Your search keyword '"Irinna Papangeli"' showing total 31 results

1. Transcriptional profile of the rat cardiovascular system at single-cell resolution

Author

Alessandro Arduini, Stephen J. Fleming, Ling Xiao, Amelia W. Hall, Amer-Denis Akkad, Mark D. Chaffin, Kayla J. Bendinelli, Nathan R. Tucker, Irinna Papangeli, Helene Mantineo, Patricio Flores-Bringas, Mehrtash Babadi, Christian M. Stegmann, Guillermo García-Cardeña, Mark E. Lindsay, Carla Klattenhoff, and Patrick T. Ellinor

Subjects

CP: Developmental biology, Biology (General), QH301-705.5

Abstract

Summary: We sought to characterize cellular composition across the cardiovascular system of the healthy Wistar rat, an important model in preclinical cardiovascular research. We performed single-nucleus RNA sequencing (snRNA-seq) in 78 samples in 10 distinct regions, including the four chambers of the heart, ventricular septum, sinoatrial node, atrioventricular node, aorta, pulmonary artery, and pulmonary veins, which produced 505,835 nuclei. We identified 26 distinct cell types and additional subtypes, with different cellular composition across cardiac regions and tissue-specific transcription for each cell type. Several cell subtypes were region specific, including a subtype of vascular smooth muscle cells enriched in the large vasculature. We observed tissue-enriched cellular communication networks, including heightened Nppa-Npr1/2/3 signaling in the sinoatrial node. The existence of tissue-restricted cell types suggests regional regulation of cardiovascular physiology. Our detailed transcriptional characterization of each cell type offers the potential to identify novel therapeutic targets and improve preclinical models of cardiovascular disease.

Published

2025

2. Endothelial β‐arrestins regulate mechanotransduction by the type II bone morphogenetic protein receptor in primary cilia

Author

Saejeong Park, Zhiyuan Ma, Georgia Zarkada, Irinna Papangeli, Sarin Paluri, Nour Nazo, Felix Rivera‐Molina, Derek Toomre, Sudarshan Rajagopal, and Hyung J. Chun

Subjects

beta‐arrestin, BMPR2, endothelial cells, primary cilia, shear stress, Diseases of the circulatory (Cardiovascular) system, RC666-701, Diseases of the respiratory system, RC705-779

Abstract

Abstract Modulation of endothelial cell behavior and phenotype by hemodynamic forces involves many signaling components, including cell surface receptors, intracellular signaling intermediaries, transcription factors, and epigenetic elements. Many of the signaling mechanisms that underlie mechanotransduction by endothelial cells are inadequately defined. Here we sought to better understand how β‐arrestins, intracellular proteins that regulate agonist‐mediated desensitization and integration of signaling by transmembrane receptors, may be involved in the endothelial cell response to shear stress. We performed both in vitro studies with primary endothelial cells subjected to β‐arrestin knockdown, and in vivo studies using mice with endothelial specific deletion of β‐arrestin 1 and β‐arrestin 2. We found that β‐arrestins are localized to primary cilia in endothelial cells, which are present in subpopulations of endothelial cells in relatively low shear states. Recruitment of β‐arrestins to cilia involved its interaction with IFT81, a component of the flagellar transport protein complex in the cilia. β‐arrestin knockdown led to marked reduction in shear stress response, including induction of NOS3 expression. Within the cilia, β‐arrestins were found to associate with the type II bone morphogenetic protein receptor (BMPR‐II), whose disruption similarly led to an impaired endothelial shear response. β‐arrestins also regulated Smad transcription factor phosphorylation by BMPR‐II. Mice with endothelial specific deletion of β‐arrestin 1 and β‐arrestin 2 were found to have impaired retinal angiogenesis. In conclusion, we have identified a novel role for endothelial β‐arrestins as key transducers of ciliary mechanotransduction that play a central role in shear signaling by BMPR‐II and contribute to vascular development.

Published

2022

3. A PPARγ-dependent miR-424/503-CD40 axis regulates inflammation mediated angiogenesis

Author

Aram Lee, Irinna Papangeli, Youngsook Park, Ha-neul Jeong, Jihea Choi, Hyesoo Kang, Ha-neul Jo, Jongmin Kim, and Hyung J. Chun

Subjects

Medicine, Science

Abstract

Abstract Activation of the endothelium by pro-inflammatory stimuli plays a key role in the pathogenesis of a multitude of vascular diseases. Angiogenesis is a crucial component of the vascular response associated with inflammatory signaling. The CD40/CD40 ligand dyad in endothelial cells (EC) has a central role in promoting vascular inflammatory response; however, the molecular mechanism underlying this component of inflammation and angiogenesis is not fully understood. Here we report a novel microRNA mediated suppression of endothelial CD40 expression. We found that CD40 is closely regulated by miR-424 and miR-503, which directly target its 3′ untranslated region. Pro-inflammatory stimuli led to increased endothelial CD40 expression, at least in part due to decreased miR-424 and miR-503 expression. In addition, miR-424 and miR-503 reduced LPS induced EC sprouting, migration and tube formation. Moreover, we found that miR-424 and miR-503 expression is directly regulated by peroxisome proliferator-activated receptor gamma (PPARγ), whose endothelial expression and activity are decreased in response to inflammatory factors. Finally, we demonstrate that mice with endothelial-specific deletion of miR-322 (miR-424 ortholog) and miR-503 have augmented angiogenic response to LPS in a Matrigel plug assay. Overall, these studies identify a PPARγ-dependent miR-424/503-CD40 signaling axis that is critical for regulation of inflammation mediated angiogenesis.

Published

2017

4. MicroRNA 139-5p coordinates APLNR-CXCR4 crosstalk during vascular maturation

Author

Irinna Papangeli, Jongmin Kim, Inna Maier, Saejeong Park, Aram Lee, Yujung Kang, Keiichiro Tanaka, Omar F. Khan, Hyekyung Ju, Yoko Kojima, Kristy Red-Horse, Daniel G. Anderson, Arndt F. Siekmann, and Hyung J. Chun

Subjects

Science

Abstract

G protein-coupled receptors APLNR and CXCR4 are crucial for vascular development. Here, the authors show that these two signaling pathways communicate and that in response to blood flow APLNR signaling induces a decrease in CXCR4 expression via miR-139-5p, thereby restricting CXCR4 expression to the non-flow exposed tip cells in the retinal vasculature.

