Your search keyword '"Robert B. Hufnagel"' showing total 9 results

1. Homozygous missense variant in BMPR1A resulting in BMPR signaling disruption and syndromic features

Author

Bianca E. Russell, Diana Rigueur, Kathryn N. Weaver, Kristen Sund, Janet S. Basil, Robert B. Hufnagel, Cynthia A. Prows, Alan Oestreich, Lihadh Al‐Gazali, Robert J Hopkin, Howard M. Saal, Karen Lyons, and Andrew Dauber

Subjects

atrial septal defect, BMP, bmpr1a protein, bone morphogenetic protein, human, Genetics, QH426-470

Abstract

Abstract Background The bone morphogenetic protein (BMP) pathway is known to play an imperative role in bone, cartilage, and cardiac tissue formation. Truncating, heterozygous variants, and deletions of one of the essential receptors in this pathway, Bone Morphogenetic Protein Receptor Type1A (BMPR1A), have been associated with autosomal dominant juvenile polyposis. Heterozygous deletions have also been associated with cardiac and minor skeletal anomalies. Populations with atrioventricular septal defects are enriched for rare missense BMPR1A variants. Methods We report on a patient with a homozygous missense variant in BMPR1A causing skeletal abnormalities, growth failure a large atrial septal defect, severe subglottic stenosis, laryngomalacia, facial dysmorphisms, and developmental delays. Results Functional analysis of this variant shows increased chondrocyte death for cells with the mutated receptor, increased phosphorylated R‐Smads1/5/8, and loss of Sox9 expression mediated by decreased phosphorylation of p38. Conclusion This homozygous missense variant in BMPR1A appears to cause a distinct clinical phenotype.

Published

2019

2. Variants of <scp> LRP2 </scp> , encoding a multifunctional cell‐surface endocytic receptor, associated with hearing loss and retinal dystrophy

Author

Rabia Faridi, Rizwan Yousaf, Shoujun Gu, Sayaka Inagaki, Amy E. Turriff, Keith Pelstring, Bin Guan, Amelia Naik, Andrew J. Griffith, Samuel Mawuli Adadey, Elvis Twumasi Aboagye, Gordon A. Awandare, Robert J. Morell, Ekaterini Tsilou, Amanda G. Noyes, Laura A. G. Sulmonte, Ambroise Wonkam, Isabelle Schrauwen, Suzanne M. Leal, Hela Azaiez, Carmen C. Brewer, Sheikh Riazuddin, Robert B. Hufnagel, Michael Hoa, Wadih M. Zein, J. Karl de Dios, and Thomas B. Friedman

Subjects

Genetics, Genetics (clinical)

Published

2023

3. A de novo hexokinase 1 ( <scp> HK1 </scp> ) variant presenting as <scp>Boucher–Neuhäuser</scp> syndrome

Author

Ryan H. Peretz, Wadih M. Zein, Robert B. Hufnagel, Christine Ku, Rena Godfrey, Lynne Wolfe, David Adams, William Gahl, and Camilo Toro

Subjects

Genetics, Genetics (clinical)

Abstract

Boucher-Neuhäuser syndrome (BNHS) is characterized by chorioretinal dystrophy, hypogonadotropic hypogonadism, and cerebellar dysfunction and atrophy. The disorder has been associated with biallelic pathogenic variants in the patatin-like phospholipase domain-containing protein 6 (PNPLA6) gene. We present an individual with a clinical diagnosis consistent with BNHS who lacked any PNPLA6 variants but on quartet family exome sequencing had a de novo variant in the hexokinase 1 (HK1) gene (NM_000188.2 [GRCh37/hg19]: g.71139826GA, c.1240GA, p.Gly414Arg), suggesting genetic heterogeneity for BNHS. Longitudinal follow-up indicated neurological deterioration, neuropsychiatric symptoms, and progressive cerebellar atrophy. The BNHS phenotype overlaps and expands the known HK1 genotypic and phenotypic spectrum. Individuals with variants in HK1 should undergo evaluation for hypogonadotropic hypogonadism, potentially amenable to treatment.

