Your search keyword '"Badduke C"' showing total 6 results

1. Prevalence estimate of sphingosine phosphate lyase insufficiency syndrome in worldwide and select populations.

Author

Sedillo JC, Badduke C, Schrodi SJ, Scaria V, Onat OE, Alfadhel M, Ober C, Wentworth-Sheilds W, Steiner RD, and Saba JD

Abstract

Purpose: Sphingosine phosphate lyase insufficiency syndrome (SPLIS) is a rare, often fatal, metabolic disorder and monogenic form of steroid-resistant nephrotic syndrome. Other manifestations include primary adrenal insufficiency, ichthyosis, and neurological defects. SPLIS is caused by biallelic pathogenic variants in SGPL1 , encoding sphingosine-1-phosphate lyase, a pyridoxal 5'-phosphate-dependent enzyme that catalyzes the final step of sphingolipid metabolism. Treatment is primarily supportive, but pyridoxine supplementation may be therapeutic in some cases, and gene therapy is being explored. We sought to determine the prevalence of SPLIS globally and among different populations to facilitate patient finding in anticipation of SPLIS clinical trials., Methods: Using publicly available genomic data sets, including Genome Aggregation Database (gnomAD) v.2.1.1 and gnomAD v3.1.2, Iranome, IndiGen, and private genomic data sets from Israeli, Saudi, South Dakota Hutterite, and Turkish populations, we estimated SPLIS prevalence based on cumulative variant allele frequencies for high-confidence pathogenic variants. SPLIS prevalence estimates were adjusted by the level of inbreeding when the inbreeding coefficient was known. A Bayesian point estimate and 95% credible interval for worldwide SPLIS were calculated based on gnomAD v2.1.1 (GRCh37)., Results: The SPLIS prevalence estimate based on the total number of samples included from gnomAD v.2.1.1 ( n  = 141,430) was 0.015/100,000 (95% CI: 0.010 to 0.021). Using additional population data sets, we calculated SPLIS prevalence ranging from 0.046/100,000 to 0.078/100,000 in Turkish and Iranian populations, respectively., Conclusion: The estimated worldwide number of SPLIS individuals is 11,707. Individuals with East Asian, Finnish, Turkish, and Iranian ancestries have an especially high estimated prevalence., Competing Interests: R.D.S. has equity interest in and has received consulting fees from Acer Therapeutics and PTC Therapeutics. He has received consulting fees from Aeglea BioTherapeutics; Best Doctors/Teladoc; Health Advances LLC; Leadiant, and Travere Therapeutics, Inc; and honoraria from Medscape/WebMD LLC and The France Foundation. He is an employee of and has equity interest in PreventionGenetics, part of Exact Sciences. He received research funding from Alexion Pharmaceuticals, Children’s Mercy Research Institute, and the Smith Lemli Opitz Foundation. J.D.S. is an author on patent “AAV-SPL as a treatment for SPLIS: International Application Serial No. PCT/US2021/018613,” “Adeno-Associated Viral (Aav)-Mediated Sgpl1 Gene Therapy for Treatment of Sphingosine-1-Phosphate Lyase Insufficiency Syndrome (SPLIS)” published on 08/26/2021 and assigned publication number WO 2021/168140. All other authors declare no conflicts of interest., (© 2023 The Authors.)

Published

2023

2. Comprehensive characterization of a Canadian cohort of von Hippel-Lindau disease patients.

Author

Salama Y, Albanyan S, Szybowska M, Bullivant G, Gallinger B, Giles RH, Asa S, Badduke C, Chiorean A, Druker H, Ezzat S, Hannah-Shmouni F, Hernandez KG, Inglese C, Jani P, Kaur Y, Krema H, Krimus L, Laperriere N, Lichner Z, Mete O, Sit M, Zadeh G, Jewett MAS, Malkin D, Stockley T, Wasserman JD, Xu W, Schachter NF, and Kim RH

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Canada epidemiology, Central Nervous System metabolism, Central Nervous System pathology, Child, Child, Preschool, Female, Hemangioblastoma epidemiology, Hemangioblastoma pathology, Humans, Male, Middle Aged, Mutation, Missense genetics, Pedigree, Penetrance, Pheochromocytoma epidemiology, Pheochromocytoma pathology, Young Adult, von Hippel-Lindau Disease epidemiology, von Hippel-Lindau Disease pathology, Hemangioblastoma genetics, Pheochromocytoma genetics, Von Hippel-Lindau Tumor Suppressor Protein genetics, von Hippel-Lindau Disease genetics

