Your search keyword '"Brink, JB"' showing total 121 results

101. Gene expression and functional annotation of the human ciliary body epithelia.

Author

Janssen SF, Gorgels TG, Bossers K, Ten Brink JB, Essing AH, Nagtegaal M, van der Spek PJ, Jansonius NM, and Bergen AA

Subjects

Glaucoma genetics, Humans, Oligonucleotide Array Sequence Analysis, Ciliary Body cytology, Gene Expression Profiling, Pigment Epithelium of Eye cytology, Pigment Epithelium of Eye metabolism

Abstract

Purpose: The ciliary body (CB) of the human eye consists of the non-pigmented (NPE) and pigmented (PE) neuro-epithelia. We investigated the gene expression of NPE and PE, to shed light on the molecular mechanisms underlying the most important functions of the CB. We also developed molecular signatures for the NPE and PE and studied possible new clues for glaucoma., Methods: We isolated NPE and PE cells from seven healthy human donor eyes using laser dissection microscopy. Next, we performed RNA isolation, amplification, labeling and hybridization against 44×k Agilent microarrays. For microarray conformations, we used a literature study, RT-PCRs, and immunohistochemical stainings. We analyzed the gene expression data with R and with the knowledge database Ingenuity., Results: The gene expression profiles and functional annotations of the NPE and PE were highly similar. We found that the most important functionalities of the NPE and PE were related to developmental processes, neural nature of the tissue, endocrine and metabolic signaling, and immunological functions. In total 1576 genes differed statistically significantly between NPE and PE. From these genes, at least 3 were cell-specific for the NPE and 143 for the PE. Finally, we observed high expression in the (N)PE of 35 genes previously implicated in molecular mechanisms related to glaucoma., Conclusion: Our gene expression analysis suggested that the NPE and PE of the CB were quite similar. Nonetheless, cell-type specific differences were found. The molecular machineries of the human NPE and PE are involved in a range of neuro-endocrinological, developmental and immunological functions, and perhaps glaucoma.

Published

2012

102. Common genetic determinants of intraocular pressure and primary open-angle glaucoma.

Author

van Koolwijk LM, Ramdas WD, Ikram MK, Jansonius NM, Pasutto F, Hysi PG, Macgregor S, Janssen SF, Hewitt AW, Viswanathan AC, ten Brink JB, Hosseini SM, Amin N, Despriet DD, Willemse-Assink JJ, Kramer R, Rivadeneira F, Struchalin M, Aulchenko YS, Weisschuh N, Zenkel M, Mardin CY, Gramer E, Welge-Lüssen U, Montgomery GW, Carbonaro F, Young TL, Bellenguez C, McGuffin P, Foster PJ, Topouzis F, Mitchell P, Wang JJ, Wong TY, Czudowska MA, Hofman A, Uitterlinden AG, Wolfs RC, de Jong PT, Oostra BA, Paterson AD, Mackey DA, Bergen AA, Reis A, Hammond CJ, Vingerling JR, Lemij HG, Klaver CC, and van Duijn CM

Subjects

Aged, Aged, 80 and over, Case-Control Studies, Ciliary Body metabolism, Ciliary Body pathology, Female, Humans, Male, Middle Aged, Optic Nerve metabolism, Optic Nerve pathology, Polymorphism, Single Nucleotide, Trabecular Meshwork metabolism, Trabecular Meshwork pathology, Genome-Wide Association Study, Glaucoma, Open-Angle genetics, Intraocular Pressure genetics, Nerve Tissue Proteins genetics

Abstract

Intraocular pressure (IOP) is a highly heritable risk factor for primary open-angle glaucoma and is the only target for current glaucoma therapy. The genetic factors which determine IOP are largely unknown. We performed a genome-wide association study for IOP in 11,972 participants from 4 independent population-based studies in The Netherlands. We replicated our findings in 7,482 participants from 4 additional cohorts from the UK, Australia, Canada, and the Wellcome Trust Case-Control Consortium 2/Blue Mountains Eye Study. IOP was significantly associated with rs11656696, located in GAS7 at 17p13.1 (p=1.4×10(-8)), and with rs7555523, located in TMCO1 at 1q24.1 (p=1.6×10(-8)). In a meta-analysis of 4 case-control studies (total N = 1,432 glaucoma cases), both variants also showed evidence for association with glaucoma (p=2.4×10(-2) for rs11656696 and p=9.1×10(-4) for rs7555523). GAS7 and TMCO1 are highly expressed in the ciliary body and trabecular meshwork as well as in the lamina cribrosa, optic nerve, and retina. Both genes functionally interact with known glaucoma disease genes. These data suggest that we have identified two clinically relevant genes involved in IOP regulation., Competing Interests: The authors have declared that no competing interests exist.

Published

2012

103. Multicenter cohort association study of SLC2A1 single nucleotide polymorphisms and age-related macular degeneration.

