expansion occurring in the brain during the lifetime of an individual, contributes to an earlier disease onset and increased severity. In this review we will discuss mouse models of two non-CAG repeat expansion diseases, specifically the Fragile X-related disorders (FXDs) and Friedreich ataxia (FRDA). We will compare and contrast these models with mouse and patient-derived cell models of various other repeat expansion disorders and the relevance of these findings for somatic expansion in HD. We will also describe additional genetic factors and pathways that modify somatic expansion in the FXD mouse model for which no comparable data yet exists in HD mice or humans. These additional factors expand the potential druggable space for diseases like HD where somatic expansion is a significant contributor to disease impact.

Published

2021

6. Modifiers of CAG/CTG Repeat Instability: Insights from Mammalian Models

Author

Vincent Dion and Vanessa C. Wheeler

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, DNA repair, Context (language use), Review, Biology, Myotonic dystrophy, Germline, Genomic Instability, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Mismatch Repair Pathway, Huntington's disease, medicine, trinucleotide repeat instability, Animals, Myotonic Dystrophy, Genetics, Genes, Modifier, medicine.disease, myotonic dystrophy 1, mismatch repair, Disease Models, Animal, 030104 developmental biology, Huntington Disease, DNA mismatch repair, Neurology (clinical), Trinucleotide repeat expansion, Trinucleotide Repeat Expansion, 030217 neurology & neurosurgery, Huntington’s disease

Abstract

At fifteen different genomic locations, the expansion of a CAG/CTG repeat causes a neurodegenerative or neuromuscular disease, the most common being Huntington’s disease and myotonic dystrophy type 1. These disorders are characterized by germline and somatic instability of the causative CAG/CTG repeat mutations. Repeat lengthening, or expansion, in the germline leads to an earlier age of onset or more severe symptoms in the next generation. In somatic cells, repeat expansion is thought to precipitate the rate of disease. The mechanisms underlying repeat instability are not well understood. Here we review the mammalian model systems that have been used to study CAG/CTG repeat instability, and the modifiers identified in these systems. Mouse models have demonstrated prominent roles for proteins in the mismatch repair pathway as critical drivers of CAG/CTG instability, which is also suggested by recent genome-wide association studies in humans. We draw attention to a network of connections between modifiers identified across several systems that might indicate pathway crosstalk in the context of repeat instability, and which could provide hypotheses for further validation or discovery. Overall, the data indicate that repeat dynamics might be modulated by altering the levels of DNA metabolic proteins, their regulation, their interaction with chromatin, or by direct perturbation of the repeat tract. Applying novel methodologies and technologies to this exciting area of research will be needed to gain deeper mechanistic insight that can be harnessed for therapies aimed at preventing repeat expansion or promoting repeat contraction.

Published

2021

7. Genetic information from discordant sibling pairs points to ESRP2 as a candidate trans-acting regulator of the CF modifier gene SCNN1B

Author

Mohammed Ibrahim, Janine Altmüller, Mohammad R. Toliat, Burkhard Tümmler, Sabina Janciauskiene, Tim Becker, Frauke Stanke, Nina Dalibor, Silke Hedtfeld, Stephanie Tamm, and Andreas Pich

Subjects

Epithelial sodium channel, Male, Cystic Fibrosis, Genotype, Science, Cystic Fibrosis Transmembrane Conductance Regulator, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Article, Gene silencing, Humans, Electrophoretic mobility shift assay, Epithelial Sodium Channels, Gene, Alleles, Genetic Association Studies, Genetic association study, Genetics, Regulation of gene expression, Multidisciplinary, Binding Sites, Genes, Modifier, Siblings, Chromosome Mapping, RNA-Binding Proteins, Epithelial Cells, Sequence Analysis, DNA, Introns, Gene regulation, Alternative Splicing, Haplotypes, Gene Knockdown Techniques, RNA splicing, Medicine, Trans-acting, Disease Susceptibility, Technology Platforms, Genetic Background, Protein Binding

Abstract

SCNN1B encodes the beta subunit of the epithelial sodium channel ENaC. Previously, we reported an association between SNP markers of SCNN1B gene and disease severity in cystic fibrosis-affected sibling pairs. We hypothesized that factors interacting with the SCNN1B genomic sequence are responsible for intrapair discordance. Concordant and discordant pairs differed at six SCNN1B markers (Praw = 0.0075, Pcorr = 0.0397 corrected for multiple testing). To identify the factors binding to these six SCNN1B SNPs, we performed an electrophoretic mobility shift assay and captured the DNA–protein complexes. Based on protein mass spectrometry data, the epithelial splicing regulatory protein ESRP2 was identified when using SCNN1B-derived probes and the ESRP2-SCNN1B interaction was independently confirmed by coimmunoprecipitation assays. We observed an alternative SCNN1B transcript and demonstrated in 16HBE14o− cells that levels of this transcript are decreased upon ESRP2 silencing by siRNA. Furthermore, we confirmed that mildly and severely affected siblings have different ESPR2 genetic backgrounds and that ESRP2 markers are linked to the response of CF patients’ nasal epithelium to amiloride, indicating ENaC involvement (Pbest = 0.0131, Pcorr = 0.068 for multiple testing). Our findings demonstrate that sibling pairs clinically discordant for CF can be used to identify meaningful DNA regulatory elements and interacting factors.

Published

2020

8. Promotion of somatic CAG repeat expansion by Fan1 knock-out in Huntington’s disease knock-in mice is blocked by Mlh1 knock-out

Author

Vanessa C. Wheeler, Ramee Lee, Marina Kovalenko, Kyung Hee Kim, Ricardo Mouro Pinto, Ihn Sik Seong, Tammy Gillis, Marissa A Andrew, Marcy E. MacDonald, Seung Kwak, James F. Gusella, Jacob M. Loupe, Jayalakshmi S. Mysore, Ryan Murtha, Jong-Min Lee, and David Howland

Subjects

AcademicSubjects/SCI01140, congenital, hereditary, and neonatal diseases and abnormalities, Somatic cell, Cell Cycle Proteins, Biology, MLH1, Mice, 03 medical and health sciences, 0302 clinical medicine, Gene interaction, Huntington's disease, Gene knockin, Ribonucleotide Reductases, mental disorders, Genetics, medicine, Animals, Humans, Genetic Predisposition to Disease, Age of Onset, Molecular Biology, Gene, Genetics (clinical), 030304 developmental biology, Mice, Knockout, Huntingtin Protein, 0303 health sciences, Endodeoxyribonucleases, Genes, Modifier, General Medicine, medicine.disease, Multifunctional Enzymes, Phenotype, nervous system diseases, Disease Models, Animal, Exodeoxyribonucleases, Huntington Disease, General Article, MutL Protein Homolog 1, Trinucleotide Repeat Expansion, Trinucleotide repeat expansion, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Recent genome-wide association studies of age-at-onset in Huntington’s disease (HD) point to distinct modes of potential disease modification: altering the rate of somatic expansion of the HTT CAG repeat or altering the resulting CAG threshold length-triggered toxicity process. Here, we evaluated the mouse orthologs of two HD age-at-onset modifier genes, FAN1 and RRM2B, for an influence on somatic instability of the expanded CAG repeat in Htt CAG knock-in mice. Fan1 knock-out increased somatic expansion of Htt CAG repeats, in the juvenile- and the adult-onset HD ranges, whereas knock-out of Rrm2b did not greatly alter somatic Htt CAG repeat instability. Simultaneous knock-out of Mlh1, the ortholog of a third HD age-at-onset modifier gene (MLH1), which suppresses somatic expansion of the Htt knock-in CAG repeat, blocked the Fan1 knock-out-induced acceleration of somatic CAG expansion. This genetic interaction indicates that functional MLH1 is required for the CAG repeat destabilizing effect of FAN1 loss. Thus, in HD, it is uncertain whether the RRM2B modifier effect on timing of onset may be due to a DNA instability mechanism. In contrast, the FAN1 modifier effects reveal that functional FAN1 acts to suppress somatic CAG repeat expansion, likely in genetic interaction with other DNA instability modifiers whose combined effects can hasten or delay onset and other CAG repeat length-driven phenotypes.

Published

2020

9. Alzheimer's disease risk modifier genes do not affect tau aggregate uptake, seeding or maintenance in cell models

Author

Marc I. Diamond and Sourav Kolay

Subjects

0301 basic medicine, Amyloid beta, Tau propagation, Cell, tau Proteins, Genome-wide association study, Models, Biological, General Biochemistry, Genetics and Molecular Biology, Protein Aggregates, 03 medical and health sciences, 0302 clinical medicine, Alzheimer Disease, Tau prion mechanism, mental disorders, medicine, Humans, GWAS, CRISPR, lcsh:QH301-705.5, Gene, Research Articles, Gene knockout, Genes, Modifier, biology, Cas9, HEK 293 cells, Alzheimer's disease, Cell biology, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), 030220 oncology & carcinogenesis, biology.protein, CRISPR-Cas Systems, Alzheimer's risk factors, Research Article

Abstract

Alzheimer's disease (AD) is a major cause of dementia. The molecular basis of disease progression is unknown. We hypothesized that the identified AD genome‐wide association study (GWAS) genes would regulate this process. We used CRISPR‐mediated knockout of these genes to test their effects in the cell model systems of tau propagation. GWAS gene knockouts had no effect in these models of tau pathology., Alzheimer's disease (AD) afflicts millions of people worldwide and is caused by accumulated amyloid beta and tau pathology. Progression of tau pathology in AD may utilize prion mechanisms of propagation in which pathological tau aggregates released from one cell are taken up by neighboring or connected cells and act as templates for their own replication, a process termed ‘seeding’. We have used HEK293T cells to model various aspects of pathological tau propagation, including uptake of tau aggregates, induced seeding by exogenous aggregates, seeding caused by Lipofectamine‐mediated delivery to the cell interior, and stable maintenance of aggregates in dividing cells. The factors that regulate these processes are not well understood, and we hypothesized that AD risk modifier genes might play a role. We identified 22 genes strongly linked to AD via meta‐analysis of genome‐wide association study (GWAS). We used CRISPR/Cas9 to individually knock out each gene in HEK293T cells and verified disruption using genomic sequencing. We then tested the effect of gene knockout in tau aggregate uptake, naked and Lipofectamine‐mediated seeding, and aggregate maintenance in these cultured cell lines. GWAS gene knockouts had no effect in these models of tau pathology. With obvious caveats due to the model systems used, these results imply that the 22 AD risk modifier genes are unlikely to directly modulate tau uptake, seeding, or aggregate maintenance in a cell‐autonomous fashion.

Published

2020

10. Common Variants Coregulate Expression of <scp> GBA </scp> and Modifier Genes to Delay Parkinson's Disease Onset

Author

Martin A. Kennedy, Tayaza Fadason, William Schierding, Sophie Farrow, Toni L. Pitcher, Alan J. Davidson, Jo K. Perry, Sara Qubisi, Antony A. Cooper, Oscar E.E. Graham, Tim J. Anderson, and Justin M. O'Sullivan

Subjects

0301 basic medicine, Parkinson's disease, Locus (genetics), Single-nucleotide polymorphism, Substantia nigra, Regular Issue Articles, Biology, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Gene, Research Articles, Genetics, Gaucher Disease, Genes, Modifier, Dementia with Lewy bodies, Haplotype, Parkinson Disease, medicine.disease, Penetrance, 030104 developmental biology, Neurology, Mutation, Glucosylceramidase, Lewy Bodies, Neurology (clinical), 030217 neurology & neurosurgery, Research Article

Abstract

Background GBA mutations are numerically the most significant genetic risk factor for Parkinson's disease (PD), yet these mutations have low penetrance, suggesting additional mechanisms. Objectives The objective of this study was to determine if the penetrance of GBA in PD can be explained by regulatory effects on GBA and modifier genes. Methods Genetic variants associated with the regulation of GBA were identified by screening 128 common single nucleotide polymorphisms (SNPs) in the GBA locus for spatial cis‐expression quantitative trail locus (supported by chromatin interactions). Results We identified common noncoding SNPs within GBA that (1) regulate GBA expression in peripheral tissues, some of which display α‐synuclein pathology and (2) coregulate potential modifier genes in the central nervous system and/or peripheral tissues. Haplotypes based on 3 of these SNPs delay disease onset by 5 years. In addition, SNPs on 6 separate chromosomes coregulate GBA expression specifically in either the substantia nigra or cortex, and their combined effect potentially modulates motor and cognitive symptoms, respectively. Conclusions This work provides a new perspective on the haplotype‐specific effects of GBA and the genetic etiology of PD, expanding the role of GBA from the gene encoding the β‐glucocerebrosidase (GCase) to that of a central regulator and modifier of PD onset, with GBA expression itself subject to distant regulation. Some idiopathic patients might possess insufficient GBA‐encoded GCase activity in the substantia nigra as the result of distant regulatory variants and therefore might benefit from GBA‐targeting therapeutics. The SNPs’ regulatory impacts provide a plausible explanation for the variable phenotypes also observed in GBA‐centric Gaucher's disease and dementia with Lewy bodies. © 2020 The Authors. Movement Disorders published by Wiley Periodicals, LLC on behalf of International Parkinson and Movement Disorder Society.

Published

2020

11. MTMR4 SNVs modulate ion channel degradation and clinical severity in congenital long QT syndrome: insights in the mechanism of action of protective modifier genes

Author

Eleonora Torre, Peter J. Schwartz, Lia Crotti, Yee-Ki Lee, Matteo Pedrazzini, Pak C. Sham, Massimiliano Gnecchi, Xinru Ran, Hung-Fat Tse, Manuela Mura, Timothy Shin Heng Mak, Marcella Rocchetti, Luca Sala, Antonio Zaza, Lee, Y, Sala, L, Mura, M, Rocchetti, M, Pedrazzini, M, Ran, X, Mak, T, Crotti, L, Sham, P, Torre, E, Zaza, A, Schwartz, P, Tse, H, and Gnecchi, M

Subjects

Physiology, Nedd4 Ubiquitin Protein Ligases, Arrhythmias, 030204 cardiovascular system & hematology, medicine.disease_cause, Electrocardiography, 0302 clinical medicine, BIO/09 - FISIOLOGIA, AcademicSubjects/MED00200, Myocytes, Cardiac, KvLQT1, Variant, Cells, Cultured, Exome sequencing, Genetics, 0303 health sciences, Mutation, biology, Variants, Protein Tyrosine Phosphatases, Non-Receptor, Phenotype, 3. Good health, KCNQ1 Potassium Channel, Long QT syndrome, Cardiology and Cardiovascular Medicine, Arrhythmia, Induced Pluripotent Stem Cells, hERG, Protein degradation, Polymorphism, Single Nucleotide, Cardiac Electrophysiology and Arrhythmia, 03 medical and health sciences, Physiology (medical), Nedd4L, medicine, Humans, Genetic Predisposition to Disease, 030304 developmental biology, NEDD4L, Genes, Modifier, business.industry, Induced pluripotent stem cell, Original Articles, medicine.disease, MTMR4, Proteolysis, biology.protein, business

Abstract

Aims In long QT syndrome (LQTS) patients, modifier genes modulate the arrhythmic risk associated with a disease-causing mutation. Their recognition can improve risk stratification and clinical management, but their discovery represents a challenge. We tested whether a cellular-driven approach could help to identify new modifier genes and especially their mechanism of action. Methods and results We generated human-induced pluripotent stem cell-derived cardiomyocytes (iPSC-CM) from two patients carrying the same KCNQ1-Y111C mutation, but presenting opposite clinical phenotypes. We showed that the phenotype of the iPSC-CMs derived from the symptomatic patient is due to impaired trafficking and increased degradation of the mutant KCNQ1 and wild-type human ether-a-go-go-related gene. In the iPSC-CMs of the asymptomatic (AS) patient, the activity of an E3 ubiquitin-protein ligase (Nedd4L) involved in channel protein degradation was reduced and resulted in a decreased arrhythmogenic substrate. Two single-nucleotide variants (SNVs) on the Myotubularin-related protein 4 (MTMR4) gene, an interactor of Nedd4L, were identified by whole-exome sequencing as potential contributors to decreased Nedd4L activity. Correction of these SNVs by CRISPR/Cas9 unmasked the LQTS phenotype in AS cells. Importantly, the same MTMR4 variants were present in 77% of AS Y111C mutation carriers of a separate cohort. Thus, genetically mediated interference with Nedd4L activation seems associated with protective effects. Conclusion Our finding represents the first demonstration of the cellular mechanism of action of a protective modifier gene in LQTS. It provides new clues for advanced risk stratification and paves the way for the design of new therapies targeting this specific molecular pathway.