Published

2016

5. Single-nucleus profiling of human dilated and hypertrophic cardiomyopathy

Author

Mark Chaffin, Irinna Papangeli, Bridget Simonson, Amer-Denis Akkad, Matthew C. Hill, Alessandro Arduini, Stephen J. Fleming, Michelle Melanson, Sikander Hayat, Maria Kost-Alimova, Ondine Atwa, Jiangchuan Ye, Kenneth C. Bedi, Matthias Nahrendorf, Virendar K. Kaushik, Christian M. Stegmann, Kenneth B. Margulies, Nathan R. Tucker, and Patrick T. Ellinor

Subjects

Multidisciplinary

Published

2022

6. BMPR1A Promotes ID2-ZEB1 Interaction to Suppress Excessive Endothelial to Mesenchymal Transition

Author

Heon-Woo Lee, Takaomi Adachi, Boryeong Pak, Saejeong Park, Xiaoyue Hu, Woosoung Choi, Piotr S Kowalski, C Hong Chang, Katharine R Clapham, Aram Lee, Irinna Papangeli, Jongmin Kim, Orjin Han, Jihwan Park, Daniel G Anderson, Michael Simons, Suk-Won Jin, and Hyung J Chun

Subjects

Physiology, Physiology (medical), Cardiology and Cardiovascular Medicine

Abstract

Aims Components of bone morphogenetic protein (BMP) signalling have been implicated in both pathogenesis of pulmonary arterial hypertension (PAH) and endothelial-mesenchymal transition (EndoMT). In particular, the importance of BMP type 2 receptor in these processes has been extensively analysed. However, the contribution of BMP type 1 receptors (BMPR1s) to the onset of PAH and EndoMT remains poorly understood. BMPR1A, one of BMPR1s, was recently implicated in the pathogenesis of PAH, and was found to be down-regulated in the lungs of PAH patients, neither the downstream mechanism nor its contribution to EndoMT has been described. Therefore, we aim to delineate the role of endothelial BMPR1A in modulating EndoMT and pathogenesis of PAH. Methods and results We find that BMPR1A knockdown in endothelial cells (ECs) induces hallmarks of EndoMT, and deletion of endothelial Bmpr1a in adult mice (Bmpr1aiECKO) leads to development of PAH-like symptoms due to excessive EndoMT. By lineage tracing, we show that endothelial-derived smooth muscle cells are increased in endothelial Bmpr1a-deleted mice. Mechanistically, we identify ZEB1 as a primary target for BMPR1A in this setting; upon BMPR1A activation, ID2 physically interacts and sequesters ZEB1 to attenuate transcription of Tgfbr2, which in turn lowers the responses of ECs towards transforming growth factor beta (TGFβ) stimulation and prevents excessive EndoMT. In Bmpr1aiECKO mice, administering endothelial targeting lipid nanoparticles containing siRNA against Tgfbr2 effectively ameliorate PAH, reiterating the importance of BMPR1A-ID2/ZEB1-TGFBR2 axis in modulating progression of EndoMT and pathogenesis of PAH. Conclusions We demonstrate that BMPR1A is key to maintain endothelial identity and to prevent excessive EndoMT. We identify BMPR1A-induced interaction between ID2 and ZEB1 is the key regulatory step for onset of EndoMT and pathogenesis of PAH. Our findings indicate that BMPR1A-ID2/ZEB1-TGFBR2 signalling axis could serve as a potential novel therapeutic target for PAH and other EndoMT-related vascular disorders.

Published

2022

7. Single-nucleus profiling of human dilated and hypertrophic cardiomyopathy

Author

Mark, Chaffin, Irinna, Papangeli, Bridget, Simonson, Amer-Denis, Akkad, Matthew C, Hill, Alessandro, Arduini, Stephen J, Fleming, Michelle, Melanson, Sikander, Hayat, Maria, Kost-Alimova, Ondine, Atwa, Jiangchuan, Ye, Kenneth C, Bedi, Matthias, Nahrendorf, Virendar K, Kaushik, Christian M, Stegmann, Kenneth B, Margulies, Nathan R, Tucker, and Patrick T, Ellinor

Subjects

Cardiomyopathy, Dilated, Cell Nucleus, Heart Failure, Transcription, Genetic, Gene Expression Profiling, Heart Ventricles, Myocardium, Cardiomyopathy, Hypertrophic, Transforming Growth Factor beta1, Gene Knockout Techniques, Case-Control Studies, Humans, RNA-Seq, CRISPR-Cas Systems, Single-Cell Analysis, Myofibroblasts, Cells, Cultured

Abstract

Heart failure encompasses a heterogeneous set of clinical features that converge on impaired cardiac contractile function

Published

2021

8. Transcriptional and Cellular Diversity of the Human Heart

Author

Kristin G. Ardlie, Nathan R. Tucker, Kenneth B. Margulies, Carolina Roselli, Seung Hoan Choi, Victoria A. Parsons, Christian Stegmann, Caroline N. Herndon, Amelia W. Hall, Patrick T. Ellinor, Stephen J. Fleming, Amer-Denis Akkad, Alessandro Arduini, Mehrtash Babadi, Kenneth Bedi, Irinna Papangeli, François Aguet, and Mark Chaffin

Subjects

Transcription, Genetic, Cell, 030204 cardiovascular system & hematology, Genome, Transcriptome, 0302 clinical medicine, cardiovascular disease, Gene expression, Adipocytes, Medicine, Homeostasis, Myocytes, Cardiac, RNA-Seq, 0303 health sciences, Sex Characteristics, HERITABILITY, Heart, ASSOCIATION, Microfluidic Analytical Techniques, Middle Aged, STEP, medicine.anatomical_structure, Single-Cell Analysis, Cardiology and Cardiovascular Medicine, EXPRESSION, Adult, Cell type, Heart Diseases, Heart Ventricles, Myocytes, Smooth Muscle, Computational biology, Biology, Article, 03 medical and health sciences, Physiology (medical), Humans, Heart Atria, Gene, Genetic association, 030304 developmental biology, Aged, IDENTIFICATION, business.industry, Macrophages, Myocardium, RNA, Human heart, Endothelial Cells, Cardiovascular Agents, Fibroblasts, Lymphocyte Subsets, Gene Ontology, Single cell sequencing, business, Pericytes, 030217 neurology & neurosurgery, Function (biology)

Abstract

Background: The human heart requires a complex ensemble of specialized cell types to perform its essential function. A greater knowledge of the intricate cellular milieu of the heart is critical to increase our understanding of cardiac homeostasis and pathology. As recent advances in low-input RNA sequencing have allowed definitions of cellular transcriptomes at single-cell resolution at scale, we have applied these approaches to assess the cellular and transcriptional diversity of the nonfailing human heart. Methods: Microfluidic encapsulation and barcoding was used to perform single nuclear RNA sequencing with samples from 7 human donors, selected for their absence of overt cardiac disease. Individual nuclear transcriptomes were then clustered based on transcriptional profiles of highly variable genes. These clusters were used as the basis for between-chamber and between-sex differential gene expression analyses and intersection with genetic and pharmacologic data. Results: We sequenced the transcriptomes of 287 269 single cardiac nuclei, revealing 9 major cell types and 20 subclusters of cell types within the human heart. Cellular subclasses include 2 distinct groups of resident macrophages, 4 endothelial subtypes, and 2 fibroblast subsets. Comparisons of cellular transcriptomes by cardiac chamber or sex reveal diversity not only in cardiomyocyte transcriptional programs but also in subtypes involved in extracellular matrix remodeling and vascularization. Using genetic association data, we identified strong enrichment for the role of cell subtypes in cardiac traits and diseases. Intersection of our data set with genes on cardiac clinical testing panels and the druggable genome reveals striking patterns of cellular specificity. Conclusions: Using large-scale single nuclei RNA sequencing, we defined the transcriptional and cellular diversity in the normal human heart. Our identification of discrete cell subtypes and differentially expressed genes within the heart will ultimately facilitate the development of new therapeutics for cardiovascular diseases.

