Your search keyword '"Karl B, Shpargel"' showing total 29 results

1. UTX promotes CD8+ T cell-mediated antiviral defenses but reduces T cell durability

Author

Joseph E. Mitchell, Makayla M. Lund, Josh Starmer, Kai Ge, Terry Magnuson, Karl B. Shpargel, and Jason K. Whitmire

Subjects

epigenetics, histone demethylation, CD8+ T cell function, persistent infection, antiviral defense, LCMV, Biology (General), QH301-705.5

Abstract

Summary: Persistent virus infections can cause pathogenesis that is debilitating or lethal. During these infections, virus-specific T cells fail to protect due to weakened antiviral activity or failure to persist. These outcomes are governed by histone modifications, although it is unknown which enzymes contribute to T cell loss or impaired function over time. In this study, we show that T cell receptor-stimulated CD8+ T cells increase their expression of UTX (ubiquitously transcribed tetratricopeptide repeat, X chromosome) to enhance gene expression. During chronic lymphocytic choriomeningitis virus (LCMV) infection in mice, UTX binds to enhancers and transcription start sites of effector genes, allowing for improved cytotoxic T lymphocyte (CTL)-mediated protection, independent of its trimethylation of histone 3 lysine 27 (H3K27me3) demethylase activity. UTX also limits the frequency and durability of virus-specific CD8+ T cells, which correspond to increased expression of inhibitory receptors. Thus, UTX guides gene expression patterns in CD8+ T cells, advancing early antiviral defenses while reducing the longevity of CD8+ T cell responses.

Published

2021

2. KDM6 demethylase independent loss of histone H3 lysine 27 trimethylation during early embryonic development.

Author

Karl B Shpargel, Joshua Starmer, Della Yee, Michael Pohlers, and Terry Magnuson

Subjects

Genetics, QH426-470

Abstract

The early mammalian embryo utilizes histone H3 lysine 27 trimethylation (H3K27me3) to maintain essential developmental genes in a repressive chromatin state. As differentiation progresses, H3K27me3 is removed in a distinct fashion to activate lineage specific patterns of developmental gene expression. These rapid changes in early embryonic chromatin environment are thought to be dependent on H3K27 demethylases. We have taken a mouse genetics approach to remove activity of both H3K27 demethylases of the Kdm6 gene family, Utx (Kdm6a, X-linked gene) and Jmjd3 (Kdm6b, autosomal gene). Male embryos null for active H3K27 demethylation by the Kdm6 gene family survive to term. At mid-gestation, embryos demonstrate proper patterning and activation of Hox genes. These male embryos retain the Y-chromosome UTX homolog, UTY, which cannot demethylate H3K27me3 due to mutations in catalytic site of the Jumonji-C domain. Embryonic stem (ES) cells lacking all enzymatic KDM6 demethylation exhibit a typical decrease in global H3K27me3 levels with differentiation. Retinoic acid differentiations of these ES cells demonstrate loss of H3K27me3 and gain of H3K4me3 to Hox promoters and other transcription factors, and induce expression similar to control cells. A small subset of genes exhibit decreased expression associated with reduction of promoter H3K4me3 and some low-level accumulation of H3K27me3. Finally, Utx and Jmjd3 mutant mouse embryonic fibroblasts (MEFs) demonstrate dramatic loss of H3K27me3 from promoters of several Hox genes and transcription factors. Our results indicate that early embryonic H3K27me3 repression can be alleviated in the absence of active demethylation by the Kdm6 gene family.

Published

2014

3. UTX promotes CD8+ T cell-mediated antiviral defenses but reduces T cell durability

Author

Jason K. Whitmire, Kai Ge, Terry Magnuson, Joseph E. Mitchell, Karl B. Shpargel, Josh Starmer, and Makayla M. Lund

Subjects

0301 basic medicine, QH301-705.5, T cell, Biology, Lymphocytic choriomeningitis, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Histone demethylation, Demethylase activity, medicine, Cytotoxic T cell, Biology (General), LCMV, CD8+ T cell function, persistent infection, epigenetics, histone demethylation, Effector, medicine.disease, Cell biology, 030104 developmental biology, Histone, medicine.anatomical_structure, biology.protein, antiviral defense, 030217 neurology & neurosurgery, CD8

Abstract

Summary Persistent virus infections can cause pathogenesis that is debilitating or lethal. During these infections, virus-specific T cells fail to protect due to weakened antiviral activity or failure to persist. These outcomes are governed by histone modifications, although it is unknown which enzymes contribute to T cell loss or impaired function over time. In this study, we show that T cell receptor-stimulated CD8+ T cells increase their expression of UTX (ubiquitously transcribed tetratricopeptide repeat, X chromosome) to enhance gene expression. During chronic lymphocytic choriomeningitis virus (LCMV) infection in mice, UTX binds to enhancers and transcription start sites of effector genes, allowing for improved cytotoxic T lymphocyte (CTL)-mediated protection, independent of its trimethylation of histone 3 lysine 27 (H3K27me3) demethylase activity. UTX also limits the frequency and durability of virus-specific CD8+ T cells, which correspond to increased expression of inhibitory receptors. Thus, UTX guides gene expression patterns in CD8+ T cells, advancing early antiviral defenses while reducing the longevity of CD8+ T cell responses.

Published

2021

4. UTX promotes CD8

Author

Joseph E, Mitchell, Makayla M, Lund, Josh, Starmer, Kai, Ge, Terry, Magnuson, Karl B, Shpargel, and Jason K, Whitmire

Subjects

Cytotoxicity, Immunologic, Histone Demethylases, Gene Expression Profiling, Programmed Cell Death 1 Receptor, Lymphocytic Choriomeningitis, Viral Load, Lymphocyte Activation Gene 3 Protein, Article, Histones, Mice, Inbred C57BL, Mice, Gene Expression Regulation, Antigens, CD, Host-Pathogen Interactions, Animals, Lymphocytic choriomeningitis virus, Hepatitis A Virus Cellular Receptor 2, Immunologic Memory, Signal Transduction, T-Lymphocytes, Cytotoxic

Abstract

SUMMARY Persistent virus infections can cause pathogenesis that is debilitating or lethal. During these infections, virus-specific T cells fail to protect due to weakened antiviral activity or failure to persist. These outcomes are governed by histone modifications, although it is unknown which enzymes contribute to T cell loss or impaired function over time. In this study, we show that T cell receptor-stimulated CD8+ T cells increase their expression of UTX (ubiquitously transcribed tetratricopeptide repeat, X chromosome) to enhance gene expression. During chronic lymphocytic choriomeningitis virus (LCMV) infection in mice, UTX binds to enhancers and transcription start sites of effector genes, allowing for improved cytotoxic T lymphocyte (CTL)-mediated protection, independent of its trimethylation of histone 3 lysine 27 (H3K27me3) demethylase activity. UTX also limits the frequency and durability of virus-specific CD8+ T cells, which correspond to increased expression of inhibitory receptors. Thus, UTX guides gene expression patterns in CD8+ T cells, advancing early antiviral defenses while reducing the longevity of CD8+ T cell responses., Graphical abstract, In brief T cells fail to eliminate chronic virus infections due to alterations in gene expression that undermine their activity. In this study, Mitchell et al. identify a histone-modifying enzyme that promotes effector gene expression and CTL activity early on yet reduces T cell survival, leading to infection persistence.

