Your search keyword '"Swagemakers, S.M.A."' showing total 43 results

1. Pathogenic variants in the paired-related homeobox 1 gene (PRRX1) cause craniosynostosis with incomplete penetrance

Author

Tooze, R., Miller, K.A., Swagemakers, S.M.A., Calpena, E., McGowan, Simon J., Boute, Odile, Leeuw, N. de, Ockeloen, Charlotte W., Twigg, S.R.F., Wilkie, Andrew O. M., Tooze, R., Miller, K.A., Swagemakers, S.M.A., Calpena, E., McGowan, Simon J., Boute, Odile, Leeuw, N. de, Ockeloen, Charlotte W., Twigg, S.R.F., and Wilkie, Andrew O. M.

Abstract

Item does not contain fulltext

Published

2023

2. SMAD6 variants in craniosynostosis : genotype and phenotype evaluation

Author

Calpena, E., Cuellar, A., Bala, K., Swagemakers, S.M.A., Koelling, N., McGowan, S.J., Phipps, J.M., Balasubramanian, M., Cunningham, M.L., Douzgou, S., Lattanzi, W., Morton, J.E.V., Shears, D., Weber, A., Wilson, L.C., Lord, H., Lester, T., Johnson, D., Wall, S.A., Twigg, S.R.F., Mathijssen, I.M.J., Boyadjiev, S.A., and Wilkie, A.O.M.

Abstract

PURPOSE: Enrichment of heterozygous missense and truncating SMAD6 variants was previously reported in nonsyndromic sagittal and metopic synostosis, and interaction of SMAD6 variants with a common polymorphism near BMP2 (rs1884302) was proposed to contribute to inconsistent penetrance. We determined the occurrence of SMAD6 variants in all types of craniosynostosis, evaluated the impact of different missense variants on SMAD6 function, and tested independently whether rs1884302 genotype significantly modifies the phenotype. METHODS: We performed resequencing of SMAD6 in 795 unsolved patients with any type of craniosynostosis and genotyped rs1884302 in SMAD6-positive individuals and relatives. We examined the inhibitory activity and stability of SMAD6 missense variants. RESULTS: We found 18 (2.3%) different rare damaging SMAD6 variants, with the highest prevalence in metopic synostosis (5.8%) and an 18.3-fold enrichment of loss-of-function variants comparedwith gnomAD data (P

Published

2020

3. Transcriptional Profiling in Fibroblasts of Patients with Mutations inMCT8and Comparative Analysis with the Human Brain Transcriptome.

Author

Visser, W.E., primary, Swagemakers, S.M.A., additional, Ozgur, Z., additional, Schot, R., additional, Verheijen, F., additional, van IJcken, W.F.J., additional, van der Spek, P.J., additional, and Visser, T.J., additional

Published

2010

4. A novel nicastrin mutation in a three‐generation Dutch family with hidradenitis suppurativa: a search for functional significance

Author

Vossen, A.R.J.V., primary, van Straalen, K.R., additional, Swagemakers, S.M.A., additional, de Klein, J.E.M.M., additional, Stubbs, A.P., additional, Venter, D.J., additional, Zee, H.H., additional, Spek, P.J., additional, and Prens, E.P., additional

Published

2020

5. Histological, immunohistochemical and transcriptomic characterization of human tracheoesophageal fistulas

Author

Brosens, E. (Erwin), Felix, J.F. (Janine F.), Munck, A. (Anne) de, Jong, E.M. (Elisabeth) de, Lodder, E.M. (Elisabeth M.), Swagemakers, S.M.A. (Sigrid), Buscop-Van Kempen, M. (Marjon), Krijger, R.R. (Ronald) de, Wijnen, R.M.H. (René), IJcken, W.F.J. (Wilfred) van, Spek, P.J. (Peter) van der, Klein, A. (Annelies) de, Tibboel, D. (Dick), Rottier, R.J. (Robbert), Brosens, E. (Erwin), Felix, J.F. (Janine F.), Munck, A. (Anne) de, Jong, E.M. (Elisabeth) de, Lodder, E.M. (Elisabeth M.), Swagemakers, S.M.A. (Sigrid), Buscop-Van Kempen, M. (Marjon), Krijger, R.R. (Ronald) de, Wijnen, R.M.H. (René), IJcken, W.F.J. (Wilfred) van, Spek, P.J. (Peter) van der, Klein, A. (Annelies) de, Tibboel, D. (Dick), and Rottier, R.J. (Robbert)

Abstract

Esophageal atresia (EA) and tracheoesophageal fistula (TEF) are relatively frequently occurring foregut malformations. EA/TEF is thought to have a strong genetic component. Not much is known regarding the biological processes disturbed or which cell type is affected in patients. This hampers the detection of the responsible culprits (genetic or environmental) for the origin of these congenital anatomical malformations. Therefore, we examined gene expression patterns in the TEF and compared them to the patterns in esophageal, tracheal and lung control samples. We studied tissue organization and key proteins using immunohistochemistry. There were clear differences between TEF and control samples. Based on the number of differentially expressed genes as well as histological characteristics, TEFs were most similar to normal esophagus. The BMP-signaling pathway, actin cytoskeleton and extracellular matrix pathways are downregulated in TEF. Genes involved in smooth muscle contraction are overexpressed in TEF compared to esophagus as well as trachea. These enriched pathways indicate myofibroblast activated fibrosis. TEF represents a specific tissue type with large contributions of intestinal smooth muscle cells and neurons. All major cell types present in esophagus are present-albeit often structurally disorganized-in TEF, indicating that it

Published

2020

6. SMAD6 variants in craniosynostosis: genotype and phenotype evaluation

Author

Calpena, E. (Eduardo), Cuellar, A. (Araceli), Bala, K. (Krithi), Swagemakers, S.M.A. (Sigrid), Koelling, N. (Nils), McGowan, S.J. (Simon), Phipps, J.M. (Julie), Balasubramanian, M. (Meena), Cunningham, M.L. (Michael L.), Douzgou, S. (Sofia), Lattanzi, W. (Wanda), Morton, J. (Jenny), Shears, D.J. (Deborah), Weber, A. (Astrid), Wilson, L.C. (Louise), Lord, H. (Helen), Lester, K.J. (Kathryn), Johnson, D. (David), Wall, S.A. (Steven A.), Twigg, S.R.F. (Stephen), Mathijssen, I.M.J. (Irene M. J.), Boyadjiev, S.A. (Simeon A.), Wilkie, A.O.M. (Andrew), Calpena, E. (Eduardo), Cuellar, A. (Araceli), Bala, K. (Krithi), Swagemakers, S.M.A. (Sigrid), Koelling, N. (Nils), McGowan, S.J. (Simon), Phipps, J.M. (Julie), Balasubramanian, M. (Meena), Cunningham, M.L. (Michael L.), Douzgou, S. (Sofia), Lattanzi, W. (Wanda), Morton, J. (Jenny), Shears, D.J. (Deborah), Weber, A. (Astrid), Wilson, L.C. (Louise), Lord, H. (Helen), Lester, K.J. (Kathryn), Johnson, D. (David), Wall, S.A. (Steven A.), Twigg, S.R.F. (Stephen), Mathijssen, I.M.J. (Irene M. J.), Boyadjiev, S.A. (Simeon A.), and Wilkie, A.O.M. (Andrew)

Abstract

Purpose: Enrichment of heterozygous missense and truncating SMAD6 variants was previously reported in nonsyndromic sagittal and metopic synostosis, and interaction of SMAD6 variants with a common polymorphism near BMP2 (rs1884302) was proposed to contribute to inconsistent penetrance. We determined the occurrence of SMAD6 variants in all types of craniosynostosis, evaluated the impact of different missense variants on SMAD6 function, and tested independently whether rs1884302 genotype significantly

Published

2020

7. Correction: SMAD6 variants in craniosynostosis: genotype and phenotype evaluation (Genetics in Medicine, (2020), 10.1038/s41436-020-0817-2)

Author

Calpena, E. (Eduardo), Cuellar, A. (Araceli), Bala, K. (Krithi), Swagemakers, S.M.A. (Sigrid), Koelling, N. (Nils), McGowan, S.J. (Simon), Phipps, J.M. (Julie), Balasubramanian, M. (Meena), Cunningham, M.L. (Michael L.), Douzgou, S. (Sofia), Lattanzi, W. (Wanda), Morton, J. (Jenny), Shears, D.J. (Deborah), Weber, A. (Astrid), Wilson, L.C. (Louise), Lord, H. (Helen), Lester, K.J. (Kathryn), Johnson, D. (David), Wall, S.A. (Steven), Twigg, S.R.F. (Stephen), Mathijssen, I.M.J. (Irene M. J.), Boardman-Pretty, F. (Freya), Boyadjiev, S.A. (Simeon A.), Wilkie, A.O.M. (Andrew), Calpena, E. (Eduardo), Cuellar, A. (Araceli), Bala, K. (Krithi), Swagemakers, S.M.A. (Sigrid), Koelling, N. (Nils), McGowan, S.J. (Simon), Phipps, J.M. (Julie), Balasubramanian, M. (Meena), Cunningham, M.L. (Michael L.), Douzgou, S. (Sofia), Lattanzi, W. (Wanda), Morton, J. (Jenny), Shears, D.J. (Deborah), Weber, A. (Astrid), Wilson, L.C. (Louise), Lord, H. (Helen), Lester, K.J. (Kathryn), Johnson, D. (David), Wall, S.A. (Steven), Twigg, S.R.F. (Stephen), Mathijssen, I.M.J. (Irene M. J.), Boardman-Pretty, F. (Freya), Boyadjiev, S.A. (Simeon A.), and Wilkie, A.O.M. (Andrew)

Abstract

The version of the Article previously published did not acknowledge Freya Boardman-Pretty17,18 and the Genomics England Research Consortium in the author list. This has now been corrected in both the PDF and HTML versions of the Article.

