Your search keyword '"Gottesfeld JM"' showing total 132 results

1. A non-synonymous single nucleotide polymorphism in SIRT6 predicts neurological severity in Friedreich ataxia.

Author

Rodden, LN, Rummey, C, Dong, YN, Lagedrost, S, Regner, S, Brocht, A, Bushara, K, Delatycki, MB, Gomez, CM, Mathews, K, Murray, S, Perlman, S, Ravina, B, Subramony, SH, Wilmot, G, Zesiewicz, T, Bolotta, A, Domissy, A, Jespersen, C, Ji, B, Soragni, E, Gottesfeld, JM, Lynch, DR, Rodden, LN, Rummey, C, Dong, YN, Lagedrost, S, Regner, S, Brocht, A, Bushara, K, Delatycki, MB, Gomez, CM, Mathews, K, Murray, S, Perlman, S, Ravina, B, Subramony, SH, Wilmot, G, Zesiewicz, T, Bolotta, A, Domissy, A, Jespersen, C, Ji, B, Soragni, E, Gottesfeld, JM, and Lynch, DR

Abstract

Introduction: Friedreich ataxia (FRDA) is a recessive neurodegenerative disease characterized by progressive ataxia, dyscoordination, and loss of vision. The variable length of the pathogenic GAA triplet repeat expansion in the FXN gene in part explains the interindividual variability in the severity of disease. The GAA repeat expansion leads to epigenetic silencing of FXN; therefore, variability in properties of epigenetic effector proteins could also regulate the severity of FRDA. Methods: In an exploratory analysis, DNA from 88 individuals with FRDA was analyzed to determine if any of five non-synonymous SNPs in HDACs/SIRTs predicted FRDA disease severity. Results suggested the need for a full analysis at the rs352493 locus in SIRT6 (p.Asn46Ser). In a cohort of 569 subjects with FRDA, disease features were compared between subjects homozygous for the common thymine SIRT6 variant (TT) and those with the less common cytosine variant on one allele and thymine on the other (CT). The biochemical properties of both variants of SIRT6 were analyzed and compared. Results: Linear regression in the exploratory cohort suggested that an SNP (rs352493) in SIRT6 correlated with neurological severity in FRDA. The follow-up analysis in a larger cohort agreed with the initial result that the genotype of SIRT6 at the locus rs352493 predicted the severity of disease features of FRDA. Those in the CT SIRT6 group performed better on measures of neurological and visual function over time than those in the more common TT SIRT6 group. The Asn to Ser amino acid change resulting from the SNP in SIRT6 did not alter the expression or enzymatic activity of SIRT6 or frataxin, but iPSC-derived neurons from people with FRDA in the CT SIRT6 group showed whole transcriptome differences compared to those in the TT SIRT6 group. Conclusion: People with FRDA in the CT SIRT6 group have less severe neurological and visual dysfunction than those in the TT SIRT6 group. Biochemical analyses indicate that t

Published

2022

2. A gene expression phenotype in lymphocytes from Friedreich ataxia patients

Author

Massimo Pandolfo, David A. Lynch, Susan Perlman, Fuying Gao, Alessandro Filla, Giovanni Coppola, Joel M. Gottesfeld, Heather L. Plasterer, Myriam Rai, Ryan Burnett, James R. Rusche, Daniel H. Geschwind, Francesco Saccà, Revital Versano, Coppola, G, Burnett, R, Perlman, S, Versano, R, Gao, F, Plasterer, H, Rai, M, Sacca', Francesco, Filla, Alessandro, Lynch, Dr, Rusche, Jr, Gottesfeld, Jm, Pandolfo, M, and Geschwind, Dh

Subjects

Adult, Male, Ataxia, Cell Culture Techniques, Gene Expression, Real-Time Polymerase Chain Reaction, Peripheral blood mononuclear cell, Article, 03 medical and health sciences, 0302 clinical medicine, Iron-Binding Proteins, Gene expression, medicine, Humans, Gene, 030304 developmental biology, 0303 health sciences, biology, Phenotype, Molecular biology, 3. Good health, Real-time polymerase chain reaction, Neurology, Friedreich Ataxia, Leukocytes, Mononuclear, Cancer research, Frataxin, biology.protein, Biomarker (medicine), Female, Neurology (clinical), medicine.symptom, 030217 neurology & neurosurgery

Abstract

Objective: Gene expression studies in peripheral tissues from patients with neurodegenerative disorders can provide insights into disease pathogenesis, and identify potential biomarkers, an important goal of translational research in neurodegeneration. Friedreich Ataxia (FRDA) is a chronic neurodegenerative disease caused by reduced transcription of frataxin, a ubiquitously expressed protein. We studied in vitro lymphocytes from FRDA patients and carriers to identify a peripheral gene expression phenotype. Peripheral biomarkers related to disease status would be extremely valuable for assessing drug efficacy and could provide new pathophysiological insights. Methods: We characterized the gene expression profiles in peripheral blood mononuclear cells (PBMCs) from FRDA patients, compared with controls and related carriers. Cells were studied both before and after in vitro treatment with compounds that increase frataxin levels. Quantitative real-time polymerase chain reaction and additional microarrays were used to confirm a core set of genes in multiple independent series. Results: We identified a subset of genes changed in cells from patients with pathological frataxin deficiency, and a core set of these genes were confirmed in independent series. Changes in gene expression were related to the mitochondria, lipid metabolism, cell cycle, and DNA repair, consistent with FRDA’s known pathophysiology. We evaluated the in vitro effect of multiple compounds (histone deacetylase inhibitors) on this putative biomarker set, and found that this biochemical phenotype was ameliorated in accordance with drug efficacy. Interpretation: Frataxin downregulation is associated with robust changes in gene expression in PBMCs, providing pathogenetic insights and a core subset of genes that, if verified in vivo, could be used as a peripheral biomarker. ANN NEUROL 2011;70:790–804

Published

2011

3. A non-synonymous single nucleotide polymorphism in SIRT6 predicts neurological severity in Friedreich ataxia.

Author

Rodden LN, Rummey C, Dong YN, Lagedrost S, Regner S, Brocht A, Bushara K, Delatycki MB, Gomez CM, Mathews K, Murray S, Perlman S, Ravina B, Subramony SH, Wilmot G, Zesiewicz T, Bolotta A, Domissy A, Jespersen C, Ji B, Soragni E, Gottesfeld JM, and Lynch DR

Abstract

Introduction: Friedreich ataxia (FRDA) is a recessive neurodegenerative disease characterized by progressive ataxia, dyscoordination, and loss of vision. The variable length of the pathogenic GAA triplet repeat expansion in the FXN gene in part explains the interindividual variability in the severity of disease. The GAA repeat expansion leads to epigenetic silencing of FXN; therefore, variability in properties of epigenetic effector proteins could also regulate the severity of FRDA. Methods: In an exploratory analysis, DNA from 88 individuals with FRDA was analyzed to determine if any of five non-synonymous SNPs in HDAC s/ SIRT s predicted FRDA disease severity. Results suggested the need for a full analysis at the rs352493 locus in SIRT6 ( p .Asn46Ser). In a cohort of 569 subjects with FRDA, disease features were compared between subjects homozygous for the common thymine SIRT6 variant (TT) and those with the less common cytosine variant on one allele and thymine on the other (CT). The biochemical properties of both variants of SIRT6 were analyzed and compared. Results: Linear regression in the exploratory cohort suggested that an SNP (rs352493) in SIRT6 correlated with neurological severity in FRDA. The follow-up analysis in a larger cohort agreed with the initial result that the genotype of SIRT6 at the locus rs352493 predicted the severity of disease features of FRDA. Those in the CT SIRT6 group performed better on measures of neurological and visual function over time than those in the more common TT SIRT6 group. The Asn to Ser amino acid change resulting from the SNP in SIRT6 did not alter the expression or enzymatic activity of SIRT6 or frataxin, but iPSC-derived neurons from people with FRDA in the CT SIRT6 group showed whole transcriptome differences compared to those in the TT SIRT6 group. Conclusion: People with FRDA in the CT SIRT6 group have less severe neurological and visual dysfunction than those in the TT SIRT6 group. Biochemical analyses indicate that the benefit conferred by T to C SNP in SIRT6 does not come from altered expression or enzymatic activity of SIRT6 or frataxin but is associated with changes in the transcriptome., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Rodden, Rummey, Dong, Lagedrost, Regner, Brocht, Bushara, Delatycki, Gomez, Mathews, Murray, Perlman, Ravina, Subramony, Wilmot, Zesiewicz, Bolotta, Domissy, Jespersen, Ji, Soragni, Gottesfeld and Lynch.)

Published

2022

4. Methylated and unmethylated epialleles support variegated epigenetic silencing in Friedreich ataxia.

Author

Rodden LN, Chutake YK, Gilliam K, Lam C, Soragni E, Hauser L, Gilliam M, Wiley G, Anderson MP, Gottesfeld JM, Lynch DR, and Bidichandani SI

Subjects

Adolescent, Adult, Alleles, Child, Child, Preschool, Female, Friedreich Ataxia genetics, Humans, Infant, Leukocytes, Mononuclear metabolism, Male, Young Adult, DNA Methylation, Epigenesis, Genetic, Friedreich Ataxia pathology, Gene Silencing, Leukocytes, Mononuclear pathology, Phenotype

Abstract

Friedreich ataxia (FRDA) is typically caused by homozygosity for an expanded GAA triplet-repeat in intron 1 of the FXN gene, which results in transcriptional deficiency via epigenetic silencing. Most patients are homozygous for alleles containing > 500 triplets, but a subset (~20%) have at least one expanded allele with < 500 triplets and a distinctly milder phenotype. We show that in FRDA DNA methylation spreads upstream from the expanded repeat, further than previously recognized, and establishes an FRDA-specific region of hypermethylation in intron 1 (~90% in FRDA versus < 10% in non-FRDA) as a novel epigenetic signature. The hypermethylation of this differentially methylated region (FRDA-DMR) was observed in a variety of patient-derived cells; it significantly correlated with FXN transcriptional deficiency and age of onset, and it reverted to the non-disease state in isogenically corrected induced pluripotent stem cell (iPSC)-derived neurons. Bisulfite deep sequencing of the FRDA-DMR in peripheral blood mononuclear cells from 73 FRDA patients revealed considerable intra-individual epiallelic variability, including fully methylated, partially methylated, and unmethylated epialleles. Although unmethylated epialleles were rare (median = 0.33%) in typical patients homozygous for long GAA alleles with > 500 triplets, a significantly higher prevalence of unmethylated epialleles (median = 9.8%) was observed in patients with at least one allele containing < 500 triplets, less severe FXN deficiency (>20%) and later onset (>15 years). The higher prevalence in mild FRDA of somatic FXN epialleles devoid of DNA methylation is consistent with variegated epigenetic silencing mediated by expanded triplet-repeats. The proportion of unsilenced somatic FXN genes is an unrecognized phenotypic determinant in FRDA and has implications for the deployment of effective therapies., (© The Author(s) 2021. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2021

5. Molecular Mechanisms and Therapeutics for the GAA·TTC Expansion Disease Friedreich Ataxia.

Author

Gottesfeld JM

Subjects

Animals, Drug Delivery Systems methods, Friedreich Ataxia metabolism, Gene Transfer Techniques trends, Genetic Therapy methods, Histone Deacetylase Inhibitors administration & dosage, Humans, Promoter Regions, Genetic genetics, Resveratrol administration & dosage, Drug Delivery Systems trends, Friedreich Ataxia genetics, Friedreich Ataxia therapy, Gene Silencing physiology, Genetic Therapy trends, Trinucleotide Repeat Expansion physiology

Abstract

Friedreich ataxia (FRDA), the most common inherited ataxia, is caused by transcriptional silencing of the nuclear FXN gene, encoding the essential mitochondrial protein frataxin. Currently, there is no approved therapy for this fatal disorder. Gene silencing in FRDA is due to hyperexpansion of the triplet repeat sequence GAA·TTC in the first intron of the FXN gene, which results in chromatin histone modifications consistent with heterochromatin formation. Frataxin is involved in mitochondrial iron homeostasis and the assembly and transfer of iron-sulfur clusters to various mitochondrial enzymes and components of the electron transport chain. Frataxin insufficiency leads to progressive spinocerebellar neurodegeneration, causing symptoms of gait and limb ataxia, slurred speech, muscle weakness, sensory loss, and cardiomyopathy in many patients, resulting in death in early adulthood. Numerous approaches are being taken to find a treatment for FRDA, including excision or correction of the repeats by genome engineering methods, gene activation with small molecules or artificial transcription factors, delivery of frataxin to affected cells by protein replacement therapy, gene therapy, or small molecules to increase frataxin protein levels, and therapies aimed at countering the cellular consequences of reduced frataxin. This review will summarize the mechanisms involved in repeat-mediated gene silencing and recent efforts aimed at development of therapeutics.