Author

Baas DC, Ho L, Tanck MW, Fritsche LG, Merriam JE, van het Slot R, Koeleman BP, Gorgels TG, van Duijn CM, Uitterlinden AG, de Jong PT, Hofman A, ten Brink JB, Vingerling JR, Klaver CC, Dean M, Weber BH, Allikmets R, Hageman GS, and Bergen AA

Subjects

Aged, Aged, 80 and over, Case-Control Studies, Cohort Studies, Female, Gene Frequency, Genetic Association Studies, Germany epidemiology, Haplotypes, Heterozygote, Homozygote, Humans, Linkage Disequilibrium, Macular Degeneration epidemiology, Male, Middle Aged, Netherlands epidemiology, Phenotype, United States epidemiology, Eye Proteins genetics, Glucose Transporter Type 1 genetics, Macular Degeneration genetics, Polymorphism, Single Nucleotide, White People

Abstract

Purpose: Age-related macular degeneration (AMD) is a major cause of blindness in older adults and has a genetically complex background. This study examines the potential association between single nucleotide polymorphisms (SNPs) in the glucose transporter 1 (SLC2A1) gene and AMD. SLC2A1 regulates the bioavailability of glucose in the retinal pigment epithelium (RPE), which might influence oxidative stress-mediated AMD pathology., Methods: Twenty-two SNPs spanning the SLC2A1 gene were genotyped in 375 cases and 199 controls from an initial discovery cohort (the Amsterdam-Rotterdam-Netherlands study). Replication testing was performed in The Rotterdam Study (the Netherlands) and study populations from Würzburg (Germany), the Age Related Eye Disease Study (AREDS; United States), Columbia University (United States), and Iowa University (United States). Subsequently, a meta-analysis of SNP association was performed., Results: In the discovery cohort, significant genotypic association between three SNPs (rs3754219, rs4660687, and rs841853) and AMD was found. Replication in five large independent (Caucasian) cohorts (4,860 cases and 4,004 controls) did not yield consistent association results. The genotype frequencies for these SNPs were significantly different for the controls and/or cases among the six individual populations. Meta-analysis revealed significant heterogeneity of effect between the studies., Conclusions: No overall association between SLC2A1 SNPs and AMD was demonstrated. Since the genotype frequencies for the three SLC2A1 SNPs were significantly different for the controls and/or cases between the six cohorts, this study corroborates previous evidence that population dependent genetic risk heterogeneity in AMD exists.

Published

2012

104. Ultrastructural localization and expression of TRPM1 in the human retina.

Author

Klooster J, Blokker J, Ten Brink JB, Unmehopa U, Fluiter K, Bergen AA, and Kamermans M

Subjects

Eye Banks, Humans, Immunohistochemistry, In Situ Hybridization, Microscopy, Electron, Retina cytology, Retinal Bipolar Cells ultrastructure, Retinal Rod Photoreceptor Cells ultrastructure, Synapses metabolism, Synapses ultrastructure, TRPM Cation Channels genetics, Dendrites metabolism, Retina metabolism, Retinal Bipolar Cells metabolism, Retinal Rod Photoreceptor Cells metabolism, TRPM Cation Channels metabolism

Abstract

Purpose: Transient receptor potential subfamily melastatin (TRPM)1 cation channels of retinal ON-bipolar cells are modulated via a mGluR6 (GMR6) signaling cascade. While light-microscopy shows these channels are located on the tips of ON-bipolar cells dendrites, near rod and cone synaptic ribbons, TRPM1 localization at the electron-microscope level is currently not described. The authors report here the ultrastructural localization of TRPM1 in the human retina., Methods: TRPM1 was localized in postmortem human retinas by immunohistochemistry at both the light and electron microscope levels. Additionally, TRPM1 expression was studied using in situ hybridization, laser dissection microscopy, and PCR techniques., Results: TRPM1-immunoreactivity was located on the dendrites and soma of ON-bipolar cells at the light microscope level. At the electron microscope level TRPM1-immunoreactivity was located on the tips of ON-bipolar cell dendrites that were invaginating cone pedicles and rod spherules. In addition, TRPM1-immunoreactivity was occasionally found on the rod spherules ribbons, suggesting that at least a proportion of rods may also express TRPM1. In situ hybridization showed TRPM1 encoding RNA in inner nuclear layer somata and in some photoreceptors. The presence of TRPM1-RNA in photoreceptors was confirmed by PCR in pure photoreceptor material obtained with a laser dissection microscope., Conclusions: In the human retina TRPM1 is expressed on ON-bipolar cell dendrites that invaginate photoreceptor terminals. TRPM1 is also expressed on the synaptic ribbons of a subclass of rods, suggesting a dual function for TRPM1 in the ON-pathway.

