Your search keyword '"HUNTINGTON'S chorea treatment"' showing total 793 results

1. Huntington's Disease Progression: A Population Modeling Approach to Characterization Using Clinical Rating Scales.

Author

Sun, Wan, Zhou, Di, Warner, John H., Langbehn, Douglas R., Hochhaus, Guenther, and Wang, Yaning

Subjects

*HUNTINGTON'S chorea treatment, *AGE distribution, *BIOLOGICAL models, *LONGITUDINAL method, *LOGISTIC regression analysis, *DISEASE progression, *FUNCTIONAL assessment, *DESCRIPTIVE statistics

Abstract

Development of effective therapeutics that slow Huntington's disease progression is a research priority that requires an understanding of natural disease progression. We applied a population‐modeling approach to describe the progression of 2 routinely used rating scales — the total motor score and the total functional capacity score. Models were fitted to data from research participants aged ≥ 18 years with Huntington's disease stage I or II at study entry (total functional capacity score ≥ 7), from a controlled clinical trial (CARE‐HD) and 2 observational studies (COHORT and Registry). A logistic model without shape factors was selected as the base model based on placebo data from CARE‐HD and validated using data from the CARE‐HD active‐treatment arms. Albeit with a smaller progression rate constant than was found in CARE‐HD, the proposed models provided reasonable predictions for both rating scales in the pooled data from COHORT and Registry and were considered suitable for use in clinical trial simulations. Results also showed that disease burden score (a product of age and expanded CAG length) is a significant covariate on both the progression rate constant and the baseline score in the total motor score model. These findings suggest that total motor score and total functional capacity progress fastest near their half‐maximal score, implying that the efficiency of clinical trials evaluating disease‐modifying therapeutics for Huntington's disease could be enhanced by enrolling patients with faster disease progression or evaluating treatment effect near their half‐maximal score, provided that the evaluated therapy is expected to be efficacious at this disease stage. [ABSTRACT FROM AUTHOR]

Published

2020

2. Quality of Care for Huntington's Disease in the United States: Findings from a National Survey of Patients and Caregivers.

Author

Anderson, Karen E., Griffin, Jack, Kinel, Al, Shaikh, Abdul R., Olofintuyi, Temitope, Ramirez, Stevan, Steinman, Joni, Yohrling, George J., and Kinel, Shari

Subjects

*DISEASE progression, *HUNTINGTON'S chorea treatment, *MEDICAL quality control, *PATIENTS' attitudes, *CAREGIVER attitudes

Abstract

Background: Little is known about the quality of care for people living with Huntington's disease (HD) in the United States. Objective: To document the current HD care experience and identify gaps in care provision in the United States. Methods: Web-based surveys for persons self-identifying as being affected by HD (PAHD, which included individuals with, or at risk for HD) or as caregivers/family members, were developed and refined with targeted input from focus groups comprised of caregivers and family members. The surveys were disseminated via social media and patient advocacy partners from April-May 2017. Results: Total valid responses numbered 797, including 585 caregiver/family respondents and 212 PAHD responses. Respondents reported care provision from HD specialty centers, primary care, movement disorder clinics, and other settings. One in five respondents reported that the person with HD was not currently receiving medical or community care. Respondents generally reported a good level of care, with HD specialists providing the highest rated healthcare experience. Caregiver/family respondents reported helping with a range of activities including budget/finances (60.5%), housekeeping (57.1%) and daily help (53.2%). Most respondents (97.9%) reported searching online, including general information about HD (86.4%), using HD social media channels (61.3%) and looking up clinical trials (59.8%). Respondents emphasized a need for support in financial planning and accessing care, and also for more HD education in the medical community. Conclusions: There is need for more support for HD patients and families. People desire more credible, accessible information. Improving resources available to patients and families should be a goal for HD organizations, along with measurement of patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2019

3. Effects of Exercise Environment and Protocol Intensity on the Efficacy of Rehabilitation Care for Patients with Huntington's Disease: A Comprehensive Review.

Author

DOLBOW, JAMES D., HAU LY, ELWERT, NICHOLAS, and GASSLER, JOHN

Subjects

EXERCISE, HUNTINGTON'S chorea treatment, MEDICAL rehabilitation, MOTOR ability, GAIT in humans, QUALITY of life

Abstract

International Journal of Exercise Science 12(3): 456-470, 2019. Huntington's disease (HD) is a neurodegenerative disease caused by astrogliosis of the putamen and caudate nucleus. Motor symptoms include progressive chorea, leading to deficits in gait, motor function, and quality of life. While many studies have examined the effects of therapeutic exercise on these factors in individuals with HD, the efficacy of such protocols has yet to be analyzed. Purpose: The purpose of this review is to analyze trends in efficacy reported by studies examining the effects of exercise on motor function, gait quality, and quality of life in individuals with HD. Methods: A literature search was performed by the primary author in September 2017. Databases include PubMed, Google Scholar Article Library, and The Cochran Article Library. Results: Though there is intrinsic variability between studies, therapeutic outcomes can be compared between settings and protocols. The increases in exercise duration/frequency and utilization of multiple supervised rehabilitation modalities in clinical/intensive inpatientbased programs resulted in greater function and psychological improvements in individuals with HD compared to those in the home/community-based programs. However, the adherence rates of high-intensity, multidisciplinary protocols are lower than less intensive regimens. Conclusion: The results of this review suggest that rehabilitation exercise protocols held in a clinical and moderately intensive inpatient setting may provide the greatest functional and psychological outcomes for those with HD as evidenced by consistent patient benefit and high adherence rates. Furthermore, the high physical and time demands of high-intensity protocols may make them less practical than less intensive protocols, though more study is needed for confirmation. [ABSTRACT FROM AUTHOR]

Published

2019

4. Sample enrichment for clinical trials to show delay of onset in huntington disease.

Author

Paulsen, Jane S., Lourens, Spencer, Kieburtz, Karl, and Zhang, Ying

Subjects

*HUNTINGTON'S chorea treatment, *MOVEMENT disorder treatments, *COMPARATIVE studies, *EXPERIMENTAL design, *HUNTINGTON disease, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *MOVEMENT disorders, *RESEARCH, *RESEARCH funding, *EVALUATION research, *DISEASE progression, *STATISTICAL models, *IMPACT of Event Scale

Abstract

Background: Disease-modifying clinical trials in persons without symptoms are often limited in methods to assess the impact associated with experimental therapeutics. This study suggests sample enrichment approaches to facilitate preventive trials to delay disease onset in individuals with the dominant gene for Huntington disease.Methods: Using published onset prediction indexes, we conducted the receiver operating curve analysis for diagnosis within a 3-year clinical trial time frame. We determined optimal cut points on the indexes for participant recruitment and then conducted sample size and power calculations to detect varying effect sizes for treatment efficacy in reducing 3-year rates of disease onset (or diagnosis).Results: Area under the curve for 3 onset prediction indexes all demonstrated excellent value in sample enrichment methodology, with the best-performing index being the multivariate risk score (MRS).Conclusions: This study showed that conducting an intervention trial in premanifest and prodromal individuals with the gene expansion for Huntington disease is highly feasible using sample enrichment recruitment methods. Ongoing natural history studies are highly likely to indicate additional markers of disease prior to diagnosis. Statistical modeling of identified markers can facilitate participant enrichment to increase the likelihood of detecting a difference between treatment arms in a cost-effective and efficient manner. Such variations may expedite translation of emerging therapies to persons in an earlier phase of the disease.Trial Registration: PREDICT-HD is registered with www.clinicaltrials.gov, number NCT00051324. © 2019 International Parkinson and Movement Disorder Society. [ABSTRACT FROM AUTHOR]

Published

2019

5. Identification of Altered Developmental Pathways in Human Juvenile HD iPSC With 71Q and 109Q Using Transcriptome Profiling.

Author

Świtońska, Karolina, Szlachcic, Wojciech J., Handschuh, Luiza, Wojciechowski, Paweł, Marczak, Łukasz, Stelmaszczuk, Michał, Figlerowicz, Marek, and Figiel, Maciej

Subjects

HUNTINGTON'S chorea diagnosis, HUNTINGTON'S chorea treatment, TRANSCRIPTOMES, STEM cells, NUCLEOTIDE sequence, MESSENGER RNA

Abstract

In Huntington disease (HD) subtle symptoms in patients may occur years or even decades prior to diagnosis. HD changes at a molecular level may begin as early as in cells that are non-lineage committed such as stem cells or HD patients induced pluripotent stem cells (iPSCs) offering opportunity to enhance the understanding of the HD pathogenesis. In addition, juvenile HD non-linage committed cells were previously not directly investigated in detail by RNA-seq. In the present manuscript, we define the early HD and juvenile HD transcriptional alterations using 6 human HD iPS cell lines from two patients, one with 71 CAGs and one with 109 CAG repeats. We identified 107 (6 HD lines), 198 (3 HD71Q lines) and 217 (3 HD109Q lines) significantly dysregulated mRNAs in each comparison group. The analyses showed that many of dysregulated transcripts in HD109Q iPSC lines are involved in DNA damage response and apoptosis, such as CCND1, CDKN1A, TP53, BAX, TNFRSF10B, TNFRSF10C, TNFRSF10D, DDB2, PLCB1, PRKCQ, HSH2D, ZMAT3, PLK2, and RPS27L. Most of them were identified as downregulated and their proteins are direct interactors with TP53. HTT probably alters the level of several TP53 interactors influencing apoptosis. This may lead to accumulation of an excessive number of progenitor cells and potential disruption of cell differentiation and production of mature neurons. In addition, HTT effects on cell polarization also demonstrated in the analysis may result in a generation of incorrect progenitors. Bioinformatics analysis of transcripts dysregulated in HD71Q iPSC lines showed that several of them act as transcription regulators during the early multicellular stages of development, such as ZFP57, PIWIL2, HIST1H3C, and HIST1H2BB. Significant upregulation of most of these transcripts may lead to a global increase in expression level of genes involved in pathways critical for embryogenesis and early neural development. In addition, MS analysis revealed altered levels of TP53 and ZFP30 proteins reflecting the functional significance of dysregulated mRNA levels of these proteins which were associated with apoptosis and DNA binding. Our finding very well corresponds to the fact that mutation in the HTT gene may cause precocious neurogenesis and identifies pathways likely disrupted during development. [ABSTRACT FROM AUTHOR]

Published

2019

6. Efficient brain uptake and distribution of an expanded CAG RNA inhibitor DB213 via intranasal administration.

Author

Wang, Qianwen, Peng, Shaohong, Hu, Yue, Wong, Chun-Ho, Kwan, Kin Ming, Chan, H.Y. Edwin, and Zuo, Zhong

Subjects

*HUNTINGTON'S chorea treatment, *BIOPHARMACEUTICS, *NEUROTRANSMITTER uptake inhibitors, *POLYGLUTAMINE, *AMINO acid transport, *ANIMAL models in research, *INTRANASAL medication