Published

2019

6. Transcriptional profiling of isogenic Friedreich ataxia neurons and effect of an HDAC inhibitor on disease signatures.

Author

Lai JI, Nachun D, Petrosyan L, Throesch B, Campau E, Gao F, Baldwin KK, Coppola G, Gottesfeld JM, and Soragni E

Subjects

Cells, Cultured, Friedreich Ataxia pathology, Gene Editing methods, Gene Expression Profiling, Humans, Induced Pluripotent Stem Cells chemistry, Iron-Binding Proteins genetics, Iron-Binding Proteins metabolism, Neurons chemistry, Trinucleotide Repeat Expansion genetics, Frataxin, Friedreich Ataxia genetics, Histone Deacetylase Inhibitors pharmacology, Neurons pathology, Transcriptome

Abstract

Friedreich ataxia (FRDA) is a neurodegenerative disorder caused by transcriptional silencing of the frataxin ( FXN ) gene, resulting in loss of the essential mitochondrial protein frataxin. Based on the knowledge that a GAA·TTC repeat expansion in the first intron of FXN induces heterochromatin, we previously showed that 2-aminobenzamide-type histone deacetylase inhibitors (HDACi) increase FXN mRNA levels in induced pluripotent stem cell (iPSC)-derived FRDA neurons and in circulating lymphocytes from patients after HDACi oral administration. How the reduced expression of frataxin leads to neurological and other systemic symptoms in FRDA patients remains unclear. Similar to other triplet-repeat disorders, it is unknown why FRDA affects only specific cell types, primarily the large sensory neurons of the dorsal root ganglia and cardiomyocytes. The combination of iPSC technology and genome-editing techniques offers the unique possibility to address these questions in a relevant cell model of FRDA, obviating confounding effects of variable genetic backgrounds. Here, using "scarless" gene-editing methods, we created isogenic iPSC lines that differ only in the length of the GAA·TTC repeats. To uncover the gene expression signatures due to the GAA·TTC repeat expansion in FRDA neuronal cells and the effect of HDACi on these changes, we performed RNA-seq-based transcriptomic analysis of iPSC-derived central nervous system (CNS) and isogenic sensory neurons. We found that cellular pathways related to neuronal function, regulation of transcription, extracellular matrix organization, and apoptosis are affected by frataxin loss in neurons of the CNS and peripheral nervous system and that these changes are partially restored by HDACi treatment., (© 2019 Lai et al.)

Published

2019

7. Milestones in transcription and chromatin published in the Journal of Biological Chemistry .

Author

Gottesfeld JM

Subjects

Epigenesis, Genetic, History, 20th Century, History, 21st Century, Humans, Periodicals as Topic, Protein Processing, Post-Translational, Biochemistry history, Chromatin genetics, Chromatin metabolism, Histones metabolism, Transcription Factors metabolism, Transcription, Genetic

Abstract

During Herbert Tabor's tenure as Editor-in-Chief from 1971 to 2010, JBC has published many seminal papers in the fields of chromatin structure, epigenetics, and regulation of transcription in eukaryotes. As of this writing, more than 21,000 studies on gene transcription at the molecular level have been published in JBC since 1971. This brief review will attempt to highlight some of these ground-breaking discoveries and show how early studies published in JBC have influenced current research. Papers published in the Journal have reported the initial discovery of multiple forms of RNA polymerase in eukaryotes, identification and purification of essential components of the transcription machinery, and identification and mechanistic characterization of various transcriptional activators and repressors and include studies on chromatin structure and post-translational modifications of the histone proteins. The large body of literature published in the Journal has inspired current research on how chromatin organization and epigenetics impact regulation of gene expression., (© 2019 Gottesfeld.)

Published

2019

8. Introduction to the Thematic Minireview Series: Chromatin and transcription.

Author

Gottesfeld JM and Carey MF

Subjects

Animals, Gene Expression Regulation, Humans, Chromatin genetics, Transcription, Genetic

Abstract

Regulation of transcription in eukaryotic cells is a dynamic interplay between chromatin structure and recruitment of a plethora of transcription factors to enhancers, upstream activator sequences, and proximal promoter elements. These factors serve to recruit RNA polymerase to the core promoter for productive transcription. In this Thematic Minireview Series on chromatin and transcription, five reviews summarize current knowledge of diverse aspects of transcriptional regulation and the role of chromatin structure in transcription and development., (© 2018 Gottesfeld and Carey.)

Published

2018

9. Repeat-Associated Non-ATG (RAN) Translation in Fuchs' Endothelial Corneal Dystrophy.

Author

Soragni E, Petrosyan L, Rinkoski TA, Wieben ED, Baratz KH, Fautsch MP, and Gottesfeld JM

Subjects

Blotting, Western, Cell Proliferation, Cells, Cultured, Endothelium, Corneal metabolism, Fibroblasts metabolism, Fluorescent Antibody Technique, Indirect, Gene Expression physiology, Humans, Introns, Real-Time Polymerase Chain Reaction, Transfection, Fuchs' Endothelial Dystrophy genetics, Protein Biosynthesis, Transcription Factor 4 genetics, Trinucleotide Repeat Expansion genetics

Abstract

Purpose: The strongest genetic association with Fuchs' endothelial corneal dystrophy (FECD) is the presence of an intronic (CTG·CAG)n trinucleotide repeat (TNR) expansion in the transcription factor 4 (TCF4) gene. Repeat-associated non-ATG (RAN) translation, an unconventional protein translation mechanism that does not require an initiating ATG, has been described in many TNR expansion diseases, including myotonic dystrophy type 1 (DM1). Given the similarities between DM1 and FECD, we wished to determine whether RAN translation occurs in FECD., Methods: Antibodies against peptides in the C-terminus of putative RAN translation products from TCF4 were raised and validated by Western blotting and immunofluorescence (IF). CTG·CAG repeats of various lengths in the context of the TCF4 gene were cloned in frame with a 3× FLAG tag and transfected in human cells. IF with antipeptide and anti-FLAG antibodies, as well as cytotoxicity and cell proliferation assays, were performed in these transfected cells. Corneal endothelium derived from patients with FECD was probed with validated antibodies by IF., Results: CTG·CAG repeats in the context of the TCF4 gene are transcribed and translated via non-ATG initiation in transfected cells and confer toxicity to an immortalized corneal endothelial cell line. An antipeptide antibody raised against the C-terminus of the TCF4 poly-cysteine frame recognized RAN translation products by IF in cells transfected with CTG·CAG repeats and in FECD corneal endothelium., Conclusions: Expanded CTG·CAG repeats in the context of the third intron of TCF4 are transcribed and translated via non-ATG initiation, providing evidence for RAN translation in corneal endothelium of patients with FECD.

Published

2018

10. Cyclic tetrapeptide HDAC inhibitors as potential therapeutics for spinal muscular atrophy: Screening with iPSC-derived neuronal cells.

Author

Lai JI, Leman LJ, Ku S, Vickers CJ, Olsen CA, Montero A, Ghadiri MR, and Gottesfeld JM

Subjects

Cells, Cultured, Drug Evaluation, Preclinical, Humans, Induced Pluripotent Stem Cells cytology, Muscular Atrophy, Spinal genetics, Neurogenesis, Neurons metabolism, Survival of Motor Neuron 2 Protein genetics, Up-Regulation drug effects, Histone Deacetylase Inhibitors chemistry, Histone Deacetylase Inhibitors pharmacology, Muscular Atrophy, Spinal drug therapy, Neurons drug effects, Peptides, Cyclic chemistry, Peptides, Cyclic pharmacology

Abstract

Spinal muscular atrophy (SMA) is an autosomal recessive neuromuscular disorder that is caused by inactivating mutations in the Survival of motor neuron 1 (SMN1) gene, resulting in decreased SMN protein expression. Humans possess a paralog gene, SMN2, which contains a splicing defect in exon 7 leading to diminished expression of full-length, fully functional SMN protein. Increasing SMN2 expression has been a focus of therapeutic development for SMA. Multiple studies have reported the efficacy of histone deacetylase inhibitors (HDACi) in this regard. However, clinical trials involving HDACi have been unsatisfactory, possibly because previous efforts to identify HDACi to treat SMA have employed non-neuronal cells as the screening platform. To address this issue, we generated an SMA-patient specific, induced pluripotent stem cell (iPSC) derived neuronal cell line that contains homogenous Tuj1+neurons. We screened a small library of cyclic tetrapeptide HDACi using this SMA neuronal platform and discovered compounds that elevate SMN2 expression by an impressive twofold or higher. These candidates are also capable of forming gems intranuclearly in SMA neurons, demonstrating biological activity. Our study identifies new potential HDACi therapeutics for SMA screened using a disease-relevant SMA neuronal cellular model., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

11. The Effects of Pharmacological Inhibition of Histone Deacetylase 3 (HDAC3) in Huntington's Disease Mice.

Author

Jia H, Wang Y, Morris CD, Jacques V, Gottesfeld JM, Rusche JR, and Thomas EA

Subjects

Acrylamides pharmacology, Animals, Cytokines genetics, Cytokines metabolism, Disease Models, Animal, Histone Deacetylase Inhibitors pharmacology, Histone Deacetylases metabolism, Huntington Disease metabolism, Intramolecular Oxidoreductases genetics, Intramolecular Oxidoreductases metabolism, Macrophage Migration-Inhibitory Factors genetics, Macrophage Migration-Inhibitory Factors metabolism, Mice, Mice, Transgenic, Motor Activity drug effects, Neuroprotective Agents pharmacology, Phenylenediamines pharmacology, RNA, Messenger metabolism, Histone Deacetylases chemistry, Huntington Disease pathology

Abstract

An important epigenetic modification in Huntington's disease (HD) research is histone acetylation, which is regulated by histone acetyltransferase and histone deacetylase (HDAC) enzymes. HDAC inhibitors have proven effective in HD model systems, and recent work is now focused on functional dissection of the individual HDAC enzymes in these effects. Histone deacetylase 3 (HDAC3), a member of the class I subfamily of HDACs, has previously been implicated in neuronal toxicity and huntingtin-induced cell death. Hence, we tested the effects of RGFP966 ((E)-N-(2-amino-4-fluorophenyl)-3-(1-cinnamyl-1H-pyrazol-4-yl)acrylamide), a benzamide-type HDAC inhibitor that selectively targets HDAC3, in the N171-82Q transgenic mouse model of HD. We found that RGFP966 at doses of 10 and 25 mg/kg improves motor deficits on rotarod and in open field exploration, accompanied by neuroprotective effects on striatal volume. In light of previous studies implicating HDAC3 in immune function, we measured gene expression changes for 84 immune-related genes elicited by RGFP966 using quantitative PCR arrays. RGFP966 treatment did not cause widespread changes in cytokine/chemokine gene expression patterns, but did significantly alter the striatal expression of macrophage migration inhibitory factor (Mif), a hormone immune modulator associated with glial cell activation, in N171-82Q transgenic mice, but not WT mice. Accordingly, RGFP966-treated mice showed decreased glial fibrillary acidic protein (GFAP) immunoreactivity, a marker of astrocyte activation, in the striatum of N171-82Q transgenic mice compared to vehicle-treated mice. These findings suggest that the beneficial actions of HDAC3 inhibition could be related, in part, with lowered Mif levels and its associated downstream effects.