Published

2020

5. UTX and UTY demonstrate histone demethylase-independent function in mouse embryonic development.

Author

Karl B Shpargel, Toru Sengoku, Shigeyuki Yokoyama, and Terry Magnuson

Subjects

Genetics, QH426-470

Abstract

UTX (KDM6A) and UTY are homologous X and Y chromosome members of the Histone H3 Lysine 27 (H3K27) demethylase gene family. UTX can demethylate H3K27; however, in vitro assays suggest that human UTY has lost enzymatic activity due to sequence divergence. We produced mouse mutations in both Utx and Uty. Homozygous Utx mutant female embryos are mid-gestational lethal with defects in neural tube, yolk sac, and cardiac development. We demonstrate that mouse UTY is devoid of in vivo demethylase activity, so hemizygous X(Utx-) Y(+) mutant male embryos should phenocopy homozygous X(Utx-) X(Utx-) females. However, X(Utx-) Y(+) mutant male embryos develop to term; although runted, approximately 25% survive postnatally reaching adulthood. Hemizygous X(+) Y(Uty-) mutant males are viable. In contrast, compound hemizygous X(Utx-) Y(Uty-) males phenocopy homozygous X(Utx-) X(Utx-) females. Therefore, despite divergence of UTX and UTY in catalyzing H3K27 demethylation, they maintain functional redundancy during embryonic development. Our data suggest that UTX and UTY are able to regulate gene activity through demethylase independent mechanisms. We conclude that UTX H3K27 demethylation is non-essential for embryonic viability.

Published

2012

6. The histone demethylase Kdm6b regulates a mature gene expression program in differentiating cerebellar granule neurons

Author

Ranjula Wijayatunge, Fang Liu, Karl B. Shpargel, Terry Magnuson, Anne E. West, Jane Valeriane Boua, Urann Chan, and Nicole J. Wayne

Subjects

0301 basic medicine, Jumonji Domain-Containing Histone Demethylases, Cerebellum, Cellular differentiation, Gene Expression, Biology, Cytoplasmic Granules, Article, Histones, 03 medical and health sciences, Cellular and Molecular Neuroscience, Histone H3, Neurotrophic factors, Conditional gene knockout, medicine, Animals, Humans, Molecular Biology, Histone Demethylases, Neurons, Gene knockdown, Cell Biology, Cell biology, 030104 developmental biology, medicine.anatomical_structure, nervous system, Cerebellar cortex, Synapse maturation

Abstract

The histone H3 lysine 27 (H3K27) demethylase Kdm6b (Jmjd3) can promote cellular differentiation, however its physiological functions in neurons remain to be fully determined. We studied the expression and function of Kdm6b in differentiating granule neurons of the developing postnatal mouse cerebellum. At postnatal day 7, Kdm6b is expressed throughout the layers of the developing cerebellar cortex, but its expression is upregulated in newborn cerebellar granule neurons (CGNs). Atoh1-Cre mediated conditional knockout of Kdm6b in CGN precursors either alone or in combination with Kdm6a did not disturb the gross morphological development of the cerebellum. Furthermore, RNAi-mediated knockdown of Kdm6b in cultured CGN precursors did not alter the induced expression of early neuronal marker genes upon cell cycle exit. By contrast, knockdown of Kdm6b significantly impaired the induction of a mature neuronal gene expression program, which includes gene products required for functional synapse maturation. Loss of Kdm6b also impaired the ability of Brain-Derived Neurotrophic Factor (BDNF) to induce expression of Grin2c and Tiam1 in maturing CGNs. Taken together, these data reveal a previously unknown role for Kdm6b in the postmitotic stages of CGN maturation and suggest that Kdm6b may work, at least in part, by a transcriptional mechanism that promotes gene sensitivity to regulation by BDNF.

Published

2018

7. A noncoding point mutation of Zeb1 causes multiple developmental malformations and obesity in Twirler mice.

Author

Kiyoto Kurima, Ronna Hertzano, Oksana Gavrilova, Kelly Monahan, Karl B Shpargel, Garani Nadaraja, Yoshiyuki Kawashima, Kyu Yup Lee, Taku Ito, Yujiro Higashi, David J Eisenman, Scott E Strome, and Andrew J Griffith

Subjects

Genetics, QH426-470

Abstract

Heterozygous Twirler (Tw) mice develop obesity and circling behavior associated with malformations of the inner ear, whereas homozygous Tw mice have cleft palate and die shortly after birth. Zeb1 is a zinc finger protein that contributes to mesenchymal cell fate by repression of genes whose expression defines epithelial cell identity. This developmental pathway is disrupted in inner ears of Tw/Tw mice. The purpose of our study was to comprehensively characterize the Twirler phenotype and to identify the causative mutation. The Tw/+ inner ear phenotype includes irregularities of the semicircular canals, abnormal utricular otoconia, a shortened cochlear duct, and hearing loss, whereas Tw/Tw ears are severely malformed with barely recognizable anatomy. Tw/+ mice have obesity associated with insulin-resistance and have lymphoid organ hypoplasia. We identified a noncoding nucleotide substitution, c.58+181G>A, in the first intron of the Tw allele of Zeb1 (Zeb1(Tw)). A knockin mouse model of c.58+181G>A recapitulated the Tw phenotype, whereas a wild-type knockin control did not, confirming the mutation as pathogenic. c.58+181G>A does not affect splicing but disrupts a predicted site for Myb protein binding, which we confirmed in vitro. In comparison, homozygosity for a targeted deletion of exon 1 of mouse Zeb1, Zeb1(ΔEx1), is associated with a subtle abnormality of the lateral semicircular canal that is different than those in Tw mice. Expression analyses of E13.5 Twirler and Zeb1(ΔEx1) ears confirm that Zeb1(ΔEx1) is a null allele, whereas Zeb1(Tw) RNA is expressed at increased levels in comparison to wild-type Zeb1. We conclude that a noncoding point mutation of Zeb1 acts via a gain-of-function to disrupt regulation of Zeb1(Tw) expression, epithelial-mesenchymal cell fate or interactions, and structural development of the inner ear in Twirler mice. This is a novel mechanism underlying disorders of hearing or balance.

Published

2011

8. HNF1A recruits KDM6A to activate differentiated acinar cell programs that suppress pancreatic cancer

Author

Irene Esposito, Miguel A. Maestro, Martin Schlensog, Anthony Beucher, Irene Millán, Mark Kalisz, Edgar Bernardo, Francisco X. Real, Karl B. Shpargel, Sagrario Ortega, Jorge Ferrer, Vanessa Grau, Natalia del Pozo, Lena Haeberle, Wolfram T. Knoefel, Eva C. Vaquero, Matías de Vas, Terry Magnuson, and SA Safi

Subjects

endocrine system, endocrine system diseases, Somatic cell, Biology, medicine.disease_cause, Chromatin, Epigenetics, Genomics & Functional Genomics, General Biochemistry, Genetics and Molecular Biology, Article, HNF1A, 03 medical and health sciences, 0302 clinical medicine, Pancreas differentiation, Pancreatic cancer, Acinar cell, medicine, KDM6A, Molecular Biology, Transcription factor, Pancreas, 11 Medical and Health Sciences, 030304 developmental biology, Epigenomics, Cancer, Phenocopy, 0303 health sciences, General Immunology and Microbiology, General Neuroscience, Articles, 06 Biological Sciences, medicine.disease, non‐classical PDAC, digestive system diseases, medicine.anatomical_structure, Cancer research, 08 Information and Computing Sciences, Carcinogenesis, Non-classical PDAC, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Defects in transcriptional regulators of pancreatic exocrine differentiation have been implicated in pancreatic tumorigenesis, but the molecular mechanisms are poorly understood. The locus encoding the transcription factor HNF1A harbors susceptibility variants for pancreatic ductal adenocarcinoma (PDAC), while KDM6A, encoding Lysine‐specific demethylase 6A, carries somatic mutations in PDAC. Here, we show that pancreas‐specific Hnf1a null mutant transcriptomes phenocopy those of Kdm6a mutations, and both defects synergize with Kras G12D to cause PDAC with sarcomatoid features. We combine genetic, epigenomic, and biochemical studies to show that HNF1A recruits KDM6A to genomic binding sites in pancreatic acinar cells. This remodels the acinar enhancer landscape, activates differentiated acinar cell programs, and indirectly suppresses oncogenic and epithelial–mesenchymal transition genes. We also identify a subset of non‐classical PDAC samples that exhibit the HNF1A/KDM6A‐deficient molecular phenotype. These findings provide direct genetic evidence that HNF1A deficiency promotes PDAC. They also connect the tumor‐suppressive role of KDM6A deficiency with a cell‐specific molecular mechanism that underlies PDAC subtype definition., Cooperation between a transcription factor and an epigenetic modifier reveals how defective transcriptional control can contribute to development of pancreatic ductal adenocarcinoma.

