Your search keyword '"J. Fielding Hejtmancik"' showing total 215 results

1. Clinical and genetic risk factors underlying severe consequence identified in 75 families with unilateral high myopia

Author

Yi Jiang, Xueshan Xiao, Wenmin Sun, Yingwei Wang, Shiqiang Li, Xiaoyun Jia, Panfeng Wang, J. Fielding Hejtmancik, and Qingjiong Zhang

Subjects

Unilateral high myopia, Genetic, Peripheral retinal examination, Anisometropia, High myopia, Medicine

Abstract

Abstract Backgrounds Unilateral high myopia (uHM), commonly observed in patients with retinal diseases or only with high myopia, is frequently associated with amblyopia with poor prognosis. This study aims to reveal the clinical and genetic spectrum of uHM in a large Chinese cohort. Methods A total of 75 probands with simplex uHM were included in our Pediatric and Genetic Eye Clinic. Patients with significant posterior anomalies other than myopic fundus changes were excluded. Variants were detected by exome sequencing and then analyzed through multiple-step bioinformatic and co-segregation analysis and finally confirmed by Sanger sequencing. Genetic findings were correlated with associated clinical data for analysis. Results Among the 75 probands with a mean age of 6.21 ± 4.70 years at the presentation, myopic fundus of C1 and C2 was observed in 73 (97.3%) probands. Surprisingly, specific peripheral changes were identified in 63 eyes involving 36 (48.0%) probands after extensive examination, including peripheral retinal avascular zone (74.6%, 47/63 eyes), neovascularization (54.0%), fluorescein leakage (31.7%), peripheral pigmentary changes (31.7%), and others. Exome sequencing identified 21 potential pathogenic variants of 13 genes in 20 of 75 (26.7%) probands, including genes for Stickler syndrome (COL11A1 and COL2A1; 6/20), FEVR (FZD4, LRP5, and TSPAN12; 5/20), and others (FBN1, GPR179, ZEB2, PAX6, GPR143, OPN1LW, FRMD7, and CACNA1F; 9/20). For the peripheral retinal changes in the 20 probands, variants in Stickler syndrome-related genes were predominantly associated with retinal pigmentary changes, lattice degeneration, and retinal avascular region, while variants in genes related to FEVR were mainly associated with the avascular zone, neovascularization, and fluorescein leakage. Conclusions Genetic defects were identified in about one-fourth of simplex uHM patients in which significant consequences may be hidden under a classic myopic fundus in up to half. To our knowledge, this is the first systematic genetic study on simplex uHM to date. In addition to routine care of strabismus and amblyopia, careful examination of the peripheral retina and genetic screening is warranted for patients with uHM in order to identify signs of risk for retinal detachment and other complications and provide meaningful genetic counseling.

Published

2024

2. Next-generation whole exome sequencing to delineate the genetic basis of primary congenital glaucoma

Author

Bushra Rauf, Shahid Y. Khan, Xiaodong Jiao, Bushra Irum, Ramla Ashfaq, Mubashra Zehra, Asma A. Khan, Muhammad Asif Naeem, Mohsin Shahzad, Sheikh Riazuddin, J. Fielding Hejtmancik, and S. Amer Riazuddin

Subjects

Medicine, Science

Abstract

Abstract To delineate the genetic bases of primary congenital glaucoma (PCG), we ascertained a large cohort consisting of 48 consanguineous families. Of these, we previously reported 26 families with mutations in CYP1B1 and six families with LTBP2, whereas the genetic bases responsible for PCG in 16 families remained elusive. We employed next-generation whole exome sequencing to delineate the genetic basis of PCG in four of these 16 familial cases. Exclusion of linkage to reported PCG loci was established followed by next-generation whole exome sequencing, which was performed on 10 affected individuals manifesting cardinal systems of PCG belonging to four unresolved families along with four control samples consisting of genomic DNAs of individuals harboring mutations in CYP1B1 and LTBP2. The analyses of sequencing datasets failed to identify potential causal alleles in the 10 exomes whereas c.1169G > A (p. Arg390His) in CYP1B1 and c.3427delC (p.Gln1143Argfs*35) in LTBP2 were identified in the control samples. Taken together, next-generation whole exome sequencing failed to delineate the genetic basis of PCG in familial cases excluded from mutations in CYP1B1 and LTBP2. These data strengthen the notion that compound heterozygous coding variants or non-coding variants might contribute to PCG.

Published

2022

3. SARS-CoV-2 ORF3A interacts with the Clic-like chloride channel-1 (CLCC1) and triggers an unfolded protein response

Author

Hannah N. Gruner, Yaohuan Zhang, Kaavian Shariati, Nicholas Yiv, Zicheng Hu, Yuhao Wang, J. Fielding Hejtmancik, Michael T. McManus, Kevin Tharp, and Gregory Ku

Subjects

COVID-19, SARS-CoV-2, CLCC1, Unfolded protein response, Medicine, Biology (General), QH301-705.5

Abstract

Understanding the interactions between SARS-CoV-2 and host cell machinery may reveal new targets to treat COVID-19. We focused on an interaction between the SARS-CoV-2 ORF3A accessory protein and the CLIC-like chloride channel-1 (CLCC1). We found that ORF3A partially co-localized with CLCC1 and that ORF3A and CLCC1 could be co-immunoprecipitated. Since CLCC1 plays a role in the unfolded protein response (UPR), we hypothesized that ORF3A may also play a role in the UPR. Indeed, ORF3A expression triggered a transcriptional UPR that was similar to knockdown of CLCC1. ORF3A expression in 293T cells induced cell death and this was rescued by the chemical chaperone taurodeoxycholic acid (TUDCA). Cells with CLCC1 knockdown were partially protected from ORF3A-mediated cell death. CLCC1 knockdown upregulated several of the homeostatic UPR targets induced by ORF3A expression, including HSPA6 and spliced XBP1, and these were not further upregulated by ORF3A. Our data suggest a model where CLCC1 silencing triggers a homeostatic UPR that prevents cell death due to ORF3A expression.

Published

2023

4. Changes in DNA methylation hallmark alterations in chromatin accessibility and gene expression for eye lens differentiation

Author

Joshua Disatham, Lisa Brennan, Xiaodong Jiao, Zhiwei Ma, J. Fielding Hejtmancik, and Marc Kantorow

Subjects

DNA methylation, Bisulfite sequencing, RNA-seq, ATAC-seq, Lens, Differentiation, Genetics, QH426-470

Abstract

Abstract Background Methylation at cytosines (mCG) is a well-known regulator of gene expression, but its requirements for cellular differentiation have yet to be fully elucidated. A well-studied cellular differentiation model system is the eye lens, consisting of a single anterior layer of epithelial cells that migrate laterally and differentiate into a core of fiber cells. Here, we explore the genome-wide relationships between mCG methylation, chromatin accessibility and gene expression during differentiation of eye lens epithelial cells into fiber cells. Results Whole genome bisulfite sequencing identified 7621 genomic loci exhibiting significant differences in mCG levels between lens epithelial and fiber cells. Changes in mCG levels were inversely correlated with the differentiation state-specific expression of 1285 genes preferentially expressed in either lens fiber or lens epithelial cells (Pearson correlation r = − 0.37, p

Published

2022

5. A genomic deletion encompassing CRYBB2-CRYBB2P1 is responsible for autosomal recessive congenital cataracts

Author

Bushra Irum, Firoz Kabir, Nadav Shoshany, Shahid Y. Khan, Bushra Rauf, Muhammad Asif Naeem, Tanveer A. Qaiser, Sheikh Riazuddin, J. Fielding Hejtmancik, and S. Amer Riazuddin

Subjects

Genetics, QH426-470, Life, QH501-531

Abstract

Abstract Here we report a consanguineous Pakistani family with multiple affected individuals with autosomal recessive congenital cataract (arCC). Exclusion analysis established linkage to chromosome 22q, and Sanger sequencing coupled with PCR-based chromosome walking identified a large homozygous genomic deletion. Our data suggest that this deletion leads to CRYBB2-CRYBB2P1 fusion, consisting of exons 1–5 of CRYBB2 and exon 6 of CRYBB2P1, the latter of which harbors the c.463 C > T (p.Gln155*) mutation, and is responsible for arCC.

Published

2022

6. CLCC1 c. 75C>A Mutation in Pakistani Derived Retinitis Pigmentosa Families Likely Originated With a Single Founder Mutation 2,000–5,000 Years Ago

Author

Yan Ma, Xun Wang, Nadav Shoshany, Xiaodong Jiao, Adrian Lee, Gregory Ku, Emma L. Baple, James Fasham, Raheela Nadeem, Muhammad Asif Naeem, Sheikh Riazuddin, S. Amer Riazuddin, Andrew H. Crosby, and J. Fielding Hejtmancik

Subjects

retinitis pigmenstosa, CLCC1, haplotype analysis, mutation age estimate, Pakistan, founder mutation, Genetics, QH426-470

Abstract

Background: A CLCC1 c. 75C > A (p.D25E) mutation has been associated with autosomal recessive pigmentosa in patients in and from Pakistan. CLCC1 is ubiquitously expressed, and knockout models of this gene in zebrafish and mice are lethal in the embryonic period, suggesting that possible retinitis pigmentosa mutations in this gene might be limited to those leaving partial activity. In agreement with this hypothesis, the mutation is the only CLCC1 mutation associated with retinitis pigmentosa to date, and all identified patients with this mutation share a common SNP haplotype surrounding the mutation, suggesting a common founder.Methods: SNPs were genotyped by a combination of WGS and Sanger sequencing. The original founder haplotype, and recombination pathways were delineated by examination to minimize recombination events. Mutation age was estimated by four methods including an explicit solution, an iterative approach, a Bayesian approach and an approach based solely on ancestral segment lengths using high density SNP data.Results: All members of each of the nine families studied shared a single autozygous SNP haplotype for the CLCC1 region ranging from approximately 1–3.5 Mb in size. The haplotypes shared by the families could be derived from a single putative ancestral haplotype with at most two recombination events. Based on the haplotype and Gamma analysis, the estimated age of the founding mutation varied from 79 to 196 generations, or approximately 2,000–5,000 years, depending on the markers used in the estimate. The DMLE (Bayesian) estimates ranged from 2,160 generations assuming a population growth rate of 0–309 generations assuming a population growth rate of 2% with broad 95% confidence intervals.Conclusion: These results provide insight into the origin of the CLCC1 mutation in the Pakistan population. This mutation is estimated to have occurred 2000–5,000 years ago and has been transmitted to affected families of Pakistani origin in geographically dispersed locations around the world. This is the only mutation in CLCC1 identified to date, suggesting that the CLCC1 gene is under a high degree of constraint, probably imposed by functional requirements for this gene during embryonic development.

Published

2022

7. Retinal Development and Pathophysiology in Kcnj13 Knockout Mice

Author

Xiaodong Jiao, Zhiwei Ma, Jingqi Lei, Pinghu Liu, Xiaoyu Cai, Pawan K. Shahi, Chi-Chao Chan, Robert Fariss, Bikash R. Pattnaik, Lijin Dong, and J. Fielding Hejtmancik

Subjects

retina, retinal dystrophy, snowflake vitreoretinal dystrophy, kcnj13/kir7.1, retinal degeneration, Biology (General), QH301-705.5

Abstract

Purpose: We constructed and characterized knockout and conditional knockout mice for KCNJ13, encoding the inwardly rectifying K+ channel of the Kir superfamily Kir7.1, mutations in which cause both Snowflake Vitreoretinal Degeneration (SVD) and Retinitis pigmentosa (RP) to further elucidate the pathology of this disease and to develop a potential model system for gene therapy trials.Methods: A Kcnj13 knockout mouse line was constructed by inserting a gene trap cassette expressing beta-galactosidase flanked by FRT sites in intron 1 with LoxP sites flanking exon two and converted to a conditional knockout by FLP recombination followed by crossing with C57BL/6J mice having Cre driven by the VMD2 promoter. Lentiviral replacement of Kcnj13 was driven by the EF1a or VMD2 promoters.Results: Blue-Gal expression is evident in E12.5 brain ventricular choroid plexus, lens, neural retina layer, and anterior RPE. In the adult eye expression is seen in the ciliary body, RPE and choroid. Adult conditional Kcnj13 ko mice show loss of photoreceptors in the outer nuclear layer, inner nuclear layer thinning with loss of bipolar cells, and thinning and disruption of the outer plexiform layer, correlating with Cre expression in the overlying RPE which, although preserved, shows morphological disruption. Fundoscopy and OCT show signs of retinal degeneration consistent with the histology, and photopic and scotopic ERGs are decreased in amplitude or extinguished. Lentiviral based replacement of Kcnj13 resulted in increased ERG c- but not a- or b- wave amplitudes.Conclusion: Ocular KCNJ13 expression starts in the choroid, lens, ciliary body, and anterior retina, while later expression centers on the RPE with no/lower expression in the neuroretina. Although KCNJ13 expression is not required for survival of the RPE, it is necessary for RPE maintenance of the photoreceptors, and loss of the photoreceptor, outer plexiform, and outer nuclear layers occur in adult KCNJ13 cKO mice, concomitant with decreased amplitude and eventual extinguishing of the ERG and signs of retinitis pigmentosa on fundoscopy and OCT. Kcnj13 replacement resulting in recovery of the ERG c- but not a- and b-waves is consistent with the degree of photoreceptor degeneration seen on histology.

