Your search keyword '"Laurie B. Griffin"' showing total 25 results

1. Exome Sequence Analysis Suggests that Genetic Burden Contributes to Phenotypic Variability and Complex Neuropathy

Author

Claudia Gonzaga-Jauregui, Tamar Harel, Tomasz Gambin, Maria Kousi, Laurie B. Griffin, Ludmila Francescatto, Burcak Ozes, Ender Karaca, Shalini N. Jhangiani, Matthew N. Bainbridge, Kim S. Lawson, Davut Pehlivan, Yuji Okamoto, Marjorie Withers, Pedro Mancias, Anne Slavotinek, Pamela J. Reitnauer, Meryem T. Goksungur, Michael Shy, Thomas O. Crawford, Michel Koenig, Jason Willer, Brittany N. Flores, Igor Pediaditrakis, Onder Us, Wojciech Wiszniewski, Yesim Parman, Anthony Antonellis, Donna M. Muzny, Nicholas Katsanis, Esra Battaloglu, Eric Boerwinkle, Richard A. Gibbs, and James R. Lupski

Subjects

Biology (General), QH301-705.5

Abstract

Charcot-Marie-Tooth (CMT) disease is a clinically and genetically heterogeneous distal symmetric polyneuropathy. Whole-exome sequencing (WES) of 40 individuals from 37 unrelated families with CMT-like peripheral neuropathy refractory to molecular diagnosis identified apparent causal mutations in ∼45% (17/37) of families. Three candidate disease genes are proposed, supported by a combination of genetic and in vivo studies. Aggregate analysis of mutation data revealed a significantly increased number of rare variants across 58 neuropathy-associated genes in subjects versus controls, confirmed in a second ethnically discrete neuropathy cohort, suggesting that mutation burden potentially contributes to phenotypic variability. Neuropathy genes shown to have highly penetrant Mendelizing variants (HPMVs) and implicated by burden in families were shown to interact genetically in a zebrafish assay exacerbating the phenotype established by the suppression of single genes. Our findings suggest that the combinatorial effect of rare variants contributes to disease burden and variable expressivity.

Published

2015

2. Ecteinascidin 743 Interferes with the Activity of EWS-FLI1 in Ewing Sarcoma Cells

Author

Patrick J. Grohar, Laurie B. Griffin, Choh Yeung, Qing-Rong Chen, Yves Pommier, Chand Khanna, Javed Khan, and Lee J. Helman

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

ET-743 (trabectedin; Yondelis) is approved in Europe for the treatment of soft tissue sarcomas. Emerging phase 1 and 2 clinical data have shown high response rates in myxoid liposarcoma in part owing to the inhibition of the FUS-CHOP transcription factor. In this report, we show that modulation of specific oncogenic transcription factors by ET-743 may extend to other tumor types. We demonstrate that, among a panel of pediatric sarcomas, Ewing sarcoma family of tumors (ESFTs) cell lines bearing the EWS-FLI1 transcription factor are the most sensitive to treatment with ET-743 compared with osteosarcoma, rhabdomyosarcoma, and synovial sarcoma. We show that ET-743 reverses a gene signature of induced downstream targets of EWS-FLI1 in two different ESFT cell lines (P = .001). In addition, ET-743 directly suppresses the promoter activity of a known EWS-FLI1 downstream target NR0B1 luciferase reporter construct without changing the activity of a constitutively active control in ESFT cells. Furthermore, the effect is specific to EWS-FLI1, as forced expression of EWS-FLI1 in a cell type that normally lacks this fusion protein, HT1080 cells, induces the same NR0B1 promoter, but this activation is completely blocked by ET-743 treatment. Finally, we used gene set enrichment analysis to confirm that other mechanisms of ET-743 are active in ESFT cells. These results suggest a particular role for ET-743 in the treatment of translocation-positive tumors. In addition, the modulation of EWS-FLI1 makes it a novel targeting agent for ESFT and suggests that further development of this compound for the treatment of ESFT is warranted.

Published

2011

3. Association between partner status and postpartum depression among collaborative care perinatal mental health program participants

Author

Adam K. Lewkowitz, Allie Sakowicz, Emma Allen, Nina K. Ayala, Laurie B. Griffin, Cynthia L. Battle, and Emily S. Miller

Subjects

Obstetrics and Gynecology

Published

2023

4. Neighborhood deprivation and preeclampsia or eclampsia in high-risk pregnancy

Author

Lauren Murphy, Brock Polnaszek, Laurie B. Griffin, Julia Rossen, Christina Raker, Methodius G. Tuuli, Emily S. Miller, Valery A. Danilack, David A. Savitz, and Adam K. Lewkowitz

Subjects

Obstetrics and Gynecology

Published

2023

5. Allele-specific RNA interference prevents neuropathy in Charcot-Marie-Tooth disease type 2D mouse models

Author

Kathryn H. Morelli, Laurie B. Griffin, Allison M. Fowler, Timothy J. Hines, James R. Lupski, Lindsay M. Wallace, Samuel G. Kocen, Scott Q. Harper, Jacob O. Kitzman, Ryuichi Takase, Stephanie N. Oprescu, Alexey I. Nesvizhskii, Rebecca Meyer-Schuman, Nettie K. Pyne, Pedro Mancias, Robert W. Burgess, Dattatreya Mellacheruvu, Ya-Ming Hou, Emily Spaulding, Anthony Antonellis, Na Wei, Xiang-Lei Yang, and Ian J. Butler

Subjects

Glycine-tRNA Ligase, 0301 basic medicine, Genetic enhancement, Mutant, Charcot-Marie-Tooth Disease Type 2D, Mice, 03 medical and health sciences, 0302 clinical medicine, Charcot-Marie-Tooth Disease, RNA interference, Mutant protein, Animals, Humans, Medicine, Allele, Alleles, Gene knockdown, business.industry, Genetic Therapy, General Medicine, medicine.disease, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Peripheral neuropathy, 030220 oncology & carcinogenesis, Mutation, Cancer research, RNA Interference, business, Research Article

Abstract

Gene therapy approaches are being deployed to treat recessive genetic disorders by restoring the expression of mutated genes. However, the feasibility of these approaches for dominantly inherited diseases — where treatment may require reduction in the expression of a toxic mutant protein resulting from a gain-of-function allele — is unclear. Here we show the efficacy of allele-specific RNAi as a potential therapy for Charcot-Marie-Tooth disease type 2D (CMT2D), caused by dominant mutations in glycyl-tRNA synthetase (GARS). A de novo mutation in GARS was identified in a patient with a severe peripheral neuropathy, and a mouse model precisely recreating the mutation was produced. These mice developed a neuropathy by 3–4 weeks of age, validating the pathogenicity of the mutation. RNAi sequences targeting mutant GARS mRNA, but not wild-type, were optimized and then packaged into AAV9 for in vivo delivery. This almost completely prevented the neuropathy in mice treated at birth. Delaying treatment until after disease onset showed modest benefit, though this effect decreased the longer treatment was delayed. These outcomes were reproduced in a second mouse model of CMT2D using a vector specifically targeting that allele. The effects were dose dependent, and persisted for at least 1 year. Our findings demonstrate the feasibility of AAV9-mediated allele-specific knockdown and provide proof of concept for gene therapy approaches for dominant neuromuscular diseases.

