Your search keyword '"mHtt"' showing total 38 results

1. Mutant huntingtin protein induces MLH1 degradation, DNA hyperexcision, and cGAS-STING-dependent apoptosis.

Author

Sun, Xiao, Liu, Lu, Wu, Chao, Li, Xueying, Guo, Jinzhen, Zhang, Junqiu, Guan, Junhong, Wang, Nan, Gu, Liya, Yang, X, and Li, Guo-Min

Subjects

Exo1, Huntington’s disease, MutLα, cGAS-STING, mHTT, Humans, Huntingtin Protein, Mutant Proteins, Huntington Disease, Nucleotidyltransferases, DNA, Apoptosis, MutL Protein Homolog 1

Abstract

Huntingtons disease (HD) is an inherited neurodegenerative disorder caused by an expanded CAG repeat in the huntingtin (HTT) gene. The repeat-expanded HTT encodes a mutated HTT (mHTT), which is known to induce DNA double-strand breaks (DSBs), activation of the cGAS-STING pathway, and apoptosis in HD. However, the mechanism by which mHTT triggers these events is unknown. Here, we show that HTT interacts with both exonuclease 1 (Exo1) and MutLα (MLH1-PMS2), a negative regulator of Exo1. While the HTT-Exo1 interaction suppresses the Exo1-catalyzed DNA end resection during DSB repair, the HTT-MutLα interaction functions to stabilize MLH1. However, mHTT displays a significantly reduced interaction with Exo1 or MutLα, thereby losing the ability to regulate Exo1. Thus, cells expressing mHTT exhibit rapid MLH1 degradation and hyperactive DNA excision, which causes severe DNA damage and cytosolic DNA accumulation. This activates the cGAS-STING pathway to mediate apoptosis. Therefore, we have identified unique functions for both HTT and mHTT in modulating DNA repair and the cGAS-STING pathway-mediated apoptosis by interacting with MLH1. Our work elucidates the mechanism by which mHTT causes HD.

Published

2024

2. Towards Standardizing Nomenclature in Huntingtons Disease Research.

Author

DiFiglia, Marian, Leavitt, Blair, Macdonald, Douglas, and Thompson, Leslie

Subjects

HTT, Huntington disease, Nomenclature, mHTT, neuroanatomy, neuropathology, preclinical models, Huntington Disease, Terminology as Topic, Humans, Biomedical Research

Abstract

The field of Huntingtons disease research covers many different scientific disciplines, from molecular biology all the way through to clinical practice, and as our understanding of the disease has progressed over the decades, a great deal of different terminology has accrued. The field is also renowned for its collaborative spirit and use of standardized reagents, assays, datasets, models, and clinical measures, so the use of standardized terms is especially important. We have set out to determine, through a consensus exercise involving basic and clinical scientists working in the field, the most appropriate language to use across disciplines. Nominally, this article will serve as the style guide for the Journal of Huntingtons Disease (JHD), the only journal devoted exclusively to HD, and we lay out the preferred and standardized terminology and nomenclature for use in JHD publications. However, we hope that this article will also serve as a useful resource to the HD research community at large and that these recommended naming conventions will be adopted widely.

Published

2024

3. An exploration of the genetics of the mutant Huntingtin (mHtt) gene in a cohort of patients with chorea from different ethnic groups in sub‐Saharan Africa.

Author

Muthinja, Mendi J, Guelngar, Carlos Othon, Fall, Maouly, Jama, Fatumah, Shuja, Huda Aldeen, Nambafu, Jamila, Massi, Daniel Gams, Ojo, Oluwadamilola O., Okubadejo, Njideka U., Taiwo, Funmilola Tolulope, Diop, Alassane Mamadou, Chacus, Coudjou J. D. G., Cissé, Fodé Abass, Cissé, Amara, Hooker, Juzar, Sokhi, Dilraj, Houlden, Henry, and Rizig, Mie

