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      The effects of huntingtin-lowering: what do we know so far?

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          Abstract

          Therapies targeting mutant huntingtin DNA, mRNA, and protein have a chance at becoming the first disease-modifying treatments for Huntington’s disease, a fatal inherited neurodegenerative disorder for which only symptom management treatments are available today. This review focuses on evidence addressing several key questions pertinent to huntingtin-lowering, ranging from the functions of wild-type huntingtin (wtHTT) that may be disrupted by huntingtin-lowering treatments through the various ways huntingtin can be lowered, the tolerability of wtHTT-lowering in mice and primates, what has been found in the Ionis Pharmaceutical safety trial of a huntingtin-lowering therapy, and to the question of how much mutant huntingtin may need to be lowered for a therapy to be clinically effective. We conclude that adverse consequences of lowering wtHTT in animals appear to be brain region-specific, and/or dependent upon the animal’s stage of development and the amount by which huntingtin is lowered. Therefore, safe approaches to huntingtin-lowering in patients may be to lower huntingtin only moderately, or lower huntingtin only in the most affected brain regions, or lower huntingtin allele-selectively, or all of the above. Many additional questions about huntingtin-lowering remain open, and will only be answered by upcoming clinical trials, such as whether the delivery approaches currently planned will be adequate to get the treatment to the necessary brain regions, and whether non-allele-selective huntingtin-lowering will be safe in the long run. Meantime, there is a role for preclinical research to address key knowledge gaps, including the effects of non-allele-selective huntingtin-lowering on protein trafficking and viability at the cellular level, the tolerability of wtHTT-lowering in the corticostriatal connections of the primate brain, and the effects of this lowering on the functioning of neurotransmitter systems and the transport of neurotrophic factors to the striatum.

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          Repair of double-strand breaks induced by CRISPR–Cas9 leads to large deletions and complex rearrangements

          Kärt Tomberg, Michael Kosicki, Allan Bradley (2018)
          CRISPR-Cas9 is poised to become the gene editing tool of choice in clinical contexts. Thus far, exploration of Cas9-induced genetic alterations has been limited to the immediate vicinity of the target site and distal off-target sequences, leading to the conclusion that CRISPR-Cas9 was reasonably specific. Here we report significant on-target mutagenesis, such as large deletions and more complex genomic rearrangements at the targeted sites in mouse embryonic stem cells, mouse hematopoietic progenitors and a human differentiated cell line. Using long-read sequencing and long-range PCR genotyping, we show that DNA breaks introduced by single-guide RNA/Cas9 frequently resolved into deletions extending over many kilobases. Furthermore, lesions distal to the cut site and crossover events were identified. The observed genomic damage in mitotically active cells caused by CRISPR-Cas9 editing may have pathogenic consequences.
          Article 0 comments Cited 733 times – based on 0 reviews     Review now
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            Huntingtin interacts with REST/NRSF to modulate the transcription of NRSE-controlled neuronal genes.

            Chiara Zuccato, Marzia Tartari, Andrea Crotti (2003)
            Huntingtin protein is mutated in Huntington disease. We previously reported that wild-type but not mutant huntingtin stimulates transcription of the gene encoding brain-derived neurotrophic factor (BDNF; ref. 2). Here we show that the neuron restrictive silencer element (NRSE) is the target of wild-type huntingtin activity on BDNF promoter II. Wild-type huntingtin inhibits the silencing activity of NRSE, increasing transcription of BDNF. We show that this effect occurs through cytoplasmic sequestering of repressor element-1 transcription factor/neuron restrictive silencer factor (REST/NRSF), the transcription factor that binds to NRSE. In contrast, aberrant accumulation of REST/NRSF in the nucleus is present in Huntington disease. We show that wild-type huntingtin coimmunoprecipitates with REST/NRSF and that less immunoprecipitated material is found in brain tissue with Huntington disease. We also report that wild-type huntingtin acts as a positive transcriptional regulator for other NRSE-containing genes involved in the maintenance of the neuronal phenotype. Consistently, loss of expression of NRSE-controlled neuronal genes is shown in cells, mice and human brain with Huntington disease. We conclude that wild-type huntingtin acts in the cytoplasm of neurons to regulate the availability of REST/NRSF to its nuclear NRSE-binding site and that this control is lost in the pathology of Huntington disease. These data identify a new mechanism by which mutation of huntingtin causes loss of transcription of neuronal genes.
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              Increased apoptosis and early embryonic lethality in mice nullizygous for the Huntington's disease gene homologue.

              S Zeitlin, J. Liu, D. L. Chapman (1995)
              The expansion of CAG triplet repeats in the translated region of the human HD gene, encoding a protein (huntingtin) of unknown function, is a dominant mutation leading to manifestation of Huntington's disease. Targeted disruption of the homologous mouse gene (Hdh), to examine the normal role of huntingtin, shows that this protein is functionally indispensable, since nullizygous embryos become developmentally retarded and disorganized, and die between days 8.5 and 10.5 of gestation. Based on the observation that the level of the regionalized apoptotic cell death in the embryonic ectoderm, a layer expressing the Hdh gene, is much higher than normal in the null mutants, we propose that huntingtin is involved in processes counterbalancing the operation of an apoptotic pathway.
              Article 0 comments Cited 178 times – based on 0 reviews     Review now
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                Author and article information

                Journal
                Journal ID (nlm-ta): Degener Neurol Neuromuscul Dis
                Journal ID (iso-abbrev): Degener Neurol Neuromuscul Dis
                Journal ID (publisher-id): Degenerative Neurological and Neuromuscular Disease
                Title: Degenerative Neurological and Neuromuscular Disease
                Publisher: Dove Medical Press
                ISSN (Electronic): 1179-9900
                Publication date Collection: 2019
                Publication date (Electronic): 08 March 2019
                Volume: 9
                Pages: 3-17
                Affiliations
                [1 ]CGTA Research Group, Eagan, MN, USA
                [2 ]Department of Neuroscience, University of Kentucky Medical Center, Lexington, KY, USA, rcgron0@ 123456uky.edu
                Author notes
                Correspondence: Richard C Grondin, Department of Neuroscience, University of Kentucky Medical Center, 800 Rose Street, Medical Science Bldg, MN210, Lexington, KY 40536-0298, USA, Tel +1 859 323 8925, Fax +1 859 257 3625, Email rcgron0@ 123456uky.edu
                Article
                Publisher ID: dnnd-9-003
                DOI: 10.2147/DNND.S163808
                PMC ID: 6413743
                PubMed ID: 30881191
                SO-VID: 9072b336-c004-4d61-a5f0-dd3614e72ffd
                Copyright © © 2019 Kaemmerer and Grondin. This work is published and licensed by Dove Medical Press Limited
                License:

                The full terms of this license are available at https://www.dovepress.com/terms.php and incorporate the Creative Commons Attribution – Non Commercial (unported, v3.0) License ( http://creativecommons.org/licenses/by-nc/3.0/). By accessing the work you hereby accept the Terms. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed.

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                Subject: Review

                Keywords: huntington’s disease,huntingtin-lowering,gene therapy,cortex,striatum,cag repeat disorder
                Data availability:
                Keywords: huntington’s disease, huntingtin-lowering, gene therapy, cortex, striatum, cag repeat disorder

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