Published

2020

8. Rapid Low-Cost Microarray-Based Genotyping for Genetic Screening in Primary Immunodeficiency

Author

Suratannon, N. (Narissara), van Wijck, R.T.A. (Rogier T. A.), Broer, L. (Linda), Xue, L. (Laixi), Meurs, J.B.J. (Joyce) van, Barendregt, B.H. (Barbara), Burg, M. (Mirjam) van der, Dik, W.A. (Willem), Chatchatee, P. (Pantipa), Langerak, A.W. (Anton), Swagemakers, S.M.A. (Sigrid), Goos, J.A.C. (Jacqueline), Mathijssen, I.M.J. (Irene M. J.), Dalm, V.A.S.H. (Virgil), Suphapeetiporn, K. (Kanya), Heezen, K. (Kim), Drabwell, J. (Jose), Uitterlinden, A.G. (André), Spek, P.J. (Peter) van der, van Hagen, P.M. (P. Martin), Suratannon, N. (Narissara), van Wijck, R.T.A. (Rogier T. A.), Broer, L. (Linda), Xue, L. (Laixi), Meurs, J.B.J. (Joyce) van, Barendregt, B.H. (Barbara), Burg, M. (Mirjam) van der, Dik, W.A. (Willem), Chatchatee, P. (Pantipa), Langerak, A.W. (Anton), Swagemakers, S.M.A. (Sigrid), Goos, J.A.C. (Jacqueline), Mathijssen, I.M.J. (Irene M. J.), Dalm, V.A.S.H. (Virgil), Suphapeetiporn, K. (Kanya), Heezen, K. (Kim), Drabwell, J. (Jose), Uitterlinden, A.G. (André), Spek, P.J. (Peter) van der, and van Hagen, P.M. (P. Martin)

Abstract

Background: Genetic tests for primary immunodeficiency disorders (PIDs) are expensive, time-consuming, and not easily accessible in developing countries. Therefore, we studied the feasibility of a customized single nucleotide variant (SNV) microarray that we developed to detect disease-causing variants and copy number variation (CNV) in patients with PIDs for only 40 Euros. Methods: Probes were custom-designed to genotype 9,415 variants of 277 PID-related genes, and were added to the genome-wide Illumina Global Screening Array (GSA). Data analysis of GSA was performed using Illumina GenomeStudio 2.0, Biodiscovery Nexus 10.0, and R-3.4.4 software. Validation of genotype calling was performed by comparing the GSA with whole-genome sequencing (WGS) data of 56 non-PID controls. DNA samples of 95 clinically diagnosed PID patients, of which 60 patients (63%) had a genetically established diagnosis (by Next-Generation Sequencing (NGS) PID panels or Sanger sequencing), we

Published

2020

9. Precursor lesions of vulvar squamous cell carcinoma – histology and biomarkers: A systematic review

Author

Dasgupta, S. (Shatavisha), Ewing, P.C. (Patricia), Swagemakers, S.M.A. (Sigrid), Spek, P.J. (Peter) van der, van Doorn, H.C. (Helena C.), Noordhoek Hegt, V. (Vincent), Koljenović, S. (Senada), Kemenade, F.J. (Folkert) van, Dasgupta, S. (Shatavisha), Ewing, P.C. (Patricia), Swagemakers, S.M.A. (Sigrid), Spek, P.J. (Peter) van der, van Doorn, H.C. (Helena C.), Noordhoek Hegt, V. (Vincent), Koljenović, S. (Senada), and Kemenade, F.J. (Folkert) van

Abstract

The precursor lesion of vulvar squamous cell carcinoma (VSCC), namely vulvar intraepithelial neoplasia (VIN), is classified as: human papillomavirus (HPV)-related high grade squamous intraepithelial lesion (HSIL), and HPV-independent differentiated VIN (dVIN). Traditionally, histology and immunohistochemistry (IHC) have been the basis of diagnosis and classification of VIN. HSIL shows conspicuous histological atypia, and positivity on p16-IHC, whereas dVIN shows less obvious histological atypia, and overexpression or null-pattern on p53-IHC. For both types of VIN, other diagnostic immunohistochemical markers have also been evaluated. Molecular characterization of VIN has been attempted in few recent studies, and novel genotypic subtypes of HPV-independent VSCC and VIN have been identified. This systematic review appraises the VSCC precursors identified so far, focusing on histology and biomarkers (immunohistochemical and molecular). To gain further insights into the carcinogenesis and to identify additional potential biomarkers, gene expression omnibus (GEO) datasets on VSCC were analyzed; the results are presented.

Published

2020

10. Functional Analysis of Genetic Variation in the SECIS Element of Thyroid Hormone Activating Type 2 Deiodinase

Author

Zevenbergen, C., Groeneweg, S., Swagemakers, S.M.A., Jong, A. de, Medici-van den Herik, E., Rispens, M., Klootwijk, W., Medici, M., Rijke, Y.B. de, Meima, M.E., Larsen, P.R., Chavatte, L., Venter, D., Peeters, R.P., Spek, P.J. van der, Visser, W.E., Zevenbergen, C., Groeneweg, S., Swagemakers, S.M.A., Jong, A. de, Medici-van den Herik, E., Rispens, M., Klootwijk, W., Medici, M., Rijke, Y.B. de, Meima, M.E., Larsen, P.R., Chavatte, L., Venter, D., Peeters, R.P., Spek, P.J. van der, and Visser, W.E.

Abstract

Contains fulltext : 215622.pdf (publisher's version ) (Closed access), CONTEXT: Thyroid hormone is important for normal brain development. The type 2 deiodinase (D2) controls thyroid hormone action in the brain by activating T4 to T3. The enzymatic activity of D2 depends on the incorporation of selenocysteine for which the selenocysteine-insertion sequence (SECIS) element located in the 3' untranslated region is indispensable. We hypothesized that mutations in the SECIS element could affect D2 function, resulting in a neurocognitive phenotype. OBJECTIVE: To identify mutations in the SECIS element of DIO2 in patients with intellectual disability and to test their functional consequences. DESIGN, SETTING, AND PATIENTS: The SECIS element of DIO2 was sequenced in 387 patients with unexplained intellectual disability using a predefined pattern of thyroid function tests. SECIS element read-through in wild-type or mutant D2 was quantified by a luciferase reporter system in transfected cells. Functional consequences were assessed by quantifying D2 activity in cell lysate or intact cell metabolism studies. RESULTS: Sequence analysis revealed 2 heterozygous mutations: c.5703C>T and c.5730A>T, which were also present in the unaffected family members. The functional evaluation showed that both mutations did not affect D2 enzyme activity in cell lysates or intact cells, although the 5730A>T mutation decreased SECIS element read-through by 75%. In the patient harboring the c.5730A>T variant, whole genome sequencing revealed a pathogenic deletion of the STXBP1 gene. CONCLUSIONS: We report on two families with mutations in the SECIS element of D2. Although functional analysis showed that nucleotide 5730 is important for normal SECIS element read-through, the two variants did not segregate with a distinct phenotype.

Published

2019

11. A de novo substitution in BCL11B leads to loss of interaction with transcriptional complexes and craniosynostosis

Author

Goos, J.A.C. (Jacqueline), Vogel, W.K. (Walter K.), Mlcochova, H. (Hana), Millard, C.J. (Christopher J.), Esfandiari, E. (Elahe), Selman, W.H. (Wisam H.), Calpena, E. (Eduardo), Koelling, N. (Nils), Carpenter, E.L. (Evan L.), Swagemakers, S.M.A. (Sigrid), Spek, P.J. (Peter) van der, Filtz, T.M. (Theresa M.), Schwabe, J.W.R. (John W.R.), Iwaniec, U.T. (Urszula T.), Mathijssen, I.M.J. (Irene M.J.), Leid, M. (Mark), Twigg, S.R.F. (Stephen), Goos, J.A.C. (Jacqueline), Vogel, W.K. (Walter K.), Mlcochova, H. (Hana), Millard, C.J. (Christopher J.), Esfandiari, E. (Elahe), Selman, W.H. (Wisam H.), Calpena, E. (Eduardo), Koelling, N. (Nils), Carpenter, E.L. (Evan L.), Swagemakers, S.M.A. (Sigrid), Spek, P.J. (Peter) van der, Filtz, T.M. (Theresa M.), Schwabe, J.W.R. (John W.R.), Iwaniec, U.T. (Urszula T.), Mathijssen, I.M.J. (Irene M.J.), Leid, M. (Mark), and Twigg, S.R.F. (Stephen)

Abstract

Craniosynostosis, the premature ossification of cranial sutures, is a developmental disorder of the skull vault, occurring in approximately 1 in 2250 births. The causes are heterogeneous, with a monogenic basis identified in ~25% of patients. Using whole-genome sequencing, we identified a novel, de novo variant in BCL11B, c.7C>A, encoding an R3S substitution (p.R3S), in a male patient with coronal suture synostosis. BCL11B is a transcription factor that interacts directly with the nucleosome remodelling and deacetylation complex (NuRD) and polycomb-related complex 2 (PRC2) through the invariant proteins RBBP4 and RBBP7. The p.R3S substitution occurs within a conserved amino-terminal motif (RRKQxxP) of BCL11B and reduces interaction with both transcriptional complexes. Equilibrium binding studies and molecular dynamics simulations show that the p.R3S substitution disrupts ionic coordination between BCL11B and the RBBP4-MTA1 complex, a subassembly of the NuRD complex, and increases the conformational flexibility of Arg-4, Lys-5 and Gln-6 of BCL11B. These alterations collectively reduce the affinity of BCL11B p.R3S for the RBBP4-MTA1 complex by nearly an order of magnitude. We generated a mouse model of the BCL11B p.R3S substitution using a CRISPR-Cas9-based approach, and we report herein that these mice exhibit craniosynostosis of the coronal suture, as well as other cranial sutures. This finding provides strong evidence that the BCL11B p.R3S substitution is causally associated with craniosynostosis and confirms an important role for BCL11B in the maintenance of cranial suture patency.

Published

2019

12. Endocrine disorders are prominent clinical features in patients with primary antibody deficiencies

Author

Coopmans, E.C. (Eva C.), Chunharojrith, P. (Paweena), Neggers, S.J.C.M.M. (Sebastian J. C. M. M.), van der Ent, M.W. (Marianne W.), Swagemakers, S.M.A. (Sigrid), Hollink, I.H.I.M. (Iris), Barendregt, B.H. (Barbara), Spek, P.J. (Peter) van der, Lely, A-J. (Aart-Jan) van der, Hagen, P.M. (Martin) van, Dalm, V.A.S.H. (Virgil), Coopmans, E.C. (Eva C.), Chunharojrith, P. (Paweena), Neggers, S.J.C.M.M. (Sebastian J. C. M. M.), van der Ent, M.W. (Marianne W.), Swagemakers, S.M.A. (Sigrid), Hollink, I.H.I.M. (Iris), Barendregt, B.H. (Barbara), Spek, P.J. (Peter) van der, Lely, A-J. (Aart-Jan) van der, Hagen, P.M. (Martin) van, and Dalm, V.A.S.H. (Virgil)

Abstract

Background: Primary antibody deficiencies (PADs) and anterior pituitary dysfunction are both rare conditions. However, recent studies have remarkably reported the occurrence of anterior pituitary dysfunction in PAD patients. Methods: In this cross-sectional, single-center study we evaluated the prevalence of endocrine disorders in adult PAD patients. Our study focused on common variable immunodeficiency (CVID), immunoglobulin G (IgG) subclass deficiency (IgGSD), and specific anti-polysaccharide antibody deficiency (SPAD). We assessed hormone levels, performed provocative tests and genetic testing in a subset of patients by direct sequencing of the nuclear factor kappa beta subunit 2 (NFKB2) gene and primary immunodeficiency (PID) gene panel testing by whole exome sequencing (WES). Results: Our results demonstrated that one out of 24 IgGSD/SPAD patients had secondary hypothyroidism and three out of 9 men with IgGSD/SPAD had secondary hypogonadism. Premature ovarian failure was observed in four out of 9 women with CVID and primary testicular failure in one out of 15 men with CVID. In two out of 26 CVID patients we found partial adrenal insufficiency (AI) and in one out of 18 patients with IgGSD/SPAD secondary AI was found. Moreover, in one out of 23 patients with CVID and in two out of 17 patients with IgGSD/SPAD severe growth hormone deficiency (GHD) was found, while one patient with IgGSD/SPAD showed mild GHD. Combined endocrine disorders were detected in two women with CVID (either partial secondary AI or autoimmune thyroiditis with primary hypogonadism) and in three men with IgGSD/SPAD (two with either mild GHD or secondary hypothyroidism combined with secondary hypogonadism, and one man with secondary AI and severe GHD). Genetic testing in a subset of patients did not reveal pathogenic variants in NFKB2 or other known PID-associated genes. Conclusion: This is the first study to describe a high prevalence of both anterior pituitary and end-organ endocrine dysfunct