Published

2020

12. ABCG2 rs2231142 variant in hyperuricemia is modified by SLC2A9 and SLC22A12 polymorphisms and cardiovascular risk factors in an elderly community-dwelling population

Author

Jia Liu, Wei Yang, Zhanyun Wei, Yun Li, and Xiaojuan Dan

Subjects

Male, 0301 basic medicine, Aging, Glucose Transport Proteins, Facilitative, Organic Anion Transporters, 030204 cardiovascular system & hematology, Cohort Studies, 0302 clinical medicine, Risk Factors, ATP Binding Cassette Transporter, Subfamily G, Member 2, Genetics (clinical), Aged, 80 and over, education.field_of_study, biology, Neoplasm Proteins, Cardiovascular Diseases, Hypertension, Population study, Female, SLC22A12, Independent Living, Research Article, China, medicine.medical_specialty, lcsh:Internal medicine, Organic Cation Transport Proteins, lcsh:QH426-470, ABCG2, Population, Single-nucleotide polymorphism, Hyperuricemia, Effect Modifier, Epidemiologic, Polymorphism, Single Nucleotide, 03 medical and health sciences, Triglyceridemia, Internal medicine, Genetics, medicine, Humans, Genetic Predisposition to Disease, education, lcsh:RC31-1245, Aged, Genes, Modifier, business.industry, Hypertriglyceridemia, Epistasis, Genetic, Odds ratio, medicine.disease, lcsh:Genetics, 030104 developmental biology, biology.protein, business, Polymorphisms, Uric acid, Dyslipidemia, Genome-Wide Association Study, SLC2A9

Abstract

Background The ABCG2 rs2231142 single nucleotide polymorphism (SNP) is one of the most significant genetic variants associated with hyperuricemia (HUA) in Asian populations. However, the risk of ABCG2 rs2231142 variants for HUA could interact with other important HUA risk variants and cardiovascular factors. This study investigated the effects of the combined association among ABCG2 rs2231142 and multiple HUA genetic variants or cardiovascular risk factors on HUA risk and serum uric acid (sUA) levels in an elderly Chinese population. Methods A total of 1206 participants over 65 years old were enrolled in this study. Physical and laboratory examinations were performed for all participants. The ABCG2 rs2231142, SLC2A9 rs3733591, and SLC22A12 rs893006 SNPs were assayed using a standardized protocol. Logistic regression analysis and liner regression were adjusted respectively to account for the association between ABCG2 rs2231142 and other genetic variants, as well as between cardiovascular risk factors and HUA risk and sUA levels. Results The prevalence of HUA was 14.71% in the elderly community-dwelling population. The ABCG2 rs2231142 risk T allele was associated with HUA risk (odds ratio (OR) = 1.63, 95% confidence interval (CI): 1.27–2.11; p = 1.65 × 10− 4) and with increased sUA levels (Beta = 0.16, p = 6.75 × 10− 9) in the whole study population. Linear regression analysis showed that the mean sUA level increased linearly with the number of risk alleles of the three candidate genetic variants (Beta = 0.18, p = 1.94 × 10− 12) The joint effect of the ABCG2 rs2231142 T allele and cardiovascular risk factors (obesity, hypertension and dyslipidemia) was also associated with increased HUA risk and sUA levels. Each copy of the risk T allele was significantly associated with enhanced HUA risk in patients with hypertriglyceridemia (OR = 2.52, 95% CI: 1.33–4.60; p = 0.003) compared to controls. Conclusion Our findings reinforce the importance of the ABCG2 rs2231143 variant as a crucial genetic locus for HUA in Chinese populations and demonstrated the combined effects of multiple genetic risk variants and cardiovascular risk exposures on HUA risk and increased sUA level.

Published

2020

13. Cardiomyopathy due to PRDM16 mutation: First description of a fetal presentation, with possible modifier genes

Author

Geoffroy Delplancq, Alexandre Vasiljevic, Antonio Vitobello, Jean Christophe Eicher, Gilles Millat, Paul Kuentz, Christophe Philippe, Georges Tarris, Martin Chevarin, Yannis Duffourd, Fara T. Harizay, Virginie Carmignac, Christel Thauvin-Robinet, Sophie Nambot, Arthur Sorlin, Laurence Faivre, Thierry Rousseau, Charlotte Denis, Bouchra Khallouk, and Sylvie Falcon-Eicher

Subjects

Adult, Heart Defects, Congenital, Male, medicine.medical_specialty, Cardiomyopathy, Biology, Labor Presentation, Genetic Heterogeneity, Pregnancy, Exome Sequencing, Genetics, medicine, Humans, Missense mutation, Genetic Predisposition to Disease, Genetics (clinical), Exome sequencing, Fetus, Genes, Modifier, Genetic heterogeneity, Infant, Newborn, Endocardial fibroelastosis, Middle Aged, Fetal Presentation, medicine.disease, Pedigree, DNA-Binding Proteins, Mutation, Medical genetics, Female, Cardiomyopathies, Transcription Factors

Abstract

PRDM16 (positive regulatory domain 16) is localized in the critical region for cardiomyopathy in patients with deletions of chromosome 1p36, as defined by Gajecka et al., American Journal of Medical Genetics, 2010, 152A, 3074-3083, and encodes a zinc finger transcription factor. We present the first fetal case of left ventricular non-compaction (LVNC) with a PRDM16 variant. The third-trimester obstetric ultrasound revealed a hydropic fetus with hydramnios and expanded hypokinetic heart. After termination of pregnancy, foetopathology showed a eutrophic fetus with isolated cardiomegaly. Endocardial fibroelastosis was associated with non-compaction of the myocardium of the left ventricle. Exome sequencing (ES) identified a de novo unreported p.(Gln353*) heterozygous nonsense variant in PRDM16. ES also identified two rare variants of unknown significance, according to the American College of Medical Genetics and Genomics guidelines, in the titin gene (TTN): a de novo missense p.(Lys14773Asn) variant and a c.33043+5A>G variant inherited from the mother. Along with the PRDM16 de novo probably pathogenic variant, TTN VOUS variants could possibly contribute to the severity and early onset of the cardiac phenotype. Because of the genetic heterogeneity of cardiomyopathies, large panels or even ES could be considered as the main approaches for the molecular diagnosis, particularly in fetal presentations, where multiple hits seem to be common.

Published

2020

14. A Kinome RNAi Screen in Drosophila Identifies Novel Genes Interacting with Lgl, aPKC, and CrB Cell Polarity Genes in Epithelial Tissues

Author

Helena E. Richardson, Peter Burke, Leonie M. Quinn, Kasun Amaratunga, Linda M. Parsons, and Nicola A. Grzeschik

Subjects

0301 basic medicine, Male, Genes, Insect, QH426-470, PI3K, Epithelium, Hippo, Cell polarity, Drosophila Proteins, Wings, Animal, Kinome, TUMOR-SUPPRESSOR, PHOSPHORYLATION, Genetics (clinical), LETHAL GIANT LARVAE, Uncategorized, Kinase, Wnt signaling pathway, Organ Size, phosphoprotein, WARTS-HIPPO PATHWAY, Cell biology, IMAGINAL DISCS, cell polarity, Drosophila melanogaster, ORGAN SIZE CONTROL, GROWTH, Female, RNA Interference, Drosophila, Signal transduction, Signal Transduction, nutrient sensing, kinase, Morphogenesis, Notch signaling pathway, Nutrient sensing, Biology, Investigations, phosphatase, 03 medical and health sciences, Wnt, YORKIE ACTIVITY, Genetics, Animals, Genetic Testing, Molecular Biology, Genes, Modifier, Tumor Suppressor Proteins, Membrane Proteins, Epistasis, Genetic, phosphoinositol, 030104 developmental biology, Gene Ontology, Wingless, CRUMBS, Ras

Abstract

In both Drosophila melanogaster and mammalian systems, epithelial structure and underlying cell polarity are essential for proper tissue morphogenesis and organ growth. Cell polarity interfaces with multiple cellular processes that are regulated by the phosphorylation status of large protein networks. To gain insight into the molecular mechanisms that coordinate cell polarity with tissue growth, we screened a boutique collection of RNAi stocks targeting the kinome for their capacity to modify Drosophila “cell polarity” eye and wing phenotypes. Initially, we identified kinase or phosphatase genes whose depletion modified adult eye phenotypes associated with the manipulation of cell polarity complexes (via overexpression of Crb or aPKC). We next conducted a secondary screen to test whether these cell polarity modifiers altered tissue overgrowth associated with depletion of Lgl in the wing. These screens identified Hippo, Jun kinase (JNK), and Notch signaling pathways, previously linked to cell polarity regulation of tissue growth. Furthermore, novel pathways not previously connected to cell polarity regulation of tissue growth were identified, including Wingless (Wg/Wnt), Ras, and lipid/Phospho-inositol-3-kinase (PI3K) signaling pathways. Additionally, we demonstrated that the “nutrient sensing” kinases Salt Inducible Kinase 2 and 3 (SIK2 and 3) are potent modifiers of cell polarity phenotypes and regulators of tissue growth. Overall, our screen has revealed novel cell polarity-interacting kinases and phosphatases that affect tissue growth, providing a platform for investigating molecular mechanisms coordinating cell polarity and tissue growth during development.

Published

2022

15. Intronic Haplotypes in <scp>GBA</scp> Modify Age at Diagnosis of Parkinson's: Replication in a Subgroup

Author

Geert Jan Groeneveld, Justin M. O'Sullivan, Antony A. Cooper, and Jonas M. den Heijer

Subjects

Genetics, Genes, Modifier, Parkinson's, Haplotype, Age at diagnosis, Parkinson Disease, Biology, intronic variants, Haplotypes, Neurology, age at diagnosis, Mutation, Replication (statistics), Glucosylceramidase, Humans, GBA, Neurology (clinical), age at onset

Published

2021

16. Consistent Assignment of Risk and Benign Allele at rs2303153 in the CF Modifier Gene SCNN1B in Three Independent F508del-CFTR Homozygous Patient Populations

Author

Anna-Maria Dittrich, Silke Hedtfeld, Haide Susanne Ismer, Burkhard Tümmler, Inga Dunsche, Frauke Stanke, Tim Becker, and Julia Kontsendorn

Subjects

Epithelial sodium channel, Biology, QH426-470, association study, Polymorphism, Single Nucleotide, Cystic fibrosis, Article, cystic fibrosis, Genotype, medicine, Genetics, Humans, Allele, Epithelial Sodium Channels, Gene, Alleles, Genetics (clinical), Genetic association, modifier gene, Genes, Modifier, Sodium channel, Homozygote, Apical membrane, medicine.disease, amiloride-sensitive sodium channel ENaC

Abstract

CFTR encodes for a chloride and bicarbonate channel expressed at the apical membrane of polarized epithelial cells. Transepithelial sodium transport mediated by the amiloride-sensitive sodium channel ENaC is thought to contribute to the manifestation of CF disease. Thus, ENaC is a therapeutic target in CF and a valid cystic fibrosis modifier gene. We have characterized SCNN1B as a genetic modifier in the three independent patient cohorts of F508del-CFTR homozygotes. We could identify a regulatory element at SCNN1B to the genomic segment rs168748-rs2303153-rs4968000 by fine-mapping (Pbest = 0.0177), consistently observing the risk allele rs2303153-C and the contrasting benign allele rs2303153-G in all three patient cohorts. Furthermore, our results show that expression levels of SCNN1B are associated with rs2303153 genotype in intestinal epithelia (p = 0.003). Our data confirm that the well-established biological role of SCNN1B can be recognized by an association study on informative endophenotypes in the rare disease cystic fibrosis and calls attention to reproducible results in association studies obtained from small, albeit carefully characterized patient populations.

Published

2021

17. Determinants of Disease Penetrance in PRPF31-Associated Retinopathy

Author

Zhiqin Huang, Dan Zhang, Jennifer A. Thompson, Alanis Lima, Shang Chih Chen, Tina M. Lamey, Sue Fletcher, Sang Yoon Moon, Mary S. Attia, Xiao Zhang, Khine Zaw, Janya Grainok, John N. De Roach, Terri L. McLaren, Fred K. Chen, Luke Jennings, Danial Roshandel, Samuel McLenachan, and Rachael C. Heath Jeffery

Subjects

Male, PRPF31, retinal pigment epithelium, Penetrance, QH426-470, chemistry.chemical_compound, Induced pluripotent stem cell, Child, Genetics (clinical), Cells, Cultured, Scavenger Receptors, Class A, MSR1, Middle Aged, medicine.anatomical_structure, Female, rod-cone dystrophy, Retinopathy, Adult, Adolescent, induced pluripotent stem cells, Biology, Article, Retina, retinitis pigmentosa, Retinitis pigmentosa, medicine, Genetics, otorhinolaryngologic diseases, non-penetrance, Humans, Eye Proteins, CNOT3, RP11, Aged, Retinal pigment epithelium, Genes, Modifier, Polymorphism, Genetic, retinal organoid, Retinal, medicine.disease, eye diseases, chemistry, Cancer research, Transcription Factors

Abstract

Retinitis pigmentosa 11 (RP11) is caused by dominant mutations in PRPF31, however a significant proportion of mutation carriers do not develop retinopathy. Here, we investigated the relationship between CNOT3 polymorphism, MSR1 repeat copy number and disease penetrance in RP11 patients and non-penetrant carriers (NPCs). We further characterized PRPF31 and CNOT3 expression in fibroblasts from eight RP11 patients and one NPC from a family carrying the c.1205C&gt, T variant. Retinal organoids (ROs) and retinal pigment epithelium (RPE) were differentiated from induced pluripotent stem cells derived from RP11 patients, an NPC and a control subject. All RP11 patients were homozygous for the 3-copy MSR1 repeat in the PRPF31 promoter, while 3/5 NPCs carried a 4-copy MSR1 repeat. The CNOT3 rs4806718 genotype did not correlate with disease penetrance. PRFP31 expression declined with age in adult cadaveric retina. PRPF31 and CNOT3 expression was reduced in RP11 fibroblasts, RO and RPE compared with controls. Both RP11 and NPC RPE displayed shortened primary cilia compared with controls, however a subpopulation of cells with normal cilia lengths was present in NPC RPE monolayers. Our results indicate that RP11 non-penetrance is associated with the inheritance of a 4-copy MSR1 repeat, but not with CNOT3 polymorphisms.

