Neuroprotection for Huntington’s Disease: Ready, Set, Slow

Hersch, Steven M.; Rosas, H. Diana

doi:10.1016/j.nurt.2008.01.003

Cited by 42 publications

(31 citation statements)

References 135 publications

(84 reference statements)

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“…toxic mRNA in HD etiology has also been suggested [7]. HD inheritance is autosomal dominant and consequently the prevailing view is that mHtt mediated symptoms result from a toxic gain-offunction mechanism although loss-of-function mechanisms for mHtt and Htt are also proposed [8,9]. Htt is conserved among vertebrates [10], is localized mainly in cytoplasm and exhibits anti-apopptotic properties [11,12].…”

Section: Huntington's Diseasementioning

confidence: 99%

“…Presently available data indicate at the following mechanisms of mHtt toxicity: protein aggregation, excitotoxicity, oxidative stress, impairment of proteolysis and proteasome, enhanced apoptosis and autophagy, transcription regulation, including epigenetic mechanisms and mitochondria dysfunction [6,8,9,[18][19][20]. Although the functional relationship of Htt to mitochondria is still uncertain [21], it is becoming increasingly apparent that mHtt can impair mitochondrial function directly [22].…”

Section: Huntington's Diseasementioning

confidence: 99%

“…Its domain model does not indicate any particular functions aside from domains that might mediate protein interactions. Indeed, numerous reports indicate that Htt interacts with above 200 proteins which represent a diverse array of biological functions, including synaptic transmission, cytoskeletal organization, signal transduction, gene expression regulation and metabolism [8,[15][16][17].Presently available data indicate at the following mechanisms of mHtt toxicity: protein aggregation, excitotoxicity, oxidative stress, impairment of proteolysis and proteasome, enhanced apoptosis and autophagy, transcription regulation, including epigenetic mechanisms and mitochondria dysfunction [6,8,9,[18][19][20]. Although the functional relationship of Htt to mitochondria is still uncertain [21], it is becoming increasingly apparent that mHtt can impair mitochondrial function directly [22].…”

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confidence: 99%

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VDAC as a Potential Target in Huntingtons Disease Therapy: The State of the Art

Karachitos¹,

Grobys²

2015

Pharmaceut Reg Affairs

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It is becoming increasingly evident that mitochondria dysfunction plays an important role in pathogenesis of Huntington's disease (HD). However, the underlying mechanism is still needs to be explained. The crucial aspect of the explanation is to indicate the upstream events in mitochondria dysfunction that could contribute to HD. In the review we propose the defect of voltage-dependent anion-selective channel (VDAC), as a causative event in HDrelated mitochondria dysfunction. Thus, we propose to consider VDAC as a crucial element in HD etiology and consequently as a reasonable target for therapeutic interventions in HD, based on developing novel therapeutic strategies eliminating mitochondria dysfunction.Keywords: Huntington's disease; VDAC; Mitochondria; Therapy Huntington's DiseaseHuntington's disease (HD) is a progressive and fatal neurodegenerative disease with a prevalence of about 5-10/100 000. Clinically, the disease is characterized by progressive chorea (involuntary dance-like movements), rigidity, weight loss, dementia, seizures and psychiatric disturbances such as depression, withdrawal and irritability. These symptoms including cognitive deterioration, psychiatric disturbances, and movement disorders result from a selective and continuous loss of neurons from the striatum and deep layers of the cerebral cortex although other brain regions such as thalamus and subthalamic nucleus are also affected [1][2][3]. Current treatments for HD relieve merely the symptoms and address the control of behavioral symptoms, motor sedatives, cognitive enhancers, and neuroprotective agents [4,5] but are not able to restore neuronal function nor to stop the insidious loss of neurons. As summarized by Kumar et al. [6], although there is an intensive research concerning development of neuroprotective strategies such as fetal neural transplantation, RNA interference (RNAi) and transglutaminase inhibitors (TGaseI), effective therapeutic strategies may not be developed until the next few decades. Thus, a new therapeutic approach involving new potential targets and to start before the symptomatic stage could contribute to HD treatment to be more specific and effective. This, in turn, requires further studies concerning molecular mechanisms underlying HD.The genetic hallmark of HD is an expansion of an unstable trinucleotide CAG repeat region within the first exon of the gene encoding the protein Huntington (Htt). This results in synthesis of its mutant form (mHtt) containing more than 36 glutamine residues at N terminus although the possible contribution of mHtt encoding mRNA, i.e. toxic mRNA in HD etiology has also been suggested [7]. HD inheritance is autosomal dominant and consequently the prevailing view is that mHtt mediated symptoms result from a toxic gain-offunction mechanism although loss-of-function mechanisms for mHtt and Htt are also proposed [8,9]. Htt is conserved among vertebrates [10], is localized mainly in cytoplasm and exhibits anti-apopptotic properties [11,12]. Importantly, Htt expression in diffe...