Published

2022

8. Autophagy Requirements for Eye Lens Differentiation and Transparency

Author

Lisa Brennan, M. Joseph Costello, J. Fielding Hejtmancik, A. Sue Menko, S. Amer Riazuddin, Alan Shiels, and Marc Kantorow

Subjects

autophagy, lens, differentiation, cataract, Cytology, QH573-671

Abstract

Recent evidence points to autophagy as an essential cellular requirement for achieving the mature structure, homeostasis, and transparency of the lens. Collective evidence from multiple laboratories using chick, mouse, primate, and human model systems provides evidence that classic autophagy structures, ranging from double-membrane autophagosomes to single-membrane autolysosomes, are found throughout the lens in both undifferentiated lens epithelial cells and maturing lens fiber cells. Recently, key autophagy signaling pathways have been identified to initiate critical steps in the lens differentiation program, including the elimination of organelles to form the core lens organelle-free zone. Other recent studies using ex vivo lens culture demonstrate that the low oxygen environment of the lens drives HIF1a-induced autophagy via upregulation of essential mitophagy components to direct the specific elimination of the mitochondria, endoplasmic reticulum, and Golgi apparatus during lens fiber cell differentiation. Pioneering studies on the structural requirements for the elimination of nuclei during lens differentiation reveal the presence of an entirely novel structure associated with degrading lens nuclei termed the nuclear excisosome. Considerable evidence also indicates that autophagy is a requirement for lens homeostasis, differentiation, and transparency, since the mutation of key autophagy proteins results in human cataract formation.

Published

2023

9. Molecular Genetic Analysis of Ukrainian Families with Congenital Cataracts

Author

Xiaodong Jiao, Mariia Viswanathan, Nadiia Fedorivna Bobrova, Tatiana Viktorivna Romanova, and J. Fielding Hejtmancik

Subjects

lens, autosomal dominant congenital cataract, whole-exome sequencing, Pediatrics, RJ1-570

Abstract

This study was designed to identify the pathogenic variants in five Ukrainian families with autosomal dominant congenital cataracts. Cataracts can be defined broadly as any opacity of the crystalline lens. Lens development is orchestrated by transcription factors. Disease-causing variants in transcription factors and their developmental target genes, including the lens crystallins, are associated with congenital cataracts and other eye diseases. Whole-exome sequencing identified heterozygous disease-causing variants in five Ukrainian families with autosomal dominant congenital cataracts and cosegregation with cataracts was confirmed using Sanger sequencing. Family 97001 showed a missense variant (c.341T>A: p.L114Q) in HSF4; family 97003 showed a missense variant (c.53A>T: p.N18I) in CRYGA; family 97004 showed a missense variant (c. 82G>A: p.V28M) in GJA3; family 97006 showed a missense variant (c.83C>T: p. P28L) in CRYGC; and family 97008 showed a single-base insertion resulting in a frameshift (c.443_444insA: p. Met148IfsTer51) in PAX6. All five families are associated with congenital cataracts. Overall, we report four novel mutations in HSF4, CRYGA, CRYGC and PAX6, and one previously reported mutation in GJA3 that cause autosomal dominant congenital cataracts.

Published

2022

10. MITF protects against oxidative damage-induced retinal degeneration by regulating the NRF2 pathway in the retinal pigment epithelium

Author

Shuxian Han, Jianjun Chen, Jiajia Hua, Xiaojuan Hu, Shuhui Jian, Guoxiao Zheng, Jing Wang, Huirong Li, Jinglei Yang, J. Fielding Hejtmancik, Jia Qu, Xiaoyin Ma, and Ling Hou

Subjects

Antioxidant, Retinal degeneration, NRF2, RPE, MITF, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Oxidative damage is one of the major contributors to retinal degenerative diseases such as age-related macular degeneration (AMD), while RPE mediated antioxidant defense plays an important role in preventing retinopathies. However, the regulatory mechanisms of antioxidant signaling in RPE cells are poorly understood. Here we show that transcription factor MITF regulates the antioxidant response in RPE cells, protecting the neural retina from oxidative damage. In the oxidative stress-induced retinal degeneration mouse model, retinal degeneration in Mitf+/- mice is significantly aggravated compared to WT mice. In contrast, overexpression of Mitf in Dct-Mitf transgenic mice and AAV mediated overexpression in RPE cells protect the neural retina against oxidative damage. Mechanistically, MITF both directly regulates the transcription of NRF2, a master regulator of antioxidant signaling, and promotes its nuclear translocation. Furthermore, specific overexpression of NRF2 in Mitf+/- RPE cells activates antioxidant signaling and partially protects the retina from oxidative damage. Taken together, our findings demonstrate the regulation of NRF2 by MITF in RPE cells and provide new insights into potential therapeutic approaches for prevention of oxidative damage diseases.

Published

2020

11. FOXE3 contributes to Peters anomaly through transcriptional regulation of an autophagy-associated protein termed DNAJB1

Author

Shahid Y. Khan, Shivakumar Vasanth, Firoz Kabir, John D. Gottsch, Arif O. Khan, Raghothama Chaerkady, Mei-Chong W. Lee, Carmen C. Leitch, Zhiwei Ma, Julie Laux, Rafael Villasmil, Shaheen N. Khan, Sheikh Riazuddin, Javed Akram, Robert N. Cole, C. Conover Talbot, Nader Pourmand, Norann A. Zaghloul, J. Fielding Hejtmancik, and S. Amer Riazuddin

Subjects

Science

Abstract

Peter's Anomaly is a developmental disorder of the eye and has been linked to mutations in a range of genes, including the transcription factor FOXE3. Here the authors use next-generation RNA sequencing and mass spectrometry to identify an autophagy-associated protein, DNAJB1 as the transcriptional target of FOXE3.

Published

2016

12. CHARACTERIZATION OF MACULAR NEOVASCULARIZATION IN BIETTI CRYSTALLINE DYSTROPHY USING MULTIMODAL IMAGING MODALITIES

Author

Qian Li, Shengjuan Zhang, Lihua Kang, Donglin Wang, Xiaodong Jiao, J. Fielding Hejtmancik, Lifei Wang, and Xiaoyan Peng

Subjects

Ophthalmology, General Medicine

Published

2023

13. Truncation mutations in MYRF underlie primary angle closure glaucoma

Author

Jiamin Ouyang, Wenmin Sun, Huangxuan Shen, Xing Liu, Yingchen Wu, Hongmei Jiang, Xueqing Li, Yingwei Wang, Yi Jiang, Shiqiang Li, Xueshan Xiao, J. Fielding Hejtmancik, Zhiqun Tan, and Qingjiong Zhang

Subjects

Genetics, Genetics (clinical)

Abstract

Mutations in myelin regulatory factor (MYRF), a gene mapped to 11q12-q13.3, are responsible for autosomal dominant high hyperopia and seem to be associated with angle closure glaucoma, which is one of the leading causes of irreversible blindness worldwide. Whether there is a causal link from the MYRF mutations to the pathogenesis of primary angle-closure glaucoma (PACG) remains unclear at this time. Six truncation mutations, including five novel and one previously reported, in MYRF are identified in seven new probands with hyperopia, of whom all six adults have glaucoma, further confirming the association of MYRF mutations with PACG. Immunofluorescence microscopy demonstrates enriched expression of MYRF in the ciliary body and ganglion cell layer in humans and mice. Myrf

Published

2022

14. A Superfolder Green Fluorescent Protein-Based Biosensor Allows Monitoring of Chloride in the Endoplasmic Reticulum

Author

Kaavian Shariati, Yaohuan Zhang, Simone Giubbolini, Riccardo Parra, Steven Liang, Austin Edwards, J. Fielding Hejtmancik, Gian Michele Ratto, Daniele Arosio, and Gregory Ku

Subjects

Fluid Flow and Transfer Processes, Protein Folding, Chlorides, Process Chemistry and Technology, Green Fluorescent Proteins, Bioengineering, Biosensing Techniques, Endoplasmic Reticulum, Instrumentation

Abstract

Though the concentration of chloride has been measured in the cytoplasm and in secretory granules of live cells, it cannot be measured within the endoplasmic reticulum (ER) due to poor fluorescence of existing biosensors. We developed a fluorescent biosensor composed of a chloride-sensitive superfolder GFP and long Stokes-shifted mKate2 for simultaneous chloride and pH measurements that retained fluorescence in the ER lumen. Using this sensor, we showed that the chloride concentration in the ER is significantly lower than that in the cytosol. This improved biosensor enables dynamic measurement of chloride in the ER and may be useful in other environments where protein folding is challenging.

Published

2022

15. The Y46D Mutation Destabilizes Dense Packing of the Second Greek Key Pair of Human γC-Crystallin Causing Congenital Nuclear Cataracts

Author

Venkata Pulla Rao Vendra, Christian Ostrowski, Rebecca Clark, Marzena Dyba, Sergey G. Tarasov, and J. Fielding Hejtmancik

Subjects

Biochemistry

Published

2023

16. Zonule Associated Gene Variants in Isolated Ectopia Lentis and Glaucoma

Author

Longxiang Huang, Tingting Xu, Jiahe Gan, Yukai Mao, Lijun Zhao, Xiaodong Jiao, Mengjie Fan, Tingting Wang, Daren Zhang, Meng Xu, Yihua Zhu, J. Fielding Hejtmancik, and Xuyang Liu

Subjects

Ophthalmology

Published

2023

17. A Bietti Crystalline Dystrophy Mouse Model Shows Increased Sensitivity to Light-Induced Injury

Author

Zhiwei Ma, Xiaodong Jiao, Martin-Paul Agbaga, Robert E. Anderson, Haohua Qian, Qian Li, Lijin Dong, and J. Fielding Hejtmancik

Subjects

Organic Chemistry, General Medicine, Bietti crystalline dystrophy, Cyp4v3, mouse model, light-induced injury, high-fat diet, Catalysis, Computer Science Applications, Inorganic Chemistry, Mice, Disease Models, Animal, Retinal Diseases, Mutation, Retinal Dystrophies, Animals, Cytochrome P450 Family 4, Physical and Theoretical Chemistry, Atrophy, Molecular Biology, Spectroscopy

Abstract

Bietti crystalline corneo-retinal dystrophy (BCD) is an autosomal recessive inherited retinal dystrophy characterized by multiple shimmering yellow-white deposits in the posterior pole of the retina in association with atrophy of the retinal pigment epithelium (RPE), pigment clumps, and choroidal atrophy and sclerosis. Blindness and severe visual damage are common in late-stage BCD patients. We generated a Cyp4v3 knockout mouse model to investigate the pathogenesis of BCD. This model exhibits decreased RPE numbers and signs of inflammation response in the retina. Rod photoreceptors were vulnerable to light-induced injury, showing increased deposits through fundoscopy, a decrease in thickness and a loss of cells in the ONL, and the degeneration of rod photoreceptors. These results suggest that an inflammatory response might be an integral part of the pathophysiology of BCD, suggesting that it might be reasonable for BCD patients to avoid strong light, and the results provide a useful model for evaluating the effects of therapeutic approaches.

