Your search keyword '"Bökenkamp A"' showing total 12 results

1. Pulmonary ductal coarctation and left pulmonary artery interruption; pathology and role of neural crest and second heart field during development.

Author

Adriana C Gittenberger-de Groot, Joshua C Peterson, Lambertus J Wisse, Arno A W Roest, Robert E Poelmann, Regina Bökenkamp, Nynke J Elzenga, Mark Hazekamp, Margot M Bartelings, Monique R M Jongbloed, and Marco C DeRuiter

Subjects

Medicine, Science

Abstract

OBJECTIVES:In congenital heart malformations with pulmonary stenosis to atresia an abnormal lateral ductus arteriosus to left pulmonary artery connection can lead to a localised narrowing (pulmonary ductal coarctation) or even interruption We investigated embryonic remodelling and pathogenesis of this area. MATERIAL AND METHODS:Normal development was studied in WntCre reporter mice (E10.0-12.5) for neural crest cells and Nkx2.5 immunostaining for second heart field cells. Data were compared to stage matched human embryos and a VEGF120/120 mutant mouse strain developing pulmonary atresia. RESULTS:Normal mouse and human embryos showed that the mid-pharyngeal endothelial plexus, connected side-ways to the 6th pharyngeal arch artery. The ventral segment formed the proximal pulmonary artery. The dorsal segment (future DA) was solely surrounded by neural crest cells. The ventral segment had a dual outer lining with neural crest and second heart field cells, while the distal pulmonary artery was covered by none of these cells. The asymmetric contribution of second heart field to the future pulmonary trunk on the left side of the aortic sac (so-called pulmonary push) was evident. The ventral segment became incorporated into the pulmonary trunk leading to a separate connection of the left and right pulmonary arteries. The VEGF120/120 embryos showed a stunted pulmonary push and a variety of vascular anomalies. SUMMARY:Side-way connection of the DA to the left pulmonary artery is a congenital anomaly. The primary problem is a stunted development of the pulmonary push leading to pulmonary stenosis/atresia and a subsequent lack of proper incorporation of the ventral segment into the aortic sac. Clinically, the aberrant smooth muscle tissue of the ductus arteriosus should be addressed to prohibit development of severe pulmonary ductal coarctation or even interruption of the left pulmonary artery.

Published

2020

2. Dlx1 and Rgs5 in the ductus arteriosus: vessel-specific genes identified by transcriptional profiling of laser-capture microdissected endothelial and smooth muscle cells.

Author

Regina Bökenkamp, Ronald van Brempt, Jacoba Cornelia van Munsteren, Ilse van den Wijngaert, Ronald de Hoogt, Livio Finos, Jelle Goeman, Adriana Cornelia Gittenberger-de Groot, Robert Eugen Poelmann, Nicolaas Andreas Blom, and Marcus Cornelis DeRuiter

Subjects

Medicine, Science

Abstract

Closure of the ductus arteriosus (DA) is a crucial step in the transition from fetal to postnatal life. Patent DA is one of the most common cardiovascular anomalies in children with significant clinical consequences especially in premature infants. We aimed to identify genes that specify the DA in the fetus and differentiate it from the aorta. Comparative microarray analysis of laser-captured microdissected endothelial (ECs) and vascular smooth muscle cells (SMCs) from the DA and aorta of fetal rats (embryonic day 18 and 21) identified vessel-specific transcriptional profiles. We found a strong age-dependency of gene expression. Among the genes that were upregulated in the DA the regulator of the G-protein coupled receptor 5 (Rgs5) and the transcription factor distal-less homeobox 1 (Dlx1) exhibited the highest and most significant level of differential expression. The aorta showed a significant preferential expression of the Purkinje cell protein 4 (Pcp4) gene. The results of the microarray analysis were validated by real-time quantitative PCR and immunohistochemistry. Our study confirms vessel-specific transcriptional profiles in ECs and SMCs of rat DA and aorta. Rgs5 and Dlx1 represent novel molecular targets for the regulation of DA maturation and closure.