Published

2019

13. De Novo Missense Substitutions in the Gene Encoding CDK8, a Regulator of the Mediator Complex, Cause a Syndromic Developmental Disorder

Author

Calpena, E., Hervieu, A., Kaserer, T., Swagemakers, S.M.A. (Sigrid), Goos, J.A.C. (Jacqueline), Popoola, O., Ortiz-Ruiz, M.J., Barbaro-Dieber, T., Bownass, L., Brilstra, EH, Brimble, E., Foulds, N., Grebe, T.A., Harder, A.V.E., Lees, M.M. (Melissa), Monaghan, K. G., Newbury-Ecob, R.A., Ong, K.-R. (Kai-Ren), Osio, D., Santos, F.J.R., Ruzhnikov, M.R.Z., Telegrafi, A., Binsbergen, E. (Ellen) van, Van Dooren, B. (Bas) van, Spek, P.J. (Peter) van der, Blagg, J., Twigg, S.R.F. (Stephen), Mathijssen, I.M.J. (Irene), Clarke, P.A. (Paul), Wilkie, A.O.M. (Andrew), Calpena, E., Hervieu, A., Kaserer, T., Swagemakers, S.M.A. (Sigrid), Goos, J.A.C. (Jacqueline), Popoola, O., Ortiz-Ruiz, M.J., Barbaro-Dieber, T., Bownass, L., Brilstra, EH, Brimble, E., Foulds, N., Grebe, T.A., Harder, A.V.E., Lees, M.M. (Melissa), Monaghan, K. G., Newbury-Ecob, R.A., Ong, K.-R. (Kai-Ren), Osio, D., Santos, F.J.R., Ruzhnikov, M.R.Z., Telegrafi, A., Binsbergen, E. (Ellen) van, Van Dooren, B. (Bas) van, Spek, P.J. (Peter) van der, Blagg, J., Twigg, S.R.F. (Stephen), Mathijssen, I.M.J. (Irene), Clarke, P.A. (Paul), and Wilkie, A.O.M. (Andrew)

Published

2019

14. De Novo and Inherited Loss-of-Function Variants in TLK2 : Clinical and Genotype-Phenotype Evaluation of a Distinct Neurodevelopmental Disorder

Author

Reijnders, M.R.F., Miller, K.A., Alvi, M., Goos, J.A.C., Lees, M.M., Burca, A. de, Henderson, A., Kraus, A., Mikat, B., Vries, B.B.A. de, Isidor, B., Kerr, B., Marcelis, C.L.M., Schluth-Bolard, C., Deshpande, C., Ruivenkamp, C.A.L., Wieczorek, D., Baralle, D., Blair, E.M., Engels, H., Ludecke, H.J., Eason, J., Santen, G.W.E., Clayton-Smith, J., Chandler, K., Tatton-Brown, K., Payne, K., Helbig, K., Radtke, K., Nugent, K.M., Cremer, K., Strom, T.M., Bird, L.M., Sinnema, M., Bitner-Glindzicz, M., Dooren, M.F. van, Alders, M., Koopmans, M., Brick, L., Kozenko, M., Harline, M.L., Klaassens, M., Steinraths, M., Cooper, N.S., Edery, P., Yap, P., Terhal, P.A., Spek, P.J. van der, Lakeman, P., Taylor, R.L., Littlejohn, R.O., Pfundt, R.P., Mercimek-Andrews, S., Stegmann, A.P.A., Kant, S.G., McLean, S., Joss, S., Swagemakers, S.M.A., Douzgou, S., Wall, S.A., Kury, S., Calpena, E., Koelling, N., McGowan, S.J., Twigg, S.R.F., Mathijssen, I.M.J., Nellaker, C., Brunner, H.G., Wilkie, A.O.M., Plastic and Reconstructive Surgery and Hand Surgery, Clinical Genetics, and Pathology

Subjects

Tousled-like, Facial Averaging, Haploinsufficiency, Intellectual Disability, Kinase, Adult, Male, Adolescent, kinase, viruses, Inheritance Patterns, Medizin, Translocation, Genetic, Cell Line, Young Adult, Loss of Function Mutation, Report, Humans, RNA, Messenger, Child, Genetic Association Studies, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Base Sequence, Facies, Infant, haploinsufficiency, Neurodevelopmental Disorders, intellectual disability, Child, Preschool, Female, Protein Kinases, facial averaging, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Human adenovirus (HAdV) E1B-55K is a multifunctional regulator of productive viral replication and oncogenic transformation in nonpermissive mammalian cells. These functions depend on E1B-55K's posttranslational modification with the SUMO protein and its binding to HAdV E4orf6. Both early viral proteins recruit specific host factors to form an E3 ubiquitin ligase complex that targets antiviral host substrates for proteasomal degradation. Recently, we reported that the PML-NB associated factor Daxx represses efficient HAdV productive infection and is proteasomally degraded via a SUMO-E1B-55K-dependent, E4orf6-independent pathway, the details of which remained to be established. RNF4, a cellular SUMO-targeted ubiquitin ligase (STUbL), induces ubiquitinylation of specific SUMOy lated proteins and plays an essential role during DNA repair. Here, we show that E1B-55K recruits RNF4 to the insoluble nuclear matrix fraction of the infected cell to support RNF4/Daxx association, promoting Daxx PTM and thus inhibiting this antiviral factor. Removing RNF4 from infected cells using RNA interference resulted in blocking the proper establishment of viral replication centers and significantly diminished viral gene expression. These results provide a model for how HAdV antagonize the antiviral host responses by exploiting the functional capacity of cellular STUbLs. Thus, RNF4 and its STUbL function represent a positive factor during lytic infection and a novel candidate for future therapeutic antiviral intervention strategies.IMPORTANCE Daxx is a PML-NB-associated transcription factor that was recently shown to repress efficient HAdV productive infection. To counteract this antiviral measurement during infection, Daxx is degraded via a novel pathway including viral E1B-55K and host proteasomes. This virus-mediated degradation is independent of the classical HAdV E3 ubiquitin ligase complex, which is essential during viral infection to target other host antiviral substrates. To maintain a productive viral life cycle, HAdV E1B-55K early viral protein inhibits the chromatin-remodeling factor Daxx in a SUMO-dependent manner. In addition, viral E1B-55K protein recruits the STUbL RNF4 and sequesters it into the insoluble fraction of the infected cell. E1B-55K promotes complex formation between RNF4-and E1B-55K-targeted Daxx protein, supporting Daxx posttranslational modification prior to functional inhibition. Hence, RNF4 represents a novel host factor that is beneficial for HAdV gene expression by supporting Daxx counteraction. In this regard, RNF4 and other STUbL proteins might represent novel targets for therapeutic intervention.

Published

2018

15. A point mutation in the pre-ZRS disrupts sonic hedgehog expression in the limb bud and results in triphalangeal thumb-polysyndactyly syndrome

Author

Potuijt, J.W.P., Baas, M., Sukenik-Halevy, R., Douben, H., Nguyen, P., Venter, D.J., Gallagher, R., Swagemakers, S.M.A., Hovius, S.E.R., Nieuwenhoven, C.A. van, Galjaard, R.H., Spek, P.J. van der, Ahituv, N., Klein, A., Potuijt, J.W.P., Baas, M., Sukenik-Halevy, R., Douben, H., Nguyen, P., Venter, D.J., Gallagher, R., Swagemakers, S.M.A., Hovius, S.E.R., Nieuwenhoven, C.A. van, Galjaard, R.H., Spek, P.J. van der, Ahituv, N., and Klein, A.

Abstract

Item does not contain fulltext, PURPOSE: The zone of polarizing activity regulatory sequence (ZRS) is an enhancer that regulates sonic hedgehog during embryonic limb development. Recently, mutations in a noncoding evolutionary conserved sequence 500 bp upstream of the ZRS, termed the pre-ZRS (pZRS), have been associated with polydactyly in dogs and humans. Here, we report the first case of triphalangeal thumb-polysyndactyly syndrome (TPT-PS) to be associated with mutations in this region and show via mouse enhancer assays how this mutation leads to ectopic expression throughout the developing limb bud. METHODS: We used linkage analysis, whole-exome sequencing, Sanger sequencing, fluorescence in situ hybridization, multiplex ligation-dependent probe amplification, single-nucleotide polymorphism array, and a mouse transgenic enhancer assay. RESULTS: Ten members of a TPT-PS family were included in this study. The mutation was linked to chromosome 7q36 (LOD score 3.0). No aberrations in the ZRS could be identified. A point mutation in the pZRS (chr7:156585476G>C; GRCh37/hg19) was detected in all affected family members. Functional characterization using a mouse transgenic enhancer essay showed extended ectopic expression dispersed throughout the entire limb bud (E11.5). CONCLUSION: Our work describes the first mutation in the pZRS to be associated with TPT-PS and provides functional evidence that this mutation leads to ectopic expression of this enhancer within the developing limb.

Published

2018

16. Type 1 interferon-inducible gene expression in QuantiFERON Gold TB-positive uveitis: A tool to stratify a high versus low risk of active tuberculosis?

Author

La Distia Nora, R. (Rina), Sitompul, R. (Ratna), Bakker, M. (Marleen), Versnel, M.A. (Marjan), Swagemakers, S.M.A. (Sigrid), van der Spek, P.J. (Peter J.), Susiyanti, M. (Made), Edwar, L. (Lukman), Sjamsoe, S. (Soedarman), Singh, G. (Gurmeet), Handayani, R.D. (Rr Diah), Rothová, A. (Aniki), Hagen, P.M. (Martin) van, Dik, W.A. (Willem), La Distia Nora, R. (Rina), Sitompul, R. (Ratna), Bakker, M. (Marleen), Versnel, M.A. (Marjan), Swagemakers, S.M.A. (Sigrid), van der Spek, P.J. (Peter J.), Susiyanti, M. (Made), Edwar, L. (Lukman), Sjamsoe, S. (Soedarman), Singh, G. (Gurmeet), Handayani, R.D. (Rr Diah), Rothová, A. (Aniki), Hagen, P.M. (Martin) van, and Dik, W.A. (Willem)

Abstract

QuantiFERON-Gold TB (QFT)-positive patients with undetermined cause of uveitis are problematic in terms of whether to diagnose and treat them for tuberculosis (TB). Here, we investigated whether peripheral blood expression of type 1 interferon (IFN)-inducible genes may be of use to stratify QFT-positive patients with uveitis into groups of high versus low risk of having active TB-associated uveitis. We recruited all new uveitis patients in Cipto Mangunkusumo Hospital, Jakarta, Indonesia for one year. We included 12 patients with uveitis and clinically diagnosed active pulmonary TB, 58 QFT-positive patients with uveitis of unknown cause, 10 newly diagnosed sputum-positive active pulmonary TB patients without uveitis and 23 QFT-negative healthy controls. Expression of 35 type 1 IFN-inducible genes was measured in peripheral blood cells from active pulmonary TB patients without uveitis and healthy controls. Differentially expressed genes were identified and used for further clustering analyses of the uveitis groups. A type-1 IFN gene signature score was calculated and the optimal cut-off value for this score to differentiate active pulmonary TB from healthy controls was determined and applied to QFT-positive patients with uveitis of unknown cause. Ten type 1 IFN-inducible genes were differentially expressed between active pulmonary TB and healthy controls. Expression of these 10 genes in QFT-positive patients with uveitis of unknown cause revealed three groups: 1); patients resembling active pulmonary TB, 2); patients resembling healthy controls, and 3); patients displaying an in-between gene expression pattern. A type 1 IFN gene signature score ≥5.61 displayed high sensitivity (100%) and specificity (91%) for identification of active TB. Application of this score to QFT-positive patients with uveitis of unknown cause yielded two groups with expected different likelihood (high vs. low) of having active-TB uveitis, and therefore may be useful in clinical management deci

Published

2018

17. Identification of causative variants in TXNL4A in Burn-McKeown syndrome and isolated choanal atresia

Author

Goos, J.A.C., Swagemakers, S.M.A., Twigg, S.R.F., Dooren, M.F. van, Hoogeboom, A.J.M., Beetz, C., Gunther, S., Magielsen, F.J., Ockeloen, C.W., Ramos-Arroyo, M.A., Pfundt, R.P., Yntema, H.G., Spek, P.J. van der, Stanier, P., Wieczorek, D., Wilkie, A.O.M., Ouweland, A.M.W. van den, Mathijssen, I.M.J., and Hurst, J.A.