Published

2019

6. Homozygosity for a mutation affecting the catalytic domain of tyrosyl-tRNA synthetase (YARS) causes multisystem disease

Author

Karlla W. Brigatti, John D. Overton, Mark Yoder, Anthony Antonellis, Vincent J Carson, Erick D Martinez, Lili Miles, Kadakkal Radhakrishnan, Vinay Kandula, Aris Baras, Claudia Gonzaga-Jauregui, Laurie B. Griffin, Jeffrey G. Reid, Robert N. Jinks, Erik G. Puffenberger, Katie B. Williams, Katryn N. Furuya, Olivia Wenger, Kevin A. Strauss, Matthew M Demczko, Laura Poskitt, and Michael D Fox

Subjects

Adult, Male, 0301 basic medicine, Heterozygote, Hearing Loss, Sensorineural, 030105 genetics & heredity, Biology, Hypoglycemia, medicine.disease_cause, Severity of Illness Index, 03 medical and health sciences, Loss of Function Mutation, Tyrosine-tRNA Ligase, Catalytic Domain, Yeasts, Exome Sequencing, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, Molecular Biology, Genetics (clinical), Exome sequencing, Mutation, Homozygote, Genetic Diseases, Inborn, Infant, Newborn, Infant, Heterozygote advantage, General Medicine, medicine.disease, Pedigree, Complementation, Phenotype, Peripheral neuropathy, Child, Preschool, Female, Sensorineural hearing loss, General Article

Abstract

Aminoacyl-tRNA synthetases (ARSs) are critical for protein translation. Pathogenic variants of ARSs have been previously associated with peripheral neuropathy and multisystem disease in heterozygotes and homozygotes, respectively. We report seven related children homozygous for a novel mutation in tyrosyl-tRNA synthetase (YARS, c.499C > A, p.Pro167Thr) identified by whole exome sequencing. This variant lies within a highly conserved interface required for protein homodimerization, an essential step in YARS catalytic function. Affected children expressed a more severe phenotype than previously reported, including poor growth, developmental delay, brain dysmyelination, sensorineural hearing loss, nystagmus, progressive cholestatic liver disease, pancreatic insufficiency, hypoglycemia, anemia, intermittent proteinuria, recurrent bloodstream infections and chronic pulmonary disease. Related adults heterozygous for YARS p.Pro167Thr showed no evidence of peripheral neuropathy on electromyography, in contrast to previous reports for other YARS variants. Analysis of YARS p.Pro167Thr in yeast complementation assays revealed a loss-of-function, hypomorphic allele that significantly impaired growth. Recombinant YARS p.Pro167Thr demonstrated normal subcellular localization, but greatly diminished ability to homodimerize in human embryonic kidney cells. This work adds to a rapidly growing body of research emphasizing the importance of ARSs in multisystem disease and significantly expands the allelic and clinical heterogeneity of YARS-associated human disease. A deeper understanding of the role of YARS in human disease may inspire innovative therapies and improve care of affected patients.

Published

2018

7. Compound heterozygosity for loss-of-function FARSB variants in a patient with classic features of recessive aminoacyl-tRNA synthetase-related disease

Author

Stephanie N. Oprescu, Anthony Antonellis, Jeffrey W. Innis, Andrea Amalfitano, Laurie B. Griffin, and Amer Heider

Subjects

Male, 0301 basic medicine, Biology, Compound heterozygosity, Article, Amino Acyl-tRNA Synthetases, 03 medical and health sciences, chemistry.chemical_compound, Loss of Function Mutation, Locus heterogeneity, Genetics, medicine, Humans, Genetic Predisposition to Disease, Gene, Genetics (clinical), Loss function, chemistry.chemical_classification, Aminoacyl tRNA synthetase, medicine.disease, Phenotype, Amino acid, 030104 developmental biology, Gene Expression Regulation, chemistry, Transfer RNA, Phenylalanine-tRNA Ligase

Abstract

Aminoacyl-tRNA synthetases (ARSs) are ubiquitously expressed enzymes that ligate amino acids onto tRNA molecules. Genes encoding ARSs have been implicated in phenotypically diverse dominant and recessive human diseases. The charging of tRNA(PHE) with phenylalanine is performed by a tetrameric enzyme that contains two alpha (FARSA) and two beta (FARSB) subunits. To date, mutations in the genes encoding these subunits (FARSA and FARSB) have not been implicated in any human disease. Here, we describe a patient with a severe, lethal, multisystem, developmental phenotype who was compound heterozygous for FARSB variants: p.Thr256Met and p.His496Lysfs*14. Expression studies using fibroblasts isolated from the proband revealed a severe depletion of both FARSB and FARSA protein levels. These data indicate that the FARSB variants destabilize total phenylalanyl-tRNA synthetase levels, thus causing a loss-of-function effect. Importantly, our patient shows strong phenotypic overlap with patients that have recessive diseases associated with other ARS loci; these observations strongly support the pathogenicity of the identified FARSB variants and are consistent with the essential function of phenylalanyl-tRNA synthetase in human cells. In sum, our clinical, genetic, and functional analyses revealed the first FARSB variants associated with a human disease phenotype and expand the locus heterogeneity of ARS-related human disease.

Published

2018

8. Pilot RCT of the Feasibility and Effectiveness of Antepartum Video Breastfeeding Education on Breastfeeding Rates

Author

Laurie B. Griffin, Marie C. Anderson, Phinnara Has, and Adam K. Lewkowitz

Subjects

Obstetrics and Gynecology

Published

2022

9. Predicting the pathogenicity of aminoacyl-tRNA synthetase mutations

Author

Stephanie N. Oprescu, Laurie B. Griffin, Anthony Antonellis, and Asim A. Beg

Subjects

0301 basic medicine, Cytoplasm, Genetic Linkage, Gene Expression, Penetrance, Biology, Mitochondrion, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Amino Acyl-tRNA Synthetases, Mice, 03 medical and health sciences, chemistry.chemical_compound, medicine, Protein biosynthesis, Animals, Humans, Genetic Predisposition to Disease, Molecular Biology, Gene, Genetics, chemistry.chemical_classification, Mutation, Aminoacyl tRNA synthetase, Prognosis, Phenotype, Mitochondria, Pedigree, Disease Models, Animal, 030104 developmental biology, Enzyme, chemistry, Transfer RNA, Hereditary Sensory and Motor Neuropathy

Abstract

Aminoacyl-tRNA synthetases (ARSs) are ubiquitously expressed, essential enzymes responsible for charging tRNA with cognate amino acids-the first step in protein synthesis. ARSs are required for protein translation in the cytoplasm and mitochondria of all cells. Surprisingly, mutations in 28 of the 37 nuclear-encoded human ARS genes have been linked to a variety of recessive and dominant tissue-specific disorders. Current data indicate that impaired enzyme function is a robust predictor of the pathogenicity of ARS mutations. However, experimental model systems that distinguish between pathogenic and non-pathogenic ARS variants are required for implicating newly identified ARS mutations in disease. Here, we outline strategies to assist in predicting the pathogenicity of ARS variants and urge cautious evaluation of genetic and functional data prior to linking an ARS mutation to a human disease phenotype.

