Your search keyword '"Marsh, J. Lawrence"' showing total 37 results

1. Serine residues 13 and 16 are key modulators of mutant huntingtin induced toxicity in Drosophila

Author

Chatterjee, Megha, Steffan, Joan S, Lukacsovich, Tamas, Marsh, J Lawrence, and Agrawal, Namita

Subjects

Biomedical and Clinical Sciences, Neurosciences, Rare Diseases, Huntington's Disease, Brain Disorders, Genetics, Neurodegenerative, Neurological, Animals, Animals, Genetically Modified, Drosophila, Humans, Huntingtin Protein, Mutation, Neurons, Phosphorylation, Protein Processing, Post-Translational, Serine, Huntington's disease, Mutant huntingtin, Post-translational modification, Clinical Sciences, Psychology, Neurology & Neurosurgery, Biological psychology

Abstract

Poly-glutamine expansion near the N-terminus of the huntingtin protein (HTT) is the prime determinant of Huntington's disease (HD) pathology; however, post-translational modifications and protein context are also reported to influence poly-glutamine induced HD toxicity. The impact of phosphorylating serine 13/16 of mutant HTT (mHTT) on HD has been documented in cell culture and murine models. However, endogenous processing of the human protein in mammalian systems complicates the interpretations. Therefore, to study the impact of S13/16 phosphorylation on the subcellular behavior of HTT under a controlled genetic background with minimal proteolytic processing of the human protein, we employed Drosophila as the model system. We ectopically expressed full-length (FL) and exon1 fragment of human HTT with phosphomimetic and resistant mutations at serines 13 and 16 in different neuronal populations. Phosphomimetic mHTT aggravates and the phosphoresistant mutation ameliorates mHTT-induced toxicity in the context of both FL- and exon1- mHTT in Drosophila although in all cases FL appears less toxic than exon1. Our observations strongly indicate that the phosphorylation status of S13/16 can affect HD pathology in Drosophila and these residues can be potential targets for affecting HD pathogenesis.

Published

2021

2. Effects of flanking sequences and cellular context on subcellular behavior and pathology of mutant HTT

Author

Chongtham, Anjalika, Bornemann, Douglas J, Barbaro, Brett A, Lukacsovich, Tamas, Agrawal, Namita, Syed, Adeela, Worthge, Shane, Purcell, Judith, Burke, John, Chin, Theodore M, and Marsh, J Lawrence

Subjects

Neurodegenerative, Neurosciences, Brain Disorders, Rare Diseases, Huntington's Disease, Aetiology, 2.1 Biological and endogenous factors, Neurological, Animals, Animals, Genetically Modified, Cell Nucleus, Drosophila melanogaster, Female, Humans, Huntingtin Protein, Huntington Disease, Inclusion Bodies, Male, Mutation, Neurons, Peptides, Trachea, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Huntington's disease (HD) is caused by an expansion of a poly glutamine (polyQ) stretch in the huntingtin protein (HTT) that is necessary to cause pathology and formation of HTT aggregates. Here we ask whether expanded polyQ is sufficient to cause pathology and aggregate formation. By addressing the sufficiency question, one can identify cellular processes and structural parameters that influence HD pathology and HTT subcellular behavior (i.e. aggregation state and subcellular location). Using Drosophila, we compare the effects of expressing mutant full-length human HTT (fl-mHTT) to the effects of mutant human HTTexon1 and to two commonly used synthetic fragments, HTT171 and shortstop (HTT118). Expanded polyQ alone is not sufficient to cause inclusion formation since full-length HTT and HTTex1 with expanded polyQ are both toxic although full-length HTT remains diffuse while HTTex1 forms inclusions. Further, inclusions are not sufficient to cause pathology since HTT171-120Q forms inclusions but is benign and co-expression of HTT171-120Q with non-aggregating pathogenic fl-mHTT recruits fl-mHTT to aggregates and rescues its pathogenicity. Additionally, the influence of sequences outside the expanded polyQ domain is revealed by finding that small modifications to the HTT118 or HTT171 fragments can dramatically alter their subcellular behavior and pathogenicity. Finally, mutant HTT subcellular behavior is strongly modified by different cell and tissue environments (e.g. fl-mHTT appears as diffuse nuclear in one tissue and diffuse cytoplasmic in another but toxic in both). These observations underscore the importance of cellular and structural context for the interpretation and comparison of experiments using different fragments and tissues to report the effects of expanded polyQ.

Published

2020

3. Systematic genetic interaction studies identify histone demethylase Utx as potential target for ameliorating Huntington’s disease

Author

Song, Wan, Zsindely, Nóra, Faragó, Anikó, Marsh, J Lawrence, and Bodai, László

Subjects

Biochemistry and Cell Biology, Genetics, Biological Sciences, Huntington's Disease, Rare Diseases, Neurodegenerative, Brain Disorders, Neurosciences, 2.1 Biological and endogenous factors, Aetiology, Animals, Animals, Genetically Modified, Chromatin, Chromatin Immunoprecipitation, Drosophila melanogaster, Female, Heterochromatin, Histone Demethylases, Histones, Huntington Disease, Male, Methylation, Polycomb-Group Proteins, Medical and Health Sciences, Genetics & Heredity

Abstract

Huntington's disease (HD) is a dominantly inherited neurodegenerative disease caused by alterations in the huntingtin gene (htt). Transcriptional dysregulation is an early event in HD progression. Protein acetylation and methylation particularly on histones regulates chromatin structure thereby preventing or facilitating transcription. Although protein acetylation has been found to affect HD symptoms, little is known about the potential role of protein methylation in HD pathology. In recent years, a series of proteins have been described that are responsible for methylating and demethylating histones as well as other proteins. We carried out systematic genetic interaction studies testing lysine and arginine methylases and demethylases in a Drosophila melanogaster HD model. We found that modulating methylation enzymes that typically affect histone positions H3K4, H3K36 or H3K79 had varying effects on HD pathology while modulating ones that typically affect constitutive heterochromatin marks at H3K9 and H4K20 generally had limited impact on HD pathology. In contrast, modulating enzymes acting on the facultative heterochromatin mark at H3K27 had specific effects on HD pathology, with reduction of the demethylase Utx rescuing HTT-induced pathology while reducing Polycomb Repressive Complex2 core methylase components led to more aggressive pathology. Further exploration of the mechanism underlying the methylation-specific interactions suggest that these lysine and arginine methylases and demethylases are likely exerting their influence through non-histone targets. These results highlight a novel therapeutic approach for HD in the form of Utx inhibition.

Published

2018

4. Phosphorylation of huntingtin at residue T3 is decreased in Huntington’s disease and modulates mutant huntingtin protein conformation

Author

Cariulo, Cristina, Azzollini, Lucia, Verani, Margherita, Martufi, Paola, Boggio, Roberto, Chiki, Anass, Deguire, Sean M, Cherubini, Marta, Gines, Silvia, Marsh, J Lawrence, Conforti, Paola, Cattaneo, Elena, Santimone, Iolanda, Squitieri, Ferdinando, Lashuel, Hilal A, Petricca, Lara, and Caricasole, Andrea

Subjects

Neurosciences, Brain Disorders, Neurodegenerative, Rare Diseases, Huntington's Disease, Neurological, Animals, Cells, Cultured, Exons, HEK293 Cells, Humans, Huntingtin Protein, Huntington Disease, Immunoassay, Mice, Mutant Proteins, Phosphorylation, Protein Conformation, Protein Processing, Post-Translational, Sensitivity and Specificity, huntingtin, posttranslational modification, immunoassay, phosphorylation, neurodegeneration

Abstract

Posttranslational modifications can have profound effects on the biological and biophysical properties of proteins associated with misfolding and aggregation. However, their detection and quantification in clinical samples and an understanding of the mechanisms underlying the pathological properties of misfolding- and aggregation-prone proteins remain a challenge for diagnostics and therapeutics development. We have applied an ultrasensitive immunoassay platform to develop and validate a quantitative assay for detecting a posttranslational modification (phosphorylation at residue T3) of a protein associated with polyglutamine repeat expansion, namely Huntingtin, and characterized its presence in a variety of preclinical and clinical samples. We find that T3 phosphorylation is greatly reduced in samples from Huntington's disease models and in Huntington's disease patients, and we provide evidence that bona-fide T3 phosphorylation alters Huntingtin exon 1 protein conformation and aggregation properties. These findings have significant implications for both mechanisms of disease pathogenesis and the development of therapeutics and diagnostics for Huntington's disease.

Published

2017

5. Polyglutamine expansion affects huntingtin conformation in multiple Huntington's disease models.

Author

Daldin, Manuel, Fodale, Valentina, Cariulo, Cristina, Azzollini, Lucia, Verani, Margherita, Martufi, Paola, Spiezia, Maria Carolina, Deguire, Sean M, Cherubini, Marta, Macdonald, Douglas, Weiss, Andreas, Bresciani, Alberto, Vonsattel, Jean-Paul Gerard, Petricca, Lara, Marsh, J Lawrence, Gines, Silvia, Santimone, Iolanda, Marano, Massimo, Lashuel, Hilal A, Squitieri, Ferdinando, and Caricasole, Andrea

Subjects

Brain, Fibroblasts, Animals, Humans, Drosophila, Huntington Disease, Disease Models, Animal, Phosphoserine, Peptides, Trinucleotide Repeat Expansion, Protein Conformation, Phosphorylation, Exons, Mutant Proteins, HEK293 Cells, Huntingtin Protein, Neurodegenerative, Rare Diseases, Huntington's Disease, Orphan Drug, Neurosciences, Brain Disorders, 2.1 Biological and endogenous factors, Neurological, Disease Models, Animal, Biochemistry and Cell Biology, Other Physical Sciences

Abstract

Conformational changes in disease-associated or mutant proteins represent a key pathological aspect of Huntington's disease (HD) and other protein misfolding diseases. Using immunoassays and biophysical approaches, we and others have recently reported that polyglutamine expansion in purified or recombinantly expressed huntingtin (HTT) proteins affects their conformational properties in a manner dependent on both polyglutamine repeat length and temperature but independent of HTT protein fragment length. These findings are consistent with the HD mutation affecting structural aspects of the amino-terminal region of the protein, and support the concept that modulating mutant HTT conformation might provide novel therapeutic and diagnostic opportunities. We now report that the same conformational TR-FRET based immunoassay detects polyglutamine- and temperature-dependent changes on the endogenously expressed HTT protein in peripheral tissues and post-mortem HD brain tissue, as well as in tissues from HD animal models. We also find that these temperature- and polyglutamine-dependent conformational changes are sensitive to bona-fide phosphorylation on S13 and S16 within the N17 domain of HTT. These findings provide key clinical and preclinical relevance to the conformational immunoassay, and provide supportive evidence for its application in the development of therapeutics aimed at correcting the conformation of polyglutamine-expanded proteins as well as the pharmacodynamics readouts to monitor their efficacy in preclinical models and in HD patients.