Subjects

Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], otorhinolaryngologic diseases, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Contains fulltext : 182761.pdf (Publisher’s version ) (Open Access) Burn-McKeown syndrome (BMKS) is a rare syndrome characterized by choanal atresia, prominent ears, abnormalities of the outer third of the lower eyelid, structural cardiac abnormalities, conductive and sensorineural hearing loss, and cleft lip. Recently, causative compound heterozygous variants were identified in TXNL4A. We analyzed an individual with clinical features of BMKS and her parents by whole-genome sequencing and identified compound heterozygous variants in TXNL4A (a novel splice site variant (c.258-2A>G, (p.?)) and a 34 bp promoter deletion (hg19 chr18:g.77748581_77748614del (type 1Delta) in the proband). Subsequently, we tested a cohort of 19 individuals with (mild) features of BMKS and 17 individuals with isolated choanal atresia for causative variants in TXNL4A by dideoxy-sequence analysis. In one individual with BMKS unrelated to the first family, we identified the identical compound heterozygous variants. In an individual with isolated choanal atresia, we found homozygosity for the same type 1Delta promoter deletion, whilst in two cousins from a family with choanal atresia and other minor anomalies we found homozygosity for a different deletion within the promoter (hg19 chr18: g.77748604_77748637del (type 2Delta)). Hence, we identified causative recessive variants in TXNL4A in two individuals with BMKS as well as in three individuals (from two families) with isolated choanal atresia.

Published

2017

18. Diagnostic value of exome and whole genome sequencing in craniosynostosis

Author

Miller, K.A. (Kerry A.), Twigg, S.R.F. (Stephen), McGowan, S.J. (Simon), Phipps, J.M. (Julie), Fenwick, A.L. (Aimée), Johnson, D. (David), Wall, S.A. (Steven), Noons, P. (Peter), Rees, K.E.M. (Katie E.M.), Tidey, E.A. (Elizabeth A.), Craft, J. (Judith), Taylor, J. (John), Taylor, J.C. (Jenny C.), Goos, J.A.C. (Jacqueline), Swagemakers, S.M.A. (Sigrid), Mathijssen, I.M.J. (Irene), Spek, P.J. (Peter) van der, Lord, H. (Helen), Lester, K.J. (Kathryn), Abid, N. (Noina), Cilliers, D. (Deirdre), Hurst, J.A. (Jane), Morton, J. (Jenny), Sweeney, E. (Elizabeth), Weber, A. (Astrid), Wilson, L.C. (Louise), Wilkie, A.O.M. (Andrew), Miller, K.A. (Kerry A.), Twigg, S.R.F. (Stephen), McGowan, S.J. (Simon), Phipps, J.M. (Julie), Fenwick, A.L. (Aimée), Johnson, D. (David), Wall, S.A. (Steven), Noons, P. (Peter), Rees, K.E.M. (Katie E.M.), Tidey, E.A. (Elizabeth A.), Craft, J. (Judith), Taylor, J. (John), Taylor, J.C. (Jenny C.), Goos, J.A.C. (Jacqueline), Swagemakers, S.M.A. (Sigrid), Mathijssen, I.M.J. (Irene), Spek, P.J. (Peter) van der, Lord, H. (Helen), Lester, K.J. (Kathryn), Abid, N. (Noina), Cilliers, D. (Deirdre), Hurst, J.A. (Jane), Morton, J. (Jenny), Sweeney, E. (Elizabeth), Weber, A. (Astrid), Wilson, L.C. (Louise), and Wilkie, A.O.M. (Andrew)

Abstract

Background Craniosynostosis, the premature fusion of one or more cranial sutures, occurs in ~1 in 2250 births, either in isolation or as part of a syndrome. Mutations in at least 57 genes have been associated with craniosynostosis, but only a minority of these are included in routine laboratory genetic testing. Methods We used exome or whole genome sequencing to seek a genetic cause in a cohort of 40 subjects with craniosynostosis, selected by clinical or molecular geneticists as being high-priority cases, and in whom prior clinically driven genetic testing had been negative. Results We identified likely associated mutations in 15 patients (37.5%), involving 14 different genes. All genes were mutated in single families, except for IL11RA (two families). We classified the other positive diagnoses as follows: commonly mutated craniosynostosis genes with atypical presentation (EFNB1, TWIST1); other core craniosynostosis genes (CDC45, MSX2, ZIC1); genes for which mutations are only rarely associated with craniosynostosis (FBN1, HUWE1, KRAS, STAT3); and known disease genes for which a causal relationship with craniosynostosis is currently unknown (AHDC1, NTRK2). In two further families, likely novel disease genes are currently undergoing functional validation. In 5 of the 15 positive cases, the (previously unanticipated) molecular diagnosis had immediate, actionable consequences for either genetic or medical management (mutations in EFNB1, FBN1, KRAS, NTRK2, STAT3). Conclusions This substantial genetic heterogeneity, and the multiple actionable mutations identified, emphasises the benefits of exome/whole genome sequencing to identify causal mutations in craniosynostosis cases for which routine clinical testing has yielded negative results.

Published

2017

19. Identification of Intragenic Exon Deletions and Duplication of TCF12 by Whole Genome or Targeted Sequencing as a Cause of TCF12-Related Craniosynostosis

Author

Goos, J.A.C. (Jacqueline), Fenwick, A.L. (Aimée), Swagemakers, S.M.A. (Sigrid), McGowan, S.J. (Simon), Knight, S.J.L. (Samantha J.L.), Twigg, S.R.F. (Stephen), Hoogeboom, A.J.M. (Jeannette), van Dooren, M.F. (Marieke F.), Magielsen, F.J. (Frank J.), Wall, S.A. (Steven A.), Mathijssen, I.M.J. (Irene), Wilkie, A.O.M. (Andrew), Spek, P.J. (Peter) van der, Ouweland, A.M.W. (Ans) van den, Goos, J.A.C. (Jacqueline), Fenwick, A.L. (Aimée), Swagemakers, S.M.A. (Sigrid), McGowan, S.J. (Simon), Knight, S.J.L. (Samantha J.L.), Twigg, S.R.F. (Stephen), Hoogeboom, A.J.M. (Jeannette), van Dooren, M.F. (Marieke F.), Magielsen, F.J. (Frank J.), Wall, S.A. (Steven A.), Mathijssen, I.M.J. (Irene), Wilkie, A.O.M. (Andrew), Spek, P.J. (Peter) van der, and Ouweland, A.M.W. (Ans) van den

Published

2016

20. Gain-of-Function Mutations in ZIC1 Are Associated with Coronal Craniosynostosis and Learning Disability

Author

Twigg, S.R.F. (Stephen), Forecki, J. (Jennifer), Goos, J.A.C. (Jacqueline), Richardson, I.C.A. (Ivy C.A.), Hoogeboom, A.J.M. (Jeannette), Ouweland, A.M.W. (Ans) van den, Swagemakers, S.M.A. (Sigrid), Leguin, M. (Maarten), Van antwerp, D. (Daniel), McGowan, S.J. (Simon J.), Westbury, I. (Isabelle), Miller, K.A. (Kerry A.), Wall, S.A. (Steven), Spek, P.J. (Peter) van der, Mathijssen, I.M.J. (Irene), Pauws, E. (Erwin), Merzdorf, C.S. (Christa S.), Wilkie, A.O.M. (Andrew), Twigg, S.R.F. (Stephen), Forecki, J. (Jennifer), Goos, J.A.C. (Jacqueline), Richardson, I.C.A. (Ivy C.A.), Hoogeboom, A.J.M. (Jeannette), Ouweland, A.M.W. (Ans) van den, Swagemakers, S.M.A. (Sigrid), Leguin, M. (Maarten), Van antwerp, D. (Daniel), McGowan, S.J. (Simon J.), Westbury, I. (Isabelle), Miller, K.A. (Kerry A.), Wall, S.A. (Steven), Spek, P.J. (Peter) van der, Mathijssen, I.M.J. (Irene), Pauws, E. (Erwin), Merzdorf, C.S. (Christa S.), and Wilkie, A.O.M. (Andrew)

Abstract

Human ZIC1 (zinc finger protein of cerebellum 1), one of five homologs of the Drosophila pair-rule gene odd-paired, encodes a transcription factor previously implicated in vertebrate brain development. Heterozygous deletions of ZIC1 and its nearby paralog ZIC4 on chromosome 3q25.1 are associated with Dandy-Walker malformation of the cerebellum, and loss of the orthologous Zic1 gene in the mouse causes cerebellar hypoplasia and vertebral defects. We describe individuals from five families with heterozygous mutations located in the final (third) exon of ZIC1 (encoding four nonsense and one missense change) who have a distinct phenotype in which severe craniosynostosis, specifically involving the coronal sutures, and variable learning disability are the most characteristic features. The location of the nonsense mutations predicts escape of mutant ZIC1 transcripts from nonsense-mediated decay, which was confirmed in a cell line from an affected individual. Both nonsense and missense mutations are associated with altered and/or enhanced expression of a target gene, engrailed-2, in a Xenopus embryo assay. Analysis of mouse embryos revealed a localized domain of Zic1 expression at embryonic days 11.5-12.5 in a region overlapping the supraorbital regulatory center, which patterns the coronal suture. We conclude that the human mutations uncover a previously unsuspected role for Zic1 in early cranial suture development, potentially by regulating engrailed 1, which was previously shown to be critical for positioning of the murine coronal suture. The diagnosis of a ZIC1 mutation has significant implications for prognosis and we recommend genetic testing when common causes of coronal synostosis have been excluded.

