Your search keyword '"Tracy Heung"' showing total 31 results

1. Polygenic risk for triglyceride levels in the presence of a high impact rare variant

Author

Shengjie Ying, Tracy Heung, Bhooma Thiruvahindrapuram, Worrawat Engchuan, Yue Yin, Christina Blagojevic, Zhaolei Zhang, Robert A. Hegele, Ryan K. C. Yuen, and Anne S. Bassett

Subjects

Triglyceride, Lipid, Polygenic risk score, 22q11.2 microdeletion, Genome sequencing, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Elevated triglyceride (TG) levels are a heritable and modifiable risk factor for cardiovascular disease and have well-established associations with common genetic variation captured in a polygenic risk score (PRS). In young adulthood, the 22q11.2 microdeletion conveys a 2-fold increased risk for mild-moderate hypertriglyceridemia. This study aimed to assess the role of the TG-PRS in individuals with this elevated baseline risk for mild-moderate hypertriglyceridemia. Methods We studied a deeply phenotyped cohort of adults (n = 157, median age 34 years) with a 22q11.2 microdeletion and available genome sequencing, lipid level, and other clinical data. The association between a previously developed TG-PRS and TG levels was assessed using a multivariable regression model adjusting for effects of sex, BMI, and other covariates. We also constructed receiver operating characteristic (ROC) curves using logistic regression models to assess the ability of TG-PRS and significant clinical variables to predict mild-moderate hypertriglyceridemia status. Results The TG-PRS was a significant predictor of TG-levels (p = 1.52E-04), along with male sex and BMI, in a multivariable model (pmodel = 7.26E-05). The effect of TG-PRS appeared to be slightly stronger in individuals with obesity (BMI ≥ 30) (beta = 0.4617) than without (beta = 0.1778), in a model unadjusted for other covariates (p-interaction = 0.045). Among ROC curves constructed, the inclusion of TG-PRS, sex, and BMI as predictor variables produced the greatest area under the curve (0.749) for classifying those with mild-moderate hypertriglyceridemia, achieving an optimal sensitivity and specificity of 0.746 and 0.707, respectively. Conclusions These results demonstrate that in addition to significant effects of sex and BMI, genome-wide common variation captured in a PRS also contributes to the variable expression of the 22q11.2 microdeletion with respect to elevated TG levels.

Published

2023

2. Correction: Polygenic risk for triglyceride levels in the presence of a high impact rare variant

Author

Shengjie Ying, Tracy Heung, Bhooma Thiruvahindrapuram, Worrawat Engchuan, Yue Yin, Christina Blagojevic, Zhaolei Zhang, Robert A. Hegele, Ryan K. C. Yuen, and Anne S. Bassett

Subjects

Internal medicine, RC31-1245, Genetics, QH426-470

Published

2023

3. Genome sequencing broadens the range of contributing variants with clinical implications in schizophrenia

Author

Bahareh A. Mojarad, Yue Yin, Roozbeh Manshaei, Ian Backstrom, Gregory Costain, Tracy Heung, Daniele Merico, Christian R. Marshall, Anne S. Bassett, and Ryan K. C. Yuen

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract The range of genetic variation with potential clinical implications in schizophrenia, beyond rare copy number variants (CNVs), remains uncertain. We therefore analyzed genome sequencing data for 259 unrelated adults with schizophrenia from a well-characterized community-based cohort previously examined with chromosomal microarray for CNVs (none with 22q11.2 deletions). We analyzed these genomes for rare high-impact variants considered causal for neurodevelopmental disorders, including single-nucleotide variants (SNVs) and small insertions/deletions (indels), for potential clinical relevance based on findings for neurodevelopmental disorders. Also, we investigated a novel variant type, tandem repeat expansions (TREs), in 45 loci known to be associated with monogenic neurological diseases. We found several of these variants in this schizophrenia population suggesting that these variants have a wider clinical spectrum than previously thought. In addition to known pathogenic CNVs, we identified 11 (4.3%) individuals with clinically relevant SNVs/indels in genes converging on schizophrenia-relevant pathways. Clinical yield was significantly enriched in females and in those with broadly defined learning/intellectual disabilities. Genome analyses also identified variants with potential clinical implications, including TREs (one in DMPK; two in ATXN8OS) and ultra-rare loss-of-function SNVs in ZMYM2 (a novel candidate gene for schizophrenia). Of the 233 individuals with no pathogenic CNVs, we identified rare high-impact variants (i.e., clinically relevant or with potential clinical implications) for 14 individuals (6.0%); some had multiple rare high-impact variants. Mean schizophrenia polygenic risk score was similar between individuals with and without clinically relevant rare genetic variation; common variants were not sufficient for clinical application. These findings broaden the individual and global picture of clinically relevant genetic risk in schizophrenia, and suggest the potential translational value of genome sequencing as a single genetic technology for schizophrenia.

Published

2021

4. Schizophrenia Risk Mediated by microRNA Target Genes Overlapped by Genome-Wide Rare Copy Number Variation in 22q11.2 Deletion Syndrome

Author

Shengjie Ying, Tracy Heung, Zhaolei Zhang, Ryan K. C. Yuen, and Anne S. Bassett

Subjects

schizophrenia, pathway enrichment analysis, neurodevelopmental disorders, DiGeorge syndrome, model system, DGCR8, Genetics, QH426-470

Abstract

The 22q11.2 deletion is associated with >20-fold increased risk for schizophrenia. The presence of gene DGCR8 in the 22q11.2 deletion region has suggested microRNA (miRNA) dysregulation as possibly contributing to this risk. We therefore investigated the role of miRNA target genes in the context of previously identified genome-wide risk for schizophrenia conveyed by additional copy number variation (CNV) in 22q11.2 deletion syndrome (22q11.2DS). Using a cohort of individuals with 22q11.2DS and documented additional rare CNVs overlapping protein coding genes, we compared those with schizophrenia (n = 100) to those with no psychotic illness (n = 118), assessing for rare CNVs that overlapped experimentally supported miRNA target genes. We further characterized the contributing miRNA target genes using gene set enrichment analyses and identified the miRNAs most implicated. Consistent with our hypothesis, we found a significantly higher proportion of individuals in the schizophrenia than in the non-psychotic group to have an additional rare CNV that overlapped one or more miRNA target genes (odds ratio = 2.12, p = 0.0138). Gene set analyses identified an enrichment of FMRP targets and genes involved in nervous system development and postsynaptic density amongst these miRNA target genes in the schizophrenia group. The miRNAs most implicated included miR-17-5p, miR-34a-5p and miR-124-3p. These results provide initial correlational evidence in support of a possible role for miRNA perturbation involving genes affected by rare genome-wide CNVs in the elevated risk for schizophrenia in 22q11.2DS, consistent with the multi-hit and multi-layered genetic mechanisms implicated in this and other forms of schizophrenia.

Published

2022

5. Incidence of infective endocarditis in adults with congenital heart disease and diagnosed 22q11.2 deletion syndrome

Author

Adonis Ng, Tracy Heung, Erwin Oechslin, Jessica Patzer, and Anne Bassett

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Published

2021

6. Abnormal spirometry in adults with 22q11.2 microdeletion and congenital heart disease

Author

Christina Blagojevic, Tracy Heung, Spencer van Mil, Erwin Oechslin, Candice K. Silversides, John T. Granton, and Anne S. Bassett

Subjects

DiGeorge syndrome, Lung, Adult congenital heart disease, Asthma, Genetics, Scoliosis, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background: In adults with congenital heart disease (CHD), pulmonary dysfunction is prevalent and associated with poor outcomes; however, underlying genetic contributors remain unexamined. We investigated whether the 22q11.2 microdeletion, an important genetic cause of CHD, was associated with abnormal spirometry in adults with CHD. Methods: We conducted a retrospective case-control study of 207 adults with CHD (predominantly tetralogy of Fallot), and spirometry data available from cardiopulmonary exercise testing, matching 58 with a confirmed 22q11.2 microdeletion to 149 controls on age (median 26.4, 28.2 years, respectively), sex, ethnicity, and CHD severity (37.9%, 29.5% complex, respectively). We examined forced vital capacity (FVC), forced expiratory volume in 1 s (FEV1), their % predicted values, and FEV1/FVC ratio. Results: All respiratory parameters assessed were significantly worse in those with 22q11.2 deletion syndrome (22q11.2DS-CHD) as compared to CHD-controls. Linear regression models indicated that the 22q11.2 microdeletion was associated with worse spirometry values even when accounting for complex CHD (FVC% predicted, p