Published

2011

105. The ERCC6 gene and age-related macular degeneration.

Author

Baas DC, Despriet DD, Gorgels TG, Bergeron-Sawitzke J, Uitterlinden AG, Hofman A, van Duijn CM, Merriam JE, Smith RT, Barile GR, ten Brink JB, Vingerling JR, Klaver CC, Allikmets R, Dean M, and Bergen AA

Subjects

Aged, Aged, 80 and over, Analysis of Variance, Case-Control Studies, Female, Gene Frequency, Genetic Predisposition to Disease, Genotype, Humans, Linkage Disequilibrium, Macular Degeneration pathology, Male, Meta-Analysis as Topic, Middle Aged, Poly-ADP-Ribose Binding Proteins, Prospective Studies, Risk Factors, DNA Helicases genetics, DNA Repair Enzymes genetics, Macular Degeneration genetics, Polymorphism, Single Nucleotide, Promoter Regions, Genetic genetics

Abstract

Background: Age-related macular degeneration (AMD) is the leading cause of irreversible visual loss in the developed countries and is caused by both environmental and genetic factors. A recent study (Tuo et al., PNAS) reported an association between AMD and a single nucleotide polymorphism (SNP) (rs3793784) in the ERCC6 (NM_000124) gene. The risk allele also increased ERCC6 expression. ERCC6 is involved in DNA repair and mutations in ERCC6 cause Cockayne syndrome (CS). Amongst others, photosensitivity and pigmentary retinopathy are hallmarks of CS., Methodology/principal Findings: Separate and combined data from three large AMD case-control studies and a prospective population-based study (The Rotterdam Study) were used to analyse the genetic association between ERCC6 and AMD (2682 AMD cases and 3152 controls). We also measured ERCC6 mRNA levels in retinal pigment epithelium (RPE) cells of healthy and early AMD affected human donor eyes. Rs3793784 conferred a small increase in risk for late AMD in the Dutch population (The Rotterdam and AMRO-NL study), but this was not replicated in two non-European studies (AREDS, Columbia University). In addition, the AMRO-NL study revealed no significant association for 9 other variants spanning ERCC6. Finally, we determined that ERCC6 expression in the human RPE did not depend on rs3793784 genotype, but, interestingly, on AMD status: Early AMD-affected donor eyes had a 50% lower ERCC6 expression than healthy donor eyes (P = 0.018)., Conclusions/significance: Our meta-analysis of four Caucasian cohorts does not replicate the reported association between SNPs in ERCC6 and AMD. Nevertheless, our findings on ERCC6 expression in the RPE suggest that ERCC6 may be functionally involved in AMD. Combining our data with those of the literature, we hypothesize that the AMD-related reduced transcriptional activity of ERCC6 may be caused by diverse, small and heterogeneous genetic and/or environmental determinants.

Published

2010

106. Course of visual decline in relation to the Best1 genotype in vitelliform macular dystrophy.

Author

Booij JC, Boon CJ, van Schooneveld MJ, ten Brink JB, Bakker A, de Jong PT, Hoyng CB, Bergen AA, and Klaver CC

Subjects

Adolescent, Adult, Age of Onset, Aged, Aged, 80 and over, Bestrophins, Child, Chromatography, High Pressure Liquid, DNA Mutational Analysis, Electrooculography, Female, Genotype, Humans, Macular Degeneration physiopathology, Male, Middle Aged, Pedigree, Phenotype, Retrospective Studies, Chloride Channels genetics, Eye Proteins genetics, Macular Degeneration genetics, Mutation, Vision Disorders physiopathology, Visual Acuity physiology

Abstract

Purpose: To describe the disease course in patients with vitelliform macular dystrophy (VMD) with a Best1 mutation and to determine the association between Best1 genotype and visual prognosis., Design: Consecutive case series., Participants: Fifty-three patients with VMD with Best1 mutations from 27 Dutch families, aged 11 to 87 years., Methods: Best-corrected visual acuity (VA), fundus appearance, and Arden ratio on the electro-oculogram (EOG) during clinical follow-up were assessed from medical records. Mutation analysis of the Best1 gene was performed on DNA samples using denaturing high-pressure liquid chromatography and direct sequencing., Main Outcome Measures: Cumulative lifetime risk of visual decline below 0.5, 0.3, and 0.1 for the entire group and stratified for genotype., Results: Median age of onset of visual symptoms was 33 years (range: 2-78). The cumulative risk of VA below 0.5 (20/40) was 50% at 55 years and 75% at 66 years. The cumulative risk of decline less than 0.3 (20/63) was 50% by age 66 years and 75% by age 74 years. Two patients progressed to VA less than 0.1 (20/200). Fourteen different mutations were found. Most patients (96%) had missense mutations; the Thr6Pro, Ala10Val, and Tyr227Asn mutations were most common. Visual decline was significantly faster in patients with an Ala10Val mutation than either the Thr6Pro or the Tyr227Asn mutation (P=0.001)., Conclusions: Age of onset of visual symptoms varies greatly among patients with VMD. All patients show a gradual decrease in VA, and most progress to visual impairment at a relatively late age. Our data suggest a phenotype-genotype correlation, because the Ala10Val mutation has a more rapid disease progression than other common mutations., Financial Disclosure(s): The author(s) have no proprietary or commercial interest in any materials discussed in this article., (Copyright 2010 American Academy of Ophthalmology. Published by Elsevier Inc. All rights reserved.)