Published

2015

21. ZC4H2, an XLID gene, is required for the generation of a specific subset of CNS interneurons

Author

May, M. (Melanie), Hwang, K.-S. (Kyu-Seok), Miles, J. (Judith), Williams, C. (Charlie), Niranjan, T. (Tejasvi), Kahler, S.G. (Stephen G.), Chiurazzi, P. (Pietro), Steindl, K. (Katharina), Spek, P.J. (Peter) van der, Swagemakers, S.M.A. (Sigrid), Mueller, J. (Jennifer), Stefl, S. (Shannon), Alexov, E. (Emil), Ryu, J.-I. (Jeong-Im), Choi, J.-H. (Jung-Hwa), Kim, H.-T. (Hyun-Taek), Tarpey, P.S. (Patrick), Neri, G. (Giovanni), Holloway, L. (Lynda), Skinner, C. (Cindy), Stevenson, R.E. (Roger E.), Dorsky, R.I. (Richard I.), Wang, T. (Tao), Schwartz, C.E., Kim, C.-H. (Cheol-Hee), May, M. (Melanie), Hwang, K.-S. (Kyu-Seok), Miles, J. (Judith), Williams, C. (Charlie), Niranjan, T. (Tejasvi), Kahler, S.G. (Stephen G.), Chiurazzi, P. (Pietro), Steindl, K. (Katharina), Spek, P.J. (Peter) van der, Swagemakers, S.M.A. (Sigrid), Mueller, J. (Jennifer), Stefl, S. (Shannon), Alexov, E. (Emil), Ryu, J.-I. (Jeong-Im), Choi, J.-H. (Jung-Hwa), Kim, H.-T. (Hyun-Taek), Tarpey, P.S. (Patrick), Neri, G. (Giovanni), Holloway, L. (Lynda), Skinner, C. (Cindy), Stevenson, R.E. (Roger E.), Dorsky, R.I. (Richard I.), Wang, T. (Tao), Schwartz, C.E., and Kim, C.-H. (Cheol-Hee)

Abstract

Miles-Carpenter syndrome (MCS) was described in 1991 as an XLID syndrome with fingertip arches and contractures and mapped to proximal Xq. Patients had microcephaly, short stature, mild spasticity, thoracic scoliosis, hyperextendable MCP joints, rocker-bottom feet, hyperextended elbows and knees. A mutation, p.L66H, in ZC4H2, was identified in a XLID resequencing project. Additional screening of linked families and next generation sequencing of XLID families identified three ZC4H2 mutations: p.R18K, p.R213W and p.V75in15aa. The families shared some relevant clinical features. In silico modeling of the mutant proteins indicated all alterations would destabilize the protein. Knockout mutations in zc4h2 were created in zebrafish and homozygous mutant larvae exhibited abnormal swimming, increased twitching, defective eye movement and pectoral fin contractures. Because several of the behavioral defects were consistent with hyperactivity, we examined the underlying neuronal defects and found that sensory neurons and motoneurons appeared normal. However, we observed a striking reduction in GABAergic interneurons. Analysis of cell-type-specificmarkers showed a specific loss of V2 interneurons in the brain and spinal cord, likely arising from mis-specification of neural progenitors. Injected human wt ZC4H2 rescued the mutant phenotype. Mutant zebrafish injectedwith human p.L66H or p.R213W mRNA failed to be rescued, while the p.R18K mRNA was able to rescue the interneuron defect. Our findings clearly support ZC4H2 as a novel XLID gene with a required function in interneuron development. Loss of function of ZC4H2 thus likely results in altered connectivity ofmany brain and spinal circuits.

Published

2015

22. Extracellular matrix defects in aneurysmal Fibulin-4 mice predispose to lung emphysema

Author

Ramnath, N.W.M. (Natasja ), Luijtgaarden, K.M. (Koen) van de, Pluijm, I. (Ingrid) van der, Nimwegen, M. (Menno) van, Heijningen, P.M. (Paula ) van, Swagemakers, S.M.A. (Sigrid), Thiel, B.S. (Bibi) van, Ridwan, R.Y. (Ruziedi Y.), Vliet, N. (Nicole) van, Vermeij, M. (Marcel), Hawinkels, L.J.A.C. (Lukas ), Munck, A. (Anne) de, Dzyubachyk, O.M. (Oleh), Meijering, H.W. (Erik), Spek, P.J. (Peter) van der, Rottier, R.J. (Robbert), Yanagisawa, J., Hendriks, R.W. (Rudi), Kanaar, R. (Roland), Rouwet, E.V. (Ellen), Kleinjan, A. (Alex), Essers, J. (Jeroen), Ramnath, N.W.M. (Natasja ), Luijtgaarden, K.M. (Koen) van de, Pluijm, I. (Ingrid) van der, Nimwegen, M. (Menno) van, Heijningen, P.M. (Paula ) van, Swagemakers, S.M.A. (Sigrid), Thiel, B.S. (Bibi) van, Ridwan, R.Y. (Ruziedi Y.), Vliet, N. (Nicole) van, Vermeij, M. (Marcel), Hawinkels, L.J.A.C. (Lukas ), Munck, A. (Anne) de, Dzyubachyk, O.M. (Oleh), Meijering, H.W. (Erik), Spek, P.J. (Peter) van der, Rottier, R.J. (Robbert), Yanagisawa, J., Hendriks, R.W. (Rudi), Kanaar, R. (Roland), Rouwet, E.V. (Ellen), Kleinjan, A. (Alex), and Essers, J. (Jeroen)

Abstract

Background: In this study we set out to investigate the clinically observed relationship between chronic obstructive pulmonary disease (COPD) and aortic aneurysms. We tested the hypothesis that an i

Published

2014

23. Pollitt syndrome patients carry mutation in TTDN1

Author

Swagemakers, S.M.A. (Sigrid), Jaspers, N.G.J. (Nicolaas), Raams, A. (Anja), Heijsman, D. (Daphne), Vermeulen, W. (Wim), Troelstra, C. (Christine), Kremer, A.E. (Andreas), Lincoln, S.E. (Stephen E.), Tearle, R. (Rick), Hoeijmakers, J.H.J. (Jan), Spek, P.J. (Peter) van der, Swagemakers, S.M.A. (Sigrid), Jaspers, N.G.J. (Nicolaas), Raams, A. (Anja), Heijsman, D. (Daphne), Vermeulen, W. (Wim), Troelstra, C. (Christine), Kremer, A.E. (Andreas), Lincoln, S.E. (Stephen E.), Tearle, R. (Rick), Hoeijmakers, J.H.J. (Jan), and Spek, P.J. (Peter) van der

Abstract

Complete human genome sequencing was used to identify the causative mutation in a family with Pollitt syndrome (MIM #. 275550), comprising two non-consanguineous parents and their two affected children. The patient's symptoms were reminiscent of the non-photosensitive form of recessively inherited trichothiodystrophy (TTD). A mutation in the TTDN1/. C7orf11 gene, a gene that is known to be involved in non-photosensitive TTD, had been excluded by others by Sanger sequencing. Unexpectedly, we did find a homozygous single-base pair deletion in the coding region of this gene, a mutation that is known to cause non-photosensitive TTD. The deleterious variant causing a frame shift at amino acid 93 (C326delA) followed the right mode of inheritance in the family and was independently validated using conventional DNA sequencing. We expect this novel DNA sequencing technology to help redefine phenotypic and genomic variation in patients with (mono) genetic disorders in an unprecedented manner.

Published

2014

24. Microarray and morphological analysis of early postnatal CRB2 mutant retinas on a pure C57BL/6J genetic background

Author

Alves, C.H. (Celso Henrique), Bossers, K. (Koen), Vos, R.M. (Rogier), Essing, A.H.W. (Anke), Swagemakers, S.M.A. (Sigrid), Spek, P.J. (Peter) van der, Verhaagen, J. (Joost), Wijnholds, J. (Jan), Alves, C.H. (Celso Henrique), Bossers, K. (Koen), Vos, R.M. (Rogier), Essing, A.H.W. (Anke), Swagemakers, S.M.A. (Sigrid), Spek, P.J. (Peter) van der, Verhaagen, J. (Joost), and Wijnholds, J. (Jan)

Abstract

In humans, the Crumbs homologue-1 (CRB1) gene is mutated in progressive types of autosomal recessive retinitis pigmentosa and Leber congenital amaurosis. The

Published

2013

25. Gene expression analysis of peripheral cells for subclassification of pediatric inflammatory bowel disease in remission

Author

Lierop, P.P.E. (Pieter) van, Swagemakers, S.M.A. (Sigrid), Bie, C.I. (Charlotte) de, Middendorp, S., Baarlen, P. (Peter) van, Samsom, J.N. (Janneke), IJcken, W.F.J. (Wilfred) van, Escher, J.C. (Johanna), Spek, P.J. (Peter) van der, Nieuwenhuis, E.E.S. (Edward), Lierop, P.P.E. (Pieter) van, Swagemakers, S.M.A. (Sigrid), Bie, C.I. (Charlotte) de, Middendorp, S., Baarlen, P. (Peter) van, Samsom, J.N. (Janneke), IJcken, W.F.J. (Wilfred) van, Escher, J.C. (Johanna), Spek, P.J. (Peter) van der, and Nieuwenhuis, E.E.S. (Edward)

Abstract

Objective: In current clinical practice, optimal treatment of inflammatory bowel disease (IBD) aims at the induction and maintenance of clinical remission. Clinical remission is apparent when laboratory markers of inflammation are normal and clinical symptoms are absent. However, sub-clinical inflammation can still be present. A detailed analysis of the immune status during this inactive state of disease may provide a useful tool to categorize patients with clinical remission into subsets with variable states of immune activation. Design: By using Affymetrix GeneChips, we analysed RNA gene expression profiles of peripheral blood leukocytes from pediatric IBD patients in clinical remission and controls. We performed (un)supervised clustering analysis of IBD-associated genes and applied Ingenuity® pathway software to identify specific molecular profiles between patients. Results: Pediatric IBD patients with disease in clinical remission display heterogeneously distributed gene expression profiles that are significantly distinct from controls. We identified three clusters of IBD patients, each displaying specific expression profiles of IBD-associated genes. Conclusion: The expression of immune- and IBD-associated genes in peripheral blood leukocytes from pediatric IBD patients in clinical remission was different from healthy controls, indicating that sub-clinical immune mechanisms are still active during remission. As such, RNA profiling of peripheral blood may allow for non-invasive patient subclassification and new perspectives in treatment regimes of IBD patients in the future.