Published

2014

3. Genes in the ureteric budding pathway: association study on vesico-ureteral reflux patients.

Author

Albertien M van Eerde, Karen Duran, Els van Riel, Carolien G F de Kovel, Bobby P C Koeleman, Nine V A M Knoers, Kirsten Y Renkema, Henricus J R van der Horst, Arend Bökenkamp, Johanna M van Hagen, Leonard H van den Berg, Katja P Wolffenbuttel, Joop van den Hoek, Wouter F Feitz, Tom P V M de Jong, Jacques C Giltay, and Cisca Wijmenga

Subjects

Medicine, Science

Abstract

Vesico-ureteral reflux (VUR) is the retrograde passage of urine from the bladder to the urinary tract and causes 8.5% of end-stage renal disease in children. It is a complex genetic developmental disorder, in which ectopic embryonal ureteric budding is implicated in the pathogenesis. VUR is part of the spectrum of Congenital Anomalies of the Kidney and Urinary Tract (CAKUT). We performed an extensive association study for primary VUR using a two-stage, case-control design, investigating 44 candidate genes in the ureteric budding pathway in 409 Dutch VUR patients. The 44 genes were selected from the literature and a set of 567 single nucleotide polymorphisms (SNPs) capturing their genetic variation was genotyped in 207 cases and 554 controls. The 14 SNPs with p

Published

2012

4. Differential temporal and spatial progerin expression during closure of the ductus arteriosus in neonates.

Author

Regina Bökenkamp, Vered Raz, Andrea Venema, Marco C DeRuiter, Conny van Munsteren, Michelle Olive, Elizabeth G Nabel, and Adriana C Gittenberger-de Groot

Subjects

Medicine, Science

Abstract

Closure of the ductus arteriosus (DA) at birth is essential for the transition from fetal to postnatal life. Before birth the DA bypasses the uninflated lungs by shunting blood from the pulmonary trunk into the systemic circulation. The molecular mechanism underlying DA closure and degeneration has not been fully elucidated, but is associated with apoptosis and cytolytic necrosis in the inner media and intima. We detected features of histology during DA degeneration that are comparable to Hutchinson Gilford Progeria syndrome and ageing. Immunohistochemistry on human fetal and neonatal DA, and aorta showed that lamin A/C was expressed in all layers of the vessel wall. As a novel finding we report that progerin, a splicing variant of lamin A/C was expressed almost selectively in the normal closing neonatal DA, from which we hypothesized that progerin is involved in DA closure. Progerin was detected in 16.2%±7.2 cells of the DA. Progerin-expressing cells were predominantly located in intima and inner media where cytolytic necrosis accompanied by apoptosis will develop. Concomitantly we found loss of α-smooth muscle actin as well as reduced lamin A/C expression compared to the fetal and non-closing DA. In cells of the adjacent aorta, that remains patent, progerin expression was only sporadically detected in 2.5%±1.5 of the cells. Data were substantiated by the detection of mRNA of progerin in the neonatal DA but not in the aorta, by PCR and sequencing analysis. The fetal DA and the non-closing persistent DA did not present with progerin expressing cells. Our analysis revealed that the spatiotemporal expression of lamin A/C and progerin in the neonatal DA was mutually exclusive. We suggest that activation of LMNA alternative splicing is involved in vascular remodeling in the circulatory system during normal neonatal DA closure.

Published

2011

5. Correction: Differential Temporal and Spatial Progerin Expression during Closure of the Ductus Arteriosus in Neonates.

Author

Regina Bökenkamp, Vered Raz, Andrea Venema, Marco C. DeRuiter, Conny van Munsteren, Michelle Olive, Elizabeth G. Nabel, and Adriana C. Gittenberger-de Groot

Subjects

Medicine, Science

Published

2011

6. Pulmonary ductal coarctation and left pulmonary artery interruption; pathology and role of neural crest and second heart field during development

Author

Gittenberger-de Groot, Adriana C., primary, Peterson, Joshua C., additional, Wisse, Lambertus J., additional, Roest, Arno A. W., additional, Poelmann, Robert E., additional, Bökenkamp, Regina, additional, Elzenga, Nynke J., additional, Hazekamp, Mark, additional, Bartelings, Margot M., additional, Jongbloed, Monique R. M., additional, and DeRuiter, Marco C., additional

Published

2020

7. Differential Temporal and Spatial Progerin Expression during Closure of the Ductus Arteriosus in Neonates

Author

Vered Raz, Michelle Olive, Andrea Venema, Adriana C. Gittenberger-de Groot, Regina Bökenkamp, Elizabeth G. Nabel, Conny J. van Munsteren, and Marco C. DeRuiter

Subjects

Pathology, Anatomy and Physiology, lcsh:Medicine, Gene Expression, Cardiovascular, Cell Fate Determination, Cardiovascular System, Pediatrics, Gene Splicing, LMNA, Progeria, Pregnancy, Ductus arteriosus, Molecular Cell Biology, Pediatric Cardiology, Morphogenesis, lcsh:Science, Neonatalology, Multidisciplinary, integumentary system, Reverse Transcriptase Polymerase Chain Reaction, Congenital Heart Disease, Nuclear Proteins, Progerin, Lamin Type A, Immunohistochemistry, medicine.anatomical_structure, Circulatory system, embryonic structures, Heart Development, Medicine, Female, Research Article, medicine.medical_specialty, Biology, In Vitro Techniques, Vascular Biology, medicine.artery, medicine, Genetics, Humans, Protein Precursors, Fetus, Aorta, lcsh:R, Infant, Newborn, Ductus Arteriosus, medicine.disease, Cardiovascular Anatomy, lcsh:Q, Tunica Intima, Lamin, Developmental Biology