Published

2020

9. The KMT2D Kabuki syndrome histone methylase controls neural crest cell differentiation and facial morphology

Author

Kai Ge, Cassidy L. Mangini, Terry Magnuson, Karl B. Shpargel, and Guojia Xie

Subjects

Biology, 03 medical and health sciences, Chondrocytes, 0302 clinical medicine, Cell Movement, Osteogenesis, Histone methylation, Morphogenesis, medicine, Animals, Abnormalities, Multiple, Cell Lineage, Craniofacial, Molecular Biology, Endochondral ossification, Alleles, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Palate, Ossification, Skull, Neural crest, Cell Differentiation, Histone-Lysine N-Methyltransferase, medicine.disease, Hematologic Diseases, Hypoplasia, Cell biology, Mice, Inbred C57BL, Neural crest cell differentiation, Phenotype, Vestibular Diseases, Neural Crest, Face, Mutation, medicine.symptom, Kabuki syndrome, Myeloid-Lymphoid Leukemia Protein, 030217 neurology & neurosurgery, Research Article, Developmental Biology

Abstract

Kabuki syndrome (KS) is a congenital craniofacial disorder resulting from mutations in the KMT2D histone methylase (KS1) or the UTX histone demethylase (KS2). With small cohorts of KS2 patients, it is not clear if differences exist in clinical manifestations relative to KS1. We mutated KMT2D in neural crest cells (NCCs) to study cellular and molecular functions in craniofacial development with respect to UTX. Similar to UTX, KMT2D NCC knockout mice demonstrate hypoplasia with reductions in frontonasal bone lengths. We have traced the onset of KMT2D and UTX mutant NCC frontal dysfunction to a stage of altered osteochondral progenitor differentiation. KMT2D NCC loss of function does exhibit unique phenotypes distinct from UTX mutation including fully penetrant cleft palate, mandible hypoplasia, and deficits in cranial base ossification. KMT2D mutant NCCs lead to defective secondary palatal shelf elevation with reduced expression of extracellular matrix components. KMT2D mutant chondrocytes in the cranial base fail to properly differentiate leading to defective endochondral ossification. We conclude that KMT2D is required for appropriate cranial NCC differentiation and KMT2D specific phenotypes may underlie differences between Kabuki syndrome subtypes.

Published

2020

10. HNF1A recruits UTX to activate a differentiation program that suppresses pancreatic cancer

Author

Jorge Ferrer, Irene Esposito, Terry Magnuson, Wolfram T. Knoefel, Irene Millán, SA Safi, Lena Haeberle, Natalia del Pozo, Eva C. Vaquero, Matías de Vas, Martin Schlensog, Sagrario Ortega, Francisco X. Real, Karl B. Shpargel, Miguel A. Maestro, Anthony Beucher, Edgar Bernardo, Mark Kalisz, and Vanessa Grau

Subjects

Phenocopy, 0303 health sciences, endocrine system, endocrine system diseases, Somatic cell, Biology, medicine.disease, medicine.disease_cause, digestive system diseases, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Pancreatic cancer, Cancer research, medicine, Enhancer, Carcinogenesis, Gene, Transcription factor, 030304 developmental biology, Epigenomics

Abstract

Defects in transcriptional regulators of pancreatic exocrine differentiation have been implicated in pancreatic tumorigenesis, but the molecular mechanisms are poorly understood. The locus encoding the transcription factor HNF1A harbors susceptibility variants for pancreatic ductal adenocarcinoma (PDAC), while KDM6A, encoding the histone demethylase UTX, carries somatic mutations in PDAC. Here, we show that pancreas-specific Hnf1a null mutations phenocopy Utx deficient mutations, and both synergize with KrasG12D to cause PDAC with sarcomatoid features. We combine genetic, epigenomic and biochemical studies to show that HNF1A recruits UTX to genomic binding sites in pancreatic acinar cells. This remodels the acinar enhancer landscape, activates a differentiation program, and indirectly suppresses oncogenic and epithelial-mesenchymal transition genes. Finally, we identify a subset of non-classical PDAC samples that exhibit the HNF1A/UTX-deficient molecular phenotype. These findings provide direct genetic evidence that HNF1A-deficiency promotes PDAC. They also connect the tumor suppressive role of UTX deficiency with a cell-specific molecular mechanism that underlies PDAC subtype definition.

Published

2019

11. UTX-guided neural crest function underlies craniofacial features of Kabuki syndrome

Author

Joshua Starmer, Karl B. Shpargel, Kai Ge, Chaochen Wang, and Terry Magnuson

Subjects

Male, 0301 basic medicine, Cell Survival, Mice, Transgenic, 03 medical and health sciences, Histone H3, Histone demethylation, medicine, Animals, Humans, Abnormalities, Multiple, Craniofacial, Histone Demethylases, Mice, Knockout, Neurocristopathy, Genetics, Multidisciplinary, biology, Lysine, Skull, Gene Expression Regulation, Developmental, Nuclear Proteins, Neural crest, medicine.disease, Hematologic Diseases, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Histone, Vestibular Diseases, PNAS Plus, Neural Crest, Face, Mutation, biology.protein, H3K4me3, Female, Kabuki syndrome

Abstract

Kabuki syndrome, a congenital craniofacial disorder, manifests from mutations in an X-linked histone H3 lysine 27 demethylase (UTX/KDM6A) or a H3 lysine 4 methylase (KMT2D). However, the cellular and molecular etiology of histone-modifying enzymes in craniofacial disorders is unknown. We now establish Kabuki syndrome as a neurocristopathy, whereby the majority of clinical features are modeled in mice carrying neural crest (NC) deletion of UTX, including craniofacial dysmorphism, cardiac defects, and postnatal growth retardation. Female UTX NC knockout (FKO) demonstrates enhanced phenotypic severity over males (MKOs), due to partial redundancy with UTY, a Y-chromosome demethylase-dead homolog. Thus, NC cells may require demethylase-independent UTX activity. Consistently, Kabuki causative point mutations upstream of the JmjC domain do not disrupt UTX demethylation. We have isolated primary NC cells at a phenocritical postmigratory timepoint in both FKO and MKO mice, and genome-wide expression and histone profiling have revealed UTX molecular function in establishing appropriate chromatin structure to regulate crucial NC stem-cell signaling pathways. However, the majority of UTX regulated genes do not experience aberrations in H3K27me3 or H3K4me3, implicating alternative roles for UTX in transcriptional control. These findings are substantiated through demethylase-dead knockin mutation of UTX, which supports appropriate facial development.

Published

2017

12. Pumping RNA: nuclear bodybuilding along the RNP pipeline

Author

A. Gregory Matera and Karl B. Shpargel

Subjects

RNA Splicing, Coiled Bodies, Nerve Tissue Proteins, Computational biology, Models, Biological, S Phase, Conserved sequence, RNA, Small Nuclear, Arabidopsis, RNA Precursors, Animals, Humans, Cyclic AMP Response Element-Binding Protein, Telomerase, Conserved Sequence, Ribonucleoprotein, Genetics, biology, RNA-Binding Proteins, RNA, SMN Complex Proteins, Cell Biology, Ribonucleoprotein, U2 Small Nuclear, Ribonucleoproteins, Small Nuclear, biology.organism_classification, Cajal body, Spliceosomes, Coilin, Biogenesis, Genetic screen

Abstract

Cajal bodies (CBs) are nuclear subdomains involved in the biogenesis of several classes of small ribonucleoproteins (RNPs). A number of recent advances highlight progress in the understanding of the organization and dynamics of CB components. For example, a class of small Cajal body-specific (sca) RNPs has been discovered. Localization of scaRNPs to CBs was shown to depend on a conserved RNA motif. Intriguingly, this motif is also present in mammalian telomerase RNA and the evidence suggests that assembly of the active form of telomerase RNP occurs in and around CBs during S phase. Important steps in the assembly and modification of spliceosomal RNPs have also been shown to take place in CBs. Additional experiments have revealed the existence of kinetically distinct subclasses of CB components. Finally, the recent identification of novel markers for CBs in both Drosophila and Arabidopsis not only lays to rest questions about the evolutionary conservation of these nuclear suborganelles, but also should enable forward genetic screens for the identification of new components and pathways involved in their assembly, maintenance and function.