Published

2017

10. Mutations in SLC25A46, encoding a UGO1-like protein, cause an optic atrophy spectrum disorder

Author

Antonio Barrientos, Kristen L. Sund, Julia E. Dallman, Adriana P. Rebelo, Stephan Züchner, Zubair M. Ahmed, Xinjian Wang, Claudia Zanna, Andrea H. Németh, Leonardo Caporali, Carlos E. Prada, Neville Patel, Ion J. Campeanu, Feifei Tao, Susan M. Downes, Laura Krueger, Alessandra Maresca, Cynthia A. Prows, Anthony Antonellis, Saskia Groenewald, Lisa Abreu, Fiorella Speziani, Alleene V. Strickland, Yaping Yang, Michael A. Gonzalez, Taosheng Huang, Elizabeth K. Schorry, Valerio Carelli, Chiara La Morgia, Rebecca Schüle, Flavia Fontanesi, Laurie B. Griffin, Alexander J. Abrams, Robert B. Hufnagel, Jeffery Prince, Rocco Liguori, Raffaele Lodi, Omar A. Abdul-Rahman, Holly H. Zimmerman, Yanyan Peng, Abrams, A.J., Hufnagel, R.B., Rebelo, A., Zanna, C., Patel, N., Gonzalez, M.A., Campeanu, I.J., Griffin, L.B., Groenewald, S., Strickland, A.V., Tao, F., Speziani, F., Abreu, L., Schule, R., Caporali, L., La Morgia, C., Maresca, A., Liguori, R., Lodi, R., Ahmed, Z.M., Sund, K.L., Wang, X., Krueger, L.A., Peng, Y., Prada, C.E., Prows, C.A., Schorry, E.K., Antonellis, A., Zimmerman, H.H., Abdul-Rahman, O.A., Yang, Y., Downes, S.M., Prince, J., Fontanesi, F., Barrientos, A., Nemeth, A.H., Carelli, V., Huang, T., Zuchner, S., and Dallman, J.E.

Subjects

Male, Embryo, Nonmammalian, MFN2, Muscle Proteins, IMMT protein, human, DOA, genetics [Muscle Proteins], medicine.disease_cause, Animals, Genetically Modified, pathology [Optic Atrophy, Autosomal Dominant], metabolism [Optic Atrophy, Autosomal Dominant], 0302 clinical medicine, Charcot-Marie-Tooth Disease, Chlorocebus aethiops, genetics [Phosphate Transport Proteins], genetics [Exome], Phosphate Transport Proteins, Exome, metabolism [Zebrafish], genetics [Genetic Predisposition to Disease], embryology [Embryo, Nonmammalian], Zebrafish, Genetics, 0303 health sciences, Mutation, Microscopy, Confocal, biology, Pedigree, genetics [Membrane Proteins], xonal peripheral neuropathy, mitochondrial fusion, Mitochondrial Membranes, COS Cells, Female, genetics [Mitochondrial Proteins], RNA Interference, genetics [Charcot-Marie-Tooth Disease], Protein Binding, UGO1 protein, S cerevisiae, metabolism [Embryo, Nonmammalian], Saccharomyces cerevisiae Proteins, Dominant optic atrophy, Charcot-Marie-Tooth type 2, CMT2, metabolism [Muscle Proteins], genetics [Optic Atrophy, Autosomal Dominant], metabolism [Phosphate Transport Proteins], Article, ultrastructure [Embryo, Nonmammalian], metabolism [Mitochondrial Proteins], Mitochondrial Proteins, 03 medical and health sciences, Atrophy, Microscopy, Electron, Transmission, ddc:570, Optic Atrophy, Autosomal Dominant, metabolism [Mitochondrial Membranes], medicine, Animals, Humans, Inner membrane, Genetic Predisposition to Disease, Hereditary Neurodegenerative Disorder, genetics [Saccharomyces cerevisiae Proteins], 030304 developmental biology, Membrane Proteins, Sequence Analysis, DNA, metabolism [Saccharomyces cerevisiae Proteins], biology.organism_classification, medicine.disease, eye diseases, HEK293 Cells, metabolism [Charcot-Marie-Tooth Disease], Membrane protein, embryology [Zebrafish], hereditary neurodegenerative disorder, metabolism [Membrane Proteins], 030217 neurology & neurosurgery, SLC25A46 protein, human

Abstract

Dominant optic atrophy (DOA) and axonal peripheral neuropathy (Charcot-Marie-Tooth type 2, or CMT2) are hereditary neurodegenerative disorders most commonly caused by mutations in the canonical mitochondrial fusion genes OPA1 and MFN2, respectively. In yeast, homologs of OPA1 (Mgm1) and MFN2 (Fzo1) work in concert with Ugo1, for which no human equivalent has been identified thus far. By whole-exome sequencing of patients with optic atrophy and CMT2, we identified four families with recessive mutations in SLC25A46. We demonstrate that SLC25A46, like Ugo1, is a modified carrier protein that has been recruited to the outer mitochondrial membrane and interacts with the inner membrane remodeling protein mitofilin (Fcj1). Loss of function in cultured cells and in zebrafish unexpectedly leads to increased mitochondrial connectivity, while severely affecting the development and maintenance of neurons in the fish. The discovery of SLC25A46 strengthens the genetic overlap between optic atrophy and CMT2 while exemplifying a new class of modified solute transporters linked to mitochondrial dynamics.

Published

2015

11. A novel AARS mutation in a family with dominant myeloneuropathy

Author

Albena Jordanova, Steven S. Scherer, Peter De Jonghe, Anthony Antonellis, Jonathan Baets, Laurie B. Griffin, Els De Vriendt, Inès Mademan, and William W. Motley

Subjects

Adult, Male, Axonal loss, Sural nerve, Biology, medicine.disease_cause, Article, Young Adult, Sural Nerve, Charcot-Marie-Tooth Disease, medicine, Humans, Missense mutation, Family, Allele, Gene, Genes, Dominant, Genetics, Mutation, Nerve biopsy, medicine.diagnostic_test, Alanine-tRNA Ligase, Middle Aged, Phenotype, Axons, Pedigree, Female, Human medicine, Neurology (clinical)

Abstract

Objective: To determine the genetic cause of neurodegeneration in a family with myeloneuropathy. Methods: We studied 5 siblings in a family with a mild, dominantly inherited neuropathy by clinical examination and electrophysiology. One patient had a sural nerve biopsy. After ruling out common genetic causes of axonal Charcot-Marie-Tooth disease, we sequenced 3 tRNA synthetase genes associated with neuropathy. Results: All affected family members had a mild axonal neuropathy, and 3 of 4 had lower extremity hyperreflexia, evidence of a superimposed myelopathy. A nerve biopsy showed evidence of chronic axonal loss. All affected family members had a heterozygous missense mutation c.304G>C (p.Gly102Arg) in the alanyl-tRNA synthetase (AARS) gene; this allele was not identified in unaffected individuals or control samples. The equivalent change in the yeast ortholog failed to complement a strain of yeast lacking AARS function, suggesting that the mutation is damaging. Conclusion: A novel mutation in AARS causes a mild myeloneuropathy, a novel phenotype for patients with mutations in one of the tRNA synthetase genes.