Published

2016

12. Translating HDAC inhibitors in Friedreich's ataxia.

Author

Soragni E and Gottesfeld JM

Abstract

Introduction: Friedreich's ataxia (FRDA) is an autosomal recessive neurodegenerative disease caused by expansion of a GAA·TTC triplet in the first intron of the FXN gene, encoding the essential mitochondrial protein frataxin. Repeat expansion results in transcriptional silencing through an epigenetic mechanism, resulting in significant decreases in frataxin protein in affected individuals. Since the FXN protein coding sequence is unchanged in FRDA, an attractive therapeutic approach for this disease would be to increase transcription of pathogenic alleles with small molecules that target the silencing mechanism., Areas Covered: We review the evidence that histone postsynthetic modifications and heterochromatin formation are responsible for FXN gene silencing in FRDA, along with efforts to reverse silencing with drugs that target histone modifying enzymes. Chemical and pharmacological properties of histone deacetylase (HDAC) inhibitors, which reverse silencing, together with enzyme target profiles and kinetics of inhibition, are discussed. Two HDAC inhibitors have been studied in human clinical trials and the properties of these compounds are compared and contrasted. Efforts to improve on bioavailability, metabolic stability, and target activity are reviewed., Expert Opinion: 2-aminobenzamide class I HDAC inhibitors are attractive therapeutic small molecules for FRDA. These molecules increase FXN gene expression in human neuronal cells derived from patient induced pluripotent stem cells, and in two mouse models for the disease, as well as in circulating lymphocytes in patients treated in a phase Ib clinical trial. Medicinal chemistry efforts have identified compounds with improved brain penetration, metabolic stability and efficacy in the human neuronal cell model. A clinical candidate will soon be identified for further human testing., Competing Interests: Declaration of interest The authors have no other relevant affiliations or financial involvement with any organization or entity with a financial interest in or financial conflict with the subject matter or materials discussed in the manuscript apart from those disclosed.

Published

2016

13. RNA toxicity and missplicing in the common eye disease fuchs endothelial corneal dystrophy.

Author

Du J, Aleff RA, Soragni E, Kalari K, Nie J, Tang X, Davila J, Kocher JP, Patel SV, Gottesfeld JM, Baratz KH, and Wieben ED

Subjects

Cornea metabolism, Cornea pathology, Fuchs' Endothelial Dystrophy pathology, Humans, RNA Splicing genetics, RNA-Binding Proteins genetics, Transcription Factor 4, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors genetics, Fuchs' Endothelial Dystrophy genetics, RNA, Messenger genetics, Transcription Factors genetics, Trinucleotide Repeat Expansion genetics

Abstract

Fuchs endothelial corneal dystrophy (FECD) is an inherited degenerative disease that affects the internal endothelial cell monolayer of the cornea and can result in corneal edema and vision loss in severe cases. FECD affects ∼5% of middle-aged Caucasians in the United States and accounts for >14,000 corneal transplantations annually. Among the several genes and loci associated with FECD, the strongest association is with an intronic (CTG·CAG)n trinucleotide repeat expansion in the TCF4 gene, which is found in the majority of affected patients. Corneal endothelial cells from FECD patients harbor a poly(CUG)n RNA that can be visualized as RNA foci containing this condensed RNA and associated proteins. Similar to myotonic dystrophy type 1, the poly(CUG)n RNA co-localizes with and sequesters the mRNA-splicing factor MBNL1, leading to missplicing of essential MBNL1-regulated mRNAs. Such foci and missplicing are not observed in similar cells from FECD patients who lack the repeat expansion. RNA-Seq splicing data from the corneal endothelia of FECD patients and controls reveal hundreds of differential alternative splicing events. These include events previously characterized in the context of myotonic dystrophy type 1 and epithelial-to-mesenchymal transition, as well as splicing changes in genes related to proposed mechanisms of FECD pathogenesis. We report the first instance of RNA toxicity and missplicing in a common non-neurological/neuromuscular disease associated with a repeat expansion. The FECD patient population with this (CTG·CAG)n trinucleotide repeat expansion exceeds that of the combined number of patients in all other microsatellite expansion disorders., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

14. Mechanism of Action of 2-Aminobenzamide HDAC Inhibitors in Reversing Gene Silencing in Friedreich's Ataxia.

Author

Soragni E, Chou CJ, Rusche JR, and Gottesfeld JM

Abstract

The genetic defect in Friedreich's ataxia (FRDA) is the hyperexpansion of a GAA•TTC triplet in the first intron of the FXN gene, encoding the essential mitochondrial protein frataxin. Histone post-translational modifications near the expanded repeats are consistent with heterochromatin formation and consequent FXN gene silencing. Using a newly developed human neuronal cell model, derived from patient-induced pluripotent stem cells, we find that 2-aminobenzamide histone deacetylase (HDAC) inhibitors increase FXN mRNA levels and frataxin protein in FRDA neuronal cells. However, only compounds targeting the class I HDACs 1 and 3 are active in increasing FXN mRNA in these cells. Structural analogs of the active HDAC inhibitors that selectively target either HDAC1 or HDAC3 do not show similar increases in FXN mRNA levels. To understand the mechanism of action of these compounds, we probed the kinetic properties of the active and inactive inhibitors, and found that only compounds that target HDACs 1 and 3 exhibited a slow-on/slow-off mechanism of action for the HDAC enzymes. HDAC1- and HDAC3-selective compounds did not show this activity. Using siRNA methods in the FRDA neuronal cells, we show increases in FXN mRNA upon silencing of either HDACs 1 or 3, suggesting the possibility that inhibition of each of these class I HDACs is necessary for activation of FXN mRNA synthesis, as there appears to be redundancy in the silencing mechanism caused by the GAA•TTC repeats. Moreover, inhibitors must have a long residence time on their target enzymes for this activity. By interrogating microarray data from neuronal cells treated with inhibitors of different specificity, we selected two genes encoding histone macroH2A (H2AFY2) and Polycomb group ring finger 2 (PCGF2) that were specifically down-regulated by the inhibitors targeting HDACs1 and 3 versus the more selective inhibitors for further investigation. Both genes are involved in transcriptional repression and we speculate their involvement in FXN gene silencing. Our results shed light on the mechanism whereby HDAC inhibitors increase FXN mRNA levels in FRDA neuronal cells.

Published

2015

15. Quantitative proteomic analysis identifies targets and pathways of a 2-aminobenzamide HDAC inhibitor in Friedreich's ataxia patient iPSC-derived neural stem cells.

Author

Shan B, Xu C, Zhang Y, Xu T, Gottesfeld JM, and Yates JR 3rd

Subjects

Humans, Induced Pluripotent Stem Cells metabolism, Mass Spectrometry, Molecular Probes metabolism, Molecular Probes pharmacology, Nuclear Proteins metabolism, Pyrazoles metabolism, Pyridinium Compounds metabolism, Friedreich Ataxia metabolism, Histone Deacetylase Inhibitors metabolism, Neural Stem Cells metabolism, Proteomics methods, Pyrazoles pharmacology, Pyridinium Compounds pharmacology, RNA Processing, Post-Transcriptional physiology, ortho-Aminobenzoates metabolism

Abstract

Members of the 2-aminobenzamide class of histone deacetylase (HDAC) inhibitors show promise as therapeutics for the neurodegenerative diseases Friedreich's ataxia (FRDA) and Huntington's disease (HD). While it is clear that HDAC3 is one of the important targets of the 2-aminobenzamide HDAC inhibitors, inhibition of other class I HDACs (HDACs 1 and 2) may also be involved in the beneficial effects of these compounds in FRDA and HD, and other HDAC interacting proteins may be impacted by the compound. To this end, we synthesized activity-based profiling probe (ABPP) versions of one of our HDAC inhibitors (compound 106), and in the present study we used a quantitative proteomic method coupled with multidimensional protein identification technology (MudPIT) to identify the proteins captured by the ABPP 106 probe. Nuclear proteins were extracted from FRDA patient iPSC-derived neural stem cells, and then were reacted with control and ABPP 106 probe. After reaction, the bound proteins were digested on the beads, and the peptides were modified using stable isotope-labeled formaldehyde to form dimethyl amine. The selectively bound proteins determined by mass spectrometry were subjected to functional and pathway analysis. Our findings suggest that the targets of compound 106 are involved not only in transcriptional regulation but also in posttranscriptional processing of mRNA.

Published

2014

16. Epigenetic therapy for Friedreich ataxia.

Author

Soragni E, Miao W, Iudicello M, Jacoby D, De Mercanti S, Clerico M, Longo F, Piga A, Ku S, Campau E, Du J, Penalver P, Rai M, Madara JC, Nazor K, O'Connor M, Maximov A, Loring JF, Pandolfo M, Durelli L, Gottesfeld JM, and Rusche JR

Subjects

Administration, Oral, Adolescent, Adult, Aminocaproates pharmacology, Aminocaproates therapeutic use, Area Under Curve, Benzamides pharmacology, Benzamides therapeutic use, Cell Differentiation drug effects, Cell Differentiation genetics, Cell Line, Transformed, Chromatin Immunoprecipitation, Cohort Studies, Cross-Sectional Studies, DNA Methylation drug effects, DNA Methylation genetics, Dose-Response Relationship, Drug, Double-Blind Method, Female, Friedreich Ataxia pathology, Gene Expression Regulation genetics, Humans, Leukocytes, Mononuclear drug effects, Leukocytes, Mononuclear metabolism, Male, Membrane Potentials drug effects, Membrane Potentials physiology, Middle Aged, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Neurons drug effects, Pluripotent Stem Cells, Trinucleotide Repeat Expansion genetics, Young Adult, Frataxin, Friedreich Ataxia drug therapy, Friedreich Ataxia genetics, Gene Expression Regulation drug effects, Histone Deacetylase Inhibitors therapeutic use, Iron-Binding Proteins genetics

Abstract

Objective: To investigate whether a histone deacetylase inhibitor (HDACi) would be effective in an in vitro model for the neurodegenerative disease Friedreich ataxia (FRDA) and to evaluate safety and surrogate markers of efficacy in a phase I clinical trial in patients., Methods: We used a human FRDA neuronal cell model, derived from patient induced pluripotent stem cells, to determine the efficacy of a 2-aminobenzamide HDACi (109) as a modulator of FXN gene expression and chromatin histone modifications. FRDA patients were dosed in 4 cohorts, ranging from 30mg/day to 240mg/day of the formulated drug product of HDACi 109, RG2833. Patients were monitored for adverse effects as well as for increases in FXN mRNA, frataxin protein, and chromatin modification in blood cells., Results: In the neuronal cell model, HDACi 109/RG2833 increases FXN mRNA levels and frataxin protein, with concomitant changes in the epigenetic state of the gene. Chromatin signatures indicate that histone H3 lysine 9 is a key residue for gene silencing through methylation and reactivation through acetylation, mediated by the HDACi. Drug treatment in FRDA patients demonstrated increased FXN mRNA and H3 lysine 9 acetylation in peripheral blood mononuclear cells. No safety issues were encountered., Interpretation: Drug exposure inducing epigenetic changes in neurons in vitro is comparable to the exposure required in patients to see epigenetic changes in circulating lymphoid cells and increases in gene expression. These findings provide a proof of concept for the development of an epigenetic therapy for this fatal neurological disease., (© 2014 American Neurological Association.)