Published

2006

13. Coilin Methylation Regulates Nuclear Body Formation

Author

Jason K. Ospina, Karen E. Tucker, Karl B. Shpargel, A. Gregory Matera, and Michael D. Hebert

Subjects

Protein-Arginine N-Methyltransferases, Adenosine, endocrine system diseases, Green Fluorescent Proteins, Molecular Sequence Data, Coiled Bodies, Nerve Tissue Proteins, RNA-binding protein, Biology, Arginine, Transfection, medicine.disease_cause, Methylation, General Biochemistry, Genetics and Molecular Biology, Cell Line, Mice, SMN Complex Proteins, Tumor Cells, Cultured, medicine, Protein methylation, Animals, Humans, Amino Acid Sequence, Enzyme Inhibitors, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Cells, Cultured, Cell Nucleus, Mutation, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Fibroblasts, Cell biology, Luminescent Proteins, nervous system, Biochemistry, Cajal body, Coilin, Peptides, Gene Deletion, Biogenesis, HeLa Cells, Developmental Biology

Abstract

Cajal bodies (CBs) are nuclear suborganelles involved in biogenesis of small RNAs. Twin structures, called gems, contain high concentrations of the survival motor neurons (SMN) protein complex. CBs and gems often colocalize, and communication between these subdomains is mediated by coilin, the CB marker. Coilin contains symmetrical dimethylarginines that modulate its affinity for SMN, and, thus, localization of SMN complexes to CBs. Inhibition of methylation or mutation of the coilin RG box dramatically decreases binding of coilin to SMN, resulting in gem formation. Coilin is hypomethylated in cells that display gems, but not in those that primarily contain CBs. Likewise, extracts prepared from cells that display gems are less efficient in methylating coilin and Sm constructs in vitro. These results demonstrate that alterations in protein methylation status can affect nuclear organization.

Published

2002

14. Residual Cajal bodies in coilin knockout mice fail to recruit Sm snRNPs and SMN, the spinal muscular atrophy gene product

Author

Erica Y. Jacobs, Jennifer J. Rossire, Karen E. Tucker, Miguel Lafarga, Maria T. Berciano, A. Gregory Matera, Karl B. Shpargel, Edward K. L. Chan, Ronald A. Conlon, and David F. LePage

Subjects

Chromosomal Proteins, Non-Histone, RNA Splicing, Recombinant Fusion Proteins, Green Fluorescent Proteins, Gene Expression, Coiled Bodies, Nerve Tissue Proteins, Biology, Autoantigens, snRNP Core Proteins, Article, Cell Line, Mice, 03 medical and health sciences, 0302 clinical medicine, SMN Complex Proteins, Animals, snRNP, RNA, Messenger, coilin, SMN, SMA, snRNPs, nuclear organization, Histone locus body, Cyclic AMP Response Element-Binding Protein, Fetal Viability, Research Articles, 030304 developmental biology, SnRNP Biogenesis, Mice, Knockout, Fibrillarin, 0303 health sciences, SnRNP Core Proteins, Homozygote, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Blotting, Northern, Phosphoproteins, Ribonucleoproteins, Small Nuclear, Molecular biology, Survival Rate, Luminescent Proteins, Cajal body, Organ Specificity, Gene Targeting, Coilin, Cell Nucleolus, 030217 neurology & neurosurgery

Abstract

Cajal bodies (CBs) are nuclear suborganelles involved in the biogenesis of small nuclear ribonucleoproteins (snRNPs). In addition to snRNPs, they are highly enriched in basal transcription and cell cycle factors, the nucleolar proteins fibrillarin (Fb) and Nopp140 (Nopp), the survival motor neuron (SMN) protein complex, and the CB marker protein, p80 coilin. We report the generation of knockout mice lacking the COOH-terminal 487 amino acids of coilin. Northern and Western blot analyses demonstrate that we have successfully removed the full-length coilin protein from the knockout animals. Some homozygous mutant animals are viable, but their numbers are reduced significantly when crossed to inbred backgrounds. Analysis of tissues and cell lines from mutant animals reveals the presence of extranucleolar foci that contain Fb and Nopp but not other typical nucleolar markers. These so-called “residual” CBs neither condense Sm proteins nor recruit members of the SMN protein complex. Transient expression of wild-type mouse coilin in knockout cells results in formation of CBs and restores these missing epitopes. Our data demonstrate that full-length coilin is essential for proper formation and/or maintenance of CBs and that recruitment of snRNP and SMN complex proteins to these nuclear subdomains requires sequences within the coilin COOH terminus.

Published

2001

15. Mutations in COL11A2 cause non-syndromic hearing loss (DFNA13)

Author

Darwin J. Prockop, Machiko Arita, Richard Mayne, Shi-Wu Li, Christina L. Runge, Andrew J. Griffith, Richard J.H. Smith, Cor W. R. J. Cremers, Mary Claire King, Glenn E. Green, Wyman T. McGuirt, Robert F. Mueller, C. Huybrechts, Karl B. Shpargel, Han G. Brunner, Masamine Takanosu, Henricus P. M. Kunst, Eric M. Lynch, Sai Prasad, and G. Van Camp

Subjects

Male, Tectorial membrane, Hearing loss, Hearing Loss, Sensorineural, Molecular Sequence Data, Mutation, Missense, Erfelijk gehoorverlies, Locus (genetics), Biology, Mice, Genetics of hearing, otorhinolaryngologic diseases, Genetics, medicine, Animals, Humans, Missense mutation, Inner ear, Amino Acid Sequence, In Situ Hybridization, Polymorphism, Single-Stranded Conformational, Genes, Dominant, Mice, Knockout, Base Sequence, Onderzoek van mitochondrieel DNA in het kader van diagnostiek van mitochondriële myopathieen, Chromosome, DNA, Analysis of mitochondrial DNA as part of the diagnosis of mitochondrial myopathies, medicine.disease, Phenotype, Pedigree, Disease Models, Animal, medicine.anatomical_structure, Chromosomes, Human, Pair 6, Female, Sensorineural hearing loss, Collagen, medicine.symptom

Abstract

We report that mutation of COL11A2 causes deafness previously mapped to the DFNA13 locus on chromosome 6p. We found two families (one American and one Dutch) with autosomal dominant, non-syndromic hearing loss to have mutations in COL11A2 that are predicted to affect the triple-helix domain of the collagen protein. In both families, deafness is non-progressive and predominantly affects middle frequencies. Mice with a targeted disruption of Col11a2 also were shown to have hearing loss. Electron microscopy of the tectorial membrane of these mice revealed loss of organization of the collagen fibrils. Our findings revealed a unique ultrastructural malformation of inner-ear architecture associated with non-syndromic hearing loss, and suggest that tectorial membrane abnormalities may be one aetiology of sensorineural hearing loss primarily affecting the mid-frequencies.