Published

2015

12. Substrate interaction defects in histidyl-tRNA synthetase linked to dominant axonal peripheral neuropathy

Author

Sharon Aharoni, Inès Mademan, Rebecca Meyer-Schuman, Carmen Espinós, Shawna M. E. Feely, Peter De Jonghe, Jonathan Baets, Vincenzo Lupo, Lina Basel-Vanagaite, Borries Demeler, Carlos Casasnovas, M. Antonia Alberti, Michael E. Shy, Anthony Antonellis, Stephan Züchner, Laurie B. Griffin, Christopher S. Francklyn, Stephanie N. Oprescu, and Jamie A. Abbott

Subjects

Male, 0301 basic medicine, Mutant, Aminoacylation, Biology, Article, Histidine-tRNA Ligase, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Catalytic Domain, Genetics, Humans, HARS, Missense mutation, aminoacyl-tRNA synthetase, Amino Acid Sequence, Enzyme kinetics, Charcot-Marie-Tooth disease type 2W, Conserved Sequence, Genetics (clinical), Histidine, Aminoacyl tRNA synthetase, hereditary motor and sensory neuropathy, Genetic Complementation Test, Peripheral Nervous System Diseases, Molecular biology, Axons, Pedigree, histidyl-tRNA synthetase, Kinetics, 030104 developmental biology, chemistry, Mutation, Transfer RNA, Biocatalysis, Female, Human medicine, Protein Multimerization, 030217 neurology & neurosurgery

Abstract

Histidyl-tRNA synthetase (HARS) ligates histidine to cognate tRNA molecules, which is required for protein translation. Mutations in HARS cause the dominant axonal peripheral neuropathy Charcot-Marie-Tooth disease type 2W (CMT2W); however, the precise molecular mechanism remains undefined. Here, we investigated three HARS missense mutations associated with CMT2W (p.Tyr330Cys, p.Ser356Asn, and p.Val155Gly). The three mutations localize to the HARS catalytic domain and failed to complement deletion of the yeast ortholog (HTS1). Enzyme kinetics, differential scanning fluorimetry (DSF), and analytical ultracentrifugation (AUC) were employed to assess the effect of these substitutions on primary aminoacylation function and overall dimeric structure. Notably, the p.Tyr330Cys, p.Ser356Asn, and p.Val155Gly HARS substitutions all led to reduced aminoacylation, providing a direct connection between CMT2W-linked HARS mutations and loss of canonical ARS function. While DSF assays revealed that only one of the variants (p.Val155Gly) was less thermally stable relative to wild-type, all three HARS mutants formed stable dimers, as measured by AUC. Our work represents the first biochemical analysis of CMT-associated HARS mutations and underscores how loss of the primary aminoacylation function can contribute to disease pathology.

Published

2018

13. AKAP9 Is Essential for Spermatogenesis and Sertoli Cell Maturation in Mice

Author

Suzanne Hartford, Kerry J. Schimenti, Laurie B. Griffin, John C. Schimenti, Sky K. Feuer, Janice K. Pendola, Carl Lessard, Claire A. Bovet, Nancy R. Graham, and Jeremy O. Ward

Subjects

Anti-Mullerian Hormone, Male, Somatic cell, A Kinase Anchor Proteins, Spindle Apparatus, Investigations, Tight Junctions, Mice, Genetics, medicine, Animals, Spermatogenesis, Blood–testis barrier, Sertoli Cells, Tight junction, biology, Gap Junctions, Anti-Müllerian hormone, Sertoli cell, Spermatozoa, Mice, Mutant Strains, Spindle apparatus, Cell biology, Meiosis, Protein Transport, medicine.anatomical_structure, Thyroid hormone receptor alpha, Organ Specificity, Connexin 43, Zonula Occludens-1 Protein, biology.protein, Microtubule-Associated Proteins, Cyclin-Dependent Kinase Inhibitor p27, Thyroid Hormone Receptors alpha

Abstract

Mammalian male fertility relies on complex inter- and intracellular signaling during spermatogenesis. Here we describe three alleles of the widely expressed A-kinase anchoring protein 9 (Akap9) gene, all of which cause gametogenic failure and infertility in the absence of marked somatic phenotypes. Akap9 disruption does not affect spindle nucleation or progression of prophase I of meiosis but does inhibit maturation of Sertoli cells, which continue to express the immaturity markers anti-Mullerian hormone and thyroid hormone receptor alpha in adults and fail to express the maturation marker p27Kip1. Furthermore, gap and tight junctions essential for blood–testis barrier (BTB) organization are disrupted. Connexin43 (Cx43) and zona occludens-1 are improperly localized in Akap9 mutant testes, and Cx43 fails to compartmentalize germ cells near the BTB. These results identify and support a novel reproductive tissue-specific role for Akap9 in the coordinated regulation of Sertoli cells in the testis.

Published

2013

14. Dimerization is required for GARS-mediated neurotoxicity in dominant CMT disease

Author

Nikos Malissovas, Dimitris Beis, Laurie B. Griffin, and Anthony Antonellis

Subjects

0301 basic medicine, Glycine-tRNA Ligase, Mutant, Biology, medicine.disease_cause, Models, Biological, 03 medical and health sciences, Mutant protein, Charcot-Marie-Tooth Disease, Genetics, medicine, Animals, Humans, Allele, Molecular Biology, Genetics (clinical), Loss function, Cells, Cultured, Zebrafish, Mutation, Genetic heterogeneity, Heterozygote advantage, General Medicine, Articles, Zebrafish Proteins, Phenotype, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, Protein Multimerization

Abstract

Charcot-Marie-Tooth (CMT) disease is a genetically heterogeneous group of peripheral neuropathies. Mutations in several aminoacyl-tRNA synthetase (ARS) genes have been implicated in inherited CMT disease. There are 12 reported CMT-causing mutations dispersed throughout the primary sequence of the human glycyl-tRNA synthetase (GARS). While there is strong genetic evidence linking GARS mutations to CMT disease, the molecular pathology underlying the neuromuscular and sensory phenotypes is still not fully understood. In particular, it is unclear whether the mutations result in a toxic gain of function, a partial loss of activity related to translation, or a combination of these mechanisms. We identified a zebrafish allele of gars (gars(s266)). Homozygous mutant embryos carry a C->A transversion, that changes a threonine to a lysine, in a residue next to a CMT-associated human mutation. We show that the neuromuscular phenotype observed in animals homozygous for T209K Gars (T130K in GARS) is due to a loss of dimerization of the mutated protein. Furthermore, we show that the loss of function, dimer-deficient and human disease-associated G319R Gars (G240R in GARS) mutant protein is unable to rescue the above phenotype. Finally, we demonstrate that another human disease-associated mutant G605R Gars (G526 in GARS) dimerizes with the remaining wild-type protein in animals heterozygous for the T209K Gars and reduces the function enough to elicit a neuromuscular phenotype. Our data indicate that dimerization is required for the dominant neurotoxicity of disease-associated GARS mutations and provide a rapid, tractable model for studying newly identified GARS variants for a role in human disease.