Abstract

Background Objective Methods Results Conclusion Africans are underrepresented in Huntington's disease (HD) research. A European ancestor was postulated to have introduced the mutant Huntingtin (mHtt) gene to the continent; however, recent work has shown the existence of a unique Htt haplotype in South‐Africa specific to indigenous Africans.We aimed to investigate the CAG trinucleotide repeats expansion in the Htt gene in a geographically diverse cohort of patients with chorea and unaffected controls from sub‐Saharan Africa.We evaluated 99 participants: 43 patients with chorea, 21 asymptomatic first‐degree relatives of subjects with chorea, and 35 healthy controls for the presence of the mHtt. Participants were recruited from 5 African countries. Additional data were collected from patients positive for the mHtt gene; these included demographics, the presence of psychiatric and (or) cognitive symptoms, family history, spoken languages, and ethnic origin. Additionally, their pedigrees were examined to estimate the number of people at risk of developing HD and to trace back the earliest account of the disease in each region.HD cases were identified in all countries. Overall, 53.4% of patients with chorea were carriers for the mHTT; median tract size was 45 CAG repeats. Of the asymptomatic relatives, 28.6% (6/21) were carriers for the mHTT; median tract size was 40 CAG. No homozygous carries were identified. Median CAG tract size in controls was 17 CAG repeats. Men and women were equally affected by HD. All patients with HD—bar three who were juvenile onset of <21 years—were defined as adult onset (median age of onset was 40 years). HD transmission followed an autosomal dominant pattern in 84.2% (16/19) of HD families. In familial cases, maternal transmission was higher 52.6% (10/19) than paternal transmission 36.8% (7/19). The number of asymptomatic individuals at risk of developing HD was estimated at ten times more than the symptomatic patients. HD could be traced back to the early 1900s in most African sites. HD cases spread over seven ethnic groups belonging to two distinct linguistic lineages separated from each other approximately 54–16 kya ago: Nilo‐Sahara and Niger‐Congo.This is the first study examining HD in multiple sites in sub‐Saharan Africa. We demonstrated that HD is found in multiple ethnic groups residing in five sub‐Saharan African countries including the first genetically confirmed HD cases from Guinea and Kenya. The prevalence of HD in the African continent, its associated socio‐economic impact, and genetic origins need further exploration and reappraisal. [ABSTRACT FROM AUTHOR]

Published

2024

4. Role of TFEB in Huntington's Disease.

Author

Ojalvo-Pacheco, Javier, Yakhine-Diop, Sokhna M. S., Fuentes, José M., Paredes-Barquero, Marta, and Niso-Santano, Mireia

Subjects

*HUNTINGTON disease, *AXONAL transport, *TRINUCLEOTIDE repeats, *HUNTINGTIN protein, *GENE expression, *RECESSIVE genes

Abstract

Simple Summary: Huntington's disease is an inherited neurodegenerative disease caused by a mutation in the gene encoding the huntingtin protein, which leads to its accumulation and neuronal death. There are several therapeutic strategies aimed at reducing the levels of mutant huntingtin, one of which is to activate cellular degradation systems such as autophagy. The transcription factor TFEB is the key regulator of gene expression in the autophagy–lysosomal pathway. In this review, we describe how the modulation of TFEB expression in HD models affect the levels of mutant huntingtin. Further studies are needed to assess whether targeting TFEB or stimulating autophagy could be a suitable therapeutic strategy to reduce the HD phenotype. Huntington's disease (HD) is an autosomal dominant neurodegenerative disease caused by an expansion of the CAG trinucleotide repeat in exon 1 of the huntingtin (HTT) gene. This expansion leads to a polyglutamine (polyQ) tract at the N-terminal end of HTT, which reduces the solubility of the protein and promotes its accumulation. Inefficient clearance of mutant HTT (mHTT) by the proteasome or autophagy–lysosomal system leads to accumulation of oligomers and toxic protein aggregates in neurons, resulting in impaired proteolytic systems, transcriptional dysregulation, impaired axonal transport, mitochondrial dysfunction and cellular energy imbalance. Growing evidence suggests that the accumulation of mHTT aggregates and autophagic and/or lysosomal dysfunction are the major pathogenic mechanisms underlying HD. In this context, enhancing autophagy may be an effective therapeutic strategy to remove protein aggregates and improve cell function. Transcription factor EB (TFEB), a master transcriptional regulator of autophagy, controls the expression of genes critical for autophagosome formation, lysosomal biogenesis, lysosomal function and autophagic flux. Consequently, the induction of TFEB activity to promote intracellular clearance may be a therapeutic strategy for HD. However, while some studies have shown that overexpression of TFEB facilitates the clearance of mHTT aggregates and ameliorates the disease phenotype, others indicate such overexpression may lead to mHTT co-aggregation and worsen disease progression. Further studies are necessary to confirm whether TFEB modulation could be an effective therapeutic strategy against mHTT-mediated toxicity in different disease models. [ABSTRACT FROM AUTHOR]