Abstract

Abstract DB213 is an expanded CAG RNA inhibitor targeting polyglutamine diseases. This current study aims to investigate biopharmaceutic characteristics of DB213 as well as its brain uptake and distribution in C57 wild type mice, R6/2 Huntington's disease mice and Sprague-Dawley (SD) rats via intranasal administration. The biopharmaceutic characteristics of DB213 were investigated in vitro using Calu-3/MDCK/HEK293 cell lines and brain slices for its membrane transport, equilibrium dialysis for its plasma protein/brain tissue bindings and liver/brain microsomes incubation for its enzyme kinetics profiles. In vivo study of DB213 brain distribution was conducted in rats via intravenous and intranasal routes at 50 mg/kg followed by its brain uptake evaluation in mice at 25 mg/kg via intranasal route. In vitro membrane transport studies found that DB213 not only had a limited passive diffusion with a P app (a→b) value of 1.75 × 10−6 cm/s in Calu-3 cell monolayer model but also was substrate of MRP2, MRP3, and amino acid transporter. Furthermore, DB213 demonstrated higher binding towards brain homogenate (80%) than plasma (10%) with limited metabolism in liver and brain. After intranasal administration of DB213, both olfactory bulb and trigeminal nerve served as its entry points to reach brain as demonstrated in rats while efficient brain uptake was observed in mice. In summary, limited nasal epithelium permeability and MRP2/MRP3 mediated efflux transport of DB213 could be overcome by its influx transport via amino acid transporter and minimal liver and brain metabolism, which further contribute to its rapid brain uptake and distribution in mice and rats. Graphical abstract Unlabelled Image [ABSTRACT FROM AUTHOR]

Published

2019

7. Disease-Modification in Huntington's Disease: Moving Away from a Single-Target Approach.

Author

Jensen, Melanie P. and Barker, Roger A.

Subjects

*HUNTINGTON disease, *PATHOLOGY, *DRUG development, *COMBINATION drug therapy, *HUNTINGTON'S chorea treatment

Abstract

To date, no candidate intervention has demonstrated a disease-modifying effect in Huntington's disease, despite promising results in preclinical studies. In this commentary we discuss disease-modifying therapies that have been trialled in Huntington's disease and speculate that these failures may be attributed, in part, to the assumption that a single drug selectively targeting one aspect of disease pathology will be universally effective, regardless of disease stage or "subtype". We therefore propose an alternative approach for effective disease-modification that uses 1) a combination approach rather than monotherapy, and 2) targets the disease process early on – before it is clinically manifest. Finally, we will consider whether this change in approach that we propose will be relevant in the future given the recent shift to targeting more proximal disease processes—e.g., huntingtin gene expression; a timely question given Roche's recent decision to take on the clinical development of a promising new drug candidate in Huntington's disease, IONIS-HTTRx. [ABSTRACT FROM AUTHOR]

Published

2019

8. Inhibition of Drp1 hyperactivation reduces neuropathology and behavioral deficits in zQ175 knock-in mouse model of Huntington's disease.

Author

Zhao, Yuanyuan, Sun, Xiaoyan, and Qi, Xin

Subjects

*HUNTINGTON'S chorea treatment, *BEHAVIOR disorders, *DYNAMIN (Genetics), *NEUROLOGICAL disorders, *ANIMAL models in research

Abstract

Abstract Mitochondrial dysfunction manifests in the pathogenesis of Huntington's disease (HD), a fatal and inherited neurodegenerative disease. Dynamin-related protein 1 (Drp1) is the primary component of mitochondrial fission and becomes hyperactivated in various models of HD. We previously reported that inhibition of Drp1 hyperactivation by P110, a rationally designed peptide inhibitor of Drp1-Fis1 interaction, is protective in the HD R6/2 mouse model, which expresses a fragment of mutant Huntingtin (mHtt). In this study, we expand our work to test the effect of P110 treatment in HD knock-in (zQ175 KI) mice that express full-length mtHtt and exhibit progressive disease symptoms, reminiscent of human HD. We find that subcutaneously sustained treatment with P110 reduces movement deficits of mice. Moreover, the treatment attenuates striatal neuronal loss, microglial hyperactivity and white matter disorganization in zQ175 KI mice. These findings provide an additional line of evidence that inhibition of Drp1 hyperactivation is sufficient to reduce HD-associated neuropathology and behavioral deficits. We propose that manipulation of Drp1 hyperactivation might be a useful strategy to develop therapeutics for treating HD. Highlights • Inhibition of Drp1 hyperactivation reduces behavioral deficits in zQ175 knock-in mice. • Inhibition of Drp1 hyperactivation attenuates striatal cell death in HD mice. • Suppression of Drp1 hyperactivation reduces white matter disorganization in HD mice. [ABSTRACT FROM AUTHOR]

Published

2018

9. Neuroprotective effect of solanesol against 3-nitropropionic acid-induced Huntington's disease-like behavioral, biochemical, and cellular alterations: Restoration of coenzyme-Q10-mediated mitochondrial dysfunction.

Subjects

*NEUROPROTECTIVE agents, *HUNTINGTON'S chorea treatment, *UBIQUINONES, *MITOCHONDRIAL pathology, *DRUG side effects

Abstract

OBJECTIVE: The aim of the present study was to evaluate the solanesol (SNL)-mediated coenzyme-Q10 restoration to ameliorate 3-nitropropionic (3-NP)-induced behavioral, biochemical, and histological changes which resemble Huntington's disease (HD)-like symptoms in men. MATERIALS AND METHODS: Various behavioral and biochemical parameters were carried out to evaluate the activity of SNL on 3-NP-treated rats. To determine the therapeutic significance of SNL on HD, different behavioral tests such as memory task, locomotor activity, grip strength, and beam cross and some biochemical test along with histopathological findings were done. RESULTS: Chronic 3-NP, 10 mg/kg i.p., caused physical and mental abnormalities in animals, including memory impairment, weak grip strength, abnormal posture, and cognitive deficit. Biochemical analysis of brain homogenate in 3-NP-treated rats showed altered mitochondrial complexes, oxidative stress, and elevated lipid biomarkers. Neurohistological alterations of hippocampus, basal ganglia, and cerebral cortex of 3-NP-treated rats exhibit severe neuronal space, irregular damaged cells, and dense pyknotic nuclei-associated marked focal diffused gliosis. SNL administered for 15 days significantly improved motor performance and cognitive behavior task and restored the histopathological changes. Further, SNL treatment significantly improved mitochondrial complexes such as coenzyme-Q10 enzyme activity and attenuated inflammatory and oxidative damage of rat brain. CONCLUSION: In the present research work, SNL (5, 10, and 15 mg/kg p.o.) provided notable neuroprotective effect, which was confirmed by behavioral paradigms and biochemical test. It restored the behavioral and biochemical alteration caused by 3-NP and confirmed the strong neuroprotective mechanism of SNL in 3-NP-intoxicated memory and cognitive abnormalities. [ABSTRACT FROM AUTHOR]

Published

2018

10. Thymoquinone loaded solid lipid nanoparticles counteracts 3-Nitropropionic acid induced motor impairments and neuroinflammation in rat model of Huntington’s disease.

Author

Ramachandran, Surekha and Thangarajan, Sumathi

Subjects

*HUNTINGTON'S chorea treatment, *NANOMEDICINE, *3-Nitropropionic acid, *GENETIC transcription, *TYROSINE hydroxylase

Abstract

Defect in gene transcription, excitotoxicity, neuroinflammation and oxidative stress are the dominant disease process that causes striatal cell loss with motor abnormalities in Huntington’s disease (HD). Homogeneous pathological reminiscent of HD was extrapolated in the present study using a potent mitochondrial toxin, 3-Nitropropionic acid (3-NP). Administration of 3-NP for 14 days in the present study portends glial cell activation, N-methyl-D-aspartate (NMDA) receptor stimulation, neuroinflammation and motor deficits. The therapeutic strategy in the present study was improvised by formulating thymoquinone, a biologically active compound into a colloidal carrier namely solid lipid nanoparticles. Treatment with 10 and 20 mg/kg b.w of thymoquinone loaded solid lipid nanoparticles (TQ-SLNs) and 80 mg/kg b.w of thymoquinone suspension (TQ-S) showed a significant (P < 0.01) improvement in ATPases function in 3-NP induced animals than TQ-S (40 mg/kg b.w) treated group. TQ-SLNs (10 and 20 mg/kg) treatment also attenuated the overexpression of glial fibrillary acidic protein (GFAP), pro-inflammatory cytokines and p-p65 NFκB nuclear translocation in 3-NP exposed animals. Further, TQ-SLNs treatment desensitizes NR2B-subtype NMDA receptor, improves tyrosine hydroxylase (TH) immune reactive neurons and ameliorated the motor abnormalities in 3-NP intoxicated animals than TQ-S treated group. Hence, the study signifies that the treatment with lower doses of nanoformulated thymoquinone than thymoquinone suspension can efficiently culminate 3-NP induced HD progression in the striatum of male wistar rats. [ABSTRACT FROM AUTHOR]

Published

2018

11. Circadian-based Treatment Strategy Effective in the BACHD Mouse Model of Huntington’s Disease.

Author

Whittaker, Daniel S., Loh, Dawn H., Wang, Huei-Bin, Tahara, Yu, Kuljis, Dika, Cutler, Tamara, Ghiani, Cristina A., Shibata, Shigenobu, Block, Gene D., and Colwell, Christopher S.

Subjects

*HUNTINGTON'S chorea treatment, *CIRCADIAN rhythms, *COGNITIVE ability, *TREATMENT effectiveness, *MOTOR ability, *DISEASE progression

Abstract

Huntington’s disease (HD) patients suffer from progressive neurodegeneration that results in cognitive, psychiatric, cardiovascular, and motor dysfunction. Disturbances in sleep-wake cycles are common among HD patients with reports of delayed sleep onset, frequent bedtime awakenings, and excessive fatigue. The BACHD mouse model exhibits many HD core symptoms including circadian dysfunction. Because circadian dysfunction manifests early in the disease in both patients and mouse models, we sought to determine if early interventions that improve circadian rhythmicity could benefit HD symptoms and delay disease progression. We evaluated the effects of time-restricted feeding (TRF) on the BACHD mouse model. At 3 months of age, the animals were divided into 2 groups: ad lib and TRF. The TRF-treated BACHD mice were exposed to a 6-h feeding/18-h fasting regimen that was designed to be aligned with the middle (ZT 15-21) of the period when mice are normally active (ZT 12-24). Following 3 months of treatment (when mice reached the early disease stage), the TRF-treated BACHD mice showed improvements in their locomotor activity and sleep behavioral rhythms. Furthermore, we found improved heart rate variability, suggesting that their autonomic nervous system dysfunction was improved. On a molecular level, TRF altered the phase but not the amplitude of the PER2::LUC rhythms measured in vivo and in vitro. Importantly, treated BACHD mice exhibited improved motor performance compared with untreated BACHD controls, and the motor improvements were correlated with improved circadian output. It is worth emphasizing that HD is a genetically caused disease with no known cure. Lifestyle changes that not only improve the quality of life but also delay disease progression for HD patients are greatly needed. Our study demonstrates the therapeutic potential of circadian-based treatment strategies in a preclinical model of HD. [ABSTRACT FROM AUTHOR]

Published

2018

12. Neuroprotective activity of tetramethylpyrazine against 3-nitropropionic acid induced Huntington’s disease-like symptoms in rats.