Published

2017

6. The phasor-FLIM fingerprints reveal shifts from OXPHOS to enhanced glycolysis in Huntington Disease.

Author

Sameni, Sara, Syed, Adeela, Marsh, J Lawrence, and Digman, Michelle A

Subjects

Eye, Cell Nucleus, Animals, Animals, Genetically Modified, Humans, Drosophila, Huntington Disease, NAD, Microscopy, Fluorescence, Gene Expression Regulation, Trinucleotide Repeat Expansion, Glycolysis, Oxidative Stress, Phosphorylation, HEK293 Cells, Huntingtin Protein, Genetically Modified, Microscopy, Fluorescence, Neurodegenerative, Neurosciences, Rare Diseases, Huntington's Disease, Brain Disorders, 2.1 Biological and endogenous factors, Neurological, Biochemistry and Cell Biology, Other Physical Sciences

Abstract

Huntington disease (HD) is an autosomal neurodegenerative disorder caused by the expansion of Polyglutamine (polyQ) in exon 1 of the Huntingtin protein. Glutamine repeats below 36 are considered normal while repeats above 40 lead to HD. Impairment in energy metabolism is a common trend in Huntington pathogenesis; however, this effect is not fully understood. Here, we used the phasor approach and Fluorescence Lifetime Imaging Microscopy (FLIM) to measure changes between free and bound fractions of NADH as a indirect measure of metabolic alteration in living cells. Using Phasor-FLIM, pixel maps of metabolic alteration in HEK293 cell lines and in transgenic Drosophila expressing expanded and unexpanded polyQ HTT exon1 in the eye disc were developed. We found a significant shift towards increased free NADH, indicating an increased glycolytic state for cells and tissues expressing the expanded polyQ compared to unexpanded control. In the nucleus, a further lifetime shift occurs towards higher free NADH suggesting a possible synergism between metabolic dysfunction and transcriptional regulation. Our results indicate that metabolic dysfunction in HD shifts to increased glycolysis leading to oxidative stress and cell death. This powerful label free method can be used to screen native HD tissue samples and for potential drug screening.

Published

2016

7. SIRT2- and NRF2-Targeting Thiazole-Containing Compound with Therapeutic Activity in Huntington's Disease Models.

Author

Quinti, Luisa, Casale, Malcolm, Moniot, Sébastien, Pais, Teresa F, Van Kanegan, Michael J, Kaltenbach, Linda S, Pallos, Judit, Lim, Ryan G, Naidu, Sharadha Dayalan, Runne, Heike, Meisel, Lisa, Rauf, Nazifa Abdul, Leyfer, Dmitriy, Maxwell, Michele M, Saiah, Eddine, Landers, John E, Luthi-Carter, Ruth, Abagyan, Ruben, Dinkova-Kostova, Albena T, Steegborn, Clemens, Marsh, J Lawrence, Lo, Donald C, Thompson, Leslie M, and Kazantsev, Aleksey G

Subjects

Cell Line, Animals, Rats, Drosophila, Huntington Disease, Disease Models, Animal, Thiazoles, Neuroprotective Agents, Structure-Activity Relationship, Dose-Response Relationship, Drug, NF-E2-Related Factor 2, Sirtuin 2, Neurosciences, Huntington's Disease, Orphan Drug, Neurodegenerative, Brain Disorders, Rare Diseases, 5.1 Pharmaceuticals, Neurological

Abstract

There are currently no disease-modifying therapies for the neurodegenerative disorder Huntington's disease (HD). This study identified novel thiazole-containing inhibitors of the deacetylase sirtuin-2 (SIRT2) with neuroprotective activity in ex vivo brain slice and Drosophila models of HD. A systems biology approach revealed an additional SIRT2-independent property of the lead-compound, MIND4, as an inducer of cytoprotective NRF2 (nuclear factor-erythroid 2 p45-derived factor 2) activity. Structure-activity relationship studies further identified a potent NRF2 activator (MIND4-17) lacking SIRT2 inhibitory activity. MIND compounds induced NRF2 activation responses in neuronal and non-neuronal cells and reduced production of reactive oxygen species and nitrogen intermediates. These drug-like thiazole-containing compounds represent an exciting opportunity for development of multi-targeted agents with potentially synergistic therapeutic benefits in HD and related disorders.

Published

2016

8. Disruption of the nuclear membrane by perinuclear inclusions of mutant huntingtin causes cell-cycle re-entry and striatal cell death in mouse and cell models of Huntington's disease.

Author

Liu, Kuan-Yu, Shyu, Yu-Chiau, Barbaro, Brett A, Lin, Yuan-Ta, Chern, Yijuang, Thompson, Leslie Michels, James Shen, Che-Kun, and Marsh, J Lawrence

Subjects

Corpus Striatum, Neurons, Nuclear Envelope, Inclusion Bodies, Animals, Mice, Transgenic, Humans, Mice, Huntington Disease, Disease Models, Animal, Nerve Tissue Proteins, Cell Cycle, Cell Death, Mutation, Huntingtin Protein, Rare Diseases, Huntington's Disease, Brain Disorders, Neurodegenerative, Neurosciences, Neurological, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Accumulation of N-terminal fragments of mutant huntingtin (mHTT) in the cytoplasm, nuclei and axons of neurons is a hallmark of Huntington's disease (HD), although how these fragments negatively impact neurons remains unclear. We followed the distribution of mHTT in the striata of transgenic R6/2-J2 HD mice as their motor function declined. The fraction of cells with diffuse, perinuclear or intranuclear mHTT changed in parallel with decreasing motor function. In transgenic mice, medium spiny neurons (MSNs) that exhibited perinuclear inclusions expressed cell-cycle markers typically not seen in the striata of normal mice, and these cells are preferentially lost as disease progresses. Electron microscopy reveals that perinuclear inclusions disrupt the nuclear envelope. The progression of perinuclear inclusions being accompanied by cell-cycle activation and culminating in cell death was also observed in 1° cortical neurons. These observations provide a strong correlation between the subcellular location of mHTT, disruption of the nucleus, re-entry into the cell-cycle and eventual neuronal death. They also highlight the fact that the subcellular distribution of mHTT is highly dynamic such that the distribution of mHTT observed depends greatly on the stage of the disease being examined.

Published

2015

9. Comparative study of naturally occurring huntingtin fragments in Drosophila points to exon 1 as the most pathogenic species in Huntington's disease

Author

Barbaro, Brett A, Lukacsovich, Tamas, Agrawal, Namita, Burke, John, Bornemann, Doug J, Purcell, Judith M, Worthge, Shane A, Caricasole, Andrea, Weiss, Andreas, Song, Wan, Morozova, Olga A, Colby, David W, and Marsh, J Lawrence

Subjects

Biochemistry and Cell Biology, Genetics, Biological Sciences, Orphan Drug, Rare Diseases, Neurodegenerative, Huntington's Disease, Neurosciences, Brain Disorders, Aetiology, 2.1 Biological and endogenous factors, Neurological, Amyloid, Animals, Animals, Genetically Modified, Disease Models, Animal, Drosophila, Drosophila Proteins, Exons, Gene Expression, Humans, Huntingtin Protein, Huntington Disease, Male, Microtubule-Associated Proteins, Nerve Tissue Proteins, Neurons, Peptide Fragments, Peptides, Protein Aggregation, Pathological, Protein Interaction Domains and Motifs, Proteolysis, Medical and Health Sciences, Genetics & Heredity

Abstract

Although Huntington's disease is caused by the expansion of a CAG triplet repeat within the context of the 3144-amino acid huntingtin protein (HTT), studies reveal that N-terminal fragments of HTT containing the expanded PolyQ region can be produced by proteolytic processing and/or aberrant splicing. N-terminal HTT fragments are also prevalent in postmortem tissue, and expression of some of these fragments in model organisms can cause pathology. This has led to the hypothesis that N-terminal peptides may be critical modulators of disease pathology, raising the possibility that targeting aberrant splicing or proteolytic processing may present attractive therapeutic targets. However, many factors can contribute to pathology, including genetic background and differential expression of transgenes, in addition to intrinsic differences between fragments and their cellular effects. We have used Drosophila as a model system to determine the relative toxicities of different naturally occurring huntingtin fragments in a system in which genetic background, transgene expression levels and post-translational proteolytic processing can be controlled. These studies reveal that among the naturally occurring N-terminal HTT peptides, the exon 1 peptide is exceptionally pathogenic and exhibits unique structural and biophysical behaviors that do not appear to be incremental changes compared with other fragments. If this proves correct, efforts to specifically reduce the levels of exon 1 peptides or to target toxicity-influencing post-translational modifications that occur with the exon 1 context are likely to have the greatest impact on pathology.