Published

2024

5. Mutant huntingtin protein induces MLH1 degradation, DNA hyperexcision, and cGAS-STING-dependent apoptosis.

Author

Xiao Sun, Lu Liu, Chao Wu, Xueying Li, Jinzhen Guo, Junqiu Zhang, Junhong Guan, Nan Wang, Liya Gu, Yang, X. Willian, and Guo-Min Li

Subjects

*HUNTINGTIN protein, *MUTANT proteins, *HUNTINGTON disease, *DOUBLE-strand DNA breaks, *APOPTOSIS

Abstract

Huntington's disease (HD) is an inherited neurodegenerative disorder caused by an expanded CAG repeat in the huntingtin (HTT) gene. The repeat-expanded HTT encodes a mutated HTT (mHTT), which is known to induce DNA double-strand breaks (DSBs), activation of the cGAS--STING pathway, and apoptosis in HD. However, the mechanism by which mHTT triggers these events is unknown. Here, we show that HTT interacts with both exonuclease 1 (Exol) and MutLα (MLH1-PMS2), a negative regulator of Exol. While the HTT-Exol interaction suppresses the Exol-catalyzed DNA end resection during DSB repair, the HTT-MutLα interaction functions to stabilize MLH1. However, mHTT displays a significantly reduced interaction with Exol or MutLα, thereby losing the ability to regulate Exol. Thus, cells expressing mHTT exhibit rapid MLHl degradation and hyperactive DNA excision, which causes severe DNA damage and cytosolic DNA accumulation. This activates the cGAS--STING pathway to mediate apoptosis. Therefore, we have identified unique functions for both HTT and mHTT in modulating DNA repair and the cGAS--STING pathway-mediated apoptosis by inter-acting with MLHl. Our work elucidates the mechanism by which mHTT causes HD. [ABSTRACT FROM AUTHOR]

Published

2024

6. Targeting the autophagy-lysosomal pathway in Huntington disease: a pharmacological perspective.

Author

Junsheng Yang and Chaoyue Zhang

Subjects

PROTEIN metabolism, NERVE tissue proteins, AUTOPHAGY, CELLULAR signal transduction, HUNTINGTON disease

Abstract

The autophagy-lysosomal pathway (ALP) is the major biological pathway responsible for clearing intracellular protein aggregates, therefore a promising target for treating diseases featuring the accumulation of aggregation-prone proteins, such as Huntington disease (HD). However, accumulating evidence indicated that targeting ALP to treat HD is pharmacologically challenging due to the complexity of autophagy and the autophagy defects in HD cells. Here in this mini-review, we summarized the current challenges in targeting ALP in HD and discussed a number of latest findings on aggrephagy and targeted protein degradation, which we believe will provide potential new targets and new strategies for treating HD via ALP. [ABSTRACT FROM AUTHOR]

Published

2023

7. Discovery of an autophagy inducer J3 to lower mutant huntingtin and alleviate Huntington’s disease-related phenotype

Author

Jiahui Long, Xia Luo, Dongmei Fang, Haikun Song, Weibin Fang, Hao Shan, Peiqing Liu, Boxun Lu, Xiao-Ming Yin, Liang Hong, and Min Li

Subjects

Autophagy, HdhQ140, Huntington’s disease, J3, mHTT, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Abstract Huntington’s disease (HD) is a neurodegenerative disorder caused by aggregation of the mutant huntingtin (mHTT) protein encoded from extra tracts of CAG repeats in exon 1 of the HTT gene. mHTT proteins are neurotoxic to render the death of neurons and a series of disease-associated phenotypes. The mHTT is degraded through autophagy pathway and ubiquitin–proteasome system (UPS). This study identified a small molecule, J3, as an autophagy inducer by high-content screening. The results revealed that J3 could inhibit mTOR, thus promoting autophagic flux and long-lived protein degradation. Further, J3 selectively lowered the soluble and insoluble mHTT but not wild type HTT levels in cell models. The HdhQ140 mice showed reduced HD-associated activity and loss of motor functions. However, administration of J3 showed increased activity and a slight improvement in the motor function in the open-field test, balance beam test, and rotarod tests. Furthermore, in vivo studies revealed that J3 decreased T-HTT and misfolded protein levels in the striatum and increased the levels of the medium spiny neuron marker DARPP-32. In addition, J3 showed good permeability across the brain-blood barrier efficiently, suggesting that J3 was a promising candidate for the treatment of HD.