Published

2021

7. 22q11.2 microdeletion and increased risk for type 2 diabetes

Author

Lily Van, Tracy Heung, Sarah L. Malecki, Christian Fenn, Andrea Tyrer, Marcos Sanches, Eva W.C. Chow, Erik Boot, Maria Corral, Satya Dash, Susan R. George, and Anne S. Bassett

Subjects

Diabetes, Genetics, Risk, Structural variant, Molecular diagnostics, Early diagnosis, Medicine (General), R5-920

Abstract

Background: The 22q11.2 microdeletion is the pathogenic copy number variation (CNV) associated with 22q11.2 deletion syndrome (22q11.2DS, formerly known as DiGeorge syndrome). Familiar endocrinological manifestations include hypoparathyroidism and hypothyroidism, with recent elucidation of elevated risk for obesity in adults. In this study, we aimed to determine whether adults with 22q11.2DS have an increased risk of developing type 2 diabetes (T2D). Methods: We studied the effect of the 22q11.2 microdeletion on risk for T2D, defined by history and glycosylated hemoglobin (HbA1c), using weighted survey data from the adult Canadian population (based on n = 11,874) and from a clinical cohort of adults with 22q11.2DS (n = 314), aged 17–69 years. Binomial logistic regression models accounted for age, sex, non-European ethnicity, family history of T2D, obesity, and antipsychotic medication use. Findings: The 22q11.2 microdeletion was a significant independent risk factor for T2D (OR 2·44, 95% CI 1·39–4·31), accounting for other factors (p < 0·0001). All factors except sex were also significant within 22q11.2DS. The median age at diagnosis of T2D was significantly younger in 22q11.2DS than in the Canadian population sample (32 vs 50 years, p

Published

2020

8. Genes and Pathways Implicated in Tetralogy of Fallot Revealed by Ultra-Rare Variant Burden Analysis in 231 Genome Sequences

Author

Roozbeh Manshaei, Daniele Merico, Miriam S. Reuter, Worrawat Engchuan, Bahareh A. Mojarad, Rajiv Chaturvedi, Tracy Heung, Giovanna Pellecchia, Mehdi Zarrei, Thomas Nalpathamkalam, Reem Khan, John B. A. Okello, Eriskay Liston, Meredith Curtis, Ryan K. C. Yuen, Christian R. Marshall, Rebekah K. Jobling, Erwin Oechslin, Rachel M. Wald, Candice K. Silversides, Stephen W. Scherer, Raymond H. Kim, and Anne S. Bassett

Subjects

tetralogy of fallot, heart disease, whole genome sequencing, NOTCH1, FLT4, rare variants, Genetics, QH426-470

Abstract

Recent genome-wide studies of rare genetic variants have begun to implicate novel mechanisms for tetralogy of Fallot (TOF), a severe congenital heart defect (CHD). To provide statistical support for case-only data without parental genomes, we re-analyzed genome sequences of 231 individuals with TOF (n = 175) or related CHD. We adapted a burden test originally developed for de novo variants to assess ultra-rare variant burden in individual genes, and in gene-sets corresponding to functional pathways and mouse phenotypes, accounting for highly correlated gene-sets and for multiple testing. For truncating variants, the gene burden test confirmed significant burden in FLT4 (Bonferroni corrected p-value < 0.01). For missense variants, burden in NOTCH1 achieved genome-wide significance only when restricted to constrained genes (i.e., under negative selection, Bonferroni corrected p-value = 0.004), and showed enrichment for variants affecting the extracellular domain, especially those disrupting cysteine residues forming disulfide bonds (OR = 39.8 vs. gnomAD). Individuals with NOTCH1 ultra-rare missense variants, all with TOF, were enriched for positive family history of CHD. Other genes not previously implicated in CHD had more modest statistical support in gene burden tests. Gene-set burden tests for truncating variants identified a cluster of pathways corresponding to VEGF signaling (FDR = 0%), and of mouse phenotypes corresponding to abnormal vasculature (FDR = 0.8%); these suggested additional candidate genes not previously identified (e.g., WNT5A and ZFAND5). Results for the most promising genes were driven by the TOF subset of the cohort. The findings support the importance of ultra-rare variants disrupting genes involved in VEGF and NOTCH signaling in the genetic architecture of TOF, accounting for 11–14% of individuals in the TOF cohort. These proof-of-principle data indicate that this statistical methodology could assist in analyzing case-only sequencing data in which ultra-rare variants, whether de novo or inherited, contribute to the genetic etiopathogenesis of a complex disorder.

Published

2020

9. Adult-onset obstructive sleep apnea and pediatric pharyngoplasty in 22q11.2 deletion syndrome

Author

Sabrina Cancelliere, Tracy Heung, Simone Fischbach, Paula Klaiman, and Anne S. Bassett

Subjects

General Medicine

Published

2023

10. Sexual knowledge and behaviour in 22q11.2 deletion syndrome, a complex care condition

Author

Maria Corral, Erik Boot, Stephanie G Brooks, Anne S. Bassett, Tracy Heung, Lisa D. Palmer, Psychiatry 1, and RS: MHeNs - R2 - Mental Health

Subjects

Adult, 030506 rehabilitation, medicine.medical_specialty, INTELLECTUAL DISABILITY, Genetic counseling, Sexual Behavior, Human sexuality, Education, 03 medical and health sciences, PEOPLE, Intellectual disability, SCHIZOPHRENIA, ADOLESCENTS, Developmental and Educational Psychology, medicine, DiGeorge Syndrome, gender, Humans, learning disabilities, sex, 0501 psychology and cognitive sciences, Deletion syndrome, genetics, sexually transmitted infections, Preventive healthcare, Reproductive health, Pregnancy, OUTCOMES, BARRIERS, business.industry, 05 social sciences, WOMEN, ADULTS, medicine.disease, PREVALENCE, INDIVIDUALS, Learning disability, pregnancy, medicine.symptom, 0305 other medical science, business, Psychology, Sexuality, 050104 developmental & child psychology, Clinical psychology

Abstract

BACKGROUND There is limited information about sexual knowledge and behaviours in adults with complex care needs, including those with 22q11.2 deletion syndrome (22q) which represents a group predisposed to intellectual disabilities. METHODS We conducted sexual health assessments with 67 adults with 22q, examining whether those with knowledge deficits and a history of engaging in sexual activities with others would be more likely to engage in high-risk behaviours. RESULTS The majority (65.7%) of adults with 22q were sexually active with others; most (70.1%) had sexual knowledge deficits. Those with intellectual disabilities were more likely (p = .0012) to have deficits in certain topics. In the sexually active subgroup, most (81.8%) engaged in high-risk sexual behaviours, regardless of intellectual disability or knowledge deficits. CONCLUSION The results suggest a need for increased dialogue, repeated education, genetic counselling and preventive healthcare measures related to sexuality in 22q and potentially in other complex care conditions.

Published

2022

11. Hypertriglyceridemia in young adults with a 22q11.2 microdeletion

Author

Christina Blagojevic, Tracy Heung, Sarah Malecki, Shengjie Ying, Sabrina Cancelliere, Robert A Hegele, and Anne S Bassett

Subjects

Adult, Cohort Studies, Hypertriglyceridemia, Male, Young Adult, Endocrinology, Risk Factors, Endocrinology, Diabetes and Metabolism, Diabetes Mellitus, Humans, Obesity, General Medicine

Abstract

Objective Mild to moderate hypertriglyceridemia is a condition often associated with obesity and diabetes, with as yet incomplete knowledge of underlying genetic architecture. The 22q11.2 microdeletion is associated with multimorbidity, including increased risk of obesity and diabetes. In this study, we sought to investigate whether the 22q11.2 microdeletion was associated with mild to moderate hypertriglyceridemia (1.7–10 mmol/L). Design This was a cohort study comparing 6793 population-based adults and 267 with a 22q11.2 microdeletion aged 17–69 years, excluding those with diabetes or on statins. Methods We used binomial logistic regression modeling to identify predictors of hypertriglyceridemia, accounting for the 22q11.2 microdeletion, male sex, BMI, ethnicity, age, and antipsychotic medications. Results The 22q11.2 microdeletion was a significant independent predictor of mild to moderate hypertriglyceridemia (odds ratio (OR): 2.35, 95% CI: 1.70–3.26). All other factors examined were also significant predictors (OR: 1.23–2.10), except for antipsychotic medication use. Within the 22q11.2 microdeletion subgroup, only male sex (OR: 3.10, 95% CI: 1.77–5.44) and BMI (OR: 1.63, 95% CI: 1.14–1.98) were significant predictors of hypertriglyceridemia, evident at mean age 31.2 years. Conclusions The 22q11.2 microdeletion is associated with hypertriglyceridemia even when accounting for other known risk factors for elevated triglycerides. This effect is seen in young adulthood (76.6% were