Published

2016

15. Identification of an Inhibitor of the EWS-FLI1 Oncogenic Transcription Factor by High-Throughput Screening

Author

Chand Khanna, Girma M. Woldemichael, Qing Rong Chen, Javed Khan, James B. McMahon, Patrick J. Grohar, Lee J. Helman, Laurie B. Griffin, Arnulfo Mendoza, Duane Currier, Sean Davis, and Choh Yeung

Subjects

Cancer Research, Small interfering RNA, Proto-Oncogene Protein c-fli-1, Oncogene Proteins, Fusion, Transcription, Genetic, Cell Survival, Immunoblotting, Transplantation, Heterologous, Protein Array Analysis, Antineoplastic Agents, Sarcoma, Ewing, Biology, medicine.disease_cause, Translocation, Genetic, Malignant transformation, Mice, Transcription (biology), Cell Line, Tumor, medicine, Animals, Humans, Transcription factor, Cell Proliferation, Gene knockdown, Microscopy, Confocal, Plicamycin, Dose-Response Relationship, Drug, Reverse Transcriptase Polymerase Chain Reaction, Articles, Immunohistochemistry, High-Throughput Screening Assays, Gene Expression Regulation, Neoplastic, Oncology, Cancer research, RNA-Binding Protein EWS, Carcinogenesis, DNA Damage, Transcription Factors, medicine.drug

Abstract

Chromosomal translocations generating oncogenic transcription factors are the hallmark of a variety of tumors, including many sarcomas. Ewing sarcoma family of tumors (ESFTs) are characterized by the t(11;22)(q24;q12) translocation that generates the Ewing sarcoma breakpoint region 1 and Friend leukemia virus integration 1 (EWS-FLI1) fusion transcription factor responsible for the highly malignant phenotype of this tumor. Although continued expression of EWS-FLI1 is believed to be critical for ESFT cell survival, a clinically effective small-molecule inhibitor remains elusive likely because EWS-FLI1 is a transcription factor and therefore widely felt to be "undruggable."We developed a high-throughput screen to evaluate more than 50 000 compounds for inhibition of EWS-FLI1 activity in TC32 ESFT cells. We used a TC32 cell-based luciferase reporter screen using the EWS-FLI1 downstream target NR0B1 promoter and a gene signature secondary screen to sort and prioritize the compounds. We characterized the lead compound, mithramycin, based on its ability to inhibit EWS-FLI1 activity in vitro using microarray expression profiling, quantitative reverse transcription-polymerase chain reaction, and immunoblot analysis, and in vivo using immunohistochemistry. We studied the impact of this inhibition on cell viability in vitro and on tumor growth in ESFT xenograft models in vivo (n = 15-20 mice per group). All statistical tests were two-sided.Mithramycin inhibited expression of EWS-FLI1 downstream targets at the mRNA and protein levels and decreased the growth of ESFT cells at half maximal inhibitory concentrations between 10 (95% confidence interval [CI] = 8 to 13 nM) and 15 nM (95% CI = 13 to 19 nM). Mithramycin suppressed the growth of two different ESFT xenograft tumors and prolonged the survival of ESFT xenograft-bearing mice by causing a decrease in mean tumor volume. For example, in the TC32 xenograft model, on day 15 of treatment, the mean tumor volume for the mithramycin-treated mice was approximately 3% of the tumor volume observed in the control mice (mithramycin vs control: 69 vs 2388 mm(3), difference = 2319 mm(3), 95% CI = 1766 to 2872 mm(3), P.001).Mithramycin inhibits EWS-FLI1 activity and demonstrates ESFT antitumor activity both in vitro and in vivo.

Published

2011

16. Ecteinascidin 743 Interferes with the Activity of EWS-FLI1 in Ewing Sarcoma Cells

Author

Chand Khanna, Lee J. Helman, Yves Pommier, Choh Yeung, Patrick J. Grohar, Laurie B. Griffin, Qing Rong Chen, and Javed Khan

Subjects

Cancer Research, Cell type, Oncogene Proteins, Fusion, Bone Neoplasms, Dioxoles, Sarcoma, Ewing, Biology, lcsh:RC254-282, Cell Line, Tumor, Tetrahydroisoquinolines, medicine, Humans, Rhabdomyosarcoma, Child, Promoter Regions, Genetic, Transcription factor, Antineoplastic Agents, Alkylating, Trabectedin, Myxoid liposarcoma, DAX-1 Orphan Nuclear Receptor, Proto-Oncogene Protein c-fli-1, Sarcoma, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Synovial sarcoma, Europe, Gene Expression Regulation, Neoplastic, Cancer research, RNA-Binding Protein FUS, RNA-Binding Protein EWS, Transcription Factor CHOP, medicine.drug, Research Article

Abstract

ET-743 (trabectedin; Yondelis) is approved in Europe for the treatment of soft tissue sarcomas. Emerging phase 1 and 2 clinical data have shown high response rates in myxoid liposarcoma in part owing to the inhibition of the FUS-CHOP transcription factor. In this report, we show that modulation of specific oncogenic transcription factors by ET-743 may extend to other tumor types. We demonstrate that, among a panel of pediatric sarcomas, Ewing sarcoma family of tumors (ESFTs) cell lines bearing the EWS-FLI1 transcription factor are the most sensitive to treatment with ET-743 compared with osteosarcoma, rhabdomyosarcoma, and synovial sarcoma. We show that ET-743 reverses a gene signature of induced downstream targets of EWS-FLI1 in two different ESFT cell lines (P = .001). In addition, ET-743 directly suppresses the promoter activity of a known EWS-FLI1 downstream target NR0B1 luciferase reporter construct without changing the activity of a constitutively active control in ESFT cells. Furthermore, the effect is specific to EWS-FLI1, as forced expression of EWS-FLI1 in a cell type that normally lacks this fusion protein, HT1080 cells, induces the same NR0B1 promoter, but this activation is completely blocked by ET-743 treatment. Finally, we used gene set enrichment analysis to confirm that other mechanisms of ET-743 are active in ESFT cells. These results suggest a particular role for ET-743 in the treatment of translocation-positive tumors. In addition, the modulation of EWS-FLI1 makes it a novel targeting agent for ESFT and suggests that further development of this compound for the treatment of ESFT is warranted.