Published

2022

8. Peripheral Biomarkers in Manifest and Premanifest Huntington's Disease.

Author

Morena, Emanuele, Romano, Carmela, Marconi, Martina, Diamant, Selene, Buscarinu, Maria Chiara, Bellucci, Gianmarco, Romano, Silvia, Scarabino, Daniela, Salvetti, Marco, and Ristori, Giovanni

Subjects

*HUNTINGTON disease, *MONONUCLEAR leukocytes, *BLOOD plasma, *DNA repair, *CENTRAL nervous system

Abstract

Huntington's disease (HD) is characterized by clinical motor impairment (e.g., involuntary movements, poor coordination, parkinsonism), cognitive deficits, and psychiatric symptoms. An inhered expansion of the CAG triplet in the huntingtin gene causing a pathogenic gain-of-function of the mutant huntingtin (mHTT) protein has been identified. In this review, we focus on known biomarkers (e.g., mHTT, neurofilament light chains) and on new biofluid biomarkers that can be quantified in plasma or peripheral blood mononuclear cells from mHTT carriers. Circulating biomarkers may fill current unmet needs in HD management: better stratification of patients amenable to etiologic treatment; the initiation of preventive treatment in premanifest HD; and the identification of peripheral pathogenic central nervous system cascades. [ABSTRACT FROM AUTHOR]

Published

2023

9. New directions in therapeutics for Huntington disease.

Author

Potkin, Katya and Potkin, Steven

Subjects

ASO, Huntington disease, RNAi, VMAT2, chorea, drug therapies, mHtt

Abstract

Huntington disease (HD) is an autosomal dominantly inherited neurodegenerative disease that affects motor, cognitive and psychiatric functions, and ultimately leads to death. The pathology of the disease is based on an expansion of CAG repeats in exon 1 of the huntingtin gene on chromosome 4, which produces a mutant huntingtin protein (mHtt). This protein is involved in neurotoxicity and brain atrophy, and can form β-sheets and abnormal mHtt aggregates. Currently, there are no approved effective treatments for HD, although tetrabenazine (Xenazine™) and deutetrabenazine (AUSTEDO™) have been approved for treatment of the motor symptom chorea in HD. This literature review aims to address the latest research on promising therapeutics based on influencing the hypothesized pathological mechanisms.

Published

2018

10. A prion-like domain of TFEB mediates the co-aggregation of TFEB and mHTT.

Author

Yang, Junsheng, Xu, Huilin, Zhang, Chaoyue, Yang, Xiaotong, Cai, Weijie, and Chen, Xiaoli

Subjects

TRANSCRIPTION factors, HUNTINGTON disease, CELL physiology, HUNTINGTIN protein, DRUG target, SCRAPIE, AUTOPHAGY, LYSOSOMES

Abstract

The aggregation of mutant HTT (huntingtin; mHTT) is a hallmark of Huntington disease (HD). mHTT aggregates interact and sequester dozens of proteins and affect diverse key cellular functions. Here we report that TFEB (transcription factor EB), a master regulator of lysosome biogenesis and autophagy, is yet another protein that co-aggregates with mHTT. We also found the mHTT-TFEB co-aggregation is mediated by a prion-like domain (PrLD) near the N terminus of TFEB. Our findings point out a possible limitation for therapeutic strategies targeting TFEB to clear mHTT, and also provided a possible explanation for controversies that TFEB overexpression lowered soluble mHTT in some HD models but failed to reduce mHTT aggregates or HD pathology in others. Moreover, we found that TFE3, another MiT family transcription factor that shares overlapping functions with TFEB, lacks PrLD and does not co-aggregate with mHTT, and thus might serve as an alternative drug target for HD. [ABSTRACT FROM AUTHOR]

Published

2023

11. Discovery of an autophagy inducer J3 to lower mutant huntingtin and alleviate Huntington's disease-related phenotype.