Published

2022

4. Auditory and olfactory findings in patients with <scp> USH2A </scp> ‐related retinal degeneration—Findings at baseline from the rate of progression in <scp> USH2A </scp> ‐related retinal degeneration natural history study ( <scp>RUSH2A</scp> )

Author

Paul S. Bernstein, Wadih M. Zein, Katarina Stingl, Isabelle Audo, Alessandro Iannaccone, Richard L. Doty, Gavin M. Bidelman, Mark H. Myers, Janet K. Cheetham, Carmen C. Brewer, Todd Durham, Jacque L. Duncan, Robert B. Hufnagel, Peiyao Cheng, Allison R Ayala, and Maureen G. Maguire

Subjects

Retinal degeneration, education.field_of_study, medicine.medical_specialty, Hearing loss, business.industry, Usher syndrome, Population, Olfaction, Audiology, medicine.disease, eye diseases, otorhinolaryngologic diseases, Genetics, medicine, Sensorineural hearing loss, Autosomal recessive retinitis pigmentosa, medicine.symptom, education, business, Genetics (clinical), Natural history study

Abstract

Sensorineural hearing loss (SNHL) is characteristic of Usher syndrome type 2 (USH2), but less is known about SNHL in nonsyndromic autosomal recessive retinitis pigmentosa (ARRP) and olfaction in USH2A-associated retinal degeneration. The Rate of Progression of USH2A-related Retinal Degeneration (RUSH2A) is a natural history study that enrolled 127 participants, 80 with USH2 and 47 with ARRP. Hearing was measured by pure-tone thresholds and word recognition scores, and olfaction by the University of Pennsylvania Smell Identification Test (UPSIT). SNHL was moderate in 72% of USH2 participants and severe or profound in 25%, while 9% of ARRP participants had moderate adult-onset SNHL. Pure-tone thresholds worsened with age in ARRP but not in USH2 participants. The degree of SNHL was not associated with other participant characteristics in either USH2 or ARRP. Median pure-tone thresholds in ARRP participants were significantly higher than the normative population (p < 0.001). Among 14 USH2 participants reporting newborn hearing screening results, 7 reported passing. Among RUSH2A participants, 7% had mild microsmia and 5% had moderate or severe microsmia. Their mean (±SD) UPSIT score was 35 (±3), similar to healthy controls (34 [±3]; p = 0.39). Olfaction differed by country (p = 0.02), but was not significantly associated with clinical diagnosis, age, gender, race/ethnicity, smoking status, visual measures, or hearing. Hearing loss in USH2A-related USH2 did not progress with age. ARRP patients had higher pure-tone thresholds than normal. Newborn hearing screening did not identify all USH2A-related hearing loss. Olfaction was not significantly worse than normal in participants with USH2A-related retinal degeneration.

Published

2021

5. Systemic and ocular manifestations of a patient with mosaic<scp>ARID1A‐</scp>a<scp>ssociated Coffin‐Siris</scp>syndrome and review of select mosaic conditions with ophthalmic manifestations

Author

Robert B. Hufnagel, Monica A Sandoval, Virginia Miraldi Utz, Howard M. Saal, and Diana S Brightman

Subjects

Male, Pathology, medicine.medical_specialty, Micrognathism, Cortical visual impairment, Disease, Article, Intellectual Disability, Genetics, medicine, Humans, Abnormalities, Multiple, Genetic Predisposition to Disease, Medical history, Global developmental delay, Child, Coffin–Siris syndrome, Genetics (clinical), Polydactyly, Mosaicism, business.industry, Macrocephaly, Brain, Infant, Nuclear Proteins, medicine.disease, eye diseases, Hypotonia, DNA-Binding Proteins, Phenotype, Child, Preschool, Face, Mutation, Female, medicine.symptom, business, Hand Deformities, Congenital, Neck, Transcription Factors