Published

2020

9. CRISPR/Cas9 gene-editing: Research technologies, clinical applications and ethical considerations

Author

Irinna Papangeli, Fani Memi, and Aglaia Ntokou

Subjects

Gene Editing, 0301 basic medicine, Genetic Research, Evidence-Based Medicine, business.industry, Cas9, Genetic enhancement, MEDLINE, Obstetrics and Gynecology, Context (language use), Genetic Therapy, Evidence-based medicine, Computational biology, Morals, 03 medical and health sciences, 030104 developmental biology, Genome editing, Pediatrics, Perinatology and Child Health, Humans, Medicine, CRISPR, Bioethical Issues, CRISPR-Cas Systems, business, Repurposing

Abstract

Gene therapy carries the potential to treat more than 10,000 human monogenic diseases and benefit an even greater number of complex polygenic conditions. The repurposing of CRISPR/Cas9, an ancient bacterial immune defense system, into a gene-editing technology has armed researchers with a revolutionary tool for gene therapy. However, as the breadth of research and clinical applications of this technology continues to expand, outstanding technical challenges and ethical considerations will need to be addressed before clinical applications become commonplace. Here, we review CRISPR/Cas9 technology and discuss its benefits and limitations in research and the clinical context, as well as ethical considerations surrounding the use of CRISPR gene editing.

Published

2018

10. Therapeutic Engagement of the Histone Deacetylase IIA–Myocyte Enhancer Factor 2 Axis Improves Experimental Pulmonary Hypertension

Author

Serpil C. Erzurum, Suzy A. A. Comhair, Hyung J. Chun, Takaomi Adachi, Irinna Papangeli, Cheol Hwangbo, John J. Schwarz, Avraham Sofer, Seyoung Lee, Paul DaSilva-Jardine, and Jongmin Kim

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, MEF2 Transcription Factors, Extramural, business.industry, Hypertension, Pulmonary, Fluorescent Antibody Technique, 030204 cardiovascular system & hematology, Critical Care and Intensive Care Medicine, medicine.disease, Pulmonary hypertension, Histone Deacetylases, Disease Models, Animal, Mice, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Text mining, Myocyte Enhancer Factor 2, Correspondence, Cancer research, Animals, Medicine, Histone deacetylase, business

Published

2018

11. Modulation of Endothelial Bone Morphogenetic Protein Receptor Type 2 Activity by Vascular Endothelial Growth Factor Receptor 3 in Pulmonary Arterial Hypertension

Author

Eun Mi Hwang, William P. Dunworth, Jean-Leon Thomas, Suk-Won Jin, Xiaoyue Hu, Omar El-Hely, Serpil C. Erzurum, Boryeong Pak, Suzy A. A. Comhair, Heon Lee, Hyung J. Chun, Cheol Hwangbo, Hyekyung Ju, Jun Dae Kim, Jinah Han, Laura A Peterson, Irinna Papangeli, Seyoung Lee, Victoria L. Bautch, Jae Yong Park, Avraham Sofer, Hyeseon Kang, and David S. Wiley

Subjects

0301 basic medicine, business.industry, Vascular Endothelial Growth Factor Receptor, Bone morphogenetic protein receptor type 2, Bone morphogenetic protein, medicine.disease, Pulmonary hypertension, Cell biology, BMPR2, Vascular endothelial growth factor B, 03 medical and health sciences, Vascular endothelial growth factor A, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Physiology (medical), medicine, Cancer research, Cardiology and Cardiovascular Medicine, business, Function (biology)

Abstract

Background: Bone morphogenetic protein (BMP) signaling has multiple roles in the development and function of the blood vessels. In humans, mutations in BMP receptor type 2 (BMPR2), a key component of BMP signaling, have been identified in the majority of patients with familial pulmonary arterial hypertension (PAH). However, only a small subset of individuals with BMPR2 mutation develops PAH, suggesting that additional modifiers of BMPR2 function play an important role in the onset and progression of PAH. Methods: We used a combination of studies in zebrafish embryos and genetically engineered mice lacking endothelial expression of Vegfr3 to determine the interaction between vascular endothelial growth factor receptor 3 (VEGFR3) and BMPR2. Additional in vitro studies were performed by using human endothelial cells, including primary lung endothelial cells from subjects with PAH. Results: Attenuation of Vegfr3 in zebrafish embryos abrogated Bmp2b-induced ectopic angiogenesis. Endothelial cells with disrupted VEGFR3 expression failed to respond to exogenous BMP stimulation. Mechanistically, VEGFR3 is physically associated with BMPR2 and facilitates ligand-induced endocytosis of BMPR2 to promote phosphorylation of SMADs and transcription of ID genes. Conditional, endothelial-specific deletion of Vegfr3 in mice resulted in impaired BMP signaling responses, and significantly worsened hypoxia-induced pulmonary hypertension. Consistent with these data, we found significant decrease in VEGFR3 expression in pulmonary arterial endothelial cells from human PAH subjects, and reconstitution of VEGFR3 expression in PAH pulmonary arterial endothelial cells restored BMP signaling responses. Conclusions: Our findings identify VEGFR3 as a key regulator of endothelial BMPR2 signaling and a potential determinant of PAH penetrance in humans.

Published

2017

12. A PPARγ-dependent miR-424/503-CD40 axis regulates inflammation mediated angiogenesis

Author

Ha-neul Jeong, Aram Lee, Jongmin Kim, Youngsook Park, Hyesoo Kang, Ha-neul Jo, Irinna Papangeli, Jihea Choi, and Hyung J. Chun

Subjects

0301 basic medicine, medicine.medical_specialty, Endothelium, Angiogenesis, Science, Peroxisome proliferator-activated receptor, Inflammation, Biology, Article, 03 medical and health sciences, Mice, Cell Movement, Internal medicine, microRNA, medicine, Morphogenesis, Animals, Humans, CD40 Antigens, Receptor, Cell Proliferation, chemistry.chemical_classification, Tube formation, Multidisciplinary, Neovascularization, Pathologic, Cell biology, PPAR gamma, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, chemistry, Medicine, medicine.symptom, Signal transduction, Signal Transduction

Abstract

Activation of the endothelium by pro-inflammatory stimuli plays a key role in the pathogenesis of a multitude of vascular diseases. Angiogenesis is a crucial component of the vascular response associated with inflammatory signaling. The CD40/CD40 ligand dyad in endothelial cells (EC) has a central role in promoting vascular inflammatory response; however, the molecular mechanism underlying this component of inflammation and angiogenesis is not fully understood. Here we report a novel microRNA mediated suppression of endothelial CD40 expression. We found that CD40 is closely regulated by miR-424 and miR-503, which directly target its 3′ untranslated region. Pro-inflammatory stimuli led to increased endothelial CD40 expression, at least in part due to decreased miR-424 and miR-503 expression. In addition, miR-424 and miR-503 reduced LPS induced EC sprouting, migration and tube formation. Moreover, we found that miR-424 and miR-503 expression is directly regulated by peroxisome proliferator-activated receptor gamma (PPARγ), whose endothelial expression and activity are decreased in response to inflammatory factors. Finally, we demonstrate that mice with endothelial-specific deletion of miR-322 (miR-424 ortholog) and miR-503 have augmented angiogenic response to LPS in a Matrigel plug assay. Overall, these studies identify a PPARγ-dependent miR-424/503-CD40 signaling axis that is critical for regulation of inflammation mediated angiogenesis.