Published

2011

17. Cover Image, Volume 39, Issue 3

Author

Jamie A. Abbott, Rebecca Meyer-Schuman, Vincenzo Lupo, Shawna Feely, Inès Mademan, Stephanie N. Oprescu, Laurie B. Griffin, M. Antonia Alberti, Carlos Casasnovas, Sharon Aharoni, Lina Basel-Vanagaite, Stephan Züchner, Peter De Jonghe, Jonathan Baets, Michael E. Shy, Carmen Espinós, Borries Demeler, Anthony Antonellis, and Christopher Francklyn

Subjects

Genetics, Genetics (clinical)

Published

2018

18. Exome Sequence Analysis Suggests that Genetic Burden Contributes to Phenotypic Variability and Complex Neuropathy

Author

Jason R. Willer, Matthew N. Bainbridge, James R. Lupski, Igor Pediaditrakis, Marjorie Withers, Nicholas Katsanis, Michel Koenig, Eric Boerwinkle, Tomasz Gambin, Donna M. Muzny, Tamar Harel, Ludmila Francescatto, Pamela J. Reitnauer, Laurie B. Griffin, Yesim Parman, Wojciech Wiszniewski, Davut Pehlivan, Richard A. Gibbs, Kim Lawson, Maria Kousi, Yuji Okamoto, Anne Slavotinek, Burcak Ozes, Michael E. Shy, Thomas O. Crawford, Ender Karaca, Meryem Tuba Goksungur, Shalini N. Jhangiani, Esra Battaloglu, Brittany N. Flores, Claudia Gonzaga-Jauregui, Anthony Antonellis, Pedro Mancias, Onder Us, Department of Pediatrics, University of North Carolina [Chapel Hill] (UNC), University of North Carolina System (UNC)-University of North Carolina System (UNC)-School of Medicine, University of Michigan [Ann Arbor], University of Michigan System, Laboratoire de génétique des maladies rares. Pathologie moleculaire, etudes fonctionnelles et banque de données génétiques (LGMR), IFR3, Université Montpellier 1 (UM1)-Université Montpellier 1 (UM1)-Université de Montpellier (UM)-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier), Human Genome Sequencing Center, Baylor College of Medicine, Baylor College of Medicine (BCM), Baylor University-Baylor University, Department of Molecular and Human Genetics (Baylor College of Medicine), and Baylor College of Medecine

Subjects

Male, Serine C-Palmitoyltransferase, Penetrance, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, Bioinformatics, medicine.disease_cause, Myelin P2 Protein, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Suppression, Genetic, Charcot-Marie-Tooth Disease, Genetic variation, medicine, Animals, Humans, Exome, lcsh:QH301-705.5, Zebrafish, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, Genetic heterogeneity, Genetic Variation, Peripheral Nervous System Diseases, HSP40 Heat-Shock Proteins, medicine.disease, Phenotype, 3. Good health, Genetic load, Pedigree, Peripheral neuropathy, lcsh:Biology (General), Female, Genetic Load, 030217 neurology & neurosurgery

Abstract

International audience; Charcot-Marie-Tooth (CMT) disease is a clinically and genetically heterogeneous distal symmetric polyneuropathy. Whole-exome sequencing (WES) of 40 individuals from 37 unrelated families with CMT-like peripheral neuropathy refractory to molecular diagnosis identified apparent causal mutations in ∼ 45% (17/37) of families. Three candidate disease genes are proposed, supported by a combination of genetic and in vivo studies. Aggregate analysis of mutation data revealed a significantly increased number of rare variants across 58 neuropathy-associated genes in subjects versus controls, confirmed in a second ethnically discrete neuropathy cohort, suggesting that mutation burden potentially contributes to phenotypic variability. Neuropathy genes shown to have highly penetrant Mendelizing variants (HPMVs) and implicated by burden in families were shown to interact genetically in a zebrafish assay exacerbating the phenotype established by the suppression of single genes. Our findings suggest that the combinatorial effect of rare variants contributes to disease burden and variable expressivity.

Published

2015

19. Loss of function mutations in HARS cause a spectrum of inherited peripheral neuropathies

Author

Andreas Ferbert, Tine Deconinck, Petra Laššuthová, Radim Mazanec, Carlo Rivolta, Roman Chrast, Thanita Pilunthanakul, Pavel Seeman, Andreas R. Janecke, Jonathan Baets, Laurie B. Griffin, Jan Senderek, Dana Safka Brozkova, Peter De Jonghe, Stephan Züchner, Jana Haberlová, Christian Roth, Bernd Rautenstrauss, Anthony Antonellis, Asim A. Beg, and Petra Zavadakova

Subjects

Male, medicine.medical_specialty, Genetic Linkage, Biology, medicine.disease_cause, Histidine-tRNA Ligase, 03 medical and health sciences, 0302 clinical medicine, Genetic linkage, Charcot-Marie-Tooth Disease, Molecular genetics, medicine, HARS, Humans, Hereditary Sensory and Autonomic Neuropathies, Loss function, Exome sequencing, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, Genetic heterogeneity, Peripheral Nervous System Diseases, Original Articles, medicine.disease, Pedigree, Peripheral neuropathy, Female, Human medicine, Neurology (clinical), 030217 neurology & neurosurgery

Abstract

Using linkage analysis and whole-exome sequencing, Safka Brozkova et al. reveal missense mutations in the histidyl-tRNA synthetase gene in 23 patients from four families with axonal and demyelinating neuropathies of varying severity. The mutations cause loss of function in yeast complementation assays and neurotoxicity in a C. elegans model.Using linkage analysis and whole-exome sequencing, Safka Brozkova et al. reveal missense mutations in the histidyl-tRNA synthetase gene in 23 patients from four families with axonal and demyelinating neuropathies of varying severity. The mutations cause loss of function in yeast complementation assays and neurotoxicity in a C. elegans model.Inherited peripheral neuropathies are a genetically heterogeneous group of disorders characterized by distal muscle weakness and sensory loss. Mutations in genes encoding aminoacyl-tRNA synthetases have been implicated in peripheral neuropathies, suggesting that these tRNA charging enzymes are uniquely important for the peripheral nerve. Recently, a mutation in histidyl-tRNA synthetase (HARS) was identified in a single patient with a late-onset, sensory-predominant peripheral neuropathy; however, the genetic evidence was lacking, making the significance of the finding unclear. Here, we present clinical, genetic, and functional data that implicate HARS mutations in inherited peripheral neuropathies. The associated phenotypic spectrum is broad and encompasses axonal and demyelinating motor and sensory neuropathies, including four young patients presenting with pure motor axonal neuropathy. Genome-wide linkage studies in combination with whole-exome and conventional sequencing revealed four distinct and previously unreported heterozygous HARS mutations segregating with autosomal dominant peripheral neuropathy in four unrelated families (p.Thr132Ile, p.Pro134His, p.Asp175Glu and p.Asp364Tyr). All mutations cause a loss of function in yeast complementation assays, and p.Asp364Tyr is dominantly neurotoxic in a Caenorhabditis elegans model. This study demonstrates the role of HARS mutations in peripheral neuropathy and expands the genetic and clinical spectrum of aminoacyl-tRNA synthetase-related human disease.