Published

2022

18. A Mouse Model with Ablated Asparaginase and Isoaspartyl Peptidase 1 (Asrgl1) Develops Early Onset Retinal Degeneration (RD) Recapitulating the Human Phenotype

Author

Pooja Biswas, Anne Marie Berry, Qais Zawaydeh, Dirk-Uwe G. Bartsch, Pongali B. Raghavendra, J. Fielding Hejtmancik, Naheed W. Khan, S. Amer Riazuddin, and Radha Ayyagari

Subjects

early onset degeneration, Neurodegenerative, Inbred C57BL, Eye, Autoantigens, Mice, Rare Diseases, Escherichia coli, Genetics, Animals, Humans, Asparaginase, 2.1 Biological and endogenous factors, Aetiology, Cas9, CRISPR/Cas9, Eye Disease and Disorders of Vision, Genetics (clinical), Animal, animal model, Retinal Degeneration, Neurosciences, Infant, ASRGL1, Phenotype, CRISPR, Disease Models, Peptide Hydrolases

Abstract

We previously identified a homozygous G178R mutation in human ASRGL1 (hASRGL1) through whole-exome analysis responsible for early onset retinal degeneration (RD) in patients with cone–rod dystrophy. The mutant G178R ASRGL1 expressed in Cos-7 cells showed altered localization, while the mutant ASRGL1 in E. coli lacked the autocatalytic activity needed to generate the active protein. To evaluate the effect of impaired ASRGL1 function on the retina in vivo, we generated a mouse model with c.578_579insAGAAA (NM_001083926.2) mutation (Asrgl1mut/mut) through the CRISPR/Cas9 methodology. The expression of ASGRL1 and its asparaginase activity were undetectable in the retina of Asrgl1mut/mut mice. The ophthalmic evaluation of Asrgl1mut/mut mice showed a significant and progressive decrease in scotopic electroretinographic (ERG) response observed at an early age of 3 months followed by a decrease in photopic response around 5 months compared with age-matched wildtype mice. Immunostaining and RT-PCR analyses with rod and cone cell markers revealed a loss of cone outer segments and a significant decrease in the expression of Rhodopsin, Opn1sw, and Opn1mw at 3 months in Asrgl1mut/mut mice compared with age-matched wildtype mice. Importantly, the retinal phenotype of Asrgl1mut/mut mice is consistent with the phenotype observed in patients harboring the G178R mutation in ASRGL1 confirming a critical role of ASRGL1 in the retina and the contribution of ASRGL1 mutations in retinal degeneration.

Published

2022

19. Pathogenicity evaluation and the genotype–phenotype analysis of OPA1 variants

Author

Shiqiang Li, Xueshan Xiao, Qingjiong Zhang, Xingyu Xu, Wenmin Sun, J. Fielding Hejtmancik, Panfeng Wang, and Xiaoyun Jia

Subjects

0106 biological sciences, 0301 basic medicine, Genetics, General Medicine, Biology, 01 natural sciences, Penetrance, eye diseases, Human genetics, Frameshift mutation, 03 medical and health sciences, Exon, 030104 developmental biology, Genotype-phenotype distinction, Missense mutation, Molecular Biology, Gene, Exome sequencing, 010606 plant biology & botany

Abstract

Autosomal dominant optic atrophy (ADOA) is an important cause of irreversible visual impairment in children and adolescents. About 60-90% of ADOA is caused by the pathogenic variants of OPA1 gene. By evaluating the pathogenicity of OPA1 variants and summarizing the relationship between the genotype and phenotype, this study aimed to provide a reference for clinical genetic test involving OPA1. Variants in OPA1 were selected from the exome sequencing results in 7092 cases of hereditary eye diseases and control groups from our in-house data. At the same time, the urine cells of some optic atrophy patients with OPA1 variants as well as their family members were collected and oxygen consumption rates (OCR) were measured in these cells to evaluate the pathogenicity of variants. As a result, 97 variants were detected, including 94 rare variants and 3 polymorphisms. And the 94 rare variants were classified into three groups: pathogenic (33), variants of uncertain significance (19), and likely benign (42). Our results indicated that the frameshift variants at the 3' terminus might be pathogenic, while the variants in exon 7 and intron 4 might be benign. The penetrance of the missense variants was higher than that of truncation variants. The OCR of cells with pathogenic OPA1 variants were significantly lower than those without pathogenic variants. In conclusion, some variants might be benign although predicted pathogenic in previous studies while some might have unknown pathogenesis. Measuring the OCR in urine cells could be used as a method to evaluate the pathogenicity of some OPA1 variants.

Published

2021

20. Unique Haplotypes in OPN1LW as a Common Cause of High Myopia With or Without Protanopia: A Potential Window Into Myopic Mechanism

Author

Yingwei Wang, Wenmin Sun, Xueshan Xiao, Yi Jiang, Jiamin Ouyang, Junwen Wang, Zhen Yi, Shiqiang Li, Xiaoyun Jia, Panfeng Wang, J. Fielding Hejtmancik, and Qingjiong Zhang

Subjects

General Medicine

Published

2023

21. The role of FYCO1-dependent autophagy in lens fiber cell differentiation

Author

Shahid Y. Khan, Muhammad Ali, Firoz Kabir, Chan Hyun Na, Michael Delannoy, Yinghong Ma, Caihong Qiu, M. Joseph Costello, J. Fielding Hejtmancik, and S. Amer Riazuddin

Subjects

Mice, Lens, Crystalline, Autophagy, Animals, Humans, Cell Differentiation, Cell Biology, Endoplasmic Reticulum, Molecular Biology, Microtubule-Associated Proteins, Cataract, Research Paper, Transcription Factors

Abstract

FYCO1 (FYVE and coiled-coil domain containing 1) is an adaptor protein, expressed ubiquitously and required for microtubule-dependent, plus-end-directed transport of macroautophagic/autophagic vesicles. We have previously shown that loss-of-function mutations in FYCO1 cause cataracts with no other ocular and/or extra-ocular phenotype. Here, we show fyco1 homozygous knockout (fyco1(−/−)) mice recapitulate the cataract phenotype consistent with a critical role of FYCO1 and autophagy in lens morphogenesis. Transcriptome coupled with proteome and metabolome profiling identified many autophagy-associated genes, proteins, and lipids respectively perturbed in fyco1(−/−) mice lenses. Flow cytometry of FYCO1 (c.2206C>T) knock-in (KI) human lens epithelial cells revealed a decrease in autophagic flux and autophagic vesicles resulting from the loss of FYCO1. Transmission electron microscopy showed cellular organelles accumulated in FYCO1 (c.2206C>T) KI lens-like organoid structures and in fyco1(−/−) mice lenses. In summary, our data confirm the loss of FYCO1 function results in a diminished autophagic flux, impaired organelle removal, and cataractogenesis. Abbreviations: CC: congenital cataracts; DE: differentially expressed; ER: endoplasmic reticulum; FYCO1: FYVE and coiled-coil domain containing 1; hESC: human embryonic stem cell; KI: knock-in; OFZ: organelle-free zone; qRT-PCR: quantitative real-time PCR; PE: phosphatidylethanolamine; RNA-Seq: RNA sequencing; SD: standard deviation; sgRNA: single guide RNA; shRNA: shorthairpin RNA; TEM: transmission electron microscopy; WT: wild type

Published

2022

22. The Genetic Confirmation and Clinical Characterization of LOXL3-Associated MYP28: A Common Type of Recessive Extreme High Myopia

Author

Yi Jiang, Lin Zhou, Yingwei Wang, Jiamin Ouyang, Shiqiang Li, Xueshan Xiao, Xiaoyun Jia, Junwen Wang, Zhen Yi, Wenmin Sun, Xiaodong Jiao, Panfeng Wang, J. Fielding Hejtmancik, and Qingjiong Zhang

Subjects

General Medicine

Published

2023

23. SIRT1 Inhibits High Glucose–Induced TXNIP/NLRP3 Inflammasome Activation and Cataract Formation

Author

Lili Lian, Zhenmin Le, Zhenzhen Wang, Ying-ao Chen, Xiaodong Jiao, Hang Qi, J. Fielding Hejtmancik, Xiaoyin Ma, Qinxiang Zheng, and Yueping Ren

Subjects

General Medicine

Published

2023

24. Aged Nrf2-Null Mice Develop All Major Types of Age-Related Cataracts

Author

Sheldon Rowan, Shuhong Jiang, Sarah G. Francisco, Laura C. D. Pomatto, Zhiwei Ma, Xiaodong Jiao, Maria M. Campos, Sandeep Aryal, Shaili D. Patel, Binapani Mahaling, S. Amer Riazuddin, Elia J. Duh, Salil A. Lachke, J. Fielding Hejtmancik, Rafael de Cabo, Paul G. FitzGerald, and Allen Taylor

Subjects

Male, Aging, antioxidant, genetic structures, NF-E2-Related Factor 2, Knockout, Inbred C57BL, Slit Lamp Microscopy, Ophthalmology & Optometry, Medical and Health Sciences, Cataract, Lens, Mice, Lens, Crystalline, Genetics, Animals, Eye Disease and Disorders of Vision, Nutrition, Mice, Knockout, Crystalline, Animal, Prevention, Cell Differentiation, Biological Sciences, eye diseases, Diet, Mice, Inbred C57BL, Disease Models, Animal, nutrition, Glucose, Phenotype, Glycemic Index, Disease Models, Female, sense organs, caloric restriction, age-related cataract

Abstract

Purpose Age-related cataracts affect the majority of older adults and are a leading cause of blindness worldwide. Treatments that delay cataract onset or severity have the potential to delay cataract surgery, but require relevant animal models that recapitulate the major types of cataracts for their development. Unfortunately, few such models are available. Here, we report the lens phenotypes of aged mice lacking the critical antioxidant transcription factor Nfe2l2 (designated as Nrf2 −/−). Methods Three independent cohorts of Nrf2 −/− and wild-type C57BL/6J mice were evaluated for cataracts using combinations of slit lamp imaging, photography of freshly dissected lenses, and histology. Mice were fed high glycemic diets, low glycemic diets, regular chow ad libitum, or regular chow with 30% caloric restriction. Results Nrf2 −/− mice developed significant opacities between 11 and 15 months and developed advanced cortical, posterior subcapsular, anterior subcapsular, and nuclear cataracts. Cataracts occurred similarly in male mice fed high or low glycemic diets, and were also observed in 21-month male and female Nrf2 −/− mice fed ad libitum or 30% caloric restriction. Histological observation of 18-month cataractous lenses revealed significant disruption to fiber cell architecture and the retention of nuclei throughout the cortical region of the lens. However, fiber cell denucleation and initiation of lens differentiation was normal at birth, with the first abnormalities observed at 3 months. Conclusions Nrf2 −/− mice offer a tool to understand how defective antioxidant signaling causes multiple forms of cataract and may be useful for screening drugs to prevent or delay cataractogenesis in susceptible adults.

Published

2021

25. LncRNA NEAT1 Recruits SFPQ to Regulate MITF Splicing and Control RPE Cell Proliferation

Author

Juan Yang, Junhao He, Ling Hou, Xiaojuan Hu, Mingyuan Jiang, Dandan Wei, Fang Li, Ye Jiang, Lifu Chang, Xiaoyin Ma, and J. Fielding Hejtmancik

Subjects

Small interfering RNA, proliferation, Human Embryonic Stem Cells, NEAT1, Cell Count, Retinal Pigment Epithelium, Biology, Real-Time Polymerase Chain Reaction, Splicing factor, Mice, splicing, Animals, Humans, RNA, Messenger, RNA, Small Interfering, PTB-Associated Splicing Factor, Promoter Regions, Genetic, Transcription factor, Cells, Cultured, Cell Proliferation, Gene knockdown, Microphthalmia-Associated Transcription Factor, MITF, integumentary system, Cell growth, Alternative splicing, Biochemistry and Molecular Biology, Cell Differentiation, Microphthalmia-associated transcription factor, Cell biology, body regions, Mice, Inbred C57BL, Alternative Splicing, Ki-67 Antigen, Gene Expression Regulation, RNA splicing, RNA, Long Noncoding, sense organs, RPE

Abstract

Purpose Retinal pigment epithelium (RPE) cell proliferation is precisely regulated to maintain retinal homoeostasis. Microphthalmia-associated transcription factor (MITF), a critical transcription factor in RPE cells, has two alternatively spliced isoforms: (+)MITF and (-)MITF. Previous work has shown that (-)MITF but not (+)MITF inhibits RPE cell proliferation. This study aims to investigate the role of long non-coding RNA (lncRNA) nuclear-enriched abundant transcript 1 (NEAT1) in regulating MITF splicing and hence proliferation of RPE cells. Methods Mouse RPE, primary cultured mouse RPE cells, and different proliferative human embryonic stem cell (hESC)-RPE cells were used to evaluate the expression of (+)MITF, (-)MITF, and NEAT1 by reverse-transcription PCR (RT-PCR) or quantitative RT-PCR. NEAT1 was knocked down using specific small interfering RNAs (siRNAs). Splicing factor proline- and glutamine-rich (SFPQ) was overexpressed with the use of lentivirus infection. Cell proliferation was analyzed by cell number counting and Ki67 immunostaining. RNA immunoprecipitation (RIP) was used to analyze the co-binding between the SFPQ and MITF or NEAT1. Results NEAT1 was highly expressed in proliferative RPE cells, which had low expression of (-)MITF. Knockdown of NEAT1 in RPE cells switched the MITF splicing pattern to produce higher levels of (-)MITF and inhibited cell proliferation. Mechanistically, NEAT1 recruited SFPQ to bind directly with MITF mRNA to regulate its alternative splicing. Overexpression of SFPQ in ARPE-19 cells enhanced the binding enrichment of SFPQ to MITF and increased the splicing efficiency of (+)MITF. The binding affinity between SFPQ and MITF was decreased after NEAT1 knockdown. Conclusions NEAT1 acts as a scaffold to recruit SFPQ to MITF mRNA and promote its binding affinity, which plays an important role in regulating the alternative splicing of MITF and RPE cell proliferation.