Published

2017

13. MicroRNA 139-5p coordinates APLNR-CXCR4 crosstalk during vascular maturation

Author

Hyekyung Ju, Omar F. Khan, Yujung Kang, Arndt F. Siekmann, Aram Lee, Saejeong Park, Irinna Papangeli, Keiichiro Tanaka, Hyung J. Chun, Inna Maier, Kristy Red-Horse, Daniel G. Anderson, Jongmin Kim, Yoko Kojima, Harvard University--MIT Division of Health Sciences and Technology, Koch Institute for Integrative Cancer Research at MIT, Khan, Omar Fizal, and Anderson, Daniel Griffith

Subjects

0301 basic medicine, medicine.medical_specialty, Receptors, CXCR4, Science, General Physics and Astronomy, Down-Regulation, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Receptors, G-Protein-Coupled, 03 medical and health sciences, Downregulation and upregulation, Adipokines, Internal medicine, microRNA, medicine, Atorvastatin, Animals, Receptor, G protein-coupled receptor, Apelin receptor, Apelin Receptors, Multidisciplinary, Endothelial Cells, Retinal Vessels, General Chemistry, Receptor Cross-Talk, Phenotype, Cell biology, Apelin, Mice, Inbred C57BL, Crosstalk (biology), MicroRNAs, 030104 developmental biology, Endocrinology, Hemorheology, Intercellular Signaling Peptides and Proteins

Abstract

G protein-coupled receptor (GPCR) signalling, including that involving apelin (APLN) and its receptor APLNR, is known to be important in vascular development. How this ligand–receptor pair regulates the downstream signalling cascades in this context remains poorly understood. Here, we show that mice with Apln, Aplnr or endothelial-specific Aplnr deletion develop profound retinal vascular defects, which are at least in part due to dysregulated increase in endothelial CXCR4 expression. Endothelial CXCR4 is negatively regulated by miR-139-5p, whose transcription is in turn induced by laminar flow and APLN/APLNR signalling. Inhibition of miR-139-5p in vivo partially phenocopies the retinal vascular defects of APLN/APLNR deficiency. Pharmacological inhibition of CXCR4 signalling or augmentation of the miR-139-5p-CXCR4 axis can ameliorate the vascular phenotype of APLN/APLNR deficient state. Overall, we identify an important microRNA-mediated GPCR crosstalk, which plays a key role in vascular development., G protein-coupled receptors APLNR and CXCR4 are crucial for vascular development. Here, the authors show that these two signaling pathways communicate and that in response to blood flow APLNR signaling induces a decrease in CXCR4 expression via miR-139-5p, thereby restricting CXCR4 expression to the non-flow exposed tip cells in the retinal vasculature.

Published

2016

14. Tissue-specific miRNA Expression Profiling in Mouse Heart Sections Using In Situ Hybridization

Author

Fani, Memi, Daniela, Tirziu, and Irinna, Papangeli

Subjects

Mice, MicroRNAs, Genetics, Animals, In Situ Hybridization

Abstract

micro-RNAs (miRNAs) are single-stranded RNA transcripts that bind to messenger RNAs (mRNAs) and inhibit their translation or promote their degradation. To date, miRNAs have been implicated in a large number of biological and disease processes, which has signified the need for the reliable detection methods of miRNA transcripts. Here, we describe a detailed protocol for digoxigenin-labeled (DIG) Locked Nucleic Acid (LNA) probe-based miRNA detection, combined with protein immunostaining on mouse heart sections. First, we performed an in situ hybridization technique using the probe to identify miRNA-182 expression in heart sections from control and cardiac hypertrophy mice. Next, we performed immunostaining for cardiac Troponin T (cTnT) protein, on the same sections, to co-localize miRNA-182 with the cardiomyocyte cells. Using this protocol, we were able to detect miRNA-182 through an alkaline phosphatase based colorimetric assay, and cTnT through fluorescent staining. This protocol can be used to detect the expression of any miRNA of interest through DIG-labeled LNA probes, and relevant protein expression on mouse heart tissue sections.

Published

2018

15. Tissue-specific miRNA Expression Profiling in Mouse Heart Sections Using In Situ Hybridization

Author

Irinna Papangeli, Fani Memi, and Daniela Tirziu

Subjects

0301 basic medicine, General Immunology and Microbiology, Chemistry, General Chemical Engineering, General Neuroscience, RNA, In situ hybridization, Molecular biology, General Biochemistry, Genetics and Molecular Biology, Gene expression profiling, 03 medical and health sciences, 030104 developmental biology, Troponin complex, Dig, microRNA, Locked nucleic acid, Immunostaining

Abstract

micro-RNAs (miRNAs) are single-stranded RNA transcripts that bind to messenger RNAs (mRNAs) and inhibit their translation or promote their degradation. To date, miRNAs have been implicated in a large number of biological and disease processes, which has signified the need for the reliable detection methods of miRNA transcripts. Here, we describe a detailed protocol for digoxigenin-labeled (DIG) Locked Nucleic Acid (LNA) probe-based miRNA detection, combined with protein immunostaining on mouse heart sections. First, we performed an in situ hybridization technique using the probe to identify miRNA-182 expression in heart sections from control and cardiac hypertrophy mice. Next, we performed immunostaining for cardiac Troponin T (cTnT) protein, on the same sections, to co-localize miRNA-182 with the cardiomyocyte cells. Using this protocol, we were able to detect miRNA-182 through an alkaline phosphatase based colorimetric assay, and cTnT through fluorescent staining. This protocol can be used to detect the expression of any miRNA of interest through DIG-labeled LNA probes, and relevant protein expression on mouse heart tissue sections.

Published

2018

16. Restoration of Impaired Endothelial Myocyte Enhancer Factor 2 Function Rescues Pulmonary Arterial Hypertension

Author

Suzy A. A. Comhair, Jongmin Kim, Devi Mehrotra, Hyekyung Ju, Serpil C. Erzurum, Hyung J. Chun, Yujung Kang, Hyekyung Park, Danielle L. McLean, Cheol Hwangbo, Xiaoyue Hu, and Irinna Papangeli

Subjects

Regulation of gene expression, Mef2, medicine.medical_specialty, business.industry, Hemodynamics, Hypoxia (medical), medicine.disease, Pulmonary hypertension, Pathogenesis, Physiology (medical), medicine.artery, Internal medicine, Pulmonary artery, cardiovascular system, Cancer research, Cardiology, Medicine, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Transcription factor

Abstract

Background— Pulmonary arterial hypertension (PAH) is a progressive disease of the pulmonary arterioles, characterized by increased pulmonary arterial pressure and right ventricular failure. The cause of PAH is complex, but aberrant proliferation of the pulmonary artery endothelial cells (PAECs) and pulmonary artery smooth muscle cells is thought to play an important role in its pathogenesis. Understanding the mechanisms of transcriptional gene regulation involved in pulmonary vascular homeostasis can provide key insights into potential therapeutic strategies. Methods and Results— We demonstrate that the activity of the transcription factor myocyte enhancer factor 2 (MEF2) is significantly impaired in the PAECs derived from subjects with PAH. We identified MEF2 as the key cis-acting factor that regulates expression of a number of transcriptional targets involved in pulmonary vascular homeostasis, including microRNAs 424 and 503, connexins 37, and 40, and Krűppel Like Factors 2 and 4, which were found to be significantly decreased in PAH PAECs. The impaired MEF2 activity in PAH PAECs was mediated by excess nuclear accumulation of 2 class IIa histone deacetylases (HDACs) that inhibit its function, namely HDAC4 and HDAC5. Selective, pharmacological inhibition of class IIa HDACs led to restoration of MEF2 activity in PAECs, as demonstrated by increased expression of its transcriptional targets, decreased cell migration and proliferation, and rescue of experimental pulmonary hypertension models. Conclusions— Our results demonstrate that strategies to augment MEF2 activity hold potential therapeutic value in PAH. Moreover, we identify selective HDAC IIa inhibition as a viable alternative approach to avoid the potential adverse effects of broad spectrum HDAC inhibition in PAH.