Published

2010

107. Dietary magnesium, not calcium, prevents vascular calcification in a mouse model for pseudoxanthoma elasticum.

Author

Gorgels TG, Waarsing JH, de Wolf A, ten Brink JB, Loves WJ, and Bergen AA

Subjects

ATP-Binding Cassette Transporters genetics, Animals, Calcinosis metabolism, Calcinosis pathology, Dietary Supplements, Gene Deletion, Kidney blood supply, Kidney pathology, Mice, Mice, Inbred C57BL, Multidrug Resistance-Associated Proteins, Myocardium pathology, Pseudoxanthoma Elasticum metabolism, Pseudoxanthoma Elasticum pathology, Blood Vessels pathology, Calcinosis diet therapy, Calcium metabolism, Magnesium metabolism, Pseudoxanthoma Elasticum diet therapy

Abstract

Pseudoxanthoma elasticum (PXE) is a heritable disorder characterized by ectopic calcification of connective tissue in skin, Bruch's membrane of the eye, and walls of blood vessels. PXE is caused by mutations in the ABCC6 gene, but the exact etiology is still unknown. While observations on patients suggest that high calcium intake worsens the clinical symptoms, the patient organization PXE International has published the dietary advice to increase calcium intake in combination with increased magnesium intake. To obtain more data on this controversial issue, we examined the effect of dietary calcium and magnesium in the Abcc6(-/-) mouse, a PXE mouse model which mimics the clinical features of PXE. Abcc6(-/-) mice were placed on specific diets for 3, 7, and 12 months. Disease severity was measured by quantifying calcification of blood vessels in the kidney. Raising the calcium content in the diet from 0.5% to 2% did not change disease severity. In contrast, simultaneous increase of both calcium (from 0.5% to 2.0%) and magnesium (from 0.05% to 0.2%) slowed down the calcification significantly. Our present findings that increase in dietary magnesium reduces vascular calcification in a mouse model for PXE should stimulate further studies to establish a dietary intervention for PXE.

Published

2010

108. A new strategy to identify and annotate human RPE-specific gene expression.

Author

Booij JC, ten Brink JB, Swagemakers SM, Verkerk AJ, Essing AH, van der Spek PJ, and Bergen AA

Subjects

Aged, Choroid cytology, Choroid metabolism, Humans, Middle Aged, Oligonucleotide Array Sequence Analysis, Organ Specificity, Photoreceptor Cells metabolism, Retinal Pigment Epithelium cytology, Signal Transduction, Gene Expression Profiling methods, Retinal Pigment Epithelium metabolism

Abstract

Background: To identify and functionally annotate cell type-specific gene expression in the human retinal pigment epithelium (RPE), a key tissue involved in age-related macular degeneration and retinitis pigmentosa., Methodology: RPE, photoreceptor and choroidal cells were isolated from selected freshly frozen healthy human donor eyes using laser microdissection. RNA isolation, amplification and hybridization to 44 k microarrays was carried out according to Agilent specifications. Bioinformatics was carried out using Rosetta Resolver, David and Ingenuity software., Principal Findings: Our previous 22 k analysis of the RPE transcriptome showed that the RPE has high levels of protein synthesis, strong energy demands, is exposed to high levels of oxidative stress and a variable degree of inflammation. We currently use a complementary new strategy aimed at the identification and functional annotation of RPE-specific expressed transcripts. This strategy takes advantage of the multilayered cellular structure of the retina and overcomes a number of limitations of previous studies. In triplicate, we compared the transcriptomes of RPE, photoreceptor and choroidal cells and we deduced RPE specific expression. We identified at least 114 entries with RPE-specific gene expression. Thirty-nine of these 114 genes also show high expression in the RPE, comparison with the literature showed that 85% of these 39 were previously identified to be expressed in the RPE. In the group of 114 RPE specific genes there was an overrepresentation of genes involved in (membrane) transport, vision and ophthalmic disease. More fundamentally, we found RPE-specific involvement in the RAR-activation, retinol metabolism and GABA receptor signaling pathways., Conclusions: In this study we provide a further specification and understanding of the RPE transcriptome by identifying and analyzing genes that are specifically expressed in the RPE.

Published

2010

109. Complement component C3 and risk of age-related macular degeneration.

Author

Despriet DD, van Duijn CM, Oostra BA, Uitterlinden AG, Hofman A, Wright AF, ten Brink JB, Bakker A, de Jong PT, Vingerling JR, Bergen AA, and Klaver CC

Subjects

Aged, Aged, 80 and over, Case-Control Studies, Chromatography, High Pressure Liquid, Complement Factor H genetics, Female, Follow-Up Studies, Genotype, Humans, Male, Middle Aged, Prospective Studies, Proteins genetics, Risk Factors, Smoking genetics, Complement C3 genetics, Macular Degeneration genetics, Polymorphism, Single Nucleotide