Published

2022

12. Adult Height, 22q11.2 Deletion Extent, and Short Stature in 22q11.2 Deletion Syndrome

Author

Tracy Heung, Brigid Conroy, Sarah Malecki, Joanne Ha, Erik Boot, Maria Corral, and Anne S. Bassett

Subjects

Adult, Heart Defects, Congenital, Intellectual Disability, Genetics, DiGeorge Syndrome, Gene Dosage, Humans, copy number variation, DiGeorge syndrome, velocardiofacial syndrome, adult phenotype, quantitative trait, Dwarfism, Child, Genetics (clinical)

Abstract

The 22q11.2 deletion syndrome (22q11.2DS) manifests as a wide range of medical conditions across a number of systems. Pediatric growth deficiency with some catch-up growth is reported, but there are few studies of final adult height. We aimed to investigate how final adult height in 22q11.2DS compared with general population norms, and to examine predictors of short stature in in a cohort of 397 adults with 22q11.2DS (aged 17.6–76.3 years) with confirmed typical 22q11.2 microdeletion (overlapping the LCR22A to LCR22B region). We defined short stature as

Published

2022

13. Influence of Parent-of-Origin on Intellectual Outcomes in the Chromosome 22q11.2 Deletion Syndrome

Author

Daniel E. McGinn, T. Blaine Crowley, Tracy Heung, Oanh Tran, Edward Moss, Elaine H. Zackai, Beverly S. Emanuel, Eva W. C. Chow, Bernice E. Morrow, Ann Swillen, Anne S. Bassett, and Donna M. McDonald-McGinn

Subjects

Genetics & Heredity, intellect, de novo, Science & Technology, familial, CHILDREN, 22q, FSIQ, Chromosomes, chromosome, deletion, DiGeorge, parent-of-origin, Intellectual Disability, PSYCHOSOCIAL ADJUSTMENT, DiGeorge Syndrome, Genetics, Humans, Chromosome Deletion, Life Sciences & Biomedicine, Genetics (clinical)

Abstract

Learning and intellectual disabilities are hallmark features of 22q11.2 deletion syndrome. Data are limited, however, regarding influences on full-scale IQ (FSIQ). Here, we investigated possible 22q11.2 deletion parent-of-origin effects. In 535 individuals, we compared FSIQ (≥50), 481 with de novo and 54 with inherited 22q11.2 deletions. In the subsets with data available, we examined parent-of-origin effects on FSIQ. We used linear regression models to account for covariates. Median FSIQ was significantly higher in de novo vs. inherited deletions (77; range 50−116 vs. 67; range 50−96, p < 0.0001). Results remained significant using a regression model accounting for age at IQ testing, sex and cohort site. No significant parent-of-origin differences in FSIQ were observed for de novo deletions (n = 81, 63.0% maternal; p = 0.6882). However, median FSIQ was significantly lower in maternally than in paternally inherited familial deletions (65, range 50−86 vs. 71.5, range 58−96, respectively, p = 0.0350), with the regression model indicating an ~8 point decrement in FSIQ for this variable (p = 0.0061). FSIQ is higher on average in de novo than in inherited 22q11.2 deletions, regardless of parental origin. However, parent-of-origin appears relevant in inherited deletions. The results have potential clinical implications with further research needed to delineate possible actionable mechanisms. ispartof: GENES vol:13 issue:10 ispartof: location:Switzerland status: published

Published

2022

14. Estimate of the contemporary live-birth prevalence of recurrent 22q11.2 deletions: a cross-sectional analysis from population-based newborn screening

Author

Mylene Theriault, Pranesh Chakraborty, Christina Blagojevic, Aoy Tomita-Mitchell, Kristin D. Kernohan, Tracy Heung, Dennis E. Bulman, and Anne S. Bassett

Subjects

Male, medicine.medical_specialty, Cross-sectional study, Developmental Disabilities, Birth weight, Population, Gestational Age, Neonatal Screening, Early Medical Intervention, Prenatal Diagnosis, DiGeorge Syndrome, Prevalence, medicine, Humans, education, Ontario, education.field_of_study, Newborn screening, Obstetrics, business.industry, Research, Infant, Newborn, Gestational age, General Medicine, Odds ratio, Infant, Low Birth Weight, Confidence interval, Cross-Sectional Studies, Molecular Diagnostic Techniques, Female, Severe Combined Immunodeficiency, business, Live birth, Live Birth, Maternal Age

Abstract

Background: Although pathogenic 22q11.2 deletions are an important cause of developmental delays and lifelong disease burden, their variable and complex clinical expression contributes to under-recognition, delayed molecular diagnosis and uncertainty about prevalence. We sought to estimate the contemporary live-birth prevalence of typical 22q11.2 deletions using a population-based newborn screening sample and to examine data available for associated clinical features. Methods: Using DNA available from an unbiased sample of about 12% of all dried blood spots collected for newborn screening in Ontario between January 2017 and September 2018, we prospectively screened for 22q11.2 deletions using multiplex quantitative polymerase chain reaction assays and conducted independent confirmatory studies. We used cross-sectional analyses to compare available clinical and T-cell receptor excision circle (TREC, used in newborn screening for severe combined immunodeficiency) data between samples with and without 22q11.2 deletions. Results: The estimated minimum prevalence of 22q11.2 deletions was 1 in 2148 (4.7 per 10 000) live births (95% confidence interval [CI] 2.5 to 7.8 per 10 000), based on a total of 30 074 samples screened, with 14 having confirmed 22q11.2 deletions. Of term singletons, samples with 22q11.2 deletions had significantly younger median maternal age (25.5 v. 32.0 yr, difference −6.5 yr, 95% CI −7 to −2 yr), a greater proportion with small birth weight for gestational age (odds ratio 7.00, 95% CI 2.36 to 23.18) and lower median TREC levels (108.9 v. 602.5 copies/3 μL, p < 0.001). Interpretation: These results indicate that the 22q11.2 deletion syndrome is one of the most common of rare genetic conditions and may be associated with relatively younger maternal ages and with prenatal growth abnormalities. The findings support the public health importance of early — prenatal and neonatal — diagnosis that would enable prompt screening for and management of well-known actionable features associated with 22q11.2 deletions.

Published

2021

15. Within-family influences on dimensional neurobehavioral traits in a high-risk genetic model

Author

Anne S. Bassett, Jacob A. S. Vorstman, Maria Corral, Christian R. Marshall, Gregory Costain, René S. Kahn, Tracy Heung, Ania Fiksinski, and Elemi J. Breetvelt

Subjects

Proband, Regression analysis, Cognition, Quantitative trait locus, medicine.disease, 030227 psychiatry, Variable Expression, 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, Schizophrenia, Genetic model, Genetic variation, medicine, Psychology, 030217 neurology & neurosurgery, Applied Psychology, Clinical psychology

Abstract

BackgroundGenotype-first and within-family studies can elucidate factors that contribute to psychiatric illness. Combining these approaches, we investigated the patterns of influence of parental scores, a high-impact variant, and schizophrenia on dimensional neurobehavioral phenotypes implicated in major psychiatric disorders.MethodsWe quantitatively assessed cognitive (FSIQ, VIQ, PIQ), social, and motor functioning in 82 adult individuals with a de novo 22q11.2 deletion (22 with schizophrenia), and 148 of their unaffected parents. We calculated within-family correlations and effect sizes of the 22q11.2 deletion and schizophrenia, and used linear regressions to assess contributions to neurobehavioral measures.ResultsProband-parent intra-class correlations (ICC) were significant for cognitive measures (e.g. FSIQ ICC = 0.549, p < 0.0001), but not for social or motor measures. Compared to biparental scores, the 22q11.2 deletion conferred significant impairments for all phenotypes assessed (effect sizes −1.39 to −2.07 s.d.), strongest for PIQ. There were further decrements in those with schizophrenia. Regression models explained up to 37.7% of the variance in IQ and indicated that for proband IQ, parental IQ had larger effects than schizophrenia.ConclusionsThis study, for the first time, disentangles the impact of a high-impact variant from the modifying effects of parental scores and schizophrenia on relevant neurobehavioral phenotypes. The robust proband-parent correlations for cognitive measures, independent of the impact of the 22q11.2 deletion and of schizophrenia, suggest that, for certain phenotypes, shared genetic variation plays a significant role in expression. Molecular genetic and predictor studies are needed to elucidate shared factors and their contribution to psychiatric illness in this and other high-risk groups.