Published

2015

10. Potential function for the Huntingtin protein as a scaffold for selective autophagy.

Author

Ochaba, Joseph, Lukacsovich, Tamás, Csikos, George, Zheng, Shuqiu, Margulis, Julia, Salazar, Lisa, Mao, Kai, Lau, Alice L, Yeung, Sylvia Y, Humbert, Sandrine, Saudou, Frédéric, Klionsky, Daniel J, Finkbeiner, Steven, Zeitlin, Scott O, Marsh, J Lawrence, Housman, David E, Thompson, Leslie M, and Steffan, Joan S

Subjects

Animals, Animals, Genetically Modified, Mice, Drosophila, Microtubule-Associated Proteins, Drosophila Proteins, Autophagy, Huntingtin Protein, Huntingtin, Huntington disease, neurodegeneration, polyglutamine, selective autophagy, Genetically Modified, Rare Diseases, Huntington's Disease, Neurodegenerative, Brain Disorders, Genetics, Neurosciences, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Neurological

Abstract

Although dominant gain-of-function triplet repeat expansions in the Huntingtin (HTT) gene are the underlying cause of Huntington disease (HD), understanding the normal functions of nonmutant HTT protein has remained a challenge. We report here findings that suggest that HTT plays a significant role in selective autophagy. Loss of HTT function in Drosophila disrupts starvation-induced autophagy in larvae and conditional knockout of HTT in the mouse CNS causes characteristic cellular hallmarks of disrupted autophagy, including an accumulation of striatal p62/SQSTM1 over time. We observe that specific domains of HTT have structural similarities to yeast Atg proteins that function in selective autophagy, and in particular that the C-terminal domain of HTT shares structural similarity to yeast Atg11, an autophagic scaffold protein. To explore possible functional similarity between HTT and Atg11, we investigated whether the C-terminal domain of HTT interacts with mammalian counterparts of yeast Atg11-interacting proteins. Strikingly, this domain of HTT coimmunoprecipitates with several key Atg11 interactors, including the Atg1/Unc-51-like autophagy activating kinase 1 kinase complex, autophagic receptor proteins, and mammalian Atg8 homologs. Mutation of a phylogenetically conserved WXXL domain in a C-terminal HTT fragment reduces coprecipitation with mammalian Atg8 homolog GABARAPL1, suggesting a direct interaction. Collectively, these data support a possible central role for HTT as an Atg11-like scaffold protein. These findings have relevance to both mechanisms of disease pathogenesis and to therapeutic intervention strategies that reduce levels of both mutant and normal HTT.

Published

2014

11. A potent and selective Sirtuin 1 inhibitor alleviates pathology in multiple animal and cell models of Huntington's disease

Author

Smith, Marianne R, Syed, Adeela, Lukacsovich, Tamas, Purcell, Judy, Barbaro, Brett A, Worthge, Shane A, Wei, Stephen R, Pollio, Giuseppe, Magnoni, Letizia, Scali, Carla, Massai, Luisa, Franceschini, Davide, Camarri, Michela, Gianfriddo, Marco, Diodato, Enrica, Thomas, Russell, Gokce, Ozgun, Tabrizi, SJ, Caricasole, Andrea, Landwehrmeyer, Bernard, Menalled, Liliana, Murphy, Carol, Ramboz, Sylvie, Luthi-Carter, Ruth, Westerberg, Goran, and Marsh, J Lawrence

Subjects

Rare Diseases, Neurosciences, Neurodegenerative, Biotechnology, Genetics, Huntington's Disease, Brain Disorders, 5.1 Pharmaceuticals, Aetiology, 2.1 Biological and endogenous factors, Development of treatments and therapeutic interventions, Generic health relevance, Animals, Carbazoles, Disease Models, Animal, Drosophila Proteins, Drosophila melanogaster, Enzyme Inhibitors, Female, Histone Deacetylases, Humans, Huntington Disease, Male, Mice, Mice, Inbred C57BL, PC12 Cells, Rats, Rats, Sprague-Dawley, Sirtuin 1, Sirtuins, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Protein acetylation, which is central to transcriptional control as well as other cellular processes, is disrupted in Huntington's disease (HD). Treatments that restore global acetylation levels, such as inhibiting histone deacetylases (HDACs), are effective in suppressing HD pathology in model organisms. However, agents that selectively target the disease-relevant HDACs have not been available. SirT1 (Sir2 in Drosophila melanogaster) deacetylates histones and other proteins including transcription factors. Genetically reducing, but not eliminating, Sir2 has been shown to suppress HD pathology in model organisms. To date, small molecule inhibitors of sirtuins have exhibited low potency and unattractive pharmacological and biopharmaceutical properties. Here, we show that highly selective pharmacological inhibition of Drosophila Sir2 and mammalian SirT1 using the novel inhibitor selisistat (selisistat; 6-chloro-2,3,4,9-tetrahydro-1H-carbazole-1-carboxamide) can suppress HD pathology caused by mutant huntingtin exon 1 fragments in Drosophila, mammalian cells and mice. We have validated Sir2 as the in vivo target of selisistat by showing that genetic elimination of Sir2 eradicates the effect of this inhibitor in Drosophila. The specificity of selisistat is shown by its effect on recombinant sirtuins in mammalian cells. Reduction of HD pathology by selisistat in Drosophila, mammalian cells and mouse models of HD suggests that this inhibitor has potential as an effective therapeutic treatment for human disease and may also serve as a tool to better understand the downstream pathways of SirT1/Sir2 that may be critical for HD.

Published

2014

12. Targeting H3K4 trimethylation in Huntington disease

Author

Vashishtha, Malini, Ng, Christopher W, Yildirim, Ferah, Gipson, Theresa A, Kratter, Ian H, Bodai, Laszlo, Song, Wan, Lau, Alice, Labadorf, Adam, Vogel-Ciernia, Annie, Troncosco, Juan, Ross, Christopher A, Bates, Gillian P, Krainc, Dimitri, Sadri-Vakili, Ghazaleh, Finkbeiner, Steven, Marsh, J Lawrence, Housman, David E, Fraenkel, Ernest, and Thompson, Leslie M

Subjects

Huntington's Disease, Neurodegenerative, Rare Diseases, Orphan Drug, Neurosciences, Genetics, Brain Disorders, Underpinning research, Aetiology, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Neurological, Animals, Animals, Genetically Modified, Blotting, Western, Brain, Brain-Derived Neurotrophic Factor, Cells, Cultured, Drosophila melanogaster, Female, Gene Expression Profiling, Histone Demethylases, Histones, Humans, Huntingtin Protein, Huntington Disease, Lysine, Male, Methylation, Mice, Mice, Inbred C57BL, Mice, Inbred CBA, Nerve Tissue Proteins, Neurons, Oxidoreductases, N-Demethylating, Promoter Regions, Genetic, RNA Interference, Reverse Transcriptase Polymerase Chain Reaction, polyglutamine, neurodegeneration

Abstract

Transcriptional dysregulation is an early feature of Huntington disease (HD). We observed gene-specific changes in histone H3 lysine 4 trimethylation (H3K4me3) at transcriptionally repressed promoters in R6/2 mouse and human HD brain. Genome-wide analysis showed a chromatin signature for this mark. Reducing the levels of the H3K4 demethylase SMCX/Jarid1c in primary neurons reversed down-regulation of key neuronal genes caused by mutant Huntingtin expression. Finally, reduction of SMCX/Jarid1c in primary neurons from BACHD mice or the single Jarid1 in a Drosophila HD model was protective. Therefore, targeting this epigenetic signature may be an effective strategy to ameliorate the consequences of HD.

Published

2013

13. Methylene Blue Modulates Huntingtin Aggregation Intermediates and Is Protective in Huntington's Disease Models

Author

Sontag, Emily Mitchell, Lotz, Gregor P, Agrawal, Namita, Tran, Andrew, Aron, Rebecca, Yang, Guocheng, Necula, Mihaela, Lau, Alice, Finkbeiner, Steven, Glabe, Charles, Marsh, J Lawrence, Muchowski, Paul J, and Thompson, Leslie M

Subjects

Biomedical and Clinical Sciences, Neurosciences, Brain Disorders, Acquired Cognitive Impairment, Rare Diseases, Neurodegenerative, Huntington's Disease, Orphan Drug, Aetiology, 2.1 Biological and endogenous factors, Neurological, Analysis of Variance, Animals, Brain-Derived Neurotrophic Factor, Cells, Cultured, Cerebral Cortex, Disease Models, Animal, Drosophila, Embryo, Mammalian, Enzyme Inhibitors, Excitatory Amino Acid Antagonists, Humans, Huntingtin Protein, Huntington Disease, Kynurenic Acid, Methylene Blue, Mice, Mice, Inbred C57BL, Microscopy, Atomic Force, Mutation, Nerve Tissue Proteins, Neurodegenerative Diseases, Neurons, Psychomotor Performance, Rats, Rotarod Performance Test, Transfection, Trinucleotide Repeat Expansion, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery

Abstract

Huntington's disease (HD) is a devastating neurodegenerative disorder with no disease-modifying treatments available. The disease is caused by expansion of a CAG trinucleotide repeat and manifests with progressive motor abnormalities, psychiatric symptoms, and cognitive decline. Expression of an expanded polyglutamine repeat within the Huntingtin (Htt) protein impacts numerous cellular processes, including protein folding and clearance. A hallmark of the disease is the progressive formation of inclusions that represent the culmination of a complex aggregation process. Methylene blue (MB), has been shown to modulate aggregation of amyloidogenic disease proteins. We investigated whether MB could impact mutant Htt-mediated aggregation and neurotoxicity. MB inhibited recombinant protein aggregation in vitro, even when added to preformed oligomers and fibrils. MB also decreased oligomer number and size and decreased accumulation of insoluble mutant Htt in cells. In functional assays, MB increased survival of primary cortical neurons transduced with mutant Htt, reduced neurodegeneration and aggregation in a Drosophila melanogaster model of HD, and reduced disease phenotypes in R6/2 HD modeled mice. Furthermore, MB treatment also promoted an increase in levels of BDNF RNA and protein in vivo. Thus, MB, which is well tolerated and used in humans, has therapeutic potential for HD.