Published

2014

17. Introduction to thematic minireview series: Development of human therapeutics based on induced pluripotent stem cell (iPSC) technology.

Author

Rao M and Gottesfeld JM

Subjects

Drug Evaluation, Preclinical, Humans, Induced Pluripotent Stem Cells cytology, Stem Cell Transplantation

Abstract

With the advent of human induced pluripotent stem cell (hiPSC) technology, it is now possible to derive patient-specific cell lines that are of great potential in both basic research and the development of new therapeutics for human diseases. Not only do hiPSCs offer unprecedented opportunities to study cellular differentiation and model human diseases, but the differentiated cell types obtained from iPSCs may become therapeutics themselves. These cells can also be used in the screening of therapeutics and in toxicology assays for potential liabilities of therapeutic agents. The remarkable achievement of transcription factor reprogramming to generate iPSCs was recognized by the award of the Nobel Prize in Medicine to Shinya Yamanaka in 2012, just 6 years after the first publication of reprogramming methods to generate hiPSCs (Takahashi, K., Tanabe, K., Ohnuki, M., Narita, M., Ichisaka, T., Tomoda, K., and Yamanaka, S. (2007) Cell 131, 861-872). This minireview series highlights both the promises and challenges of using iPSC technology for disease modeling, drug screening, and the development of stem cell therapeutics.

Published

2014

18. Length-dependent CTG·CAG triplet-repeat expansion in myotonic dystrophy patient-derived induced pluripotent stem cells.

Author

Du J, Campau E, Soragni E, Jespersen C, and Gottesfeld JM

Subjects

3' Untranslated Regions genetics, Cell Culture Techniques, DNA-Binding Proteins biosynthesis, DNA-Binding Proteins genetics, Fibroblasts metabolism, Fibroblasts pathology, Gene Expression Regulation, Humans, Huntington Disease genetics, Huntington Disease pathology, MutS Homolog 2 Protein biosynthesis, MutS Homolog 2 Protein genetics, MutS Homolog 3 Protein, Myotonic Dystrophy pathology, Myotonin-Protein Kinase, Pluripotent Stem Cells pathology, Myotonic Dystrophy genetics, Pluripotent Stem Cells metabolism, Protein Serine-Threonine Kinases genetics, Trinucleotide Repeat Expansion genetics

Abstract

Myotonic dystrophy type 1 (DM1) is an inherited dominant muscular dystrophy caused by expanded CTG·CAG triplet repeats in the 3' untranslated region of the DMPK1 gene, which produces a toxic gain-of-function CUG RNA. It has been shown that the severity of disease symptoms, age of onset and progression are related to the length of the triplet repeats. However, the mechanism(s) of CTG·CAG triplet-repeat instability is not fully understood. Herein, induced pluripotent stem cells (iPSCs) were generated from DM1 and Huntington's disease patient fibroblasts. We isolated 41 iPSC clones from DM1 fibroblasts, all showing different CTG·CAG repeat lengths, thus demonstrating somatic instability within the initial fibroblast population. During propagation of the iPSCs, the repeats expanded in a manner analogous to the expansion seen in somatic cells from DM1 patients. The correlation between repeat length and expansion rate identified the interval between 57 and 126 repeats as being an important length threshold where expansion rates dramatically increased. Moreover, longer repeats showed faster triplet-repeat expansion. However, the overall tendency of triplet repeats to expand ceased on differentiation into differentiated embryoid body or neurospheres. The mismatch repair components MSH2, MSH3 and MSH6 were highly expressed in iPSCs compared with fibroblasts, and only occupied the DMPK1 gene harboring longer CTG·CAG triplet repeats. In addition, shRNA silencing of MSH2 impeded CTG·CAG triplet-repeat expansion. The information gained from these studies provides new insight into a general mechanism of triplet-repeat expansion in iPSCs.

Published

2013

19. Increasing frataxin gene expression with histone deacetylase inhibitors as a therapeutic approach for Friedreich's ataxia.

Author

Gottesfeld JM, Rusche JR, and Pandolfo M

Subjects

Animals, Clinical Trials as Topic, Gene Silencing, Heterochromatin metabolism, Histone Deacetylase Inhibitors chemistry, Humans, Iron-Binding Proteins drug effects, Mice, Structure-Activity Relationship, Frataxin, Gene Expression physiology, Histone Deacetylase Inhibitors therapeutic use, Iron-Binding Proteins biosynthesis, Iron-Binding Proteins genetics

Abstract

The genetic defect in Friedreich's ataxia (FRDA) is the expansion of a GAA·TCC triplet in the first intron of the FXN gene, which encodes the mitochondrial protein frataxin. Previous studies have established that the repeats reduce transcription of this essential gene, with a concomitant decrease in frataxin protein in affected individuals. As the repeats do not alter the FXN protein coding sequence, one therapeutic approach would be to increase transcription of pathogenic FXN genes. Histone posttranslational modifications near the expanded repeats are consistent with heterochromatin formation and FXN gene silencing. In an effort to find small molecules that would reactivate this silent gene, histone deacetylase inhibitors were screened for their ability to up-regulate FXN gene expression in patient cells and members of the pimelic 2-aminobenzamide family of class I histone deacetylase inhibitors were identified as potent inducers of FXN gene expression and frataxin protein. Importantly, these molecules up-regulate FXN expression in human neuronal cells derived from patient-induced pluripotent stem cells and in two mouse models for the disease. Preclinical studies of safety and toxicity have been completed for one such compound and a phase I clinical trial in FRDA patients has been initiated. Furthermore, medicinal chemistry efforts have identified improved compounds with superior pharmacological properties., (© 2013 International Society for Neurochemistry.)

Published

2013

20. Minireview series on sirtuins: from biochemistry to health and disease.

Author

Denu JM and Gottesfeld JM

Subjects

Acetylation, Animals, Biocatalysis, Humans, Mice, Mitochondria metabolism, Disease, Health, Review Literature as Topic, Sirtuins metabolism

Published

2012

21. Rationale for the development of 2-aminobenzamide histone deacetylase inhibitors as therapeutics for Friedreich ataxia.

Author

Soragni E, Xu C, Plasterer HL, Jacques V, Rusche JR, and Gottesfeld JM

Subjects

Animals, Clinical Trials, Phase I as Topic, Disease Models, Animal, Fluorescent Dyes, Friedreich Ataxia genetics, Humans, Iron-Binding Proteins genetics, Iron-Binding Proteins metabolism, Mice, Mutation genetics, Proteomics, Trinucleotide Repeat Expansion genetics, ortho-Aminobenzoates, Frataxin, Friedreich Ataxia drug therapy, Friedreich Ataxia enzymology, Gene Expression Regulation drug effects, Histone Deacetylase Inhibitors therapeutic use

Abstract

Numerous studies have pointed to histone deacetylase inhibitors as potential therapeutics for various neurodegenerative diseases, and clinical trials with several histone deacetylase inhibitors have been performed or are under way. However, histone deacetylase inhibitors tested to date either are highly cytotoxic or have very low specificities for different histone deacetylase enzymes. The authors' laboratories have identified a novel class of histone deacetylase inhibitors (2-aminobenzamides) that reverses heterochromatin-mediated silencing of the frataxin (FXN) gene in Friedreich ataxia. The authors have identified the histone deacetylase enzyme isotype target of these compounds and present evidence that compounds that target this enzyme selectively increase FXN expression from pathogenic alleles. Studies with model compounds show that these histone deacetylase inhibitors increase FXN messenger RNA levels in the brain in mouse models for Friedreich ataxia and relieve neurological symptoms observed in mouse models and support the notion that this class of molecules may serve as therapeutics for the human disease.

Published

2012

22. Role of mismatch repair enzymes in GAA·TTC triplet-repeat expansion in Friedreich ataxia induced pluripotent stem cells.

Author

Du J, Campau E, Soragni E, Ku S, Puckett JW, Dervan PB, and Gottesfeld JM

Subjects

Animals, Cell Differentiation genetics, Cell Line, Fibroblasts metabolism, Fibroblasts pathology, Friedreich Ataxia genetics, Friedreich Ataxia pathology, Humans, Induced Pluripotent Stem Cells pathology, Introns genetics, Iron-Binding Proteins genetics, Kruppel-Like Factor 4, Mice, MutS Homolog 2 Protein genetics, Neural Stem Cells metabolism, Neural Stem Cells pathology, Spheroids, Cellular metabolism, Spheroids, Cellular pathology, Transcription Factors genetics, Transcription Factors metabolism, Frataxin, DNA Mismatch Repair, Friedreich Ataxia metabolism, Genome, Human, Induced Pluripotent Stem Cells metabolism, Iron-Binding Proteins metabolism, Models, Biological, MutS Homolog 2 Protein metabolism, Trinucleotide Repeat Expansion

Abstract

The genetic mutation in Friedreich ataxia (FRDA) is a hyperexpansion of the triplet-repeat sequence GAA·TTC within the first intron of the FXN gene. Although yeast and reporter construct models for GAA·TTC triplet-repeat expansion have been reported, studies on FRDA pathogenesis and therapeutic development are limited by the availability of an appropriate cell model in which to study the mechanism of instability of the GAA·TTC triplet repeats in the human genome. Herein, induced pluripotent stem cells (iPSCs) were generated from FRDA patient fibroblasts after transduction with the four transcription factors Oct4, Sox2, Klf4, and c-Myc. These cells were differentiated into neurospheres and neuronal precursors in vitro, providing a valuable cell model for FRDA. During propagation of the iPSCs, GAA·TTC triplet repeats expanded at a rate of about two GAA·TTC triplet repeats/replication. However, GAA·TTC triplet repeats were stable in FRDA fibroblasts and neuronal stem cells. The mismatch repair enzymes MSH2, MSH3, and MSH6, implicated in repeat instability in other triplet-repeat diseases, were highly expressed in pluripotent stem cells compared with fibroblasts and neuronal stem cells and occupied FXN intron 1. In addition, shRNA silencing of MSH2 and MSH6 impeded GAA·TTC triplet-repeat expansion. A specific pyrrole-imidazole polyamide targeting GAA·TTC triplet-repeat DNA partially blocked repeat expansion by displacing MSH2 from FXN intron 1 in FRDA iPSCs. These studies suggest that in FRDA, GAA·TTC triplet-repeat instability occurs in embryonic cells and involves the highly active mismatch repair system.

Published

2012

23. Chromatin structure determines accessibility of a hairpin polyamide-chlorambucil conjugate at histone H4 genes in pancreatic cancer cells.

Author

Jespersen C, Soragni E, James Chou C, Arora PS, Dervan PB, and Gottesfeld JM

Subjects

Acetylation, Antineoplastic Agents, Alkylating pharmacology, Cell Cycle Checkpoints drug effects, Cell Cycle Checkpoints genetics, Cell Line, Tumor, Chlorambucil pharmacology, Chromatin ultrastructure, Chromatin Immunoprecipitation, Down-Regulation, HEK293 Cells, Humans, Imidazoles chemistry, Nylons pharmacology, Organ Specificity, Pancreatic Neoplasms, Pyrroles chemistry, RNA, Messenger antagonists & inhibitors, RNA, Messenger biosynthesis, Transcription, Genetic drug effects, Antineoplastic Agents, Alkylating chemistry, Chlorambucil chemistry, Chromatin metabolism, Histones genetics, Nylons chemistry

Abstract

We have shown that a specific pyrrole-imidazole polyamide-DNA alkylator (chlorambucil) conjugate, 1R-Chl, alters the growth characteristics of various cancer cell lines in culture, and causes these cells to arrest in the G2/M stage of the cell cycle, without apparent cytotoxicity. This molecule has also shown efficacy in several mouse xenograft models, preventing tumor growth. Previous microarray studies have suggested that members of the histone H4 gene family, H4c and H4j/k, are the primary targets of this molecule, leading to reduced histone mRNA synthesis and growth arrest in cancer cells. In the present study, we examine the effects of 1R-Chl on transcription of other members of the H4 gene family, with the result that mRNA transcription of most genomic copies of H4 are down-regulated by 1R-Chl in a human pancreatic cancer cell line (MIA PaCa-2), but not in a cell line of non-cancerous origin (HEK293 cells). The basis for this differential effect is likely an open chromatin conformation within the H4 genes in cancer cells. Chromatin immunoprecipitation experiments show increased histone acetylation on the histone H4 genes in cancer cells, compared to HEK293 cells, explaining the differential activity of this molecule in cancer versus non-cancer cells., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

24. Histone deacetylase (HDAC) inhibitors targeting HDAC3 and HDAC1 ameliorate polyglutamine-elicited phenotypes in model systems of Huntington's disease.