Published

2013

26. NPHP4 variants are associated with pleiotropic heart malformations

Author

French, V.M. (Vanessa), Laar, I.M.B.H. (Ingrid) van de, Wessels, M.W. (Marja), Rohe, C.F., Roos-Hesselink, J.W. (Jolien), Wang, G. (Guangliang), Frohn-Mulder, I.M.E. (Ingrid), Severijnen, E.A.W.F.M. (Lies-Anne), Graaf, B.M. (Bianca) de, Schot, R. (Rachel), Breedveld, G.J. (Guido), Mientjes, E.J. (Edwin), Tienhoven, M. (Marianne) van, Jadot, E. (Elodie), Jiang, Z. (Zhengxin), Verkerk, A., Swagemakers, S.M.A. (Sigrid), Venselaar, H. (Hanka), Rahimi, Z. (Zohreh), Najmabadi, H. (Hossein), Meijers-Heijboer, E.J. (Hanne), Graaff, E. (Esther) de, Helbing, W.A. (Willem), Willemsen, R. (Rob), Devriendt, K. (Koenraad), Belmont, J.W. (John), Oostra, B.A. (Ben), Amack, J.D. (Jeffrey), Bertoli Avella, A.M. (Aida), French, V.M. (Vanessa), Laar, I.M.B.H. (Ingrid) van de, Wessels, M.W. (Marja), Rohe, C.F., Roos-Hesselink, J.W. (Jolien), Wang, G. (Guangliang), Frohn-Mulder, I.M.E. (Ingrid), Severijnen, E.A.W.F.M. (Lies-Anne), Graaf, B.M. (Bianca) de, Schot, R. (Rachel), Breedveld, G.J. (Guido), Mientjes, E.J. (Edwin), Tienhoven, M. (Marianne) van, Jadot, E. (Elodie), Jiang, Z. (Zhengxin), Verkerk, A., Swagemakers, S.M.A. (Sigrid), Venselaar, H. (Hanka), Rahimi, Z. (Zohreh), Najmabadi, H. (Hossein), Meijers-Heijboer, E.J. (Hanne), Graaff, E. (Esther) de, Helbing, W.A. (Willem), Willemsen, R. (Rob), Devriendt, K. (Koenraad), Belmont, J.W. (John), Oostra, B.A. (Ben), Amack, J.D. (Jeffrey), and Bertoli Avella, A.M. (Aida)

Abstract

Rationale: Congenital heart malformations are a major cause of morbidity and mortality, especially in young children. Failure to establish normal left-right (L-R) asymmetry often results in cardiovascular malformations and other laterality defects of visceral organs. Objective: To identify genetic mutations causing cardiac laterality defects. Methods and Results: We performed a genome-wide linkage analysis in patients with cardiac laterality defects from a consanguineous family. The patients had combinations of defects that included dextrocardia, transposition of great arteries, double-outlet right ventricle, atrioventricular septal defects, and caval vein abnormalities. Sequencing of positional candidate genes identified mutations in NPHP4. We performed mutation analysis of NPHP4 in 146 unrelated patients with similar cardiac laterality defects. Forty-one percent of these patients also had laterality defects of the abdominal organs. We identified 8 additional missense variants that were absent or very rare in control subjects. To study the role of nphp4 in establishing L-R asymmetry, we used antisense morpholinos to knockdown nphp4 expression in zebrafish. Depletion of nphp4 disrupted L-R patterning as well as cardiac and gut laterality. Cardiac laterality defects were partially rescued by human NPHP4 mRNA, whereas mutant NPHP4 containing genetic variants found in patients failed to rescue. We show that nphp4 is involved in the formation of motile cilia in Kupffer's vesicle, which generate asymmetrical fluid flow necessary for normal L-R asymmetry. Conclusions: NPHP4 mutations are associated with cardiac laterality defects and heterotaxy. In zebrafish, nphp4 is essential for the development and function of Kupffer's vesicle cilia and is required for global L-R patterning.

Published

2012

27. SOX2 redirects the developmental fate of the intestinal epithelium toward a premature gastric phenotype

Author

Raghoebir, L. (Lalini), Bakker, E.R.M. (Elvira), Mills, J.C. (Jason), Swagemakers, S.M.A. (Sigrid), Kempen, M. (Marjon) van, Boerema-de Munck, A. (Anne), Driegen, M.J.F. (Siska), Meijer, D.N. (Dies), Grosveld, F.G. (Frank), Tibboel, D. (Dick), Smits, M.J.M. (Ron), Rottier, R.J. (Robbert), Raghoebir, L. (Lalini), Bakker, E.R.M. (Elvira), Mills, J.C. (Jason), Swagemakers, S.M.A. (Sigrid), Kempen, M. (Marjon) van, Boerema-de Munck, A. (Anne), Driegen, M.J.F. (Siska), Meijer, D.N. (Dies), Grosveld, F.G. (Frank), Tibboel, D. (Dick), Smits, M.J.M. (Ron), and Rottier, R.J. (Robbert)

Abstract

__Abstract__ Various factors play an essential role in patterning the digestive tract. During development, Sox2 and Cdx2 are exclusively expressed in the anterior and the posterior parts of the primitive gut, respectively. However, it is unclear whether these transcription factors influence each other in determining specification of the naïve gut endoderm. We therefore investigated whether Sox2 redirects the fate of the prospective intestinal part of the primitive gut. Ectopic expression of Sox2 in the posterior region of the primitive gut caused anteriorization of the gut toward a gastric-like phenotype. Sox2 activated the foregut transcriptional program, in spite of sustained co-expression of endogenous Cdx2. However, binding of Cdx2 to its genomic targets and thus its transcriptional activity was strongly reduced. Recent findings indicate that endodermal Cdx2 is required to initiate the intestinal program and to suppress anterior cell fate. Our findings suggest that reduced Cdx2 expression by itself is not sufficient to cause anteriorization, but that Sox2 expression is also required. Moreover, it indicates that the balance between Sox2 and Cdx2 function is essential for proper specification of the primitive gut and that Sox2 may overrule the initial patterning of the primitive gut, emphasizing the plasticity of the primitive gut.

Published

2012

28. Marked reduction of AKT1 expression and deregulation of AKT1-associated pathways in peripheral blood mononuclear cells of schizophrenia patients

Author

Beveren, N.J.M. (Nico) van, Buitendijk, G.H.S. (Gabrielle), Swagemakers, S.M.A. (Sigrid), Krab, L.C. (Lianne), Röder, C.H. (Christian), Haan, L. (Lieuwe) de, Spek, P.J. (Peter) van der, Elgersma, Y. (Ype), Beveren, N.J.M. (Nico) van, Buitendijk, G.H.S. (Gabrielle), Swagemakers, S.M.A. (Sigrid), Krab, L.C. (Lianne), Röder, C.H. (Christian), Haan, L. (Lieuwe) de, Spek, P.J. (Peter) van der, and Elgersma, Y. (Ype)

Abstract

Background: Recent studies have suggested that deregulated AKT1 signaling is associated with schizophrenia. We hypothesized that if this is indeed the case, we should observe both decreased AKT1 expression as well as deregulation of AKT1 regulated pathways in Peripheral Blood M

Published

2012

29. Functional gene-expression analysis shows involvement of schizophrenia-relevant pathways in patients with 22q11 deletion syndrome

Author

Beveren, N.J.M. (Nico) van, Krab, L.C. (Lianne), Swagemakers, S.M.A. (Sigrid), Buitendijk, G.H.S. (Gabrielle), Boot, E. (Erik), Spek, P.J. (Peter) van der, Elgersma, Y. (Ype), Amelsvoort, T.A.M.J. (Therese) van, Beveren, N.J.M. (Nico) van, Krab, L.C. (Lianne), Swagemakers, S.M.A. (Sigrid), Buitendijk, G.H.S. (Gabrielle), Boot, E. (Erik), Spek, P.J. (Peter) van der, Elgersma, Y. (Ype), and Amelsvoort, T.A.M.J. (Therese) van

Abstract

22q11 Deletion Syndrome (22q11DS) is associated with dysmorphology and a high prevalence of schizophrenia-like symptoms. Several genes located on chromosome 22q11 have been linked to schizophrenia. The deletion is thought to disrupt the expression of multiple genes involved in maturation and development of neurons and neuronal circuits, and neurotransmission. We investigated whole-genome gene expression of Peripheral Blood Mononuclear Cells (PBMC's) of 8 22q11DS patients and 8 age- and gender-matched controls, to (1) investigate the expression levels of 22q11 genes and (2) to investigate whether 22q11 genes participate in functional genetic networks relevant to schizophrenia. Functional relationships between genes differentially expressed in patients (as identified by Locally Adaptive Statistical procedure (LAP) or satisfying p<0.05 and fold-change >1.5) were investigated with the Ingenuity Pathways Analysis (IPA). 14 samples (7 patients, 7 controls) passed quality controls. LAP identified 29 deregulated genes. Pathway analysis showed 262 transcripts differentially expressed between patients and controls. Functional pathways most disturbed were cell death, cell morphology, cellular assembly and organization, and cell-to-cell signaling. In addition, 10 canonical pathways were identified, among which the signal pathways for Natural Killer-cells, neurotrophin/Trk, neuregulin, axonal guidance, and Huntington's disease. Our findings support the use of 22q11DS as a research model for schizophrenia. We identified decreased expression of several genes (among which COMT, Ufd1L, PCQAP, and GNB1L) previously linked to schizophrenia as well as involvement of signaling pathways relevant to schizophrenia, of which Neurotrophin/Trk and neuregulin signaling seems to be especially notable.

Published

2012

30. Enhanced RAD21 cohesin expression confers poor prognosis and resistance to chemotherapy in high grade luminal, basal and HER2 breast cancers

Author

Xu, H. (Huiling), Yan, M. (Max), Patra, J. (Jennifer), Natrajan, R. (Rachael), Swagemakers, S.M.A. (Sigrid), Tomaszewski, J.M. (Jonathan), Verschoor, S. (Sandra), Millar, E.K.A. (Ewan), Spek, P.J. (Peter) van der, Reis-Filho, J.S. (Jorge), Ramsay, R.G. (Robert), O'Toole, S.A. (Sandra), McNeil, C.M. (Catriona), Sutherland, R.L. (Robert), Mckay, M.J. (Michael), Fox, S.B. (Stephen), Xu, H. (Huiling), Yan, M. (Max), Patra, J. (Jennifer), Natrajan, R. (Rachael), Swagemakers, S.M.A. (Sigrid), Tomaszewski, J.M. (Jonathan), Verschoor, S. (Sandra), Millar, E.K.A. (Ewan), Spek, P.J. (Peter) van der, Reis-Filho, J.S. (Jorge), Ramsay, R.G. (Robert), O'Toole, S.A. (Sandra), McNeil, C.M. (Catriona), Sutherland, R.L. (Robert), Mckay, M.J. (Michael), and Fox, S.B. (Stephen)

Abstract

Introduction: RAD21 is a component of the cohesin complex, which is essential for chromosome segregation and error-free DNA repair. We assessed its prognostic and predictive power in a cohort of in situ and invasive breast cancers, and its effect on chemosensitivity in vitro.Methods: RAD21 immunohistochemistry was performed on 345 invasive and 60 pure in situ carcinomas. Integrated genomic and transcriptomic analyses were performed on a further 48 grade 3 invasive cancers. Chemosensitivity was assessed in breast cancer cell lines with an engineered spectrum of RAD21 expression.Results: RAD21 expression correlated with early relapse in all patients (hazard ratio (HR) 1.74, 95% confidence interval (CI) 1.06 to 2.86, P = 0.029). This was due to the effect of grade 3 tumors (but not grade 1 or 2) in which RAD21 expression correlated with early relapse in luminal (P = 0.040), basal (P = 0.018) and HER2 (P = 0.039) groups. In patients treated with chemotherapy, RAD21 expression was associated with shorter overall survival (P = 0.020). RAD21 mRNA expression correlated with DNA copy number, with amplification present in 32% (7/22) of luminal, 31% (4/13) of basal and 22% (2/9) of HER2 grade 3 cancers. Variations in RAD21 mRNA expression in the clinical samples were reflected in the gene expression data from 36 breast cancer cell lines. Knockdown of RAD21 in the MDA-MB-231 breast cancer cell line significantly enhanced sensitivity to cyclophosphamide, 5-fluorouracil and etoposide. The findings for the former two drugs recapitulated the clinical findings.Conclusions: RAD21 expression confers poor prognosis and resistance to chemotherapy in high grade luminal, basal and HER2 breast cancers. RAD21 may be a novel therapeutic target.