Published

2012

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

Author

Jia, Haiqun, Pallos, Judit, Jacques, Vincent, Lau, Alice, Tang, Bin, Cooper, Andrew, Syed, Adeela, Purcell, Judith, Chen, Yi, Sharma, Shefali, Sangrey, Gavin R, Darnell, Shayna B, Plasterer, Heather, Sadri-Vakili, Ghazaleh, Gottesfeld, Joel M, Thompson, Leslie M, Rusche, James R, Marsh, J Lawrence, and Thomas, Elizabeth A

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Neurosciences, Brain Disorders, Rare Diseases, Orphan Drug, Huntington's Disease, Neurodegenerative, Biotechnology, Development of treatments and therapeutic interventions, 2.1 Biological and endogenous factors, Aetiology, 5.1 Pharmaceuticals, Animals, Cells, Cultured, Disease Models, Animal, Drosophila melanogaster, Drug Delivery Systems, HCT116 Cells, Histone Deacetylase 1, Histone Deacetylase Inhibitors, Histone Deacetylases, Humans, Huntington Disease, Mice, Mice, Inbred C57BL, Mice, Inbred CBA, Mice, Transgenic, Peptides, Phenotype, Striatum, Disease, Epigenetic, Therapeutic, Chromatin, Gene expression, Clinical Sciences, Neurology & Neurosurgery, Biochemistry and cell biology

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

15. A novel target for Huntington's disease: ERK at the crossroads of signaling

Author

Bodai, László and Marsh, J Lawrence

Subjects

Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, Neurodegenerative, Brain Disorders, Orphan Drug, Huntington's Disease, Neurosciences, Aetiology, 2.1 Biological and endogenous factors, Neurological, Animals, Brain-Derived Neurotrophic Factor, Extracellular Signal-Regulated MAP Kinases, Glutamic Acid, Humans, Huntingtin Protein, Huntington Disease, MAP Kinase Signaling System, Nerve Tissue Proteins, Nuclear Proteins, ERK, Huntington's disease, MAP kinase, neurodegenerative disorders, polyglutamine, Medical and Health Sciences, Psychology and Cognitive Sciences, Developmental Biology, Biological sciences

Abstract

Activating the ERK pathway (extracellular signal-regulated kinase pathway) has proven beneficial in several models of Huntington's disease (HD), and drugs that are protective in HD models have recently been found to activate ERK. Thus, the ERK cascade may be a potential target for therapeutic intervention in this currently untreatable disorder. HD is caused by an expanded polyglutamine repeat in the huntingtin (Htt) protein that actuates a diverse set of pathogenic mechanisms. In response to mutant Htt, ERK is activated and directs a protective transcriptional response and inhibits caspase activation. Paradoxically, Htt also interferes with several signaling events of the ERK pathway. Mutant Htt compromises the ERK-dependent transcriptional response to corticostriatal BDNF signaling. Mutant Htt also hinders glutamate uptake from the synaptic cleft by down-regulating ERK-dependent expression of glutamate transporters, leaving cells vulnerable to excitotoxicity. Some of this cellular complexity can be capitalized on to achieve selective activation of ERK, which can be protective.

Published

2012

16. Pcaf Modulates Polyglutamine Pathology in a Drosophila Model of Huntington’s Disease

Author

Bodai, Laszlo, Pallos, Judit, Thompson, Leslie Michels, and Marsh, J Lawrence

Subjects

Rare Diseases, Neurodegenerative, Neurosciences, Brain Disorders, Genetics, Huntington's Disease, 2.1 Biological and endogenous factors, Aetiology, Neurological, Animals, Animals, Genetically Modified, Disease Models, Animal, Drosophila Proteins, Drosophila melanogaster, Histone Acetyltransferases, Huntington Disease, Immunoblotting, Nerve Degeneration, Peptides, Polyglutamine, Huntington's disease, Histone acetyltransferase, Pcaf, Nejire, Drosophila, Clinical Sciences, Cognitive Sciences, Neurology & Neurosurgery

Abstract

Huntingtin peptides with elongated polyglutamine domains, the root causes of Huntington's disease, hinder histone acetylation, which leads to transcriptional dysregulation. However, the range of acetyltransferases interacting with mutant Huntingtin has not been systematically evaluated. We used genetic interaction tests in Drosophila to determine whether specific acetyltransferases belonging to distinct protein families influence polyglutamine pathology. We found that flies expressing a mutant form of the Huntingtin protein (Httex1pQ93) exhibit reduced viability, which is further decreased by partial loss of Pcaf or nejire, while the tested MYST family acetyltransferases did not affect pathology. Reduced levels of Pcaf also led to the increased degeneration of photoreceptor neurons in the retina. Overexpression of Pcaf, however, was not sufficient to ameliorate these phenotypes, and the level of soluble Pcaf is unchanged in Httex1pQ93-expressing flies. Thus, our results indicate that while Pcaf has a significant impact on Huntington's disease pathology, therapeutic strategies aimed at elevating its levels are likely to be ineffective in ameliorating Huntington's disease pathology; however, strategies that aim to increase the specific activity of Pcaf remain to be tested.

Published

2012

17. Mithramycin Is a Gene-Selective Sp1 Inhibitor That Identifies a Biological Intersection between Cancer and Neurodegeneration

Author

Sleiman, Sama F, Langley, Brett C, Basso, Manuela, Berlin, Jill, Xia, Li, Payappilly, Jimmy B, Kharel, Madan K, Guo, Hengchang, Marsh, J Lawrence, Thompson, Leslie Michels, Mahishi, Lata, Ahuja, Preeti, MacLellan, W Robb, Geschwind, Daniel H, Coppola, Giovanni, Rohr, Jürgen, and Ratan, Rajiv R

Subjects

Biomedical and Clinical Sciences, Neurosciences, Cancer, Rare Diseases, Neurodegenerative, Genetics, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, 2.1 Biological and endogenous factors, Aetiology, Neurological, Analysis of Variance, Animals, Animals, Genetically Modified, Antibiotics, Antineoplastic, Blotting, Western, Cell Survival, Cells, Cultured, Cerebral Cortex, Chromatin Immunoprecipitation, Drosophila, Neurons, Plicamycin, Rats, Rats, Sprague-Dawley, Sp1 Transcription Factor, Structure-Activity Relationship, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery

Abstract

Oncogenic transformation of postmitotic neurons triggers cell death, but the identity of genes critical for degeneration remain unclear. The antitumor antibiotic mithramycin prolongs survival of mouse models of Huntington's disease in vivo and inhibits oxidative stress-induced death in cortical neurons in vitro. We had correlated protection by mithramycin with its ability to bind to GC-rich DNA and globally displace Sp1 family transcription factors. To understand how antitumor drugs prevent neurodegeneration, here we use structure-activity relationships of mithramycin analogs to discover that selective DNA-binding inhibition of the drug is necessary for its neuroprotective effect. We identify several genes (Myc, c-Src, Hif1α, and p21(waf1/cip1)) involved in neoplastic transformation, whose altered expression correlates with protective doses of mithramycin or its analogs. Most interestingly, inhibition of one these genes, Myc, is neuroprotective, whereas forced expression of Myc induces Rattus norvegicus neuronal cell death. These results support a model in which cancer cell transformation shares key genetic components with neurodegeneration.

Published

2011

18. ERK activation by the polyphenols fisetin and resveratrol provides neuroprotection in multiple models of Huntington's disease

Author

Maher, Pamela, Dargusch, Richard, Bodai, Laszlo, Gerard, Paul E, Purcell, Judith M, and Marsh, J Lawrence

Subjects

Complementary and Integrative Health, Neurodegenerative, Huntington's Disease, Orphan Drug, Neurosciences, Rare Diseases, Brain Disorders, Neurological, Animals, Disease Models, Animal, Drosophila, Enzyme Activation, Extracellular Signal-Regulated MAP Kinases, Flavonoids, Flavonols, Gene Dosage, Gene Expression Regulation, Huntingtin Protein, Huntington Disease, JNK Mitogen-Activated Protein Kinases, Mice, Motor Activity, Nerve Tissue Proteins, Neuroprotective Agents, Nuclear Proteins, PC12 Cells, Rats, Resveratrol, Stilbenes, Survival Analysis, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Huntington's disease (HD) is an inherited, progressive and ultimately fatal neurodegenerative disorder that is characterized by psychiatric, cognitive and motor symptoms. Among the pathways implicated in HD are those involving mitogen-activated protein kinase signaling and particularly the Ras-extracellular signal-regulated kinase (ERK) cascade. Studies in both cells and animal models suggest that ERK activation might provide a novel therapeutic target for the treatment of HD but compounds that specifically activate ERK are few. To test the hypothesis that pharmaceutical activation of ERK might be protective for HD, a polyphenol, fisetin, which was previously shown to activate the Ras-ERK cascade, was tested in three different models of HD: PC12 cells expressing mutant Httex1 under the control of an inducible promoter, Drosophila expressing mutant Httex1 and the R6/2 mouse model of HD. The results indicate that fisetin can reduce the impact of mutant huntingtin in each of these disease models. Prompted by this observation, we determined that the related polyphenol, resveratrol, also activates ERK and is protective in HD models. Notably, although more than a dozen small molecule inhibitors of ERK activation are in clinical trials, very few small molecule activators of ERK signaling are reported. Thus, fisetin, resveratrol and related compounds might be useful for the treatment of HD by virtue of their unique ability to activate ERK.