Published

1999

16. An epigenetic switch induced by Shh signalling regulates gene activation during development and medulloblastoma growth

Author

Xuanming Shi, Shizuo Akira, Kai Ge, Qingtian Li, Chaochen Wang, Takashi Satoh, Mou Cao, Jiang Wu, Karl B. Shpargel, Rongfu Wang, Terry Magnuson, Xiaoming Zhan, and Zilai Zhang

Subjects

Jumonji Domain-Containing Histone Demethylases, animal structures, Kruppel-Like Transcription Factors, General Physics and Astronomy, Zinc Finger Protein GLI1, General Biochemistry, Genetics and Molecular Biology, Article, Epigenesis, Genetic, Pregnancy, Cerebellum, Coactivator, Animals, Hedgehog Proteins, Epigenetics, Sonic hedgehog, Cells, Cultured, Genetics, Multidisciplinary, biology, Polycomb Repressive Complex 2, General Chemistry, Histone-Lysine N-Methyltransferase, Hedgehog signaling pathway, Cell biology, Mice, Inbred C57BL, embryonic structures, biology.protein, H3K4me3, Demethylase, Female, PRC2, Myeloid-Lymphoid Leukemia Protein, Bivalent chromatin, Medulloblastoma

Abstract

The Sonic hedgehog (Shh) signalling pathway plays important roles during development and in cancer. Here we report a Shh-induced epigenetic switch that cooperates with Gli to control transcription outcomes. Before induction, poised Shh target genes are marked by a bivalent chromatin domain containing a repressive histone H3K27me3 mark and an active H3K4me3 mark. Shh activation induces a local switch of epigenetic cofactors from the H3K27 methyltransferase polycomb repressive complex 2 (PRC2) to an H3K27me3 demethylase Jmjd3/Kdm6b-centred coactivator complex. We also find that non-enzymatic activities of Jmjd3 are important and that Jmjd3 recruits the Set1/MLL H3K4 methyltransferase complexes in a Shh-dependent manner to resolve the bivalent domain. In vivo, changes of the bivalent domain accompanied Shh-activated cerebellar progenitor proliferation. Overall, our results reveal a regulatory mechanism that underlies the activation of Shh target genes and provides insight into the causes of various diseases and cancers exhibiting altered Shh signalling.

Published

2014

17. KDM6 demethylase independent loss of histone H3 lysine 27 trimethylation during early embryonic development

Author

Michael Pohlers, Della Yee, Terry Magnuson, Karl B. Shpargel, and Joshua Starmer

Subjects

Male, Cancer Research, Jumonji Domain-Containing Histone Demethylases, lcsh:QH426-470, Cellular differentiation, Retinoic acid, Embryonic Development, macromolecular substances, Biology, 03 medical and health sciences, chemistry.chemical_compound, Histone H3, Mice, 0302 clinical medicine, Pregnancy, Genetics, Gene family, Animals, Hox gene, Molecular Biology, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Embryonic Stem Cells, 030304 developmental biology, Regulation of gene expression, Histone Demethylases, 0303 health sciences, Gene Expression Regulation, Developmental, Biology and Life Sciences, Cell Differentiation, Embryo, Mammalian, Molecular biology, Chromatin, lcsh:Genetics, chemistry, Mutation, biology.protein, H3K4me3, Demethylase, Female, 030217 neurology & neurosurgery, Research Article, Developmental Biology

Abstract

The early mammalian embryo utilizes histone H3 lysine 27 trimethylation (H3K27me3) to maintain essential developmental genes in a repressive chromatin state. As differentiation progresses, H3K27me3 is removed in a distinct fashion to activate lineage specific patterns of developmental gene expression. These rapid changes in early embryonic chromatin environment are thought to be dependent on H3K27 demethylases. We have taken a mouse genetics approach to remove activity of both H3K27 demethylases of the Kdm6 gene family, Utx (Kdm6a, X-linked gene) and Jmjd3 (Kdm6b, autosomal gene). Male embryos null for active H3K27 demethylation by the Kdm6 gene family survive to term. At mid-gestation, embryos demonstrate proper patterning and activation of Hox genes. These male embryos retain the Y-chromosome UTX homolog, UTY, which cannot demethylate H3K27me3 due to mutations in catalytic site of the Jumonji-C domain. Embryonic stem (ES) cells lacking all enzymatic KDM6 demethylation exhibit a typical decrease in global H3K27me3 levels with differentiation. Retinoic acid differentiations of these ES cells demonstrate loss of H3K27me3 and gain of H3K4me3 to Hox promoters and other transcription factors, and induce expression similar to control cells. A small subset of genes exhibit decreased expression associated with reduction of promoter H3K4me3 and some low-level accumulation of H3K27me3. Finally, Utx and Jmjd3 mutant mouse embryonic fibroblasts (MEFs) demonstrate dramatic loss of H3K27me3 from promoters of several Hox genes and transcription factors. Our results indicate that early embryonic H3K27me3 repression can be alleviated in the absence of active demethylation by the Kdm6 gene family., Author Summary H3K27me3 represses developmental genes at initial embryonic stages. The KDM6 family, comprised of UTX and JMJD3, are the only known proteins that demethylate H3K27me3 and they are hypothesized to catalyze the rapid removal of repressive chromatin in early mammalian development. However, we report that male embryos carrying mutations in both Utx and Jmjd3 survive to term and appear phenotypically normal at mid-gestation. We utilize several cell culture models to demonstrate that H3K27me3 is lost from repressed promoters in the absence of active KDM6 demethylation. Our data indicate that KDM6 H3K27me3 demethylation is not essential in the early embryo and that H3K27me3 loss from developmental genes occurs via novel mechanisms.

Published

2013

18. UTX and UTY demonstrate histone demethylase-independent function in mouse embryonic development

Author

Toru Sengoku, Terry Magnuson, Karl B. Shpargel, and Shigeyuki Yokoyama

Subjects

Male, Cancer Research, Embryology, Jumonji Domain-Containing Histone Demethylases, Mouse, Mutant, Gene Expression, medicine.disease_cause, urologic and male genital diseases, Mice, 0302 clinical medicine, Demethylase activity, Molecular Cell Biology, Genetics (clinical), Regulation of gene expression, Histone Demethylases, 0303 health sciences, Mutation, biology, Homozygote, Gene Expression Regulation, Developmental, Cell Differentiation, Histone Modification, Animal Models, female genital diseases and pregnancy complications, Epigenetics, Female, Research Article, lcsh:QH426-470, Embryonic Development, Y chromosome, Methylation, Minor Histocompatibility Antigens, 03 medical and health sciences, Histone H3, Genomic Imprinting, Model Organisms, Genetic Mutation, medicine, Genetics, Animals, Humans, Molecular Biology, Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Phenocopy, Hemizygote, Proteins, Molecular biology, lcsh:Genetics, biology.protein, Demethylase, 030217 neurology & neurosurgery, Developmental Biology

Abstract

UTX (KDM6A) and UTY are homologous X and Y chromosome members of the Histone H3 Lysine 27 (H3K27) demethylase gene family. UTX can demethylate H3K27; however, in vitro assays suggest that human UTY has lost enzymatic activity due to sequence divergence. We produced mouse mutations in both Utx and Uty. Homozygous Utx mutant female embryos are mid-gestational lethal with defects in neural tube, yolk sac, and cardiac development. We demonstrate that mouse UTY is devoid of in vivo demethylase activity, so hemizygous XUtx− Y+ mutant male embryos should phenocopy homozygous XUtx− XUtx− females. However, XUtx− Y+ mutant male embryos develop to term; although runted, approximately 25% survive postnatally reaching adulthood. Hemizygous X+ YUty− mutant males are viable. In contrast, compound hemizygous XUtx− YUty− males phenocopy homozygous XUtx− XUtx− females. Therefore, despite divergence of UTX and UTY in catalyzing H3K27 demethylation, they maintain functional redundancy during embryonic development. Our data suggest that UTX and UTY are able to regulate gene activity through demethylase independent mechanisms. We conclude that UTX H3K27 demethylation is non-essential for embryonic viability., Author Summary Trimethylation at Lysine 27 of histone H3 (H3K27me3) establishes a repressive chromatin state in silencing an array of crucial developmental genes. Polycomb repressive complex 2 (PRC2) catalyzes this precise posttranslational modification and is required in several critical aspects of development including Hox gene repression, gastrulation, X-chromosome inactivation, mono-allelic gene expression and imprinting, stem cell maintenance, and oncogenesis. Removal of H3K27 trimethylation has been proposed to be a mechanistic switch to activate large sets of genes in differentiating cells. Mouse Utx is an X-linked H3K27 demethylase that is essential for embryonic development. We now demonstrate that Uty, the Y-chromosome homolog of Utx, has overlapping redundancy with Utx in embryonic development. Mouse UTY has a polymorphism in the JmjC demethylase domain that renders the protein incapable of H3K27 demethylation. Therefore, the overlapping function of UTX and UTY in embryonic development is due to H3K27 demethylase independent mechanism. Moreover, the presence of UTY allows UTX-deficient mouse embryos to survive until birth. Thus, UTX H3K27 demethylation is not essential for embryonic viability. These intriguing results raise new questions on how H3K27me3 repression is removed in the early embryo.