Abstract

Mosaic genetic mutations may be somatic, germline, or “gonosomal” and have the potential to cause genetic syndromes, disorders, or malformations. Mutations can occur at any point in embryonic development and the timing determines the extent of distribution of the mutation throughout the body and different tissue types. The eye and visual pathway offer a unique opportunity to study somatic and gonosomal mosaic mutations as the eye consists of tissues derived from all three germ layers allowing disease pathology to be assessed with noninvasive imaging. In this review, we describe systemic and ocular manifestations in a child with mosaic Coffin-Siris syndrome. The patient presented with a significant medical history of accommodative esotropia and hyperopia, macrocephaly, polydactyly, global developmental delay, hypotonia, ureteropelvic junction (UPJ) obstruction, and brain MRI abnormalities. The ophthalmic findings in this patient were nonspecific, however, they are consistent with ocular manifestations reported in other patients with Coffin-Siris syndrome. We also review ophthalmic findings of select mosaic chromosomal and single-gene disorders. Ophthalmic assessment alongside clinical genetic testing may play an important role in diagnosis of genetic syndromes as well as understanding disease pathology, particularly when mosaicism plays a role.

Published

2020

6. Ocular genetics in the genomics age

Author

Michael A. Walter, Tayebeh Rezaie, Gavin Arno, and Robert B. Hufnagel

Subjects

Genetics, Phenocopy, Genome, Human, Inheritance (genetic algorithm), Eye Diseases, Hereditary, Genomics, Biology, Article, Ophthalmology, Exon, symbols.namesake, Missing heritability problem, Mendelian inheritance, symbols, Humans, Exome, Gene, Genetics (clinical)

Abstract

Current genetic screening methods for inherited eye diseases are concentrated on the coding exons of known disease genes (gene panels, clinical exome). These tests have a variable and often limited diagnostic rate depending on the clinical presentation, size of the gene panel and our understanding of the inheritance of the disorder (with examples described in this issue). There are numerous possible explanations for the missing heritability of these cases including undetected variants within the relevant gene (intronic, up/down-stream and structural variants), variants harbored in genes outside the targeted panel, intergenic variants, variants undetectable by the applied technology, complex/non-Mendelian inheritance, and nongenetic phenocopies. In this article we further explore and review methods to investigate these sources of missing heritability.

Published

2020

7. Novel progressive <scp>acrodysostosis‐like</scp> skeletal dysplasia, cerebellar atrophy, and ichthyosis

Author

Harvy Velasco, Robert B. Hufnagel, Angela M. Martin, Carlos E. Prada, and Ehsan Ullah

Subjects

Adult, Heterozygote, Pathology, medicine.medical_specialty, Ataxia, Adolescent, Developmental Disabilities, Acrodysostosis, Mutation, Missense, Nervous System Malformations, Osteochondrodysplasias, Article, Young Adult, Cerebellum, Intellectual Disability, Exome Sequencing, Phosphoprotein Phosphatases, Genetics, Humans, Medicine, Child, Cerebellar hypoplasia, Genetics (clinical), Exome sequencing, Cerebellar ataxia, business.industry, Ichthyosis, Calcium-Binding Proteins, Dysostoses, Middle Aged, Lamellar ichthyosis, medicine.disease, Musculoskeletal Abnormalities, Child, Preschool, Female, Cerebellar atrophy, Atrophy, medicine.symptom, business, Epiphyses

Abstract

Acrodysostosis refers to a rare heterogeneous group of bone dysplasias that share skeletal features, hormone resistance, and intellectual disability. Two genes have been associated with acrodysostosis with or without hormone resistance (PRKAR1A and PDE4D). Severe intellectual disability has been reported with acrodysostosis but brain malformations and ichthyosis have not been reported in these syndromes. Here we describe a female patient with acrodysostosis, intellectual disability, cerebellar hypoplasia, and lamellar ichthyosis. The patient has an evolving distinctive facial phenotype and childhood onset ataxia. X-rays showed generalized osteopenia, shortening of middle and distal phalanges, and abnormal distal epiphysis of the ulna and radius. Brain magnetic resonance imaging showed cerebellar atrophy without other brainstem abnormalities. Genetic workup included nondiagnostic chromosomal microarray and skeletal dysplasia molecular panels. These clinical findings are different from any recognized form of acrodysostosis syndrome. Whole exome sequencing did not identify rare or predicted pathogenic variants in genes associated with known acrodysostosis, lamellar ichthyosis, and other overlapping disorders. A broader search for rare alleles absent in healthy population databases and controls identified two heterozygous truncating alleles in FBNL7 and PPM1M genes, and one missense allele in the NPEPPS gene. Identification of additional patients is required to delineate the mechanism of this unique disorder.