Abstract

Objective: To explore the association between polymorphisms in the complement component 3 (C3) gene and age-related macular degeneration (AMD), and to investigate the modifying effect of complement factor H (CFH) Y402H, LOC387715 A69S and smoking., Design: Pooled data from the prospective, population-based Rotterdam Study (enrolment between 1990 and 1993, and 3 follow-up examinations between September 1, 1993, and December 31, 2004) and an independent case-control study from the Netherlands., Participants: The Rotterdam Study comprised a total of 6418 persons aged >or=55 years who had gradable fundus photographs. The case-control study consisted of 357 unrelated AMD patients and 173 control individuals aged >or=55 years., Methods: The variants R102G and P314L of the C3 gene, CFH Y402H and LOC387715 A69S, were genotyped in all study participants. Information on cigarette smoking was obtained by interview at baseline., Main Outcome Measures: Early and late stages of prevalent and incident AMD, graded according to the international classification and grading system for AMD., Results: We found a population frequency of 0.217 for R102G and 0.211 for P314L in the Rotterdam Study. Both alleles significantly increased the risk of early AMD and all subtypes of late AMD, and this risk seemed to be independent of CFH Y402H, LOC387715 A69S, and smoking. Detailed analysis showed that the haplotype carrying both alleles had the highest frequency difference between cases and controls (P=0.006). We estimated a total population-attributable risk of 14.6%. A meta-analysis of all currently available data yielded a pooled odds ratio (OR) of 1.61 (95% confidence interval [CI], 1.46-1.78) for the R102G allele, and an OR of 1.50 (95% CI, 1.31-1.71) for the P314L allele., Conclusions: Our study showed a significant association between variants in the C3 gene and AMD and further highlights the crucial role of the complement pathway in the etiology of AMD.

Published

2009

110. Comparison of human retinal pigment epithelium gene expression in macula and periphery highlights potential topographic differences in Bruch's membrane.

Author

van Soest SS, de Wit GM, Essing AH, ten Brink JB, Kamphuis W, de Jong PT, and Bergen AA

Subjects

Adolescent, Adult, Computer Systems, Humans, Immunohistochemistry, Microarray Analysis, Pigment Epithelium of Eye cytology, Polymerase Chain Reaction, Tissue Distribution, Bruch Membrane metabolism, Gene Expression, Macula Lutea metabolism, Pigment Epithelium of Eye metabolism, Retina metabolism

Abstract

Purpose: To describe gene expression differences between healthy, young human retinal pigment epithelium (RPE) cells from the macular area and RPE cells from two locations in the retinal periphery., Methods: RPE cells from six human donor eyes, ages 17-36, without histopathological abnormalities, were dissected by laser and isolated from cryosections. Total RNA was isolated, amplified, and hybridized to a custom made oligonucleotide array containing 22,000 genes. Bioinformatic analysis was carried out using the computer programs Rosetta Resolver and the webtools EASE/David and GoStat. Confirmatory real time PCR (RT-PCR) and immunohistochemistry were performed according to standard protocols., Results: Microarray and statistical analysis yielded 438 genes that were differentially expressed between macular RPE, and at least one out of two peripheral RPE locations. Out of these genes, 33 that showed fold changes of four, or higher, were selected for RT-PCR confirmation. For 17 genes (51%), a significant differential expression was found, while 11 additional genes (33%) showed a similar trend. Immuno-staining of one target (WFDC1) confirmed its differential expression on the protein level. Functional annotation and overrepresentation analysis independently defined extracellular matrix (ECM) genes as a statistically overrepresented class of genes in our RPE dataset. In total, 33 ECM genes were differentially expressed between macular and peripheral RPE regions. A subset of proteins corresponding to these genes is known to be present in Bruch's membrane., Conclusions: Our data showed that consistent topographical gene expression differences in the human RPE constitute around 1-5% of the RPE transcriptome. These changes may underlie topographical differences in RPE physiology, and pathology and may reflect local differences in the molecular composition and turnover of Bruch's membrane.

Published

2007

111. Identification of mutations in the AIPL1, CRB1, GUCY2D, RPE65, and RPGRIP1 genes in patients with juvenile retinitis pigmentosa.

Author

Booij JC, Florijn RJ, ten Brink JB, Loves W, Meire F, van Schooneveld MJ, de Jong PT, and Bergen AA

Subjects

Adaptor Proteins, Signal Transducing, Adolescent, Adult, Aged, Child, Child, Preschool, Cloning, Molecular, Cytoskeletal Proteins, Female, Humans, Infant, Male, Middle Aged, Phenotype, Polymorphism, Genetic, cis-trans-Isomerases, Carrier Proteins genetics, DNA Mutational Analysis, Eye Proteins genetics, Guanylate Cyclase genetics, Membrane Proteins genetics, Mutation, Nerve Tissue Proteins genetics, Proteins genetics, Receptors, Cell Surface genetics, Retinitis Pigmentosa genetics

Abstract

Objective: To identify mutations in the AIPL1, CRB1, GUCY2D, RPE65, and RPGRIP1 genes in patients with juvenile retinitis pigmentosa., Methods: Mutation analysis was carried out in a group of 35 unrelated patients with juvenile autosomal recessive retinitis pigmentosa (ARRP), Leber's congenital amaurosis (LCA), or juvenile isolated retinitis pigmentosa (IRP), by denaturing high performance liquid chromatography followed by direct sequencing., Results: All three groups of patients showed typical combinations of eye signs associated with retinitis pigmentosa: pale optic discs, narrow arterioles, pigmentary changes, and nystagmus. Mutations were found in 34% of, Patients: in CRB1 (11%), GUCY2D (11%), RPE65 (6%), and RPGRIP1 (6%). Nine mutations are reported, including a new combination of two mutations in CRB1, and new mutations in GUCY2D and RPGRIP1. The new GUCY2D mutation (c.3283delC, p.Pro1069ArgfsX37) is the first pathological sequence change reported in the intracellular C-terminal domain of GUCY2D, and did not lead to the commonly associated LCA, but to a juvenile retinitis pigmentosa phenotype. The polymorphic nature of three previously described (pathological) sequence changes in AIPL1, CRB1, and RPGRIP1 was established. Seven new polymorphic changes, useful for further association studies, were found., Conclusions: New and previously described sequence changes were detected in retinitis pigmentosa in CRB1, GUCY2D, and RPGRIP1; and in LCA patients in CRB1, GUCY2D, and RPE65. These data, combined with previous reports, suggest that LCA and juvenile ARRP are closely related and belong to a continuous spectrum of juvenile retinitis pigmentosa.