Published

2021

26. Retinal Development and Pathophysiology in Kcnj13 Knockout Mice

Author

Xiaodong Jiao, Zhiwei Ma, Jingqi Lei, Pinghu Liu, Xiaoyu Cai, Pawan K. Shahi, Chi-Chao Chan, Robert Fariss, Bikash R. Pattnaik, Lijin Dong, and J. Fielding Hejtmancik

Subjects

retina, genetic structures, QH301-705.5, Cell Biology, eye diseases, snowflake vitreoretinal dystrophy, Cell and Developmental Biology, retinal degeneration, kcnj13/kir7.1, sense organs, Biology (General), retinal dystrophy, Developmental Biology, Original Research

Abstract

Purpose: We constructed and characterized knockout and conditional knockout mice for KCNJ13, encoding the inwardly rectifying K+ channel of the Kir superfamily Kir7.1, mutations in which cause both Snowflake Vitreoretinal Degeneration (SVD) and Retinitis pigmentosa (RP) to further elucidate the pathology of this disease and to develop a potential model system for gene therapy trials.Methods: A Kcnj13 knockout mouse line was constructed by inserting a gene trap cassette expressing beta-galactosidase flanked by FRT sites in intron 1 with LoxP sites flanking exon two and converted to a conditional knockout by FLP recombination followed by crossing with C57BL/6J mice having Cre driven by the VMD2 promoter. Lentiviral replacement of Kcnj13 was driven by the EF1a or VMD2 promoters.Results: Blue-Gal expression is evident in E12.5 brain ventricular choroid plexus, lens, neural retina layer, and anterior RPE. In the adult eye expression is seen in the ciliary body, RPE and choroid. Adult conditional Kcnj13 ko mice show loss of photoreceptors in the outer nuclear layer, inner nuclear layer thinning with loss of bipolar cells, and thinning and disruption of the outer plexiform layer, correlating with Cre expression in the overlying RPE which, although preserved, shows morphological disruption. Fundoscopy and OCT show signs of retinal degeneration consistent with the histology, and photopic and scotopic ERGs are decreased in amplitude or extinguished. Lentiviral based replacement of Kcnj13 resulted in increased ERG c- but not a- or b- wave amplitudes.Conclusion: Ocular KCNJ13 expression starts in the choroid, lens, ciliary body, and anterior retina, while later expression centers on the RPE with no/lower expression in the neuroretina. Although KCNJ13 expression is not required for survival of the RPE, it is necessary for RPE maintenance of the photoreceptors, and loss of the photoreceptor, outer plexiform, and outer nuclear layers occur in adult KCNJ13 cKO mice, concomitant with decreased amplitude and eventual extinguishing of the ERG and signs of retinitis pigmentosa on fundoscopy and OCT. Kcnj13 replacement resulting in recovery of the ERG c- but not a- and b-waves is consistent with the degree of photoreceptor degeneration seen on histology.

Published

2021

27. Deciphering the genetic architecture and ethnographic distribution of IRD in three ethnic populations by whole genome sequence analysis

Author

John Suk, S. Amer Riazuddin, Kelly A. Frazer, Kari Branham, Pooja Biswas, Sindhu Devalaraja, Jeffrey L. Goldberg, Qais Zawaydeh, Benjamin Bakall, Pongali B. Raghavendra, J. Fielding Hejtmancik, Angel Soto-Hermida, Bonnie Huang, Paul A. Sieving, Sheikh Riazuddin, Richard G. Weleber, Berzhan Kurmanov, Jason Zhou, Gabriele Richard, Jacque L. Duncan, Shahid Y. Khan, Adda Villanueva, Akhila Alapati, Shyamanga Borooah, Radha Ayyagari, Hiroko Matsui, Luis Alexandre Rassi Gabriel, Andrew Huynh, Naheed W. Khan, John R. Heckenlively, and Iyengar, Sudha K

Subjects

Male, Cancer Research, Mexican People, Heredity, Genetic Linkage, DNA Mutational Analysis, Gene Identification and Analysis, Pedigree chart, Gene mutation, QH426-470, Biochemistry, Homozygosity, Geographical Locations, Database and Informatics Methods, Consanguinity, Genotype, Ethnicity, Ethnicities, 2.1 Biological and endogenous factors, Pakistan, Exome, Aetiology, Frameshift Mutation, Genetics (clinical), Exome sequencing, Genetics, education.field_of_study, Heterozygosity, Retinal Degeneration, Population groupings, Pedigree, Europe, Nucleic acids, Female, Research Article, Biotechnology, Population, Biology, Research and Analysis Methods, Retina, Genetic linkage, Clinical Research, parasitic diseases, Exome Sequencing, Humans, Genetic Testing, education, Eye Proteins, Molecular Biology, Mutation Detection, Mexico, Ecology, Evolution, Behavior and Systematics, Genetic Association Studies, Whole Genome Sequencing, Genetic heterogeneity, Human Genome, Biology and Life Sciences, Latin American people, DNA, Biological Databases, Mutation Databases, Mutation, DNA damage, People and places, Developmental Biology

Abstract

Patients with inherited retinal dystrophies (IRDs) were recruited from two understudied populations: Mexico and Pakistan as well as a third well-studied population of European Americans to define the genetic architecture of IRD by performing whole-genome sequencing (WGS). Whole-genome analysis was performed on 409 individuals from 108 unrelated pedigrees with IRDs. All patients underwent an ophthalmic evaluation to establish the retinal phenotype. Although the 108 pedigrees in this study had previously been examined for mutations in known IRD genes using a wide range of methodologies including targeted gene(s) or mutation(s) screening, linkage analysis and exome sequencing, the gene mutations responsible for IRD in these 108 pedigrees were not determined. WGS was performed on these pedigrees using Illumina X10 at a minimum of 30X depth. The sequence reads were mapped against hg19 followed by variant calling using GATK. The genome variants were annotated using SnpEff, PolyPhen2, and CADD score; the structural variants (SVs) were called using GenomeSTRiP and LUMPY. We identified potential causative sequence alterations in 61 pedigrees (57%), including 39 novel and 54 reported variants in IRD genes. For 57 of these pedigrees the observed genotype was consistent with the initial clinical diagnosis, the remaining 4 had the clinical diagnosis reclassified based on our findings. In seven pedigrees (12%) we observed atypical causal variants, i.e. unexpected genotype(s), including 4 pedigrees with causal variants in more than one IRD gene within all affected family members, one pedigree with intrafamilial genetic heterogeneity (different affected family members carrying causal variants in different IRD genes), one pedigree carrying a dominant causative variant present in pseudo-recessive form due to consanguinity and one pedigree with a de-novo variant in the affected family member. Combined atypical and large structural variants contributed to about 20% of cases. Among the novel mutations, 75% were detected in Mexican and 50% found in European American pedigrees and have not been reported in any other population while only 20% were detected in Pakistani pedigrees and were not previously reported. The remaining novel IRD causative variants were listed in gnomAD but were found to be very rare and population specific. Mutations in known IRD associated genes contributed to pathology in 63% Mexican, 60% Pakistani and 45% European American pedigrees analyzed. Overall, contribution of known IRD gene variants to disease pathology in these three populations was similar to that observed in other populations worldwide. This study revealed a spectrum of mutations contributing to IRD in three populations, identified a large proportion of novel potentially causative variants that are specific to the corresponding population or not reported in gnomAD and shed light on the genetic architecture of IRD in these diverse global populations., Author summary The study was performed to identify the underlying cause of inherited retinal degeneration (IRD) in 409 individuals from 108 families. Primarily, these families were recruited from three different geographic regions: Mexico, Pakistan and European Americans from the United States. Blood samples were collected from all individuals for genome analysis. This analysis detected causative variants in 61 out of the 108 pedigrees. A total of 93 gene variants were found in the 61 families. Among these, 54 were previously reported as causative variants and the remaining 39 have not been reported in IRD pedigrees. Interestingly, 54% of these novel variants were not listed in gnomAD. In addition to these findings, complex causative genotypes were observed in 20% of pedigrees. Overall, causative variants were detected in 63% Mexican, 60% Pakistani and 45% European American pedigrees. This study revealed the distribution of IRD causative variants in pedigrees with diverse ethnic and geographic backgrounds.

Published

2021

28. Understanding the genetic architecture of human retinal degenerations

Author

J. Fielding Hejtmancik and Stephen P. Daiger

Subjects

0301 basic medicine, Retinal degeneration, Biology, Retina, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Retinitis pigmentosa, Prevalence, medicine, Humans, Genetics, Multidisciplinary, Retinal pigment epithelium, Genetic heterogeneity, Retinal Degeneration, Retinal, Biological Sciences, Macular degeneration, medicine.disease, Penetrance, 030104 developmental biology, medicine.anatomical_structure, chemistry, Multifactorial Inheritance, 030217 neurology & neurosurgery

Abstract

Inherited retinal degenerations are a clinically and genetically heterogeneous group of blinding diseases characterized by progressive degeneration of the neuroretina and/or the retinal pigment epithelium. Currently, over 300 genes have been implicated in retinal degenerations (RetNet: https://sph.uth.edu/RetNet/). While mutations, or causative variants, in each of these genes are relatively rare, taken together they are a significant cause of blindness, especially in working-age individuals, which increases their economic and societal impact. Clinically, inherited retinal degenerations vary from retinitis pigmentosa and Leber congenital amaurosis, which are often manifest at birth and initially involve rod photoreceptors in the retinal periphery, to early-onset macular degeneration, which is a progressive degeneration affecting central vision (1). Inherited retinal degenerations can show autosomal-dominant, autosomal-recessive, and X-linked inheritance, as well as more complex or multifactorial inheritance patterns, especially for some of the later-onset progressive diseases. While mutations in the same gene usually show the same inheritance pattern, it is not uncommon for mutations in the same gene to cause two or more forms of retinal disease, complicating the nosology of this group of diseases (2). In addition, the presence of disease-associated alleles at one gene can affect the penetrance or expressivity of mutations at a second, resulting in complicated family histories and in some cases even digenic diallelic (3) or digenic triallelic (4) inheritance. In PNAS, Hanany et al. (5) address this intimidating set of related diseases by developing a system to identify disease alleles at each of the associated genes and, beyond that, to calculate the gene-specific carrier frequency and the prevalence of homozygosity for variants causing autosomal recessive retinal degenerations. While appearing somewhat mundane on the surface, this work actually has far-reaching implications for both the basic science of the retina and the clinical practice of ophthalmology. The genes associated with retinal degeneration and the changes … [↵][1]1To whom correspondence may be addressed. Email: hejtmancikj{at}nei.nih.gov. [1]: #xref-corresp-1-1

Published

2020

29. Biology of Inherited Cataracts and Opportunities for Treatment

Author

Alan Shiels and J. Fielding Hejtmancik

Subjects

0301 basic medicine, genetic structures, Apoptosis, Protein aggregation, Biology, Cataract, Article, 03 medical and health sciences, 0302 clinical medicine, Cataracts, Crystallin, medicine, Humans, Intermediate filament, Eye Diseases, Hereditary, medicine.disease, Crystallins, eye diseases, Cell biology, Ophthalmology, 030104 developmental biology, Membrane protein, 030221 ophthalmology & optometry, Congenital cataracts, Unfolded protein response, sense organs, Neurology (clinical), Chemical chaperone, Stem Cell Transplantation

Abstract

Cataract, the clinical correlate of opacity or light scattering in the eye lens, is usually caused by the presence of high-molecular-weight (HMW) protein aggregates or disruption of the lens microarchitecture. In general, genes involved in inherited cataracts reflect important processes and pathways in the lens including lens crystallins, connexins, growth factors, membrane proteins, intermediate filament proteins, and chaperones. Usually, mutations causing severe damage to proteins cause congenital cataracts, while milder variants increasing susceptibility to environmental insults are associated with age-related cataracts. These may have different pathogenic mechanisms: Congenital cataracts induce the unfolded protein response and apoptosis. By contrast, denatured crystallins in age-related cataracts are bound by α-crystallin and form light-scattering HMW aggregates. New therapeutic approaches to age-related cataracts use chemical chaperones to solubilize HMW aggregates, while attempts are being made to regenerate lenses using endogenous stem cells to treat congenital cataracts.