Published

2015

17. Endothelial APLNR regulates tissue fatty acid uptake and is essential for apelin’s glucose-lowering effects

Author

Ming O. Li, Takaomi Adachi, Thomas Quertermous, Guoliang Cui, Hyekyung Ju, Alan R. Morrison, Gwang-woong Go, Lina Zhao, Kristy Red-Horse, Mohammed Inayathullah, Bikram Sharma, Jayakumar Rajadas, Stephanie L. Kwei, Judith K. Job, Hyung J. Chun, Jingxia Wu, Arya Mani, Cheol Hwangbo, Irinna Papangeli, and Saejeong Park

Subjects

Male, 0301 basic medicine, Aging, medicine.medical_specialty, Adipose tissue, FOXO1, Type 2 diabetes, 030204 cardiovascular system & hematology, Carbohydrate metabolism, Biology, Fatty Acid-Binding Proteins, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Human Umbilical Vein Endothelial Cells, medicine, Animals, Humans, Endothelium, Receptor, Mice, Knockout, Apelin Receptors, Forkhead Box Protein O1, Fatty Acids, Skeletal muscle, General Medicine, medicine.disease, Apelin, Glucose, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Signal transduction, Signal Transduction

Abstract

Treatment of type 2 diabetes mellitus continues to pose an important clinical challenge, with most existing therapies lacking demonstrable ability to improve cardiovascular outcomes. The atheroprotective peptide apelin (APLN) enhances glucose utilization and improves insulin sensitivity. However, the mechanism of these effects remains poorly defined. We demonstrate that the expression of APLNR (APJ/AGTRL1), the only known receptor for apelin, is predominantly restricted to the endothelial cells (ECs) of multiple adult metabolic organs, including skeletal muscle and adipose tissue. Conditional endothelial-specific deletion of Aplnr (AplnrECKO) resulted in markedly impaired glucose utilization and abrogation of apelin-induced glucose lowering. Furthermore, we identified in-activation of Forkhead box protein O1 (FOXO1) and inhibition of endothelial expression of fatty acid (FA) binding protein 4 (FABP4) as key downstream signaling targets of apelin/APLNR signaling. Both the Apln−/− and AplnrECKO mice demonstrated increased endothelial FABP4 expression and excess tissue FA accumulation, whereas concurrent endothelial Foxo1 deletion or pharmacologic FABP4 inhibition rescued the excess FA accumulation phenotype of the Apln−/− mice. The impaired glucose utilization in the AplnrECKO mice was associated with excess FA accumulation in the skeletal muscle. Treatment of these mice with an FABP4 inhibitor abrogated these metabolic phenotypes. These findings provide mechanistic insights that could greatly expand the therapeutic repertoire for type 2 diabetes and related metabolic disorders.

Published

2017

18. Essential Role of Apelin Signaling During Lymphatic Development in Zebrafish

Author

Suk-Won Jin, Emily R. Nadelmann, Hyekyung Park, Jongmin Kim, Stanley G. Rockson, Yujung Kang, Irinna Papangeli, Hyung J. Chun, Hyeseon Kang, Jingxia Wu, and Jun Dae Kim

Subjects

Time Factors, Mitogen-Activated Protein Kinase 3, government.form_of_government, Vascular Endothelial Growth Factor C, Biology, Transfection, Article, Receptors, G-Protein-Coupled, Thoracic Duct, Animals, Humans, Lymphangiogenesis, Phosphorylation, Protein kinase B, Cells, Cultured, Zebrafish, Mitogen-Activated Protein Kinase 1, Apelin Receptors, Endothelial Cells, Zebrafish Proteins, Vascular Endothelial Growth Factor Receptor-3, Apelin, Lymphatic Endothelium, Vascular endothelial growth factor C, Protein kinase B signaling, Cancer research, government, Intercellular Signaling Peptides and Proteins, RNA Interference, Chemokines, Endothelium, Lymphatic, Signal transduction, Cardiology and Cardiovascular Medicine, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

Objective— Apelin and its cognate receptor Aplnr/Apj are essential for diverse biological processes. However, the function of Apelin signaling in lymphatic development remains to be identified, despite the preferential expression of Apelin and Aplnr within developing blood and lymphatic endothelial cells in vertebrates. In this report, we aim to delineate the functions of Apelin signaling during lymphatic development. Approach and Results— We investigated the functions of Apelin signaling during lymphatic development using zebrafish embryos and found that attenuation of Apelin signaling substantially decreased the formation of the parachordal vessel and the number of lymphatic endothelial cells within the developing thoracic duct, indicating an essential role of Apelin signaling during the early phase of lymphatic development. Mechanistically, we found that abrogation of Apelin signaling selectively attenuates lymphatic endothelial serine–threonine kinase Akt 1/2 phosphorylation without affecting the phosphorylation status of extracellular signal–regulated kinase 1/2. Moreover, lymphatic abnormalities caused by the reduction of Apelin signaling were significantly exacerbated by the concomitant partial inhibition of serine–threonine kinase Akt/protein kinase B signaling. Apelin and vascular endothelial growth factor-C (VEGF-C) signaling provide a nonredundant activation of serine–threonine kinase Akt/protein kinase B during lymphatic development because overexpression of VEGF-C or apelin was unable to rescue the lymphatic defects caused by the lack of Apelin or VEGF-C, respectively. Conclusions— Taken together, our data present compelling evidence suggesting that Apelin signaling regulates lymphatic development by promoting serine–threonine kinase Akt/protein kinase B activity in a VEGF-C/VEGF receptor 3–independent manner during zebrafish embryogenesis.

Published

2014

19. Tbx1 Genetically Interacts With the Transforming Growth Factor-beta/Bone Morphogenetic Protein Inhibitor Smad7 During Great Vessel Remodeling

Author

Irinna Papangeli and Peter J. Scambler

Subjects

TBX1, Aortic arch, Heterozygote, Pathology, medicine.medical_specialty, Vascular smooth muscle, Physiology, Gestational Age, Mice, Transgenic, Haploinsufficiency, Regulatory Sequences, Nucleic Acid, Biology, Muscle, Smooth, Vascular, Smad7 Protein, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Transforming Growth Factor beta, medicine.artery, DiGeorge syndrome, DiGeorge Syndrome, Morphogenesis, medicine, Animals, Cell Lineage, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Binding Sites, Gene Expression Regulation, Developmental, Cell Differentiation, Arteries, Anatomy, medicine.disease, Fibronectins, Mice, Inbred C57BL, Branchial Region, Phenotype, medicine.anatomical_structure, Great vessels, Bone Morphogenetic Proteins, T-Box Domain Proteins, Cardiology and Cardiovascular Medicine, 030217 neurology & neurosurgery, Pharyngeal arch, Signal Transduction, Artery