Published

2005

112. A locum adventure.

Author

Vanden Brink RD and Vanden Brink JB

Subjects

Anecdotes as Topic, Humans, Life Style, Michigan, United States, Workforce, Contract Services, Internal Medicine, Personnel Staffing and Scheduling

Published

2003

113. Frequent mutation in the ABCC6 gene (R1141X) is associated with a strong increase in the prevalence of coronary artery disease.

Author

Trip MD, Smulders YM, Wegman JJ, Hu X, Boer JM, ten Brink JB, Zwinderman AH, Kastelein JJ, Feskens EJ, and Bergen AA

Subjects

Adult, Case-Control Studies, Coronary Artery Disease epidemiology, Female, Genetic Testing, Heterozygote, Humans, Male, Middle Aged, Netherlands epidemiology, Odds Ratio, Prevalence, Pseudoxanthoma Elasticum genetics, Risk Assessment, Risk Factors, Coronary Artery Disease genetics, Multidrug Resistance-Associated Proteins genetics, Mutation

Abstract

Background: Pseudoxanthoma elasticum (PXE) is an inborn disorder of the connective tissue with specific skin, ocular, and cardiovascular disease (CVD) manifestations. Recently, we and others have identified mutations in the gene coding for the ABCC6 transporter in PXE patients with ocular and skin involvement. In the Netherlands, as in the rest of Europe, a particular premature truncation variant ABCC6 (R1141X) was found in a large cohort of PXE patients. Given the association between CVD and PXE, we hypothesized that heterozygosity of this ABCC6 mutation could also confer an increased risk for CVD., Methods and Results: To assess the relationship between the frequent R1141X mutation in the ABCC6 gene and the prevalence of premature coronary artery disease (CAD), we conducted a case-control study of 441 patients under the age of 50 years who had definite CAD and 1057 age- and sex-matched population-based controls who were free of coronary disease. Strikingly, the prevalence of the R1141X mutation was 4.2 times higher among patients than among controls (3.2% versus 0.8%; P<0.001). Consequently, among subjects with the R1141X mutation, the odds ratio for a coronary event was 4.23 (95% CI: 1.76 to 10.20, P= 0.001)., Conclusion: The presence of the R1141X mutation in the ABCC6 gene is associated with a sharply increased risk of premature CAD.

Published

2002

114. Sorsby fundus dystrophy without a mutation in the TIMP-3 gene.

Author

Assink JJ, de Backer E, ten Brink JB, Kohno T, de Jong PT, Bergen AA, and Meire F

Subjects

Aged, Aged, 80 and over, Atrophy etiology, Chromosome Mapping, Chromosomes, Human, Pair 22 genetics, DNA analysis, Exons, Female, Genes, Dominant, Humans, Macular Degeneration complications, Male, Middle Aged, Pedigree, Polymerase Chain Reaction methods, Promoter Regions, Genetic, Retinal Drusen etiology, Retinal Neovascularization etiology, Macular Degeneration genetics, Mutation genetics, Tissue Inhibitor of Metalloproteinase-3 genetics

Abstract

Aims: To examine a large family with an autosomal dominant fundus dystrophy and to investigate whether or not mutations in TIMP-3 gene were involved., Methods: A large family of 58 individuals with an autosomal dominant fundus dystrophy was examined ophthalmologically. A DNA linkage analysis in the 22q12.1-q13.2 region was performed. The TIMP-3 gene was screened for mutations in all five exons., Results: In this large family 15 individuals were affected. All other individuals were found to be clinically unaffected. Pisciform flecks in the midperiphery and drusen-like deposits were the most typical ophthalmological finding in this family and were encountered from the fifth decade on. Chorioretinal atrophy and neovascularisation with disciform lesions characterised the disease from the sixth decade on. Linkage analysis using an affected only analysis, showed a maximum positive lod score of 3.94 at theta = 0.0 with marker D22S283. No mutations possibly causing Sorsby fundus dystrophy were found in either the exonic sequences, the promotor region, or the 3'UTR., Conclusion: The family in this pedigree has an autosomal dominant fundus dystrophy, which is most probably Sorsby fundus dystrophy. Although, in the linkage analysis, significant positive lod scores were found with the region 22q12.1-q13.2, no causative mutations could be identified in the TIMP-3 gene.