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Section: Huntington's Diseasementioning

confidence: 99%

Section: Huntington's Diseasementioning

confidence: 99%

mentioning

confidence: 99%

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VDAC as a Potential Target in Huntingtons Disease Therapy: The State of the Art

Karachitos¹,

Grobys²

2015

Pharmaceut Reg Affairs

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“…For patients with these diseases it is imperative to develop in-vivo measures (biomarkers) that can track early disease-induced neural changes, especially before overt symptoms arise. Such biomarkers could provide metrics to evaluate neural change over time as well as the outcome of neuroprotective trials (reviewed by Bohanna et al, 2008;Hersch and Rosas, 2008).…”

Section: Introductionmentioning

confidence: 99%

Evaluating imaging biomarkers for neurodegeneration in pre-symptomatic Huntington's disease using machine learning techniques

et al. 2011

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“…1 mtHtt misfolds, undergoes posttranslational modifications, fragments, and forms soluble oligomers and insoluble intracellular aggregates, [2][3][4] which are differentially toxic. 5,6 Huntingtin (Htt) is the most salient target for neuroprotective therapies [7][8][9] and it is both essential and challenging to reliably measure it 1,2,10 to enable the development of therapies. We adapted a semiquantitative cell-based immunoassay that measures soluble mtHtt and total Htt (tHtt) using homogeneous time-resolved fluorescence (HTRF) Förster resonance energy transfer.…”

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confidence: 99%

HTRF analysis of soluble huntingtin in PHAROS PBMCs

et al. 2013

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Objective: We measured the levels of mutant huntingtin (mtHtt) and total huntingtin (tHtt) in blood leukocytes from Prospective Huntington At-Risk Observational Study (PHAROS) subjects at 50% risk of carrying the Huntington disease mutation using a homogeneous time-resolved fluorescence (HTRF) assay to assess its potential as a biomarker.Methods: Peripheral blood mononuclear cells from consenting PHAROS subjects were analyzed by HTRF using antibodies that simultaneously measured mtHtt and tHtt. mtHtt levels were normalized to tHtt, double-stranded DNA, or protein and analyzed according to cytosine-adenineguanine repeat length (CAGn), demographics, predicted time to clinical onset or known time since clinical onset, and available clinical measures.Results: From 363 assayed samples, 342 met quality control standards. Levels of mtHtt and mt/tHtt were higher in 114 subjects with expanded CAG repeats (CAG $37) compared with 228 subjects with nonexpanded CAG repeats (CAG ,37) (p , 0.0001). Analysis of relationships to predicted time to onset or to phenoconversion suggested that the HTRF signal could mark changes during the Huntington disease prodrome or after clinical onset. Conclusions:The HTRF assay can effectively measure mtHtt in multicenter sample sets and may be useful in trials of therapies targeting huntingtin. Huntington disease (HD) is caused by the expression of the toxic mutant huntingtin (mtHtt) protein, which contains an expanded polyglutamine repeat sequence near its N-terminus.1 mtHtt misfolds, undergoes posttranslational modifications, fragments, and forms soluble oligomers and insoluble intracellular aggregates, 2-4 which are differentially toxic. 5,6 Huntingtin (Htt) is the most salient target for neuroprotective therapies 7-9 and it is both essential and challenging to reliably measure it 1,2,10 to enable the development of therapies. We adapted a semiquantitative cell-based immunoassay that measures soluble mtHtt and total Htt (tHtt) using homogeneous time-resolved fluorescence (HTRF) Förster resonance energy transfer. 11,12 This HTRF assay is sensitive, reliable, and specific for soluble mtHtt in tissues and blood from HD mouse models, 11 in postmortem tissue, and in single-site studies using human peripheral blood mononuclear cells (PBMCs) from subjects with premanifest and manifest HD. [11][12][13] We optimized and technically validated the HTRF assay according to Good Laboratory Practice (GLP) standards for analyzing mtHtt and tHtt in clinical PBMC samples.12 To validate the HTRF assay in the context of a blinded multicenter study encompassing subjects with and without the HD mutation, to assess normalization methods for Htt values, and to examine whether the HD prodrome or the development of clinical

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Neuroprotection for Huntington’s Disease: Ready, Set, Slow

Cited by 42 publications

References 135 publications

VDAC as a Potential Target in Huntingtons Disease Therapy: The State of the Art

VDAC as a Potential Target in Huntingtons Disease Therapy: The State of the Art

Evaluating imaging biomarkers for neurodegeneration in pre-symptomatic Huntington's disease using machine learning techniques

HTRF analysis of soluble huntingtin in PHAROS PBMCs

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