Published

2019

30. Novel truncation mutations in MYRF cause autosomal dominant high hyperopia mapped to 11p12–q13.3

Author

Zhiqun Tan, Wenmin Sun, Shiqiang Li, Xiaoyun Jia, Jiamin Ouyang, J. Fielding Hejtmancik, Xueshan Xiao, and Qingjiong Zhang

Subjects

Male, Proband, Eye Diseases, genetic structures, DNA Mutational Analysis, Neurodegenerative, Eye, medicine.disease_cause, Gene Knockout Techniques, Pair 11, Fluorescein Angiography, Zebrafish, Genetics (clinical), Original Investigation, Genes, Dominant, Genetics & Heredity, Genetics, 0303 health sciences, Mutation, 030305 genetics & heredity, Chromosome Mapping, Eye Diseases, Hereditary, Phenotype, Pedigree, Hereditary, Hyperopia, Female, Human, Biotechnology, Biology, Chromosomes, Paediatrics and Reproductive Medicine, 03 medical and health sciences, Complementary and Alternative Medicine, medicine, Animals, Humans, Dominant, Genetic Predisposition to Disease, Gene, Genetic Association Studies, 030304 developmental biology, Chromosomes, Human, Pair 11, Human Genome, Neurosciences, Membrane Proteins, Chromosome, biology.organism_classification, eye diseases, Human genetics, Genes, Genetic Loci, Lod Score, Transcription Factors

Abstract

High hyperopia is a common and severe form of refractive error. Genetic factors play important roles in the development of high hyperopia but the exact gene responsible for this condition is mostly unknown. We identified a large Chinese family with autosomal dominant high hyperopia. A genome-wide linkage scan mapped the high hyperopia to chromosome 11p12–q13.3, with maximum log of the odds scores of 4.68 at theta = 0 for D11S987. Parallel whole-exome sequencing detected a novel c.3377delG (p.Gly1126Valfs*31) heterozygous mutation in the MYRF gene within the linkage interval. Whole-exome sequencing in other 121 probands with high hyperopia identified additional novel mutations in MYRF within two other families: a de novo c.3274_3275delAG (p.Leu1093Profs*22) heterozygous mutation and a c.3194+2T>C heterozygous mutation. All three mutations are located in the C-terminal region of MYRF and are predicted to result in truncation of that portion. Two patients from two of the three families developed angle-closure glaucoma. These three mutations were present in neither the ExAC database nor our in-house whole-exome sequencing data from 3280 individuals. No other truncation mutations in MYRF were detected in the 3280 individuals. Knockdown of myrf resulted in small eye size in zebrafish. These evidence all support that truncation mutations in the C-terminal region of MYRF are responsible for autosomal dominant high hyperopia in these families. Our results may provide useful clues for further understanding the functional role of the C-terminal region of this critical myelin regulatory factor, as well as the molecular pathogenesis of high hyperopia and its associated angle-closure glaucoma. Electronic supplementary material The online version of this article (10.1007/s00439-019-02039-z) contains supplementary material, which is available to authorized users.

Published

2019

31. Congenital and Inherited Cataracts

Author

Maria Lee, J. Fielding Hejtmancik, Sohan Rao, Elizabeth Fielding, Luke Xia, Celestine Zhao, Alan Shiels, William Fielding, and Manuel B. Datiles

Subjects

medicine.medical_specialty, Retina, genetic structures, Blindness, business.industry, medicine.disease, eye diseases, Genetic architecture, medicine.anatomical_structure, Cataracts, Lens (anatomy), Ophthalmology, medicine, Congenital cataracts, sense organs, business

Abstract

Congenital cataracts cause approximately one-third of blindness in infants worldwide. If untreated they can cause permanent blindness by interfering with the sharp focus of light onto the retina and thus fail to establish appropriate synaptic connections between the retina and the visual cortex. Between 8 and 30% (see later) of congenital cataracts are inherited, and our understanding of their genetic architecture is increasing. Delineating the relationship between the genes and mutations causing cataracts and their phenotypic presentation can help us to understand the biology of the lens and provide a framework for the clinical approach to diagnosis and treatment.

Published

2021

32. Genotype–Phenotype of RPE65 Mutations: A Reference Guide for Gene Testing and Its Clinical Application

Author

Zhen Yi, Qingjiong Zhang, J. Fielding Hejtmancik, Christina Zeitz, and Takeshi Iwata

Subjects

Retinal degeneration, Genetics, Vitelliform macular dystrophy, Biology, medicine.disease, Penetrance, eye diseases, Choroideremia, Frameshift mutation, RPE65, Retinitis pigmentosa, medicine, Missense mutation, sense organs

Abstract

The RPE65 gene encodes a retinal pigment epithelium-specific isomerase that catalyzes the conversion of all-trans retinyl esters to 11-cis retinol, the activity of which affects the formation of visual pigment in photoreceptors. Mutations in RPE65 in inherited retinal dystrophies have been studied widely worldwide, especially now that gene therapy for patients with RPE65 mutations is available in the clinic. The aim of this study is to reveal the RPE65 mutation spectrum and frequency, the associated phenotypic characteristics, and potential genotype–phenotype correlations. In total, 201 mutations in RPE65 were identified in 479 patients from 353 families based on data reported in the literature. Mutations in 349 families caused autosomal recessive retinal degeneration, while a c.1430A>G (p.Asp477Gly) mutation in four families resulted in autosomal dominant retinal degeneration resembling retinitis pigmentosa, choroideremia, or vitelliform macular dystrophy with incomplete penetrance. Mutations identified in families with biallelic RPE65 mutations included missense (113/200 [56.5%]), frameshift indel (39/200 [19.5%]), splicing defect (24/200 [12.0%]), nonsense (19/200 [9.5%]), inframe indel (4/200 [2.0%]), and start loss (1/200 [0.5%]). A significant reduction in visual acuity was noticeable at 15 years of age and at 35 years of age, suggesting a critical window for treatment including gene therapy. Two major types of fundus changes were observed: (1) mild or obvious tapetoretinal degeneration, generalized or located mainly in the mid-peripheral retina; and (2) fundus albipunctatus-like retinopathy. Typical bone-spicule pigmentation was rarely seen in early childhood but may be observed after 35 years of age. A severe phenotype (Leber congenital amaurosis) is frequently associated with biallelic loss-of-function mutations, while milder phenotypes are more likely to be associated with one or two missense mutations. The overall information presented here should be useful as a reference guide in clinical practice, especially for clinical gene testing and enrollment in gene therapy.

Published

2021

33. Patterns of Crystallin Gene Expression in Differentiation State Specific Regions of the Embryonic Chicken Lens

Author

Zhiwei Ma, Daniel Chauss, Joshua Disatham, Xiaodong Jiao, Lisa Ann Brennan, A. Sue Menko, Marc Kantorow, and J. Fielding Hejtmancik

Subjects

Lens, Crystalline, Animals, Gene Expression, Cell Differentiation, Chick Embryo, Chickens, Crystallins, Transcription Factors

Abstract

Transition from lens epithelial cells to lens fiber cell is accompanied by numerous changes in gene expression critical for lens transparency. We identify expression patterns of highly prevalent genes including ubiquitous and enzyme crystallins in the embryonic day 13 chicken lens.Embryonic day 13 chicken lenses were dissected into central epithelial cell (EC), equatorial epithelial cell (EQ), cortical fiber cell (FP), and nuclear fiber cell (FC) compartments. Total RNA was prepared, subjected to high-throughput unidirectional mRNA sequencing, analyzed, mapped to the chicken genome, and functionally grouped.A total of 77,097 gene-specific transcripts covering 17,450 genes were expressed, of which 10,345 differed between two or more lens subregions. Ubiquitous crystallin gene expression increased from EC to EQ and was similar in FP and FC. Highly expressed crystallin genes fell into three coordinately expressed groups with R2 ≥ 0.93: CRYAA, CRYBB2, CRYAB, and CRYBA2; CRYBB1, CRYBA4, CRYGN, ASL1, and ASL; and CRYBB3 and CRYBA1. The highly expressed transcription factors YBX1, YBX3, PNRC1, and BASP1 were coordinately expressed with the second group of crystallins (r20.88).Although it is well known that lens crystallin gene expression changes during the epithelial to fiber cell transition, these data identify for the first time three distinct patterns of expression for specific subsets of crystallin genes, each highly correlated with expression of specific transcription factors. The results provide a quantitative basis for designing functional experiments pinpointing the mechanisms governing the landscape of crystallin expression during fiber cell differentiation to attain lens transparency.

Published

2022

34. Whole genome sequencing data of multiple individuals of Pakistani descent

Author

Shahid Y. Khan, Muhammad Ali, Sheikh Riazuddin, Mei-Chong Wendy Lee, J. Fielding Hejtmancik, Radha Ayyagari, Muhammad Asif Naeem, Saima Riazuddin, S. Amer Riazuddin, Zhiwei Ma, Asma A. Khan, and Pooja Biswas

Subjects

Statistics and Probability, Data Descriptor, Single-nucleotide polymorphism, Library and Information Sciences, Biology, Polymorphism, Single Nucleotide, Genome, Haplogroup, Education, 03 medical and health sciences, 0302 clinical medicine, Intergenic region, Genotype, Genetics, Humans, SNP, Pakistan, Polymorphism, 1000 Genomes Project, lcsh:Science, 030304 developmental biology, Whole genome sequencing, 0303 health sciences, Whole Genome Sequencing, Genome, Human, Comparative genomics, Human Genome, Single Nucleotide, Computer Science Applications, Next-generation sequencing, lcsh:Q, Statistics, Probability and Uncertainty, 030217 neurology & neurosurgery, Human, Information Systems

Abstract

Here we report whole genome sequencing of four individuals (H3, H4, H5, and H6) from a family of Pakistani descent. Whole genome sequencing yielded 1084.92, 894.73, 1068.62, and 1005.77 million mapped reads corresponding to 162.73, 134.21, 160.29, and 150.86 Gb sequence data and 52.49x, 43.29x, 51.70x, and 48.66x average coverage for H3, H4, H5, and H6, respectively. We identified 3,529,659, 3,478,495, 3,407,895, and 3,426,862 variants in the genomes of H3, H4, H5, and H6, respectively, including 1,668,024 variants common in the four genomes. Further, we identified 42,422, 39,824, 28,599, and 35,206 novel variants in the genomes of H3, H4, H5, and H6, respectively. A major fraction of the variants identified in the four genomes reside within the intergenic regions of the genome. Single nucleotide polymorphism (SNP) genotype based comparative analysis with ethnic populations of 1000 Genomes database linked the ancestry of all four genomes with the South Asian populations, which was further supported by mitochondria based haplogroup analysis. In conclusion, we report whole genome sequencing of four individuals of Pakistani descent., Measurement(s) SNV • genome Technology Type(s) whole genome sequencing • DNA sequencing Factor Type(s) individual Sample Characteristic - Organism Homo sapiens Sample Characteristic - Location Pakistan Machine-accessible metadata file describing the reported data: 10.6084/m9.figshare.12642761

Published

2020

35. Pathogenicity evaluation and the genotype-phenotype analysis of OPA1 variants

Author

Xingyu, Xu, Panfeng, Wang, Xiaoyun, Jia, Wenmin, Sun, Shiqiang, Li, Xueshan, Xiao, J Fielding, Hejtmancik, and Qingjiong, Zhang

Subjects

Adult, Male, Polymorphism, Genetic, Adolescent, DNA Mutational Analysis, Mutation, Missense, Urinalysis, Urine, GTP Phosphohydrolases, Pedigree, Young Adult, Phenotype, Case-Control Studies, Child, Preschool, Optic Atrophy, Autosomal Dominant, Humans, Family, Female, Genetic Testing, Child, Cells, Cultured, Genetic Association Studies

Abstract

Autosomal dominant optic atrophy (ADOA) is an important cause of irreversible visual impairment in children and adolescents. About 60-90% of ADOA is caused by the pathogenic variants of OPA1 gene. By evaluating the pathogenicity of OPA1 variants and summarizing the relationship between the genotype and phenotype, this study aimed to provide a reference for clinical genetic test involving OPA1. Variants in OPA1 were selected from the exome sequencing results in 7092 cases of hereditary eye diseases and control groups from our in-house data. At the same time, the urine cells of some optic atrophy patients with OPA1 variants as well as their family members were collected and oxygen consumption rates (OCR) were measured in these cells to evaluate the pathogenicity of variants. As a result, 97 variants were detected, including 94 rare variants and 3 polymorphisms. And the 94 rare variants were classified into three groups: pathogenic (33), variants of uncertain significance (19), and likely benign (42). Our results indicated that the frameshift variants at the 3' terminus might be pathogenic, while the variants in exon 7 and intron 4 might be benign. The penetrance of the missense variants was higher than that of truncation variants. The OCR of cells with pathogenic OPA1 variants were significantly lower than those without pathogenic variants. In conclusion, some variants might be benign although predicted pathogenic in previous studies while some might have unknown pathogenesis. Measuring the OCR in urine cells could be used as a method to evaluate the pathogenicity of some OPA1 variants.