Published

2021

16. Biallelic PAN2 variants in individuals with a syndromic neurodevelopmental disorder and multiple congenital anomalies

Author

Miriam S. Reuter, Michael Zech, Maja Hempel, Janine Altmüller, Tracy Heung, Laura Pölsler, René Santer, Holger Thiele, Brett Trost, Christian Kubisch, Stephen W. Scherer, Sabine Rudnik-Schöneborn, Anne S. Bassett, Davor Lessel, and Medical Genetics

Subjects

Phenotype, Neurodevelopmental Disorders, Intellectual Disability, Genetics, Humans, Muscle Hypotonia, Abnormalities, Multiple, Dwarfism, RNA, Messenger, Genetics (clinical), Article

Abstract

PAN2 encodes a subunit of a deadenylation complex with important functions in mRNA stability and post-transcriptional regulation of gene expression. A homozygous frameshift deletion in PAN2 was reported in a single affected individual with developmental delay and multiple congenital anomalies. Here, we describe five additional individuals from three unrelated families with homozygous predicted loss-of-function variants in PAN2. The affected individuals presented with significant overlap in their clinical features, including mild-moderate intellectual disability, hypotonia, sensorineural hearing loss, EEG abnormalities, congenital heart defects (tetralogy of Fallot, septal defects, dilated aortic root), urinary tract malformations, ophthalmological anomalies, short stature with other skeletal anomalies, and craniofacial features including flat occiput, ptosis, long philtrum, and short neck. Our data confirm that biallelic predicted loss-of-function variants in PAN2 cause a syndrome with multiple congenital anomalies, and suggest an important role of mRNA polyA tail length for proper organ formation.

Published

2022

17. The role of 22q11.2 deletion syndrome in the relationship between congenital heart disease and scoliosis

Author

Michiel L. Houben, Jelle F. Homans, Tracy Heung, René M. Castelein, Moyo C. Kruyt, Anne S. Bassett, Steven de Reuver, Erwin Oechslin, Donna M. McDonald-McGinn, and Candice K. Silversides

Subjects

Adult, Heart Defects, Congenital, Down syndrome, Pediatrics, medicine.medical_specialty, Heart disease, Population, Context (language use), Scoliosis, Article, Marfan Syndrome, Young Adult, 03 medical and health sciences, 0302 clinical medicine, DiGeorge syndrome, DiGeorge Syndrome, Humans, Medicine, Orthopedics and Sports Medicine, cardiovascular diseases, Child, education, 030222 orthopedics, education.field_of_study, Cobb angle, business.industry, medicine.disease, United States, Cross-Sectional Studies, Cohort, Female, Surgery, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

BACKGROUND CONTEXT: For over four decades, clinicians and researchers have suggested a relationship between congenital heart disease (CHD) and scoliosis, attributed to either the disease itself or to the long-term effects of cardiac surgery on the immature thoracic cage. However, no study has yet accounted for 22q11.2 deletion syndrome (22q11.2DS), the second most common cause of CHD after Down syndrome. 22q11.2DS has a scoliosis risk of 50%, but within 22q11.2DS a previous report found no significant association between scoliosis and CHD. We, therefore, hypothesized that scoliosis within a CHD cohort would be related to an underlying 22q11.2 deletion. PURPOSE: To determine the prevalence of scoliosis in CHD patients with and without 22q11.2DS. STUDY DESIGN/SETTING: Cross-sectional. PATIENT SAMPLE: A well-characterized existing database of 315 adults with CHD (primarily tetralogy of Fallot), with (n=86) and without (n=229) 22q11.2DS, matched by sex and CHD severity, and excluding other known syndromic diagnoses. We compared the scoliosis prevalence of patients with 22q11.2DS and CHD patients to the prevalence of scoliosis in a cohort of adults with 22q11.2DS without CHD based on medical records. OUTCOME MEASURES: Presence of scoliosis (Cobb angle ≥10°). METHODS: We systematically determined the presence of scoliosis in all included patients using chest radiographs, blind to genetic diagnosis. Besides 22q11.2DS, we analyzed other suspected risk factors for scoliosis using a regression model: thoracotomy before the age of 12 years, severe CHD type and sex. RESULTS: The prevalence of scoliosis in adults with CHD and 22q11.2DS (n=46, 53.5%) was significantly greater than in those without 22q11.2DS (n=18, 7.9%, p

Published

2020

18. Elevated regional cerebral blood flow in adults with 22q11.2 deletion syndrome

Author

Maurice Pasternak, Zahra Shirzadi, Henk J. M. M. Mutsaerts, Erik Boot, Nancy J. Butcher, Bradley J. MacIntosh, Tracy Heung, Anne S. Bassett, Mario Masellis, and Radiology and nuclear medicine

Subjects

Psychiatry and Mental health, Biological Psychiatry

Abstract

Objectives: Recurrent chromosome 22q11.2 deletions cause 22q11 deletion syndrome (22q11DS), a multisystem disorder associated with high rates of schizophrenia. Neuroanatomical changes on brain MRI have been reported in relation to 22q11DS. However, to date no 22q11DS neuroimaging studies have examined cerebral blood flow (CBF). This exploratory case-control study seeks to identify differences in regional cerebral blood flow between 22q11DS subjects and controls, and their association with psychotic symptoms. Methods: This study of 23 adults used arterial spin labelling MRI to investigate voxel-wise CBF in 22q11DS individuals compared with age- and sex-matched healthy controls. Results: Four significant clusters, involving the right and left putamen, right fusiform gyrus and left middle temporal gyrus, delineated significantly elevated CBF in individuals with 22q11DS compared to controls. Post-hoc analysis determined that this elevation in CBF trended with psychotic symptom diagnosis within the 22q11DS group. Conclusions: These findings suggest possible relevance to schizophrenia risk and support further functional neuroimaging studies of 22q11DS with larger sample sizes to improve our understanding of the underlying pathophysiology.

Published

2022

19. Genome-wide tandem repeat expansions contribute to schizophrenia risk

Author

Bahareh A. Mojarad, Worrawat Engchuan, Brett Trost, Ian Backstrom, Yue Yin, Bhooma Thiruvahindrapuram, Linda Pallotto, Aleksandra Mitina, Mahreen Khan, Giovanna Pellecchia, Bushra Haque, Keyi Guo, Tracy Heung, Gregory Costain, Stephen W. Scherer, Christian R. Marshall, Christopher E. Pearson, Anne S. Bassett, and Ryan K. C. Yuen

Subjects

Adult, Cellular and Molecular Neuroscience, Psychiatry and Mental health, Multifactorial Inheritance, Tandem Repeat Sequences, Schizophrenia, Humans, Genetic Predisposition to Disease, Molecular Biology, Polymorphism, Single Nucleotide, Genome-Wide Association Study

Abstract

Tandem repeat expansions (TREs) can cause neurological diseases but their impact in schizophrenia is unclear. Here we analyzed genome sequences of adults with schizophrenia and found that they have a higher burden of TREs that are near exons and rare in the general population, compared with non-psychiatric controls. These TREs are disproportionately found at loci known to be associated with schizophrenia from genome-wide association studies, in individuals with clinically-relevant genetic variants at other schizophrenia loci, and in families where multiple individuals have schizophrenia. We showed that rare TREs in schizophrenia may impact synaptic functions by disrupting the splicing process of their associated genes in a loss-of-function manner. Our findings support the involvement of genome-wide rare TREs in the polygenic nature of schizophrenia.