Published

2000

115. Mutations in ABCC6 cause pseudoxanthoma elasticum.

Author

Bergen AA, Plomp AS, Schuurman EJ, Terry S, Breuning M, Dauwerse H, Swart J, Kool M, van Soest S, Baas F, ten Brink JB, and de Jong PT

Subjects

ATP-Binding Cassette Transporters chemistry, Base Sequence, Chromosome Mapping, Chromosomes, Human, Pair 16 genetics, DNA Mutational Analysis, Exons genetics, Female, Gene Expression Profiling, Genes, Dominant genetics, Genes, Recessive genetics, Homozygote, Humans, Male, Molecular Sequence Data, Multidrug Resistance-Associated Proteins, Pedigree, Pseudoxanthoma Elasticum pathology, RNA, Messenger analysis, RNA, Messenger genetics, Sequence Deletion genetics, ATP-Binding Cassette Transporters genetics, Mutation genetics, Pseudoxanthoma Elasticum genetics

Abstract

Pseudoxanthoma elasticum (PXE) is a heritable disorder of the connective tissue. PXE patients frequently experience visual field loss and skin lesions, and occasionally cardiovascular complications. Histopathological findings reveal calcification of the elastic fibres and abnormalities of the collagen fibrils. Most PXE patients are sporadic, but autosomal recessive and dominant inheritance are also observed. We previously localized the PXE gene to chromosome 16p13.1 (refs 8,9) and constructed a physical map. Here we describe homozygosity mapping in five PXE families and the detection of deletions or mutations in ABCC6 (formerly MRP6) associated with all genetic forms of PXE in seven patients or families.

Published

2000

116. Mutations in a human homologue of Drosophila crumbs cause retinitis pigmentosa (RP12).

Author

den Hollander AI, ten Brink JB, de Kok YJ, van Soest S, van den Born LI, van Driel MA, van de Pol DJ, Payne AM, Bhattacharya SS, Kellner U, Hoyng CB, Westerveld A, Brunner HG, Bleeker-Wagemakers EM, Deutman AF, Heckenlively JR, Cremers FP, and Bergen AA

Subjects

Alu Elements genetics, Amino Acid Sequence, Amino Acid Substitution, Animals, Base Sequence, Blotting, Northern, Cell Line, Chromosome Mapping, Chromosomes, Human, Pair 1 genetics, DNA Mutational Analysis, DNA, Complementary chemistry, DNA, Complementary genetics, Drosophila melanogaster genetics, Family Health, Female, Gene Expression Regulation, Developmental, Homozygote, Humans, Male, Molecular Sequence Data, Mutagenesis, Insertional, Mutation, Pedigree, Point Mutation, Polymorphism, Single-Stranded Conformational, RNA, Messenger genetics, RNA, Messenger metabolism, Retinitis Pigmentosa pathology, Sequence Analysis, DNA, Tissue Distribution, Drosophila Proteins, Eye Proteins genetics, Membrane Proteins genetics, Retinitis Pigmentosa genetics

Abstract

Retinitis pigmentosa (RP) comprises a clinically and genetically heterogeneous group of diseases that afflicts approximately 1.5 million people worldwide. Affected individuals suffer from a progressive degeneration of the photoreceptors, eventually resulting in severe visual impairment. To isolate candidate genes for chorioretinal diseases, we cloned cDNAs specifically or preferentially expressed in the human retina and the retinal pigment epithelium (RPE) through a novel suppression subtractive hybridization (SSH) method. One of these cDNAs (RET3C11) mapped to chromosome 1q31-q32.1, a region harbouring a gene involved in a severe form of autosomal recessive RP characterized by a typical preservation of the para-arteriolar RPE (RP12; ref. 3). The full-length cDNA encodes an extracellular protein with 19 EGF-like domains, 3 laminin A G-like domains and a C-type lectin domain. This protein is homologous to the Drosophila melanogaster protein crumbs (CRB), and denoted CRB1 (crumbs homologue 1). In ten unrelated RP patients with preserved para-arteriolar RPE, we identified a homozygous AluY insertion disrupting the ORF, five homozygous missense mutations and four compound heterozygous mutations in CRB1. The similarity to CRB suggests a role for CRB1 in cell-cell interaction and possibly in the maintenance of cell polarity in the retina. The distinct RPE abnormalities observed in RP12 patients suggest that CRB1 mutations trigger a novel mechanism of photoreceptor degeneration.

Published

1999

117. A gene for X-linked optic atrophy is closely linked to the Xp11.4-Xp11.2 region of the X chromosome.

Author

Assink JJ, Tijmes NT, ten Brink JB, Oostra RJ, Riemslag FC, de Jong PT, and Bergen AA

Subjects

Adolescent, Adult, Child, Chromosome Mapping, Color Perception, Evoked Potentials, Visual, Female, Genetic Linkage, Genetic Markers, Humans, Likelihood Functions, Lod Score, Male, Netherlands, Ophthalmoscopy, Optic Atrophy physiopathology, Pedigree, Visual Acuity, Optic Atrophy genetics, X Chromosome

Abstract

The aim of this study was to identify the chromosomal location of the disease-causing gene in a family apparently segregating X-linked optic atrophy. A large family of 45 individuals with a four-generation history of X-linked optic atrophy was reexamined in a full ophthalmic as well as electrophysiological examination. A DNA linkage analysis of the family was undertaken in order to identify the chromosomal location of the disease-causing gene. Linkage analysis was performed with 26 markers that spanned the entire X chromosome. The affected males showed very early onset and slow progression of the disease. Ophthalmic study of the female carriers did not reveal any abnormalities. Close linkage without recombination was found at the MAOB locus (maximum LOD score [Zmax] 4.19). The Zmax - 1 support interval was found at a recombination fraction of .076 distal and .018 proximal to MAOB. Multipoint linkage analysis placed the optic atrophy-causing gene in the Xp11.4-p11.21 interval between markers DXS993 and DXS991, whereas any other localization along the X chromosome could be excluded.