Author

Long, Jiahui, Luo, Xia, Fang, Dongmei, Song, Haikun, Fang, Weibin, Shan, Hao, Liu, Peiqing, Lu, Boxun, Yin, Xiao-Ming, Hong, Liang, and Li, Min

Subjects

HUNTINGTON disease, BLOOD-brain barrier, EQUILIBRIUM testing, PROTEOLYSIS, SMALL molecules

Abstract

Huntington's disease (HD) is a neurodegenerative disorder caused by aggregation of the mutant huntingtin (mHTT) protein encoded from extra tracts of CAG repeats in exon 1 of the HTT gene. mHTT proteins are neurotoxic to render the death of neurons and a series of disease-associated phenotypes. The mHTT is degraded through autophagy pathway and ubiquitin–proteasome system (UPS). This study identified a small molecule, J3, as an autophagy inducer by high-content screening. The results revealed that J3 could inhibit mTOR, thus promoting autophagic flux and long-lived protein degradation. Further, J3 selectively lowered the soluble and insoluble mHTT but not wild type HTT levels in cell models. The HdhQ140 mice showed reduced HD-associated activity and loss of motor functions. However, administration of J3 showed increased activity and a slight improvement in the motor function in the open-field test, balance beam test, and rotarod tests. Furthermore, in vivo studies revealed that J3 decreased T-HTT and misfolded protein levels in the striatum and increased the levels of the medium spiny neuron marker DARPP-32. In addition, J3 showed good permeability across the brain-blood barrier efficiently, suggesting that J3 was a promising candidate for the treatment of HD. [ABSTRACT FROM AUTHOR]

Published

2022

12. Longitudinal preclinical evaluation of the novel radioligand [11C]CHDI-626 for PET imaging of mutant huntingtin aggregates in Huntington's disease.

Author

Bertoglio, Daniele, Verhaeghe, Jeroen, Miranda, Alan, Wyffels, Leonie, Stroobants, Sigrid, Mrzljak, Ladislav, Khetarpal, Vinod, Skinbjerg, Mette, Liu, Longbin, Dominguez, Celia, Munoz-Sanjuan, Ignacio, Bard, Jonathan, and Staelens, Steven

Subjects

*HUNTINGTON disease, *EMISSION-computed tomography, *DRUG efficacy, *DISEASE progression, *BRAIN imaging, *BIOLOGICAL tags, *ANIMAL models in research

Abstract

Purpose : As several therapies aimed at lowering mutant huntingtin (mHTT) brain levels in Huntington's disease (HD) are currently being investigated, noninvasive positron emission tomography (PET) imaging of mHTT could be utilized to directly evaluate therapeutic efficacy and monitor disease progression. Here we characterized and longitudinally assessed the novel radioligand [11C]CHDI-626 for mHTT PET imaging in the zQ175DN mouse model of HD. Methods: After evaluating radiometabolites and radioligand kinetics, we conducted longitudinal dynamic PET imaging at 3, 6, 9, and 13 months of age (M) in wild-type (WT, n = 17) and heterozygous (HET, n = 23) zQ175DN mice. Statistical analysis was performed to evaluate temporal and genotypic differences. Cross-sectional cohorts at each longitudinal time point were included for post-mortem [3H]CHDI-626 autoradiography. Results: Despite fast metabolism and kinetics, the radioligand was suitable for PET imaging of mHTT. Longitudinal quantification could discriminate between genotypes already at premanifest stage (3 M), showing an age-associated increase in signal in HET mice in parallel with mHTT aggregate load progression, as supported by the post-mortem [3H]CHDI-626 autoradiography. Conclusion: With clinical evaluation underway, [11C]CHDI-626 PET imaging appears to be a suitable preclinical candidate marker to monitor natural HD progression and for the evaluation of mHTT-lowering therapies. [ABSTRACT FROM AUTHOR]

Published

2022

13. Modulation of mTOR and CREB pathways following mGluR5 blockade contribute to improved Huntington’s pathology in zQ175 mice