Published

2012

19. Lipopolysaccharide-induced microglial activation and neuroprotection against experimental brain injury is independent of hematogenous TLR4

Author

Bruce D. Trapp, Zhihong Chen, Xinghua Yin, Kenneth T. Farabaugh, Grahame J. Kidd, Cornelia C. Bergmann, Walid Jalabi, Ranjan Dutta, Stephen A. Stohlman, and Karl B. Shpargel

Subjects

Central Nervous System, Lipopolysaccharides, Lipopolysaccharide, Central nervous system, Stimulation, Apoptosis, Pharmacology, Biology, Neuroprotection, Drug Administration Schedule, Article, chemistry.chemical_compound, Mice, Immune system, Antigens, CD, medicine, In Situ Nick-End Labeling, Animals, Microscopy, Immunoelectron, Bone Marrow Transplantation, Cell Proliferation, Mice, Knockout, Mice, Inbred C3H, Transplantation Chimera, Innate immune system, Microglia, Dose-Response Relationship, Drug, General Neuroscience, Motor Cortex, Flow Cytometry, Microarray Analysis, Immunity, Innate, Mice, Inbred C57BL, Toll-Like Receptor 4, Disease Models, Animal, medicine.anatomical_structure, Neuroprotective Agents, chemistry, Bromodeoxyuridine, Brain Injuries, Immunology, Synapses, TLR4

Abstract

Intraperitoneal injection of the Gram-negative bacterial endotoxin lipopolysaccharide (LPS) elicits a rapid innate immune response. While this systemic inflammatory response can be destructive, tolerable low doses of LPS render the brain transiently resistant to subsequent injuries. However, the mechanism by which microglia respond to LPS stimulation and participate in subsequent neuroprotection has not been documented. In this study, we first established a novel LPS treatment paradigm where mice were injected intraperitoneally with 1.0 mg/kg LPS for four consecutive days to globally activate CNS microglia. By using a reciprocal bone marrow transplantation procedure between wild-type and Toll-like receptor 4 (TLR4) mutant mice, we demonstrated that the presence of LPS receptor (TLR4) is not required on hematogenous immune cells but is required on cells that are not replaced by bone marrow transplantation, such as vascular endothelia and microglia, to transduce microglial activation and neuroprotection. Furthermore, we showed that activated microglia physically ensheathe cortical projection neurons, which have reduced axosomatic inhibitory synapses from the neuronal perikarya. In line with previous reports that inhibitory synapse reduction protects neurons from degeneration and injury, we show here that neuronal cell death and lesion volumes are significantly reduced in LPS-treated animals following experimental brain injury. Together, our results suggest that activated microglia participate in neuroprotection and that this neuroprotection is likely achieved through reduction of inhibitory axosomatic synapses. The therapeutic significance of these findings rests not only in identifying neuroprotective functions of microglia, but also in establishing the CNS location of TLR4 activation.

Published

2012

20. Gemin3 Is an Essential Gene Required for Larval Motor Function and Pupation in Drosophila

Author

A. Gregory Matera, Karl B. Shpargel, T. K. Rajendra, and Kavita Praveen

Subjects

Ecdysone, Recombinant Fusion Proteins, Molecular Sequence Data, SMN1, Motor Activity, snRNP Core Proteins, SMN complex, DEAD Box Protein 20, SMN Complex Proteins, medicine, Animals, Drosophila Proteins, Humans, snRNP, Amino Acid Sequence, Transgenes, Molecular Biology, Genetics, SnRNP Core Proteins, biology, Cell Biology, Spinal muscular atrophy, Articles, biology.organism_classification, medicine.disease, Ribonucleoproteins, Small Nuclear, nervous system diseases, Drosophila melanogaster, Larva, RNA Interference, Sequence Alignment, Drosophila Protein, Signal Transduction

Abstract

The assembly of metazoan Sm-class small nuclear ribonucleoproteins (snRNPs) is an elaborate, step-wise process that takes place in multiple subcellular compartments. The initial steps, including formation of the core RNP, are mediated by the survival motor neuron (SMN) protein complex. Loss-of-function mutations in human SMN1 result in a neuromuscular disease called spinal muscular atrophy. The SMN complex is comprised of SMN and a number of tightly associated proteins, collectively called Gemins. In this report, we identify and characterize the fruitfly ortholog of the DEAD box protein, Gemin3. Drosophila Gemin3 (dGem3) colocalizes and interacts with dSMN in vitro and in vivo. RNA interference for dGem3 codepletes dSMN and inhibits efficient Sm core assembly in vitro. Transposon insertion mutations in Gemin3 are larval lethals and also codeplete dSMN. Transgenic overexpression of dGem3 rescues lethality, but overexpression of dSMN does not, indicating that loss of dSMN is not the primary cause of death. Gemin3 mutant larvae exhibit motor defects similar to previously characterized Smn alleles. Remarkably, appreciable numbers of Gemin3 mutants (along with one previously undescribed Smn allele) survive as larvae for several weeks without pupating. Our results demonstrate the conservation of Gemin3 protein function in metazoan snRNP assembly and reveal that loss of either Smn or Gemin3 can contribute to neuromuscular dysfunction.

Published

2009

21. A Drosophila melanogaster model of spinal muscular atrophy reveals a function for SMN in striated muscle

Author

Helen K. Salz, Michael P. Walker, A. Gregory Matera, T. K. Rajendra, Karl B. Shpargel, and Graydon B. Gonsalvez

Subjects

Sarcomeres, Nerve Tissue Proteins, Actinin, SMN1, macromolecular substances, Biology, Sarcomere, Article, Muscular Atrophy, Spinal, 03 medical and health sciences, 0302 clinical medicine, Atrophy, Myofibrils, SMN Complex Proteins, medicine, Animals, Drosophila Proteins, Protein Isoforms, snRNP, Cyclic AMP Response Element-Binding Protein, Muscle, Skeletal, Research Articles, 030304 developmental biology, 0303 health sciences, RNA-Binding Proteins, Cell Biology, Spinal muscular atrophy, medicine.disease, SMA, Ribonucleoproteins, Small Nuclear, Molecular biology, Survival of Motor Neuron 1 Protein, Actins, nervous system diseases, Disease Models, Animal, Drosophila melanogaster, Phenotype, nervous system, Mutation, 030217 neurology & neurosurgery

Abstract

Mutations in human survival motor neurons 1 (SMN1) cause spinal muscular atrophy (SMA) and are associated with defects in assembly of small nuclear ribonucleoproteins (snRNPs) in vitro. However, the etiological link between snRNPs and SMA is unclear. We have developed a Drosophila melanogaster system to model SMA in vivo. Larval-lethal Smn-null mutations show no detectable snRNP reduction, making it unlikely that these animals die from global snRNP deprivation. Hypomorphic mutations in Smn reduce dSMN protein levels in the adult thorax, causing flightlessness and acute muscular atrophy. Mutant flight muscle motoneurons display pronounced axon routing and arborization defects. Moreover, Smn mutant myofibers fail to form thin filaments and phenocopy null mutations in Act88F, which is the flight muscle–specific actin isoform. In wild-type muscles, dSMN colocalizes with sarcomeric actin and forms a complex with α-actinin, the thin filament crosslinker. The sarcomeric localization of Smn is conserved in mouse myofibrils. These observations suggest a muscle-specific function for SMN and underline the importance of this tissue in modulating SMA severity.