Published

2020

36. MITF protects against oxidative damage-induced retinal degeneration by regulating the NRF2 pathway in the retinal pigment epithelium

Author

Jianjun Chen, Xiaojuan Hu, Shuhui Jian, Xiaoyin Ma, Jiajia Hua, Jing Wang, Shuxian Han, Guoxiao Zheng, J. Fielding Hejtmancik, Huirong Li, Jinglei Yang, Ling Hou, and Jia Qu

Subjects

0301 basic medicine, Genetically modified mouse, Retinal degeneration, NF-E2-Related Factor 2, Clinical Biochemistry, Oxidative phosphorylation, Retinal Pigment Epithelium, Biochemistry, NRF2, 03 medical and health sciences, chemistry.chemical_compound, Macular Degeneration, Mice, 0302 clinical medicine, medicine, Animals, Transcription factor, lcsh:QH301-705.5, Retina, Microphthalmia-Associated Transcription Factor, MITF, lcsh:R5-920, Retinal pigment epithelium, integumentary system, Chemistry, Organic Chemistry, Retinal, Microphthalmia-associated transcription factor, medicine.disease, eye diseases, Cell biology, body regions, Oxidative Stress, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), sense organs, RPE, Antioxidant, lcsh:Medicine (General), 030217 neurology & neurosurgery, Research Paper

Abstract

Oxidative damage is one of the major contributors to retinal degenerative diseases such as age-related macular degeneration (AMD), while RPE mediated antioxidant defense plays an important role in preventing retinopathies. However, the regulatory mechanisms of antioxidant signaling in RPE cells are poorly understood. Here we show that transcription factor MITF regulates the antioxidant response in RPE cells, protecting the neural retina from oxidative damage. In the oxidative stress-induced retinal degeneration mouse model, retinal degeneration in Mitf+/- mice is significantly aggravated compared to WT mice. In contrast, overexpression of Mitf in Dct-Mitf transgenic mice and AAV mediated overexpression in RPE cells protect the neural retina against oxidative damage. Mechanistically, MITF both directly regulates the transcription of NRF2, a master regulator of antioxidant signaling, and promotes its nuclear translocation. Furthermore, specific overexpression of NRF2 in Mitf+/- RPE cells activates antioxidant signaling and partially protects the retina from oxidative damage. Taken together, our findings demonstrate the regulation of NRF2 by MITF in RPE cells and provide new insights into potential therapeutic approaches for prevention of oxidative damage diseases., Graphical abstract Image 1, Highlights • MITF haploinsufficiency exacerbates oxidative stress-induced retinal degeneration. • Specific overexpression of MITF in RPE cells protects retinas from oxidative damage in vivo. • MITF directly regulates the transcription and nuclear translocation of NRF2. • Partial rescue of retinal oxidative damage in Mitf ±mice by gene transfer mediated RPE cell specific expression of NRF2.

Published

2020

37. A missense allele of PEX5 is responsible for the defective import of PTS2 cargo proteins into peroxisomes

Author

Saima Riazuddin, S. Amer Riazuddin, Michael L. Robinson, Xiaodong Jiao, Muhammad Ali, Mohsin Shahzad, Muhammad Hassaan Ali, Bushra Rauf, Asma A. Khan, Tânia Francisco, Jorge E. Azevedo, Azra Mehmood, Bushra Irum, Hang Qi, Javed Akram, Shehla Javed Akram, J. Fielding Hejtmancik, Muhammad Zaman Khan Assir, Myriam Baes, Firoz Kabir, Khaled K. Abu-Amero, Shahid Y. Khan, Tony A. Rodrigues, Sheikh Riazuddin, and Muhammad Asif Naeem

Subjects

Male, Peroxisome-Targeting Signal 1 Receptor, Genetic Linkage, Mutant, Mutation, Missense, Biological Transport, Active, Chromosomal translocation, Biology, Cataract, Peroxisomal Targeting Signals, 03 medical and health sciences, Consanguinity, Mice, Peroxisomal disorder, Lens, Crystalline, Sequestosome-1 Protein, Exome Sequencing, Genetics, medicine, Peroxisomes, Missense mutation, Animals, Humans, Genetics (clinical), 030304 developmental biology, Mice, Knockout, 0303 health sciences, Chromosomes, Human, Pair 12, Peroxisomal Targeting Signal 1, 030305 genetics & heredity, Peroxisome Targeting Signal 2, Peroxisome, medicine.disease, Cell biology, Cytosol, ATP-Binding Cassette Transporters, Female

Abstract

Peroxisomes, single-membrane intracellular organelles, play an important role in various metabolic pathways. The translocation of proteins from the cytosol to peroxisomes depends on peroxisome import receptor proteins and defects in peroxisome transport result in a wide spectrum of peroxisomal disorders. Here, we report a large consanguineous family with autosomal recessive congenital cataracts and developmental defects. Genome-wide linkage analysis localized the critical interval to chromosome 12p with a maximum two-point LOD score of 4.2 (θ = 0). Next-generation exome sequencing identified a novel homozygous missense variant (c.653 T > C; p.F218S) in peroxisomal biogenesis factor 5 (PEX5), a peroxisome import receptor protein. This missense mutation was confirmed by bidirectional Sanger sequencing. It segregated with the disease phenotype in the family and was absent in ethnically matched control chromosomes. The lens-specific knockout mice of Pex5 recapitulated the cataractous phenotype. In vitro import assays revealed a normal capacity of the mutant PEX5 to enter the peroxisomal Docking/Translocation Module (DTM) in the presence of peroxisome targeting signal 1 (PTS1) cargo protein, be monoubiquitinated and exported back into the cytosol. Importantly, the mutant PEX5 protein was unable to form a stable trimeric complex with peroxisomal biogenesis factor 7 (PEX7) and a peroxisome targeting signal 2 (PTS2) cargo protein and, therefore, failed to promote the import of PTS2 cargo proteins into peroxisomes. In conclusion, we report a novel missense mutation in PEX5 responsible for the defective import of PTS2 cargo proteins into peroxisomes resulting in congenital cataracts and developmental defects.

Published

2020

38. Mutations in CERKL and RP1 cause retinitis pigmentosa in Pakistani families

Author

Libe Gradstein, Raheela Nadeem, Xiaodong Jiao, Muhammad Asif Naeem, J. Fielding Hejtmancik, S. Amer Riazuddin, Jiali Li, Bushra Rauf, Muhammad Zaman Khan Assir, Firoz Kabir, Radha Ayyagari, and Sheikh Riazuddin

Subjects

lcsh:QH426-470, Nonsense mutation, lcsh:Life, Neurodegenerative, Biology, Eye, Biochemistry, Nyctalopia, 03 medical and health sciences, Exon, symbols.namesake, Rare Diseases, 0302 clinical medicine, Clinical Research, Genetic linkage, Retinitis pigmentosa, Genetics, medicine, Data Report, 2.1 Biological and endogenous factors, Aetiology, Eye Disease and Disorders of Vision, Molecular Biology, 030304 developmental biology, Sanger sequencing, 0303 health sciences, Genetic heterogeneity, Neurosciences, medicine.disease, eye diseases, lcsh:Genetics, lcsh:QH501-531, Genetic linkage study, 030221 ophthalmology & optometry, symbols, Genetic markers, medicine.symptom, Retinal Dystrophies

Abstract

This study was conducted to identify the genetic basis of retinal dystrophies in consanguineous Pakistani families. We recruited two families with retinitis pigmentosa (RP) displaying visual difficulties, including nyctalopia and constricted visual fields. Linkage analysis and Sanger sequencing resulted in the identification of a previously reported nonsense mutation, c.847C > T, in exon 5 of CERKL in one family and a novel four-base pair deletion in exon 4 of RP1, c.delAGAA4218_4221, leading to premature protein termination in the second family. Here, we report two RP-causing mutations extending the genetic heterogeneity of the disease.

Published

2020

39. Functional non-coding polymorphism in an EPHA2 promoter PAX2 binding site modifies expression and alters the MAPK and AKT pathways

Author

Zhiwei Ma, J. Fielding Hejtmancik, Xiaodong Jiao, and Xiaoyin Ma

Subjects

0301 basic medicine, MAPK/ERK pathway, Transcription, Genetic, lcsh:Medicine, Biology, Polymorphism, Single Nucleotide, Article, Receptor tyrosine kinase, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Humans, Binding site, Promoter Regions, Genetic, lcsh:Science, Protein kinase B, Gene, Gene knockdown, Binding Sites, Multidisciplinary, Receptor, EphA2, PAX2 Transcription Factor, lcsh:R, Epithelial Cells, Promoter, Molecular biology, 030104 developmental biology, 030221 ophthalmology & optometry, biology.protein, lcsh:Q, sense organs, Signal transduction, Signal Transduction

Abstract

To identify possible genetic variants influencing expression of EPHA2 (Ephrin-receptor Type-A2), a tyrosine kinase receptor that has been shown to be important for lens development and to contribute to both congenital and age related cataract when mutated, the extended promoter region of EPHA2 was screened for variants. SNP rs6603883 lies in a PAX2 binding site in the EPHA2 promoter region. The C (minor) allele decreased EPHA2 transcriptional activity relative to the T allele by reducing the binding affinity of PAX2. Knockdown of PAX2 in human lens epithelial (HLE) cells decreased endogenous expression of EPHA2. Whole RNA sequencing showed that extracellular matrix (ECM), MAPK-AKT signaling pathways and cytoskeleton related genes were dysregulated in EPHA2 knockdown HLE cells. Taken together, these results indicate a functional non-coding SNP in EPHA2 promoter affects PAX2 binding and reduces EPHA2 expression. They further suggest that decreasing EPHA2 levels alters MAPK, AKT signaling pathways and ECM and cytoskeletal genes in lens cells that could contribute to cataract. These results demonstrate a direct role for PAX2 in EPHA2 expression and help delineate the role of EPHA2 in development and homeostasis required for lens transparency.

Published

2017

40. Mutations and mechanisms in congenital and age-related cataracts

Author

Alan Shiels and J. Fielding Hejtmancik

Subjects

0301 basic medicine, Aging, medicine.medical_specialty, genetic structures, Visual impairment, Biology, Bioinformatics, medicine.disease_cause, Cataract, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Crystallin, Ophthalmology, Lens, Crystalline, medicine, Animals, Humans, Lens transparency, Lens crystalline, Mutation, Crystallins, eye diseases, Sensory Systems, 030104 developmental biology, medicine.anatomical_structure, Lens (anatomy), 030221 ophthalmology & optometry, sense organs, medicine.symptom, Age-related cataract

Abstract

The crystalline lens plays an important role in the refractive vision of vertebrates by facilitating variable fine focusing of light onto the retina. Loss of lens transparency, or cataract, is a frequently acquired cause of visual impairment in adults and may also present during childhood. Genetic studies have identified mutations in over 30 causative genes for congenital or other early-onset forms of cataract as well as several gene variants associated with age-related cataract. However, the pathogenic mechanisms resulting from genetic determinants of cataract are only just beginning to be understood. Here, we briefly summarize current concepts pointing to differences in the molecular mechanisms underlying congenital and age-related forms of cataract.