Author

Khaled S. Abd-Elrahman and Stephen S. G. Ferguson

Subjects

mGluR5, Huntington’s disease, zQ175, mHTT, CTEP, ULK1, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Huntington’s disease (HD) is a neurodegenerative disorder caused by a genetic abnormality in the huntingtin gene that leads to a polyglutamine repeat expansion of the huntingtin protein. The cleaved polyglutamine expansion of mutant huntingtin (mHTT) protein can form aggregates strongly correlated with HD progression. We have previously shown that the inhibition of mGluR5 using CTEP, a selective negative allosteric mGluR5 modulator, can delay disease progression and reduce in mHTT aggregates in the zQ175 mouse model of HD. This was paralleled by enhanced catalytic activity of Unc-51-like kinase 1 (ULK1), a kinase modulated by mammalian target of rapamycin (mTOR) and key regulator of autophagy initiation. In the present study, we show that CTEP can correct aberrant phosphoinositide 3-kinase (PI3K)/Akt/mTOR signaling detected in zQ175 mice that may underlie the enhanced ULK1 activity and activation of autophagy. We also show that CTEP can facilitate cAMP response element-binding protein (CREB)-mediated expression of brain-derived neurotrophic factor (BDNF) to foster neuronal survival and reduce apoptosis. Taken together, our findings provide the molecular evidence for how targeting mGluR5 using a well-tolerated selective NAM can mitigate two critical mechanisms of neurodegeneration, autophagy and apoptosis.

Published

2019

14. Small, Seeding-Competent Huntingtin Fibrils Are Prominent Aggregate Species in Brains of zQ175 Huntington’s Disease Knock-in Mice

Author

Franziska Schindler, Nicole Praedel, Nancy Neuendorf, Severine Kunz, Sigrid Schnoegl, Michael A. Mason, Bridget A. Taxy, Gillian P. Bates, Ali Khoshnan, Josef Priller, Jan Grimm, Marcel Maier, Annett Boeddrich, and Erich E. Wanker

Subjects

Huntington’s disease, aggregates, seeding, mHTT, zQ175, brain, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The deposition of mutant huntingtin (mHTT) protein aggregates in neurons of patients is a pathological hallmark of Huntington’s disease (HD). Previous investigations in cell-free and cell-based disease models showed mHTT exon-1 (mHTTex1) fragments with pathogenic polyglutamine (polyQ) tracts (>40 glutamines) to self-assemble into highly stable, β-sheet-rich protein aggregates with a fibrillar morphology. HD knock-in mouse models have not been extensively studied with regard to mHTT aggregation. They endogenously produce full-length mHTT with a pathogenic polyQ tract as well as mHTTex1 fragments. Here, we demonstrate that seeding-competent, fibrillar mHTT aggregates can be readily detected in brains of zQ175 knock-in HD mice. To do this, we applied a highly sensitive FRET-based protein amplification assay that is capable of detecting seeding-competent mHTT aggregate species down to the femtomolar range. Furthermore, we show that fibrillar structures with an average length of ∼200 nm can be enriched with aggregate-specific mouse and human antibodies from zQ175 mouse brain extracts through immunoprecipitations, confirming that such structures are formed in vivo. Together these studies indicate that small, fibrillar, seeding-competent mHTT structures are prominent aggregate species in brains of zQ175 mice.

Published

2021

15. Small, Seeding-Competent Huntingtin Fibrils Are Prominent Aggregate Species in Brains of zQ175 Huntington's Disease Knock-in Mice.

Author

Schindler, Franziska, Praedel, Nicole, Neuendorf, Nancy, Kunz, Severine, Schnoegl, Sigrid, Mason, Michael A., Taxy, Bridget A., Bates, Gillian P., Khoshnan, Ali, Priller, Josef, Grimm, Jan, Maier, Marcel, Boeddrich, Annett, and Wanker, Erich E.