Published

2007

22. Gemin proteins are required for efficient assembly of Sm-class ribonucleoproteins

Author

A. Gregory Matera and Karl B. Shpargel

Subjects

Snurportin1, animal diseases, Blotting, Western, Green Fluorescent Proteins, Fluorescent Antibody Technique, Coiled Bodies, Nerve Tissue Proteins, Biology, DEAD-box RNA Helicases, Minor Histocompatibility Antigens, Muscular Atrophy, Spinal, SMN complex, DEAD Box Protein 20, SMN Complex Proteins, Humans, snRNP, Cyclic AMP Response Element-Binding Protein, SnRNP Biogenesis, DNA Primers, Multidisciplinary, Nuclear Proteins, RNA-Binding Proteins, Biological Transport, Biological Sciences, Ribonucleoproteins, Small Nuclear, Molecular biology, nervous system diseases, Cajal body, nervous system, Mutagenesis, Coilin, RNA Interference, Small nuclear RNA, RNA Helicases, HeLa Cells

Abstract

Spinal muscular atrophy (SMA) is a neurodegenerative disease characterized by loss of spinal motor neurons. The gene encoding the survival of motor neurons (SMN) protein is mutated in >95% of SMA cases. SMN is the central component of a large oligomeric complex, including Gemins2–7, that is necessary and sufficient for the in vivo assembly of Sm proteins onto the small nuclear (sn)RNAs that mediate pre-mRNA splicing. After cytoplasmic assembly of the Sm core, both SMN and splicing snRNPs are imported into the nucleus, accumulating in Cajal bodies for additional snRNA maturation steps before targeting to splicing factor compartments known as “speckles.” In this study, we analyzed the function of individual SMN complex members by RNA interference (RNAi). RNAi-mediated knockdown of SMN, Gemin2, Gemin3, and Gemin4 each disrupted Sm core assembly, whereas knockdown of Gemin5 and Snurportin1 had no effect. Assembly activity was rescued by expression of a GFP-SMN construct that is refractive to RNAi but not by similar constructs that contain SMA patient-derived mutations. Our results also demonstrate that Cajal body homeostasis requires SMN and ongoing snRNP biogenesis. Perturbation of SMN function results in disassembly of Cajal bodies and relocalization of the marker protein, coilin, to nucleoli. Moreover, in SMN-deficient cells, newly synthesized SmB proteins fail to associate with U2 snRNA or accumulate in Cajal bodies. Collectively, our results identify a previously uncharacterized function for Gemin3 and Gemin4 in Sm core assembly and correlate the activity of this pathway with SMA.

Published

2005

23. The C-terminal domain of coilin interacts with Sm proteins and U snRNPs

Author

A. Gregory Matera, Karl B. Shpargel, Christian Kambach, Daniel Schümperli, Teldja N. Azzouz, Michael D. Hebert, Ramesh S. Pillai, and Hongzhi Xu

Subjects

Immunoprecipitation, Recombinant Fusion Proteins, Green Fluorescent Proteins, Plasma protein binding, Biology, Transfection, environment and public health, Methylation, Article, Protein structure, Genetics, Escherichia coli, Humans, snRNP, Nuclear protein, Genetics (clinical), Ribonucleoprotein, Binding Sites, Nuclear Proteins, Ribonucleoproteins, Small Nuclear, Cell biology, Protein Structure, Tertiary, Cajal body, Biochemistry, 570 Life sciences, biology, Coilin, Protein Processing, Post-Translational, HeLa Cells, Protein Binding

Abstract

Coilin is the signature protein of the Cajal body (CB), a nuclear suborganelle involved in the biogenesis of small nuclear ribonucleoproteins (snRNPs). Newly imported Sm-class snRNPs are thought to traffic through CBs before proceeding to their final nuclear destinations. Loss of coilin function in mice leads to significant viability and fertility problems. Coilin interacts directly with the spinal muscular atrophy (SMA) protein via dimethylarginine residues in its C-terminal domain. Although coilin hypomethylation results in delocalization of survival of motor neurons (SMN) from CBs, high concentrations of snRNPs remain within these structures. Thus, CBs appear to be involved in snRNP maturation, but factors that tether snRNPs to CBs have not been described. In this report, we demonstrate that the coilin C-terminal domain binds directly to various Sm and Lsm proteins via their Sm motifs. We show that the region of coilin responsible for this binding activity is separable from that which binds to SMN. Interestingly, U2, U4, U5, and U6 snRNPs interact with the coilin C-terminal domain in a glutathione S-transferase (GST)-pulldown assay, whereas U1 and U7 snRNPs do not. Thus, the ability to interact with free Sm (and Lsm) proteins as well as with intact snRNPs, indicates that coilin and CBs may facilitate the modification of newly formed snRNPs, the regeneration of 'mature' snRNPs, or the reclamation of unassembled snRNP components.

Published

2005

24. Col11a1 and Col11a2 mRNA expression in the developing mouse cochlea: implications for the correlation of hearing loss phenotype with mutant type XI collagen genotype

Author

Andrew J. Griffith, Karl B. Shpargel, and Tomoko Makishima

Subjects

Pathology, medicine.medical_specialty, Genotype, Tectorial Membrane, Tectorial membrane, Hearing loss, Hearing Loss, Sensorineural, Cochlear duct, In situ hybridization, Biology, Collagen Type XI, Mice, medicine, Animals, Stickler syndrome, RNA, Messenger, Marshall syndrome, Cochlea, In Situ Hybridization, Gene Expression Regulation, Developmental, General Medicine, medicine.disease, Basilar Membrane, Cell biology, Extracellular Matrix, Mice, Inbred C57BL, medicine.anatomical_structure, Phenotype, Otorhinolaryngology, Mutation, Regression Analysis, Sensorineural hearing loss, medicine.symptom

Abstract

Mutations in the fibrillar collagen genes COL11A1 and COL11A2 can cause sensorineural hearing loss associated with Stickler syndrome. There is a correlation of hearing loss severity, onset, progression and affected frequencies with the underlying mutated collagen gene. We sought to determine whether differences in spatial or temporal expression of these genes underlie this correlation, and to identify the cochlear cell populations expressing these genes and the structures likely to be affected by mutations.We used in situ hybridization analysis of C57BL/6J mouse temporal bones.Similar, diffuse expression of Col11a1 and Col11a2 mRNA was first observed in the cochlear duct at embryonic Day 15.5, with increasingly focal hybridization being noted at postnatal Days 1 and 5 in the greater epithelial ridge and lateral wall of the cochlea. The greater epithelial ridge appeared to be the main, if not only, source of mRNA encoding Col11a1 and Col11a2 in the tectorial membrane. At postnatal Day 13, Col11a1 and Col11a2 expression became more focal and co-localized in the inner sulcus, Claudius' cells and cells of Boettcher.We did not observe spatial or temporal differences in mRNA expression that could account for the auditory phenotype genotype correlation. The expression patterns suggest essential roles for Col11a1 and Col11a2 in the basilar or tectorial membranes.

Published

2004

25. In vivo kinetics of Cajal body components

Author

Karl B. Shpargel, David Stanek, Tom Misteli, A. Gregory Matera, Tatiana S. Karpova, Karla M. Neugebauer, Michael D. Hebert, Miroslav Dundr, Hongzi Xu, and U. Thomas Meier

Subjects

Time Factors, Macromolecular Substances, RNA Splicing, Recombinant Fusion Proteins, Coiled Bodies, Nerve Tissue Proteins, Biology, Cajal body, gems, coilin, SMN, iFRAP, 7. Clean energy, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, SMN complex, SMN Complex Proteins, Fluorescence Resonance Energy Transfer, Animals, Humans, snRNP, Histone locus body, Cyclic AMP Response Element-Binding Protein, 030304 developmental biology, 0303 health sciences, Fluorescence recovery after photobleaching, Nuclear Proteins, RNA-Binding Proteins, Cell Biology, Ribonucleoproteins, Small Nuclear, Biochemistry, Biophysics, Spliceosomes, Coilin, 030217 neurology & neurosurgery, Small nuclear ribonucleoprotein, Cell Nucleolus, Fluorescence Recovery After Photobleaching, HeLa Cells

Abstract

Cajal bodies (CBs) are subnuclear domains implicated in small nuclear ribonucleoprotein (snRNP) biogenesis. In most cell types, CBs coincide with nuclear gems, which contain the survival of motor neurons (SMN) complex, an essential snRNP assembly factor. Here, we analyze the exchange kinetics of multiple components of CBs and gems in living cells using photobleaching microscopy. We demonstrate differences in dissociation kinetics of CB constituents and relate them to their functions. Coilin and SMN complex members exhibit relatively long CB residence times, whereas components of snRNPs, small nucleolar RNPs, and factors shared with the nucleolus have significantly shorter residence times. Comparison of the dissociation kinetics of these shared proteins from either the nucleolus or the CB suggests the existence of compartment-specific retention mechanisms. The dynamic properties of several CB components do not depend on their interaction with coilin because their dissociation kinetics are unaltered in residual nuclear bodies of coilin knockout cells. Photobleaching and fluorescence resonance energy transfer experiments demonstrate that coilin and SMN can interact within CBs, but their interaction is not the major determinant of their residence times. These results suggest that CBs and gems are kinetically independent structures.