Published

2021

18. Coordinate regulation of ELF5 and EHF at the chr11p13 CF modifier region

Author

Shih Hsing Leir, Monali NandyMazumdar, Shiyi Yin, Eric M. Mendenhall, Kay-Marie Lamar, Jenny L. Kerschner, Hannah Swahn, Jey Sabith Ebron, Ann Harris, and Candice J. Coppola

Subjects

0301 basic medicine, Cystic Fibrosis, cis‐regulatory elements, Biology, lung epithelium, 03 medical and health sciences, 0302 clinical medicine, chromatin architecture, LNCaP, Humans, airway epithelial biology, E74‐like factor 5, Enhancer, Promoter Regions, Genetic, Transcription factor, Gene, lung diseases, Sequence Deletion, Regulation of gene expression, Genes, Modifier, Chromosomes, Human, Pair 11, ETS Homologous Factor, Cell Biology, Original Articles, ETS‐homologous factor, ETS family transcription factors, Chromatin, Introns, Cell biology, DNA-Binding Proteins, 030104 developmental biology, Gene Expression Regulation, Genetic Loci, 030220 oncology & carcinogenesis, Cancer cell, Molecular Medicine, Original Article, enhancers, regulation of gene expression, Transcription Factors

Abstract

E74‐like factor 5 (ELF5) and ETS‐homologous factor (EHF) are epithelial selective ETS family transcription factors (TFs) encoded by genes at chr11p13, a region associated with cystic fibrosis (CF) lung disease severity. EHF controls many key processes in lung epithelial function so its regulatory mechanisms are important. Using CRISPR/Cas9 technology, we removed three key cis‐regulatory elements (CREs) from the chr11p13 region and also activated multiple open chromatin sites with CRISPRa in airway epithelial cells. Deletion of the CREs caused subtle changes in chromatin architecture and site‐specific increases in EHF and ELF5. CRISPRa had most effect on ELF5 transcription. ELF5 levels are low in airway cells but higher in LNCaP (prostate) and T47D (breast) cancer cells. ATAC‐seq in these lines revealed novel peaks of open chromatin at the 5’ end of chr11p13 associated with an expressed ELF5 gene. Furthermore, 4C‐seq assays identified direct interactions between the active ELF5 promoter and sites within the EHF locus, suggesting coordinate regulation between these TFs. ChIP‐seq for ELF5 in T47D cells revealed ELF5 occupancy within EHF introns 1 and 6, and siRNA‐mediated depletion of ELF5 enhanced EHF expression. These results define a new role for ELF5 in lung epithelial biology.

Published

2019

19. Dopamine β Hydroxylase (DBH) is a potential modifier gene associated with Parkinson's disease in Eastern India

Author

Arindam Biswas, Shyamal Kumar Das, Jharna Ray, Arunibha Ghosh, Subhajit Giri, Tamal Sadhukhan, and Kunal Ray

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Candidate gene, Parkinson's disease, India, Single-nucleotide polymorphism, Dopamine beta-Hydroxylase, Disease, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Dopamine, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Promoter Regions, Genetic, Alleles, Genetic Association Studies, Genes, Modifier, General Neuroscience, Neurodegeneration, Haplotype, Dopaminergic, Parkinson Disease, Middle Aged, medicine.disease, 030104 developmental biology, Endocrinology, Haplotypes, Female, 030217 neurology & neurosurgery, medicine.drug

Abstract

Background Parkinson’s disease (PD) is the debilitating movement disorder, distinguished by dopaminergic and norepinephrinergic neurodegeneration. Apart from candidate gene mutations, several modifier loci have been reported to be associated with the disease manifestation. The Dopamine β-Hydroxylase (DBH) maintains cellular dopamine content and regulates dopamine turn over in neurons. Genetic polymorphisms of DBH are associated with PD and are found to alter plasma DBH activity in patients compared to healthy controls. Therefore, DBH activity in plasma could be a potential and easily detectable biomarkers for alteration of dopaminergic neuronal function in PD. Methods Plasma DBH activity has been assessed among PD cases and age-matched controls to identify correlation with PD. To elucidate the role of DBH polymorphisms in Eastern Indian PD patients, three SNPs (rs1611115, rs1108580 and rs129882) were selected and screened by PCR-RFLP and DNA sequencing analysis. Results The T-allele of rs129882 was more prevalent among patients than controls posing risk (p-value = 0.02, OR = 1.404, 95% CI = 1.047–1.883) towards PD. The dual-Luciferase assay in SHSY5Y cell line revealed that the T-allele of rs129882 increases Luciferase signal (p = 0.0269). However, the rs1611115 and rs1108580 did not show association with PD; plasma DBH activity was not significantly different between patients and controls (p-value > 0.05). Haplotypes constructed with three SNPs showed that the CAT haplotype to pose risk, TAC haplotype to provide protection against early disease onset and CGT being protective against non-motor symptoms. Conclusion These data suggest that DBH might influence the susceptibility of PD.

Published

2019

20. Complex modifier landscape underlying genetic background effects

Author

Gerald R. Fink, Jing Hou, Charles Boone, Brenda J. Andrews, and Guihong Tan

Subjects

Saccharomyces cerevisiae, conditional gene essentiality, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, medicine, Genetics, Cysteine, Allele, Allele frequency, Gene, Loss function, Alleles, Phylogeny, 030304 developmental biology, 0303 health sciences, Mutation, complex modifier interactions, Multidisciplinary, Genes, Essential, Genes, Modifier, biology, rare variants, Biological Sciences, biology.organism_classification, Phenotype, Yeast, Biosynthetic Pathways, PNAS Plus, background effect, Genome, Fungal, Genetic Background, 030217 neurology & neurosurgery

Abstract

Significance Genetic background impacts the phenotypic outcome of a mutation in different individuals; however, the underlying molecular mechanisms are often unclear. We characterized genes exhibiting conditional essentiality when mutated in two genetically distinct yeast strains. Hybrid crosses and whole-genome sequencing revealed that conditional essentiality can be associated with nonchromosomal elements or a single-modifier locus, but most involve a complex set of modifier loci. Detailed analysis of the cysteine biosynthesis pathway showed that independent, rare, single-gene modifiers, related to both up- and downstream pathway functions, can arise in multiple allelic forms from separate lineages. For several genes, we also resolved complex sets of modifying loci underlying conditional essentiality, revealing specific genetic interactions that drive an individual strain’s background effect., The phenotypic consequence of a given mutation can be influenced by the genetic background. For example, conditional gene essentiality occurs when the loss of function of a gene causes lethality in one genetic background but not another. Between two individual Saccharomyces cerevisiae strains, S288c and Σ1278b, ∼1% of yeast genes were previously identified as “conditional essential.” Here, in addition to confirming that some conditional essential genes are modified by a nonchromosomal element, we show that most cases involve a complex set of genomic modifiers. From tetrad analysis of S288C/Σ1278b hybrid strains and whole-genome sequencing of viable hybrid spore progeny, we identified complex sets of multiple genomic regions underlying conditional essentiality. For a smaller subset of genes, including CYS3 and CYS4, each of which encodes components of the cysteine biosynthesis pathway, we observed a segregation pattern consistent with a single modifier associated with conditional essentiality. In natural yeast isolates, we found that the CYS3/CYS4 conditional essentiality can be caused by variation in two independent modifiers, MET1 and OPT1, each with roles associated with cellular cysteine physiology. Interestingly, the OPT1 allelic variation appears to have arisen independently from separate lineages, with rare allele frequencies below 0.5%. Thus, while conditional gene essentiality is usually driven by genetic interactions associated with complex modifier architectures, our analysis also highlights the role of functionally related, genetically independent, and rare variants.

Published

2019

21. A Very Oil Yellow1 Modifier of the Oil Yellow1-N1989 Allele Uncovers a Cryptic Phenotypic Impact of Cis-regulatory Variation in Maize

Author

Sandeep R. Marla, Bala P. Venkata, Rajdeep S. Khangura, Gurmukh S. Johal, Nicholas J. Heller, and Brian P. Dilkes

Subjects

0106 biological sciences, epistasis, Mutant, Lyases, Genome-wide association study, Locus (genetics), Biology, Quantitative trait locus, QH426-470, Investigations, 01 natural sciences, Zea mays, complex traits, 03 medical and health sciences, Genetics, cryptic variation, Allele, cis-acting, Gene, Alleles, 030304 developmental biology, Plant Proteins, 2. Zero hunger, 0303 health sciences, Genes, Modifier, Polymorphism, Genetic, Epistasis, Genetic, Phenotype, Regulatory sequence, Genetic marker, Chlorophyll biosynthesis, 010606 plant biology & botany

Abstract

Forward genetics determines the function of genes underlying trait variation by identifying the change in DNA responsible for changes in phenotype. Detecting phenotypically-relevant variation outside protein coding sequences and distinguishing this from neutral variants is not trivial; partly because the mechanisms by which DNA polymorphisms in the intergenic regions affect gene regulation are poorly understood. Here we utilized a dominant genetic marker with a convenient phenotype to investigate the effect of cis and trans-acting regulatory variation. We performed a forward genetic screen for natural variation that suppress or enhance the semi-dominant mutant alleleOy1-N1989,encoding the magnesium chelatase subunit I of maize. This mutant permits rapid phenotyping of leaf color as a reporter for chlorophyll accumulation, and mapping of natural variation in maize affecting chlorophyll metabolism. We identified a single modifier locus segregating between B73 and Mo17 that was linked to the reporter gene itself, which we callvery oil yellow1. Based on the variation in OY1 transcript abundance and genome-wide association data,vey1is predicted to consist of multiple cis-acting regulatory sequence polymorphisms encoded at the wild-typeoy1alleles. Thevey1allele appears to be a common polymorphism in the maize germplasm that alters the expression level of a key gene in chlorophyll biosynthesis. Thesevey1alleles have no discernable impact on leaf chlorophyll in the absence of theOy1-N1989reporter. Thus, use of a mutant as a simple and efficient reporter for magnesium chelatase activity resulted in the detection of expression-level polymorphisms not readily visible in the laboratory.

Published

2018

22. Identification of fibronectin 1 as a candidate genetic modifier in a Col4a1 mutant mouse model of Gould syndrome

Author

Saunak Sen, Tanav Popli, Kendall Hoff, Marion Jeanne, Douglas B. Gould, and Mao Mao

Subjects

Collagen Type IV, Integrins, Basement membrane, COL4A1, Mutant, Extracellular matrix component, Integrin, Neuroscience (miscellaneous), Medicine (miscellaneous), Locus (genetics), medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Muscular Diseases, Immunology and Microbiology (miscellaneous), medicine, Animals, Abnormalities, Multiple, Integrin-linked kinase, Eye Abnormalities, Modifier, Genes, Suppressor, Myopathy, Fibronectin, Cerebral Hemorrhage, Mutation, Genes, Modifier, biology, Gould syndrome, Chromosome Mapping, Syndrome, Chromosomes, Mammalian, Phenotype, Mice, Mutant Strains, Fibronectins, Cell biology, Integrin signaling, Porencephaly, Genetic Loci, biology.protein, Allelic heterogeneity, medicine.symptom, Signal Transduction, Research Article

Abstract

Collagen type IV alpha 1 and alpha 2 (COL4A1 and COL4A2) are major components of almost all basement membranes. COL4A1 and COL4A2 mutations cause a multisystem disorder that can affect any organ but typically involves the cerebral vasculature, eyes, kidneys and skeletal muscles. In recent years, patient advocacy and family support groups have united under the name of Gould syndrome. The manifestations of Gould syndrome are highly variable, and animal studies suggest that allelic heterogeneity and genetic context contribute to the clinical variability. We previously characterized a mouse model of Gould syndrome caused by a Col4a1 mutation in which the severities of ocular anterior segment dysgenesis (ASD), myopathy and intracerebral hemorrhage (ICH) were dependent on genetic background. Here, we performed a genetic modifier screen to provide insight into the mechanisms contributing to Gould syndrome pathogenesis and identified a single locus [modifier of Gould syndrome 1 (MoGS1)] on Chromosome 1 that suppressed ASD. A separate screen showed that the same locus ameliorated myopathy. Interestingly, MoGS1 had no effect on ICH, suggesting that this phenotype could be mechanistically distinct. We refined the MoGS1 locus to a 4.3 Mb interval containing 18 protein-coding genes, including Fn1, which encodes the extracellular matrix component fibronectin 1. Molecular analysis showed that the MoGS1 locus increased Fn1 expression, raising the possibility that suppression is achieved through a compensatory extracellular mechanism. Furthermore, we found evidence of increased integrin-linked kinase levels and focal adhesion kinase phosphorylation in Col4a1 mutant mice that is partially restored by the MoGS1 locus, implicating the involvement of integrin signaling. Taken together, our results suggest that tissue-specific mechanistic heterogeneity contributes to the variable expressivity of Gould syndrome and that perturbations in integrin signaling may play a role in ocular and muscular manifestations., Summary: We performed a genetic screen in Col4a1 mutant mice to elucidate the mechanisms contributing to Gould syndrome. Our results implicate FN1 as a genetic modifier of some, but not all, aspects of Gould syndrome.