Published

2011

19. A Two-Step Path to Inclusion Formation of Huntingtin Peptides Revealed by Number and Brightness Analysis

Author

Ossato, Giulia, Digman, Michelle A, Aiken, Charity, Lukacsovich, Tamas, Marsh, J Lawrence, and Gratton, Enrico

Subjects

Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, Huntington's Disease, Brain Disorders, Neurodegenerative, Neurosciences, Generic health relevance, Neurological, Animals, COS Cells, Calibration, Chlorocebus aethiops, Green Fluorescent Proteins, Humans, Huntingtin Protein, Microscopy, Confocal, Molecular Imaging, Nerve Tissue Proteins, Nuclear Proteins, Peptide Fragments, Peptides, Protein Multimerization, Protein Structure, Quaternary, Rats, Physical Sciences, Chemical Sciences, Biophysics, Biological sciences, Chemical sciences, Physical sciences

Abstract

Protein aggregation is a hallmark of several neurodegenerative diseases including Huntington's disease. We describe the use of the recently developed number and brightness method (N&B) that uses confocal images to monitor aggregation of Huntingtin exon 1 protein (Httex1p) directly in living cells. N&B measures the molecular brightness of protein aggregates in the entire cell noninvasively based on intensity fluctuations at each pixel in an image. N&B applied to mutant Httex1p in living cells showed a two-step pathway leading to inclusion formation that is polyQ length dependent and involves four phases. An initial phase of monomer accumulation is followed by formation of small oligomers (5-15 proteins); as protein concentration increases, an inclusion is seeded and forms in the cytoplasm; the growing inclusion recruits most of the Httex1p and depletes the cell leaving only a low concentration of monomers. The behavior of Httex1p in COS-7 and ST14A cells is compared.

Published

2010

20. SIRT2 inhibition achieves neuroprotection by decreasing sterol biosynthesis

Author

Luthi-Carter, Ruth, Taylor, David M, Pallos, Judit, Lambert, Emmanuel, Amore, Allison, Parker, Alex, Moffitt, Hilary, Smith, Donna L, Runne, Heike, Gokce, Ozgun, Kuhn, Alexandre, Xiang, Zhongmin, Maxwell, Michele M, Reeves, Steven A, Bates, Gillian P, Neri, Christian, Thompson, Leslie M, Marsh, J Lawrence, and Kazantsev, Aleksey G

Subjects

Genetics, Rare Diseases, Huntington's Disease, Neurosciences, Neurodegenerative, Brain Disorders, Aetiology, 2.1 Biological and endogenous factors, Neurological, Analysis of Variance, Animals, Blotting, Western, Brain, Caenorhabditis elegans, Drosophila, Gene Expression Profiling, Gene Expression Regulation, Huntington Disease, Immunohistochemistry, Mice, Microscopy, Confocal, Neuroprotective Agents, Sirtuin 2, Sterol Regulatory Element Binding Protein 2, Sterols, cholesterol, Huntington's disease, metabolism, sirtuin, transcription factor SREBP-2

Abstract

Huntington's disease (HD), an incurable neurodegenerative disorder, has a complex pathogenesis including protein aggregation and the dysregulation of neuronal transcription and metabolism. Here, we demonstrate that inhibition of sirtuin 2 (SIRT2) achieves neuroprotection in cellular and invertebrate models of HD. Genetic or pharmacologic inhibition of SIRT2 in a striatal neuron model of HD resulted in gene expression changes including significant down-regulation of RNAs responsible for sterol biosynthesis. Whereas mutant huntingtin fragments increased sterols in neuronal cells, SIRT2 inhibition reduced sterol levels via decreased nuclear trafficking of SREBP-2. Importantly, manipulation of sterol biosynthesis at the transcriptional level mimicked SIRT2 inhibition, demonstrating that the metabolic effects of SIRT2 inhibition are sufficient to diminish mutant huntingtin toxicity. These data identify SIRT2 inhibition as a promising avenue for HD therapy and elucidate a unique mechanism of SIRT2-inhibitor-mediated neuroprotection. Furthermore, the ascertainment of SIRT2's role in regulating cellular metabolism demonstrates a central function shared with other sirtuin proteins.

Published

2010

21. IKK phosphorylates Huntingtin and targets it for degradation by the proteasome and lysosome

Author

Thompson, Leslie Michels, Aiken, Charity T, Kaltenbach, Linda S, Agrawal, Namita, Illes, Katalin, Khoshnan, Ali, Martinez-Vincente, Marta, Arrasate, Montserrat, O'Rourke, Jacqueline Gire, Khashwji, Hasan, Lukacsovich, Tamas, Zhu, Ya-Zhen, Lau, Alice L, Massey, Ashish, Hayden, Michael R, Zeitlin, Scott O, Finkbeiner, Steven, Green, Kim N, LaFerla, Frank M, Bates, Gillian, Huang, Lan, Patterson, Paul H, Lo, Donald C, Cuervo, Ana Maria, Marsh, J Lawrence, and Steffan, Joan S

Subjects

Neurosciences, Aging, Rare Diseases, Neurodegenerative, Huntington's Disease, Brain Disorders, Orphan Drug, Underpinning research, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Aetiology, Generic health relevance, Neurological, Animals, Brain, Cell Line, Humans, Huntingtin Protein, I-kappa B Kinase, Lysosomes, Mice, Nerve Tissue Proteins, Nuclear Proteins, Phosphorylation, Proteasome Endopeptidase Complex, Protein Structure, Tertiary, Rats, Rats, Sprague-Dawley, Solubility, Ubiquitination, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Expansion of the polyglutamine repeat within the protein Huntingtin (Htt) causes Huntington's disease, a neurodegenerative disease associated with aging and the accumulation of mutant Htt in diseased neurons. Understanding the mechanisms that influence Htt cellular degradation may target treatments designed to activate mutant Htt clearance pathways. We find that Htt is phosphorylated by the inflammatory kinase IKK, enhancing its normal clearance by the proteasome and lysosome. Phosphorylation of Htt regulates additional post-translational modifications, including Htt ubiquitination, SUMOylation, and acetylation, and increases Htt nuclear localization, cleavage, and clearance mediated by lysosomal-associated membrane protein 2A and Hsc70. We propose that IKK activates mutant Htt clearance until an age-related loss of proteasome/lysosome function promotes accumulation of toxic post-translationally modified mutant Htt. Thus, IKK activation may modulate mutant Htt neurotoxicity depending on the cell's ability to degrade the modified species.

Published

2009

22. Phosphorylation of Threonine 3 IMPLICATIONS FOR HUNTINGTIN AGGREGATION AND NEUROTOXICITY*

Author

Aiken, Charity T, Steffan, Joan S, Guerrero, Cortnie M, Khashwji, Hasan, Lukacsovich, Tamas, Simmons, Danielle, Purcell, Judy M, Menhaji, Kimia, Zhu, Ya-Zhen, Green, Kim, LaFerla, Frank, Huang, Lan, Thompson, Leslie Michels, and Marsh, J Lawrence

Subjects

Biochemistry and Cell Biology, Biological Sciences, Neurodegenerative, Brain Disorders, Huntington's Disease, Neurosciences, Rare Diseases, Genetics, Aetiology, 2.1 Biological and endogenous factors, Neurological, Acetylation, HeLa Cells, Humans, Huntingtin Protein, Huntington Disease, Nerve Tissue Proteins, Nuclear Proteins, Peptides, Phosphorylation, Protein Processing, Post-Translational, Protein Structure, Tertiary, Threonine, Hela Cells, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

Huntingtin (Htt) is a widely expressed protein that causes tissue-specific degeneration when mutated to contain an expanded polyglutamine (poly(Q)) domain. Although Htt is large, 350 kDa, the appearance of amino-terminal fragments of Htt in extracts of postmortem brain tissue from patients with Huntington disease (HD), and the fact that an amino-terminal fragment, Htt exon 1 protein (Httex1p), is sufficient to cause disease in models of HD, points to the importance of the amino-terminal region of Htt in the disease process. The first exon of Htt encodes 17 amino acids followed by a poly(Q) repeat of variable length and culminating with a proline-rich domain of 50 amino acids. Because modifications to this fragment have the potential to directly affect pathogenesis in several ways, we have surveyed this fragment for potential post-translational modifications that might affect Htt behavior and detected several modifications of Httex1p. Here we report that the most prevalent modifications of Httex1p are NH(2)-terminal acetylation and phosphorylation of threonine 3 (pThr-3). We demonstrate that pThr-3 occurs on full-length Htt in vivo, and that this modification affects the aggregation and pathogenic properties of Htt. Thus, therapeutic strategies that modulate these events could in turn affect Htt pathogenesis.