Abstract

Rationale: Growth and remodeling of the pharyngeal arch arteries are vital for the development of a mature great vessel system. Dysmorphogenesis of the fourth arch arteries can result in interruption of the aortic arch type B, typically found in DiGeorge syndrome. Tbx1 haploinsufficient embryos, which model DiGeorge syndrome, display fourth arch artery defects during formation of the vessels. Recovery from such defects is a documented yet unexplained phenotype in Tbx1 haploinsufficiency. Objective: To understand the nature of fourth arch artery growth recovery in Tbx1 haploinsufficiency and its underlying genetic control. Methods and Results: We categorized vessel phenotypes of Tbx1 heterozygotes as hypoplastic or aplastic at the conclusion of pharyngeal artery formation and compared these against the frequency of vessel defects scored at the end of great vessel development. The frequency of hypoplastic vessels decreased during embryogenesis, whereas no reduction of vessel aplasia was seen, implying recovery is attributable to remodeling of hypoplastic vessels. We showed that Smad7 , an inhibitory Smad within the transforming growth factor-β pathway, is regulated by Tbx1, is required for arch artery remodeling, and genetically interacts with Tbx1 in this process. Tbx1 and Tbx1 ; Smad7 haploinsufficiency affected several remodeling processes; however, concurrent haploinsufficiency particularly impacted on the earliest stage of vascular smooth muscle cell vessel coverage and subsequent fibronectin deposition. Conditional reconstitution of Smad7 with a Tbx1Cre driver indicated that the interaction between the 2 genes is cell autonomous. Conclusions: Tbx1 acts upstream of Smad7 controlling vascular smooth muscle and extracellular matrix investment of the fourth arch artery.

Published

2013

20. FGF Signaling in Pulmonary Hypertension

Author

Irinna Papangeli and Hyung J. Chun

Subjects

medicine.medical_specialty, Endocrinology, business.industry, Internal medicine, Medicine, business, Fibroblast growth factor, medicine.disease, Pulmonary hypertension

Published

2016

21. miR-182 Modulates Myocardial Hypertrophic Response Induced by Angiogenesis in Heart

Author

Daniela Tirziu, Nicole Mikush, Hyung J. Chun, Na Li, Irina M. Jaba, Jinah Han, Lawrence H. Young, Cheol Hwangbo, Bruno Larrivée, Irinna Papangeli, Anne Eichmann, and Jiasheng Zhang

Subjects

0301 basic medicine, Placental growth factor, Nitric Oxide Synthase Type III, Angiogenesis, Cardiomegaly, mTORC1, Mechanistic Target of Rapamycin Complex 1, Nitric Oxide, Article, Muscle hypertrophy, Neovascularization, 03 medical and health sciences, Mice, Medicine, Animals, Myocytes, Cardiac, Endothelium, Protein kinase B, Pressure overload, Mice, Knockout, Multidisciplinary, Neovascularization, Pathologic, business.industry, TOR Serine-Threonine Kinases, Membrane Proteins, Proteins, Up-Regulation, MicroRNAs, 030104 developmental biology, Multiprotein Complexes, Immunology, FOXO3, Cancer research, medicine.symptom, business, Proto-Oncogene Proteins c-akt, RGS Proteins

Abstract

Myocardial hypertrophy is an adaptive response to hemodynamic demands. Although angiogenesis is critical to support the increase in heart mass with matching blood supply, it may also promote a hypertrophic response. Previously, we showed that cardiac angiogenesis induced by placental growth factor (PlGF), promotes myocardial hypertrophy through the paracrine action of endothelium-derived NO, which triggers the degradation of regulator of G protein signaling 4 (RGS4) to activate the Akt/mTORC1 pathways in cardiomyocytes. Here, we investigated whether miRNAs contribute to the development of hypertrophic response associated with myocardial angiogenesis. We show that miR-182 is upregulated concurrently with the development of hypertrophy in PlGF mice, but not when hypertrophy was blocked by concomitant expression of PlGF and RGS4, or by PlGF expression in eNOS−/− mice. Anti-miR-182 treatment inhibits the hypertrophic response and prevents the Akt/mTORC1 activation in PlGF mice and NO-treated cardiomyocytes. miR-182 reduces the expression of Bcat2, Foxo3 and Adcy6 to regulate the hypertrophic response in PlGF mice. Particularly, depletion of Bcat2, identified as a new miR-182 target, promotes AktSer473/p70-S6KThr389 phosphorylation and cardiomyocyte hypertrophy. LV pressure overload did not upregulate miR-182. Thus, miR-182 is a novel target of endothelial-cardiomyocyte crosstalk and plays an important role in the angiogenesis induced-hypertrophic response.

Published

2016

22. The 22q11 deletion: DiGeorge and velocardiofacial syndromes and the role ofTBX1

Author

Irinna Papangeli and Peter J. Scambler

Subjects

TBX1, Genetics, Cellular differentiation, Neural crest, Cell Biology, Biology, medicine.disease, Fibroblast growth factor, 22q11 Deletion Syndrome, DiGeorge syndrome, embryonic structures, medicine, Haploinsufficiency, Molecular Biology, Developmental biology, Developmental Biology

Abstract

Hemizygous deletion of 22q11 affects approximately 1:4000 live births and may give rise to many different malformations but classically results in a constellation of phenotypes that receive a diagnosis of DiGeorge syndrome or velocardiofacial syndrome. Particularly affected are the heart and great vessels, the endocrine glands of the neck, the face, the soft palate, and cognitive development. Although up to 50 genes may be deleted, it is haploinsufficiency of the transcription factor TBX1 that is thought to make the greatest contribution to the disorder. Mouse embryos are exquisitely sensitive to varying levels of Tbx1 mRNA, and Tbx1 is required in all three germ layers of the embryonic pharyngeal region for normal development. TBX1 controls cell proliferation and affects cellular differentiation in a cell autonomous fashion, but it also directs non-cell autonomous effects, most notably in the signaling between pharyngeal surface ectoderm and the rostral neural crest. TBX1 interacts with several signaling pathways, including fibroblast growth factor, retinoic acid, CTNNB1 (formerly known as β-catenin), and bone morphogenetic protein (BMP), and may regulate pathways by both DNA-binding and non-binding activity. In addition to the structural abnormalities seen in 22q11 deletion syndrome (DS) and Tbx1 mutant mouse models, patients reaching adolescence and adulthood have a predisposition to psychiatric illness. Whether this has a developmental basis and, if so, which genes are involved is an ongoing strand of research. Thus, knowledge of the genetic and developmental mechanisms underlying 22q11DS has the potential to inform about common disease as well as developmental defect.

Published

2012

23. A Tale of Two Elabela Null Mice

Author

Irinna Papangeli and Hyung J. Chun

Subjects

0301 basic medicine, Null mice, medicine.medical_specialty, Peptide Hormones, Placenta, Endocrinology, Diabetes and Metabolism, Cardiovascular Abnormalities, Neovascularization, Physiologic, Biology, Peptide hormone, Article, Mice, 03 medical and health sciences, Endocrinology, Pre-Eclampsia, Pregnancy, Internal medicine, medicine, Animals, Birth Weight, Peptide ligand, Apelin receptor, G protein-coupled receptor, Mice, Knockout, Embryogenesis, Phenotype, Placentation, Proteinuria, 030104 developmental biology, medicine.anatomical_structure, embryonic structures, Apelin, Female, Endoderm, Carrier Proteins, Placental Hormones, Signal Transduction

Abstract

Preeclampsia (PE) is a gestational hypertensive syndrome affecting between 5 and 8% of all pregnancies. Although PE is the leading cause of fetal and maternal morbidity and mortality, its molecular etiology is still unclear. Here, we show that ELABELA (ELA), an endogenous ligand of the apelin receptor (APLNR, or APJ), is a circulating hormone secreted by the placenta.