Author

Danduga, Ravi Chandra Sekhara Reddy, Dondapati, Subba Reddy, Kola, Phani Kumar, Grace, Lilly, Tadigiri, Rahil Vandana Bisky, and Kanakaraju, Vijaya Kishore

Subjects

*HUNTINGTON'S chorea treatment, *PYRAZINE derivatives, *NEUROPROTECTIVE agents, *PROPIONIC acid derivatives, *NEUROCHEMISTRY, *LABORATORY rats

Abstract

Huntington’s disease (HD) is an autosomal neurodegenerative disease characterized by chorea, dystonia, motor ataxia, cognitive decline and psychiatric disorders with gradual loss of nerve cells and has no existing cure for the disease. In the present study, a mitochondrial toxin, 3-nitropropionic acid (3-NP) is used to induce HD like symptoms in rats. Tetramethylpyrazine is one of the active ingredients of Chuan Xiong which was reported to have neurotrophic and neuroprotective activities. The present study was designed to evaluate the role of TMP on 3-NP induced behavioral, biochemical, neurochemical, and histological alterations in the different regions of the brain. Animals were pretreated with normal saline/TMP for 7 days. From 8th day, the treatment groups were co-administered with 3-NP (10 mg/kg, i.p) and continued to the 21st day of the treatment protocol. At the end of the study, we found that the TMP improved all the behavioral performances of 3-NP induced neurotoxic rats, significantly. Further, oxidative stress parameters (lipid peroxidation, reduced glutathione, catalase, and superoxide dismutase), succinate dehydrogenase enzyme, and neurochemical (GABA and glutamate) estimations were done in the brain homogenate. In our study, the treatment with TMP ameliorated the 3-NP induced alterations, in the biochemical and neurochemical parameter in the brain homogenate, dose-dependently. The protective role of TMP further confirmed by measuring the lesion area with the 2,3,5-triphenyltetrazolium chloride staining of the brain slices and histopathological alteration in the hippocampus (CA1 and CA3) and striatal regions of the brain. Hence, the present findings suggest that the protective role of TMP against 3-NP induced behavioral, biochemical, neurochemical, and histological alterations in rats. [ABSTRACT FROM AUTHOR]

Published

2018

13. DARING TO HOPE.

Author

Wadman, Meredith

Subjects

*HUNTINGTON'S chorea treatment, *ANTISENSE drugs, *CEREBROSPINAL fluid, *INJECTIONS, *CLINICAL trials

Abstract

The article discusses the reactions of patients with Huntington disease to the development of an antisense drug that may be able to treat the disease. Topics include the role of the drug RG6042 in reducing the protein that causes Huntington disease, the injection of the drug into cerebrospinal fluid (CSF), and the work of the firm Ionis in a clinical trial of the drug.

Published

2018

14. Huntington's disease: Neuropsychiatric manifestations of Huntington's disease.

Author

Goh, Anita M. Y., Wibawa, Pierre, Loi, Samantha M., Walterfang, Mark, Velakoulis, Dennis, Looi, Jeffrey C. L., Goh, Anita My, and Looi, Jeffrey Cl

Subjects

*HUNTINGTON'S chorea treatment, *NEURODEGENERATION, *QUALITY of life, *NEUROPSYCHIATRY, *PSYCHIATRY

Abstract

Objectives: Huntington's disease (HD) is a profoundly incapacitating, and ultimately fatal, neurodegenerative disease. HD is presently incurable, so the current goal is to allow affected individuals to live as well as possible with the illness, to maximise functional independence and quality of life for the person with HD, their carers and family members. This clinical update review focuses on the common neuropsychiatric manifestations in HD, and outlines and evaluates the various neuropsychiatric facets of HD, including the aetiology, symptoms and diagnosis.Conclusions: Neuropsychiatric symptoms can precede the classic motor clinical symptoms of HD (prodromal HD) by decades, and cause significant functional impairment. HD provides key insights and understanding into the organic psychiatric disorders, including contemporary clinical insights into the process of neurodegeneration and manifestation of neuropsychiatric symptoms. [ABSTRACT FROM AUTHOR]

Published

2018

15. Huntington's disease: Managing neuropsychiatric symptoms in Huntington's disease.

Author

Loi, Samantha M., Walterfang, Mark, Velakoulis, Dennis, Looi, Jeffrey C. L., and Looi, Jeffrey Cl

Subjects

*HUNTINGTON'S chorea treatment, *NEUROPSYCHIATRY, *PHARMACOLOGY, *GENETIC disorders, *PSYCHIATRY

Abstract

Objectives: This clinical update review focuses on the management of the neuropsychiatric manifestations of Huntington's disease (HD). The review highlights current issues regarding pharmacological and non-pharmacological treatment, putative therapeutics and recent relevant research findings in this area.Conclusions: Neuropsychiatric symptoms may precede the classic motor clinical symptoms of HD (prodromal HD) by decades and cause significant functional impairment. Early recognition and comprehensive non-pharmacological, usually in combination with pharmacological, treatment is essential. [ABSTRACT FROM AUTHOR]

Published

2018

16. Huntington’s disease: the coming of age.

Author

Pandey, Mritunjay and Rajamma, Usha

Subjects

*HUNTINGTON'S chorea treatment, *AGE factors in disease, *POLYGLUTAMINE, *NEURONS, *MOLECULAR diagnosis

Abstract

Huntington’s disease (HD) is caused due to an abnormal expansion of polyglutamine repeats in the first exon of huntingtin gene. The mutation in huntingtin causes abnormalities in the functioning of protein, leading to deleterious effects ultimately to the demise of specific neuronal cells. The disease is inherited in an autosomal dominant manner and leads to a plethora of neuropsychiatric behaviour and neuronal cell death mainly in striatal and cortical regions of the brain, eventually leading to death of the individual. The discovery of the mutant gene led to a surge in molecular diagnostics of the disease and in making different transgenic models in different organisms to understand the function of wild-type and mutant proteins. Despite difficult challenges, there has been a significant increase in understanding the functioning of the protein in normal and other gain-of-function interactions in mutant form. However, there have been no significant improvements in treatments of the patients suffering from this ailment and most of the treatment is still symptomatic. HD warrants more attention towards better understanding and treatment as more advancement in molecular diagnostics and therapeutic interventions are available. Several different transgenic models are available in different organisms, ranging from fruit flies to primate monkeys, for studies on understanding the pathogenicity of the mutant gene. It is the right time to assess the advancement in the field and try new strategies for neuroprotection using key pathways as target. The present review highlights the key ingredients of pathology in the HD and discusses important studies for drug trials and future goals for therapeutic interventions. [ABSTRACT FROM AUTHOR]

Published

2018

17. Huntington’s Disease Clinical Trials Corner: August 2018.

Author

Rodrigues, Filipe B. and Wild, Edward J.

Subjects

*HUNTINGTON'S chorea treatment, *CLINICAL trials, *SEMAPHORINS, *CREATINE, *MEDICATION safety, *DRUG tolerance, *PHARMACOKINETICS

Abstract

In the third edition of the Huntington’s Disease Clinical Trials Corner we list all currently registered and ongoing clinical trials, expand on the SIGNAL trial (NCT02481674), and cover the recently finished CREST-E trial (NCT00712426). [ABSTRACT FROM AUTHOR]

Published

2018

18. Prospective evaluation of Globus pallidus internus deep brain stimulation in Huntington's disease.

Author

Zittel, S., Tadic, V., Moll, C.K.E., Bäumer, T., Fellbrich, A., Gulberti, A., Rasche, D., Brüggemann, N., Tronnier, V., and Münchau, A.

Subjects

*HUNTINGTON'S chorea treatment, *HUNTINGTON disease, *GLOBUS pallidus, *DEEP brain stimulation, *HYPOKINESIA, *DYSTONIA

Abstract

Introduction: Pharmacological treatment of chorea in Huntington's disease (HD) is often limited by poor efficacy or side effects. Pallidal deep brain stimulation (DBS) has been considered in these patients but experience is so far limited.Methods: We prospectively evaluated the effects of bilateral DBS of the Globus pallidus internus (GPi) over one year in six severely affected HD patients with treatment refractory chorea in an advanced stage of the disease. Primary endpoint of the study was improvement in chorea. Additionally, we evaluated the effects of GPi DBS on the motor part of the Unified Huntington's Disease Rating Scale (UHDRS), bradykinesia, dystonia, functional impairment, psychiatric and cognitive symptoms. Side effects were systematically assessed.Results: The chorea subscore was significantly reduced postoperatively (-47% six months, -40% twelve months postoperatively). The UHDRS total motor score was significantly reduced at six months postoperatively (- 17%) but the effect was not sustained twelve months after the operation (- 5%). Pallidal DBS did not improve other motor symptoms or functional impairment. There was no effect on psychiatric symptoms or cognition. A number of side effects were noted, especially spasticity in three of the patients.Conclusions: Pallidal DBS is a treatment option for HD patients with severe pharmacologically refractory chorea. Further studies are needed to define optimal candidates for this procedure. [ABSTRACT FROM AUTHOR]

Published

2018

19. Artificial miRNAs Reduce Human Mutant Huntingtin Throughout the Striatum in a Transgenic Sheep Model of Huntington's Disease.