Published

2015

20. Impaired Function is a Common Feature of Neuropathy-Associated Glycyl-tRNA Synthetase Mutations

Author

Charles Searby, David Mcguigan, Reiko Sakaguchi, Ya-Ming Hou, Anthony Antonellis, Stephan Züchner, Laurie B. Griffin, and Michael A. Gonzalez

Subjects

Glycine-tRNA Ligase, Male, congenital, hereditary, and neonatal diseases and abnormalities, DNA Mutational Analysis, Population, Gene Expression, Biology, medicine.disease_cause, Article, Conserved sequence, Glycine—tRNA ligase, Mice, chemistry.chemical_compound, Charcot-Marie-Tooth Disease, Yeasts, Genetics, medicine, Animals, Humans, Aminoacylation, Amino Acid Sequence, education, Gene, Conserved Sequence, Genetic Association Studies, Genetics (clinical), Neurons, education.field_of_study, Mutation, Aminoacyl tRNA synthetase, medicine.disease, Molecular biology, Pedigree, nervous system diseases, Complementation, Kinetics, Protein Transport, Peripheral neuropathy, chemistry, Female, Nervous System Diseases

Abstract

Charcot-Marie-Tooth disease type 2D (CMT2D) is an autosomal dominant axonal peripheral neuropathy characterized by impaired motor and sensory function in the distal extremities. Mutations in the glycyl-tRNA synthetase (GARS) gene cause CMT2D. GARS is a member of the ubiquitously expressed aminoacyl-tRNA synthetase (ARS) family and is responsible for charging tRNA with glycine. To date, thirteen GARS mutations have been identified in patients with CMT disease. While functional studies have revealed loss-of-function characteristics, only four GARS mutations have been rigorously studied. Here, we report the functional evaluation of nine CMT-associated GARS mutations in tRNA charging, yeast complementation, and subcellular localization assays. Our results demonstrate that impaired function is a common characteristic of CMT-associated GARS mutations. Additionally, one mutation previously associated with CMT disease (p.Ser581Leu) does not demonstrate impaired function, was identified in the general population, and failed to segregate with disease in two newly identified families with CMT disease. Thus, we propose that this variant is not a disease-causing mutation. Together, our data indicate that impaired function is a key component of GARS-mediated CMT disease and emphasize the need for careful genetic and functional evaluation before implicating a variant in disease onset.

Published

2014

21. A novel FGD1 mutation in a family with Aarskog–Scott syndrome and predominant features of congenital joint contractures

Author

Laurie B. Griffin, Anthony Antonellis, Frances A. Farley, and Catherine E. Keegan

Subjects

Research Report, 0301 basic medicine, Proband, clinodactyly of the fifth finger, low-set, posteriorly rotated ears, 030105 genetics & heredity, Biology, nonrestrictive ventricular septal defect, medicine.disease_cause, 03 medical and health sciences, FGD1, Embryonic morphogenesis, medicine, short nose, Aarskog–Scott syndrome, ankyloglossia, Peptide sequence, metatarsus adductus, Genetics, Mutation, Shawl scrotum, bilateral cryptorchidism, General Medicine, medicine.disease, unilateral ptosis, flexion contracture, Pleckstrin homology domain, deep philtrum, downslanted palpebral fissures, 030104 developmental biology, congenital foot contractures, decreased palmar creases, shawl scrotum, medicine.symptom

Abstract

Mutations in FGD1 cause Aarskog–Scott syndrome (AAS), an X-linked condition characterized by abnormal facial, skeletal, and genital development due to abnormal embryonic morphogenesis and skeletal formation. Here we report a novel FGD1 mutation in a family with atypical features of AAS, specifically bilateral upper and lower limb congenital joint contractures and cardiac abnormalities. The male proband and his affected maternal uncle are hemizygous for the novel FGD1 mutation p.Arg921X. This variant is the most carboxy-terminal FGD1 mutation identified in a family with AAS and is predicted to truncate the FGD1 protein at the second to last amino acid of the carboxy-terminal pleckstrin homology (PH) domain. Our study emphasizes the importance of the 3′ peptide sequence in the structure and/or function of the FGD1 protein and further demonstrates the need to screen patients with X-linked congenital joint contractures for FGD1 mutations.

Published

2016

22. Mutation in mouse hei10, an e3 ubiquitin ligase, disrupts meiotic crossing over

Author

Marilyn J. O'Brien, Laura G. Reinholdt, Vickie L. Backus, Lisa M Niswander, Laurie B. Griffin, William W. Motley, Kerry J. Schimenti, Dekker C. Deacon, Jeremy O. Ward, Kristofor K. Langlais, John J. Eppig, and John C. Schimenti

Subjects

Male, Cancer Research, Base Pair Mismatch, Eukaryotes, Cell Cycle Proteins, QH426-470, medicine.disease_cause, Chromosomal crossover, Mice, Crossing Over, Genetic, Meiotic Prophase I, Genetics (clinical), Genetics, Mice, Knockout, Recombination, Genetic, Mammals, 0303 health sciences, Mutation, Mice, Inbred C3H, 030302 biochemistry & molecular biology, Mus (Mouse), 3. Good health, Ubiquitin ligase, Vertebrates, Female, Research Article, DNA repair, Ubiquitin-Protein Ligases, Biology, 03 medical and health sciences, Prophase, Meiosis, medicine, Animals, Humans, Molecular Biology, Metaphase, Ecology, Evolution, Behavior and Systematics, Alleles, 030304 developmental biology, Adaptor Proteins, Signal Transducing, Cyclin-Dependent Kinase 2, Genetics and Genomics, Cell Biology, Mice, Inbred C57BL, biology.protein, Cattle

Abstract

Crossing over during meiotic prophase I is required for sexual reproduction in mice and contributes to genome-wide genetic diversity. Here we report on the characterization of an N-ethyl-N-nitrosourea-induced, recessive allele called mei4, which causes sterility in both sexes owing to meiotic defects. In mutant spermatocytes, chromosomes fail to congress properly at the metaphase plate, leading to arrest and apoptosis before the first meiotic division. Mutant oocytes have a similar chromosomal phenotype but in vitro can undergo meiotic divisions and fertilization before arresting. During late meiotic prophase in mei4 mutant males, absence of cyclin dependent kinase 2 and mismatch repair protein association from chromosome cores is correlated with the premature separation of bivalents at diplonema owing to lack of chiasmata. We have identified the causative mutation, a transversion in the 5′ splice donor site of exon 1 in the mouse ortholog of Human Enhancer of Invasion 10 (Hei10; also known as Gm288 in mouse and CCNB1IP1 in human), a putative B-type cyclin E3 ubiquitin ligase. Importantly, orthologs of Hei10 are found exclusively in deuterostomes and not in more ancestral protostomes such as yeast, worms, or flies. The cloning and characterization of the mei4 allele of Hei10 demonstrates a novel link between cell cycle regulation and mismatch repair during prophase I., Author Summary Human infertility and reproductive complications have devastating social and monetary costs. Errors in meiosis during reproduction may lead to birth defects, spontaneous abortion, or infertility. Many of the genes essential for meiosis function in DNA repair and mutations in several of these genes have been shown to contribute to cancer. The identification of the genes necessary for normal meiosis is an important goal and will potentially influence the fields of reproductive and cancer biology. In this study, genetic screens in mice have generated the mutation mei4. mei4 causes male and female sterility by disrupting meiosis and altering the function of the DNA repair system known as mismatch repair. We have identified the causative mutation behind the mei4 phenotype in a gene called Human Enhancer of Invasion 10 or Hei10. This work demonstrates that Hei10 is essential for the completion of meiosis and that it functions to coordinate the DNA repair system and the progression of the cell cycle during meiosis.