Published

2009

23. Inhibition of specific HDACs and sirtuins suppresses pathogenesis in a Drosophila model of Huntington’s disease

Author

Pallos, Judit, Bodai, Laszlo, Lukacsovich, Tamas, Purcell, Judith M, Steffan, Joan S, Thompson, Leslie Michels, and Marsh, J Lawrence

Subjects

Neurodegenerative, Neurosciences, Brain Disorders, Aging, Genetics, Rare Diseases, Huntington's Disease, 2.1 Biological and endogenous factors, Aetiology, Neurological, Animals, Disease Models, Animal, Down-Regulation, Drosophila, Drosophila Proteins, Histone Deacetylase 1, Histone Deacetylase Inhibitors, Histone Deacetylases, Humans, Huntington Disease, Repressor Proteins, Sirtuins, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Huntington's disease (HD) is associated with transcriptional dysregulation, and multiple studies with histone deacetylase (HDAC) inhibitors suggest that global approaches for restoring transcriptional balance and appropriate protein acetylation are therapeutically promising. To determine whether more targeted approaches might be effective, we have tested the impact of all the HDACs in Drosophila on Huntingtin (Htt)-induced pathology. Among the zinc-dependent or 'classic' HDACs, we find that neurodegeneration is most sensitive to levels of Rpd3. We also find that among the NAD(+)-dependent class III deacetylases, genetic or pharmacological reduction of either Sir2 or Sirt2 provides neuroprotection to Htt-challenged animals and that even greater neuroprotection is achieved when Rpd3 and Sir2 are simultaneously reduced. Our experiments suggest that longevity promoting strategies may be distinct from those that protect against neurodegeneration in Drosophila challenged with mutant human Htt. These results highlight a novel therapeutic approach for HD in the form of Sir2 inhibition and possible combinatorial inhibition of Sir2 and Rpd3.

Published

2008

24. CEP-1347 reduces mutant huntingtin-associated neurotoxicity and restores BDNF levels in R6/2 mice

Author

Apostol, Barbara L, Simmons, Danielle A, Zuccato, Chiara, Illes, Katalin, Pallos, Judit, Casale, Malcolm, Conforti, Paola, Ramos, Catarina, Roarke, Margaret, Kathuria, Satish, Cattaneo, Elena, Marsh, J Lawrence, and Thompson, Leslie Michels

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Rare Diseases, Brain Disorders, Neurosciences, Neurodegenerative, Huntington's Disease, 2.1 Biological and endogenous factors, Aetiology, Neurological, Animals, Animals, Genetically Modified, Brain-Derived Neurotrophic Factor, Carbazoles, Cell Line, Disease Models, Animal, Drosophila melanogaster, Enzyme Activation, Enzyme Inhibitors, Extracellular Signal-Regulated MAP Kinases, Humans, Huntingtin Protein, Huntington Disease, Indole Alkaloids, JNK Mitogen-Activated Protein Kinases, Mice, Molecular Structure, Nerve Tissue Proteins, Neuroprotective Agents, Nuclear Proteins, Phenotype, Rats, Psychology, Cognitive Sciences, Neurology & Neurosurgery, Biochemistry and cell biology

Abstract

Huntington's disease (HD) is a devastating neurodegenerative disorder caused by an expanded polyglutamine repeat within the protein Huntingtin (Htt). We previously reported that mutant Htt expression activates the ERK1/2 and JNK pathways [Apostol, B.L., Illes, K., Pallos, J., Bodai, L., Wu, J., Strand, A., Schweitzer, E.S., Olson, J.M., Kazantsev, A., Marsh, J.L., Thompson, L.M., 2006. Mutant huntingtin alters MAPK signaling pathways in PC12 and striatal cells: ERK1/2 protects against mutant huntingtin-associated toxicity. Hum. Mol. Genet. 15, 273-285]. Chemical and genetic modulation of these pathways promotes cell survival and death, respectively. Here we test the ability of two closely related compounds, CEP-11004 and CEP-1347, which inhibit Mixed Lineage Kinases (MLKs) and are neuroprotective, to suppress mutant Htt-mediated pathogenesis in multiple model systems. CEP-11004/CEP-1347 treatment significantly decreased toxicity in mutant Htt-expressing cells that evoke a strong JNK response. However, suppression of cellular dysfunction in cell lines that exhibit only mild Htt-associated toxicity and little JNK activation was associated with activation of ERK1/2. These compounds also reduced neurotoxicity in immortalized striatal neurons from mutant knock-in mice and Drosophila expressing a mutant Htt fragment. Finally, CEP-1347 improved motor performance in R6/2 mice and restored expression of BDNF, a critical neurotrophic factor that is reduced in HD. These studies suggest a novel therapeutic approach for a currently untreatable neurodegenerative disease, HD, via CEP-1347 up-regulation of BDNF.

Published

2008

25. The first 17 amino acids of Huntingtin modulate its sub-cellular localization, aggregation and effects on calcium homeostasis

Author

Rockabrand, Erica, Slepko, Natalia, Pantalone, Antonello, Nukala, Vidya N, Kazantsev, Aleksey, Marsh, J Lawrence, Sullivan, Patrick G, Steffan, Joan S, Sensi, Stefano L, and Thompson, Leslie Michels

Subjects

Biochemistry and Cell Biology, Biological Sciences, Neurodegenerative, Huntington's Disease, Brain Disorders, Neurosciences, Rare Diseases, Aetiology, 2.1 Biological and endogenous factors, Neurological, Animals, Calcium, Cell Membrane, Cerebellar Cortex, Cytoplasm, Electron Transport Chain Complex Proteins, Endoplasmic Reticulum, Golgi Apparatus, Homeostasis, Huntingtin Protein, Male, Membrane Potential, Mitochondrial, Mitochondria, Nerve Tissue Proteins, Nuclear Proteins, PC12 Cells, Peptides, Proline, Protein Structure, Tertiary, Rats, Rats, Sprague-Dawley, Reactive Oxygen Species, Transfection, Medical and Health Sciences, Genetics & Heredity, Genetics

Abstract

A truncated form of the Huntington's disease (HD) protein that contains the polyglutamine repeat, Httex1p, causes HD-like phenotypes in multiple model organisms. Molecular signatures of pathogenesis appear to involve distinct domains within this polypeptide. We studied the contribution of each domain, singly or in combination, to sub-cellular localization, aggregation and intracellular Ca2+ ([Ca2+]i) dynamics in cells. We demonstrate that sub-cellular localization is most strongly influenced by the first 17 amino acids, with this sequence critically controlling Httex1p mitochondrial localization and also promoting association with the endoplasmic reticulum (ER) and Golgi. This domain also enhances the formation of visible aggregates and together with the expanded polyQ repeat acutely disrupts [Ca2+]i levels in glutamate-challenged PC12 cells. Isolated cortical mitochondria incubated with Httex1p resulted in uncoupling and depolarization of these organelles, further supporting the idea that Httex1p-dependent mitochondrial dysfunction could be instrumental in promoting acute Ca2+ dyshomeostasis. Interestingly, neither mitochondrial nor ER associations seem to be required to promote long-term [Ca2+]i dyshomeostasis.

Published

2007

26. Drosophila in the Study of Neurodegenerative Disease

Author

Marsh, J Lawrence and Thompson, Leslie Michels

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Neurodegenerative, Neurological, Generic health relevance, Good Health and Well Being, Animals, Disease Models, Animal, Drosophila, Humans, Neurodegenerative Diseases, Cognitive Sciences, Neurology & Neurosurgery, Biological psychology

Abstract

As populations benefit from increasing lifespans, neurodegenerative diseases have emerged as a critical health concern. How can the fruit fly, Drosophila melanogaster, contribute to curing human diseases of the nervous system? A growing number of neurodegenerative diseases, as well as other human diseases, are being modeled in Drosophila and used as a platform to identify and validate cellular pathways that contribute to neurodegeneration and to identify promising therapeutic targets by using a variety of approaches from screens to target validation. The unique properties and tools available in the Drosophila system, coupled with the fact that testing in vivo has proven highly productive, have accelerated the progress of testing therapeutic strategies in mice and, ultimately, humans. This review highlights selected recent applications to illustrate the use of Drosophila in studying neurodegenerative diseases.

Published

2006

27. Green tea (−)-epigallocatechin-gallate modulates early events in huntingtin misfolding and reduces toxicity in Huntington's disease models

Author

Ehrnhoefer, Dagmar E, Duennwald, Martin, Markovic, Phoebe, Wacker, Jennifer L, Engemann, Sabine, Roark, Margaret, Legleiter, Justin, Marsh, J Lawrence, Thompson, Leslie M, Lindquist, Susan, Muchowski, Paul J, and Wanker, Erich E

Subjects

Complementary and Integrative Health, Brain Disorders, Huntington's Disease, Rare Diseases, Neurosciences, Orphan Drug, Neurodegenerative, 2.1 Biological and endogenous factors, Aetiology, Neurological, Animals, Animals, Genetically Modified, Camellia sinensis, Catechin, Drosophila melanogaster, Exons, Humans, Huntingtin Protein, Huntington Disease, In Vitro Techniques, Microscopy, Atomic Force, Models, Biological, Motor Neurons, Multiprotein Complexes, Mutation, Nerve Degeneration, Nerve Tissue Proteins, Nuclear Proteins, Photoreceptor Cells, Invertebrate, Phytotherapy, Protein Conformation, Protein Folding, Protein Structure, Quaternary, Recombinant Fusion Proteins, Saccharomyces cerevisiae, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Huntington's disease (HD) is a progressive neurodegenerative disorder for which only symptomatic treatments of limited effectiveness are available. Preventing early misfolding steps and thereby aggregation of the polyglutamine (polyQ)-containing protein huntingtin (htt) in neurons of patients may represent an attractive therapeutic strategy to postpone the onset and progression of HD. Here, we demonstrate that the green tea polyphenol (-)-epigallocatechin-3-gallate (EGCG) potently inhibits the aggregation of mutant htt exon 1 protein in a dose-dependent manner. Dot-blot assays and atomic force microscopy studies revealed that EGCG modulates misfolding and oligomerization of mutant htt exon 1 protein in vitro, indicating that it interferes with very early events in the aggregation process. Also, EGCG significantly reduced polyQ-mediated htt protein aggregation and cytotoxicity in an yeast model of HD. When EGCG was fed to transgenic HD flies overexpressing a pathogenic htt exon 1 protein, photoreceptor degeneration and motor function improved. These results indicate that modulators of htt exon 1 misfolding and oligomerization like EGCG are likely to reduce polyQ-mediated toxicity in vivo. Our studies may provide the basis for the development of a novel pharmacotherapy for HD and related polyQ disorders.