Author

Pfister, Edith L., DiNardo, Natalie, Mondo, Erica, Borel, Florie, Conroy, Faith, Fraser, Cara, Gernoux, Gwladys, Han, Xin, Hu, Danjing, Johnson, Emily, Kennington, Lori, Liu, PengPeng, Reid, Suzanne J., Sapp, Ellen, Vodicka, Petr, Kuchel, Tim, Morton, A. Jennifer, Howland, David, Moser, Richard, and Sena-Esteves, Miguel

Subjects

*HUNTINGTON'S chorea treatment, *MICRORNA, *HUNTINGTIN protein, *NEURODEGENERATION, *SHEEP as laboratory animals

Abstract

Huntington's disease (HD) is a fatal neurodegenerative disease caused by a genetic expansion of the CAG repeat region in the huntingtin (HTT) gene. Studies in HD mouse models have shown that artificial miRNAs can reduce mutant HTT, but evidence for their effectiveness and safety in larger animals is lacking. HD transgenic sheep express the full-length human HTT with 73 CAG repeats. AAV9 was used to deliver unilaterally to HD sheep striatum an artificial miRNA targeting exon 48 of the human HTT mRNA under control of two alternative promoters: U6 or CβA. The treatment reduced human mutant (m) HTT mRNA and protein 50–80% in the striatum at 1 and 6 months post injection. Silencing was detectable in both the caudate and putamen. Levels of endogenous sheep HTT protein were not affected. There was no significant loss of neurons labeled by DARPP32 or NeuN at 6 months after treatment, and Iba1-positive microglia were detected at control levels. It is concluded that safe and effective silencing of human mHTT protein can be achieved and sustained in a large-animal brain by direct delivery of an AAV carrying an artificial miRNA. [ABSTRACT FROM AUTHOR]

Published

2018

20. Hybrid nanoparticles as a new technological approach to enhance the delivery of cholesterol into the brain.

Author

Belletti, Daniela, Grabrucker, Andreas Martin, Pederzoli, Francesca, Menrath, Isabel, Vandelli, Maria Angela, Tosi, Giovanni, Duskey, Thomas Jason, Forni, Flavio, and Ruozi, Barbara

Subjects

*HUNTINGTON'S chorea treatment, *CHOLESTEROL, *DRUG delivery systems, *LYSOSOMES, *NANOMEDICINE, *BLOOD-brain barrier, *THERAPEUTICS

Abstract

Restoration of the Chol homeostasis in the Central Nervous System (CNS) could be beneficial for the treatment of Huntington’s Disease (HD), a progressive, fatal, adult-onset, neurodegenerative disorder. Unfortunately, Chol is unable to cross the blood–brain barrier (BBB), thus a novel strategy for a targeted delivery of Chol into the brain is highly desired. This article aims to investigate the production of hybrid nanoparticles composed by Chol and PLGA (MIX-NPs) modified with g7 ligand for BBB crossing. We described the impact of ratio between components (Chol and PLGA) and formulation process (nanoprecipitation or single emulsion process) on physico-chemical and structural characteristics, we tested MIX-NPs in vitro using primary hippocampal cell cultures evaluating possible toxicity, uptake, and the ability to influence excitatory synaptic receptors. Our results elucidated that both formulation processes produce MIX-NPs with a Chol content higher that 40%, meaning that Chol is a structural particle component and active compound at the same time. The formulation strategy impacted the architecture and reorganization of components leading to some differences in Chol availability between the two types of g7 MIX-NPs. Our results identified that both kinds of MIX-NPs are efficiently taken up by neurons, able to escape lysosomes and release Chol into the cells resulting in an efficient modification in expression of synaptic receptors that could be beneficial in HD. [ABSTRACT FROM AUTHOR]

Published

2018

21. Brain mitochondrial iron accumulates in Huntington's disease, mediates mitochondrial dysfunction, and can be removed pharmacologically.

Author

Agrawal, Sonal, Fox, Julia, Thyagarajan, Baskaran, and Fox, Jonathan H.

Subjects

*MITOCHONDRIAL proteins, *HUNTINGTON'S chorea treatment, *BIOENERGETIC measurements, *NEURODEGENERATION, *IRON-sulfur proteins, *DIAGNOSIS

Abstract

Mitochondrial bioenergetic dysfunction is involved in neurodegeneration in Huntington's disease (HD). Iron is critical for normal mitochondrial bioenergetics but can also contribute to pathogenic oxidation. The accumulation of iron in the brain occurs in mouse models and in human HD. Yet the role of mitochondria-related iron dysregulation as a contributor to bioenergetic pathophysiology in HD is unclear. We demonstrate here that human HD and mouse model HD (12-week R6/2 and 12-month YAC128) brains accumulated mitochondrial iron and showed increased expression of iron uptake protein mitoferrin 2 and decreased iron-sulfur cluster synthesis protein frataxin. Mitochondria-enriched fractions from mouse HD brains had deficits in membrane potential and oxygen uptake and increased lipid peroxidation. In addition, the membrane-permeable iron-selective chelator deferiprone (1 μM) rescued these effects ex-vivo , whereas hydrophilic iron and copper chelators did not. A 10-day oral deferiprone treatment in 9-week R6/2 HD mice indicated that deferiprone removed mitochondrial iron, restored mitochondrial potentials, decreased lipid peroxidation, and improved motor endurance. Neonatal iron supplementation potentiates neurodegeneration in mouse models of HD by unknown mechanisms. We found that neonatal iron supplementation increased brain mitochondrial iron accumulation and potentiated markers of mitochondrial dysfunction in HD mice. Therefore, bi-directional manipulation of mitochondrial iron can potentiate and protect against markers of mouse HD. Our findings thus demonstrate the significance of iron as a mediator of mitochondrial dysfunction and injury in mouse models of human HD and suggest that targeting the iron-mitochondrial pathway may be protective. [ABSTRACT FROM AUTHOR]

Published

2018

22. Cysteine Metabolism in Neuronal Redox Homeostasis.

Author

Paul, Bindu D., Sbodio, Juan I., and Snyder, Solomon H.

Subjects

*CYSTEINE metabolism, *TREATMENT of neurodegeneration, *HUNTINGTON'S chorea diagnosis, *HUNTINGTON'S chorea treatment, *OXIDATIVE stress, *PHYSIOLOGICAL control systems

Abstract

Besides its essential role in protein synthesis, cysteine plays vital roles in redox homeostasis, being a component of the major antioxidant glutathione (GSH) and a potent antioxidant by itself. In addition, cysteine undergoes a variety of post-translational modifications that modulate several physiological processes. It is becoming increasingly clear that redox-modulated events play important roles not only in peripheral tissues but also in the brain where cysteine disposition is central to these pathways. Dysregulated cysteine metabolism is associated with several neurodegenerative disorders. Accordingly, restoration of cysteine balance has therapeutic benefits. This review discusses metabolic signaling pathways pertaining to cysteine disposition in the brain under normal and pathological conditions, highlighting recent findings on cysteine metabolism during aging and in neurodegenerative conditions such as Huntington’s disease (HD) and molybdenum cofactor (MoCo) deficiency (MoCD) among others. [ABSTRACT FROM AUTHOR]

Published

2018

23. The S1P Axis: New Exciting Route for Treating Huntington’s Disease.

Author

Di Pardo, Alba and Maglione, Vittorio

Subjects

*HUNTINGTON disease, *HUNTINGTON'S chorea treatment, *MOLECULAR pathology, *TARGETED drug delivery, *SPHINGOSINE-1-phosphate, *GENETICS

Abstract

Huntington’s disease (HD) is a single-gene inheritable neurodegenerative disorder with an associated complex molecular pathogenic profile that renders it the most ‘curable incurable’ brain disorder. Continuous effort in the field has contributed to the recent discovery of novel potential pathogenic mechanisms. Findings in preclinical models of the disease as well as in human post-mortem brains from affected patients demonstrate that alteration of the sphingosine-1-phosphate (S1P) axis may represent a possible key player in the pathogenesis of the disease and may act as a potential actionable drug target for the development of more targeted and effective therapeutic approaches. The relevance of the path of this new ‘therapeutic route’ is underscored by the fact that some drugs targeting the S1P axis are currently in clinical trials for the treatment of other brain disorders. [ABSTRACT FROM AUTHOR]

Published

2018

24. Pridopidine Reverses Phencyclidine-Induced Memory Impairment.

Author

Sahlholm, Kristoffer, Valle-León, Marta, Fernández-Dueñas, Víctor, and Ciruela, Francisco

Subjects

HUNTINGTON'S chorea treatment, PHENCYCLIDINE, CLINICAL trials

Abstract

Pridopidine is in clinical trials for Huntington's disease treatment. Originally developed as a dopamine D2 receptor (D2R) ligand, pridopidine displays about 100-fold higher affinity for the sigma-1 receptor (sigma-1R). Interestingly, pridopidine slows disease progression and improves motor function in Huntington's disease model mice and, in preliminarily reports, Huntington's disease patients. The present study examined the anti-amnesic potential of pridopidine. Thus, memory impairment was produced in mice by administration of phencyclidine (PCP, 10 mg/kg/day) for 10 days, followed by 14 days' treatment with pridopidine (6 mg/kg/day), or saline. Finally, novel object recognition performance was assessed in the animals. Mice receiving PCP and saline exhibited deficits in novel object recognition, as expected, while pridopidine treatment counteracted PCP-induced memory impairment. The effect of pridopidine was attenuated by co-administration of the sigma receptor antagonist, NE-100 (10 mg/kg). Our results suggest that pridopidine exerts anti-amnesic and potentially neuroprotective actions. These data provide new insights into the therapeutic potential of pridopidine as a pro-cognitive drug. [ABSTRACT FROM AUTHOR]

Published

2018

25. Dose-Dependent Lowering of Mutant Huntingtin Using Antisense Oligonucleotides in Huntington Disease Patients.

Author

van Roon-Mom, Willeke M.C., Roos, Raymund A.C., and de Bot, Susanne T.

Subjects

*HUNTINGTIN protein, *DNA mutational analysis, *HUNTINGTON'S chorea treatment, *GENE therapy, *OLIGONUCLEOTIDES

Abstract

On December 11 of 2017, Ionis Pharmaceuticals published a press release announcing dose-dependent reductions of mutant huntingtin protein in their HTTRx Phase 1/2a study in Huntington disease (HD) patients. The results from this Ionis trial have gained much attention from the patient community and the oligonucleotide therapeutics field, since it is the first trial targeting the cause of HD, namely the mutant huntingtin protein, using antisense oligonucleotides (ASOs). The press release also states that the primary endpoints of the study (safety and tolerability) were met, but does not contain data. This news follows the approval of another therapeutic ASO nusinersen (trade name Spinraza) for a neurological disease, spinal muscular atrophy, by the U.S. Food and Drug Administration and European Medicines Agency, in 2016 and 2017, respectively. Combined, this offers hope for the development of the HTTRx therapy for HD patients. [ABSTRACT FROM AUTHOR]

Published

2018

26. Physician perceptions of pharmacologic treatment options for chorea associated with Huntington disease in the United States.

Author

Sung, Victor W., Iyer, Ravi G., Gandhi, Sanjay K., Shah-Manek, Bijal, DiBonaventura, Marco, Abler, Victor, and Claassen, Daniel O.

Subjects

*HUNTINGTON'S chorea treatment, *DRUG efficacy, *DRUG tolerance

Abstract

Objective: To survey neurologists and obtain clinical perceptions of tetrabenazine for the treatment of chorea in patients with Huntington disease (HD).Methods: Board-certified/board-eligible neurologists, in practice for ≥5 years, who had treated treat ≥3 HD patients in the past 2 years, were recruited from an online physician panel to participate in a cross-sectional, web-based survey. Respondents provided information about themselves, their practice, approaches to HD chorea management and perceptions of available treatments.Results: Two hundred neurologists responded to the survey. Based on clinician responses, the most common reasons to treat chorea are impairment in activities of daily living (54%) and quality of life (41%). Although tetrabenazine was the only approved treatment for chorea in HD patients at the time of this analysis, it was only prescribed to ∼50% of patients with HD-related chorea. More than half of physicians perceive tetrabenazine as having minimal or no effectiveness in improving chorea. More than 40% of physicians consider tetrabenazine to be a non-optimal treatment, and 51% of physicians agree that they are unable to titrate to efficacious doses due to adverse side effects or tolerability concerns. Physicians report that side effects leading to dose interruptions (33%) and reductions (30%) occur in their patients "often" or "almost always". The most common side effects that led to insufficient dosing and disruptions in titration were sedation and somnolence (41%), depression (24%) and anxiety (22%).Conclusions: Many physicians who treat HD-related chorea report that tolerability issues with tetrabenazine impact their ability to effectively use tetrabenazine in their clinical practice. [ABSTRACT FROM AUTHOR]

Published

2018

27. Reactive Neuroblastosis in Huntington's Disease: A Putative Therapeutic Target for Striatal Regeneration in the Adult Brain.