Published

2007

23. An Ugo1-like protein is associated with optic atrophy ‘plus’ disorders

Author

Yaping Yang, Yanyan Peng, Cynthia A. Prows, Kevin E. Bove, Jeffery Prince, Xinjian Wang, Leonardo Caporali, Susan M. Downes, Neville Patel, Taosheng Huang, Dallman Julia, Alleene V. Strickland, Michael A. Gonzalez, Feifei Tao, Claudia Zanna, Anthony Antonellis, Laura Krueger, Adriana P. Rebelo, Alexander J. Abrams, Fiorella Speziani, Carlos E. Prada, Rocco Liguori, Andrea H. Németh, Holly H. Zimmerman, Laurie B. Griffin, Stephan Züchner, Elizabeth K. Schorry, Ion J. Campeanu, Raffaele Lodi, Omar A. Abdul-Rahman, Kristen L. Sund, Zubair M. Ahmed, Robert B. Hufnagel, Saskia Groenewald, Valerio Carelli, and Chiara La Morgia

Subjects

Pathology, medicine.medical_specialty, Atrophy, business.industry, medicine, Molecular Medicine, Cell Biology, medicine.disease, business, Molecular Biology

Published

2015

24. Abstract 3414: High-throughput screening identifies mithramycin as a potent inhibitor of the EWS-FLI1 transcription factor and a strong cytotoxic agent in Ewing's sarcoma cells

Author

Choh Yeung, Laurie B. Griffin, Chand Khanna, Patrick J. Grohar, Javed Khan, Girma M. Woldemichael, Qing-Rong Chen, James B. McMahon, and Lee J. Helman

Subjects

Cancer Research, medicine.drug_class, Gene signature, Biology, Molecular biology, Malignant transformation, Real-time polymerase chain reaction, Oncology, Cell culture, medicine, Luciferase, Transcription factor, Gene, Topoisomerase inhibitor

Abstract

Background: Chromosomal translocations involving the EWS gene and one of the members of the ETS family of transcriptions factors are the hallmark of the Ewings Sarcoma Family of Tumors (ESFT). The most common translocation, EWS-FLI1, is found in 85% of the tumors and plays an important role in malignant transformation and maintenance of the oncogenic phenotype. Multiple groups have demonstrated that continued expression of this transcription factor is required for cellular survival. Methods: High throughput screening of a library of more than 50,000 pure compounds was utilized to identify inhibitors of a known EWS-FLI1 downstream target, NR0B1, luciferase promoter construct. The top compounds were subsequently validated and sorted by using a novel 17 gene multiplex PCR assay that quantitates a gene signature of EWS-FLI1. The results were confirmed by quantitative PCR and western blot analysis. The resulting compounds were analyzed for cytotoxicity and selectivity in a panel of ESFT cell lines and compared to cell lines that do not contain the EWS-FLI1 transcription factor. Results Several compounds have been identified that appear to modulate the activity of the EWS-FLI1 transcription factor. These compounds include microtubule inhibitors, topoisomerase inhibitors, compounds of unknown mechanism and an sp1 inhibitor. One of the most potent inhibitors identified was Mithramycin, a natural product known to inhibit sp1. Mithramycin inhibits expression of luciferase in a dose dependent fashion in the NR0B1 promoter reporter construct at concentrations between 10 and 100 nM without decreasing expression in a constitutively active CMV promoter construct. This effect translates into an LD50 of 10 to 25 nM in a panel of ESFT cell lines and increased selectivity relative to osteosarcoma, breast carcinoma and ovarian carcinoma cell lines. Mithramycin also inhibits the expression of the gene signature of EWS-FLI1 as determined by multiplex PCR and confirmed by quantitative PCR. Western blot analysis confirms the inhibition of the downstream target ID2 with a corresponding induction of apoptosis as demonstrated by an increase in cleaved PARP. A review of the literature identified a small panel of patients treated with Mithramycin in the 1960s with at least one documented durable complete response. Conclusion: We have developed a method to screen for transcription factor inhibitors and have utilized it to identify inhibitors of the EWS-FLI1 transcription factor. The most potent inhibitor was Mithramycin which inhibits the expression of a gene signature of EWS-FLI1, has a nanomolar LD50 in ESFT cells and shows some selectivity compared to cells that do not contain EWS-FLI1. Work continues to define the relationship between EWS-FLI1 and sp1 and evaluate the safety and efficacy profile in xenograft models. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 101st Annual Meeting of the American Association for Cancer Research; 2010 Apr 17-21; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2010;70(8 Suppl):Abstract nr 3414.

Published

2010

25. Mutation in mouse hei10, an e3 ubiquitin ligase, disrupts meiotic crossing over.

Author

Jeremy O Ward, Laura G Reinholdt, William W Motley, Lisa M Niswander, Dekker C Deacon, Laurie B Griffin, Kristofor K Langlais, Vickie L Backus, Kerry J Schimenti, Marilyn J O'Brien, John J Eppig, and John C Schimenti

Subjects

Genetics, QH426-470

Abstract

Crossing over during meiotic prophase I is required for sexual reproduction in mice and contributes to genome-wide genetic diversity. Here we report on the characterization of an N-ethyl-N-nitrosourea-induced, recessive allele called mei4, which causes sterility in both sexes owing to meiotic defects. In mutant spermatocytes, chromosomes fail to congress properly at the metaphase plate, leading to arrest and apoptosis before the first meiotic division. Mutant oocytes have a similar chromosomal phenotype but in vitro can undergo meiotic divisions and fertilization before arresting. During late meiotic prophase in mei4 mutant males, absence of cyclin dependent kinase 2 and mismatch repair protein association from chromosome cores is correlated with the premature separation of bivalents at diplonema owing to lack of chiasmata. We have identified the causative mutation, a transversion in the 5' splice donor site of exon 1 in the mouse ortholog of Human Enhancer of Invasion 10 (Hei10; also known as Gm288 in mouse and CCNB1IP1 in human), a putative B-type cyclin E3 ubiquitin ligase. Importantly, orthologs of Hei10 are found exclusively in deuterostomes and not in more ancestral protostomes such as yeast, worms, or flies. The cloning and characterization of the mei4 allele of Hei10 demonstrates a novel link between cell cycle regulation and mismatch repair during prophase I.

Published

2007