Published

2021

20. Genome-wide tandem repeat expansions contribute to schizophrenia risk

Author

Bahareh A Mojarad, Worrawat Engchuan, Brett Trost, Ian Backstrom, Yue Yin, Bhooma Thiruvahindrapuram, Linda Pallotto, Mahreen Khan, Giovanna Pellecchia, Bushra Haque, Keyi Guo, Tracy Heung, Gregory Costain, Stephen W Scherer, Christian R Marshall, Christopher E Pearson, Anne S Bassett, and Ryan KC Yuen

Subjects

mental disorders, behavioral disciplines and activities

Abstract

Tandem repeat expansions (TREs) can cause neurological diseases but their impact in schizophrenia is unclear. Here we analyzed genome sequences of adults with schizophrenia and found that they have a higher burden of TREs that are near exons and rare in the general population, compared with non-psychiatric controls. These TREs are disproportionately found at loci known to be associated with schizophrenia from genome-wide association studies, in individuals with clinically-relevant genetic variants at other schizophrenia loci, and in families where multiple individuals have schizophrenia. Our findings support the involvement of genome-wide rare TREs in the polygenic nature of schizophrenia.

Published

2021

21. Incidence of infective endocarditis in adults with congenital heart disease and diagnosed 22q11.2 deletion syndrome

Author

Anne S. Bassett, Jessica Patzer, Adonis Ng, Erwin Oechslin, and Tracy Heung

Subjects

Pediatrics, medicine.medical_specialty, Heart disease, business.industry, Incidence (epidemiology), Infective endocarditis, RC666-701, medicine, Diseases of the circulatory (Cardiovascular) system, Deletion syndrome, business, medicine.disease

Published

2021

22. Reproductive Outcomes in Adults with 22q11.2 Deletion Syndrome

Author

Lisa D. Palmer, Zoë McManus, Tracy Heung, Grace McAlpine, Christina Blagojevic, Maria Corral, and Anne S. Bassett

Subjects

Adult, Delayed Diagnosis, Adolescent, Middle Aged, Abortion, Spontaneous, Young Adult, sex, stillborn, abortion, prenatal, schizophrenia, DiGeorge syndrome, Pregnancy, Intellectual Disability, DiGeorge Syndrome, Genetics, Humans, Female, Genetic Fitness, Live Birth, Genetics (clinical), Aged

Abstract

The 22q11.2 microdeletion and its associated conditions could affect reproductive outcomes but there is limited information on this important area. We investigated reproductive outcomes in a sample of 368 adults with typical 22q11.2 deletions (median age 32.8, range 17.9–76.3 years; 195 females), and without moderate-severe intellectual disability, who were followed prospectively. We examined all reproductive outcomes and possible effects of diagnosis as a transmitting parent on these outcomes. We used logistic regression to investigate factors relevant to reproductive fitness (liveborn offspring). There were 63 (17.1%) individuals with 157 pregnancy outcomes, 94 (60.3%) of which involved live births. Amongst the remainder involving a form of loss, were seven (5.77%) stillbirths, significantly greater than population norms (p < 0.0001). For 35 (55.6%) individuals, diagnosis of 22q11.2 deletion syndrome (22q11.2DS) followed diagnosis of an offspring, with disproportionately fewer individuals had major congenital heart disease (CHD) in that transmitting parent subgroup. The regression model indicated that major CHD, in addition to previously identified factors, was a significant independent predictor of reduced reproductive fitness. There was evidence of persisting diagnostic delay and limited prenatal genetic testing. The findings indicate that pregnancy loss is an important health issue for adults with 22q11.2DS. CHD and/or its absence is a factor to consider in reproductive outcome research. Further studies are warranted to better appreciate factors that may contribute to reproductive outcomes, including technological advances. The results suggest the need for ongoing efforts to provide optimal education and supports to individuals with 22q11.2DS, and their clinicians, around reproductive issues and early diagnosis.

Published

2022

23. All-cause mortality and survival in adults with 22q11.2 deletion syndrome

Author

Lily Van, Sarah L. Malecki, Kathleen A. Hodgkinson, Candice K. Silversides, Maria Corral, Anne S. Bassett, Tracy Heung, Enoch Ng, Justin Graffi, Spencer van Mil, Eva W.C. Chow, and Erik Boot

Subjects

0301 basic medicine, Adult, Heart Defects, Congenital, Male, Pediatrics, medicine.medical_specialty, Heart disease, Adolescent, Genetic counseling, Chromosomes, Human, Pair 22, Genetic Counseling, 030105 genetics & heredity, Article, 03 medical and health sciences, velocardiofacial syndrome, DiGeorge syndrome, Intellectual Disability, Intellectual disability, medicine, DiGeorge Syndrome, Humans, Prospective Studies, Genetics (clinical), Aged, business.industry, Hazard ratio, Microdeletion syndrome, Middle Aged, medicine.disease, 3. Good health, schizophrenia, 030104 developmental biology, Schizophrenia, Case-Control Studies, Life expectancy, heart defects, Female, prognosis, Chromosome Deletion, business

Abstract

Purpose Given limited data available on long-term outcomes in 22q11.2 deletion syndrome (22q11.2DS), we investigated mortality risk in adults with this microdeletion syndrome. Methods We studied 309 well-characterized adults (age ≥17 years) with 22q11.2DS and their 1014 unaffected parents and siblings, using a prospective case–control design. We used Cox proportional hazards regression modeling and Kaplan–Meier curves to investigate effects of the 22q11.2 deletion and its associated features on all-cause mortality and survival. Results The 22q11.2 deletion (hazard ratio [HR] 8.86, 95% CI 2.87–27.37) and major congenital heart disease (CHD; HR 5.03, 95% CI 2.27–11.17), but not intellectual disability or psychotic illness, were significant independent predictors of mortality for adults with 22q11.2DS compared with their siblings. Amongst those with 22q11.2DS, there were 31 deaths that occurred at a median age of 46.4 (range 18.1–68.6) years; a substantial minority had outlived both parents. Probability of survival to age 45 years was approximately 72% for those with major CHD, and 95% for those with no major CHD (p

Published

2019

24. 22q11.2 microdeletion and increased risk for type 2 diabetes

Author

Erik Boot, Andrea Tyrer, Lily Van, Tracy Heung, Christian Fenn, Anne S. Bassett, Eva W.C. Chow, Sarah L. Malecki, Marcos Sanches, Maria Corral, Susan R. George, and Satya Dash

Subjects

Risk, Pediatrics, medicine.medical_specialty, endocrine system diseases, Genotype, Population, Type 2 diabetes, 01 natural sciences, 03 medical and health sciences, 0302 clinical medicine, Diabetes mellitus, DiGeorge syndrome, medicine, Genetics, Molecular diagnostics, 030212 general & internal medicine, 0101 mathematics, Risk factor, Family history, education, lcsh:R5-920, education.field_of_study, business.industry, 010102 general mathematics, Diabetes, nutritional and metabolic diseases, General Medicine, medicine.disease, Early diagnosis, Obesity, 3. Good health, Hypoparathyroidism, Structural variant, lcsh:Medicine (General), business, Research Paper

Abstract

Background: The 22q11.2 microdeletion is the pathogenic copy number variation (CNV) associated with 22q11.2 deletion syndrome (22q11.2DS, formerly known as DiGeorge syndrome). Familiar endocrinological manifestations include hypoparathyroidism and hypothyroidism, with recent elucidation of elevated risk for obesity in adults. In this study, we aimed to determine whether adults with 22q11.2DS have an increased risk of developing type 2 diabetes (T2D). Methods: We studied the effect of the 22q11.2 microdeletion on risk for T2D, defined by history and glycosylated hemoglobin (HbA1c), using weighted survey data from the adult Canadian population (based on n = 11,874) and from a clinical cohort of adults with 22q11.2DS (n = 314), aged 17–69 years. Binomial logistic regression models accounted for age, sex, non-European ethnicity, family history of T2D, obesity, and antipsychotic medication use. Findings: The 22q11.2 microdeletion was a significant independent risk factor for T2D (OR 2·44, 95% CI 1·39–4·31), accounting for other factors (p < 0·0001). All factors except sex were also significant within 22q11.2DS. The median age at diagnosis of T2D was significantly younger in 22q11.2DS than in the Canadian population sample (32 vs 50 years, p