Author

Kandasamy, Mahesh and Aigner, Ludwig

Subjects

HUNTINGTON disease, HUNTINGTON'S chorea treatment, DEVELOPMENTAL neurobiology, NEURODEGENERATION, GUIDED tissue regeneration, PATIENTS

Abstract

The cellular and molecular mechanisms underlying the reciprocal relationship between adult neurogenesis, cognitive and motor functions have been an important focus of investigation in the establishment of effective neural replacement therapies for neurodegenerative disorders. While neuronal loss, reactive gliosis and defects in the self-repair capacity have extensively been characterized in neurodegenerative disorders, the transient excess production of neuroblasts detected in the adult striatum of animal models of Huntington's disease (HD) and in post-mortem brain of HD patients, has only marginally been addressed. This abnormal cellular response in the striatum appears to originate from the selective proliferation and ectopic migration of neuroblasts derived from the subventricular zone (SVZ). Based on and in line with the term "reactive astrogliosis", we propose to name the observed cellular event "reactive neuroblastosis". Although, the functional relevance of reactive neuroblastosis is unknown, we speculate that this process may provide support for the tissue regeneration in compensating the structural and physiological functions of the striatum in lieu of aging or of the neurodegenerative process. Thus, in this review article, we comprehend different possibilities for the regulation of striatal neurogenesis, neuroblastosis and their functional relevance in the context of HD. [ABSTRACT FROM AUTHOR]

Published

2018

28. Epidemiology of Huntington disease in Cyprus: A 20‐year retrospective study.

Author

Demetriou, C. A., Heraclides, A., Salafori, C., Tanteles, G. A., Christodoulou, K., Christou, Y., and Zamba‐papanicolaou, E.

Subjects

*HUNTINGTON'S chorea treatment, *HUNTINGTON'S chorea diagnosis, *EPIDEMIOLOGY, *PRENATAL diagnosis, *NEURODEGENERATION, *PATIENTS

Abstract

Huntington disease (HD) is most prevalent among populations of western European descent and isolated populations where founder effects may operate. The aim of this study was to examine the epidemiology of HD in Cyprus, an island in southern Europe with extensive western European colonization in the past. All registered HD patients in the Cyprus, since 1994, were included. Detailed pedigrees and clinical information were recorded and maps, showing the geographic distribution of HD, were constructed. Requests for genetic testing were also examined. The project identified 58 clinically manifested cases of HD belonging to 19 families. The 16 families of Cypriot origin were concentrated in a confined geographical cluster in southeast Cyprus. In 2015, prevalence of symptomatic HD was 4.64/100 000 population, while incidence was 0.12/100 000 person‐years. Prevalence displayed a marked increase during the past 20 years. Disease characteristics of HD patients were similar to those reported in western European populations. Lastly, the uptake of predictive and/or prenatal testing was limited. HD disease characteristics, incidence and prevalence in Cyprus were comparable to western European populations. Together with the geographical clustering observed, these results support the possibility for a relatively recent founder effect of HD in Cyprus, potentially of western European origin. [ABSTRACT FROM AUTHOR]

Published

2018

29. Apathy Profile in Parkinson’s and Huntington’s Disease: A Comparative Cross-Sectional Study.

Author

Sousa, Mário, Moreira, Fradique, Jesus-Ribeiro, Joana, Marques, Inês, Cunha, Flávia, Canário, Nádia, Freire, António, and Januário, Cristina

Subjects

*PARKINSON'S disease treatment, *HUNTINGTON'S chorea treatment, *BRAIN diseases, *MOVEMENT disorders, *PREVENTION of mental depression

Abstract

Background/Aims: Apathy is one of the most frequent, disabling and difficult-to-treat symptoms that show up in many neurodegenerative disorders. The aim of this study was to assess and compare apathy profile in Parkinson’s and Huntington’s patients using the same comprehensive instruments to measure apathy, cognition and depressive symptoms. Materials and Methods: We consecutively assessed Parkinson’s disease (PD) and Huntington’s disease (HD) patients recruited from a Movement Disorders Unit. In all patients, information related to demographics, clinical data, motor score (Movement Disorders Society-Unified Parkinson Disease Rating Scale; Unified Huntington Disease Rating Scale), cognition (Montreal Cognitive Assessment scale), depressive symptoms (Beck Depression Inventory II) and apathy (Apathy Evaluation Scale – clinical version) was collected. Patients with dementia or major depression according to Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition, Text Revised criteria were excluded from the study. Results: Seventy-five patients were enrolled, 45 with PD and 30 with HD. Apathy was present in 42.5% of PD patients and 51.7% of HD patients. In PD patients, apathy was associated with motor score, shorter duration of disease, lower dose of levodopa equivalent daily dose and depressive symptomatology, whereas in HD patients, apathy was related to disease duration, motor score and cognitive impairment. Conclusions: We found a similar prevalence of apathy in PD and HD patients but with different clinical correlations and different apathy domains involved, and this may warrant the development of different therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2018

30. Progress in developing transgenic monkey model for Huntington’s disease.

Author

Snyder, Brooke R. and Chan, Anthony W. S.

Subjects

*TRANSGENIC animals, *LABORATORY monkeys, *HUNTINGTON'S chorea treatment, *MONKEY diseases, *ANIMAL models in research

Abstract

Huntington’s disease (HD) is a complex neurodegenerative disorder that has no cure. Although treatments can often be given to relieve symptoms, the neuropathology associated with HD cannot be stopped or reversed. HD is characterized by degeneration of the striatum and associated pathways that leads to impairment in motor and cognitive functions as well as psychiatric disturbances. Although cell and rodent models for HD exist, longitudinal study in a transgenic HD nonhuman primate (i.e., rhesus macaque; HD monkeys) shows high similarity in its progression with human patients. Progressive brain atrophy and changes in white matter integrity examined by magnetic resonance imaging are coherent with the decline in cognitive behaviors related to corticostriatal functions and neuropathology. HD monkeys also express higher anxiety and irritability/aggression similar to human HD patients that other model systems have not yet replicated. While a comparative model approach is critical for advancing our understanding of HD pathogenesis, HD monkeys could provide a unique platform for preclinical studies and long-term assessment of translatable outcome measures. This review summarizes the progress in the development of the transgenic HD monkey model and the opportunities for advancing HD preclinical research. [ABSTRACT FROM AUTHOR]

Published

2018

31. Efeitos da equoterapia sobre o equilíbrio estático e dinâmico no transtorno neurocognitivo maior ou leve devido à Doença de Huntington.

Author

Leme da Costa, João Vitor, Serrão Júnior, Nelson Francisco, Luvizutto, Gustavo José, Borges de Araujo, Thaís, Peralta Safons, Marisete, and Gonçalves de Rezende, Alexandre Luíz

Subjects

HUNTINGTON'S chorea treatment, HUNTINGTON'S chorea diagnosis, COGNITION disorders treatment, POSTURAL balance, EXERCISE therapy, ACCIDENTAL falls, TREATMENT effectiveness

Abstract

Copyright of Fisioterapia Brasil is the property of Atlantica Editora and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

32. Predictive testing and clinical trials in Huntington's disease: An ethical analysis.

Author

Sampaio, Cristina, Levey, Jamie, and Klitzman, Robert

Subjects

*HUNTINGTON'S chorea treatment, *HUNTINGTON'S chorea diagnosis, *CLINICAL trials, *COMPARATIVE studies, *DNA, *ETHICS, *HUNTINGTON disease, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *EVALUATION research

Published

2018

33. Exploring computerised cognitive training as a therapeutic intervention for people with Huntington's disease (CogTrainHD): protocol for a randomised feasibility study.

Author

Yhnell, Emma, Furby, Hannah, Breen, Rachel S., Brookes-Howell, Lucy C., Drew, Cheney J. G., Playle, Rebecca, Watson, Gareth, Metzler-Baddeley, Claudia, Rosser, Anne E., and Busse, Monica E.

Subjects

*HUNTINGTON'S chorea treatment, *COGNITIVE training, *MEDICAL protocols, *RANDOMIZED controlled trials, *EXECUTIVE function

Abstract

Background: Cognitive impairments, especially deficits of executive function, have been well documented as a core and early feature in Huntington's disease (HD). Cognitive impairments represent considerable burden and can be devastating for people and families affected by HD. Computerised cognitive training interventions that focus on improving executive function present a possible non-pharmacological treatment option. We propose to determine the feasibility, acceptability and appropriate outcome measures for use in a randomised controlled feasibility study. Methods/design: Participants will be randomised into either a computerised cognitive training group or a control group. Those randomised to the training group will be asked to complete a cognitive training intervention based on the HappyNeuron Pro software tasks of executive function, for a minimum of 30 min, three times a week for the 12-week study duration. Participants in the control group will not receive computerised cognitive training but will receive a similar degree of social interaction via equivalent study and home visits. We will explore quantitative outcome measures, including measures of cognitive performance, motor function, questionnaires and semi-structured interviews, as well as magnetic resonance imaging (MRI) measures in a subset of participants. Feasibility will be determined through assessment of recruitment, retention, adherence and acceptability of the intervention. Discussion: The results of this study will provide crucial guidance and information regarding the feasibility of conducting a randomised controlled study into computerised cognitive training in HD. This study is crucial for the development of larger definitive randomised controlled trials which are powered to determine efficacy and for the development of future cognitive training programmes for people affected by HD. [ABSTRACT FROM AUTHOR]

Published

2018

34. Utilization of Hospice Services in a Population of Patients With Huntington's Disease.

Author

Johnson, Margaret O., Frank, Samuel, Mendlik, Matthew, and Casarett, David

Subjects

*HUNTINGTON disease, *HUNTINGTON'S chorea treatment, *HOSPICE care, *ELECTRONIC health records, *LENGTH of stay in hospitals, *PATIENTS, *MEDICAL care, *MEDICAL records, *RETROSPECTIVE studies