Subjects

HUNTINGTON disease, CELL sheets (Biology), LABORATORY mice, SPECIES, MICE

Abstract

The deposition of mutant huntingtin (mHTT) protein aggregates in neurons of patients is a pathological hallmark of Huntington's disease (HD). Previous investigations in cell-free and cell-based disease models showed mHTT exon-1 (mHTTex1) fragments with pathogenic polyglutamine (polyQ) tracts (>40 glutamines) to self-assemble into highly stable, β-sheet-rich protein aggregates with a fibrillar morphology. HD knock-in mouse models have not been extensively studied with regard to mHTT aggregation. They endogenously produce full-length mHTT with a pathogenic polyQ tract as well as mHTTex1 fragments. Here, we demonstrate that seeding-competent, fibrillar mHTT aggregates can be readily detected in brains of zQ175 knock-in HD mice. To do this, we applied a highly sensitive FRET-based protein amplification assay that is capable of detecting seeding-competent mHTT aggregate species down to the femtomolar range. Furthermore, we show that fibrillar structures with an average length of ∼200 nm can be enriched with aggregate-specific mouse and human antibodies from zQ175 mouse brain extracts through immunoprecipitations, confirming that such structures are formed in vivo. Together these studies indicate that small, fibrillar, seeding-competent mHTT structures are prominent aggregate species in brains of zQ175 mice. [ABSTRACT FROM AUTHOR]

Published

2021

16. Escins Isolated from Aesculus chinensis Bge. Promote the Autophagic Degradation of Mutant Huntingtin and Inhibit its Induced Apoptosis in HT22 cells

Author

Yueshan Sun, Xueqin Jiang, Rong Pan, Xiaogang Zhou, Dalian Qin, Rui Xiong, Yiling Wang, Wenqiao Qiu, Anguo Wu, and Jianming Wu

Subjects

Huntington’s disease, autophagy, mHtt, Aesculus chinensis Bge., HT22 cells, Therapeutics. Pharmacology, RM1-950

Abstract

The pathogenesis of Huntington’s disease (HD), an inherited progressive neurodegenerative disease, is highly associated with the cytotoxicity-inducing mutant huntingtin (mHtt) protein. Emerging evidence indicates that autophagy plays a pivotal role in degrading aggregated proteins such as mHtt to enhance neuronal viability. In this study, by employing preparative high-performance liquid chromatography (pre-HPLC), ultra-high performance liquid chromatography diode-array-detector quadrupole time-of-flight mass spectrometry (UHPLC-DAD-Q-TOF-MS) and nuclear magnetic resonance (NMR), three escins, escin IA (EA), escin IB (EB) and isoescin IA (IEA), were isolated and identified from the seed of Aesculus chinensis Bge. (ACB). After EGFP-HTT74-overexpressing HT22 cells were treated with EA, EB and IEA at safe concentrations, the clearance of mHtt and mHtt-induced apoptosis were investigated by Western blot, immunofluorescence microscopy and flow cytometry methods. In addition, the autophagy induced by these escins in HT22 cells was monitored by detecting GFP-LC3 puncta, P62 and LC3 protein expression. The results showed that EA, EB and IEA could significantly decrease mHtt levels and inhibit its induced apoptosis in HT22 cells. In addition, these three saponins induced autophagic flux by increasing the ratio of RFP-LC3 to GFP-LC3, and by decreasing P62 expression. Among the tested escins, EB displayed the best autophagy induction, which was regulated via both the mTOR and ERK signaling pathways. Furthermore, the degradation of mHtt and the commensurate decrease in its cytotoxic effects by EA, EB and IEA were demonstrated to be closely associated with autophagy induction, which depended on ATG7. In conclusion, we are the first to report that the escins, including EA, EB and IEA are novel autophagy inducers that degrade mHtt and inhibit mHtt-induced apoptosis in vitro and in vivo. As a result of these findings, the triterpenoid saponins in ACB might be considered to be promising candidates for the treatment of HD in the future.

Published

2020

17. Escins Isolated from Aesculus chinensis Bge. Promote the Autophagic Degradation of Mutant Huntingtin and Inhibit its Induced Apoptosis in HT22 cells.

Author

Sun, Yueshan, Jiang, Xueqin, Pan, Rong, Zhou, Xiaogang, Qin, Dalian, Xiong, Rui, Wang, Yiling, Qiu, Wenqiao, Wu, Anguo, and Wu, Jianming

Subjects

HUNTINGTON disease, TIME-of-flight mass spectrometry, HIGH performance liquid chromatography, AUTOPHAGY, TRITERPENOID saponins, NUCLEAR magnetic resonance