Author

Jia H, Pallos J, Jacques V, Lau A, Tang B, Cooper A, Syed A, Purcell J, Chen Y, Sharma S, Sangrey GR, Darnell SB, Plasterer H, Sadri-Vakili G, Gottesfeld JM, Thompson LM, Rusche JR, Marsh JL, and Thomas EA

Subjects

Animals, Cells, Cultured, Drosophila melanogaster, Drug Delivery Systems methods, HCT116 Cells, Histone Deacetylase 1 metabolism, Humans, Huntington Disease drug therapy, Mice, Mice, Inbred C57BL, Mice, Inbred CBA, Mice, Transgenic, Disease Models, Animal, Histone Deacetylase 1 antagonists & inhibitors, Histone Deacetylase Inhibitors administration & dosage, Histone Deacetylases metabolism, Huntington Disease enzymology, Huntington Disease genetics, Peptides physiology, Phenotype

Abstract

We have previously demonstrated amelioration of Huntington's disease (HD)-related phenotypes in R6/2 transgenic mice in response to treatment with the novel histone deacetylase (HDAC) inhibitor 4b. Here we have measured the selectivity profiles of 4b and related compounds against class I and class II HDACs and have tested their ability to restore altered expression of genes related to HD pathology in mice and to rescue disease effects in cell culture and Drosophila models of HD. R6/2 transgenic and wild-type (wt) mice received daily injections of HDAC inhibitors for 3 days followed by real-time PCR analysis to detect expression differences for 13 HD-related genes. We find that HDACi 4b and 136, two compounds showing high potency for inhibiting HDAC3 were most effective in reversing the expression of genes relevant to HD, including Ppp1r1b, which encodes DARPP-32, a marker for medium spiny striatal neurons. In contrast, compounds targeting HDAC1 were less effective at correcting gene expression abnormalities in R6/2 transgenic mice, but did cause significant increases in the expression of selected genes. An additional panel of 4b-related compounds was tested in a Drosophila model of HD and in STHdhQ111 striatal cells to further distinguish HDAC selectivity. Significant improvement in huntingtin-elicited Drosophila eye neurodegeneration in the fly was observed in response to treatment with compounds targeting human HDAC1 and/or HDAC3. In STHdhQ111 striatal cells, the ability of HDAC inhibitors to improve huntingtin-elicited metabolic deficits correlated with the potency at inhibiting HDAC1 and HDAC3, although the IC50 values for HDAC1 inhibition were typically 10-fold higher than for inhibition of HDAC3. Assessment of HDAC protein localization in brain tissue by Western blot analysis revealed accumulation of HDAC1 and HDAC3 in the nucleus of HD transgenic mice compared to wt mice, with a concurrent decrease in cytoplasmic localization, suggesting that these HDACs contribute to a repressive chromatin environment in HD. No differences were detected in the localization of HDAC2, HDAC4 or HDAC7. These results suggest that inhibition of HDACs 1 and 3 can relieve HD-like phenotypes in model systems and that HDAC inhibitors targeting these isotypes might show therapeutic benefit in human HD.

Published

2012

25. Improved Histone Deacetylase Inhibitors as Therapeutics for the Neurodegenerative Disease Friedreich's Ataxia: A New Synthetic Route.

Author

Xu C, Soragni E, Jacques V, Rusche JR, and Gottesfeld JM

Abstract

Friedreich's ataxia (FRDA) is caused by transcriptional repression of the nuclear FXN gene encoding the essential mitochondrial protein frataxin. Based on the hypothesis that the acetylation state of the histone proteins is responsible for gene silencing in FRDA, previous work in our lab identified a first generation of HDAC inhibitors (pimelic o-aminobenzamides), which increase FXN mRNA in lymphocytes from FRDA patients. Importantly, these compounds also function in a FRDA mouse model to increase FXN mRNA levels in the brain and heart. While the first generation of HDAC inhibitors hold promise as potential therapeutics for FRDA, they have two potential problems: less than optimal brain penetration and metabolic instability in acidic conditions. Extensive optimization focusing on modifying the left benzene ring, linker and the right benzene ring lead to a novel class of HDAC inhibitors that have optimized pharmacological properties (increased brain penetration and acid stability) compared to the previous HDAC inhibitors. This article will describe the chemical synthesis and pharmacological properties of these new HDAC inhibitors.

Published

2011

26. A gene expression phenotype in lymphocytes from Friedreich ataxia patients.

Author

Coppola G, Burnett R, Perlman S, Versano R, Gao F, Plasterer H, Rai M, Saccá F, Filla A, Lynch DR, Rusche JR, Gottesfeld JM, Pandolfo M, and Geschwind DH

Subjects

Adult, Cell Culture Techniques, Female, Friedreich Ataxia genetics, Gene Expression, Humans, Iron-Binding Proteins genetics, Leukocytes, Mononuclear cytology, Male, Phenotype, Real-Time Polymerase Chain Reaction, Frataxin, Friedreich Ataxia metabolism, Iron-Binding Proteins drug effects, Leukocytes, Mononuclear metabolism

Abstract

Objective: Gene expression studies in peripheral tissues from patients with neurodegenerative disorders can provide insights into disease pathogenesis, and identify potential biomarkers, an important goal of translational research in neurodegeneration. Friedreich Ataxia (FRDA) is a chronic neurodegenerative disease caused by reduced transcription of frataxin, a ubiquitously expressed protein. We studied in vitro lymphocytes from FRDA patients and carriers to identify a peripheral gene expression phenotype. Peripheral biomarkers related to disease status would be extremely valuable for assessing drug efficacy and could provide new pathophysiological insights., Methods: We characterized the gene expression profiles in peripheral blood mononuclear cells (PBMCs) from FRDA patients, compared with controls and related carriers. Cells were studied both before and after in vitro treatment with compounds that increase frataxin levels. Quantitative real-time polymerase chain reaction and additional microarrays were used to confirm a core set of genes in multiple independent series., Results: We identified a subset of genes changed in cells from patients with pathological frataxin deficiency, and a core set of these genes were confirmed in independent series. Changes in gene expression were related to the mitochondria, lipid metabolism, cell cycle, and DNA repair, consistent with FRDA's known pathophysiology. We evaluated the in vitro effect of multiple compounds (histone deacetylase inhibitors) on this putative biomarker set, and found that this biochemical phenotype was ameliorated in accordance with drug efficacy., Interpretation: Frataxin downregulation is associated with robust changes in gene expression in PBMCs, providing pathogenetic insights and a core subset of genes that, if verified in vivo, could be used as a peripheral biomarker., (Copyright © 2011 American Neurological Association.)

Published

2011

27. Prolonged treatment with pimelic o-aminobenzamide HDAC inhibitors ameliorates the disease phenotype of a Friedreich ataxia mouse model.

Author

Sandi C, Pinto RM, Al-Mahdawi S, Ezzatizadeh V, Barnes G, Jones S, Rusche JR, Gottesfeld JM, and Pook MA

Subjects

Aconitate Hydratase metabolism, Analysis of Variance, Animals, Benzamides pharmacology, Benzamides therapeutic use, Blotting, Western, Body Weight drug effects, Body Weight physiology, Chromatin Immunoprecipitation, Disease Models, Animal, Exploratory Behavior drug effects, Exploratory Behavior physiology, Friedreich Ataxia genetics, Friedreich Ataxia physiopathology, Histone Deacetylase Inhibitors pharmacology, Mice, Motor Activity physiology, Phenotype, Reverse Transcriptase Polymerase Chain Reaction, Rotarod Performance Test, Friedreich Ataxia drug therapy, Histone Deacetylase Inhibitors therapeutic use, Motor Activity drug effects

Abstract

Friedreich ataxia (FRDA) is an inherited neurodegenerative disorder caused by GAA repeat expansion within the FXN gene, leading to epigenetic changes and heterochromatin-mediated gene silencing that result in a frataxin protein deficit. Histone deacetylase (HDAC) inhibitors, including pimelic o-aminobenzamide compounds 106, 109 and 136, have previously been shown to reverse FXN gene silencing in short-term studies of FRDA patient cells and a knock-in mouse model, but the functional consequences of such therapeutic intervention have thus far not been described. We have now investigated the long-term therapeutic effects of 106, 109 and 136 in our GAA repeat expansion mutation-containing YG8R FRDA mouse model. We show that there is no overt toxicity up to 5 months of treatment and there is amelioration of the FRDA-like disease phenotype. Thus, while the neurological deficits of this model are mild, 109 and 106 both produced an improvement of motor coordination, whereas 109 and 136 produced increased locomotor activity. All three compounds increased global histone H3 and H4 acetylation of brain tissue, but only 109 significantly increased acetylation of specific histone residues at the FXN locus. Effects on FXN mRNA expression in CNS tissues were modest, but 109 significantly increased frataxin protein expression in brain tissue. 109 also produced significant increases in brain aconitase enzyme activity, together with reduction of neuronal pathology of the dorsal root ganglia (DRG). Overall, these results support further assessment of HDAC inhibitors for treatment of Friedreich ataxia., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

28. Introduction to the thematic minireview series on epigenetics.

Author

Gottesfeld JM

Subjects

Animals, Humans, Epigenomics, Gene Expression Regulation physiology, Genome, Human physiology

Published

2011

29. Evaluation of histone deacetylase inhibitors as therapeutics for neurodegenerative diseases.

Author

Soragni E, Xu C, Cooper A, Plasterer HL, Rusche JR, and Gottesfeld JM

Subjects

Acetylation drug effects, Blotting, Western, Cell Line, Cell Proliferation drug effects, Cell Separation, Chromatin metabolism, Chromatin Immunoprecipitation, Friedreich Ataxia genetics, Friedreich Ataxia metabolism, Gene Expression Regulation drug effects, Gene Silencing drug effects, Histones metabolism, Humans, Huntington Disease genetics, Huntington Disease metabolism, Iron-Binding Proteins genetics, Iron-Binding Proteins metabolism, Laboratories, Leukocytes, Mononuclear drug effects, Leukocytes, Mononuclear metabolism, Male, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Frataxin, Drug Evaluation, Preclinical methods, Friedreich Ataxia drug therapy, Histone Deacetylase Inhibitors pharmacology, Histone Deacetylase Inhibitors therapeutic use, Histone Deacetylases metabolism, Huntington Disease drug therapy

Abstract

Various neurodegenerative diseases are associated with aberrant gene expression. We recently identified a novel class of pimelic o-aminobenzamide histone deacetylase (HDAC) inhibitors that show promise as therapeutics in the neurodegenerative diseases Friedreich's ataxia (FRDA) and Huntington's disease (HD). Here, we describe the various techniques used in our laboratories to dissect mechanisms of gene silencing in FRDA and HD, and to test our HDAC inhibitors for their ability to reverse changes in gene expression in cellular models.