Published

2020

25. Genetic contributors to risk of schizophrenia in the presence of a 22q11.2 deletion

Author

Richard Duncan, Tao Wang, Carrie E. Bearden, David J. Cutler, Stephen T. Warren, Maria Pontillo, Robert Sean Gallagher, Elemi J. Breetvelt, Tingwei Guo, Nancy J. Butcher, Jennifer G. Mulle, Claudia Ornstein, Claudia Vingerhoets, Clodagh M. Murphy, Ehud Mekori-Domachevsky, Wendy R. Kates, Jacob A. S. Vorstman, Tracy Heung, Joris Vermeesch, Maria Gudbrandsen, Ann Swillen, H. Richard Johnston, Oanh Tran, Marco Armando, Joseph F. Cubells, Raoul Belzeaux, Jeroen Breckpot, Bruno Marino, Tony J. Simon, Harold I. Salmons, Maria Jalbrzikowski, Wanda Fremont, Anna J. Voss, Worrawat Engchuan, Opal Y. Ousley, Stefano Vicari, Jordi Rosell, Sixto García-Miñaur, Declan G. Murphy, Alexander Diacou, Ania Fiksinski, Abraham Weizman, Edward Moss, Stephan Eliez, Miri Carmel, Vandana Shashi, Anne S. Bassett, Ronnie Weinberger, Hayley Moss, Marianne Bernadette van den Bree, Kelly Schoch, Maude Schneider, Linda E. Campbell, Sasja N. Duijff, Eileen Daly, Annick Vogels, Stephen R. Hooper, David Fraguas, Sarah E. Prasad, Chelsea Lowther, Michael John Owen, Frédérique Béna, Gabriela M. Repetto, Eva W.C. Chow, Bernice E. Morrow, Robert J. Sharkus, Celso Arango, Christian R. Marshall, Jasna Raventos-Simic, Jaume Morey-Canyelles, Tiffany Busa, Andrea Jin, James T.R. Walters, Leila Kushan, Wolfram Demaerel, Monica E. Calkins, Jhih Rong Lin, Elaine H. Zackai, Esther D.A. van Duin, Antonio Buzzanca, Corrado Sandini, Kieran C. Murphy, Beverly S. Emanuel, Erik Boot, Maria Niarchou, Nigel Williams, Elfi Vergaelen, Maria Cristina Digilio, Daniele Merico, Karlene Coleman, Gregory A. Costain, Matthew S. Hestand, Peter Holmans, Michael E. Zwick, Michael P. Epstein, Damià H. Suñer, Yingjie Zhao, Marta Unolt, Kathryn McCabe, Aaron M. Holleman, Zhengdong Zhang, Rosemarie Fritsch, Alex V. Kotlar, Elena Michaelovsky, T. Blaine Crowley, Brenna Lilley, Sunny X. Tang, Rens Evers, Ruben C. Gur, Isabelle Cleynen, Flora Tassone, Nicole Philip, Kevin M. Antshel, Koen Devriendt, Antonio F. Pardiñas, Pankaj Chopra, Thomas Monfeuga, Fabio Di Fabio, Therese van Amelsvoort, Aaron Golden, Doron Gothelf, Donna M. McDonald-McGinn, Raquel E. Gur, Daniel E. McGinn, Catholic University of Leuven - Katholieke Universiteit Leuven (KU Leuven), The Hospital for sick children [Toronto] (SickKids), Emory University [Atlanta, GA], Cardiff University, University of Pennsylvania [Philadelphia], Albert Einstein College of Medicine [New York], University Hospitals Leuven [Leuven], University of Toronto, University Medical Center [Utrecht], University of California, Children’s Hospital of Philadelphia (CHOP ), Emory University School of Medicine, University Health Network, Centre for Addiction and Mental Health [Toronto] (CAMH), Maastricht University [Maastricht], Universidad de Chile, Clínica Alemana & Universidad del Desarrollo, Royal College of Surgeons in Ireland (RCSI), King‘s College London, Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Children's Hospital Bambino Gesù [Rome, Italie], Tel Aviv University [Tel Aviv], The Edmond and Lily Safra Children's Hospital [Tel-Hahsomer, Israel], University of Pittsburgh School of Medicine, Pennsylvania Commonwealth System of Higher Education (PCSHE), University of Geneva [Switzerland], Geneva University Hospitals and Geneva University, Syracuse University, SUNY Upstate Medical University, State University of New York (SUNY), Hôpital Sainte-Marguerite [CHU - APHM] (Hôpitaux Sud ), Hôpital d'Enfants de la Timone [Marseille], Assistance Publique - Hôpitaux de Marseille (APHM), 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), University of Newcastle [Australia] (UoN), University of North Carolina [Chapel Hill] (UNC), University of North Carolina System (UNC), Duke University School of Medicine, University of California [Davis] (UC Davis), Universidad Complutense de Madrid = Complutense University of Madrid [Madrid] (UCM), La Paz University Hospital, Hospital Universitario Son Espases, University of Pennsylvania, University of California (UC), Universidad de Chile = University of Chile [Santiago] (UCHILE), Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome] (UNIROMA), Tel Aviv University (TAU), Université de Genève = University of Geneva (UNIGE), University of Newcastle [Callaghan, Australia] (UoN), Caugant, Julien, RS: MHeNs - R2 - Mental Health, Psychiatrie & Neuropsychologie, and MUMC+: MA Med Staf Spec Psychiatrie (9)

Subjects

0301 basic medicine, [SDV]Life Sciences [q-bio], VARIANTS, Cohort Studies, 0302 clinical medicine, Medicine, Copy-number variation, BRAIN, ddc:616, Genetics, education.field_of_study, PSYCHIATRIC-DISORDERS, ASSOCIATION, 3. Good health, [SDV] Life Sciences [q-bio], Psychiatry and Mental health, Schizophrenia, Cohort, BEHAVIOR, Adult, DATABASE, Population, COPY-NUMBER VARIATION, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, mental disorders, DiGeorge Syndrome, Humans, genetics, 22q11deletion syndrome, schizophrenia, education, Molecular Biology, Gene, Microarray analysis techniques, business.industry, MUTATIONS, CONSORTIUM, medicine.disease, Institutional repository, INDIVIDUALS, 030104 developmental biology, Psychotic Disorders, Case-Control Studies, 22q11.2 deletion syndrome, genetic factors, Polygenic risk score, business, 030217 neurology & neurosurgery, International 22q11.2DS Brain and Behavior Consortium

Abstract

Schizophrenia occurs in about one in four individuals with 22q11.2 deletion syndrome (22q11.2DS). The aim of this International Brain and Behavior 22q11.2DS Consortium (IBBC) study was to identify genetic factors that contribute to schizophrenia, in addition to the ~20-fold increased risk conveyed by the 22q11.2 deletion. Using whole-genome sequencing data from 519 unrelated individuals with 22q11.2DS, we conducted genome-wide comparisons of common and rare variants between those with schizophrenia and those with no psychotic disorder at age ≥25 years. Available microarray data enabled direct comparison of polygenic risk for schizophrenia between 22q11.2DS and independent population samples with no 22q11.2 deletion, with and without schizophrenia (total n = 35,182). Polygenic risk for schizophrenia within 22q11.2DS was significantly greater for those with schizophrenia (padj = 6.73 × 10−6). Novel reciprocal case–control comparisons between the 22q11.2DS and population-based cohorts showed that polygenic risk score was significantly greater in individuals with psychotic illness, regardless of the presence of the 22q11.2 deletion. Within the 22q11.2DS cohort, results of gene-set analyses showed some support for rare variants affecting synaptic genes. No common or rare variants within the 22q11.2 deletion region were significantly associated with schizophrenia. These findings suggest that in addition to the deletion conferring a greatly increased risk to schizophrenia, the risk is higher when the 22q11.2 deletion and common polygenic risk factors that contribute to schizophrenia in the general population are both present. ispartof: Molecular Psychiatry vol:26 issue:8 pages:1-15 ispartof: location:England status: published

Published

2020

26. Complete Sequence of the 22q11.2 Allele in 1,053 Subjects with 22q11.2 Deletion Syndrome Reveals Modifiers of Conotruncal Heart Defects