Published

1997

118. Conclusive evidence for a distinct congenital stationary night blindness locus in Xp21.1.

Author

Bergen AA, ten Brink JB, Riemslag F, Schuurman EJ, Meire F, Tijmes N, and de Jong PT

Subjects

DNA analysis, Female, Genetic Linkage, Humans, Male, Night Blindness congenital, Pedigree, Night Blindness genetics, X Chromosome

Abstract

X linked congenital stationary night blindness (CSNBX) is a non-progressive retinal disorder characterised by decreased visual acuity and disturbance of night vision. CSNBX appears to be not only clinically but also genetically heterogeneous. On studying a single large family, we recently suggested the presence of a distinct locus for CSNBX in Xp21.1. Here, we describe the results of a linkage analysis in another large CSNBX family, which confirms this finding. Thus, the data presented here provide conclusive evidence for a distinct CSNBX locus in Xp21.1, closely linked to the X linked retinitis pigmentosa type 3 gene. The results combined with other published results indicate the order Xpter-DXS451-DMD-DYS1-(DXS1110, CSNBX1, XLRP3)-DXS7-(CSNBX2, XLRP2)-DXS14-Xcen.

Published

1996

119. Efficient DNA carrier detection in X linked juvenile retinoschisis.

Author

Bergen AA, ten Brink JB, and van Schooneveld MJ

Subjects

Base Sequence, Blotting, Southern, Female, Genetic Markers, Humans, Molecular Sequence Data, Pedigree, Polymerase Chain Reaction, Retinal Degeneration diagnosis, DNA genetics, Genetic Carrier Screening methods, Genetic Linkage, Retinal Degeneration genetics, X Chromosome

Abstract

Juvenile retinoschisis is a rare, X linked hereditary vitroretinal degeneration. Female carriers of the disease do not develop any ocular abnormalities. Therefore, carrier detection by DNA analysis is extremely useful for these females. In order to evaluate the usefulness of a new class of DNA markers for carrier detection in X linked juvenile retinoschisis, DNA carrier detection or carrier exclusion was carried out in four possible carriers for X linked juvenile retinoschisis. The use of these highly polymorphic CA repeats, closely linked to the RS gene, greatly enhances both the reliability and feasibility of carrier detection in X linked juvenile retinoschisis.

Published

1995

120. Localization of a novel X-linked congenital stationary night blindness locus: close linkage to the RP3 type retinitis pigmentosa gene region.

Author

Bergen AA, ten Brink JB, Riemslag F, Schuurman EJ, and Tijmes N

Subjects

Chromosome Mapping, Female, Genotype, Humans, Male, Pedigree, Phenotype, Retinitis Pigmentosa classification, Genetic Linkage, Night Blindness genetics, Retinitis Pigmentosa genetics, X Chromosome

Abstract

X-linked congenital stationary night blindness (CSNBX) is a non-progressive retinal disorder characterized by decreased visual acuity and loss of night vision. CSNBX is clinically heterogeneous with respect to the involvement of retinal rods and/or cones in the disease. In this study, we localize a new locus for CSNBX to Xp21.1, thus providing evidence that CSNBX is also genetically heterogeneous. A clear correlation between different genotypes and phenotypes cannot be found yet. The new CSNBX gene described here is closely linked to the X-linked retinitis pigmentosa type 3 gene region, which supports the hypothesis that there may be a functional relationship between congenital stationary night blindness and retinitis pigmentosa.

Published

1995

121. Refinement of the chromosomal position of the X linked juvenile retinoschisis gene.

Author

Bergen AA, ten Brink JB, Bleeker-Wagemakers LM, and van Schooneveld MJ

Subjects

Chromosome Mapping, Female, Genetic Linkage, Humans, Male, Pedigree, Recombination, Genetic, Retinal Degeneration genetics, Vitreous Body, X Chromosome

Abstract

Linkage analysis was carried out in seven X linked juvenile retinoschisis (XLRS) families using four DNA probes and four CA repeat polymorphisms from the Xp22 region. Close linkage was observed between the XLRS locus and DXS207 (theta max = 0.04, Zmax = 3.71), DXS999 (theta max = 0.00, Zmax = 4.59), DXS365 (theta max = 0.07, Zmax = 2.22), and DXS451 (theta max = 0.05, Zmax = 3.26). The analysis of recombination breakpoints and multipoint linkage analysis suggests the order Xpter-DXS16-(DXS43, DXS207)-RS-DXS365-(DXS451, DXS41)-Xcen, thereby refining the position of the XLRS locus to an interval of approximately 3-4 cM. These results improve the feasibility of diagnosis in XLRS considerably, since carriers of this disease cannot be identified clinically.

Published

1994