Published

2011

30. Friedreich's ataxia induced pluripotent stem cells model intergenerational GAA⋅TTC triplet repeat instability.

Author

Ku S, Soragni E, Campau E, Thomas EA, Altun G, Laurent LC, Loring JF, Napierala M, and Gottesfeld JM

Subjects

Cells, Cultured, DNA Repeat Expansion, Humans, Iron-Binding Proteins genetics, Microsatellite Instability, Frataxin, Friedreich Ataxia genetics, Induced Pluripotent Stem Cells, Trinucleotide Repeat Expansion genetics

Abstract

The inherited neurodegenerative disease Friedreich's ataxia (FRDA) is caused by GAA⋅TTC triplet repeat hyperexpansions within the first intron of the FXN gene, encoding the mitochondrial protein frataxin. Long GAA⋅TTC repeats cause heterochromatin-mediated gene silencing and loss of frataxin in affected individuals. We report the derivation of induced pluripotent stem cells (iPSCs) from FRDA patient fibroblasts by transcription factor reprogramming. FXN gene repression is maintained in the iPSCs, as are the global gene expression signatures reflecting the human disease. GAA⋅TTC repeats uniquely in FXN in the iPSCs exhibit repeat instability similar to patient families, where they expand and/or contract with discrete changes in length between generations. The mismatch repair enzyme MSH2, implicated in repeat instability in other triplet repeat diseases, is highly expressed in pluripotent cells and occupies FXN intron 1, and shRNA silencing of MSH2 impedes repeat expansion, providing a possible molecular explanation for repeat expansion in FRDA., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

31. Chemical biology meets biological chemistry minireview series.

Author

Cravatt BF and Gottesfeld JM

Subjects

Animals, Biology methods, Chemistry methods, Humans, Biochemistry methods

Published

2010

32. Two new pimelic diphenylamide HDAC inhibitors induce sustained frataxin upregulation in cells from Friedreich's ataxia patients and in a mouse model.

Author

Rai M, Soragni E, Chou CJ, Barnes G, Jones S, Rusche JR, Gottesfeld JM, and Pandolfo M

Subjects

Animals, Base Sequence, DNA Primers, Humans, Mice, Polymerase Chain Reaction, Frataxin, Disease Models, Animal, Friedreich Ataxia genetics, Histone Deacetylase Inhibitors pharmacology, Iron-Binding Proteins genetics, Models, Animal, Pimelic Acids pharmacology, Up-Regulation drug effects

Abstract

Background: Friedreich's ataxia (FRDA), the most common recessive ataxia in Caucasians, is due to severely reduced levels of frataxin, a highly conserved protein, that result from a large GAA triplet repeat expansion within the first intron of the frataxin gene (FXN). Typical marks of heterochromatin are found near the expanded GAA repeat in FRDA patient cells and mouse models. Histone deacetylase inhibitors (HDACIs) with a pimelic diphenylamide structure and HDAC3 specificity can decondense the chromatin structure at the FXN gene and restore frataxin levels in cells from FRDA patients and in a GAA repeat based FRDA mouse model, KIKI, providing an appealing approach for FRDA therapeutics., Methodology/principal Findings: In an effort to further improve the pharmacological profile of pimelic diphenylamide HDACIs as potential therapeutics for FRDA, we synthesized additional compounds with this basic structure and screened them for HDAC3 specificity. We characterized two of these compounds, 136 and 109, in FRDA patients' peripheral blood lymphocytes and in the KIKI mouse model. We tested their ability to upregulate frataxin at a range of concentrations in order to determine a minimal effective dose. We then determined in both systems the duration of effect of these drugs on frataxin mRNA and protein, and on total and local histone acetylation. The effects of these compounds exceeded the time of direct exposure in both systems., Conclusions/significance: Our results support the pre-clinical development of a therapeutic approach based on pimelic diphenylamide HDACIs for FRDA and provide information for the design of future human trials of these drugs, suggesting an intermittent administration of the drug.

Published

2010

33. Reduced histone deacetylase 7 activity restores function to misfolded CFTR in cystic fibrosis.

Author

Hutt DM, Herman D, Rodrigues AP, Noel S, Pilewski JM, Matteson J, Hoch B, Kellner W, Kelly JW, Schmidt A, Thomas PJ, Matsumura Y, Skach WR, Gentzsch M, Riordan JR, Sorscher EJ, Okiyoneda T, Yates JR 3rd, Lukacs GL, Frizzell RA, Manning G, Gottesfeld JM, and Balch WE

Subjects

Animals, Bronchi metabolism, Cell Membrane metabolism, Cricetinae, Epithelial Cells metabolism, Gene Silencing, Humans, Hydroxamic Acids chemistry, Protein Denaturation, Protein Folding, RNA, Small Interfering metabolism, Vorinostat, Cystic Fibrosis metabolism, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Histone Deacetylases metabolism, Mutation

Abstract

Chemical modulation of histone deacetylase (HDAC) activity by HDAC inhibitors (HDACi) is an increasingly important approach for modifying the etiology of human disease. Loss-of-function diseases arise as a consequence of protein misfolding and degradation, which lead to system failures. The DeltaF508 mutation in cystic fibrosis transmembrane conductance regulator (CFTR) results in the absence of the cell surface chloride channel and a loss of airway hydration, leading to the premature lung failure and reduced lifespan responsible for cystic fibrosis. We now show that the HDACi suberoylanilide hydroxamic acid (SAHA) restores surface channel activity in human primary airway epithelia to levels that are 28% of those of wild-type CFTR. Biological silencing of all known class I and II HDACs reveals that HDAC7 plays a central role in restoration of DeltaF508 function. We suggest that the tunable capacity of HDACs can be manipulated by chemical biology to counter the onset of cystic fibrosis and other human misfolding disorders.

Published

2010

34. Potent activity against K562 cells by polyamide-seco-CBI conjugates targeting histone H4 genes.

Author

Minoshima M, Chou JC, Lefebvre S, Bando T, Shinohara K, Gottesfeld JM, and Sugiyama H

Subjects

Antineoplastic Agents, Alkylating chemical synthesis, Antineoplastic Agents, Alkylating chemistry, Apoptosis drug effects, DNA metabolism, Gene Expression Regulation, Neoplastic drug effects, Humans, Imidazoles chemical synthesis, Imidazoles chemistry, K562 Cells, Leukemia, Erythroblastic, Acute drug therapy, Nylons chemical synthesis, Nylons chemistry, Pyrroles chemical synthesis, Pyrroles chemistry, Antineoplastic Agents, Alkylating pharmacology, Genes drug effects, Histones genetics, Imidazoles pharmacology, Nylons pharmacology, Pyrroles pharmacology

Abstract

We designed and synthesized conjugates between pyrrole-imidazole polyamides and seco-CBI that alkylate within the coding regions of the histone H4 genes. DNA alkylating activity on the histone H4 fragment and cellular effects against K562 chronic myelogenous leukemia cells were investigated. One of the conjugates, 5-CBI, showed strong DNA alkylation activity and good sequence specificity on a histone H4 gene fragment. K562 cells treated with 5-CBI down-regulated the histone H4 gene and induced apoptosis efficiently. Global gene expression data revealed that a number of histone H4 genes were down-regulated by 5-CBI treatment. These results suggest that sequence-specific DNA alkylating agents may have the potential of targeting specific genes for cancer chemotherapy., (Copyright (c) 2009 Elsevier Ltd. All rights reserved.)

Published

2010

35. Development of histone deacetylase inhibitors as therapeutics for neurological disease.

Author

Gottesfeld JM and Pandolfo M

Abstract

Postsynthetic modifications of histone and other chromosomal proteins by reversible acetylation and/or methylation regulate many aspects of chromatin dynamics, such as transcription, replication and DNA repair. Aberrant modification states are associated with several neurological and neuromotor diseases. Thus, small molecules that inhibit or activate the enzymes responsible for these chromatin modifications have received considerable attention as potential human therapeutics. This paper summarizes the current state of development of histone deacetylase inhibitors in a variety of neurological diseases.

Published

2009

36. Chemical probes identify a role for histone deacetylase 3 in Friedreich's ataxia gene silencing.

Author

Xu C, Soragni E, Chou CJ, Herman D, Plasterer HL, Rusche JR, and Gottesfeld JM

Subjects

Animals, Cell Line, Drug Design, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Friedreich Ataxia genetics, Histone Deacetylase 1 antagonists & inhibitors, Histone Deacetylase 1 metabolism, Histone Deacetylase 2 antagonists & inhibitors, Histone Deacetylase 2 metabolism, Histone Deacetylase Inhibitors pharmacology, Histone Deacetylases metabolism, Humans, Iron-Binding Proteins genetics, Iron-Binding Proteins metabolism, Mice, Neuroprotective Agents chemistry, Neuroprotective Agents pharmacology, Photoaffinity Labels chemistry, Pimelic Acids chemistry, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins metabolism, Frataxin, Friedreich Ataxia enzymology, Gene Silencing, Histone Deacetylases physiology, Pimelic Acids pharmacology

Abstract

We recently identified a class of pimelic diphenylamide histone deacetylase (HDAC) inhibitors that show promise as therapeutics in the neurodegenerative diseases Friedreich's ataxia (FRDA) and Huntington's disease. Here, we describe chemical approaches to identify the HDAC enzyme target of these inhibitors. Incubation of a trifunctional activity-based probe with a panel of class I and class II recombinant HDAC enzymes, followed by click chemistry addition of a fluorescent dye and gel electrophoresis, identifies HDAC3 as a unique high-affinity target of the probe. Photoaffinity labeling in a nuclear extract prepared from human lymphoblasts with the trifunctional probe, followed by biotin addition through click chemistry, streptavidin enrichment, and Western blotting also identifies HDAC3 as the preferred cellular target of the inhibitor. Additional inhibitors with different HDAC specificity profiles were synthesized, and results from transcription experiments in FRDA cells point to a unique role for HDAC3 in gene silencing in Friedreich's ataxia.

Published

2009

37. Design and synthesis of novel hybrid benzamide-peptide histone deacetylase inhibitors.

Author

Hu F, Chou CJ, and Gottesfeld JM

Subjects

Cyclization, Drug Design, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Histone Deacetylase 1, Histone Deacetylases metabolism, Humans, Neuroprotective Agents chemistry, Neuroprotective Agents pharmacology, Peptides chemical synthesis, Benzamides chemistry, Enzyme Inhibitors chemical synthesis, Histone Deacetylase Inhibitors, Neuroprotective Agents chemical synthesis, Peptides chemistry

Abstract

We designed and synthesized a series of novel hybrid histone deacetylase inhibitors based on conjugation of benzamide-type inhibitors with either linear or cyclic peptides. Linear tetrapeptides (compounds 13 and 14), cyclic tetrapeptides (compounds 1 and 11), and heptanediamide-peptide conjugates (compounds 10, 12, 15 and 16) were synthesized through on-resin solid-phase peptide synthesis (SPPS). All compounds were found to be moderate HDAC1 and HDAC3 inhibitors, with IC(50) values ranging from 1.3 microM to 532 microM. Interestingly, compound 15 showed 19-fold selectivity for HDAC3 versus HDAC1.