Published

2017

24. Abstract 12518: MicroRNA 139-5p Coordinates APLNR-CXCR4 Crosstalk During Vascular Maturation

Author

Jongmin Kim, Arndt F. Siekmann, Aram Lee, Yoko Kojima, Keiichiro Tanaka, Irinna Papangeli, Inna Maier, Yujung Kang, Hyekyung Ju, and Hyung J. Chun

Subjects

Sprouting angiogenesis, Crosstalk (biology), business.industry, Angiogenesis, Physiology (medical), microRNA, Medicine, Cardiology and Cardiovascular Medicine, business, CXCR4, Sprouting, Apelin, Cell biology

Abstract

Rationale: Sprouting angiogenesis is governed by the concept of tip/stalk cells that guides our understanding of the transition from vascular sprouting to maturation and ultimately quiescence. The VEGF and Notch signaling pathways have been extensively described in regulating the discrimination between these two cell populations. However, several additional tip and stalk cell specific genes have been identified. To date, unresolved questions remain, and our understanding of the mechanisms by which these signaling processes are integrated is incomplete. Objective: We set out to investigate novel mechanisms by which signaling pathways involving two G protein coupled receptors (GPCRs), expressed in a mutually exclusive fashion in the tip/stalk cell populations, are intricately linked in vascular development. Methods/Results: Using a combination of in vivo and in vitro techniques, we demonstrate the critical role of crosstalk between APLNR and CXCR4 in vascular maturation. We show robust flow induced expression of the stalk cell specific APLNR, that leads to marked suppression of CXCR4 expression, a mechanism to achieve tip cell restricted expression of the latter. Retinas from Apln (ligand), Aplnr (receptor) and endothelial specific Aplnr deleted mice show retarded vascular expansion, reduced vascularized area and fewer vascular branch points. These phenotypes are in part due to increased expression of Cxcr4 in Apln-/- and Aplnr-/- retinal vessels as Cxcr4 inhibition through a selective inhibitor can ameliorate the Aplnr phenotype. The crosstalk between the two GPCRs was found to involve a key shear responsive microRNA, miR-139-5p, which is upregulated by APLN/APLNR signaling and directly targets CXCR4 in endothelial cells. In accordance, Apln-/- and Aplnr-/- retinal endothelial cells showed depleted levels of miR-139-5p. Lastly, we demonstrate that atorvastatin, an HMG-CoA reductase inhibitor shown to enhance APLNR signaling, can induce miR-139-5p expression and rescue the vascular phenotypes associated with APLN/APLNR deficiency. Conclusions: These findings provide key mechanistic insights into a critical microRNA based crosstalk between two GPCR signaling cascades, which regulates important steps in vascular maturation.

Published

2015

25. Letter to the Editors regarding: 'The ERG-APLNR Axis Controls Pulmonary Venule Endothelial Proliferation in Pulmonary Veno-Occlusive Disease' by Lathen, et.al: Papangeli, Pulmonary Arteriolar Endothelium Express Aplnr

Author

Hyung J. Chun, Irinna Papangeli, and Bikram Sharma

Subjects

Male, Oncogene Proteins, Pathology, medicine.medical_specialty, Endothelial proliferation, Venule, business.industry, Disease, Article, Apelin, Receptors, G-Protein-Coupled, Physiology (medical), medicine, Trans-Activators, Animals, Humans, Pulmonary Veno-Occlusive Disease, Female, Cardiology and Cardiovascular Medicine, business, Erg, Transcription Factors

Abstract

We have read with great interest the article by Lathen and colleagues titled “The ERG–APLNR Axis Controls Pulmonary Venule Endothelial Proliferation in Pulmonary Veno-Occlusive Disease,” and congratulate the authors for their thorough approach using human samples and modern genetic techniques.1 However, there are 2 key points that, in our opinion, deserve attention. First, following a literature review, the authors conclude that “These studies point to the concept that Aplnr signaling has direct and unique effects on the venous circulation.” However, the majority of the cited studies do not describe venous-specific mechanisms. Cheng et al2 demonstrated that apelin administration decreased both the mean arterial …

Published

2015

26. Endothelium as a gatekeeper of fatty acid transport

Author

Irinna Papangeli, Hyung J. Chun, Jingxia Wu, and Devi Mehrotra

Subjects

Vascular Endothelial Growth Factor B, Endothelium, Endocrinology, Diabetes and Metabolism, Adipose Tissue, White, Peroxisome proliferator-activated receptor, Biology, Article, Endocrinology, medicine, Diabetes Mellitus, Animals, Humans, Obesity, chemistry.chemical_classification, Fatty Acids, Fatty acid, Biological Transport, Peroxisome, Cell biology, Apelin, Vascular endothelial growth factor B, PPAR gamma, medicine.anatomical_structure, chemistry, Biochemistry, Intercellular Signaling Peptides and Proteins, Signal transduction, Insulin Resistance, Energy source, Signal Transduction

Abstract

The endothelium transcends all clinical disciplines and is key to the function of every organ system. A crucial, but poorly understood role of the endothelium is its ability to control the transport of energy supply according to organ needs. Fatty acids (FAs) in particular represent a key energy source that is utilized by a number of tissues, but whose utilization must be tightly regulated to avoid potentially deleterious consequences of excess accumulation, including insulin resistance. Recent studies have identified key endothelial signaling mechanisms involving vascular endothelial growth factor B, peroxisome proliferator-activated receptor-γ, and the peptide ligand apelin, that are critical to endothelial regulation of FA transport. Here we discuss the mechanisms by which these signaling pathways regulate this key endothelial function.

Published

2013

27. The 22q11 deletion: DiGeorge and velocardiofacial syndromes and the role of TBX1

Author

Irinna, Papangeli and Peter, Scambler

Subjects

Fibroblast Growth Factors, 22q11 Deletion Syndrome, Bone Morphogenetic Proteins, Mutation, DiGeorge Syndrome, Animals, Humans, Tretinoin, RNA, Messenger, T-Box Domain Proteins, Gene Deletion, beta Catenin, Signal Transduction

Abstract

Hemizygous deletion of 22q11 affects approximately 1:4000 live births and may give rise to many different malformations but classically results in a constellation of phenotypes that receive a diagnosis of DiGeorge syndrome or velocardiofacial syndrome. Particularly affected are the heart and great vessels, the endocrine glands of the neck, the face, the soft palate, and cognitive development. Although up to 50 genes may be deleted, it is haploinsufficiency of the transcription factor TBX1 that is thought to make the greatest contribution to the disorder. Mouse embryos are exquisitely sensitive to varying levels of Tbx1 mRNA, and Tbx1 is required in all three germ layers of the embryonic pharyngeal region for normal development. TBX1 controls cell proliferation and affects cellular differentiation in a cell autonomous fashion, but it also directs non-cell autonomous effects, most notably in the signaling between pharyngeal surface ectoderm and the rostral neural crest. TBX1 interacts with several signaling pathways, including fibroblast growth factor, retinoic acid, CTNNB1 (formerly known as β-catenin), and bone morphogenetic protein (BMP), and may regulate pathways by both DNA-binding and non-binding activity. In addition to the structural abnormalities seen in 22q11 deletion syndrome (DS) and Tbx1 mutant mouse models, patients reaching adolescence and adulthood have a predisposition to psychiatric illness. Whether this has a developmental basis and, if so, which genes are involved is an ongoing strand of research. Thus, knowledge of the genetic and developmental mechanisms underlying 22q11DS has the potential to inform about common disease as well as developmental defect.