Published

2021

23. Peroxiredoxin alleviates the fitness costs of imidacloprid resistance in an insect pest of rice

Author

Yi Dong, Yan Ling, Ke Xing, Zhikun Liang, Xianchun Li, Rui Pang, Xiangzhao Yue, Meng Chen, Longyu Yuan, Wenqing Zhang, and Xionglei He

Subjects

0106 biological sciences, 0301 basic medicine, Insecticides, Life Cycles, Single Nucleotide Polymorphisms, Adaptation, Biological, Genes, Insect, 01 natural sciences, Insecticide Resistance, Neonicotinoids, chemistry.chemical_compound, Biology (General), Genetics, Drosophila Melanogaster, General Neuroscience, Chromosome Mapping, Eukaryota, Agriculture, Animal Models, Plants, Nitro Compounds, Insects, Chemistry, Experimental Organism Systems, Physical Sciences, Drosophila, Brown planthopper, Agrochemicals, General Agricultural and Biological Sciences, Research Article, Arthropoda, QH301-705.5, Biology, Research and Analysis Methods, Gene Expression Regulation, Enzymologic, General Biochemistry, Genetics and Molecular Biology, Hemiptera, 03 medical and health sciences, Model Organisms, Plant and Algal Models, Imidacloprid, Toxicity Tests, Animals, Grasses, Allele, Gene, Alleles, Genetic Association Studies, Genes, Modifier, General Immunology and Microbiology, Resistance (ecology), Organisms, Chemical Compounds, Biology and Life Sciences, Oryza, Peroxiredoxins, biology.organism_classification, Invertebrates, Nymphs, 010602 entomology, 030104 developmental biology, chemistry, Genetic Loci, Animal Studies, Genetic Fitness, Rice, PEST analysis, Reactive Oxygen Species, Peroxiredoxin, Zoology, Entomology, Function (biology), Developmental Biology

Abstract

Chemical insecticides have been heavily employed as the most effective measure for control of agricultural and medical pests, but evolution of resistance by pests threatens the sustainability of this approach. Resistance-conferring mutations sometimes impose fitness costs, which may drive subsequent evolution of compensatory modifier mutations alleviating the costs of resistance. However, how modifier mutations evolve and function to overcome the fitness cost of resistance still remains unknown. Here we show that overexpression of P450s not only confers imidacloprid resistance in the brown planthopper, Nilaparvata lugens, the most voracious pest of rice, but also leads to elevated production of reactive oxygen species (ROS) through metabolism of imidacloprid and host plant compounds. The inevitable production of ROS incurs a fitness cost to the pest, which drives the increase or fixation of the compensatory modifier allele T65549 within the promoter region of N. lugens peroxiredoxin (NlPrx) in the pest populations. T65549 allele in turn upregulates the expression of NlPrx and thus increases resistant individuals’ ability to clear the cost-incurring ROS of any source. The frequent involvement of P450s in insecticide resistance and their capacity to produce ROS while metabolizing their substrates suggest that peroxiredoxin or other ROS-scavenging genes may be among the common modifier genes for alleviating the fitness cost of insecticide resistance., This study shows that peroxiredoxin is a modifier gene whose cis-upregulation in the brown planthopper (Nilaparvata lugens) increases the ability of resistant populations to clear the fitness cost-incurring reactive oxygen species that inevitably result from P450-meditated metabolism of imidacloprid insecticide.

Published

2021

24. Natural variants suppress mutations in hundreds of essential genes

Author

Gianni Liti, Bryan-Joseph San Luis, Jolanda van Leeuwen, Leopold Parts, Meredith Laver, Michael W Yuen, Carles Pons, Elise Eray, Amandine Batté, Patrick Aloy, Maykel Lopes, Jia-Xing Yue, University of Toronto, Université de Lausanne (UNIL), Institut de Recherche sur le Cancer et le Vieillissement (IRCAN), Université Nice Sophia Antipolis (... - 2019) (UNS), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Côte d'Azur (UCA), Institute for Research in Biomedicine [Barcelona, Spain] (IRB), University of Barcelona-Barcelona Institute of Science and Technology (BIST), Université de Lausanne = University of Lausanne (UNIL), Université Nice Sophia Antipolis (1965 - 2019) (UNS), and Liti, Gianni

Subjects

genetic interactions, Medicine (General), Saccharomyces cerevisiae Proteins, QH301-705.5, Mutant, Context (language use), Saccharomyces cerevisiae, [SDV.GEN] Life Sciences [q-bio]/Genetics, Biology, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, 0302 clinical medicine, R5-920, Gene Expression Regulation, Fungal, Genetic variation, medicine, [SDV.BID.EVO] Life Sciences [q-bio]/Biodiversity/Populations and Evolution [q-bio.PE], natural variation, Allele, Biology (General), Gene, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, [SDV.GEN]Life Sciences [q-bio]/Genetics, Genes, Essential, Genes, Modifier, General Immunology and Microbiology, Applied Mathematics, [SDV.BID.EVO]Life Sciences [q-bio]/Biodiversity/Populations and Evolution [q-bio.PE], compensatory evolution, Genetic Variation, Articles, genetic modifiers, Phenotype, Computational Theory and Mathematics, Gain of Function Mutation, genetic suppression, Genetics, Gene Therapy & Genetic Disease, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery, Function (biology), Information Systems

Abstract

The consequence of a mutation can be influenced by the context in which it operates. For example, loss of gene function may be tolerated in one genetic background, and lethal in another. The extent to which mutant phenotypes are malleable, the architecture of modifiers and the identities of causal genes remain largely unknown. Here, we measure the fitness effects of ~ 1,100 temperature‐sensitive alleles of yeast essential genes in the context of variation from ten different natural genetic backgrounds and map the modifiers for 19 combinations. Altogether, fitness defects for 149 of the 580 tested genes (26%) could be suppressed by genetic variation in at least one yeast strain. Suppression was generally driven by gain‐of‐function of a single, strong modifier gene, and involved both genes encoding complex or pathway partners suppressing specific temperature‐sensitive alleles, as well as general modifiers altering the effect of many alleles. The emerging frequency of suppression and range of possible mechanisms suggest that a substantial fraction of monogenic diseases could be managed by modulating other gene products., A survey of ~ 1,100 temperature‐sensitive alleles of yeast essential genes in ten diverse strains shows that natural genetic variants frequently suppress deleterious mutations. Genetic mapping and allele replacement identify causal suppressor genes.

Published

2021

25. Association analysis of chromosome X to identify genetic modifiers of Huntington's disease

Author

Marcy E. MacDonald, Michael J. Chao, Eun Pyo Hong, Darren G. Monckton, Vanessa C. Wheeler, Thomas Massey, Diane Lucente, Marc Ciosi, James F. Gusella, Seung Kwak, Michael Orth, Lesley Jones, Jeffrey D. Long, Peter Holmans, S. V. Lobanov, Jong-Min Lee, and Branduff McAllister

Subjects

0301 basic medicine, Male, Huntingtin, X Chromosome, DNA repair, Single-nucleotide polymorphism, Biology, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Huntington's disease, Genetic variation, medicine, Humans, Age of Onset, X chromosome, Genetic association, Genetics, Huntingtin Protein, Genes, Modifier, medicine.disease, 030104 developmental biology, Huntington Disease, Female, Neurology (clinical), Trinucleotide repeat expansion, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Background: Huntington’s disease (HD) is caused by an expanded (>35) CAG trinucleotide repeat in huntingtin (HTT). Age-at-onset of motor symptoms is inversely correlated with the size of the inherited CAG repeat, which expands further in brain regions due to somatic repeat instability. Our recent genetic investigation focusing on autosomal SNPs revealed that age-at-onset is also influenced by genetic variation at many loci, the majority of which encode genes involved in DNA maintenance/repair processes and repeat instability. Objective: We performed a complementary association analysis to determine whether variants in the X chromosome modify HD. Methods: We imputed SNPs on chromosome X for ∼9,000 HD subjects of European ancestry and performed an X chromosome-wide association study (XWAS) to test for association with age-at-onset corrected for inherited CAG repeat length. Results: In a mixed effects model XWAS analysis of all subjects (males and females), assuming random X-inactivation in females, no genome-wide significant onset modification signal was found. However, suggestive significant association signals were detected at Xq12 (top SNP, rs59098970; p-value, 1.4E-6), near moesin (MSN), in a region devoid of DNA maintenance genes. Additional suggestive signals not involving DNA repair genes were observed in male- and female-only analyses at other locations. Conclusion: Although not genome-wide significant, potentially due to small effect size compared to the power of the current study, our data leave open the possibility of modification of HD by a non-DNA repair process. Our XWAS results are publicly available at the updated GEM EURO 9K website hosted at https://www.hdinhd.org/ for browsing, pathway analysis, and data download.

Published

2021

26. A simple expression for the strength of selection on recombination generated by interference among mutations

Author

Denis Roze, Evolutionary Biology and Ecology of Algae (EBEA), Pontificia Universidad Católica de Chile (UC)-Sorbonne Université (SU)-Universidad Austral de Chile-Centre National de la Recherche Scientifique (CNRS)-Station biologique de Roscoff (SBR), and Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS)

Subjects

0106 biological sciences, Genotype, Genetic Linkage, [SDV]Life Sciences [q-bio], Biology, multilocus population genetics, Interference (genetic), 010603 evolutionary biology, 01 natural sciences, Genetic recombination, Evolution, Molecular, 03 medical and health sciences, Effective population size, meiosis, Selection, Genetic, Alleles, Selection (genetic algorithm), ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, Population Density, Recombination, Genetic, Genetics, 0303 health sciences, Genes, Modifier, Multidisciplinary, Natural selection, Reproduction, [SDV.BID.EVO]Life Sciences [q-bio]/Biodiversity/Populations and Evolution [q-bio.PE], Genetic Variation, Epistasis, Genetic, Biological Sciences, genetic architecture, Genetic architecture, genetic interference, Mutation, Evolution evolution of recombination, Epistasis, Recombination

Abstract

One of the most widely cited hypotheses to explain the evolutionary maintenance of genetic recombination states that the reshuffling of genotypes at meiosis increases the efficiency of natural selection by reducing interference among selected loci. However, and despite several decades of theoretical work, a quantitative estimation of the possible selective advantage of a mutant allele increasing chromosomal map length (the average number of cross-overs at meiosis) remains difficult. This article derives a simple expression for the strength of selection acting on a modifier gene affecting the genetic map length of a whole chromosome or genome undergoing recurrent mutation. In particular, it shows that indirect selection for recombination caused by interference among mutations is proportional to [Formula: see text] , where [Formula: see text] is the effective population size, [Formula: see text] is the deleterious mutation rate per chromosome, and [Formula: see text] is the chromosome map length. Indirect selection is relatively insensitive to the fitness effects of deleterious alleles, epistasis, or the genetic architecture of recombination rate variation and may compensate for substantial costs associated with recombination when linkage is tight. However, its effect generally stays weak in large, highly recombining populations.

Published

2021

27. New Omics–Derived Perspectives on Retinal Dystrophies: Could Ion Channels-Encoding or Related Genes Act as Modifier of Pathological Phenotype?

Author

Rosalia D'Angelo, Concetta Scimone, Karim Mahmoud Nabil, Luigi Donato, Ebtesam M. Abdalla, Antonina Sidoti, and Simona Alibrandi

Subjects

0301 basic medicine, Male, Computational biology, Biology, ENCODE, Catalysis, Article, lcsh:Chemistry, Inorganic Chemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Retinal Dystrophies, Humans, Exome, Physical and Theoretical Chemistry, lcsh:QH301-705.5, Molecular Biology, Gene, Integral membrane protein, Spectroscopy, Ion channel, Exome sequencing, Genes, Modifier, Polymorphism, Genetic, Organic Chemistry, ion channels, Retinal, General Medicine, Phenotype, Computer Science Applications, Pedigree, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, chemistry, retinal degenerations, WES, Female, synapses, 030217 neurology & neurosurgery

Abstract

Ion channels are membrane-spanning integral proteins expressed in multiple organs, including the eye. Here, ion channels play a role in several physiological processes, like signal transmission and visual processing. A wide range of mutations have been reported in the corresponding genes and their interacting subunit coding genes, which contribute significantly to a wide spectrum of ocular diseases collectively called channelopathies, a subgroup of inherited retinal dystrophies. Such mutations result in either a loss or gain-of channel functions affecting the structure, assembly, trafficking and localization of channel proteins. We investigated the probands of seven Italian and Egyptian families affected by not completely defined forms of inherited retinal dystrophies, by whole exome sequencing (WES) experiments, and found interesting variants in already known causative genes probably able to impair retinal functionalities. However, because such variants did not completely explain the phenotype manifested by each patient, we proceed to further investigate possible related genes carrying mutations that might complement previously found data, based on the common aspect linked to neurotransmission impairments. We found 10 mutated genes whose variants might alter important ligand binding sites differently distributed through all considered patients. Such genes encode for ion channels, or their regulatory proteins, and strictly interact with known causative genes, also sharing with them synaptic-related pathways. Taking into account several limitations that will be resolved by further experiments, we believe that our exploratory investigation will help scientists to provide a new promising paradigm for precise diagnosis of retinal dystrophies to facilitate the development of rational treatments.

Published

2020

28. Identification of disease-relevant modulators of the SHH pathway in the developing brain

Author

Tamrat M Mamo, Bettina Purfürst, Annette Hammes, Anje Sporbert, Martin Lehmann, Jessica Görne, Alena Laier, Franziska Witte, Hannes Gonschior, Matthias Richter, Nora Mecklenburg, Norbert Hubner, and Izabela Kowalczyk

Subjects

Heart Defects, Congenital, Congenic, Neuroepithelial Cells, Penetrance, Protein Serine-Threonine Kinases, Transcriptome, Mice, Holoprosencephaly, Downregulation and upregulation, medicine, Animals, Hedgehog Proteins, Cilia, Sonic hedgehog, Molecular Biology, Gene, Genes, Modifier, biology, Cilium, Brain, medicine.disease, Cell biology, Securin, Disease Models, Animal, Low Density Lipoprotein Receptor-Related Protein-2, Phenotype, Cardiovascular and Metabolic Diseases, Mutation, biology.protein, Technology Platforms, Function and Dysfunction of the Nervous System, Developmental Biology, Signal Transduction

Abstract

Pathogenic gene variants in humans that affect the sonic hedgehog (SHH) pathway lead to severe brain malformations with variable penetrance due to unknown modifier genes. To identify such modifiers, we established novel congenic mouse models. LRP2-deficient C57BL/6N mice suffer from heart outflow tract defects and holoprosencephaly caused by impaired SHH activity. These defects are fully rescued on a FVB/N background, indicating a strong influence of modifier genes. Applying comparative transcriptomics, we identified Pttg1 and Ulk4 as candidate modifiers upregulated in the rescue strain. Functional analyses showed that ULK4 and PTTG1, both microtubule-associated proteins, are positive regulators of SHH signaling, rendering the pathway more resilient to disturbances. In addition, we characterized ULK4 and PTTG1 as previously unidentified components of primary cilia in the neuroepithelium. The identification of genes that powerfully modulate the penetrance of genetic disturbances affecting the brain and heart is likely relevant to understanding the variability in human congenital disorders.