Published

2009

38. Pimelic diphenylamide 106 is a slow, tight-binding inhibitor of class I histone deacetylases.

Author

Chou CJ, Herman D, and Gottesfeld JM

Subjects

Animals, Disease Models, Animal, Enzyme Inhibitors pharmacology, Friedreich Ataxia enzymology, Histone Deacetylases metabolism, Humans, Huntington Disease enzymology, Isoenzymes antagonists & inhibitors, Isoenzymes metabolism, Kinetics, Mice, Neoplasm Proteins metabolism, Neoplasms enzymology, Pimelic Acids pharmacology, Enzyme Inhibitors chemistry, Friedreich Ataxia drug therapy, Histone Deacetylase Inhibitors, Huntington Disease drug therapy, Neoplasm Proteins antagonists & inhibitors, Neoplasms drug therapy, Pimelic Acids chemistry

Abstract

Histone deacetylase (HDAC) inhibitors, including various benzamides and hydroxamates, are currently in clinical development for a broad range of human diseases, including cancer and neurodegenerative diseases. We recently reported the identification of a family of benzamide-type HDAC inhibitors that are relatively non-toxic compared with the hydroxamates. Members of this class of compounds have shown efficacy in cell-based and mouse models for the neurodegenerative diseases Friedreich ataxia and Huntington disease. Considerable differences in IC(50) values for the various HDAC enzymes have been reported for many of the HDAC inhibitors, leading to confusion as to the HDAC isotype specificities of these compounds. Here we show that a benzamide HDAC inhibitor, a pimelic diphenylamide (106), is a class I HDAC inhibitor, demonstrating no activity against class II HDACs. 106 is a slow, tight-binding inhibitor of HDACs 1, 2, and 3, although inhibition for these enzymes occurs through different mechanisms. Inhibitor 106 also has preference toward HDAC3 with K(i) of approximately 14 nm, 15 times lower than the K(i) for HDAC1. In comparison, the hydroxamate suberoylanilide hydroxamic acid does not discriminate between these enzymes and exhibits a fast-on/fast-off inhibitory mechanism. These observations may explain a paradox involving the relative activities of pimelic diphenylamides versus hydroxamates as gene activators.

Published

2008

39. Long intronic GAA*TTC repeats induce epigenetic changes and reporter gene silencing in a molecular model of Friedreich ataxia.

Author

Soragni E, Herman D, Dent SY, Gottesfeld JM, Wells RD, and Napierala M

Subjects

Cell Line, Genes, Reporter, Green Fluorescent Proteins genetics, Heterochromatin metabolism, Histones metabolism, Humans, Introns, Models, Genetic, Models, Molecular, Transcription, Genetic, Frataxin, DNA Repeat Expansion, Friedreich Ataxia genetics, Gene Silencing, Iron-Binding Proteins genetics

Abstract

Friedreich ataxia (FRDA) is caused by hyperexpansion of GAA*TTC repeats located in the first intron of the FXN gene, which inhibits transcription leading to the deficiency of frataxin. The FXN gene is an excellent target for therapeutic intervention since (i) 98% of patients carry the same type of mutation, (ii) the mutation is intronic, thus leaving the FXN coding sequence unaffected and (iii) heterozygous GAA*TTC expansion carriers with approximately 50% decrease of the frataxin are asymptomatic. The discovery of therapeutic strategies for FRDA is hampered by a lack of appropriate molecular models of the disease. Herein, we present the development of a new cell line as a molecular model of FRDA by inserting 560 GAA*TTC repeats into an intron of a GFP reporter minigene. The GFP&#95;(GAA*TTC)(560) minigene recapitulates the molecular hallmarks of the mutated FXN gene, i.e. inhibition of transcription of the reporter gene, decreased levels of the reporter protein and hypoacetylation and hypermethylation of histones in the vicinity of the repeats. Additionally, selected histone deacetylase inhibitors, known to stimulate the FXN gene expression, increase the expression of the GFP&#95;(GAA*TTC)(560) reporter. This FRDA model can be adapted to high-throughput analyses in a search for new therapeutics for the disease.

Published

2008

40. The HDAC inhibitor 4b ameliorates the disease phenotype and transcriptional abnormalities in Huntington's disease transgenic mice.

Author

Thomas EA, Coppola G, Desplats PA, Tang B, Soragni E, Burnett R, Gao F, Fitzgerald KM, Borok JF, Herman D, Geschwind DH, and Gottesfeld JM

Subjects

Anilides administration & dosage, Anilides chemical synthesis, Animals, Chromatin Immunoprecipitation, Disease Models, Animal, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors chemical synthesis, Histone Deacetylases metabolism, Huntington Disease drug therapy, Male, Mice, Mice, Transgenic, Neuroprotective Agents administration & dosage, Neuroprotective Agents chemical synthesis, Neuroprotective Agents pharmacology, Phenotype, Anilides pharmacology, Enzyme Inhibitors pharmacology, Histone Deacetylase Inhibitors, Huntington Disease genetics, Transcription, Genetic drug effects

Abstract

Transcriptional dysregulation has emerged as a core pathologic feature of Huntington's disease (HD), one of several triplet-repeat disorders characterized by movement deficits and cognitive dysfunction. Although the mechanisms contributing to the gene expression deficits remain unknown, therapeutic strategies have aimed to improve transcriptional output via modulation of chromatin structure. Recent studies have demonstrated therapeutic effects of commercially available histone deacetylase (HDAC) inhibitors in several HD models; however, the therapeutic value of these compounds is limited by their toxic effects. Here, beneficial effects of a novel pimelic diphenylamide HDAC inhibitor, HDACi 4b, in an HD mouse model are reported. Chronic oral administration of HDACi 4b, beginning after the onset of motor deficits, significantly improved motor performance, overall appearance, and body weight of symptomatic R6/2(300Q) transgenic mice. These effects were associated with significant attenuation of gross brain-size decline and striatal atrophy. Microarray studies revealed that HDACi 4b treatment ameliorated, in part, alterations in gene expression caused by the presence of mutant huntingtin protein in the striatum, cortex, and cerebellum of R6/2(300Q) transgenic mice. For selected genes, HDACi 4b treatment reversed histone H3 hypoacetylation observed in the presence of mutant huntingtin, in association with correction of mRNA expression levels. These findings suggest that HDACi 4b, and possibly related HDAC inhibitors, may offer clinical benefit for HD patients and provide a novel set of potential biomarkers for clinical assessment.

Published

2008

41. HDAC inhibitors correct frataxin deficiency in a Friedreich ataxia mouse model.

Author

Rai M, Soragni E, Jenssen K, Burnett R, Herman D, Coppola G, Geschwind DH, Gottesfeld JM, and Pandolfo M

Subjects

Acetylation drug effects, Animals, Cerebellum drug effects, Cerebellum metabolism, Chromatin metabolism, Enzyme Inhibitors pharmacology, Epigenesis, Genetic drug effects, Gene Expression Profiling, Histones metabolism, Introns genetics, Mice, Myocardium metabolism, Protein Processing, Post-Translational drug effects, RNA, Messenger genetics, RNA, Messenger metabolism, Frataxin, Disease Models, Animal, Enzyme Inhibitors therapeutic use, Friedreich Ataxia drug therapy, Histone Deacetylase Inhibitors, Iron-Binding Proteins genetics, Iron-Binding Proteins metabolism

Abstract

Background: Friedreich ataxia, an autosomal recessive neurodegenerative and cardiac disease, is caused by abnormally low levels of frataxin, an essential mitochondrial protein. All Friedreich ataxia patients carry a GAATTC repeat expansion in the first intron of the frataxin gene, either in the homozygous state or in compound heterozygosity with other loss-of-function mutations. The GAA expansion inhibits frataxin expression through a heterochromatin-mediated repression mechanism. Histone modifications that are characteristic of silenced genes in heterochromatic regions occur at expanded alleles in cells from Friedreich ataxia patients, including increased trimethylation of histone H3 at lysine 9 and hypoacetylation of histones H3 and H4., Methodology/principal Findings: By chromatin immunoprecipitation, we detected the same heterochromatin marks in homozygous mice carrying a (GAA)(230) repeat in the first intron of the mouse frataxin gene (KIKI mice). These animals have decreased frataxin levels and, by microarray analysis, show significant gene expression changes in several tissues. We treated KIKI mice with a novel histone deacetylase inhibitor, compound 106, which substantially increases frataxin mRNA levels in cells from Friedreich ataxia individuals. Treatment increased histone H3 and H4 acetylation in chromatin near the GAA repeat and restored wild-type frataxin levels in the nervous system and heart, as determined by quantitative RT-PCR and semiquantitative western blot analysis. No toxicity was observed. Furthermore, most of the differentially expressed genes in KIKI mice reverted towards wild-type levels., Conclusions/significance: Lack of acute toxicity, normalization of frataxin levels and of the transcription profile changes resulting from frataxin deficiency provide strong support to a possible efficacy of this or related compounds in reverting the pathological process in Friedreich ataxia, a so far incurable neurodegenerative disease.

Published

2008

42. Small molecules targeting histone H4 as potential therapeutics for chronic myelogenous leukemia.

Author

Chou CJ, Farkas ME, Tsai SM, Alvarez D, Dervan PB, and Gottesfeld JM

Subjects

Alkylation, Animals, Base Sequence, Blotting, Western, Cell Cycle drug effects, Cell Survival drug effects, Chlorambucil chemical synthesis, Chlorambucil chemistry, Female, Humans, Imidazoles chemistry, Mice, Mice, Nude, Molecular Sequence Data, Nylons chemical synthesis, Nylons chemistry, Pyrroles chemistry, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Cell Proliferation drug effects, Chlorambucil therapeutic use, Histones antagonists & inhibitors, Leukemia, Myelogenous, Chronic, BCR-ABL Positive drug therapy, Nylons pharmacology

Abstract

We recently identified a polyamide-chlorambucil conjugate, 1R-Chl, which alkylates and down-regulates transcription of the human histone H4c gene and inhibits the growth of several cancer cell lines in vitro and in a murine SW620 xenograft model, without apparent animal toxicity. In this study, we analyzed the effects of 1R-Chl in the chronic myelogenous leukemia cell line K562 and identified another polyamide conjugate, 6R-Chl, which targets H4 genes and elicits a similar cellular response. Other polyamide conjugates that do not target the H4 gene do not elicit this response. In a murine model, both 1R-Chl and 6R-Chl were found to be highly effective in blocking K562 xenograft growth with high-dose tolerance. Unlike conventional and distamycin-based alkylators, little or no cytotoxicities and animal toxicities were observed in mg/kg dosage ranges. These results suggest that these polyamide alkylators may be a viable treatment alternative for chronic myelogenous leukemia.

Published

2008

43. Targeting specific gene by alkylating pyrrole-imidazole polyamides.

Author

Minoshima M, Chou J, Lefebvre S, Bando T, Shinohara K, Gottesfeld JM, and Sugiyama H

Subjects

Antineoplastic Agents, Alkylating chemical synthesis, Gene Silencing, Nylons chemical synthesis, Antineoplastic Agents, Alkylating chemistry, Histones genetics, Imidazoles chemistry, Nylons chemistry, Pyrroles chemistry

Abstract

Targeting specific genes or gene products by small molecules is novel approach of cancer chemotherapy. We have developed sequence-specific DNA alkylating agents, conjugates between pyrrole (Py)-imidazole (Im) polyamides and 1-(chloromethyl)-5-hydroxy-1,2-dihydro-3H benz[e]indole (seco-CBI) with an indole linker. These compounds efficiently alkylate DNA at a targeted sequence and inhibit gene expression caused by alkylation at template strand of coding region. Recently, histone H4c gene could be targeted by polyamide-chlorambucil (Chl) conjugates. Thus, we designed and synthesized polyamide seco-CBI conjugates 1-5 targeting histone H4c coding sequence. High resolution denaturing polyacrylamide gel electrophoresis (PAGE) showed polyamide seco-CBI conjugates alkylated at the histone H4c coding sequence.