Published

2013

28. Hes1 expression is reduced in Tbx1 null cells and is required for the development of structures affected in 22q11 deletion syndrome

Author

Peter J. Scambler, Amelie Calmont, Francesca Rochais, Shoumo Bhattacharya, Kerra Pearce, Robert G. Kelly, Kelly Lammerts van Bueren, Irinna Papangeli, Catherine Roberts, Dorota Szumska, Institut de Biologie du Développement de Marseille (IBDM), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS), North Carolina State University, Center for High Performance Simulation and Department of Chemical and Biomolecular Engineering, North Carolina State University [Raleigh] (NC State), and University of North Carolina System (UNC)

Subjects

Mouse, Microarray, Mice, 0302 clinical medicine, Null cell, Basic Helix-Loop-Helix Transcription Factors, Basic Helix-Loop-Helix Transcription Factors/genetics/*metabolism, HES1, ComputingMilieux_MISCELLANEOUS, In Situ Hybridization, Sequence Deletion, Mice, Knockout, 0303 health sciences, Tbx1, Heart, Syndrome, Mammalian/metabolism, Thymus Gland/*embryology/metabolism, Cell biology, Thymus, medicine.anatomical_structure, Embryo, embryonic structures, Haploinsufficiency, TBX1, medicine.medical_specialty, Knockout, FACS, Pharyngeal arch artery, Thymus Gland, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, Article, Chromosomes, 03 medical and health sciences, Heart/*embryology, 22q11 Deletion Syndrome, stomatognathic system, Internal medicine, Pharyngeal apparatus, medicine, Homeodomain Proteins/genetics/*metabolism, Animals, beta-Galactosidase/genetics/metabolism, Molecular Biology, 030304 developmental biology, T-Box Domain Proteins/genetics/metabolism, Phenocopy, Homeodomain Proteins, Chromosomes/genetics, Cell Biology, Embryo, Mammalian, beta-Galactosidase, 22q11, Hes1, Endocrinology, Branchial Region, Transcription Factor HES-1, Branchial Region/*embryology/metabolism, T-Box Domain Proteins, 030217 neurology & neurosurgery, Pharyngeal arch, Developmental Biology

Abstract

22q11 deletion syndrome (22q11DS) is characterised by aberrant development of the pharyngeal apparatus and the heart with haploinsufficiency of the transcription factor TBX1 being considered the major underlying cause of the disease. Tbx1 mutations in mouse phenocopy the disorder. In order to identify the transcriptional dysregulation in Tbx1-expressing lineages we optimised fluorescent-activated cell sorting of beta-galactosidase expressing cells (FACS-Gal) to compare the expression profile of Df1/Tbx1(lacZ) (effectively Tbx1 null) and Tbx1 heterozygous cells isolated from mouse embryos. Hes1, a major effector of Notch signalling, was identified as downregulated in Tbx1(-)(/)(-) mutants. Hes1 mutant mice exhibited a partially penetrant range of 22q11DS-like defects including pharyngeal arch artery (PAA), outflow tract, craniofacial and thymic abnormalities. Similar to Tbx1 mice, conditional mutagenesis revealed that Hes1 expression in embryonic pharyngeal ectoderm contributes to thymus and pharyngeal arch artery development. These results suggest that Hes1 acts downstream of Tbx1 in the morphogenesis of pharyngeal-derived structures.

Published

2010

29. 06-P036 Dissecting the embryonic requirement of the Notch pathway gene, Hes1, in the context of DiGeorge syndrome

Author

Kerra Pearce, Irinna Papangeli, Catherine Roberts, Kelly Lammerts van Bueren, Dorota Szumska, Shoumo Bhattacharya, and Peter J. Scambler

Subjects

Embryology, DiGeorge syndrome, medicine, Notch signaling pathway, Context (language use), Biology, HES1, medicine.disease, Embryonic stem cell, Gene, Cell biology, Developmental Biology

Published

2009

30. Tbx1 controls cardiac neural crest cell migration during arch artery development by regulating Gbx2 expression in the pharyngeal ectoderm

Author

William Andrews, Elizabeth Illingworth, Kelly Lammerts van Bueren, M. Albert Basson, Vanessa Kyriakopoulou, Amelie Calmont, James F. Martin, Sarah Ivins, Irinna Papangeli, Peter J. Scambler, and Anne M. Moon

Subjects

TBX1, Ectoderm, Nerve Tissue Proteins, Biology, Mice, Cell Movement, medicine, Animals, Sonic hedgehog, Receptors, Immunologic, GBX2, Molecular Biology, Body Patterning, Glycoproteins, Homeodomain Proteins, Mice, Knockout, Cardiac neural crest cells, Neural crest, Heart, Arteries, biochemical phenomena, metabolism, and nutrition, Embryo, Mammalian, Surface ectoderm, Cell biology, medicine.anatomical_structure, Branchial Region, Neural Crest, Immunology, embryonic structures, biology.protein, Development and Disease, T-Box Domain Proteins, Pharyngeal arch, Developmental Biology, Signal Transduction

Abstract

Elucidating the gene regulatory networks that govern pharyngeal arch artery (PAA) development is an important goal, as such knowledge can help to identify new genes involved in cardiovascular disease. The transcription factor Tbx1 plays a vital role in PAA development and is a major contributor to cardiovascular disease associated with DiGeorge syndrome. In this report, we used various genetic approaches to reveal part of a signalling network by which Tbx1 controls PAA development in mice. We investigated the crucial role played by the homeobox-containing transcription factor Gbx2 downstream of Tbx1. We found that PAA formation requires the pharyngeal surface ectoderm as a key signalling centre from which Gbx2, in response to Tbx1, triggers essential directional cues to the adjacent cardiac neural crest cells (cNCCs) en route to the caudal PAAs. Abrogation of this signal generates cNCC patterning defects leading to PAA abnormalities. Finally, we showed that the Slit/Robo signalling pathway is activated during cNCC migration and that components of this pathway are affected in Gbx2 and Tbx1 mutant embryos at the time of PAA development. We propose that the spatiotemporal control of this tightly orchestrated network of genes participates in crucial aspects of PAA development.

Published

2009

31. 13-P005 Tbx1 controls cardiac neural crest cell migration during arch artery development by regulating Gbx2 expression in the pharyngeal ectoderm

Author

Amelie Calmont, Sarah Ivins, Kelly Lammerts Van Bueren, Irinna Papangeli, Vanessa Kyriakopoulou, William Andrews, James Martin, Anne Moon, Elizabeth Illingworth, Albert Basson, and Peter Scambler

Subjects

Embryology, Developmental Biology

Published

2009