Published

2020

29. Exploiting codon usage identifies intensity-specific modifiers of Ras/MAPK signaling in vivo

Author

Erez Cohen, Rebeccah Stewart, Christopher M. Counter, Hamed Zaribafzadeh, Jessica K. Sawyer, Zahra Kabiri, Donald T. Fox, Sarah V. Paramore, Ruth A. Montague, and Scott R Allen

Subjects

MAPK/ERK pathway, Cancer Research, Regulator, ERK signaling cascade, QH426-470, Genome, 0302 clinical medicine, Cell Signaling, Medicine and Health Sciences, Drosophila Proteins, Codon Usage, Genetics (clinical), 0303 health sciences, biology, Drosophila Melanogaster, Signaling cascades, Eukaryota, Animal Models, Insects, Experimental Organism Systems, 030220 oncology & carcinogenesis, Codon usage bias, Mitogen-activated protein kinase, Engineering and Technology, Drosophila, Anatomy, Mitogen-Activated Protein Kinases, Drosophila melanogaster, Signal transduction, Genomic Signal Processing, Research Article, Signal Transduction, MAPK signaling cascades, Arthropoda, MAP Kinase Signaling System, Ras Signaling, Computational biology, Research and Analysis Methods, 03 medical and health sciences, Model Organisms, Ocular System, Gene Types, Genetics, Animals, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Genes, Modifier, Organisms, Biology and Life Sciences, Cell Biology, biology.organism_classification, Invertebrates, Signal Processing, Animal Studies, ras Proteins, biology.protein, Eyes, Regulator Genes, Head, Zoology, Entomology

Abstract

Signal transduction pathways are intricately fine-tuned to accomplish diverse biological processes. An example is the conserved Ras/mitogen-activated-protein-kinase (MAPK) pathway, which exhibits context-dependent signaling output dynamics and regulation. Here, by altering codon usage as a novel platform to control signaling output, we screened the Drosophila genome for modifiers specific to either weak or strong Ras-driven eye phenotypes. Our screen enriched for regions of the genome not previously connected with Ras phenotypic modification. We mapped the underlying gene from one modifier to the ribosomal gene RpS21. In multiple contexts, we show that RpS21 preferentially influences weak Ras/MAPK signaling outputs. These data show that codon usage manipulation can identify new, output-specific signaling regulators, and identify RpS21 as an in vivo Ras/MAPK phenotypic regulator., Author summary Cellular communication is critical in controlling the growth of organs and must be carefully regulated to prevent disease. The Ras signaling pathway is frequently used for cellular communication of tissue growth regulation but can operate at different signaling strengths. Here, we used a novel strategy to identify genes that specifically tune weak or strong Ras signaling states. We find that the gene RpS21 preferentially tunes weak Ras signaling states.

Published

2020

30. SVEP1 as a Genetic Modifier of TEK-Related Primary Congenital Glaucoma

Author

Nickie Stangel, Yongwook Dan, Conceição Egas, Terri L. Young, Kristina N. Whisenhunt, Jacob S Martin, Fatemeh Suri, Reza Maroofian, Samuel J Huang, Susana Carmona, Susan E. Quaggin, Tomokazu Souma, Emmanuelle Souzeau, Behzad Fallahi Motlagh, Jing Jin, Sarah M LaMartina, Nicole M Jody, Brendan M Lawson, Mehrnaz Narooie-Nejad, Heather D. Potter, Emily C. Higuchi, Owen M. Siggs, Jamie E Craig, Eduardo Silva, Vachiranee Limviphuvadh, Sebastian Maurer-Stroh, Xue Zhang, Elahe Elahi, Yasmin S. Bradfield, Maria José Simões, Evie Anagnos, Sean Martin, and Stuart W. Tompson

Subjects

0301 basic medicine, Male, Pathology, genetic structures, Genotyping Techniques, Glaucoma, Penetrance, Mice, 0302 clinical medicine, Gene Frequency, Missense mutation, Protein Isoforms, Phosphorylation, Exome sequencing, Middle Aged, Receptor, TIE-2, Pedigree, Schlemm's canal, Child, Preschool, Female, Haploinsufficiency, medicine.medical_specialty, Blotting, Western, Mutation, Missense, Biology, 03 medical and health sciences, Dysgenesis, Exome Sequencing, medicine, Genetics, Human Umbilical Vein Endothelial Cells, Animals, Humans, Allele, Allele frequency, SVEP1, Intraocular Pressure, Aged, modifier, Genes, Modifier, Hydrophthalmos, Infant, Newborn, Infant, medicine.disease, 030104 developmental biology, glaucoma, HEK293 Cells, TEK, 030221 ophthalmology & optometry, Cell Adhesion Molecules

Abstract

Purpose Affecting children by age 3, primary congenital glaucoma (PCG) can cause debilitating vision loss by the developmental impairment of aqueous drainage resulting in high intraocular pressure (IOP), globe enlargement, and optic neuropathy. TEK haploinsufficiency accounts for 5% of PCG in diverse populations, with low penetrance explained by variable dysgenesis of Schlemm's canal (SC) in mice. We report eight families with TEK-related PCG, and provide evidence for SVEP1 as a disease modifier in family 8 with a higher penetrance and severity. Methods Exome sequencing identified coding/splice site variants with an allele frequency less than 0.0001 (gnomAD). TEK variant effects were assayed in construct-transfected HEK293 cells via detection of autophosphorylated (active) TEK protein. An enucleated eye from an affected member of family 8 was examined via histology. SVEP1 expression in developing outflow tissues was detected by immunofluorescent staining of 7-day mouse anterior segments. SVEP1 stimulation of TEK expression in human umbilical vascular endothelial cells (HUVECs) was measured by TaqMan quantitative PCR. Results Heterozygous TEK loss-of-function alleles were identified in eight PCG families, with parent-child disease transmission observed in two pedigrees. Family 8 exhibited greater disease penetrance and severity, histology revealed absence of SC in one eye, and SVEP1:p.R997C was identified in four of the five affected individuals. During SC development, SVEP1 is secreted by surrounding tissues. SVEP1:p.R997C abrogates stimulation of TEK expression by HUVECs. Conclusions We provide further evidence for PCG caused by TEK haploinsufficiency, affirm autosomal dominant inheritance in two pedigrees, and propose SVEP1 as a modifier of TEK expression during SC development, affecting disease penetrance and severity.

Published

2020

31. Identifying genetic modifiers of age-associated penetrance in X-linked dystonia-parkinsonism

Author

Pia Otto, Katja Lohmann, Christine Klein, Jelena Pozojevic, Frank J. Kaiser, Henrike Hanssen, Nutan Sharma, Cid Czarina E. Diesta, Arndt Rolfs, Andre Franke, Patrick Acuna, Criscely L. Go, Inke R. König, Gerard Saranza, Jana Quismundo, Susen Schaake, Roland Dominic G. Jamora, Trisha Multhaupt-Buell, Norbert Brüggemann, Marija Dulovic-Mahlow, Aloysius Domingo, Ulrich Müller, Raymond L. Rosales, Karen Grütz, Laurie J. Ozelius, Peter Bauer, Björn-Hergen Laabs, Fabian Kilpert, Michael Wittig, Ana Westenberger, and Valerija Dobricic

Subjects

0301 basic medicine, Adult, Male, Science, Medizin, General Physics and Astronomy, Single-nucleotide polymorphism, Genome-wide association study, Penetrance, X-Linked Dystonia Parkinsonism, Biology, DNA Mismatch Repair, Polymorphism, Single Nucleotide, Genome-wide association studies, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Young Adult, 0302 clinical medicine, PMS2, Humans, Allele, Age of Onset, Alleles, Aged, Genetics, Multidisciplinary, Genes, Modifier, Molecular medicine, Genetic Diseases, X-Linked, General Chemistry, Middle Aged, Protective Factors, 030104 developmental biology, MSH3, Dystonic Disorders, Genetic Loci, Case-Control Studies, Age of onset, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

X-linked dystonia-parkinsonism is a neurodegenerative disorder caused by a founder retrotransposon insertion, in which a polymorphic hexanucleotide repeat accounts for ~50% of age at onset variability. Employing a genome-wide association study to identify additional factors modifying age at onset, we establish that three independent loci are significantly associated with age at onset (p, Age at onset of X-linked dystonia-parkinsonism is 50% explained by the length of a repeat in an SVA insert. The authors perform a GWAS for genetic modifiers and discover three more loci, accounting for another 13% of variability in age at onset with the protective alleles delaying onset by seven years.

Published

2020

32. Genetic modifiers in rare disorders : the case of fragile X syndrome

Author

Lucy Wilde, Gaia Scerif, Joanne D. Stockton, Pria Sandhu, Hayley Crawford, Chris Oliver, Lauren Shelley, Andrew D Beggs, and Joseph P. McCleery

Subjects

Adult, Adolescent, Challenging behaviour, RJ, Population, Single-nucleotide polymorphism, Biology, Catechol O-Methyltransferase, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, 0302 clinical medicine, Genetic variation, Genotype, Genetics, medicine, Humans, ADHD, education, Child, Monoamine Oxidase, Genetics (clinical), 030304 developmental biology, Genetic association, Problem Behavior, Serotonin Plasma Membrane Transport Proteins, 0303 health sciences, education.field_of_study, Genes, Modifier, Autism spectrum disorders, medicine.disease, Fragile X syndrome, Phenotype, Risk factors, Child, Preschool, Fragile X Syndrome, Behavioural genetics, Autism, Genetic markers, 030217 neurology & neurosurgery, RC

Abstract

Methods employed in genome-wide association studies are not feasible ways to explore genotype–phenotype associations in rare disorders due to limited statistical power. An alternative approach is to examine relationships among specific single nucleotide polymorphisms (SNPs), selected a priori, and behavioural characteristics. Here, we adopt this strategy to examine relationships between three SNPs (5-HTTLPR, MAOA, COMT) and specific clinically-relevant behaviours that are phenotypic of fragile X syndrome (FXS) but vary in severity and frequency across individuals. Sixty-four males with FXS participated in the current study. Data from standardised informant measures of challenging behaviour (defined as physical aggression, property destruction, stereotyped behaviour, and self-injury), autism symptomatology, attention-deficit-hyperactivity-disorder characteristics, repetitive behaviour and mood/interest and pleasure were compared between each SNP genotype. No association was observed between behavioural characteristics and either 5-HTTLPR (serotonin) or MAOA (monoamine oxidase) genotypes. However, compared to the COMT (dopamine) AG and GG genotypes, the AA genotype was associated with greater interest and pleasure in the environment, and with reduced risk for property destruction, stereotyped behaviour and compulsive behaviour. The results suggest that common genetic variation in the COMT genotype affecting dopamine levels in the brain may contribute to the variability of challenging and repetitive behaviours and interest and pleasure in this population. This study identifies a role for additional genetic risk in understanding the neural and genetic mechanisms contributing to phenotypic variability in neurodevelopmental disorders, and highlights the merit of investigating SNPs that are selected a priori on a theoretical basis in rare populations.

Published

2020

33. Mitochondrial DNA Haplotypes as Genetic Modifiers of Cancer

Author

Prashant Mishra, David G. McFadden, and Alpaslan Tasdogan

Subjects

0301 basic medicine, Cancer Research, Mitochondrial DNA, Carcinogenesis, Apoptosis, Mitochondrion, Biology, medicine.disease_cause, DNA, Mitochondrial, 03 medical and health sciences, Genetic Heterogeneity, 0302 clinical medicine, Loss of Function Mutation, Neoplasms, medicine, Humans, chemistry.chemical_classification, Genetics, Reactive oxygen species, Cellular metabolism, Genes, Modifier, Haplotype, Cancer, medicine.disease, 030104 developmental biology, Oncology, chemistry, Haplotypes, 030220 oncology & carcinogenesis, Genome, Mitochondrial, Reactive Oxygen Species

Abstract

Mitochondria play an essential role in cellular metabolism, generation of reactive oxygen species (ROS), and the initiation of apoptosis. These properties enable mitochondria to be crucial integrators in the pathways of tumorigenesis. An open question is to what extent variation in the mitochondrial genome (mtDNA) contributes to the biological heterogeneity observed in human tumors. In this review, we summarize our current understanding of the role of mtDNA genetics in relation to human cancers.

Published

2020

34. Strain-dependent modifier genes determine survival inZfp423mice

Author

Zheng Liu, Eunnie Kim, Edward Chen, A. Gonzalez, Cinny Wong, Dorothy Concepcion, Wendy A. Alcaraz, Shelby Wade, Phoebe Valdes, Alison Ponn, Bruce A. Hamilton, and Hsiang-Hua M. Chen

Subjects

Null mice, inbred strains, Congenic, brain development, Locus (genetics), ZNF423, Investigations, QH426-470, Biology, Ciliopathies, Mice, 03 medical and health sciences, 0302 clinical medicine, Inbred strain, medicine, Genetics, Animals, Allele, Molecular Biology, Gene, Alleles, Genetics (clinical), 030304 developmental biology, Mice, Inbred BALB C, 0303 health sciences, Genes, Modifier, smad signaling, medicine.disease, Mice, Inbred C57BL, Ciliopathy, ciliopathy, 030217 neurology & neurosurgery, Transcription Factors, Modifier Genes

Abstract

Zfp423encodes a transcriptional regulatory protein that interacts with canonical signaling and lineage pathways. Mutations in mouseZfp423or its human orthologZNF423are associated with a range of developmental abnormalities reminiscent of ciliopathies, including cerebellar vermis hypoplasia and other midline brain defects. Null mice have reduced viability in most strain backgrounds. Here we show complete lethality on a C57BL/6J background, dominant rescue in backcrosses to any of 13 partner strains, with strain-dependent survival frequencies, and evidence for a BALB/c-derived survival modifier locus on chromosome 5. Survival data indicate both perinatal and postnatal periods of lethality. Anatomical data from a hypomorphic gene trap allele observed on both C57BL/6J and BALB/c congenic backgrounds shows an aggregate effect of background on sensitivity to Zfp423 loss rather than a binary effect on viability.

Published

2020

35. Queen pheromone modulates the expression of epigenetic modifier genes in the brain of honeybee workers

Author

Carlos Antônio Mendes Cardoso-Junior, Isobel Ronai, Benjamin P. Oldroyd, and Klaus Hartfelder

Subjects

Epigenomics, Queen mandibular pheromone, Biology, Molecular Evolution, Pheromones, Epigenesis, Genetic, COMPORTAMENTO SOCIAL ANIMAL, 03 medical and health sciences, 0302 clinical medicine, Animals, Epigenetics, Social Behavior, Gene, 030304 developmental biology, Genetics, 0303 health sciences, Genes, Modifier, fungi, Brain, Honey bee, Bees, Agricultural and Biological Sciences (miscellaneous), Eusociality, Histone, Sex pheromone, biology.protein, behavior and behavior mechanisms, Pheromone, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery

Abstract

Pheromones are used by many insects to mediate social interactions. In the highly eusocial honey bee ( Apis mellifera ) queen mandibular pheromone is involved in the regulation of reproduction and the rate of ageing of workers. The molecular mechanisms by which queen mandibular pheromone acts remain largely unknown. Here we investigate how genes responsible for epigenetic modifications to DNA, RNA and histones expressed in the brain of honey bee workers respond to the presence of queen mandibular pheromone. Several of these genes are upregulated in workers exposed to queen mandibular pheromone. This suggests that epigenetic mechanisms are mediated by pheromonal communication between queens and workers, and that the interaction of pheromone signalling and epigenetics may mediate some of the neural plasticity that underlies ageing-associated traits in social insects. We suggest that pheromonal communication systems, such as those used by social insects, evolved to respond to environmental clues by making use of epigenomic machineries.