Published

2006

28. Biologically active molecules that reduce polyglutamine aggregation and toxicity

Author

Desai, Urvee A, Pallos, Judit, K., Aye Aye, Stockwell, Brent R, Thompson, Leslie Michels, Marsh, J Lawrence, and Diamond, Marc I

Subjects

Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, Brain Disorders, Neurodegenerative, Orphan Drug, Huntington's Disease, Neurosciences, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Neurological, Androgen Receptor Antagonists, Animals, Biological Assay, Cell Line, Dose-Response Relationship, Drug, Drosophila melanogaster, Drug Evaluation, Preclinical, Drugs, Investigational, Fluorescence Resonance Energy Transfer, Humans, Huntingtin Protein, Huntington Disease, Molecular Structure, Nerve Tissue Proteins, Neurodegenerative Diseases, Nuclear Proteins, PC12 Cells, Peptides, Protein Folding, Rats, Receptors, Androgen, Structure-Activity Relationship, Trinucleotide Repeat Expansion, Medical and Health Sciences, Genetics & Heredity, Genetics

Abstract

Polyglutamine expansion in certain proteins causes neurodegeneration in inherited disorders such as Huntington disease and X-linked spinobulbar muscular atrophy. Polyglutamine tracts promote protein aggregation in vitro and in vivo with a strict length-dependence that strongly implicates alternative protein folding and/or aggregation as a proximal cause of cellular toxicity and neurodegeneration. We used an intracellular polyglutamine protein aggregation assay based on fluorescence resonance energy transfer (FRET) to identify inhibitors of androgen receptor (AR) aggregation in three libraries of biologically active small molecules: the Annotated Compound Library, the NINDS Custom Collection and a kinase inhibitor collection. In the primary screen 10 compounds reduced AR aggregation. While 10/10 also reduced huntingtin (Htt) exon 1 aggregation, only 2/10 reduced aggregation of pure polyglutamine peptides. In a PC-12 model 9/10 compounds reduced aggregation. Five out of nine compounds tested in an Htt exon 1 assay of neurodegeneration in Drosophila partially rescued the phenotype. Three of the five compounds effective in flies are FDA-approved drugs. These compounds provide new leads for therapeutic development for the polyglutamine diseases based on their efficacy in mammalian cells and a Drosophila model. The high predictive value of the primary screen suggests that the FRET-based screening assay may be useful for further primary and secondary screens for genes or small molecules that inhibit polyglutamine protein aggregation.

Published

2006

29. Mutant huntingtin alters MAPK signaling pathways in PC12 and striatal cells: ERK1/2 protects against mutant huntingtin-associated toxicity

Author

Apostol, Barbara L, Illes, Katalin, Pallos, Judit, Bodai, Laszlo, Wu, Jun, Strand, Andrew, Schweitzer, Erik S, Olson, James M, Kazantsev, Aleksey, Marsh, J Lawrence, and Thompson, Leslie Michels

Subjects

Rare Diseases, Neurosciences, Brain Disorders, Neurodegenerative, Huntington's Disease, 2.1 Biological and endogenous factors, Aetiology, Neurological, Animals, Blotting, Northern, Cell Line, Cell Survival, DNA Primers, Enzyme Activation, Gene Expression Profiling, Huntingtin Protein, Huntington Disease, Microarray Analysis, Mitogen-Activated Protein Kinases, Mutation, Nerve Tissue Proteins, Nuclear Proteins, Rats, Signal Transduction, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Huntington's disease (HD) is a devastating neurodegenerative disorder caused by an expanded polyglutamine (polyQ) tract within the huntingtin protein (Htt). Identifying the pathways that are altered in response to the mutant protein is crucial for understanding the cellular processes impacted by the disease as well as for the rational development of effective pharmacological interventions. Here, expression profiling of a cellular HD model identifies genes that implicate altered mitogen-activated protein kinase (MAPK) signaling. Targeted biochemical studies and pharmacological modulation of these MAPK pathways suggest that mutant Htt affects signaling at upstream points such that both ERK and JNK are activated. Modulation of the ERK pathway suggests that this pathway is associated with cell survival, whereas inhibition of JNK was found to effectively suppress pathogenesis. These studies suggest that pharmacological intervention in MAPK pathways, particularly at the level of ERK activation, may be an appropriate approach to HD therapy.

Published

2006

30. Suppression of Huntington's disease pathology in Drosophila by human single-chain Fv antibodies

Author

Wolfgang, William J, Miller, Todd W, Webster, Jack M, Huston, James S, Thompson, Leslie M, Marsh, J Lawrence, and Messer, Anne

Subjects

Rare Diseases, Huntington's Disease, Neurosciences, Biotechnology, Neurodegenerative, Dementia, Bioengineering, Brain Disorders, Acquired Cognitive Impairment, Aging, Aetiology, 2.1 Biological and endogenous factors, Neurological, Animals, Blotting, Western, Drosophila, Epitopes, Humans, Huntingtin Protein, Huntington Disease, Immunoglobulin Fragments, Immunotherapy, Lymphokines, Nerve Tissue Proteins, Nuclear Proteins, Protein Engineering, Sialoglycoproteins, Survival Analysis, neurodegeneration, antibody engineering, immunotherapy, nanomedicine

Abstract

Misfolded neuronal proteins have been identified in a number of neurodegenerative disorders and have been implicated in the pathogenesis of diseases that include Alzheimer's disease, Parkinson's disease, prion-based dementia, Huntington's disease (HD), and other polyglutamine diseases. Although underlying mechanisms remain the subject of ongoing research, it is clear that aberrant processing, protein degradation, and aggregate formation or spurious protein association of the abnormal neuronal proteins may be critical factors in disease progression. Recent work in these diseases has demonstrated in vitro that specific engineered antibody species, peptides, or other general agents may suppress the formation of aggregates. We have modified an approach with intracellularly expressed single-chain Fv (sFv) antibodies (intrabodies) that bind with unique HD protein epitopes. In cell and tissue culture models of HD, anti-N-terminal huntingtin intrabodies (C4 sFv) reduce aggregation and cellular toxicity. Here, we present the crucial experiment of intrabody-mediated in vivo suppression of neuropathology, using a Drosophila model of HD. In the presence of the C4 sFv intrabody, the proportion of HD flies surviving to adulthood increases from 23% to 100%, and the mean and maximum lifespan of adult HD flies is significantly prolonged. Neurodegeneration and formation of visible huntingtin aggregates are slowed. We conclude from this investigation that engineered intrabodies are a potential new class of therapeutic agents for the treatment of neurodegenerative diseases. They may also serve as tools for drug discovery and validation of sites on mutant neuronal proteins that could be exploited for rational drug design.

Published

2005

31. A potent small molecule inhibits polyglutamine aggregation in Huntington's disease neurons and suppresses neurodegeneration in vivo

Author

Zhang, Xiaoqian, Smith, Donna L, Meriin, Anatoli B, Engemann, Sabine, Russel, Deborah E, Roark, Margo, Washington, Shetia L, Maxwell, Michele M, Marsh, J Lawrence, Thompson, Leslie Michels, Wanker, Erich E, Young, Anne B, Housman, David E, Bates, Gillian P, Sherman, Michael Y, and Kazantsev, Aleksey G

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Medicinal and Biomolecular Chemistry, Biological Sciences, Genetics, Chemical Sciences, Orphan Drug, Huntington's Disease, Neurodegenerative, Brain Disorders, Neurosciences, Rare Diseases, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Neurological, Anilides, Animals, Brain, Dimerization, Disease Models, Animal, Drosophila, Huntington Disease, Inhibitory Concentration 50, Mice, Mice, Transgenic, Neurodegenerative Diseases, Neurons, Peptides, Polycyclic Aromatic Hydrocarbons, Structure-Activity Relationship, Sulfonamides, high-throughput screen, small-molecule therapeutics, R6/2 brain slices, genetic disease

Abstract

Polyglutamine (polyQ) disorders, including Huntington's disease (HD), are caused by expansion of polyQ-encoding repeats within otherwise unrelated gene products. In polyQ diseases, the pathology and death of affected neurons are associated with the accumulation of mutant proteins in insoluble aggregates. Several studies implicate polyQ-dependent aggregation as a cause of neurodegeneration in HD, suggesting that inhibition of neuronal polyQ aggregation may be therapeutic in HD patients. We have used a yeast-based high-throughput screening assay to identify small-molecule inhibitors of polyQ aggregation. We validated the effects of four hit compounds in mammalian cell-based models of HD, optimized compound structures for potency, and then tested them in vitro in cultured brain slices from HD transgenic mice. These efforts identified a potent compound (IC50=10 nM) with long-term inhibitory effects on polyQ aggregation in HD neurons. Testing of this compound in a Drosophila HD model showed that it suppresses neurodegeneration in vivo, strongly suggesting an essential role for polyQ aggregation in HD pathology. The aggregation inhibitors identified in this screen represent four primary chemical scaffolds and are strong lead compounds for the development of therapeutics for human polyQ diseases.