Published

2020

8. A novelCHST3allele associated with spondyloepiphyseal dysplasia and hearing loss in Pakistani kindred

Author

Ali Muhammad Waryah, Saima Riazuddin, Zubair M. Ahmed, Shakeel A. Sheikh, Robert B. Hufnagel, Asadullah Makhdoom, Naseem Aslam Channa, Hina Shaikh, and Mohsin Shahzad

Subjects

0301 basic medicine, Spondyloepiphyseal dysplasia, Genetics, Pediatrics, medicine.medical_specialty, business.industry, Hearing loss, Consanguinity, medicine.disease, Short stature, 03 medical and health sciences, 030104 developmental biology, medicine, Joint dislocation, medicine.symptom, business, Kyphoscoliosis, Exome, Genetics (clinical), Exome sequencing

Abstract

Skeletal dysplasias (SDs) are highly heterogeneous disorders composed of 40 clinical sub-types that are part of 456 well-delineated syndromes in humans. Here, we enrolled consanguineous kindred from a remote area of Sindh province of Pakistan, with 14 affected individuals suffering with short stature, kyphoscoliosis, joint dislocations, clubfoot, heart valve anomalies and progressive bilateral mixed hearing loss. To identify pathogenic variants in this family, whole exome sequencing (WES) was performed in one affected and one normal individual, which revealed a novel transversion mutation (c.802G>T; p.Glu268*) in CHST3 associated with the phenotype. CHST3 encodes a chondroitin 6-O-sulfotransferase-1 (C6ST-1) enzyme that is essential for the sulfation of proteoglycans found in cartilages. Previously, mutations in CHST3 have largely been reported in sporadic cases of SD, primarily with severe spinal abnormalities, joint dislocations, joint contractures, and clubfoot. Clinical and radiological examination of the affected individuals in this family provides new insights into phenotypic spectrum of CHST3 alleles and disease progression with age.

Published

2015

9. A novel dominant COL11A1 mutation resulting in a severe skeletal dysplasia

Author

Robert B. Hufnagel, Patricia I. Bader, K. Nicole Weaver, Sophia B. Hufnagel, Elizabeth K. Schorry, and Robert J. Hopkin

Subjects

Pathology, medicine.medical_specialty, Germline mosaicism, Biology, Collagen Type XI, Article, Myopia, Genetics, medicine, Humans, Severe Myopia, Hearing Loss, Genetics (clinical), Bone Diseases, Developmental, Genetic heterogeneity, Brachydactyly, medicine.disease, Musculoskeletal Abnormalities, Pedigree, Dysplasia, Micromelia, Mutation, Mutation (genetic algorithm), Female, Fibrochondrogenesis

Abstract

Mutations in the type XI collagen alpha-1 chain gene (COL11A1) cause a change in protein structure that alters its interactions with collagens II and V, resulting in abnormalities in cartilage and ocular vitreous. The most common type XI collagenopathies are dominantly inherited Stickler or Marshall syndromes, while severe recessive skeletal dysplasias, such as fibrochondrogenesis, occur less frequently. We describe a family with a severe skeletal dysplasia caused by a novel dominantly inherited COL11A1 mutation. The siblings each presented with severe myopia, hearing loss, micromelia, metaphyseal widening of the long bones, micrognathia, and airway compromise requiring tracheostomy. The first child lived for over 2 years, while the second succumbed at 5 months of age. Their mother has mild rhizomelic shortening of the limbs, brachydactyly, and severe myopia. Sequencing of COL11A1 revealed a novel deleterious heterozygous mutation in COL11A1 involving the triple helical domain in both siblings, and a mosaic mutation in their mother, indicating germline mosaicism with subsequent dominant inheritance. These are the first reported individuals with a dominantly inherited mutation in COL11A1 associated with a severe skeletal dysplasia. The skeletal involvement is similar to, yet milder than fibrochondrogenesis and allowed for survival beyond the perinatal period. These cases highlight both a novel dominant COL11A1 mutation causing a significant skeletal dysplasia and the phenotypic heterogeneity of collagenopathies.

Published

2014