Author

Claudia Ornstein, Anne S. Bassett, Matthew S. Hestand, Bruno Marino, Kelly Schoch, Tony J. Simon, Therese van Amelsvoort, Doron Gothelf, Carrie E. Bearden, Elemi J. Breetvelt, Michael P. Epstein, Tiffany Busa, Robert J. Shprintzen, David Cutler, Tao Wang, Leila Kushan-Wells, Donna M. McDonald-McGinn, Raquel E. Gur, Hayley Moss, Esther D. A. van Duin, B Dallapiccola, Joris Vermeesch, Clodagh M. Murphy, Yingjie Zhao, Rens Evers, María Angeles de la Fuente Sanches, Ann Swillen, H. Richard Johnston, Maria Pontillo, Steve Warren, Guido Lattanzi, Michael E. Zwick, Jacob A. S. Vorstman, Jeroen Breckpot, Oanh Tran, Stylianos E. Antonarakis, Stefano Vicari, Andrea Jin, Alexander Diacou, Miri Carmel, Christian R. Marshall, Abraham Weizman, Bernice E. Morrow, Fadi I Musfee, Wendy R. Kates, Michael John Owen, Fabio Di Fabio, Marco Armando, Erik Boot, Claudia Vingerhoets, Elizabeth Goldmuntz, Massimo Biondi, Kieran C. Murphy, Nancy Butcher, Declan G. Murphy, Candice K. Silversides, Isabelle Cleynen, T. Blaine Crowley, Vandana Shashi, Linda E. Campbell, Elaine H. Zackai, Ronnie Weinberger, Sixto García-Miñaur, Marianne Bernadette van den Bree, Fernando García Algas, Damian Heine-Suñer, Tracy Heung, Daniel E. McGinn, Maude Schneider, Stephan Eliez, Marta Unolt, Stephen R. Hooper, Kathryn McCabe, A. J. Agopian, Tingwei Guo, Zhengdong Zhang, Rosemarie Fritsch, Luis Fernández, Beverly S. Emanuel, Elfi Vergaelen, Alejandra Laorden-Nieto, Flora Tassone, Gabriela M. Repetto, Laura E. Mitchell, Antonino Buzzanca, Elena Michaelovsky, M. Cristina Digilio, Nicole Philip, RS: MHeNs - R2 - Mental Health, Psychiatrie & Neuropsychologie, MUMC+: MA Med Staf Spec Psychiatrie (9), and Antonarakis, Stylianos

Subjects

Male, Heart disease, PREDICTION, Chromosomes, Human, Pair 22, Haploinsufficiency, Cardiovascular, Medical and Health Sciences, Genetic modifier, Proto-Oncogene Mas, Linkage Disequilibrium, Cohort Studies, Congenital, ddc:616.89, Segmental Duplications, Genomic, DiGeorge syndrome, 2.1 Biological and endogenous factors, Chromosome 22q11.2 deletion syndrome, Copy-number variation, Aetiology, Genetics (clinical), Heart Defects, Pediatric, Genetics & Heredity, Genetics, cardio-facial syndrome, II DEFICIENCY, 0303 health sciences, variants, MOLECULAR DEFINITION, 030305 genetics & heredity, TBX1, Single Nucleotide, Biological Sciences, Segmental Duplications, Complex trait, Heart Disease, Phenotype, Female, tbx1 haploinsufficiency, Chromosome Deletion, Human, Heart Defects, Congenital, prevalence, Biology, Polymorphism, Single Nucleotide, Chromosomes, Article, 03 medical and health sciences, Complete sequence, Clinical Research, LOW-COPY REPEATS, medicine, Humans, Polymorphism, Allele, Conotruncal heart defects, International 22q11.2 Brain and Behavior Consortium, 030304 developmental biology, Sequence (medicine), Congenital heart disease, Copy number variation, Human Genome, association, CRKL, medicine.disease, chromosome 22q11.2 deletion syndrome, complex trait, congenital heart disease, conotruncal heart defects, copy number variation, genetic association, genetic modifier, haploinsufficiency, Case-Control Studies, Genome-Wide Association Study, Genomic, Genetic association, Pair 22

Abstract

The 22q11.2 deletion syndrome (22q11.2DS) results from non-allelic homologous recombination between low-copy repeats termed LCR22. About 60%-70% of individuals with the typical 3 megabase (Mb) deletion from LCR22A-D have congenital heart disease, mostly of the conotruncal type (CTD), whereas others have normal cardiac anatomy. In this study, we tested whether variants in the hemizygous LCR22A-D region are associated with risk for CTDs on the basis of the sequence of the 22q11.2 region from 1,053 22q11.2DS individuals. We found a significant association (FDR p < 0.05) of the CTD subset with 62 common variants in a single linkage disequilibrium (LD) block in a 350 kb interval harboring CRKL. A total of 45 of the 62 variants were associated with increased risk for CTDs (odds ratio [OR) ranges: 1.64-4.75). Associations of four variants were replicated in a meta-analysis of three genome-wide association studies of CTDs in affected individuals without 22q11.2DS. One of the replicated variants, rs178252, is located in an open chromatin region and resides in the double-elite enhancer, GH22J020947, that is predicted to regulate CRKL (CRK-like proto-oncogene, cytoplasmic adaptor) expression. Approximately 23% of patients with nested LCR22C-D deletions have CTDs, and inactivation of Crkl in mice causes CTDs, thus implicating this gene as a modifier. Rs178252 and rs6004160 are expression quantitative trait loci (eQTLs) of CRKL. Furthermore, set-based tests identified an enhancer that is predicted to target CRKL and is significantly associated with CTD risk (GH22J020946, sequence kernal association test (SKAT) p = 7.21 × 10-5) in the 22q11.2DS cohort. These findings suggest that variance in CTD penetrance in the 22q11.2DS population can be explained in part by variants affecting CRKL expression. ispartof: AMERICAN JOURNAL OF HUMAN GENETICS vol:106 issue:1 pages:26-40 ispartof: location:United States status: published

Published

2020

27. Haploinsufficiency of vascular endothelial growth factor related signaling genes is associated with tetralogy of Fallot

Author

Anne S. Bassett, Meredith Curtis, Gregory Costain, Miriam S. Reuter, Stephen W. Scherer, Chelsea Lowther, Rebekah Jobling, Christian R. Marshall, Candice K. Silversides, Erwin Oechslin, Raymond H. Kim, Heinrich Sticht, Bhooma Thiruvahindrapuram, Rajiv Chaturvedi, Susan Walker, S. Mohsen Hosseini, Roozbeh Manshaei, Spencer van Mil, Tracy Heung, Rachel M. Wald, and Eriskay Liston

Subjects

0301 basic medicine, Proband, Adult, Male, Vascular Endothelial Growth Factor A, Haploinsufficiency, 030105 genetics & heredity, Biology, Brief Communication, Pathogenesis, 03 medical and health sciences, chemistry.chemical_compound, Loss of Function Mutation, Conotruncal defect, medicine, Humans, Genetic Predisposition to Disease, FLT4, Genetics (clinical), Genetic Association Studies, Tetralogy of Fallot, Aged, Genetics, Whole Genome Sequencing, conotruncal defects, Middle Aged, medicine.disease, Vascular Endothelial Growth Factor Receptor-3, VEGF, congenital heart disease, Vascular Endothelial Growth Factor Receptor-2, 3. Good health, Vascular endothelial growth factor, genome sequencing, Vascular endothelial growth factor A, 030104 developmental biology, chemistry, Female, Signal Transduction

Abstract

Purpose To determine disease-associated single-gene variants in conotruncal defects, particularly tetralogy of Fallot (TOF). Methods We analyzed for rare loss-of-function and deleterious variants in FLT4 (VEGFR3) and other genes in the vascular endothelial growth factor (VEGF) pathway, as part of a genome sequencing study involving 175 adults with TOF from a single site. Results We identified nine (5.1%) probands with novel FLT4 variants: seven loss-of-function, including an 8-kb deletion, and two predicted damaging. In ten other probands we found likely disruptive variants in VEGF-related genes: KDR (VEGFR2; two stopgain and two nonsynonymous variants), VEGFA, FGD5, BCAR1, IQGAP1, FOXO1, and PRDM1. Detection of VEGF-related variants (19/175, 10.9%) was associated with an increased prevalence of absent pulmonary valve (26.3% vs. 3.4%, p

Published

2018

28. Atypical chromosome 22q11.2 deletions are complex rearrangements and have different mechanistic origins

Author

Matthew S. Hestand, Ann Swillen, Elfi Vergaelen, Jeroen Breckpot, Adrian Odrzywolski, Lisanne Vervoort, Anne S. Bassett, Ania Fiksinski, Bernice E. Morrow, Laura Yissel Rengifo, Donna M. McDonald-McGinn, Vandana Shashi, Jacob A. S. Vorstman, Tracy Heung, Wolfram Demaerel, Joris Vermeesch, Janneke Zinkstok, Koen Devriendt, and Eva W.C. Chow