Published

2020

36. A breeding strategy to identify modifiers of high genetic risk for methamphetamine intake

Author

Alexandra M. Stafford, John R. K. Mootz, Harue Baba, Tamara J. Phillips, Jason Erk, and Cheryl Reed

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Amphetamine-Related Disorders, Biology, Selective breeding, Article, Body Temperature, Methamphetamine, Receptors, G-Protein-Coupled, 03 medical and health sciences, Behavioral Neuroscience, chemistry.chemical_compound, Mice, 0302 clinical medicine, Control line, Internal medicine, Genotype, Genetics, medicine, Animals, Allele, Receptor, Saccharin, Sensitization, Genes, Modifier, Feeding Behavior, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Phenotype, Neurology, chemistry, Mice, Inbred DBA, Hybridization, Genetic, Female, 030217 neurology & neurosurgery, Locomotion, medicine.drug, Selective Breeding

Abstract

Trace amine-associated receptor 1 (Taar1) impacts methamphetamine (MA) intake. A mutant allele (Taar1(m1J)) derived from the DBA/2J mouse strain codes for a non-functional receptor, and Taar1(m1J/m1J) mice consume more MA than mice possessing the reference Taar1(+) allele. To study the impact of this mutation in a genetically diverse population, heterogeneous stock-collaborative cross (HS-CC) mice, the product of an 8-way cross of standard and wild-derived strains, were tested for MA intake. HS-CC had low MA intake, so a HS-CC by DBA/2J strain F2 intercross was created to transfer the mutant allele onto the diverse background, and used for selective breeding. To study residual variation in MA intake existing in Taar1(m1J/m1J) mice, selective breeding for higher (MAH) vs. lower (MAL) MA intake was initiated from Taar1(m1J/m1J) F2 individuals; a control line of Taar1(+/+) individuals (MAC) was retained. The lines were also examined for MA-induced locomotor and thermal responses, and fluid and tastant consumption. Taar1(m1J/m1J) F2 mice consumed significantly more MA than Taar1(+/+) F2 mice. Response to selection was significant by generation 2 and there were corresponding differences in fluid consumed. Fluid consumption was not different in non-MA drinking studies. Taar1(m1J/m1J) genotype (MAL or MAH vs. MAC mice) was associated with heighted MA locomotor and reduced hypothermic responses. MAL mice exhibited greater sensitization than MAH mice, but the selected lines did not consistently differ for thermal or tastant phenotypes. Residual variation among high risk Taar1(m1J/m1J) mice appears to involve mechanisms associated with neuroadaptation to MA, but not sensitivity to hypothermic effects of MA.

Published

2020

37. Modifier genes in SCN1A‐related epilepsy syndromes

Author

Bobby P. C. Koeleman, Iris M de Lange, Ruben van 't Slot, Nine V A M Knoers, Marjan J. A. van Kempen, Eva H. Brilstra, Robert F Ernst, Isaac J. Nijman, Flip Mulder, and Anja C M Sonsma

Subjects

0301 basic medicine, Male, DRAVET-SYNDROME, VARIANTS, 030105 genetics & heredity, Dravet, Epilepsy, modifier genes, Exome, SCN1A, Child, Genetics (clinical), Genetics, SEVERE MYOCLONIC EPILEPSY, MOUSE MODEL, Middle Aged, Phenotype, Child, Preschool, Cohort, Original Article, Female, GEFS+, Adult, lcsh:QH426-470, Adolescent, PHENOTYPES, Genomics, Biology, 03 medical and health sciences, medicine, GEFS PLUS, Humans, Molecular Biology, Gene, Aged, SPECTRUM, Genes, Modifier, DELETION, Original Articles, FRAMEWORK, medicine.disease, Minor allele frequency, NAV1.1 Voltage-Gated Sodium Channel, lcsh:Genetics, 030104 developmental biology, Epilepsy syndromes, epilepsy, SCN1A MUTATION, phenotypic variability, Epileptic Syndromes, Modifier Genes

Abstract

Background SCN1A is one of the most important epilepsy‐related genes, with pathogenic variants leading to a range of phenotypes with varying disease severity. Different modifying factors have been hypothesized to influence SCN1A‐related phenotypes. We investigate the presence of rare and more common variants in epilepsy‐related genes as potential modifiers of SCN1A‐related disease severity. Methods 87 patients with SCN1A‐related epilepsy were investigated. Whole‐exome sequencing was performed by the Beijing Genomics Institute (BGI). Functional variants in 422 genes associated with epilepsy and/or neuronal excitability were investigated. Differences in proportions of variants between the epilepsy genes and four control gene sets were calculated, and compared to the proportions of variants in the same genes in the ExAC database. Results Statistically significant excesses of variants in epilepsy genes were observed in the complete cohort and in the combined group of mildly and severely affected patients, particularly for variants with minor allele frequencies of, Relatively common variants in epilepsy genes may play a large role in modulating SCN1A‐related phenotypes. They may modify the phenotypes of both severely and mildly affected patients.

Published

2020

38. Mouse genetics reveals Barttin as a genetic modifier of Joubert syndrome

Author

Colin G. Miles, Heather J. Cordell, Simon A. Ramsbottom, Meral Gunay-Aygun, Shirlee Shril, Elisa Molinari, John A. Sayer, Helena L. Spiewak, Laura A. Devlin, Peter E. Thelwall, Sophie Saunier, Flora Silbermann, Friedhelm Hildebrandt, Katrina M Wood, Gavin J. Clowry, Newcastle University [Newcastle], Newcastle Upon Tyne Hospitals NHS Foundation Trust, Imagine - Institut des maladies génétiques (IHU) (Imagine - U1163), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), Harvard Medical School [Boston] (HMS), National Human Genome Research Institute (NHGRI), Johns Hopkins University School of Medicine [Baltimore], and Saunier, Sophie

Subjects

0301 basic medicine, [SDV]Life Sciences [q-bio], Cell Cycle Proteins, 030105 genetics & heredity, Biology, Polymorphism, Single Nucleotide, Severity of Illness Index, Retina, Joubert syndrome, Mice, 03 medical and health sciences, Cystic kidney disease, Antigens, Neoplasm, Chloride Channels, Cerebellum, medicine, Animals, Abnormalities, Multiple, Genetic Predisposition to Disease, genetics, Eye Abnormalities, Barttin, Genetics, Cystic kidney, modifier, Genes, Modifier, Multidisciplinary, Genetic heterogeneity, Biological Sciences, Kidney Diseases, Cystic, medicine.disease, Phenotype, Mice, Inbred C57BL, [SDV] Life Sciences [q-bio], Cytoskeletal Proteins, Disease Models, Animal, Ciliopathy, 030104 developmental biology, ciliopathy, Mutation, Kidney Diseases, Rare disease, Kidney disease

Abstract

Significance Our current understanding of genetic disease is often inadequate, largely due to genetic background effects that modify disease presentation. This is particularly challenging for rare diseases that lack sufficient numbers of patients for genome-wide association studies. We show in a series of experiments using a murine model of Joubert syndrome, a multisystem ciliopathy, that a single locus is a modifier of cystic kidney disease. We go on to show that the human homolog plays a similar role in disease using a cohort of patients. These findings make a significant contribution to the underplayed (and often ignored) role of genetic background in murine models and how this can be exploited to understand further rare inherited disease., Genetic and phenotypic heterogeneity and the lack of sufficiently large patient cohorts pose a significant challenge to understanding genetic associations in rare disease. Here we identify Bsnd (alias Barttin) as a genetic modifier of cystic kidney disease in Joubert syndrome, using a Cep290-deficient mouse model to recapitulate the phenotypic variability observed in patients by mixing genetic backgrounds in a controlled manner and performing genome-wide analysis of these mice. Experimental down-regulation of Bsnd in the parental mouse strain phenocopied the severe cystic kidney phenotype. A common polymorphism within human BSND significantly associates with kidney disease severity in a patient cohort with CEP290 mutations. The striking phenotypic modifications we describe are a timely reminder of the value of mouse models and highlight the significant contribution of genetic background. Furthermore, if appropriately managed, this can be exploited as a powerful tool to elucidate mechanisms underlying human disease heterogeneity.

Published

2020

39. TCTEX1D1 is a genetic modifier of disease progression in Duchenne muscular dystrophy

Author

Spitali, P., Zaharieva, I., Bohringer, S., Hiller, M., Chaouch, A., Roos, A., Scotton, C., Claustres, M., Bello, L., McDonald, C.M., Hoffman, E.P., Koeks, Z., Suchiman, H.E., Cirak, S., Scoto, M., Reza, M., Hoen, P.A.C. t, Niks, E.H., Tuffery-Giraud, S., Lochmuller, H., Ferlini, A., Muntoni, F., Aartsma-Rus, A., Dubrovsky, A., Kornberg, A., North, K., Ryan, M., Webster, R., Biggar, W.D., McAdam, L.C., Mah, J.K., Kolski, H., Vishwanathan, V., Chidambaranathan, S., Nevo, Y., Gorni, K., Carlo, J., Tulinius, M., Lotze, T., Bertorini, T.E., Day, J.W., Karachunski, P., Clemens, P.R., Abdel-Hamid, H., Teasley, J., Kuntz, N., Driscoll, S., Bodensteiner, J.B., Connolly, A.M., Pestronk, A., Abresch, R.T., Henricson, E.K., Joyce, N.C., Cnaan, A., Gordish-Dressmsn, H., Morgenroth, L.P., Leshner, R., Tesi-Rocha, C., Thangarajh, M., Duong, T., CINRG Investigators, Leibniz-Institut für Analytische Wissenschaften - ISAS - e.V., Laboratoire de génétique des maladies rares. Pathologie moleculaire, etudes fonctionnelles et banque de données génétiques (LGMR), IFR3, Université Montpellier 1 (UM1)-Université Montpellier 1 (UM1)-Université de Montpellier (UM)-Institut National de la Santé et de la Recherche Médicale (INSERM), Universita degli Studi di Padova, Newcastle University [Newcastle], Department of Reproduction and Growth, UOL of Medical Genetics (University Hospital St Anna, Ferrara), University of Ferrara at St. Anna Hospital, Dubowitz Neuromuscular Center, Institute of Child Health, and Human Genetics

Subjects

Male, 0301 basic medicine, Adolescent, Duchenne muscular dystrophy, [SDV]Life Sciences [q-bio], Locus (genetics), Polymorphism, Single Nucleotide, Genome-wide association studies, Article, Prognostic markers, 03 medical and health sciences, Exon, 0302 clinical medicine, Genotype, Genetics, medicine, Humans, Allele, Muscular dystrophy, Child, Genetics (clinical), Genes, Modifier, biology, business.industry, Neuromuscular disease, medicine.disease, Muscular Dystrophy, Duchenne, Phenotype, 030104 developmental biology, Disease Progression, biology.protein, Human genome, Dystrophin, business, 030217 neurology & neurosurgery

Abstract

Duchenne muscular dystrophy (DMD) is caused by pathogenic variants in the DMD gene leading to the lack of dystrophin. Variability in the disease course suggests that other factors influence disease progression. With this study we aimed to identify genetic factors that may account for some of the variability in the clinical presentation. We compared whole-exome sequencing (WES) data in 27 DMD patients with extreme phenotypes to identify candidate variants that could affect disease progression. Validation of the candidate SNPs was performed in two independent cohorts including 301 (BIO-NMD cohort) and 109 (CINRG cohort of European ancestry) DMD patients, respectively. Variants in the Tctex1 domain containing 1 (TCTEX1D1) gene on chromosome 1 were associated with age of ambulation loss. The minor alleles of two independent variants, known to affect TCTEX1D1 coding sequence and induce skipping of its exon 4, were associated with earlier loss of ambulation. Our data show that disease progression of DMD is affected by a new locus on chromosome 1 and demonstrate the possibility to identify genetic modifiers in rare diseases by studying WES data in patients with extreme phenotypes followed by multiple layers of validation.

Published

2020

40. X-linked muscular dystrophy in a Labrador Retriever strain: phenotypic and molecular characterisation

Author

Jean-Laurent Thibaud, Christophe Béroud, Adeline Vulin, Kevin M. Flanigan, Nicolas Wein, Nathalie Deburgrave, Stéphane Blot, Jean-Claude Kaplan, Isabel Punzón, Laurent Tiret, Cécile Peccate, Robert B. Weiss, Catherine Escriou, Inès Barthélémy, Nadège Calmels, Luis Garcia, Carole Drougard, Gestionnaire, Hal Sorbonne Université, Institut Mondor de Recherche Biomédicale (IMRB), Institut National de la Santé et de la Recherche Médicale (INSERM)-IFR10-Université Paris-Est Créteil Val-de-Marne - Paris 12 (UPEC UP12), École nationale vétérinaire - Alfort (ENVA), Service de biochimie et de génétique moléculaire [CHU Cochin], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpital Cochin [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Laboratoire de Diagnostic Génétique [CHU Strasbourg], Université de Strasbourg (UNISTRA)-CHU Strasbourg, University of Utah School of Medicine [Salt Lake City], Université de Versailles Saint-Quentin-en-Yvelines (UVSQ), Ohio State University [Columbus] (OSU), Centre de recherche en Myologie – U974 SU-INSERM, Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), Institut de Myologie, Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Association française contre les myopathies (AFM-Téléthon)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Marseille medical genetics - Centre de génétique médicale de Marseille (MMG), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire de Génétique Moléculaire [Hôpital de la Timone - APHM], Département de génétique médicale [Hôpital de la Timone - APHM], Aix Marseille Université (AMU)-Assistance Publique - Hôpitaux de Marseille (APHM)- Hôpital de la Timone [CHU - APHM] (TIMONE)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Aix Marseille Université (AMU)-Assistance Publique - Hôpitaux de Marseille (APHM)- Hôpital de la Timone [CHU - APHM] (TIMONE)-Institut National de la Santé et de la Recherche Médicale (INSERM), Handicap neuromusculaire : Physiopathologie, Biothérapie et Pharmacologies appliquées (END-ICAP), Université de Versailles Saint-Quentin-en-Yvelines (UVSQ)-Institut National de la Santé et de la Recherche Médicale (INSERM), École nationale vétérinaire d'Alfort (ENVA), Centre National de la Recherche Scientifique (CNRS)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Association française contre les myopathies (AFM-Téléthon)-Sorbonne Université (SU), CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Institut National de la Santé et de la Recherche Médicale (INSERM)-Aix Marseille Université (AMU), and Centre de Recherche en Myologie

Subjects

0301 basic medicine, Male, lcsh:Diseases of the musculoskeletal system, Duchenne muscular dystrophy, [SDV]Life Sciences [q-bio], Canine, Dystrophin, 03 medical and health sciences, 0302 clinical medicine, Dogs, LRMD, DMD, medicine, Dog, X-linked muscular dystrophy, Animals, Orthopedics and Sports Medicine, Animal model, Disease-causing Mutation, Muscular dystrophy, Muscle, Skeletal, Molecular Biology, Gene, Genetics, Genes, Modifier, biology, Research, Inversion, Cell Biology, medicine.disease, Phenotype, 3. Good health, Muscular Dystrophy, Duchenne, [SDV] Life Sciences [q-bio], Disease Models, Animal, 030104 developmental biology, Mutation, biology.protein, Labrador Retriever, lcsh:RC925-935, Dp71, 030217 neurology & neurosurgery, Neuromuscular disorders

Abstract

Background Canine models of Duchenne muscular dystrophy (DMD) are a valuable tool to evaluate potential therapies because they faithfully reproduce the human disease. Several cases of dystrophinopathies have been described in canines, but the Golden Retriever muscular dystrophy (GRMD) model remains the most used in preclinical studies. Here, we report a new spontaneous dystrophinopathy in a Labrador Retriever strain, named Labrador Retriever muscular dystrophy (LRMD). Methods A colony of LRMD dogs was established from spontaneous cases. Fourteen LRMD dogs were followed-up and compared to the GRMD standard using several functional tests. The disease causing mutation was studied by several molecular techniques and identified using RNA-sequencing. Results The main clinical features of the GRMD disease were found in LRMD dogs; the functional tests provided data roughly overlapping with those measured in GRMD dogs, with similar inter-individual heterogeneity. The LRMD causal mutation was shown to be a 2.2-Mb inversion disrupting the DMD gene within intron 20 and involving the TMEM47 gene. In skeletal muscle, the Dp71 isoform was ectopically expressed, probably as a consequence of the mutation. We found no evidence of polymorphism in either of the two described modifier genes LTBP4 and Jagged1. No differences were found in Pitpna mRNA expression levels that would explain the inter-individual variability. Conclusions This study provides a full comparative description of a new spontaneous canine model of dystrophinopathy, found to be phenotypically equivalent to the GRMD model. We report a novel large DNA mutation within the DMD gene and provide evidence that LRMD is a relevant model to pinpoint additional DMD modifier genes.