Published

2004

26. Simple tests to detect errors in high-throughput genotype data in the molecular laboratory

Author

David J, Vandenbergh, Kathrine, Heron, Ryan, Peterson, Karl B, Shpargel, Abigail, Woodroffe, David A, Blizard, Gerald E, McClearn, and George P, Vogler

Subjects

Genetic Markers, Male, Genotype, Chromosome Mapping, DNA, Articles, Mice, Inbred C57BL, Mice, Mice, Inbred DBA, Data Display, Animals, Female, Algorithms, Alleles, Crosses, Genetic

Abstract

With the advent of high-density DNA marker data sets for the mouse and other model systems, 100 or more genotype are routinely generated from large groups of mice. Issues of the accuracy and reliability of the genotyping are extremely important but often not addressed until genetic analysis is conducted. Simple tests that rely on the robust predictions arising from Mendelian genetics can be made quickly in the molecular laboratory as the data are generated, and require only a spreadsheet program. In this report, genotype data from 392 mice tested at 96 marker sites were analyzed for errors that are typical when handling large volumes of data generated in a repetitive process. The testing consisted of: (1) repeating the genotyping of approximately 1% of the samples; (2) examining the deviation from the expected segregation ratio ( 1:2:1 ) on a marker-by-marker basis; and (3) testing the correlation of the genotype at one marker with that at neighboring genetic markers on a chromosome. These three steps allowed analysis at the level of the microtiter plate, where errors are most likely to occur. A set of 96 dinucleotide repeat markers that are polymorphic between the C57BL/6J and DBA/2J mouse strains and can be multiplexed is reported for use in other genotyping projects.

Published

2003

27. Control of Cajal body number is mediated by the coilin C-terminus

Author

Karen E. Tucker, Michael D. Hebert, A. Gregory Matera, Jason K. Ospina, and Karl B. Shpargel

Subjects

Cytoplasm, Recombinant Fusion Proteins, Molecular Sequence Data, Coiled Bodies, Biology, Mice, RNA, Small Nuclear, Genes, Regulator, medicine, Serine, Animals, Humans, RNA, Small Nucleolar, Small nucleolar RNA, Nuclear protein, Phosphorylation, Cell Nucleus, Sequence Homology, Amino Acid, Nuclear Proteins, Cell Biology, Molecular biology, Protein Structure, Tertiary, Cell nucleus, medicine.anatomical_structure, Eukaryotic Cells, Cajal body, Mutation, Coilin, Nuclear localization sequence, Small nuclear RNA, HeLa Cells, Signal Transduction

Abstract

Cajal bodies (CBs) are nuclear suborganelles implicated in the post-transcriptional maturation of small nuclear and small nucleolar RNAs. The number of CBs displayed by various cell lines and tissues varies, and factors that control CB numbers within a given cell have yet to be described. In this report, we show that specific regions within the C-terminus of coilin, the CB marker protein, are responsible for regulating the number of nuclear foci. Despite the fact that the coilin N-terminal domain is responsible for its self-oligomerization activity, truncation or mutation of predicted sites of phosphorylation in the conserved C-terminal region leads to a striking alteration in the number of nuclear bodies. Similarly, coilin constructs from various species display differential propensities to form nuclear foci when expressed in heterologous backgrounds. We mapped the domain responsible for this variability to the coilin C-terminus utilizing chimeric proteins. Furthermore, the activities responsible for regulating coilin self-association must reside in the nucleus, as constructs lacking critical nuclear localization sequences fail to form foci in the cytoplasm. Factors controlling the putative signal transduction cascade that phosphorylates coilin are also discussed. The results point to a model whereby phosphorylation of the coilin C-terminus regulates the availability of the N-terminal self-interaction domain.

Published

2002

28. Coilin forms the bridge between Cajal bodies and SMN, the spinal muscular atrophy protein

Author

A. Gregory Matera, Piotr Szymczyk, Karl B. Shpargel, and Michael D. Hebert

Subjects

animal diseases, Molecular Sequence Data, Genes, myc, Fluorescent Antibody Technique, Gene Expression, Coiled Bodies, Nerve Tissue Proteins, SMN1, Biology, Transfection, Cell Line, Muscular Atrophy, Spinal, Mice, SMN complex, SMN Complex Proteins, Genetics, Animals, Humans, Amino Acid Sequence, Histone locus body, Cyclic AMP Response Element-Binding Protein, SnRNP Biogenesis, DNA Primers, Glutathione Transferase, Mice, Knockout, Sequence Homology, Amino Acid, Fishes, Nuclear Proteins, RNA-Binding Proteins, Survival of motor neuron, Molecular biology, Survival of Motor Neuron 1 Protein, nervous system diseases, Cajal body, nervous system, Coilin, Anura, Chickens, Developmental Biology, HeLa Cells, Research Paper

Abstract

Spinal muscular atrophy (SMA) is a genetic disorder caused by mutations in the human survival of motor neuron 1 gene,SMN1. SMN protein is part of a large complex that is required for biogenesis of various small nuclear ribonucleoproteins (snRNPs). Here, we report that SMN interacts directly with the Cajal body signature protein, coilin, and that this interaction mediates recruitment of the SMN complex to Cajal bodies. Mutation or deletion of specific RG dipeptide residues within coilin inhibits the interaction both in vivo and in vitro. Interestingly, GST-pulldown experiments show that coilin also binds directly to SmB‘. Competition studies show that coilin competes with SmB‘ for binding sites on SMN. Ectopic expression of SMN and coilin constructs in mouse embryonic fibroblasts lacking endogenous coilin confirms that recruitment of SMN and splicing snRNPs to Cajal bodies depends on the coilin C-terminal RG motif. A cardinal feature of SMA patient cells is a defect in the targeting of SMN to nuclear foci; our results uncover a role for coilin in this process.

Published

2001

29. Preconditioning paradigms and pathways in the brain

Author

Karl B. Shpargel, Yongming Jin, Bruce D. Trapp, Marc S. Penn, Walid Jalabi, and Alisher Dadabayev

Subjects

Ischemia, Nitric Oxide, Receptors, N-Methyl-D-Aspartate, Brain Ischemia, Nitric oxide, Proinflammatory cytokine, chemistry.chemical_compound, medicine, Humans, Ischemic Preconditioning, Innate immune system, business.industry, General Medicine, Hypoxia (medical), Hypothermia, medicine.disease, chemistry, Immune System, Anesthesia, Cortical spreading depression, Cytokines, NMDA receptor, Microglia, medicine.symptom, business, Neuroscience

Abstract

Preconditioning is a phenomenon in which the brain protects itself against future injury by adapting to low doses of noxious insults. Preconditioning stimuli include ischemia, low doses of endotoxin, hypoxia, hypothermia and hyperthermia, cortical spreading depression, anesthetics, and 3-nitropropionic acid, among others. Understanding of the mechanisms underlying preconditioning has been elusive, but NMDA receptor activation, nitric oxide, inflammatory cytokines, and suppression of the innate immune system appear to have a role. Elucidation of the endogenous cell survival pathways involved in preconditioning has significant clinical implications for preventing neuronal damage in susceptible patients.

Published

2008