Published

2011

31. A genome-wide association study identifies a susceptibility locus for refractive errors and myopia at 15q14

Author

Solouki, A.M. (Abbas), Verhoeven, V.J.M. (Virginie), Duijn, C.M. (Cornelia) van, Verkerk, A.J.H.M. (Annemieke), Ikram, M.K. (Kamran), Hysi, P.G. (Pirro), Despriet, D.D.G. (Dominique), Koolwijk, L.M.E. (Leonieke) van, Ho, L. (Lintje), Ramdas, W.D. (Wishal), Czudowska, M.A. (Monika), Kuijpers, R.W.A.M. (Robert), Amin, N. (Najaf), Struchalin, M.V. (Maksim), Aulchenko, Y.S. (Yurii), Rij, G. (Gabriel) van, Riemslag, F.C.C. (Frans), Young, T.L. (Terry), Mackey, D.A. (David), Spector, T.D. (Timothy), Gorgels, T.G.M.F. (Theo), Willemse-Assink, J.J.M. (Jacqueline), Isaacs, A.J. (Aaron), Kramer, R. (Rogier), Swagemakers, S.M.A. (Sigrid), Bergen, A.A.B. (Arthur), Oosterhout, A.A.L.J. (Andrew) van, Oostra, B.A. (Ben), Rivadeneira Ramirez, F. (Fernando), Uitterlinden, A.G. (André), Hofman, A. (Albert), Jong, P.T.V.M. (Paulus) de, Hammond, C.J. (Christopher), Vingerling, J.R. (Hans), Klaver, C.C.W. (Caroline), Solouki, A.M. (Abbas), Verhoeven, V.J.M. (Virginie), Duijn, C.M. (Cornelia) van, Verkerk, A.J.H.M. (Annemieke), Ikram, M.K. (Kamran), Hysi, P.G. (Pirro), Despriet, D.D.G. (Dominique), Koolwijk, L.M.E. (Leonieke) van, Ho, L. (Lintje), Ramdas, W.D. (Wishal), Czudowska, M.A. (Monika), Kuijpers, R.W.A.M. (Robert), Amin, N. (Najaf), Struchalin, M.V. (Maksim), Aulchenko, Y.S. (Yurii), Rij, G. (Gabriel) van, Riemslag, F.C.C. (Frans), Young, T.L. (Terry), Mackey, D.A. (David), Spector, T.D. (Timothy), Gorgels, T.G.M.F. (Theo), Willemse-Assink, J.J.M. (Jacqueline), Isaacs, A.J. (Aaron), Kramer, R. (Rogier), Swagemakers, S.M.A. (Sigrid), Bergen, A.A.B. (Arthur), Oosterhout, A.A.L.J. (Andrew) van, Oostra, B.A. (Ben), Rivadeneira Ramirez, F. (Fernando), Uitterlinden, A.G. (André), Hofman, A. (Albert), Jong, P.T.V.M. (Paulus) de, Hammond, C.J. (Christopher), Vingerling, J.R. (Hans), and Klaver, C.C.W. (Caroline)

Abstract

Refractive errors are the most common ocular disorders worldwide and may lead to blindness. Although this trait is highly heritable, identification of susceptibility genes has been challenging. We conducted a genome-wide association study for refractive error in 5,328 individuals from a Dutch population-based study with replication in four independent cohorts (combined 10,280 individuals in the replication stage). We identified a significant association at chromosome 15q14 (rs634990, P = 2.21 × 10−14). The odds ratio of myopia compared to hyperopia for the minor allele (minor allele frequency = 0.47) was 1.41 (95% CI 1.16–1.70) for individuals heterozygous for the allele and 1.83 (95% CI 1.42–2.36) for individuals homozygous for the allele. The associated locus is near two genes that are expressed in the retina, GJD2 and ACTC1, and appears to harbor regulatory elements which may influence transcription of these genes. Our data suggest that common variants at 15q14 influence susceptibility for refractive errors in the general population.

Published

2010

32. Proteomic Analysis of Human Osteoblastic Cells: Relevant Proteins and Functional Categories for Differentiation

Author

Alves, R.D.A.M. (Rodrigo), Eijken, H.J.M. (Marco), Swagemakers, S.M.A. (Sigrid), Chiba, H. (Hideki), Titulaer, M.K. (Mark), Burgers, P.C. (Peter), Luider, T.M. (Theo), Leeuwen, J.P.T.M. (Hans) van, Alves, R.D.A.M. (Rodrigo), Eijken, H.J.M. (Marco), Swagemakers, S.M.A. (Sigrid), Chiba, H. (Hideki), Titulaer, M.K. (Mark), Burgers, P.C. (Peter), Luider, T.M. (Theo), and Leeuwen, J.P.T.M. (Hans) van

Abstract

Osteoblasts are the bone forming cells, capable of secreting an extracellular matrix with mineralization potential. The exact mechanism by which osteoblasts differentiate and form a mineralized extracellular matrix is presently not fully understood. To increase our knowledge about this process, we conducted proteomics analysis in human immortalized preosteoblasts (SV-HFO) able to differentiate and mineralize. We identified 381 proteins expressed during the time course of osteoblast differentiation. Gene ontology analysis revealed an overrepresentation of protein categories established as important players for osteoblast differentiation, bone formation, and mineralization such as pyrophosphatases. Proteins involved in antigen presentation, energy metabolism and cytoskeleton rearrangement constitute other overrepresented processes, whose function, albeit interesting, is not fully understood in the context of osteoblast differentiation and bone formation. Correlation analysis, based on quantitative data, revealed a biphasic osteoblast differentiation, encompassing a premineralization and a mineralization period. Identified differentially expressed proteins between mineralized and nonmineralized cells include cytoskeleton (e.g., CCT2, PLEC1, and FLNA) and extracellular matrix constituents (FN1, ANXA2, and LGALS1) among others. FT-ICR-MS data obtained for FN1, ANXA2, and LMNA shows a specific regulation of these proteins during the different phases of osteoblast differentiation. Taken together, this study increases our understanding of the proteomics changes that accompany osteoblast differentiation and may permit the discovery of novel modulators of bone formation.

Published

2010

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

Author

Booij, J.C. (Judith), Brink, J.B. (Jacoline) ten, Swagemakers, S.M.A. (Sigrid), Verkerk, A.J.H.M. (Annemieke), Essing, A.H.W. (Anke), Spek, P.J. (Peter) van der, Bergen, A.A.B. (Arthur), Booij, J.C. (Judith), Brink, J.B. (Jacoline) ten, Swagemakers, S.M.A. (Sigrid), Verkerk, A.J.H.M. (Annemieke), Essing, A.H.W. (Anke), Spek, P.J. (Peter) van der, and Bergen, A.A.B. (Arthur)

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

34. A novel 16p locus associated with BSCL2 hereditary motor neuronopathy: a genetic modifier?

Author

Brusse, E. (Esther), Majoor-Krakauer, D.F. (Danielle), Graaf, B.M. (Bianca) de, Visser, G.H. (Gerhard Henk), Swagemakers, S.M.A. (Sigrid), Boon, A.J.W. (Andrea), Oostra, B.A. (Ben), Bertoli Avella, A.M. (Aida), Brusse, E. (Esther), Majoor-Krakauer, D.F. (Danielle), Graaf, B.M. (Bianca) de, Visser, G.H. (Gerhard Henk), Swagemakers, S.M.A. (Sigrid), Boon, A.J.W. (Andrea), Oostra, B.A. (Ben), and Bertoli Avella, A.M. (Aida)

Abstract

We describe the neurological, electrophysiological, and genetic features of autosomal dominant distal hereditary motor neuronopathy (HMN) in a three-generation Dutch family, including 12 patients with distal muscle weakness and atrophy. The severity of disease ranged from disabling muscle weakness to a subclinical phenotype. Neurologic exams of nine patients and nerve conduction studies (NCS) and myography in five endorsed the variable presentations of HMN in this family, including patients with only lower (four), upper (one), or both upper and lower extremities involvement (four). Asymmetrical or strictly unilateral disease was noted in three patients. Three also showed pyramidal features. A genome-wide search combining SNP arrays (250K) with parametric linkage analysis identified a novel locus on chromosome 16p (mLOD = 3.28) spanning 6 Mb (rs6500882-rs7192086). Direct sequencing excluded mutations in the SIMPLE/LITAF gene (mapping to the 16p locus) and identified a pathogenic mutation (p.N88S) in BCLS2 (11q12-q14). All 12 affected relatives had the BSCL2 mutation and the chromosome 16p haplotype and showed features of motor neuron degeneration. One patient had a very mild phenotype with bilateral pes cavus, normal concentric needle electromyography but signs of motor neuron involvement at electrophysiological muscle scan (EMS). Similar EMS abnormalities in addition to abnormal NCS and myography were observed in a clinically unaffected person (carrying only the 16p haplotype). These results expand the clinical spectrum of HMN and suggest a digenic inheritance of HMN in this family with a BSCL2 mutation and a chromosome 16 locus likely contributing to the phenotype.