Abstract

Von Hippel-Lindau disease (VHL) is a heritable condition caused by pathogenic variants in VHL and is characterized by benign and malignant lesions in the central nervous system (CNS) and abdominal viscera. Due to its variable expressivity, existing efforts to collate VHL patient data do not adequately capture all VHL manifestations. We developed a comprehensive and standardized VHL database in the web-based application, REDCap, that thoroughly captures all VHL manifestation data. As an initial trial, information from 86 VHL patients from the University Health Network/Hospital for Sick Children was populated into the database. Analysis of this cohort showed missense variants occurring with the greatest frequency, with all variants localizing to the α- or β-domains of VHL. The most prevalent manifestations were central nervous system (CNS), renal, and retinal neoplasms, which were associated with frameshift variants and large deletions. We observed greater age-related penetrance for CNS hemangioblastomas with truncating variants compared to missense, while the reverse was true for pheochromocytomas. We demonstrate the utility of a comprehensive VHL database, which supports the standardized collection of clinical and genetic data specific to this patient population. Importantly, we expect that its web-based design will facilitate broader international collaboration and lead to a better understanding of VHL., (© 2019 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2019

3. Exome sequencing identified a de novo mutation of PURA gene in a patient with familial Xp22.31 microduplication.

Author

Qiao Y, Bagheri H, Tang F, Badduke C, Martell S, Lewis SME, Robinson W, Connolly MB, Arbour L, and Rajcan-Separovic E

Subjects

Child, Craniofacial Abnormalities pathology, Developmental Disabilities pathology, Genetic Diseases, X-Linked pathology, Heterozygote, Humans, Male, Mutation, Missense, Syndrome, Chromosome Duplication, Chromosomes, Human, X genetics, Craniofacial Abnormalities genetics, DNA-Binding Proteins genetics, Developmental Disabilities genetics, Genetic Diseases, X-Linked genetics, Phenotype, Transcription Factors genetics

Abstract

The clinical significance of Xp22.31 microduplication is controversial as it is reported in subjects with developmental delay (DD), their unaffected relatives and unrelated controls. We performed multifaceted studies in a family of a boy with hypotonia, dysmorphic features and DD who carried a 600 Kb Xp22.31 microduplication (7515787-8123310bp, hg19) containing two genes, VCX and PNPLA4. The duplication was transmitted from his cognitively normal maternal grandfather. We found no evidence of the duplication causing the proband's DD and congenital anomalies based on unaltered expression of PNPLA4 in the proband and his mother in comparison to controls and preferential activation of the paternal chromosome X with Xp22.31 duplication in proband's mother. However, a de novo, previously reported deleterious, missense mutation in Pur-alpha gene (PURA) (5q31.2), with a role in neuronal differentiation was detected in the proband by exome sequencing. We propose that the variability in the phenotype in carriers of Xp22.31 microduplication can be due to a second and more deleterious genetic mutation in more severely affected carriers. Widespread use of whole genome next generation sequencing in families with Xp22.31 CNV could help identify such cases., (Copyright © 2018. Published by Elsevier Masson SAS.)

Published

2019

4. Whole exome sequencing of families with 1q21.1 microdeletion or microduplication.

Author

Qiao Y, Badduke C, Tang F, Cowieson D, Martell S, Lewis SME, Peñaherrera MS, Robinson WP, Volchuk A, and Rajcan-Separovic E

Abstract

Recurrent microduplications/microdeletions of 1q21.1 are characterized by variable phenotypes ranging from normal development to developmental delay (DD) and congenital anomalies. Their interpretation is challenging especially in families with affected and unaffected carriers. We used whole exome sequencing (WES) to look for sequence variants in two male probands with inherited 1q21.1 CNVs that could explain their more severe phenotypes. One proband had a 1q21.1 deletion transmitted from maternal grandmother, while the other had a paternal duplication. We found mutations in five genes (SMPD1, WNK3, NOS1, ATF6, and EFHC1) that could contribute to the more severe phenotype in the probands in comparison to their mildly affected or unaffected 1q21.1 CNV carrying relatives. Interestingly, all genes have roles in stress responses (oxidative/Endoplasmic Reticulum (ER)/osmotic). One of the variants was in an X-linked gene WNK3 and segregated with the developmental features and X inactivation pattern in the family with 1q21.1 deletion transmitted from maternal grandmother. In silico analysis of all rare deleterious variants in both probands identified enrichment in nervous system diseases, metabolic pathways, protein processing in the ER and protein export. Our studies suggest that rare deleterious variants outside of the 1q21.1 CNV, individually or as a pool, could contribute to phenotypic variability in carriers of this CNV. Rare deleterious variants in stress response genes are of interest and raise the possibility of susceptibility of carriers to variable environmental influences. Next generation sequencing of additional familial cases with 1q21.1 CNV could further help determine the possible causes of phenotypic variability in carriers of this CNV., (© 2017 Wiley Periodicals, Inc.)