Abstract

Closure of the ductus arteriosus (DA) at birth is essential for the transition from fetal to postnatal life. Before birth the DA bypasses the uninflated lungs by shunting blood from the pulmonary trunk into the systemic circulation. The molecular mechanism underlying DA closure and degeneration has not been fully elucidated, but is associated with apoptosis and cytolytic necrosis in the inner media and intima. We detected features of histology during DA degeneration that are comparable to Hutchinson Gilford Progeria syndrome and ageing. Immunohistochemistry on human fetal and neonatal DA, and aorta showed that lamin A/C was expressed in all layers of the vessel wall. As a novel finding we report that progerin, a splicing variant of lamin A/C was expressed almost selectively in the normal closing neonatal DA, from which we hypothesized that progerin is involved in DA closure. Progerin was detected in 16.2%±7.2 cells of the DA. Progerin-expressing cells were predominantly located in intima and inner media where cytolytic necrosis accompanied by apoptosis will develop. Concomitantly we found loss of α-smooth muscle actin as well as reduced lamin A/C expression compared to the fetal and non-closing DA. In cells of the adjacent aorta, that remains patent, progerin expression was only sporadically detected in 2.5%±1.5 of the cells. Data were substantiated by the detection of mRNA of progerin in the neonatal DA but not in the aorta, by PCR and sequencing analysis. The fetal DA and the non-closing persistent DA did not present with progerin expressing cells. Our analysis revealed that the spatiotemporal expression of lamin A/C and progerin in the neonatal DA was mutually exclusive. We suggest that activation of LMNA alternative splicing is involved in vascular remodeling in the circulatory system during normal neonatal DA closure.

Published

2011

8. Genes in the ureteric budding pathway: association study on vesico-ureteral reflux patients

Author

Cisca Wijmenga, Nine V A M Knoers, Albertien M. van Eerde, Karen Duran, Johanna M. van Hagen, Tom P.V.M. de Jong, Els van Riel, Katja P. Wolffenbuttel, Wouter F.J. Feitz, Joop van den Hoek, Henricus J. R. van der Horst, Leonard H. van den Berg, Arend Bökenkamp, Bobby P. C. Koeleman, Kirsten Y. Renkema, Carolien G.F. de Kovel, Jacques C. Giltay, Urology, Paediatric Urology, Pediatric surgery, Human genetics, ICaR - Circulation and metabolism, and Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI)

Subjects

Candidate gene, Embryology, Heredity, Anatomy and Physiology, Genome-wide association study, Bioinformatics, urologic and male genital diseases, Gastroenterology, DISEASE, Linkage Disequilibrium, Morphogenesis, Tissue engineering and pathology Renal disorder [NCMLS 3], Receptors, Immunologic, Netherlands, Uroplakin III, Multidisciplinary, Pediatric Urology, Pediatric Nephrology, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, ROBO2, Developmental Nephrology, female genital diseases and pregnancy complications, medicine.anatomical_structure, Nephrology, Intercellular Signaling Peptides and Proteins, Medicine, Research Article, medicine.medical_specialty, Genotype, Science, Urinary system, Urology, Single-nucleotide polymorphism, Genetic Counseling, Biology, Polymorphism, Single Nucleotide, Transforming Growth Factor beta1, Ureter, KIDNEY BRANCHING MORPHOGENESIS, Genetic Mutation, Internal medicine, Genetic variation, medicine, Genetic predisposition, LINKAGE, Genetics, Humans, Renal Anatomy, GENOME-WIDE ASSOCIATION, Genetic Association Studies, Vesico-Ureteral Reflux, MUTATIONS, Complex Traits, Case-control study, UROPLAKIN-III GENE, Genetic Variation, Human Genetics, Renal System, POLYMORPHISM, Case-Control Studies, Genetics of Disease, TRACT MALFORMATIONS, Protein Tyrosine Phosphatases, Developmental Biology

Abstract

Contains fulltext : 107989.pdf (Publisher’s version ) (Open Access) Vesico-ureteral reflux (VUR) is the retrograde passage of urine from the bladder to the urinary tract and causes 8.5% of end-stage renal disease in children. It is a complex genetic developmental disorder, in which ectopic embryonal ureteric budding is implicated in the pathogenesis. VUR is part of the spectrum of Congenital Anomalies of the Kidney and Urinary Tract (CAKUT). We performed an extensive association study for primary VUR using a two-stage, case-control design, investigating 44 candidate genes in the ureteric budding pathway in 409 Dutch VUR patients. The 44 genes were selected from the literature and a set of 567 single nucleotide polymorphisms (SNPs) capturing their genetic variation was genotyped in 207 cases and 554 controls. The 14 SNPs with p