Published

2009

35. Functional annotation of the human retinal pigment epithelium transcriptome

Author

Booij, J.C. (Judith), Soest, S. (Simone) van, Swagemakers, S.M.A. (Sigrid), Essing, A.H.W. (Anke), Verkerk, A.J.H.M. (Annemieke), Spek, P.J. (Peter) van der, Gorgels, T.G.M.F. (Theo), Bergen, A.A.B. (Arthur), Booij, J.C. (Judith), Soest, S. (Simone) van, Swagemakers, S.M.A. (Sigrid), Essing, A.H.W. (Anke), Verkerk, A.J.H.M. (Annemieke), Spek, P.J. (Peter) van der, Gorgels, T.G.M.F. (Theo), and Bergen, A.A.B. (Arthur)

Abstract

Background: To determine level, variability and functional annotation of gene expression of the human retinal pigment epithelium (RPE), the key tissue involved in retinal diseases like age-related macular degeneration and retinitis pigmentosa. Macular RPE cells from six selected healthy human donor eyes (aged 63-78 years) were laser dissected and used for 22k microarray studies (Agilent technologies). Data were analyzed with Rosetta Resolver, the web tool DAVID and Ingenuity software. Results: In total, we identified 19,746 array entries with significant expression in the RPE. Gene expression was analyzed according to expression levels, interindividual variability and functionality. A group of highly (n = 2,194) expressed RPE genes showed an overrepresentation of genes of the oxidative phosphorylation, ATP synthesis and ribosome pathways. In the group of moderately expressed genes (n = 8,776) genes of the phosphatidylinositol signaling system and aminosugars metabolism were overrepresented. As expected, the top 10 percent (n = 2,194) of genes with the highest interindividual differences in expression showed functional overrepresentation of the complement cascade, essential in inflammation in age-related macular degeneration, and other signaling pathways. Surprisingly, this same category also includes the genes involved in Bruch's membrane (BM) composition. Among the top 10 percent of genes with low interindividual differences, there was an overrepresentation of genes involved in local glycosaminoglycan turnover. Conclusion: Our study expands current knowledge of the RPE transcriptome by assigning new genes, and adding data about expression level and interindividual variation. Functional annotation suggests that the RPE has high levels of protein synthesis, strong energy demands, and is exposed to high levels of oxidative stress and a variable degree of inflammation. Our data sheds new light on the molecular composition of BM, adjacent to the RPE, and is useful for c

Published

2009

36. A genome-wide linkage scan in a Dutch family identifies a premature ovarian failure susceptibility locus

Author

Oldenburg, R.A. (Rogier), Dooren, M.F. (Marieke) van, Graaf, B.M. (Bianca) de, Simons, E.J. (Erik), Govaerts, L.C. (Lutgarde), Swagemakers, S.M.A. (Sigrid), Verkerk, A.J.H.M. (Annemieke), Oostra, B.A. (Ben), Bertoli Avella, A.M. (Aida), Oldenburg, R.A. (Rogier), Dooren, M.F. (Marieke) van, Graaf, B.M. (Bianca) de, Simons, E.J. (Erik), Govaerts, L.C. (Lutgarde), Swagemakers, S.M.A. (Sigrid), Verkerk, A.J.H.M. (Annemieke), Oostra, B.A. (Ben), and Bertoli Avella, A.M. (Aida)

Abstract

BACKGROUND: Premature ovarian failure (POF) is characterized by elevated gonadotrophins and amenorrhea before the age of 40 years and occurs approximately in 1% of women. POF etiology is highly heterogeneous with a wide spectrum of etiological pathogenic mechanisms including genetic causes. These mostly involve numerical, structural or monogenic defects on the X-chromosome. Mutations in a small number of autosomal genes (such as FOXL2 and NOBOX) have been identified as a cause of POF. However, in most cases, the disease underlying mechanisms are largely unknown. METHODS: We performed a genome-wide linkage analysis in a relatively large Dutch family with seven patients suffering from POF, showing a domina

Published

2008

37. 1α,25‐(OH)2D3 acts in the early phase of osteoblast differentiation to enhance mineralization via accelerated production of mature matrix vesicles

Author

Woeckel, V.J., primary, Alves, R.D.A.M., additional, Swagemakers, S.M.A., additional, Eijken, M., additional, Chiba, H., additional, van der Eerden, B.C.J., additional, and van Leeuwen, J.P.T.M., additional

Published

2010

38. Homologous and non-homologous recombination differentially affect DNA damage repair in mice.

Author

Essers, J. (Jeroen), Steeg, H. (Harry) van, Wit, J. (Jan) de, Vermeij, M. (Marcel), Hoeijmakers, J.H.J. (Jan), Kanaar, R. (Roland), Swagemakers, S.M.A. (Sigrid), Essers, J. (Jeroen), Steeg, H. (Harry) van, Wit, J. (Jan) de, Vermeij, M. (Marcel), Hoeijmakers, J.H.J. (Jan), Kanaar, R. (Roland), and Swagemakers, S.M.A. (Sigrid)

Abstract

Ionizing radiation and interstrand DNA crosslinking compounds provide important treatments against cancer due to their extreme genotoxicity for proliferating cells. Both the efficacies of such treatments and the mutagenic potential of these agents are modulated by the ability of cells to repair the inflicted DNA damage. Here we demonstrate that homologous recombination-deficient mRAD54(-/-) mice are hypersensitive to ionizing radiation at the embryonic but, unexpectedly, not at the adult stage. However, at the adult stage mRAD54 deficiency dramatically aggravates the ionizing radiation sensitivity of severe combined immune deficiency (scid) mice that are impaired in DNA double-strand break repair through DNA end-joining. In contrast, regardless of developmental stage, mRAD54(-/-) mice are hypersensitive to the interstrand DNA crosslinking compound mitomycin C. These results demonstrate that the two major DNA double-strand break repair pathways in mammals have overlapping as well as specialized roles, and that the relative contribution of these pathways towards repair of ionizing radiation-induced DNA damage changes during development of the animal.

Published

2000

39. The human RAD54 recombinational DNA repair protein is a double-stranded DNA-dependent ATPase

Author

Essers, J. (Jeroen), Wit, J. (Jan) de, Kanaar, R. (Roland), Hoeijmakers, J.H.J. (Jan), Swagemakers, S.M.A. (Sigrid), Essers, J. (Jeroen), Wit, J. (Jan) de, Kanaar, R. (Roland), Hoeijmakers, J.H.J. (Jan), and Swagemakers, S.M.A. (Sigrid)

Abstract

DNA double-strand break repair through the RAD52 homologous recombination pathway in the yeast Saccharomyces cerevisiae requires, among others, the RAD51, RAD52, and RAD54 genes. The biological importance of homologous recombination is underscored by the conservation of the RAD52 pathway from fungi to humans. The critical roles of the RAD52 group proteins in the early steps of recombination, the search for DNA homology and strand exchange, are now becoming apparent. Here, we report the purification of the human Rad54 protein. We showed that human Rad54 has ATPase activity that is absolutely dependent on double-stranded DNA. Unexpectedly, the ATPase activity appeared not absolutely required for the DNA repair function of human Rad54 in vivo. Despite the presence of amino acid sequence motifs that are conserved in a large family of DNA helicases, no helicase activity of human Rad54 was observed on a variety of different DNA substrates. Possible functions of human Rad54 in homologous recombination that couple the energy gained from ATP hydrolysis to translocation along DNA, rather than disruption of base pairing, are discussed.

Published

1998

40. Disruption of mouse RAD54 reduces ionizing radiation resistance and homologous recombination.

Author

Essers, J. (Jeroen), Hendriks, R.W. (Rudi), Swagemakers, S.M.A. (Sigrid), Troelstra, C. (Christine), Wit, J. (Jan) de, Bootsma, D. (Dirk), Hoeijmakers, J.H.J. (Jan), Kanaar, R. (Roland), Essers, J. (Jeroen), Hendriks, R.W. (Rudi), Swagemakers, S.M.A. (Sigrid), Troelstra, C. (Christine), Wit, J. (Jan) de, Bootsma, D. (Dirk), Hoeijmakers, J.H.J. (Jan), and Kanaar, R. (Roland)

Abstract

Double-strand DNA break (DSB) repair by homologous recombination occurs through the RAD52 pathway in Saccharomyces cerevisiae. Its biological importance is underscored by the conservation of many RAD52 pathway genes, including RAD54, from fungi to humans. We have analyzed the phenotype of mouse RAD54-/- (mRAD54-/-) cells. Consistent with a DSB repair defect

Published

1997

41. Human and mouse homologs of the Saccharomyces cerevisiae RAD54 DNA repair gene: evidence for functional conservation.

Author

Kanaar, R. (Roland), Troelstra, C. (Christine), Swagemakers, S.M.A. (Sigrid), Essers, J. (Jeroen), Smit, B. (Bep), Franssen, J.H., Pastink, A. (Albert), Bezzubova, O.Y. (Olga), Buerstedde, J-M., Clever, B. (Beate), Heyer, W-D. (Wolf-Dietrich), Hoeijmakers, J.H.J. (Jan), Kanaar, R. (Roland), Troelstra, C. (Christine), Swagemakers, S.M.A. (Sigrid), Essers, J. (Jeroen), Smit, B. (Bep), Franssen, J.H., Pastink, A. (Albert), Bezzubova, O.Y. (Olga), Buerstedde, J-M., Clever, B. (Beate), Heyer, W-D. (Wolf-Dietrich), and Hoeijmakers, J.H.J. (Jan)

Abstract

BACKGROUND: Homologous recombination is of eminent importance both in germ cells, to generate genetic diversity during meiosis, and in somatic cells, to safeguard DNA from genotoxic damage. The genetically well-defined RAD52 pathway is required for these processes in the yeast Saccharomyces cerevisiae. Genes similar to those in the RAD52 group have been identified in mammals. It is not known whether this conservation of primary sequence extends to conservation of function. RESULTS: Here we report the isolation of cDNAs encoding a human and a mouse homolog of RAD54. The human (hHR54) and mouse (mHR54) proteins were 48% identical to Rad54 and belonged to the SNF2/SW12 family, which is characterized by amino-acid motifs found in DNA-dependent ATPases. The hHR54 gene was mapped to chromosome 1p32, and the hHR54 protein was located in the nucleus. We found that the levels of hHR54 mRNA increased in late G1 phase, as has been found for RAD54 mRNA. The level of mHR54 mRNA was el

Published

1996

42. RAD26, the functional S. cerevisiae homolog of the Cockayne syndrome B gene ERCC6.

Author

Gool, A.J. (Alain) van, Verhage, R., Swagemakers, S.M.A. (Sigrid), Putte, P. (Pieter) van de, Brouwer, J. (Jaap), Troelstra, C. (Christine), Bootsma, D. (Dirk), Hoeijmakers, J.H.J. (Jan), Gool, A.J. (Alain) van, Verhage, R., Swagemakers, S.M.A. (Sigrid), Putte, P. (Pieter) van de, Brouwer, J. (Jaap), Troelstra, C. (Christine), Bootsma, D. (Dirk), and Hoeijmakers, J.H.J. (Jan)

Abstract

Transcription-coupled repair (TCR) is a universal sub-pathway of the nucleotide excision repair (NER) system that is limited to the transcribed strand of active structural genes. It accomplishes the preferential elimination of transcription-blocking DNA lesions and permits rapid resumption of the vital process of transcription. A defect in TCR is responsible for the rare hereditary disorder Cockayne syndrome (CS). Recently we found that mutations in the ERCC6 repair gene, encoding a putative helicase, underly the repair defect of CS complementation group B. Here we report the cloning and characterization of the Saccharomyces cerevisiae homolog of CSB/ERCC6, which we designate RAD26. A rad26 disruption mutant appears viable and grows normally, indicating that the gene does not have an essential function. In analogy with CS, preferential repair of UV-induced cyclobutane pyrimidine dimers in the transcribed strand of the active RBP2 gene is severely impaired. Surprisingly, in contrast to the human CS mutant, yeast RAD26 disruption does not induce any UV-, cisPt- or X-ray sensitivity, explaining why it was not isolated as a mutant before. Recovery of growth after UV exposure was somewhat delayed in rad26. These findings suggest that TCR in lower eukaryotes is not very important for cell survival and that the global genome repair pathway of NER is the major determinant of cellular resistance to genotoxicity.

Published

1994

43. Mouse Rad54 affects DNA conformation and DNA-damage-induced Rad51 foci formation

Author

Tan, T.L.R., primary, Essers, J., additional, Citterio, E., additional, Swagemakers, S.M.A., additional, de Wit, J., additional, Benson, F.E., additional, Hoeijmakers, J.H.J., additional, and Kanaar, R., additional

Published

1999