Published

2020

41. The GENDULF Algorithm: Mining Transcriptomics to Uncover Modifier Genes for Monogenic Diseases

Author

Thomas O. Crawford, Charlotte J. Sumner, Hiren Karathia, Ivette Zelaya, Eytan Ruppin, Alejandro A. Schäffer, Daniel M. Ramos, and Noam Auslander

Subjects

Medicine (General), Genetic Linkage, Method, Disease, digenic inheritance, cystic fibrosis, Transcriptome, Exon, 0302 clinical medicine, Gene expression, Methods, Data Mining, Molecular Biology of Disease, Biology (General), spinal muscular atrophy, 0303 health sciences, Gene knockdown, Applied Mathematics, SMA, Computational Theory and Mathematics, General Agricultural and Biological Sciences, Algorithms, Information Systems, QH301-705.5, Genomics, Computational biology, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, R5-920, medicine, Humans, Gene, Genetic Association Studies, Loss function, 030304 developmental biology, modifier gene, Genes, Modifier, General Immunology and Microbiology, Mechanism (biology), Computational Biology, Reproducibility of Results, Spinal muscular atrophy, medicine.disease, HEK293 Cells, gene expression, Genetics, Gene Therapy & Genetic Disease, 030217 neurology & neurosurgery

Abstract

Modifier genes are believed to account for the clinical variability observed in many Mendelian disorders, but their identification remains challenging due to the limited availability of genomics data from large patient cohorts. Here, we present GENDULF (GENetic moDULators identiFication), one of the first methods to facilitate prediction of disease modifiers using healthy and diseased tissue gene expression data. GENDULF is designed for monogenic diseases in which the mechanism is loss of function leading to reduced expression of the mutated gene. When applied to cystic fibrosis, GENDULF successfully identifies multiple, previously established disease modifiers, including EHF, SLC6A14, and CLCA1. It is then utilized in spinal muscular atrophy (SMA) and predicts U2AF1 as a modifier whose low expression correlates with higher SMN2 pre‐mRNA exon 7 retention. Indeed, knockdown of U2AF1 in SMA patient‐derived cells leads to increased full‐length SMN2 transcript and SMN protein expression. Taking advantage of the increasing availability of transcriptomic data, GENDULF is a novel addition to existing strategies for prediction of genetic disease modifiers, providing insights into disease pathogenesis and uncovering novel therapeutic targets., GENDULF predicts modifiers of loss‐of‐function monogenetic diseases using healthy and disease gene expression data. Application to cystic fibrosis (CF) and spinal muscular atrophy (SMA) identifies established CF modifiers and a new putative modifier of SMA, U2AF1.

Published

2020

42. Genetic Modifiers of Fetal Haemoglobin in Sickle Cell Disease

Author

Stephan Menzel and Swee Lay Thein

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Anemia, Locus (genetics), Anemia, Sickle Cell, beta-Globins, Disease, Biology, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Gene cluster, Genetics, medicine, Humans, Gene, Fetal Hemoglobin, Gene Editing, Pharmacology, Genes, Modifier, General Medicine, medicine.disease, Molecular medicine, Human genetics, Genetic architecture, 030104 developmental biology, Multigene Family, 030220 oncology & carcinogenesis, Immunology, Molecular Medicine

Abstract

Fetal haemoglobin (HbF) levels have a clinically beneficial effect on sickle cell disease (SCD). Patients with SCD demonstrate extreme variability in HbF levels (1-30%), a large part of which is likely genetically determined. The main genetic modifier loci for HbF persistence, HBS1L-MYB, BCL11A and the β-globin gene cluster in adults also act in SCD patients. Their effects are, however, modified significantly by a disease pathology that includes a drastically shortened erythrocyte lifespan with an enhanced survival of those red blood cells that carry HbF (F cells). We propose a model of how HbF modifier genes and disease pathology interact to shape HbF levels measured in patients. We review current knowledge on the action of these loci in SCD, their genetic architecture, and their putative functional components. At each locus, one strong candidate for a causative, functional DNA change has been proposed: Xmn1-HBG2 at the β-globin cluster, rs1427407 at BCL11A and the 3 bp deletion rs66650371 at HBS1L-MYB. These, however, explain only part of the impact of these loci and additional variants are yet to be identified. Further progress in understanding the genetic control of HbF levels requires that confounding factors inherent in SCD, such as ethnic complexity, the role of F cells and the influence of drugs, are suitably addressed. This will depend on international collaboration and on large, well-characterised patient cohorts with genome-wide single-nucleotide polymorphism or sequence data.

Published

2018

43. Synergistic triad epistasis of epigenetic H3K27me modifier genes, EZH2, KDM6A, and KDM6B, in gastric cancer susceptibility

Author

Miyoung Kim, Changwon Kang, Seon-Woo Lee, and Do Youn Park

Subjects

Adult, Male, Jumonji Domain-Containing Histone Demethylases, Cancer Research, Methyltransferase, Single-nucleotide polymorphism, Methylation, Polymorphism, Single Nucleotide, Epigenesis, Genetic, Histones, 03 medical and health sciences, 0302 clinical medicine, Stomach Neoplasms, Genotype, Biomarkers, Tumor, Humans, Medicine, SNP, Enhancer of Zeste Homolog 2 Protein, Genetic Predisposition to Disease, Epigenetics, Aged, Retrospective Studies, Aged, 80 and over, Histone Demethylases, Genetics, Genes, Modifier, biology, business.industry, Gastroenterology, Nuclear Proteins, Cancer, Epistasis, Genetic, General Medicine, Middle Aged, Prognosis, medicine.disease, Gene Expression Regulation, Neoplastic, Oncology, Case-Control Studies, 030220 oncology & carcinogenesis, biology.protein, Epistasis, Demethylase, Female, 030211 gastroenterology & hepatology, business, Follow-Up Studies

Abstract

For an epigenetic regulation of human genome, three enzymes write or erase methylation of lysine-27 residue on histone H3 (H3K27me). This methylation is catalyzed by EZH2 (KMT6A) methyltransferase and reversed by KDM6A (UTX) or KDM6B (JMJD3) demethylase. Genetic cancer risk association has been reported on EZH2, but not on KDM6A or KDM6B yet. A total of 23 tag single-nucleotide polymorphisms (SNPs) of the three genes were genotyped in 2349 Korean participants, and their gastric cancer risk associations and epistases were statistically examined by comparing the SNP genotypes of 1100 gastric cancer patients and 1249 healthy controls. All three genes are individually associated with gastric cancer susceptibility, as evident with the genotypes of KDM6A SNP rs5952279 (P = 0.00010) and rs144974719 (P = 0.00024), KDM6B rs78633955 (P = 0.0019) and rs11657063 (P = 0.0036), and EZH2 rs67648693 (P = 0.0028) and rs1061037 (P = 0.023). Furthermore, when odds ratio of interaction (ORint) is calculated for all intergenic SNP pairs, synergistic epistasis is evident among the three genes. Specifically, the interaction is synergistic between EZH2 rs58579167 and KDM6A rs5952279 (ORint = 3.2, P = 0.00066), between KDM6A rs2230018 and KDM6B rs78633955 (ORint = 1.9, P = 0.044), and between KDM6B rs78633955 and EZH2 rs73158295 (ORint = 1.7, P = 0.00030). These inter-SNP interactions together constitute a synergistic triad epistasis of ring-type topology. All three H3K27me modifier genes are individually associated with gastric cancer susceptibility with synergistic triad interaction. Not only two enzymes with the same function (KDM6A and KDM6B), but also those with opposite functions (EZH2 versus KDM6A or KDM6B) synergistically affect H3K27me consequences such as gastric cancer susceptibility.

Published

2018

44. Mutations inPDLIM5are rare in dilated cardiomyopathy but are emerging as potential disease modifiers

Author

Kari Casas, Emma L. Robinson, Radek Szklarczyk, Ingrid P.C. Krapels, Gabriel Kringlen, Mohamed W. Mohamed, Kiely N. James, Godelieve R.F. Claes, Shareef Nahas, Jan F. C. Glatz, Els K. Vanhoutte, Michele M. Pasierb, Arthur van den Wijngaard, Stephane Heymans, Job Verdonschot, Han G. Brunner, Mark R. Hazebroek, RS: Carim - H02 Cardiomyopathy, Promovendi CD, Cardiologie, MUMC+: DA KG Lab Centraal Lab (9), MUMC+: DA KG Polikliniek (9), MUMC+: MA Med Staf Artsass Cardiologie (9), Moleculaire Genetica, MUMC+: MA Med Staf Spec Cardiologie (9), MUMC+: DA Klinische Genetica (5), Klinische Genetica, and RS: GROW - R4 - Reproductive and Perinatal Medicine

Subjects

Male, 0301 basic medicine, Muscle Proteins, Genome-wide association study, VARIANTS, 030105 genetics & heredity, medicine.disease_cause, Exon, Loss of Function Mutation, MYOZ2, Connectin, genetics, Genetics (clinical), Genetics & Heredity, Genetics, genetic modifier, Mutation, Microfilament Proteins, LIM Domain Proteins, Middle Aged, Penetrance, Phenotype, Pedigree, SEVERE FORM, LEADS, ENIGMA HOMOLOG, cardiovascular system, Female, Original Article, Life Sciences & Biomedicine, Adult, Cardiomyopathy, Dilated, lcsh:QH426-470, PROTEINS, Biology, 03 medical and health sciences, Exome Sequencing, medicine, Humans, Genetic Testing, GENOME-WIDE ASSOCIATION, Molecular Biology, Gene, Adaptor Proteins, Signal Transducing, Aged, Genes, Modifier, Science & Technology, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Myocardium, Original Articles, LDB3, dilated cardiomyopathy, lcsh:Genetics, 030104 developmental biology, sarcomere, Carrier Proteins

Abstract

Background A causal genetic mutation is found in 40% of families with dilated cardiomyopathy (DCM), leaving a large percentage of families genetically unsolved. This prevents adequate counseling and clear recommendations in these families. We aim to identify novel genes or modifiers associated with DCM. Methods We performed computational ranking of human genes based on coexpression with a predefined set of genes known to be associated with DCM, which allowed us to prioritize gene candidates for their likelihood of being involved in DCM. Top candidates will be checked for variants in the available whole‐exome sequencing data of 142 DCM patients. RNA was isolated from cardiac biopsies to investigate gene expression. Results PDLIM5 was classified as the top candidate. An interesting heterozygous variant (189_190delinsGG) was found in a DCM patient with a known pathogenic truncating TTN‐variant. The PDLIM5 loss‐of‐function (LoF) variant affected all cardiac‐specific isoforms of PDLIM5 and no LoF variants were detected in the same region in a control cohort of 26,000 individuals. RNA expression of PDLIM5 and its direct interactors (MYOT, LDB3, and MYOZ2) was increased in cardiac tissue of this patient, indicating a possible compensatory mechanism. The PDLIM5 variant cosegregated with the TTN‐variant and the phenotype, leading to a high disease penetrance in this family. A second patient was an infant with a homozygous 10 kb‐deletion of exon 2 in PDLIM5 resulting in early‐onset cardiac disease, showing the importance of PDLIM5 in cardiac function. Conclusions Heterozygous PDLIM5 variants are rare and therefore will not have a major contribution in DCM. Although they likely play a role in disease development as this gene plays a major role in contracting cardiomyocytes and homozygous variants lead to early‐onset cardiac disease. Other environmental and/or genetic factors are probably necessary to unveil the cardiac phenotype in PDLIM5 mutation carriers., A computational ranking‐based method performed in whole exome sequencing data of dilated cardiomyopathy patient put PDLIM5 forward as novel gene implicated in this cardiac disease.

Published

2019

45. Candidate modifier genes for immune function in 22q11.2 deletion syndrome

Author

Lucy E. DesJardin, John Robert Manak, Catherina T. Pinnaro, Travis S. Henry, Mrutyunjaya Parida, Heather J. Major, and Benjamin W. Darbro

Subjects

0301 basic medicine, TBX1, 22q11 Deletion Syndrome, lcsh:QH426-470, Retinoic acid, 030105 genetics & heredity, Biology, medicine.disease_cause, Immunophenotyping, 03 medical and health sciences, chemistry.chemical_compound, Immune system, immune dysregulation, retinoic acid, Genetics, medicine, Humans, Nuclear Receptor Co-Repressor 2, Lymphocytes, Molecular Biology, Genetics (clinical), Immunodeficiency, Exome sequencing, Phenocopy, Genes, Modifier, Genetic heterogeneity, Original Articles, genetic modifiers, Immune dysregulation, medicine.disease, 3. Good health, lcsh:Genetics, Phenotype, 030104 developmental biology, chemistry, 22q11.2 deletion syndrome, Immunology, Original Article, E1A-Associated p300 Protein

Abstract

Background The 22q11.2 deletion syndrome (22q11.2DS) is the most common contiguous microdeletion affecting humans and exhibits extreme phenotypic heterogeneity. Patients can manifest any combination of comorbidities including congenital heart disease, hypoparathyroidism, cleft palate, kidney abnormalities, neurodevelopmental disorders, and immune dysfunction. Immunodeficiency is present in the majority of patients with 22q11.2DS and is the second leading cause of death in these patients. Knowing the genetic determinants of immune dysfunction will aid in prognostication and potentially novel treatments. Methods We performed exome sequencing and gene‐based variant association analysis on 31 deeply phenotyped individuals with the canonical 3Mb 22q11.2 deletion to identify what genes outside the 22q11.2 locus may be modifying the immune dysregulated phenotype. Immunophenotyping was performed using preexisting medical data and a novel scoring system developed from numerous clinical laboratory values including immunoglobulin levels, lymphocyte transformation to antigens (LTA), lymphocyte transformation to mitogens (LTM), and peripheral blood flow cytometry. Immunophenotypic scoring was validated against newborn screening T‐cell receptor excision circle (TREC) results. Results Rare DNA variants in transcriptional regulators involved in retinoic acid signaling (NCOR2, OMIM *600848 and EP300, OMIM *602700) were found to be associated with immunophenotype. Conclusion The expression of TBX1, which seems to confer the major phenotypic features of 22q11.2DS, is regulated via retinoic acid signaling, and alterations in retinoic acid signaling during embryonic development can lead to phenocopies of 22q11.2DS. These observations support the hypothesis that genetic modifiers outside the microdeletion locus may influence the immune function in 22q11.2DS patients., We performed deep phenotyping for immune status on 31 individuals with the canonical 3Mb 22q11.2 deletion followed by whole exome sequencing. DNA variants in transcriptional regulators involved in retinoic acid signaling (NCOR2, EP300) were found to be associated with immune status.