Published

2008

44. Growth arrest of BCR-ABL positive cells with a sequence-specific polyamide-chlorambucil conjugate.

Author

Chou CJ, O'Hare T, Lefebvre S, Alvarez D, Tyner JW, Eide CA, Druker BJ, and Gottesfeld JM

Subjects

Animals, Antineoplastic Agents, Alkylating administration & dosage, Antineoplastic Agents, Alkylating pharmacology, Base Sequence drug effects, Benzamides, Blood Cells metabolism, Blood Cells pathology, Bone Marrow Cells metabolism, Bone Marrow Cells physiology, Cells, Cultured, Chlorambucil administration & dosage, Chlorambucil chemistry, Drug Evaluation, Preclinical, Fusion Proteins, bcr-abl metabolism, Humans, Imatinib Mesylate, Leukemia, Myelogenous, Chronic, BCR-ABL Positive pathology, Mice, Models, Biological, Nylons chemistry, Piperazines administration & dosage, Piperazines pharmacology, Pyrimidines administration & dosage, Pyrimidines pharmacology, Substrate Specificity drug effects, Transduction, Genetic, Cell Proliferation drug effects, Chlorambucil pharmacology, Fusion Proteins, bcr-abl genetics, Nylons pharmacology

Abstract

Chronic myeloid leukemia (CML) is characterized by the presence of a constitutively active Abl kinase, which is the product of a chimeric BCR-ABL gene, caused by the genetic translocation known as the Philadelphia chromosome. Imatinib, a selective inhibitor of the Bcr-Abl tyrosine kinase, has significantly improved the clinical outcome of patients with CML. However, subsets of patients lose their response to treatment through the emergence of imatinib-resistant cells, and imatinib treatment is less durable for patients with late stage CML. Although alternative Bcr-Abl tyrosine kinase inhibitors have been developed to overcome drug resistance, a cocktail therapy of different kinase inhibitors and additional chemotherapeutics may be needed for complete remission of CML in some cases. Chlorambucil has been used for treatment of B cell chronic lymphocytic leukemia, non-Hodgkin's and Hodgkin's disease. Here we report that a DNA sequence-specific pyrrole-imidazole polyamide-chlorambucil conjugate, 1R-Chl, causes growth arrest of cells harboring both unmutated BCR-ABL and three imatinib resistant strains. 1R-Chl also displays selective toxicities against activated lymphocytes and a high dose tolerance in a murine model.

Published

2008

45. Small molecules affecting transcription in Friedreich ataxia.

Author

Gottesfeld JM

Subjects

Animals, Disease Models, Animal, Enzyme Inhibitors pharmacology, Enzyme Inhibitors therapeutic use, Friedreich Ataxia genetics, Friedreich Ataxia therapy, Histone Deacetylase Inhibitors, Humans, Mice, Mutation, RNA, Messenger metabolism, Transcription, Genetic, Frataxin, Friedreich Ataxia physiopathology, Gene Expression Regulation, Iron-Binding Proteins genetics

Abstract

This review concerns the development of small molecule therapeutics for the inherited neurodegenerative disease Friedreich ataxia (FRDA). FRDA is caused by transcriptional repression of the nuclear FXN gene, encoding the essential mitochondrial protein frataxin and accompanying loss of frataxin protein. Frataxin insufficiency leads to mitochrondrial dysfunction and progressive neurodegeneration, along with scoliosis, diabetes and cardiomyopathy. Individuals with FRDA generally die in early adulthood from the associated heart disease, the most common cause of death in FRDA. While antioxidants and iron chelators have shown promise in ameliorating the symptoms of the disease, there is no effective therapy for FRDA that addresses the cause of the disease, the loss of frataxin protein. Gene therapy and protein replacement strategies for FRDA are promising approaches; however, current technology is not sufficiently advanced to envisage treatments for FRDA coming from these approaches in the near future. Since the FXN mutation in FRDA, expanded GAA.TTC triplets in an intron, does not alter the amino acid sequence of frataxin protein, gene reactivation would be of therapeutic benefit. Thus, a number of laboratories have focused on small molecule activators of FXN gene expression as potential therapeutics, and this review summarizes the current status of these efforts, as well as the molecular basis for gene silencing in FRDA.

Published

2007

46. Unanticipated differences between alpha- and gamma-diaminobutyric acid-linked hairpin polyamide-alkylator conjugates.

Author

Tsai SM, Farkas ME, Chou CJ, Gottesfeld JM, and Dervan PB

Subjects

Alkylating Agents chemical synthesis, Alkylation, Animals, Base Sequence, Cell Cycle drug effects, Cell Proliferation drug effects, Chlorambucil chemistry, DNA chemistry, Female, Humans, Mice, Mice, Inbred BALB C, Nylons chemical synthesis, Plasmids genetics, Stereoisomerism, Time Factors, Alkylating Agents chemistry, Alkylating Agents toxicity, Aminobutyrates chemistry, DNA drug effects, Nylons chemistry, Nylons toxicity

Abstract

Hairpin polyamide-chlorambucil conjugates containing an alpha-diaminobutyric acid (alpha-DABA) turn moiety are compared to their constitutional isomers containing the well-characterized gamma-DABA turn. Although the DNA-binding properties of unconjugated polyamides are similar, the alpha-DABA conjugates display increased alkylation specificity and decreased rate of reaction. Treatment of a human colon carcinoma cell line with alpha-DABA versus gamma-DABA hairpin conjugates shows only slight differences in toxicities while producing similar effects on cell morphology and G2/M stage cell cycle arrest. However, striking differences in animal toxicity between the two classes are observed. Although mice treated with an alpha-DABA hairpin polyamide do not differ significantly from control mice, the analogous gamma-DABA hairpin is lethal. This dramatic difference from a subtle structural change would not have been predicted.

Published

2007

47. Histone deacetylase inhibitors reverse gene silencing in Friedreich's ataxia.

Author

Herman D, Jenssen K, Burnett R, Soragni E, Perlman SL, and Gottesfeld JM

Subjects

Acetylation, Alleles, Anilides chemical synthesis, Anilides chemistry, Cell Line, Cells, Cultured, Dose-Response Relationship, Drug, Enzyme Inhibitors chemistry, Enzyme Inhibitors therapeutic use, Friedreich Ataxia drug therapy, Gene Expression Regulation drug effects, HeLa Cells, Heterochromatin drug effects, Heterochromatin genetics, Histones chemistry, Histones drug effects, Histones metabolism, Humans, Iron-Binding Proteins biosynthesis, Iron-Binding Proteins drug effects, Molecular Structure, RNA, Messenger drug effects, RNA, Messenger genetics, Transcription, Genetic drug effects, Frataxin, Anilides pharmacology, Enzyme Inhibitors pharmacology, Friedreich Ataxia genetics, Gene Silencing drug effects, Histone Deacetylase Inhibitors

Abstract

Expansion of GAA x TTC triplets within an intron in FXN (the gene encoding frataxin) leads to transcription silencing, forming the molecular basis for the neurodegenerative disease Friedreich's ataxia. Gene silencing at expanded FXN alleles is accompanied by hypoacetylation of histones H3 and H4 and trimethylation of histone H3 at Lys9, observations that are consistent with a heterochromatin-mediated repression mechanism. We describe the synthesis and characterization of a class of histone deacetylase (HDAC) inhibitors that reverse FXN silencing in primary lymphocytes from individuals with Friedreich's ataxia. We show that these molecules directly affect the histones associated with FXN, increasing acetylation at particular lysine residues on histones H3 and H4 (H3K14, H4K5 and H4K12). This class of HDAC inhibitors may yield therapeutics for Friedreich's ataxia.

Published

2006

48. DNA sequence-specific polyamides alleviate transcription inhibition associated with long GAA.TTC repeats in Friedreich's ataxia.

Author

Burnett R, Melander C, Puckett JW, Son LS, Wells RD, Dervan PB, and Gottesfeld JM

Subjects

Cell Line, Humans, Ligands, Molecular Structure, Nucleic Acid Conformation, Oligonucleotide Array Sequence Analysis, Frataxin, Friedreich Ataxia genetics, Iron-Binding Proteins genetics, Nylons metabolism, Transcription, Genetic, Trinucleotide Repeats

Abstract

The DNA abnormality found in 98% of Friedreich's ataxia (FRDA) patients is the unstable hyperexpansion of a GAA.TTC triplet repeat in the first intron of the frataxin gene. Expanded GAA.TTC repeats result in decreased transcription and reduced levels of frataxin protein in affected individuals. Beta-alanine-linked pyrrole-imidazole polyamides bind GAA.TTC tracts with high affinity and disrupt the intramolecular DNA.DNA-associated region of the sticky-DNA conformation formed by long GAA.TTC repeats. Fluorescent polyamide-Bodipy conjugates localize in the nucleus of a lymphoid cell line derived from a FRDA patient. The synthetic ligands increase transcription of the frataxin gene in cell culture, resulting in increased levels of frataxin protein. DNA microarray analyses indicate that a limited number of genes are significantly affected in FRDA cells. Polyamides may increase transcription by altering the DNA conformation of genes harboring long GAA.TTC repeats or by chromatin opening.

Published

2006

49. A two-hit mechanism for pre-mitotic arrest of cancer cell proliferation by a polyamide-alkylator conjugate.

Author

Alvarez D, Chou CJ, Latella L, Zeitlin SG, Ku S, Puri PL, Dervan PB, and Gottesfeld JM

Subjects

Cell Division, Cell Line, Tumor, Cell Proliferation, Chlorambucil therapeutic use, G2 Phase, Gene Expression Regulation drug effects, Histones antagonists & inhibitors, Histones genetics, Humans, Polymers pharmacology, Polymers therapeutic use, RNA, Small Interfering pharmacology, Chlorambucil pharmacology, Interphase, Models, Biological, Neoplasms pathology

Abstract

A polyamide-chlorambucil conjugate (1R-Chl) arrests a wide range of human cancer cell lines at the G2/M phase of the cell cycle and downregulates histone H4c gene expression. However, an siRNA against H4c mRNA causes G1/S arrest. Here, we report that 1R-Chl downregulates H4c prior to G2/M arrest. G2/M arrest is the result of extensive DNA damage by 1R-Chl, which leads to phosphorylation of H2A.X at serine 139, recruitment of the Nbs1 repair protein, and a cascade of unknown events culminating with cdc2 phosphorylation at tyrosine 15 and abolishment of cdc2 kinase activity. A control polyamide-Chl conjugate, which neither binds to the H4c gene nor has an anti-proliferative effect by itself, causes G2/M arrest when cells are treated with siRNAs specific for H3 or H4c.

Published

2006

50. Induced fit and "lock and key" recognition of 5S RNA by zinc fingers of transcription factor IIIA.

Author

Lee BM, Xu J, Clarkson BK, Martinez-Yamout MA, Dyson HJ, Case DA, Gottesfeld JM, and Wright PE

Subjects

Amino Acid Sequence, Animals, Base Sequence, Gene Expression Regulation, Macromolecular Substances, Models, Molecular, Molecular Sequence Data, Protein Structure, Secondary, RNA, Ribosomal, 5S chemistry, RNA, Ribosomal, 5S metabolism, Sequence Alignment, Transcription Factor TFIIIA genetics, Transcription Factor TFIIIA metabolism, Xenopus laevis, Nucleic Acid Conformation, Protein Structure, Tertiary, RNA, Ribosomal, 5S genetics, Transcription Factor TFIIIA chemistry, Zinc Fingers

Abstract

Transcription factor IIIA (TFIIIA) is a Cys2His2 zinc finger protein that regulates expression of the 5 S ribosomal RNA gene by binding specifically to the internal control element. TFIIIA also functions in transport and storage of 5 S RNA by binding directly to the RNA transcript. To obtain insights into the mechanism by which TFIIIA recognizes 5 S RNA, we determined the solution structure of the middle three zinc fingers bound to the central core of 5 S RNA. Finger 4 utilizes "lock and key" recognition to bind in the widened major groove of the pre-structured RNA loop E motif. This interaction is mediated by direct hydrogen bonding interactions with bases. In contrast, recognition of loop A, a flexible junction of three helices, occurs by an induced fit mechanism that involves reorganization of the conserved CAUA motif and structuring of the finger 5-finger 6 interface to form a complementary RNA binding surface.

Published

2006