Subjects

Adult, Male, Chromosomes, Human, Pair 22, Chromosome Breakpoints, Biology, Chromosomes, Article, 03 medical and health sciences, 0302 clinical medicine, Segmental Duplications, Genomic, Genetics, DiGeorge Syndrome, Humans, International 22q11.2 Brain, Allele, Homologous Recombination, Molecular Biology, Genetics (clinical), Alleles, In Situ Hybridization, Fluorescence, 030304 developmental biology, Segmental duplication, Sequence (medicine), Whole genome sequencing, 0303 health sciences, Whole Genome Sequencing, Breakpoint, Chromosome, Chromosome Mapping, General Medicine, Chromosome Inversion, Female, Chromosome Deletion, Homologous recombination, 030217 neurology & neurosurgery, Behavior Consortium

Abstract

The majority (99%) of individuals with 22q11.2 deletion syndrome (22q11.2DS) have a deletion that is caused by non-allelic homologous recombination between two of four low copy repeat clusters on chromosome 22q11.2 (LCR22s). However, in a small subset of patients, atypical deletions are observed with at least one deletion breakpoint within unique sequence between the LCR22s. The position of the chromosome breakpoints and the mechanisms driving those atypical deletions remain poorly studied. Our large-scale, whole genome sequencing study of >1500 subjects with 22q11.2DS identified six unrelated individuals with atypical deletions of different types. Using a combination of whole genome sequencing data and fiber-fluorescence in situ hybridization, we mapped the rearranged alleles in these subjects. In four of them, the distal breakpoints mapped within one of the LCR22s and we found that the deletions likely occurred by replication-based mechanisms. Interestingly, in two of them, an inversion probably preceded inter-chromosomal 'allelic' homologous recombination between differently oriented LCR22-D alleles. Inversion associated allelic homologous recombination (AHR) may well be a common mechanism driving (atypical) deletions on 22q11.2. ispartof: HUMAN MOLECULAR GENETICS vol:28 issue:22 pages:3724-3733 ispartof: location:England status: published

Published

2019

29. Abnormal spirometry in adults with 22q11.2 microdeletion and congenital heart disease

Author

Candice K. Silversides, Christina Blagojevic, Anne S. Bassett, John Granton, Spencer van Mil, Erwin Oechslin, and Tracy Heung

Subjects

Spirometry, medicine.medical_specialty, Vital capacity, Heart disease, 030204 cardiovascular system & hematology, Pulmonary function testing, 03 medical and health sciences, FEV1/FVC ratio, 0302 clinical medicine, Internal medicine, Genetics, medicine, Diseases of the circulatory (Cardiovascular) system, Adult congenital heart disease, cardiovascular diseases, DiGeorge syndrome, Lung, 030304 developmental biology, Genetic testing, Tetralogy of Fallot, 0303 health sciences, medicine.diagnostic_test, business.industry, 22q11 2 microdeletion, General Medicine, medicine.disease, Asthma, 3. Good health, Scoliosis, RC666-701, Cardiology, business

Abstract

Background: In adults with congenital heart disease (CHD), pulmonary dysfunction is prevalent and associated with poor outcomes; however, underlying genetic contributors remain unexamined. We investigated whether the 22q11.2 microdeletion, an important genetic cause of CHD, was associated with abnormal spirometry in adults with CHD. Methods: We conducted a retrospective case-control study of 207 adults with CHD (predominantly tetralogy of Fallot), and spirometry data available from cardiopulmonary exercise testing, matching 58 with a confirmed 22q11.2 microdeletion to 149 controls on age (median 26.4, 28.2 years, respectively), sex, ethnicity, and CHD severity (37.9%, 29.5% complex, respectively). We examined forced vital capacity (FVC), forced expiratory volume in 1 s (FEV1), their % predicted values, and FEV1/FVC ratio. Results: All respiratory parameters assessed were significantly worse in those with 22q11.2 deletion syndrome (22q11.2DS-CHD) as compared to CHD-controls. Linear regression models indicated that the 22q11.2 microdeletion was associated with worse spirometry values even when accounting for complex CHD (FVC% predicted, p

Published

2021

30. Obesity in adults with 22q11.2 deletion syndrome

Author

Eva W.C. Chow, Nancy J. Butcher, Sarah L. Voll, Tracy Heung, Candice K. Silversides, Anne S. Bassett, Samantha Cooper, and Erik Boot

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Canada, Adolescent, DNA Copy Number Variations, Type 2 diabetes, Logistic regression, Article, Body Mass Index, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Intellectual disability, energy metabolism, medicine, DiGeorge Syndrome, Humans, Obesity, Genetics (clinical), 2. Zero hunger, Genetics, Psychotropic Drugs, business.industry, copy number variation, Age Factors, Odds ratio, Middle Aged, medicine.disease, congenital heart disease, Confidence interval, 3. Good health, 030104 developmental biology, Logistic Models, Phenotype, Diabetes Mellitus, Type 2, Medical genetics, Female, hypothyroidism, business, Body mass index, 030217 neurology & neurosurgery

Abstract

To characterize the prevalence of and contributing factors to adult obesity in the most common recurrent copy-number variation (CNV), 22q11.2 deletion, given that other rare CNVs are known to have obesity phenotypes. In 207 adults with 22q11.2 deletion syndrome (22q11.2DS), we used available height and weight measurements to calculate body mass index (BMI) and recorded associated factors that could play a role in obesity. We used the maximum BMI per subject and logistic regression to test a model predicting obesity class. The prevalence of obesity (BMI ≥30) in 22q11.2DS (n = 90, 43.5%; at median age of 26.7 years) was significantly greater than for Canadian norms (odds ratio (OR) 2.30, 95% confidence interval (CI) = 1.74–3.02, P < 0.0001), even after excluding individuals with a history of antipsychotic use. The regression model was significant (P < 0.0001). Psychotropic medication use and age, but not sex or presence of intellectual disability, were associated with higher obesity level. Ten (4.8%) individuals were diagnosed with type 2 diabetes at a median age of 39.5 years; the prevalence was higher in those with obesity (P < 0.01). The results suggest that adult obesity is related to the 22q11.2 deletion. The findings expand the potential genetic causes of obesity and have important implications for management of 22q11.2DS. Genet Med 19 2, 204–208.

Published

2016

31. Elucidating the diagnostic odyssey of 22q11.2 deletion syndrome

Author

Lisa D. Palmer, Donna M. McDonald-McGinn, Kathleen A. Hodgkinson, Alina Guna, Erik Boot, Elaine H. Zackai, Nancy J. Butcher, Tracy Heung, Anne S. Bassett, T. Blaine Crowley, Eva W.C. Chow, and Academic Medical Center

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Pediatrics, Neurology, Adolescent, Specialty, Scoliosis, Kaplan-Meier Estimate, 030105 genetics & heredity, Article, 03 medical and health sciences, Young Adult, DiGeorge syndrome, Intellectual disability, Genetics, medicine, DiGeorge Syndrome, Humans, Deletion syndrome, Genetic Testing, 10. No inequality, Child, Genetics (clinical), Newborn screening, business.industry, Infant, Newborn, Infant, Middle Aged, medicine.disease, 3. Good health, Phenotype, Child, Preschool, Cohort, Female, Chromosome Deletion, business

Abstract

Clinical molecular testing has been available for 22q11.2 deletion syndrome (22q11.2DS) for over two decades yet under-recognition and diagnostic delays are common. To characterize the “diagnostic odyssey” in 22q11.2DS we studied 202 well-characterized unrelated adults, none ascertained through an affected relative. We used a regression model to identify clinical and demographic factors associated with length of time to molecular diagnosis. Kaplan–Meier analysis compared time to diagnosis for the molecular testing era (since 1994) and earlier birth cohorts. The results showed that the median time to molecular diagnosis of the 22q11.2 deletion was 4.7 (range 0–20.7) years. Palatal and cardiac anomalies, but not developmental delay/intellectual disability, were associated with a shorter time to molecular diagnosis. Non-European ethnicity was associated with longer time to diagnosis. Inclusion of a cohort from another 22q11.2DS center increased power to observe a significantly earlier diagnosis for patients born in the molecular testing era. Nonetheless, only a minority were diagnosed in the first year of life. On average, patients were seen in seven (range 2–15) different clinical specialty areas prior to molecular diagnosis. The findings indicate that even for those born in the molecular testing era, individuals with 22q11.2DS and their families face a diagnostic odyssey that is often prolonged, particularly in the absence of typical physical congenital features or for those of non-European ancestry. The results support educational efforts to improve clinical recognition and testing, and ultimately newborn screening as a means of maximizing early detection that would provide the best opportunity to optimize outcomes.

Published

2018