Published

2005

32. SUMO Modification of Huntingtin and Huntington's Disease Pathology

Author

Steffan, Joan S, Agrawal, Namita, Pallos, Judit, Rockabrand, Erica, Trotman, Lloyd C, Slepko, Natalia, Illes, Katalin, Lukacsovich, Tamas, Zhu, Ya-Zhen, Cattaneo, Elena, Pandolfi, Pier Paolo, Thompson, Leslie Michels, and Marsh, J Lawrence

Subjects

Biochemistry and Cell Biology, Biological Sciences, Neurosciences, Rare Diseases, Brain Disorders, Neurodegenerative, Huntington's Disease, Aetiology, 2.1 Biological and endogenous factors, Neurological, Animals, Animals, Genetically Modified, Cell Line, Cell Nucleus, Corpus Striatum, Cytoplasm, Drosophila, Genes, MDR, HeLa Cells, Humans, Huntingtin Protein, Huntington Disease, Lysine, Mutation, Nerve Degeneration, Nerve Tissue Proteins, Neurons, Nuclear Proteins, Proline, Promoter Regions, Genetic, Rats, Recombinant Fusion Proteins, SUMO-1 Protein, Transcription, Genetic, Transfection, Ubiquitin, Hela Cells, General Science & Technology

Abstract

Huntington's disease (HD) is characterized by the accumulation of a pathogenic protein, Huntingtin (Htt), that contains an abnormal polyglutamine expansion. Here, we report that a pathogenic fragment of Htt (Httex1p) can be modified either by small ubiquitin-like modifier (SUMO)-1 or by ubiquitin on identical lysine residues. In cultured cells, SUMOylation stabilizes Httex1p, reduces its ability to form aggregates, and promotes its capacity to repress transcription. In a Drosophila model of HD, SUMOylation of Httex1p exacerbates neurodegeneration, whereas ubiquitination of Httex1p abrogates neurodegeneration. Lysine mutations that prevent both SUMOylation and ubiquitination of Httex1p reduce HD pathology, indicating that the contribution of SUMOylation to HD pathology extends beyond preventing Htt ubiquitination and degradation.

Published

2004

33. A Rapid Cellular FRET Assay of Polyglutamine Aggregation Identifies a Novel Inhibitor

Author

Pollitt, Sonia K, Pallos, Judit, Shao, Jieya, Desai, Urvee A, K, Aye Aye, Thompson, Leslie Michels, Marsh, J Lawrence, and Diamond, Marc I

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Aging, Neurodegenerative, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Neurological, Amides, Animals, Animals, Genetically Modified, Biological Assay, COS Cells, Cell Death, Disease Models, Animal, Down-Regulation, Drosophila melanogaster, Drug Evaluation, Preclinical, Enzyme Inhibitors, Fluorescence Resonance Energy Transfer, Humans, Huntingtin Protein, Inclusion Bodies, Intracellular Signaling Peptides and Proteins, Nerve Tissue Proteins, Neurodegenerative Diseases, Nuclear Proteins, Peptides, Photoreceptor Cells, Invertebrate, Protein Folding, Protein Serine-Threonine Kinases, Pyridines, Signal Transduction, Trinucleotide Repeat Expansion, rho-Associated Kinases, Cognitive Sciences, Neurology & Neurosurgery, Biological psychology

Abstract

Many neurodegenerative diseases, including tauopathies, Parkinson's disease, amyotrophic lateral sclerosis, and the polyglutamine diseases, are characterized by intracellular aggregation of pathogenic proteins. It is difficult to study modifiers of this process in intact cells in a high-throughput and quantitative manner, although this could facilitate molecular insights into disease pathogenesis. Here we introduce a high-throughput assay to measure intracellular polyglutamine protein aggregation using fluorescence resonance energy transfer (FRET). We screened over 2800 biologically active small molecules for inhibitory activity and have characterized one lead compound in detail. Y-27632, an inhibitor of the Rho-associated kinase p160ROCK, diminished polyglutamine protein aggregation (EC(50) congruent with 5 microM) and reduced neurodegeneration in a Drosophila model of polyglutamine disease. This establishes a novel high-throughput approach to study protein misfolding and aggregation associated with neurodegenerative diseases and implicates a signaling pathway of previously unrecognized importance in polyglutamine protein processing.

Published

2003

34. Fly models of Huntington's disease

Author

Marsh, J Lawrence, Pallos, Judit, and Thompson, Leslie M

Subjects

Brain Disorders, Rare Diseases, Huntington's Disease, Neurosciences, Neurodegenerative, Neurological, Animals, Disease Models, Animal, Drosophila, Humans, Huntington Disease, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Can Drosophila models be engineered that accurately reflect Huntington's disease (HD) and other neurological diseases and can they contribute to the search for treatments and cures? A number of publications seem to provide a resounding yes to that question. Here we seek to review some of the salient features of these models.

Published

2003

35. A bivalent Huntingtin binding peptide suppresses polyglutamine aggregation and pathogenesis in Drosophila.

Author

Kazantsev, Aleksey, Walker, Heli A, Slepko, Natalia, Bear, James E, Preisinger, Elizabeth, Steffan, Joan S, Zhu, Ya-Zhen, Gertler, Frank B, Housman, David E, Marsh, J Lawrence, and Thompson, Leslie M

Subjects

Neurons, Cells, Cultured, Cell Line, COS Cells, Animals, Drosophila, Glutathione Transferase, Peptides, Luminescent Proteins, Green Fluorescent Proteins, Nerve Tissue Proteins, Nuclear Proteins, Recombinant Fusion Proteins, DNA, Complementary, Epitopes, Microscopy, Fluorescence, Microscopy, Video, Blotting, Western, Transfection, Suppression, Genetic, Repetitive Sequences, Amino Acid, Protein Structure, Tertiary, Protein Binding, Kinetics, Mutation, Plasmids, Time Factors, Molecular Sequence Data, Photoreceptor Cells, Invertebrate, Cells, Cultured, DNA, Complementary, Microscopy, Fluorescence, Video, Blotting, Western, Suppression, Genetic, Repetitive Sequences, Amino Acid, Protein Structure, Tertiary, Photoreceptor Cells, Invertebrate, Neurodegenerative, Rare Diseases, Huntington's Disease, Neurosciences, Brain Disorders, 2.1 Biological and endogenous factors, Neurological, Developmental Biology, Medical and Health Sciences, Biological Sciences

Abstract

Huntington disease is caused by the expansion of a polyglutamine repeat in the Huntingtin protein (Htt) that leads to degeneration of neurons in the central nervous system and the appearance of visible aggregates within neurons. We have developed and tested suppressor polypeptides that bind mutant Htt and interfere with the process of aggregation in cell culture. In a Drosophila model, the most potent suppressor inhibits both adult lethality and photoreceptor neuron degeneration. The appearance of aggregates in photoreceptor neurons correlates strongly with the occurrence of pathology, and expression of suppressor polypeptides delays and limits the appearance of aggregates and protects photoreceptor neurons. These results suggest that targeting the protein interactions leading to aggregate formation may be beneficial for the design and development of therapeutic agents for Huntington disease.

Published

2002

36. EVIDENCE FOR EVOLUTIONARY DUPLICATION OF GENES IN THE DOPA DECARBOXYLASE REGION OF DROSOPHILA

Author

Eveleth, David D and Marsh, J Lawrence

Subjects

Biological Sciences, Bioinformatics and Computational Biology, Genetics, Neurodegenerative, Generic health relevance, Amino Acid Sequence, Animals, Aromatic-L-Amino-Acid Decarboxylases, Base Sequence, Biological Evolution, Chromosome Mapping, DNA Restriction Enzymes, Dopa Decarboxylase, Drosophila, Genes, Sequence Homology, Nucleic Acid, Developmental Biology, Biochemistry and cell biology

Abstract

The region surrounding the dopa decarboxylase gene (Ddc) of Drosophila contains a cluster of genes, many of which appear to be functionally related by virtue of their effects on cuticle development and/or catecholamine metabolism. In this report we describe evidence that the Ddc gene and the closely linked alpha-methyldopa hypersensitive (amd) gene share extensive sequence homology and are the products of a gene duplication event. The two genes are transcribed convergently and are separated by 2.4 kb. A gene located between Ddc and amd expresses a 2.0-kb mRNA and appears to partially overlap the Ddc gene. The organization of these transcripts implies a complex series of events giving rise to the present pattern. The patterns of expression of these genes do not support a model of coordinate regulation, but are more consistent with a pattern of duplication and divergence to various related metabolic subspecialties. These data provide the first evidence for structural relationships among genes in the 37C cluster.

Published

1986

37. MOLECULAR LOCALIZATION, DEVELOPMENTAL EXPRESSION AND NUCLEOTIDE SEQUENCE OF THE ALPHA-METHYLDOPA HYPERSENSITIVE GENE OF DROSOPHILA

Author

Marsh, J Lawrence, Erfle, Mary P, and Leeds, Carol A

Subjects

Biological Sciences, Bioinformatics and Computational Biology, Genetics, Neurodegenerative, Amino Acid Sequence, Animals, Aromatic-L-Amino-Acid Decarboxylases, Base Sequence, Codon, DNA, DNA Restriction Enzymes, Dopa Decarboxylase, Drosophila, Genes, Methyldopa, Nucleic Acid Hybridization, Developmental Biology, Biochemistry and cell biology

Abstract

The region surrounding the dopa decarboxylase gene of Drosophila contains a cluster of functionally related genes, many of which affect cuticle development and/or catecholamine metabolism. In this report we describe the molecular mapping and sequencing of a full-length cDNA copy of a transcript that maps to the alpha-methyldopa hypersensitive region. Developmental RNA blots show stage-specific patterns of transcription and multiple RNA transcripts. A 2-kb transcript is most abundant at about 12 hr of embryogenesis, and lower levels are detected throughout most of embryogenesis. Lower levels of this transcript are also detected in adults. Smaller stage-specific transcripts are detected in late third-instar larvae. This pattern of transcription is consistent with the known lethal phases and phenotypes of the alpha-methyldopa hypersensitive gene (amd). Based on map position, pattern of transcription, homology with dopa decarboxylase and association with altered DNA in mutants, we conclude that this transcript represents the amd gene.

Published

1986