Abstract

Context: Although the early and middle stages of Huntington's disease (HD) and its complications have been well described, less is known about the course of late-stage illness. In particular, little is known about the population of patients who enroll in hospice.Objectives: Our goal is to describe the characteristics of patients with HD who enrolled in hospice.Methods: This is a retrospective cohort study of electronic medical record data from 12 not-for-profit hospices in the United States from 2008 to 2012.Results: Of the 164,032 patients admitted to these hospices, 101 (0.06%) had a primary diagnosis of HD. Their median age was 57 (IQR 48-65) and 53 (52.5%) were women. Most patients were cared for by a spouse (n = 36, 36.6%) or adult child (n = 20, 19.8%). At the time of admission, most patients were living either at home (n = 39, 38.6%) or in a nursing home (n = 41, 40.6%). All were either bedbound or could ambulate only with assistance. The most common symptom reported during enrollment in hospice was pain (n = 34, 33.7%) followed by anxiety (n = 30, 29.7%), nausea (n = 18, 17.8%), and dyspnea (n = 10, 9.9%). Patients had a median length of stay in hospice of 42 days, which was significantly longer than that of other hospice patients in the sample (17 days), P < 0.001. Of the 101 patients who were admitted to hospice, 73 died, 11 were still enrolled at the time of data analysis, and 17 left hospice either because they no longer met eligibility criteria (n = 14, 13.7%) or because they decided to seek treatment for other medical conditions (n = 3, 3.0%). Of the 73 patients who died while on hospice, most died either in a nursing home (n = 29; 40%) or a hospital (n = 27; 37%). Seventeen patients (23%) died at home. No patient that started in a facility died at home.Conclusion: Patients with HD are admitted to hospice at a younger age compared with other patients (57 vs. 76 years old) but have a significant symptom burden and limited functional status. Although hospice care emphasizes the importance of helping patients to remain in their homes, only a minority of these patients were able to die at home. [ABSTRACT FROM AUTHOR]

Published

2018

35. Localization of neuroglobin in the brain of R6/2 mouse model of Huntington's disease.

Author

Cardinale, A., Fusco, F. R., Paldino, E., Giampà, C., Marino, M., Nuzzo, M. T., D’Angelo, V., Laurenti, D., Straccia, G., Fasano, D., Sarnataro, D., Squillaro, T., Paladino, S., Melone, Mariarosa A. B., and D'Angelo, V

Subjects

*HUNTINGTON'S chorea treatment, *GLOBIN gene expression, *NEUROPROTECTIVE agents, *OXIDATIVE stress, *FLUORESCENCE resonance energy transfer

Abstract

Neuroglobin (Ngb) is expressed in the central and peripheral nervous system, cerebrospinal fluid, retina, and endocrine tissues where it is involved in binding O2 and other gasotransmitters. Several studies have highlighted its endogenous neuroprotective function. Huntington's disease (HD), a dominant hereditary disease, is characterized by the gradual loss of neurons in discrete areas of the central nervous system. We analyzed the expression of Ngb in the brain tissue of a mouse model of HD, in order to define the role of Ngb with respect to individual cell type vulnerability in HD and to gender and age of mice. Our results showed different expressions of Ngb among neurons of a specific region and between different brain regions. We evidenced a decreased intensity of Ngb at 13 weeks of age, compared to 7 weeks of age. The double immunofluorescence and fluorescence resonance energy transfer (FRET) experiments showed that the co-localization between Ngb and huntingtin at the subcellular level was not close enough to account for a direct interaction. We also observed a different expression of Ngb in the striatum, depending on the sex and age of animals. These findings provide the first experimental evidence for an adaptive response of Ngb in HD, suggesting that Ngb may exert neuroprotective effects in HD beyond its role in reducing sensitivity to oxidative stress. [ABSTRACT FROM AUTHOR]

Published

2018

36. Complete suppression of Htt fibrilization and disaggregation of Htt fibrils by a trimeric chaperone complex.

Author

Scior, Annika, Buntru, Alexander, Arnsburg, Kristin, Ast, Anne, Iburg, Manuel, Juenemann, Katrin, Pigazzini, Maria Lucia, Mlody, Barbara, Puchkov, Dmytro, Priller, Josef, Wanker, Erich E., Prigione, Alessandro, and Kirstein, Janine

Subjects

*MOLECULAR chaperones, *HUNTINGTON'S chorea treatment, *NEURODEGENERATION, *CAENORHABDITIS elegans, *NUCLEATION, *THERAPEUTICS

Abstract

Abstract: Huntington's disease (HD) is a neurodegenerative disorder caused by an expanded CAG trinucleotide repeat in the huntingtin gene (HTT). Molecular chaperones have been implicated in suppressing or delaying the aggregation of mutant Htt. Using in vitro and in vivo assays, we have identified a trimeric chaperone complex (Hsc70, Hsp110, and J‐protein) that completely suppresses fibrilization of HttExon1Q48. The composition of this chaperone complex is variable as recruitment of different chaperone family members forms distinct functional complexes. The trimeric chaperone complex is also able to resolubilize Htt fibrils. We confirmed the biological significance of these findings in HD patient‐derived neural cells and on an organismal level in Caenorhabditis elegans. Among the proteins in this chaperone complex, the J‐protein is the concentration‐limiting factor. The single overexpression of DNAJB1 in HEK293T cells is sufficient to profoundly reduce HttExon1Q97 aggregation and represents a target of future therapeutic avenues for HD. [ABSTRACT FROM AUTHOR]

Published

2018

37. Stem cell transplantation for Huntington’s diseases.

Author

Choi, Kyung-Ah, Choi, Yeonho, and Hong, Sunghoi

Subjects

*HUNTINGTON'S chorea treatment, *NEURODEGENERATION, *STEM cell transplantation, *TREATMENT effectiveness, *SOMATIC cells

Abstract

Therapeutic approaches based on stem cells have received considerable attention as potential treatments for Huntington’s disease (HD), which is a fatal, inherited neurodegenerative disorder, caused by progressive loss of GABAergic medium spiny neurons (MSNs) in the striatum of the forebrain. Transplantation of stem cells or their derivatives in animal models of HD, efficiently improved functions by replacing the damaged or lost neurons. In particular, neural stem cells (NSCs) for HD treatments have been developed from various sources, such as the brain itself, the pluripotent stem cells (PSCs), and the somatic cells of the HD patients. However, the brain-derived NSCs are difficult to obtain, and the PSCs have to be differentiated into a population of the desired neuronal cells that may cause a risk of tumor formation after transplantation. In contrast, induced NSCs, derived from somatic cells as a new stem cell source for transplantation, are less likely to form tumors. Given that the stem cell transplantation strategy for treatment of HD, as a genetic disease, is to replace the dysfunctional or lost neurons, the correction of mutant genes containing the expanded CAG repeats is essential. In this review, we will describe the methods for obtaining the optimal NSCs for transplantation-based HD treatment and the differentiation conditions for the functional GABAergic MSNs as therapeutic cells. Also, we will discuss the valuable gene correction of the disease stem cells by the CRISPR/Cas9 system for HD treatment. [ABSTRACT FROM AUTHOR]

Published

2018

38. Pridopidine: Overview of Pharmacology and Rationale for its Use in Huntington's Disease.

Author

Waters, Susanna, Tedroff, Joakim, Ponten, Henrik, Klamer, Daniel, Sonesson, Clas, and Waters, Nicholas

Subjects

*HUNTINGTON'S chorea treatment, *DOPAMINE receptors, *MOTOR ability, *PHARMACOLOGY, *PATHOLOGICAL physiology

Abstract

Despite advances in understanding the pathophysiology of Huntington's disease (HD), there are currently no effective pharmacological agents available to treat core symptoms or to stop or prevent the progression of this hereditary neurodegenerative disorder. Pridopidine, a novel small molecule compound, has demonstrated potential for both symptomatic treatment and disease modifying effects in HD. While pridopidine failed to achieve its primary efficacy outcomes (Modified motor score) in two trials (MermaiHD and HART) there were consistent effects on secondary outcomes (TMS). In the most recent study (PrideHD) pridiopidine did not differ from placebo on TMS, possibly due to a large enduring placebo effect. This review describes the process, based on in vivo systems response profiling, by which pridopidine was discovered and discusses its pharmacological profile, aiming to provide a model for the system-level effects and a rationale for the use of pridopidine in patients affected by HD. Considering the effects on brain neurochemistry, gene expression and behaviour in vivo, pridopidine displays a unique effect profile. A hallmark feature in the behavioural pharmacology of pridopidine is its state-dependent inhibition or activation of dopamine-dependent psychomotor functions. Such effects are paralleled by strengthening of synaptic connectivity in cortico-striatal pathways suggesting pridopidine has potential to modify phenotypic expression as well as progression of HD. The preclinical pharmacological profile is discussed with respect to the clinical results for pridopidine and proposals are made for further investigation, including preclinical and clinical studies addressing disease progression and effects at different stages of HD. [ABSTRACT FROM AUTHOR]

Published

2018

39. TAKING CARE OF PEOPLE SUFFERING FROM HUNTINGTON'S DISEASE: THE IMPACT ON INFORMAL CAREGIVERS' QUALITY OF LIFE.

Author

Martins, Rosa, Carvalho, Nélia, Andrade, Ana Isabel, Martins, Conceição, and Dinis, Alexandra

Subjects

*HUNTINGTON'S chorea diagnosis, *HUNTINGTON'S chorea treatment, *QUALITY of life, *CAREGIVERS, *NEURODEGENERATION

Abstract

Background: Huntington's disease (HD) is an inherited neurodegenerative disease which affects the movement and leads to the progressive cognitive deficits and behavioral capacities. Care for a Huntington patient is a complex process with a major impact on health, well-being and quality of life of Informal Caregivers (IC). Objectives: To evaluate the impact of HD in the Quality of Life (QoL) Informal Caregiver, and to verify if the socio-demographic, contextual and clinical variables relate to that QoL. Methods: This is a quantitative study, descriptive and correlational with 50 IC members of the "Asociación de Corea de Huntington Española ". We used the Spanish version of the questionnaire: Huntington's Disease Quality of Life Battery for Carers (HDQoL-C) as the data collection instrument. Results: The participants are mostly female, averaging 50.04 years of age, married with a high level of literacy and active. The IC have a moderate QoL in which the caregiver role has great impact. However "the life satisfaction" and "feelings about life with HD" which appear to alleviate this burden. Data showed that the educational level and the number of hours of daily care influenced the QoL. Conclusions: The results reinforce the multidimensionality and variability of QoL of the Huntington's patients IC and highlight the need for health professionals to take a chance on intervention programs in the community, in order to capacitate the IC to provide care and promote their QoL. [ABSTRACT FROM AUTHOR]

Published

2018

40. Buccal Respiratory Chain Complexes I and IV Quantities in Huntington's Disease Patients.

Author

DUŠEK, P., RODINOVÁ, M., LIŠKOVÁ, I., KLEMPÍŘ, J., ZEMAN, J., ROTH, J., and HANSÍKOVÁ, H.

Subjects

HUNTINGTON'S chorea treatment, HUNTINGTON disease, MITOCHONDRIA, ORAL drug administration, IMMUNOASSAY, PATIENTS

Abstract

Alterations in mitochondrial parameters are an important hallmark of Huntington's disease (HD). The ubiquitous expression of mutant huntingtin raises the prospect that mitochondrial disturbances can also be detected and monitored through buccal epithelial cells. In a group of 34 patients with Huntington's disease and a group of 22 age-related healthy volunteers, respiratory complex I and IV protein quantities in buccal epithelial cells were measured using the dipstick immunocapture assay. The protein quantity of respiratory complex I correlates with age (r = 0.427, P = 0.026, FWE-P = 0.156) in the patient group, but not in the group of healthy subjects. Our non-invasive approach allows us to obtain valuable information for the studies of mitochondrial biochemical parameters in patients with neurodegenerative diseases and could also be useful in epidemiological studies. [ABSTRACT FROM AUTHOR]

Published

2018

41. Transplantation of Neuronal Precursors Derived from Induced Pluripotent Stem Cells into the Striatum of Rats with the Toxin-induced Model of Huntington's Disease.