Published

2011

9. Dlx1 and Rgs5 in the Ductus Arteriosus: Vessel-Specific Genes Identified by Transcriptional Profiling of Laser-Capture Microdissected Endothelial and Smooth Muscle Cells

Author

Bökenkamp, Regina, primary, van Brempt, Ronald, additional, van Munsteren, Jacoba Cornelia, additional, van den Wijngaert, Ilse, additional, de Hoogt, Ronald, additional, Finos, Livio, additional, Goeman, Jelle, additional, Groot, Adriana Cornelia Gittenberger-de, additional, Poelmann, Robert Eugen, additional, Blom, Nicolaas Andreas, additional, and DeRuiter, Marcus Cornelis, additional

Published

2014

10. Genes in the Ureteric Budding Pathway: Association Study on Vesico-Ureteral Reflux Patients

Author

van Eerde, Albertien M., primary, Duran, Karen, additional, van Riel, Els, additional, de Kovel, Carolien G. F., additional, Koeleman, Bobby P. C., additional, Knoers, Nine V. A. M., additional, Renkema, Kirsten Y., additional, van der Horst, Henricus J. R., additional, Bökenkamp, Arend, additional, van Hagen, Johanna M., additional, van den Berg, Leonard H., additional, Wolffenbuttel, Katja P., additional, van den Hoek, Joop, additional, Feitz, Wouter F., additional, de Jong, Tom P. V. M., additional, Giltay, Jacques C., additional, and Wijmenga, Cisca, additional

Published

2012

11. Differential Temporal and Spatial Progerin Expression during Closure of the Ductus Arteriosus in Neonates

Author

Bökenkamp, Regina, primary, Raz, Vered, additional, Venema, Andrea, additional, DeRuiter, Marco C., additional, van Munsteren, Conny, additional, Olive, Michelle, additional, Nabel, Elizabeth G., additional, and Gittenberger-de Groot, Adriana C., additional

Published

2011

12. Genes in the Ureteric Budding Pathway: Association Study on Vesico-Ureteral Reflux Patients.

Author

Eerde, Albertien M. van, Duran, Karen, Riel, Els van, Kovel, Carolien G. F. de, Koeleman, Bobby P. C., Knoers, Nine V. A. M., Renkema, Kirsten Y., van der Horst, Henricus J. R, Bökenkamp, Arend, van Hagen, Johanna M., van den Berg, Leonard H., Wolffenbuttel, Katja P., van den Hoek, Joop, Feitz, Wouter F., de Jong, Tom P. V. M., Giltay, Jacques C., and Wijmenga, Cisca

Subjects

GENES, VESICO-ureteral reflux, KIDNEY diseases, SINGLE nucleotide polymorphisms, URINARY organs, PATIENTS

Abstract

Vesico-ureteral reflux (VUR) is the retrograde passage of urine from the bladder to the urinary tract and causes 8.5% of end-stage renal disease in children. It is a complex genetic developmental disorder, in which ectopic embryonal ureteric budding is implicated in the pathogenesis. VUR is part of the spectrum of Congenital Anomalies of the Kidney and Urinary Tract (CAKUT). We performed an extensive association study for primary VUR using a two-stage, case-control design, investigating 44 candidate genes in the ureteric budding pathway in 409 Dutch VUR patients. The 44 genes were selected from the literature and a set of 567 single nucleotide polymorphisms (SNPs) capturing their genetic variation was genotyped in 207 cases and 554 controls. The 14 SNPs with p<0.005 were included in a follow-up study in 202 cases and 892 controls. Of the total cohort, ∼50% showed a clear-cut primary VUR phenotype and ∼25% had both a duplex collecting system and VUR. We also looked for association in these two extreme phenotype groups. None of the SNPs reached a significant p-value. Common genetic variants in four genes (GREM1, EYA1, ROBO2 and UPK3A) show a trend towards association with the development of primary VUR (GREM1, EYA1, ROBO2) or duplex collecting system (EYA1 and UPK3A). SNPs in three genes (TGFB1, GNB3 and VEGFA) have been shown to be associated with VUR in other populations. Only the result of rs1800469 in TGFB1 hinted at association in our study. This is the first extensive study of common variants in the genes of the ureteric budding pathway and the genetic susceptibility to primary VUR. [ABSTRACT FROM AUTHOR]

Published

2012