Published

2017

41. Homozygosity Mapping and Genetic Analysis of Autosomal Recessive Retinal Dystrophies in 144 Consanguineous Pakistani Families

Author

Chongfei Jin, Li Huang, J. Fielding Hejtmancik, Gowthaman Govindarajan, Shaheen N. Khan, Javed Akram, Oussama M’Hamdi, Xiaoyin Ma, Muhammad Asif Naeem, Jianjun Chen, Yabin Chen, Lin Li, S. Amer Riazuddin, Yan Ma, Wenmin Sun, Jiali Li, Nikhil Gupta, Zhiwei Ma, Paul A. Sieving, Patricia E. Cabrera, Xiaodong Jiao, Mukesh Tanwar, Radha Ayyagari, Sheikh Riazuddin, and Dan Jiang

Subjects

0301 basic medicine, Male, Candidate gene, Genetic Linkage, Population, Locus (genetics), Consanguinity, genetic analysis, Neurodegenerative, Biology, Ophthalmology & Optometry, Genetic analysis, Medical and Health Sciences, 03 medical and health sciences, 0302 clinical medicine, autosomal recessive retinal dystrophies, Clinical Research, Genetic linkage, Retinal Dystrophies, Genetics, 2.1 Biological and endogenous factors, Humans, Recessive, Genetic Predisposition to Disease, Pakistan, Genetic Testing, Aetiology, education, Eye Disease and Disorders of Vision, education.field_of_study, Genetic heterogeneity, Homozygote, Chromosome Mapping, Genetic Variation, Biological Sciences, Disease gene identification, Brain Disorders, Pedigree, 030104 developmental biology, consanguineous, Haplotypes, Genes, homozygosity mapping, 030221 ophthalmology & optometry, Female, Biotechnology, Microsatellite Repeats

Abstract

Author(s): Li, Lin; Chen, Yabin; Jiao, Xiaodong; Jin, Chongfei; Jiang, Dan; Tanwar, Mukesh; Ma, Zhiwei; Huang, Li; Ma, Xiaoyin; Sun, Wenmin; Chen, Jianjun; Ma, Yan; M'hamdi, Oussama; Govindarajan, Gowthaman; Cabrera, Patricia E; Li, Jiali; Gupta, Nikhil; Naeem, Muhammad Asif; Khan, Shaheen N; Riazuddin, Sheikh; Akram, Javed; Ayyagari, Radha; Sieving, Paul A; Riazuddin, S Amer; Hejtmancik, J Fielding | Abstract: PurposeThe Pakistan Punjab population has been a rich source for identifying genes causing or contributing to autosomal recessive retinal degenerations (arRD). This study was carried out to delineate the genetic architecture of arRD in the Pakistani population.MethodsThe genetic origin of arRD in a total of 144 families selected only for having consanguineous marriages and multiple members affected with arRD was examined. Of these, causative mutations had been identified in 62 families while only the locus had been identified for an additional 15. The remaining 67 families were subjected to homozygosity exclusion mapping by screening of closely flanking microsatellite markers at 180 known candidate genes/loci followed by sequencing of the candidate gene for pathogenic changes.ResultsOf these 67 families subjected to homozygosity mapping, 38 showed homozygosity for at least one of the 180 regions, and sequencing of the corresponding genes showed homozygous cosegregating mutations in 27 families. Overall, mutations were detected in approximately 61.8 % (89/144) of arRD families tested, with another 10.4% (15/144) being mapped to a locus but without a gene identified.ConclusionsThese results suggest the involvement of unmapped novel genes in the remaining 27.8% (40/144) of families. In addition, this study demonstrates that homozygosity mapping remains a powerful tool for identifying the genetic defect underlying genetically heterogeneous arRD disorders in consanguineous marriages for both research and clinical applications.

Published

2017

42. Mutations in

Author

Hira, Iqbal, Shahid Y, Khan, Lin, Zhou, Bushra, Irum, Muhammad, Ali, Mariya R, Ahmed, Mohsin, Shahzad, Muhammad Hassaan, Ali, Muhammad Asif, Naeem, Sheikh, Riazuddin, J Fielding, Hejtmancik, and S Amer, Riazuddin

Subjects

Adult, Male, Genetic Linkage, Mutation, Missense, Genes, Recessive, Cataract, Consanguinity, Humans, Family, Genetic Predisposition to Disease, Pakistan, Child, Frameshift Mutation, Alleles, Phylogeny, Homozygote, Infant, eye diseases, Pedigree, Haplotypes, Codon, Nonsense, Child, Preschool, Female, Chromosomes, Human, Pair 3, Microtubule-Associated Proteins, Microsatellite Repeats, Research Article

Abstract

Purpose This study was designed to identify the pathogenic variants in three consanguineous families with congenital cataracts segregating as a recessive trait. Methods Consanguineous families with multiple individuals manifesting congenital cataracts were ascertained. All participating members underwent an ophthalmic examination. A small aliquot of the blood sample was collected from all participating individuals, and genomic DNAs were extracted. Homozygosity-based linkage analysis was performed using short tandem repeat (STR) markers. The haplotypes were constructed with alleles of the STR markers, and the two-point logarithm of odds (LOD) scores were calculated. The candidate gene was sequenced bidirectionally to identify the disease-causing mutations. Results Linkage analysis localized the disease interval to chromosome 3p in three families. Subsequently, bidirectional Sanger sequencing identified two novel mutations—a single base deletion resulting in a frameshift (c.3196delC; p.His1066IlefsTer10) mutation and a single base substitution resulting in a nonsense (c.4270C>T; p.Arg1424Ter) mutation—and a known missense (c.4127T>C, p.Leu1376Pro) mutation in FYCO1. All three mutations showed complete segregation with the disease phenotype and were absent in 96 ethnically matched control individuals. Conclusions We report two novel mutations and a previously reported mutation in FYCO1 in three large consanguineous families. Taken together, mutations in FYCO1 contribute nearly 15% to the total genetic load of autosomal recessive congenital cataracts in this cohort.

Published

2019

43. Structural variations in a non-coding region at 1q32.1 are responsible for the NYS7 locus in two large families

Author

Xueshan Xiao, Panfeng Wang, Wenmin Sun, J. Fielding Hejtmancik, Xiaoyun Jia, Shiqiang Li, and Qingjiong Zhang

Subjects

Male, Genetic Linkage, Pseudogene, Locus (genetics), Biology, DNA sequencing, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Genetics, Coding region, Humans, Gene, Genetics (clinical), 030304 developmental biology, Original Investigation, Sanger sequencing, 0303 health sciences, Whole Genome Sequencing, Breakpoint, Chromosome Mapping, Membrane Proteins, Genetic Diseases, X-Linked, Human genetics, Pedigree, Cytoskeletal Proteins, Genomic Structural Variation, Mutation, symbols, Female, Nystagmus, Congenital, 030217 neurology & neurosurgery, Gene Deletion

Abstract

Congenital motor nystagmus (CMN) is characterized by early-onset bilateral ocular oscillations without other ocular deficits. To date, mutations in only one gene have been identified to be responsible for CMN, i.e., FRMD7 for X-linked CMN. Four loci for autosomal dominant CMN, including NYS7 (OMIM 614826), have been mapped but the causative genes have yet to be identified. NYS7 was mapped to 1q32.1 based on independent genome-wide linkage scan on two large families with CMN. In this study, mutations in all known protein-coding genes, both intronic sequence with predicted effect and coding sequence, in the linkage interval were excluded by whole-genome sequencing. Then, long-read genome sequencing based on the Nanopore platform was performed with a sample from each of the two families. Two deletions with an overlapping region of 775,699 bp, located in a region without any known protein-coding genes, were identified in the two families in the linkage region. The two deletions as well as their breakpoints were confirmed by Sanger sequencing and co-segregated with CMN in the two families. The 775,699 bp deleted region contains uncharacterized non-protein-coding expressed sequences and pseudogenes but no protein-coding genes. However, Hi-C data predicted that the deletions span two topologically associated domains and probably lead to a change in the 3D genomic architecture. These results provide novel evidence of a strong association between structural variations in non-coding genomic regions and human hereditary diseases like CMN with a potential mechanism involving changes in 3D genome architecture, which provides clues regarding the molecular pathogenicity of CMN. Electronic supplementary material The online version of this article (10.1007/s00439-020-02156-0) contains supplementary material, which is available to authorized users.

Published

2019

44. Thyroid hormone receptor beta mutations alter photoreceptor development and function inDanio rerio(zebrafish)

Author

Sachihiro C. Suzuki, Takeshi Yoshimatsu, Asha Krishnakumar, Ciana Deveau, Xiaodong Jiao, Ralph Nelson, and J. Fielding Hejtmancik

Subjects

Photoreceptors, Life Cycles, Cancer Research, Opsin, Sensory Receptors, genetic structures, Mutant, Social Sciences, QH426-470, Animals, Genetically Modified, chemistry.chemical_compound, Larvae, 0302 clinical medicine, INDEL Mutation, Animal Cells, Medicine and Health Sciences, Psychology, Frameshift Mutation, Zebrafish, Genetics (clinical), Sequence Deletion, Neurons, 0303 health sciences, biology, Chemistry, Genes, erbA, Gene Expression Regulation, Developmental, Eukaryota, Cell Differentiation, Thyroid Hormone Receptors beta, Animal Models, Cone Opsins, Cell biology, medicine.anatomical_structure, Experimental Organism Systems, Osteichthyes, Larva, Models, Animal, Vertebrates, Photoreceptor Cells, Invertebrate, Sensory Perception, Cellular Types, Anatomy, Erg, Research Article, Signal Transduction, Imaging Techniques, Fish Biology, Ocular Anatomy, Transgene, Danio, Research and Analysis Methods, Retina, Frameshift mutation, Thyroid hormone receptor beta, 03 medical and health sciences, Model Organisms, Ocular System, Fluorescence Imaging, Fish Physiology, Genetics, medicine, Animals, Animal Physiology, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Thyroid hormone receptor, Color Vision, Organisms, Biology and Life Sciences, Afferent Neurons, Retinal, Cell Biology, Zebrafish Proteins, biology.organism_classification, Vertebrate Physiology, Fish, Cellular Neuroscience, Mutation, Trans-Activators, Animal Studies, Eyes, sense organs, Head, Zoology, 030217 neurology & neurosurgery, Developmental Biology, Neuroscience

Abstract

We investigate mutations in trβ2, a splice variant of thrb, identifying changes in function, structure, and behavior in larval and adult zebrafish retinas. Two N-terminus CRISPR mutants were identified. The first is a 6BP+1 insertion deletion frameshift resulting in a truncated protein. The second is a 3BP in frame deletion with intact binding domains. ERG recordings of isolated cone signals showed that the 6BP+1 mutants did not respond to red wavelengths of light while the 3BP mutants did respond. 6BP+1 mutants lacked optomotor and optokinetic responses to red/black and green/black contrasts. Both larval and adult 6BP+1 mutants exhibit a loss of red-cone contribution to the ERG and an increase in UV-cone contribution. Transgenic reporters show loss of cone trβ2 activation in the 6BP+1 mutant but increase in the density of cones with active blue, green, and UV opsin genes. Antibody reactivity for red-cone LWS1 and LWS2 opsin was absent in the 6BP+1 mutant, as was reactivity for arrestin3a. Our results confirm a critical role for trβ2 in long-wavelength cone development., Author summary There are four cone photoreceptors responsible for color vision in zebrafish: red, green, blue, and UV. The thyroid hormone receptor trβ2 is localized in the vertebrate retina. We know that it is necessary for the development of cones expressing long-wavelength-sensitive opsins (red cones), but here we investigate the functional alterations that accompany a loss of trβ2. Our work contributes to the ongoing investigations of retinal development and the involvement of thyroid hormone receptors. As suggested by previous morphological findings, fish became red colorblind when trβ2 was knocked out, and the contributions of the other three cone types shifted. Our work highlights the plasticity of photoreceptor patterning as we see changes in opsin peaks and cone sensitivity, increases in contributions of UV cones, and an attempt at a mosaic pattern in the adult retina, all in the absence of trβ2 and red cones. We now have an increased understanding of mechanisms underlying retinal development.