Published

2019

46. Association of modifiers and other genetic factors explain Marfan syndrome clinical variability

Author

Catherine Boileau, Anne Boland, Guillaume Jondeau, Mélodie Aubart, Jean-François Deleuze, Olivier Milleron, M. S. Gross, Steven Gazal, Nadine Hanna, Louise Benarroch, Marie-Paule Jacob, Emmanuelle Génin, Chantal Stheneur, Julien Buratti, Vincent Meyer, Thomas Bourgeron, Pauline Arnaud, Laurent Gouya, Isabelle Desguerre, Habib Zouali, Laboratoire de Recherche Vasculaire Translationnelle (LVTS (UMR_S_1148 / U1148)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité)-Université Sorbonne Paris Nord, AP-HP - Hôpital Bichat - Claude Bernard [Paris], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), CHU Necker - Enfants Malades [AP-HP], Infection, Anti-microbiens, Modélisation, Evolution (IAME (UMR_S_1137 / U1137)), Génétique humaine et fonctions cognitives - Human Genetics and Cognitive Functions (GHFC (UMR_3571 / U-Pasteur_1)), Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Gènes, Synapses et Cognition (CNRS - UMR3571 ), Institut de Génomique d'Evry (IG), Université Paris-Saclay-Institut de Biologie François JACOB (JACOB), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Centre d'Etude du Polymorphisme Humain (CEPH), Institut Universitaire d'Hématologie (IUH), Université Paris Diderot - Paris 7 (UPD7)-Université Paris Diderot - Paris 7 (UPD7)-Fondation Jean Dausset-Université Paris Cité (UPCité), Université Paris Descartes - Paris 5 (UPD5), Centre de recherche sur l'Inflammation (CRI (UMR_S_1149 / ERL_8252 / U1149)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Génétique, génomique fonctionnelle et biotechnologies (UMR 1078) (GGB), EFS-Université de Brest (UBO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Brestois Santé Agro Matière (IBSAM), Université de Brest (UBO), Centre Hospitalier Régional Universitaire de Brest (CHRU Brest), and Benarroch, Louise

Subjects

Adult, Collagen Type IV, Male, 0301 basic medicine, Marfan syndrome, Multifactorial Inheritance, Adolescent, Genetic Linkage, Fibrillin-1, [SDV]Life Sciences [q-bio], Quantitative Trait Loci, 030204 cardiovascular system & hematology, Biology, Thoracic aortic aneurysm, Article, Marfan Syndrome, 03 medical and health sciences, 0302 clinical medicine, Genetic linkage, Genotype, Genetics, medicine, Humans, Cells, Cultured, Genetics (clinical), Exome sequencing, Aged, Genes, Modifier, Fibroblasts, Middle Aged, medicine.disease, Genetic architecture, [SDV] Life Sciences [q-bio], Phenotype, 030104 developmental biology, Mutation, Expression quantitative trait loci, Female, Age of onset

Abstract

International audience; Marfan syndrome (MFS) is a rare autosomal dominant connective tissue disorder related to variants in the FBN1 gene. Prognosis is related to aortic risk of dissection following aneurysm. MFS clinical variability is notable, for age of onset as well as severity and number of clinical manifestations. To identify genetic modifiers, we combined genome-wide approaches in 1070 clinically well-characterized FBN1 disease-causing variant carriers: (1) an FBN1 eQTL analysis in 80 fibroblasts of FBN1 stop variant carriers, (2) a linkage analysis, (3) a kinship matrix association study in 14 clinically concordant and discordant sib-pairs, (4) a genome-wide association study and (5) a whole exome sequencing in 98 extreme phenotype samples.Three genetic mechanisms of variability were found. A new genotype/phenotype correlation with an excess of loss-of-cysteine variants (P = 0.004) in severely affected subjects. A second pathogenic event in another thoracic aortic aneurysm gene or the COL4A1 gene (known to be involved in cerebral aneurysm) was found in nine individuals. A polygenic model involving at least nine modifier loci (named gMod-M1-9) was observed through cross-mapping of results. Notably, gMod-M2 which co-localizes with PRKG1, in which activating variants have already been described in thoracic aortic aneurysm, and gMod-M3 co-localized with a metalloprotease (proteins of extra-cellular matrix regulation) cluster. Our results represent a major advance in understanding the complex genetic architecture of MFS and provide the first steps toward prediction of clinical evolution.

Published

2018

47. Collective interaction effects associated with mammalian behavioral traits reveal genetic factors connecting fear and hemostasis

Author

Hyung Jun Woo and Jaques Reifman

Subjects

Male, 0301 basic medicine, Multifactorial Inheritance, Heart Diseases, lcsh:RC435-571, Genetics, Behavioral, Disease, Quantitative trait locus, Anxiety, Quantitative trait, Extinction, Psychological, Stress Disorders, Post-Traumatic, Mice, 03 medical and health sciences, Dogs, lcsh:Psychiatry, Neural Pathways, medicine, Animals, Humans, Genetic Association Studies, Prepulse inhibition, Serotonin transporter, Behavioural genetics, Hemostasis, Genes, Modifier, Behavior, Animal, biology, Post-traumatic stress disorder, Thrombin, Fear, Extinction (psychology), medicine.disease, Comorbidity, Psychiatry and Mental health, 030104 developmental biology, biology.protein, Epistasis, Behavioral genetics, medicine.symptom, Neuroscience, Algorithms, Signal Transduction

Abstract

Background Investigation of the genetic architectures that influence the behavioral traits of animals can provide important insights into human neuropsychiatric phenotypes. These traits, however, are often highly polygenic, with individual loci contributing only small effects to the overall association. The polygenicity makes it challenging to explain, for example, the widely observed comorbidity between stress and cardiac disease. Methods We present an algorithm for inferring the collective association of a large number of interacting gene variants with a quantitative trait. Using simulated data, we demonstrate that by taking into account the non-uniform distribution of genotypes within a cohort, we can achieve greater power than regression-based methods for high-dimensional inference. Results We analyzed genome-wide data sets of outbred mice and pet dogs, and found neurobiological pathways whose associations with behavioral traits arose primarily from interaction effects: γ-carboxylated coagulation factors and downstream neuronal signaling were highly associated with conditioned fear, consistent with our previous finding in human post-traumatic stress disorder (PTSD) data. Prepulse inhibition in mice was associated with serotonin transporter and platelet homeostasis, and noise-induced fear in dogs with hemostasis. Conclusions Our findings suggest a novel explanation for the observed comorbidity between PTSD/anxiety and cardiovascular diseases: key coagulation factors modulating hemostasis also regulate synaptic plasticity affecting the learning and extinction of fear.

Published

2018

48. A Strategy To Isolate Modifiers of Caenorhabditis elegans Lethal Mutations: Investigating the Endoderm Specifying Ability of the Intestinal Differentiation GATA Factor ELT-2

Author

James D. McGhee, Vinci Au, Tobias Wiesenfahrt, Craig J. Marshall, Dylan M. Parker, Paul E Mains, Erica Li-Leger, Frances Snider, Don Moerman, Stephane Flibotte, Erin Osborne Nishimura, and Jingjie Duanmu

Subjects

0301 basic medicine, Embryo, Nonmammalian, Genotype, Zygote, Transgene, Mutant, QH426-470, GATA Transcription Factors, 03 medical and health sciences, C . elegans, Extrachromosomal DNA, medicine, Genetics, Animals, Amino Acid Sequence, Genetic Testing, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Molecular Biology, Gene, intestine, Genetics (clinical), tasp-1, Genes, Modifier, pqn-82, Whole Genome Sequencing, biology, Endoderm, Mutant Screen Report, Reproducibility of Results, Cell Differentiation, Extrachromosomal array, biology.organism_classification, Survival Analysis, ELT-2 GATA factor, Cell biology, Intestines, 030104 developmental biology, medicine.anatomical_structure, endoderm specification, taspase, Mutation, C. elegans, Genetic screen

Abstract

The ELT-2 GATA factor normally functions in differentiation of the C. elegans endoderm, downstream of endoderm specification. We have previously shown that, if ELT-2 is expressed sufficiently early, it is also able to specify the endoderm and to replace all other members of the core GATA-factor transcriptional cascade (END-1, END-3, ELT-7). However, such rescue requires multiple copies (and presumably overexpression) of the end-1p::elt-2 cDNA transgene; a single copy of the transgene does not rescue. We have made this observation the basis of a genetic screen to search for genetic modifiers that allow a single copy of the end-1p::elt-2 cDNA transgene to rescue the lethality of the end-1 end-3 double mutant. We performed this screen on a strain that has a single copy insertion of the transgene in an end-1 end-3 background. These animals are kept alive by virtue of an extrachromosomal array containing multiple copies of the rescuing transgene; the extrachromosomal array also contains a toxin under heat shock control to counterselect for mutagenized survivors that have been able to lose the rescuing array. A screen of ∼14,000 mutagenized haploid genomes produced 17 independent surviving strains. Whole genome sequencing was performed to identify genes that incurred independent mutations in more than one surviving strain. The C. elegans gene tasp-1 was mutated in four independent strains. tasp-1 encodes the C. elegans homolog of Taspase, a threonine-aspartic acid protease that has been found, in both mammals and insects, to cleave several proteins involved in transcription, in particular MLL1/trithorax and TFIIA. A second gene, pqn-82, was mutated in two independent strains and encodes a glutamine-asparagine rich protein. tasp-1 and pqn-82 were verified as loss-of-function modifiers of the end-1p::elt-2 transgene by RNAi and by CRISPR/Cas9-induced mutations. In both cases, gene loss leads to modest increases in the level of ELT-2 protein in the early endoderm although ELT-2 levels do not strictly correlate with rescue. We suggest that tasp-1 and pqn-82 represent a class of genes acting in the early embryo to modulate levels of critical transcription factors or to modulate the responsiveness of critical target genes. The screen’s design, rescuing lethality with an extrachromosomal transgene followed by counterselection, has a background survival rate of

Published

2018

49. Genome-wide search for higher order epistasis as modifiers of treatment effects on bone mineral density in childhood cancer survivors

Author

Cindy Im, Melissa M. Hudson, Wonjong Moon, Leslie L. Robison, Sue C. Kaste, Kirsten K. Ness, Carmen L. Wilson, Yutaka Yasui, Wassim Chemaitilly, Russell J. Brooke, and Yadav Sapkota

Subjects

Adult, Male, 0301 basic medicine, Adolescent, Antineoplastic Agents, Single-nucleotide polymorphism, 030105 genetics & heredity, Biology, Polymorphism, Single Nucleotide, Genome, Article, 03 medical and health sciences, Bone Density, Genetics, medicine, Humans, SNP, Enhancer, Gene, Genetics (clinical), Genes, Modifier, Cancer, Epistasis, Genetic, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Pediatric cancer, 030104 developmental biology, Epistasis, Female

Abstract

Single-nucleotide polymorphisms (SNPs) contributing to interactions between regulatory elements that modulate gene transcription may explain some of the uncharacterized variation for complex traits. We explored this hypothesis among 856 adult survivors of pediatric cancer exposed to curative treatments that adversely affect bone mineral density (BMD). To restrict our search to interactions among SNPs in regulatory elements, our analysis considered 75523 SNPs mapped to putative promoter or enhancer regions. In anticipation that power to detect higher order epistasis would be low using an exhaustive search and a Bonferroni-corrected threshold for genome-wide significance (e.g., P

Published

2018

50. Histone modifier gene mutations in peripheral T-cell lymphoma not otherwise specified

Author

Wei-Li Zhao, Feng Liu, Li Wang, Anne Janin, Zhao-Fu Wang, Di Fu, Meng-Meng Ji, Christophe Leboeuf, Yi-Ming Lu, Han Liu, Jing Ye, Shu Cheng, Yao-Hui Huang, and Jinyan Huang

Subjects

0301 basic medicine, medicine.drug_class, Non-Hodgkin Lymphoma, DNA Mutational Analysis, Peripheral T-cell lymphoma not otherwise specified, Decitabine, Aminopyridines, Apoptosis, Methylation, Article, Histones, 03 medical and health sciences, chemistry.chemical_compound, Mice, Chidamide, Cell Line, Tumor, Histone methylation, medicine, Tumor Cells, Cultured, Animals, Humans, Epigenetics, Genes, Modifier, biology, Histone deacetylase inhibitor, Lymphoma, T-Cell, Peripheral, Acetylation, Hematology, medicine.disease, Prognosis, Survival Analysis, Neoplasm Proteins, DNA-Binding Proteins, 030104 developmental biology, Histone, chemistry, Hypomethylating agent, Benzamides, Mutation, biology.protein, Cancer research, Heterografts, medicine.drug

Abstract

Due to heterogeneous morphological and immunophenotypic features, approximately 50% of peripheral T-cell lymphomas are unclassifiable and categorized as peripheral T-cell lymphomas, not otherwise specified. These conditions have an aggressive course and poor clinical outcome. Identification of actionable biomarkers is urgently needed to develop better therapeutic strategies. Epigenetic alterations play a crucial role in tumor progression. Histone modifications, particularly methylation and acetylation, are generally involved in chromatin state regulation. Here we screened the core set of genes related to histone methylation (KMT2D, SETD2, KMT2A, KDM6A) and acetylation (EP300, CREBBP) and identified 59 somatic mutations in 45 of 125 (36.0%) patients with peripheral T-cell lymphomas, not otherwise specified. Histone modifier gene mutations were associated with inferior progression-free survival time of the patients, irrespective of chemotherapy regimens, but an increased response to the histone deacetylase inhibitor chidamide. In vitro, chidamide significantly inhibited the growth of EP300-mutated T-lymphoma cells and KMT2D-mutated T-lymphoma cells when combined with the hypomethylating agent decitabine. Mechanistically, decitabine acted synergistically with chidamide to enhance the interaction of KMT2D with transcription factor PU.1, regulated H3K4me-associated signaling pathways, and sensitized T-lymphoma cells to chidamide. In a xenograft KMT2D-mutated T-lymphoma model, dual treatment with chidamide and decitabine significantly retarded tumor growth and induced cell apoptosis through modulation of the KMT2D/H3K4me axis. Our work thus contributes to the understanding of aberrant histone modification in peripheral T-cell lymphomas, not otherwise specified and the stratification of a biological subset that can benefit from epigenetic treatment.

Published

2018