Author

Stavrovskaya, A. V., Yamshchikova, N. G., Ol'shanskiy, A. S., Konovalova, E. V., and Illarioshkin, S. N.

Subjects

*HUNTINGTON'S chorea treatment, *INDUCED pluripotent stem cells, *CELLULAR therapy, *LOCOMOTION, *NEUROTOXIC agents

Abstract

Introduction. Huntington's disease (HD) is a severe neurodegenerative disorder characterized by choreic hyperkinesis, cognitive decline, behavioral disorders, and progressive neuronal death, mostly in the striatum. Since HD is a fatal disorder, searching for efficient treatment methods, including those based on cell replacement therapy, is quite relevant. The experimental models of HD are used increasingly often. The objective of the study was to assess effectiveness and safety of transplantation of neuronal precursors differentiated from induced pluripotent stem cells (iPSCs) from a healthy donor into the striatum of rats with 3-NPAinduced HD model. Materials and methods. We studied the influence of neurotransplantation on the behavioral effects in rats with HD model induced by intrastriatal injection of 3-nitropropiotic acid (3-NPA). In the study group of animals (n = 11), human neuronal precursors derived from iPSCs of a healthy volunteer were transplanted into the caudate nuclei (5 × 105 per 5 µL of normal saline solution bilaterally); the control group of animals (n = 10) received normal saline solution. The animals were tested using the ANY-maze video tracking system; the parameters of the open-field test and the conditioned avoidance response test were evaluated. Results. An analysis of behavioral effects after transplantation demonstrated that introduction of neuronal iPSC derivatives into the caudate nuclei of rats with induced HD model was accompanied by recovery of locomotor activity of the animals (horizontal and vertical), as opposed to the control group. It was found when testing the reproducibility of the conditioned avoidance responses that the conditioned avoidance responses in control animals were weakened, whereas intrastriatal transplantation of neurons abruptly increased the latency of moving into the dark compartment of the chamber in the conditioned avoidance response test. Conclusions. The pilot experiment using the HD model showed that neurotransplantation using iPSC derivatives recovers the reduced locomotor activity in rats and improves memory trace keeping, which contributes to correction of locomotor and cognitive disorders induced by 3-NPA neurotoxin. [ABSTRACT FROM AUTHOR]

Published

2017

42. An open-label study to assess the feasibility and tolerability of rilmenidine for the treatment of Huntington's disease.

Author

Underwood, Benjamin, Green-Thompson, Zeyn, Pugh, Peter, Lazic, Stanley, Mason, Sarah, Griffin, Jules, Jones, P., Rowe, James, Rubinsztein, David, and Barker, Roger

Subjects

*NEURODEGENERATION, *HUNTINGTON'S chorea treatment, *MENTAL depression, *THERAPEUTICS, *MAGNETIC resonance imaging, *VENOUS puncture, *PATIENTS

Abstract

Preclinical data have shown that rilmenidine can regulate autophagy in models of Huntington's disease (HD), providing a potential route to alter the disease course in patients. Consequently, a 2-year open-label study examining the tolerability and feasibility of rilmenidine in mild-moderate HD was undertaken. 18 non-demented patients with mild to moderate HD took daily doses of 1 mg Rilmenidine for 6 months and 2 mg for a further 18 months followed by a 3-month washout period. The primary outcome was the number of withdrawals and serious adverse events. Secondary outcomes included safety parameters and changes in disease-specific variables, such as motor, cognitive and functional performance, structural MRI and serum metabolomic analysis. 12 patients completed the study; reasons for withdrawal included problems tolerating study procedures (MRI, and venepuncture), depression requiring hospital admission and logistical reasons. Three serious adverse events were recorded, including hospitalisation for depression, but none were thought to be drug-related. Changes in secondary outcomes were analysed as the annual rate of change in the study group. The overall change was comparable to changes seen in recent large observational studies in HD patients, though direct statistical comparisons to these studies were not made. Chronic oral administration of rilmenidine is feasible and well-tolerated and future, larger, placebo-controlled, studies in HD are warranted. Trial registration: EudraCT number 2009-018119-14. [ABSTRACT FROM AUTHOR]

Published

2017

43. Tetrahydrocannabinolic acid is a potent PPARγ agonist with neuroprotective activity.

Author

Nadal, Xavier, Río, Carmen, Casano, Salvatore, Palomares, Belén, Ferreiro‐Vera, Carlos, Navarrete, Carmen, Sánchez‐Carnerero, Carolina, Cantarero, Irene, Bellido, Maria Luz, Meyer, Stefan, Morello, Gaetano, Appendino, Giovanni, Muñoz, Eduardo, Del Río, Carmen, Palomares, Belén, Ferreiro-Vera, Carlos, Sánchez-Carnerero, Carolina, and Muñoz, Eduardo

Subjects

*CANNABINOIDS, *PEROXISOME proliferator-activated receptors, *MITOCHONDRIA, *HUNTINGTIN protein, *CANCER cells, *HUNTINGTON'S chorea treatment, *TREATMENT of neurodegeneration

Abstract

Background and Purpose: Phytocannabinoids are produced in Cannabis sativa L. in acidic form and are decarboxylated upon heating, processing and storage. While the biological effects of decarboxylated cannabinoids such as Δ9 -tetrahydrocannabinol have been extensively investigated, the bioactivity of Δ9 -tetahydrocannabinol acid (Δ9 -THCA) is largely unknown, despite its occurrence in different Cannabis preparations. Here we have assessed possible neuroprotective actions of Δ9 -THCA through modulation of PPARγ pathways.Experimental Approach: The effects of six phytocannabinoids on PPARγ binding and transcriptional activity were investigated. The effect of Δ9 -THCA on mitochondrial biogenesis and PPARγ coactivator 1-α expression was investigated in Neuro-2a (N2a) cells. The neuroprotective effect was analysed in STHdhQ111/Q111 cells expressing a mutated form of the huntingtin protein and in N2a cells infected with an adenovirus carrying human huntingtin containing 94 polyQ repeats (mHtt-q94). The in vivo neuroprotective activity of Δ9 -THCA was investigated in mice intoxicated with the mitochondrial toxin 3-nitropropionic acid (3-NPA).Key Results: Cannabinoid acids bind and activate PPARγ with higher potency than their decarboxylated products. Δ9 -THCA increased mitochondrial mass in neuroblastoma N2a cells and prevented cytotoxicity induced by serum deprivation in STHdhQ111/Q111 cells and by mutHtt-q94 in N2a cells. Δ9 -THCA, through a PPARγ-dependent pathway, was neuroprotective in mice treated with 3-NPA, improving motor deficits and preventing striatal degeneration. In addition, Δ9 -THCA attenuated microgliosis, astrogliosis and up-regulation of proinflammatory markers induced by 3-NPA.Conclusions and Implications: Δ9 -THCA shows potent neuroprotective activity, which is worth considering for the treatment of Huntington's disease and possibly other neurodegenerative and neuroinflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2017

44. Ameliorating effect of Celastrus paniculatus standardized extract and its fractions on 3-nitropropionic acid induced neuronal damage in rats: possible antioxidant mechanism.

Author

Malik, Jai, Karan, Maninder, and Dogra, Rachna

Subjects

*CELASTRUS, *HUNTINGTON'S chorea treatment, *ANTIOXIDANTS, *LINOLEIC acid, *ETHERS, *ETHYL acetate, *BUTANOL

Abstract

Context:Celastrus paniculatusWild. (Celasteraceae) (CP) is a well-known Ayurvedic ‘Medhya Rasayana’ (nervine tonic), used extensively as a neuro-protective and memory enhancer, and in different central nervous system disorders. Objective:To evaluate the effect of CP against 3-nitropropionic acid (3-NP) induced Huntington's disease (HD) like symptoms in Wistar male rats. Materials and methods:The ethanol extract of CP seeds (CPEE), prepared by maceration, was standardized on the basis of linoleic acid content (6.42%) using thin layer chromatography densitometric analysis. Protective effect of CPEE (100 and 200 mg/kg) and its various fractions, viz., petroleum ether (40 mg/kg), ethyl acetate (2.5 mg/kg),n-butanol (7 mg/kg) and aqueous (18 mg/kg), administered orally for 20 days, against 3-NP (10 mg/kg, i.p. for 14 days) was assessed by their effect on body weight, locomotor activity, grip strength, gait pattern and cognitive dysfunction and biochemical parameters for oxidative damage in the striatum and cortex regions of the brain. Results:CPEE (100 and 200 mg/kg) treated animals exhibited a significant (p < 0.05) improvement in behavioural and oxidative stress parameters in comparison to only 3-NP treated animals. Amongst various tested fractions of CPEE, aqueous fraction (AF) at 18 mg/kg exhibited maximum reversal of 3-NP induced behavioural and biochemical alterations, and was therefore also tested at 9 and 36 mg/kg. CPEE (100 mg/kg) and AF (36 mg/kg) exhibited maximum and significant (p < 0.05) attenuation of 3-NP induced alterations in comparison to 3-NP treated rats. Conclusions:CPEE has a protective action against 3-NP induced HD like symptoms due to its strong antioxidant effect. [ABSTRACT FROM PUBLISHER]

Published

2017

45. RNAi mechanisms in Huntington's disease therapy: siRNA versus shRNA.

Author

Aguiar, Sebastian, van der Gaag, Bram, and Cortese, Francesco Albert Bosco

Subjects

*HUNTINGTON'S chorea treatment, *RNA interference, *ANTISENSE RNA

Abstract

Huntington's Disease (HD) is a genetically dominant trinucleotide repeat disorder resulting from CAG repeats within the Huntingtin (HTT) gene exceeding a normal range (> 36 CAGs). Symptoms of the disease manifest in middle age and include chorea, dystonia, and cognitive decline. Typical latency from diagnosis to death is 20 years. There are currently no disease-modifying therapies available to HD patients. RNAi is a potentially curative therapy for HD. A popular line of research employs siRNA or antisense oligonucleotides (ASO) to knock down mutant Huntingtin mRNA (mHTT). Unfortunately, this modality requires repeated dosing, commonly exhibit off target effects (OTEs), and exert renal and hepatic toxicity. In contrast, a single AAV-mediated short-hairpin RNA (shRNA) dose can last years with low toxicity. In addition, we highlight research indicating that shRNA elicits fewer OTEs than siRNA when tested head-to-head. Despite this promise, shRNA therapy has been held back by difficulties controlling expression (oversaturating cells with toxic levels of RNA construct). In this review, we compare RNAi modalities for HD and propose novel methods of optimizing shRNA expression and on-target fidelity. [ABSTRACT FROM AUTHOR]

Published

2017

46. Induced Pluripotent Stem Cell-Derived Neural Stem Cell Transplantations Reduced Behavioral Deficits and Ameliorated Neuropathological Changes in YAC128 Mouse Model of Huntington's Disease.