Published

2019

45. Apoferritin is maintaining the native conformation of citrate synthase

Author

Yuri V, Sergeev, Monika B, Dolinska, and J Fielding, Hejtmancik

Subjects

molecular crowding, ferritin, protection of protein catalytic activity, Article, apoferritin, chaperoning-like property

Abstract

Ferritin, a member of a family of iron storage proteins, is expressed in conditions of oxidative or thermal stress in the cell. Ferritin widely found in human tissues including the eye and brain. Increased expression under oxidative or temperature stress conditions and protective effect on cell viability suggest that apo form of ferritin (apoferritin) may have a role in the formation or maintenance of the native conformation of proteins. To test this hypothesis, we studied the influence of apoferritin on the unfolding and refolding of citrate synthase (CS) in vitro. Here we show that at stoichiometric amounts apoferritin is remarkably protecting the CS catalytic activity, stabilize the aggregation of CS under heat stress and act as chaperone-like molecules in these folding reactions in vitro. Furthermore, apoferritin promote the functional refolding of CS after guanidinium hydrochloride denaturation. Finally, these results confirm that apoferritin has chaperone-like activity in vitro and suggests that apoferritin might have a role in protection and maintaining of protein native conformation.

Published

2019

46. Variants in three probands by whole-exome sequencing v1

Author

Xueshan Xiao, Wenmin Sun, Jiamin Ouyang, Shiqiang Li, Xiaoyun Jia, Zhiqun Tan, J. Fielding Hejtmancik, and Qingjiong Zhang

Abstract

High hyperopia is a common and severe form of refractive error. Genetic factors play important roles in the development of high hyperopia but the exact gene responsible for this condition is mostly unknown. We identified a large Chinese family with autosomal dominant high hyperopia. A genome-wide linkage scan mapped the high hyperopia to chromosome 11p12-q13.3, with maximum log of the odds (LOD) scores of 4.68 at theta=0 for D11S987. Parallel whole-exome sequencing detected a novel c.3377delG (p.Gly1126Valfs*31) heterozygous mutation in the MYRF gene within the linkage interval. Whole-exome sequencing in other 121 probands with high hyperopia identified additional novel mutations in MYRF within two other families: a de novo c.3274_3275delAG (p.Leu1093Profs*22) heterozygous mutation and a c.3194+2T>C heterozygous mutation. All three mutations are located in the C-terminal region of MYRF and are predicted to result in truncation of that portion. Two patients from two of the three families developed angle-closure glaucoma. These three mutations were present in neither the ExAC database nor our in-house whole-exome sequencing data from 3280 individuals. No other truncation mutations in MYRF were detected in the 3280 individuals. Knockdown of myrf resulted in small eye size in zebrafish. These evidence all support that truncation mutations in the C-terminal region of MYRF are responsible for autosomal dominant high hyperopia in these families. Our results may provide useful clues for further understanding the functional role of the C-terminal region of this critical myelin regulatory factor, as well as the molecular pathogenesis of high hyperopia and its associated angle-closure glaucoma.

Published

2019

47. Human βA3/A1-crystallin splicing mutation causes cataracts by activating the unfolded protein response and inducing apoptosis in differentiating lens fiber cells

Author

Chitra Kannabiran, Eric F. Wawrousek, Zhiwei Ma, Chi-Chao Chan, J. Fielding Hejtmancik, and Wenliang Yao

Subjects

0301 basic medicine, RNA Splicing, Nonsense-mediated decay, Mutant, Apoptosis, Mice, Transgenic, Biology, Article, Cataract, Cell Line, beta-Crystallin A Chain, 03 medical and health sciences, 0302 clinical medicine, Cataracts, Crystallin, Lens, Crystalline, medicine, Animals, Humans, Protein Isoforms, RNA, Messenger, Molecular Biology, Sequence Deletion, Base Sequence, Exons, medicine.disease, Molecular biology, eye diseases, Lens Fiber, 030104 developmental biology, RNA splicing, Unfolded Protein Response, 030221 ophthalmology & optometry, Unfolded protein response, Molecular Medicine, Protein folding, sense organs

Abstract

βγ-Crystallins, having a uniquely stable two domain four Greek key structure, are crucial for transparency of the eye lens,. Mutations in lens crystallins have been proposed to cause cataract formation by a variety of mechanisms most of which involve destabilization of the protein fold. The underlying molecular mechanism for autosomal dominant zonular cataracts with sutural opacities in an Indian family caused by a c.215+1G>A splice mutation in the βA3/A1-crystallin gene CRYBA1 was elucidated using three transgenic mice models. This mutation causes a splice defect in which the mutant mRNA escapes nonsense mediated decay by skipping both exons 3 and 4. Skipping these exons results in an in-frame deletion of the mRNA and synthesis of an unstable p.Ile33_Ala119del mutant βA3/A1-crystallin protein. Transgenic expression of mutant βA3/A1-crystallin but not the wild type protein results in toxicity and abnormalities in the maturation and orientation of differentiating lens fibers in c.97_357del CRYBA1 transgenic mice, leading to a small spherical lens, cataract, and often lens capsule rupture. On a cellular level, the lenses accumulated p.Ile33_Ala119del βA3/A1-crystallin with resultant activation of the stress signaling pathway - unfolded protein response (UPR) and inhibition of normal protein synthesis, culminating in apoptosis. This highlights the mechanistic contrast between mild mutations that destabilize crystallins and other proteins, resulting in their being bound by the α-crystallins that buffer lens cells against damage by denatured proteins, and severely misfolded proteins that are not bound by α-crystallin but accumulate and have a direct toxic effect on lens cells, resulting in early onset cataracts.

Published

2016

48. Mutation in the intracellular chloride channel CLCC1 associated with autosomal recessive retinitis pigmentosa

Author

Michel Michaelides, Sheikh Riazuddin, Yan Ma, Lin Li, Muhammad Ali, Muhammad Imran Khan, Ralph Nelson, Ahmed Salman, S. Amer Riazuddin, J. Fielding Hejtmancik, Siying Lin, Andrew H. Crosby, Zeynep Coban Akdemir, Longhua Zhang, James Fasham, Gavin Arno, Abdul Hameed, Chi-Chao Chan, Paul A. Sieving, Raheel Qamar, Sarah Hull, Muhammad Asif Naeem, John K. Chilton, Frans P.M. Cremers, Shalini N. Jhangiani, Xiaodong Jiao, Firoz Kabir, Barry A. Chioza, Ilaria D'Atri, James R. Lupski, Zhiwei Ma, Radha Ayyagari, Fumihito Ono, Naoki Nakaya, Xiaoying Cai, Gaurav V. Harlalka, Jay E. Self, Emma L. Baple, Javed Akram, Anthony T. Moore, Holly Hardy, and Mundlos, Stefan

Subjects

0301 basic medicine, Cancer Research, Cytoplasm, genetic structures, Neurodegenerative, Eye, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], chemistry.chemical_compound, Mice, 0302 clinical medicine, Retinal Rod Photoreceptor Cells, 2.1 Biological and endogenous factors, Pakistan, Aetiology, Zebrafish, Genetics (clinical), Mice, Knockout, biology, Homozygote, medicine.anatomical_structure, Chloride channel, Retinal Cone Photoreceptor Cells, Erg, Intracellular, Retinitis Pigmentosa, Asian Continental Ancestry Group, lcsh:QH426-470, Knockout, Mutation, Missense, Retina, Cell Line, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Rare Diseases, Asian People, Chloride Channels, medicine, Genetics, Animals, Humans, Eye Proteins, Molecular Biology, Eye Disease and Disorders of Vision, Ecology, Evolution, Behavior and Systematics, CLCC1, Wild type, Neurosciences, Retinal, biology.organism_classification, Molecular biology, eye diseases, lcsh:Genetics, 030104 developmental biology, HEK293 Cells, chemistry, Mutation, biology.protein, sense organs, Missense, 030217 neurology & neurosurgery, Developmental Biology

Abstract

We identified a homozygous missense alteration (c.75C>A, p.D25E) in CLCC1, encoding a presumptive intracellular chloride channel highly expressed in the retina, associated with autosomal recessive retinitis pigmentosa (arRP) in eight consanguineous families of Pakistani descent. The p.D25E alteration decreased CLCC1 channel function accompanied by accumulation of mutant protein in granules within the ER lumen, while siRNA knockdown of CLCC1 mRNA induced apoptosis in cultured ARPE-19 cells. TALEN KO in zebrafish was lethal 11 days post fertilization. The depressed electroretinogram (ERG) cone response and cone spectral sensitivity of 5 dpf KO zebrafish and reduced eye size, retinal thickness, and expression of rod and cone opsins could be rescued by injection of wild type CLCC1 mRNA. Clcc1+/-KO mice showed decreased ERGs and photoreceptor number. Together these results strongly suggest that intracellular chloride transport by CLCC1 is a critical process in maintaining retinal integrity, and CLCC1 is crucial for survival and function of retinal cells.

Published

2018

49. Identification of Novel Deletions as the Underlying Cause of Retinal Degeneration in Two Pedigrees

Author

Kari, Branham, Aditya A, Guru, Igor, Kozak, Pooja, Biswas, Mohammad, Othman, Kameron, Kishaba, Hassan, Mansoor, Sheikh, Riazuddin, John R, Heckenlively, S Amer, Riazuddin, J Fielding, Hejtmancik, Paul A, Sieving, and Radha, Ayyagari

Subjects

Male, Genetic Linkage, Retinal Degeneration, Pedigree, Consanguinity, Haplotypes, Codon, Nonsense, Genes, X-Linked, North America, Exome Sequencing, Humans, Female, Pakistan, Eye Proteins, Adaptor Proteins, Signal Transducing, Sequence Deletion

Abstract

Retinal dystrophies are a phenotypically and genetically complex group of conditions. Because of this complexity, it can be challenging in many families to determine the inheritance based on pedigree analysis alone. Clinical examinations were performed and blood samples were collected from a North American (M1186) and a consanguineous Pakistani (PKRD168) pedigree affected with two different retinal dystrophies (RD). Based on the structure of the pedigrees, inheritance patterns in the families were difficult to determine. In one family, linkage analysis was performed with markers on X-chromosome. In the second family, whole-exome sequencing (WES) was performed. Subsequent Sanger sequencing of genes of interest was performed. Linkage and haplotype analysis localized the disease interval to a 70 Mb region on the X chromosome that encompassed RP2 and RPGR in M1186 . The disease haplotype segregated with RD in all individuals except for an unaffected man (IV:3) and his affected son (V:1) in this pedigree. Subsequent analysis identified a novel RPGR mutation (p. Lys857Glu fs221X) in all affected members of M1186 except V:1. This information suggests that there is an unidentified second cause of retinitis pigmentosa (RP) within the family. A novel two-base-pair deletion (p. Tyr565Ter fsX) in CHM (choroideremia) was found to segregate with RD in PKRD168. This paper highlights the challenges of interpreting family history in families with RD and reports on the identification of novel mutations in two RD families.

Published

2018

50. Whole-Exome Sequencing Identifies Novel Variants that Co-segregates with Autosomal Recessive Retinal Degeneration in a Pakistani Pedigree

Author

Pooja, Biswas, Muhammad Asif, Naeem, Muhammad Hassaan, Ali, Muhammad Zaman, Assir, Shaheen N, Khan, Sheikh, Riazuddin, J Fielding, Hejtmancik, S Amer, Riazuddin, and Radha, Ayyagari

Subjects

Sequence Homology, Amino Acid, Genetic Linkage, Chromosomes, Human, Pair 11, DNA Mutational Analysis, Retinal Degeneration, Genes, Recessive, Polymorphism, Single Nucleotide, Pedigree, DNA-Binding Proteins, Consanguinity, INDEL Mutation, Species Specificity, Exome Sequencing, Animals, Humans, Pakistan, Sequence Alignment, Conserved Sequence, Transcription Factors

Abstract

To identify the molecular basis of inherited retinal degeneration (IRD) in a familial case of Pakistani origin using whole-exome sequencing.A thorough ophthalmic examination was completed, and genomic DNA was extracted using standard protocols. Whole exome(s) were captured with Agilent V5 + UTRs probes and sequenced on Illumina HiSeq genome analyzer. The exomeSuite software was used to filter variants, and the candidate causal variants were prioritized, examining their allele frequency and PolyPhen2, SIFT, and MutationTaster predictions. Sanger dideoxy sequencing was performed to confirm the segregation with disease phenotype and absence in ethnicity-matched control chromosomes.Ophthalmic examination confirmed retinal degeneration in all affected individuals that segregated as an autosomal recessive trait in the family. Whole-exome sequencing identified two homozygous missense variants: c.1304G A; p.Arg435Gln in ZNF408 (NM_024741) and c.902G A; p.Gly301Asp in C1QTNF4 (NM_031909). Both variants segregated with the retinal phenotype in the PKRD320 and were absent in ethnically matched control chromosomes.Whole-exome sequencing coupled with bioinformatics analysis identified potential novel variants that might be responsible for IRD.

Published

2018