Published

2017

5. Identifying candidate genes for 2p15p16.1 microdeletion syndrome using clinical, genomic, and functional analysis.

Author

Bagheri H, Badduke C, Qiao Y, Colnaghi R, Abramowicz I, Alcantara D, Dunham C, Wen J, Wildin RS, Nowaczyk MJ, Eichmeyer J, Lehman A, Maranda B, Martell S, Shan X, Lewis SM, O'Driscoll M, Gregory-Evans CY, and Rajcan-Separovic E

Subjects

Adolescent, Animals, Carrier Proteins genetics, Child, Child, Preschool, Developmental Disabilities genetics, Female, Gene Knockdown Techniques, Humans, Infant, Karyopherins genetics, Male, Microcephaly genetics, Nuclear Proteins genetics, Proto-Oncogene Proteins c-rel genetics, Receptors, Cytoplasmic and Nuclear genetics, Repressor Proteins, Zebrafish, Exportin 1 Protein, Abnormalities, Multiple genetics, Chromosome Deletion, Chromosome Disorders genetics, Chromosomes, Human, Pair 2 genetics

Abstract

The 2p15p16.1 microdeletion syndrome has a core phenotype consisting of intellectual disability, microcephaly, hypotonia, delayed growth, common craniofacial features, and digital anomalies. So far, more than 20 cases of 2p15p16.1 microdeletion syndrome have been reported in the literature; however, the size of the deletions and their breakpoints vary, making it difficult to identify the candidate genes. Recent reports pointed to 4 genes ( XPO1 , USP34 , BCL11A , and REL ) that were included, alone or in combination, in the smallest deletions causing the syndrome. Here, we describe 8 new patients with the 2p15p16.1 deletion and review all published cases to date. We demonstrate functional deficits for the above 4 candidate genes using patients' lymphoblast cell lines (LCLs) and knockdown of their orthologs in zebrafish. All genes were dosage sensitive on the basis of reduced protein expression in LCLs. In addition, deletion of XPO1 , a nuclear exporter, cosegregated with nuclear accumulation of one of its cargo molecules (rpS5) in patients' LCLs. Other pathways associated with these genes (e.g., NF-κB and Wnt signaling as well as the DNA damage response) were not impaired in patients' LCLs. Knockdown of xpo1a , rel , bcl11aa , and bcl11ab resulted in abnormal zebrafish embryonic development including microcephaly, dysmorphic body, hindered growth, and small fins as well as structural brain abnormalities. Our multifaceted analysis strongly implicates XPO1 , REL , and BCL11A as candidate genes for 2p15p16.1 microdeletion syndrome.

Published

2016

6. miRNA and miRNA target genes in copy number variations occurring in individuals with intellectual disability.

Author

Qiao Y, Badduke C, Mercier E, Lewis SM, Pavlidis P, and Rajcan-Separovic E

Subjects

Case-Control Studies, Cognition, Databases, Genetic, Female, Humans, Intellectual Disability physiopathology, Male, DNA Copy Number Variations genetics, Genomics, Intellectual Disability genetics, MicroRNAs genetics

Abstract

Background: MicroRNAs (miRNAs) are a family of short, non-coding RNAs modulating expression of human protein coding genes (miRNA target genes). Their dysfunction is associated with many human diseases, including neurodevelopmental disorders. It has been recently shown that genomic copy number variations (CNVs) can cause aberrant expression of integral miRNAs and their target genes, and contribute to intellectual disability (ID)., Results: To better understand the CNV-miRNA relationship in ID, we investigated the prevalence and function of miRNAs and miRNA target genes in five groups of CNVs. Three groups of CNVs were from 213 probands with ID (24 de novo CNVs, 46 familial and 216 common CNVs), one group of CNVs was from a cohort of 32 cognitively normal subjects (67 CNVs) and one group of CNVs represented 40 ID related syndromic regions listed in DECIPHER (30 CNVs) which served as positive controls for CNVs causing or predisposing to ID. Our results show that 1). The number of miRNAs is significantly higher in de novo or DECIPHER CNVs than in familial or common CNV subgroups (P < 0.01). 2). miRNAs with brain related functions are more prevalent in de novo CNV groups compared to common CNV groups. 3). More miRNA target genes are found in de novo, familial and DECIPHER CNVs than in the common CNV subgroup (P < 0.05). 4). The MAPK signaling cascade is found to be enriched among the miRNA target genes from de novo and DECIPHER CNV subgroups., Conclusions: Our findings reveal an increase in miRNA and miRNA target gene content in de novo versus common CNVs in subjects with ID. Their expression profile and participation in pathways support a possible role of miRNA copy number change in cognition and/or CNV-mediated developmental delay. Systematic analysis of expression/function of miRNAs in addition to coding genes integral to CNVs could uncover new causes of ID.

Published

2013