Author

Al-Gharaibeh, Abeer, Culver, Rebecca, Stewart, Andrew N., Srinageshwar, Bhairavi, Spelde, Kristin, Frollo, Laura, Kolli, Nivya, Story, Darren, Paladugu, Leela, Anwar, Sarah, Crane, Andrew, Wyse, Robert, Maiti, Panchanan, Dunbar, Gary L., and Rossignol, Julien

Subjects

HUNTINGTON'S chorea treatment, TREATMENT of neurodegeneration, STEM cell transplantation

Abstract

Huntington's disease (HD) is a genetic neurodegenerative disorder characterized by neuronal loss and motor dysfunction. Although there is no effective treatment, stem cell transplantation offers a promising therapeutic strategy, but the safety and efficacy of this approach needs to be optimized. The purpose of this study was to test the potential of intra-striatal transplantation of induced pluripotent stem cell-derived neural stem cells (iPS-NSCs) for treating HD. For this purpose, we developed mouse adenovirus-generated iPSCs, differentiated them into neural stem cells in vitro, labeled them with Hoechst, and transplanted them bilaterally into striata of 10-month old wild type (WT) and HD YAC128 mice. We assessed the efficiency of these transplanted iPS-NSCs to reduce motor deficits in YAC128 mice by testing them on an accelerating rotarod task at 1 day prior to transplantation, and then weekly for 10 weeks. Our results showed an amelioration of locomotor deficits in YAC128 mice that received iPS-NSC transplantations. Following testing, the mice were sacrificed, and their brains were analyzed using immunohistochemistry and Western blot (WB). The results from our histological examinations revealed no signs of tumors and evidence that many iPS-NSCs survived and differentiated into region-specific neurons (medium spiny neurons) in both WT and HD mice, as confirmed by co-labeling of Hoechst-labeled transplanted cells with NeuN and DARPP-32. Also, counts of Hoechst-labeled cells revealed that a higher proportion were co-labeled with DARPP-32 and NeuN in HD-, compared to WT- mice, suggesting a dissimilar differentiation pattern in HD mice. Whereas significant decreases were found in counts of NeuN- and DARPP-32-labeled cells, and for neuronal density measures in striata of HD vehicle controls, such decrements were not observed in the iPS-NSCs-transplanted-HDmice. WB analysis showed increase of BDNF and TrkB levels in striata of transplanted HD mice compared to HD vehicle controls. Collectively, our data suggest that iPS-NSCs may provide an effective option for neuronal replacement therapy in HD. [ABSTRACT FROM AUTHOR]

Published

2017

47. Remodeling of heterochromatin structure slows neuropathological progression and prolongs survival in an animal model of Huntington's disease.

Author

Lee, Junghee, Hwang, Yu, Kim, Yunha, Lee, Min, Hyeon, Seung, Lee, Soojin, Kim, Dong, Jang, Sung, Im, Hyoenjoo, Min, Sun-Joon, Choo, Hyunah, Pae, Ae, Cho, Kyung, Kowall, Neil, and Ryu, Hoon

Subjects

*HUNTINGTON'S chorea treatment, *NEUROLOGICAL disorders, *HETEROCHROMATIN, *DISEASE risk factors

Abstract

Huntington's disease (HD) is an autosomal-dominant inherited neurological disorder caused by expanded CAG repeats in exon 1 of the Huntingtin ( HTT) gene. Altered histone modifications and epigenetic mechanisms are closely associated with HD suggesting that transcriptional repression may play a pathogenic role. Epigenetic compounds have significant therapeutic effects in cellular and animal models of HD, but they have not been successful in clinical trials. Herein, we report that dSETDB1/ESET, a histone methyltransferase (HMT), is a mediator of mutant HTT-induced degeneration in a fly HD model. We found that nogalamycin, an anthracycline antibiotic and a chromatin remodeling drug, reduces trimethylated histone H3K9 (H3K9me3) levels and pericentromeric heterochromatin condensation by reducing the expression of Setdb1/Eset. H3K9me3-specific ChIP-on-ChIP analysis identified that the H3K9me3-enriched epigenome signatures of multiple neuronal pathways including Egr1, Fos, Ezh1, and Arc are deregulated in HD transgenic (R6/2) mice. Nogalamycin modulated the expression of the H3K9me3-landscaped epigenome in medium spiny neurons and reduced mutant HTT nuclear inclusion formation. Moreover, nogalamycin slowed neuropathological progression, preserved motor function, and extended the life span of R6/2 mice. Together, our results indicate that modulation of SETDB1/ESET and H3K9me3-dependent heterochromatin plasticity is responsible for the neuroprotective effects of nogalamycin in HD and that small compounds targeting dysfunctional histone modification and epigenetic modification by SETDB1/ESET may be a rational therapeutic strategy in HD. [ABSTRACT FROM AUTHOR]

Published

2017

48. Design optimization for clinical trials in early-stage manifest Huntington's disease.

Author

Frost, Chris, Mulick, Amy, Scahill, Rachael I., Owen, Gail, Aylward, Elizabeth, Leavitt, Blair R., Durr, Alexandra, Roos, Raymund A. C., Borowsky, Beth, Stout, Julie C., Reilmann, Ralf, Langbehn, Douglas R., Tabrizi, Sarah J., Sampaio, Cristina, and TRACK-HD Investigators

Subjects

*HUNTINGTON'S chorea treatment, *BASAL ganglia, *CLINICAL trials, *COMPARATIVE studies, *EXPERIMENTAL design, *HUNTINGTON disease, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *HEALTH outcome assessment, *RESEARCH, *EVALUATION research, *ATROPHY, *STATISTICAL models

Abstract

Objectives: The purpose of this study was to inform the design of randomized clinical trials in early-stage manifest Huntington's disease through analysis of longitudinal data from TRACK-Huntington's Disease (TRACK-HD), a multicenter observational study.Methods: We compute sample sizes required for trials with candidate clinical, functional, and imaging outcomes, whose aims are to reduce rates of change. The calculations use a 2-stage approach: first using linear mixed models to estimate mean rates of change and components of variability from TRACK-HD data and second using these to predict sample sizes for a range of trial designs.Results: For each outcome, the primary drivers of the required sample size were the anticipated treatment effect and the duration of treatment. Extending durations from 1 to 2 years yielded large sample size reductions. Including interim visits and incorporating stratified randomization on predictors of outcome together with covariate adjustment gave more modest, but nontrivial, benefits. Caudate atrophy, expressed as a percentage of its baseline, was the outcome that gave smallest required sample sizes.Discussion: Here we consider potential required sample sizes for clinical trials estimated from naturalistic observation of longitudinal change. Choice among outcome measures for a trial must additionally consider their relevance to patients and the expected effect of the treatment under study. For all outcomes considered, our results provide compelling arguments for 2-year trials, and we also demonstrate the benefits of incorporating stratified randomization coupled with covariate adjustment, particularly for trials with caudate atrophy as the primary outcome. The benefits of enrichment are more debatable, with statistical benefits offset by potential recruitment difficulties and reduced generalizability. © 2017 International Parkinson and Movement Disorder Society. [ABSTRACT FROM AUTHOR]

Published

2017

49. Huntington disease care: From the past to the present, to the future.

Author

Mestre, T.A. and Shannon, K.

Subjects

*HUNTINGTON'S chorea treatment, *HUNTINGTON disease, *HEALTH care teams, *PALLIATIVE treatment, *DONEPEZIL, *CLOZAPINE, *AMANTADINE, *PATIENTS, *THERAPEUTICS

Abstract

Introduction: Huntington disease is a progressive neurodegenerative disorder without a cure. Its clinical presentation makes complex the care of patients with HD, further impacted by the progressive loss of dependence and disability. Intuitively, HD management calls for multispecialty care.Methods: Literature review and expert-based statement.Results: Chorea is the only indication for symptomatic treatments in HD. Surgical therapies are experimental, and exercise-based physical interventions have been assessed but in small feasibility studies. In HD, multispecialty care requires the active involvement of physicians, therapists, social workers and nutritionists. In about half of the HD clinics, a multidisciplinary case review is offered. It is still unknown what is the care delivery model that is best for HD. Palliative care is an important concept in HD care focusing in quality of life, considering physical, psychosocial, and spiritual problems. Palliative care may delay nursing home placement in advanced HD.Conclusion: There is a support for multispecialty care in HD, but more evidence needs to be generated through clinical research. The implementation of technology in the multispecialty care of patients with HD has a significant potential for reducing the care burden for families and the healthcare team, and to secure a wider care delivery. [ABSTRACT FROM AUTHOR]

Published

2017

50. Modulation of nuclear REST by alternative splicing: a potential therapeutic target for Huntington's disease.

Author

Chen, Guo‐Lin, Ma, Qi, Goswami, Dharmendra, Shang, Jianyu, and Miller, Gregory M.

Subjects

HUNTINGTON disease, HUNTINGTON'S chorea treatment, IMMUNOMODULATORS, CYTOSOL, GENE silencing, GENETICS

Abstract

Huntington's disease ( HD) is caused by a genetically mutated huntingtin ( mHtt) protein with expanded polyQ stretch, which impairs cytosolic sequestration of the repressor element-1 silencing transcription factor ( REST), resulting in excessive nuclear REST and subsequent repression of neuronal genes. We recently demonstrated that REST undergoes extensive, context-dependent alternative splicing, of which exon-3 skipping (∆E3)-a common event in human and nonhuman primates-causes loss of a motif critical for REST nuclear targeting. This study aimed to determine whether ∆E3 can be targeted to reduce nuclear REST and rescue neuronal gene expression in mouse striatal-derived, mHtt-expressing STHdhQ111/Q111 cells-a well-established cellular model of HD. We designed two morpholino antisense oligos ( ASOs) targeting the splice sites of Rest E3 and examined their effects on ∆E3, nuclear Rest accumulation and Rest-controlled gene expression in STHdhQ111/Q111 cells. We found that (1) the ASOs treatment significantly induced ∆E3, reduced nuclear Rest, and rescued transcription and/or mis-splicing of specific neuronal genes ( e.g. Syn1 and Stmn2) in STHdhQ111/Q111 cells; and (2) the ASOs-induced transcriptional regulation was dependent on ∆E3 induction and mimicked by si RNA-mediated knock-down of Rest expression. Our findings demonstrate modulation of nuclear REST by ∆E3 and its potential as a new therapeutic target for HD and provide new insights into environmental regulation of genome function and pathogenesis of HD. As ∆E3 is modulated by cellular signalling and linked to various types of cancer, we anticipate that ∆E3 contributes to environmentally tuned REST function and may have a broad range of clinical implications. [ABSTRACT FROM AUTHOR]

Published

2017