Abstract

The pathogenesis of Huntington's disease (HD), an inherited progressive neurodegenerative disease, is highly associated with the cytotoxicity-inducing mutant huntingtin (mHtt) protein. Emerging evidence indicates that autophagy plays a pivotal role in degrading aggregated proteins such as mHtt to enhance neuronal viability. In this study, by employing preparative high-performance liquid chromatography (pre-HPLC), ultra-high performance liquid chromatography diode-array-detector quadrupole time-of-flight mass spectrometry (UHPLC-DAD-Q-TOF-MS) and nuclear magnetic resonance (NMR), three escins, escin IA (EA), escin IB (EB) and isoescin IA (IEA), were isolated and identified from the seed of Aesculus chinensis Bge. (ACB). After EGFP-HTT74-overexpressing HT22 cells were treated with EA, EB and IEA at safe concentrations, the clearance of mHtt and mHtt-induced apoptosis were investigated by Western blot, immunofluorescence microscopy and flow cytometry methods. In addition, the autophagy induced by these escins in HT22 cells was monitored by detecting GFP-LC3 puncta, P62 and LC3 protein expression. The results showed that EA, EB and IEA could significantly decrease mHtt levels and inhibit its induced apoptosis in HT22 cells. In addition, these three saponins induced autophagic flux by increasing the ratio of RFP-LC3 to GFP-LC3, and by decreasing P62 expression. Among the tested escins, EB displayed the best autophagy induction, which was regulated via both the mTOR and ERK signaling pathways. Furthermore, the degradation of mHtt and the commensurate decrease in its cytotoxic effects by EA, EB and IEA were demonstrated to be closely associated with autophagy induction, which depended on ATG7. In conclusion, we are the first to report that the escins, including EA, EB and IEA are novel autophagy inducers that degrade mHtt and inhibit mHtt-induced apoptosis in vitro and in vivo. As a result of these findings, the triterpenoid saponins in ACB might be considered to be promising candidates for the treatment of HD in the future. [ABSTRACT FROM AUTHOR]

Published

2020

18. Number and molecular brightness analysis reveals Htt25Q protein aggregation upon the uptake of Htt97Q aggregates.

Author

Sameni, Sara, Zhang, Run, and Digman, Michelle A.

Subjects

*CELL aggregation, *PROTEINS, *POLYGLUTAMINE, *OLIGOMERIZATION

Abstract

Number and molecular Brightness (N&B) analysis is a powerful method used to monitor protein aggregation in living cells. Here, we used the N&B method to characterize the unexpanded HTT protein oligomerization after the internalization of the mutant HTT (mHTT) which contains a CAG repeat extensions encoding for long polyglutamine (polyQ) proteins resulting in misfolding and aggregation. HEK cells expressing Htt25Q-mCherry proteins were infected with Htt97Q-EGFP aggregates, by cell to cell uptake, in cultured conditions resulting in an increasing population of dimers and tetramers compared to our controls. This study shows for the first time the impact of protein aggregation in the unexpanded Htt25Q-mCherry expressing cells that occurs from cell to cell transfer of the expanded Htt97Q-EGFP. These results signify the sporadic behavior of the polyQ inclusion that gives insight into the mechanism of protein dynamics as a consequence of secreted mHTT aggregates. • Uptake of exogenous Htt97Q-EGFP aggregates at the early stage by healthy cells. • N&B analysis method monitors monomers and oligomers in live mammalian cells. • polyQ Oligomerization in healthy cells after the internalization of mHTT aggregates. [ABSTRACT FROM AUTHOR]

Published

2020

19. Transcriptional Assessment of Striatal mRNAs as Valid Biomarkers of Disease Progression in Three Mouse Models of Huntington's Disease.

Author

Ghavami, Afshin, Olsen, Michael, Kwan, Mei, Beltran, Jose, Shea, John, Ramboz, Sylvie, Duan, Wenzhen, Lavery, Daniel, Howland, David, and Park, Larry C.

Subjects

*HUNTINGTON disease, *DISEASE progression, *SPINOCEREBELLAR ataxia, *BASAL ganglia, *CHIMERIC proteins, *BASAL ganglia diseases, *MICE

Abstract

Background: Huntington's disease (HD) is a progressive neurodegenerative disorder that prominently affects the basal ganglia, leading to affective, cognitive, behavioral, and motor decline. The primary site of neuron loss in HD is the striatal part of the basal ganglia, with GABAergic medium size spiny neurons (MSNs) being nearly completely lost in advanced HD. Objective: Based on the hypothesis that mutant huntingtin (mHTT) protein injures neurons via transcriptional dysregulation, we set out to establish a transcriptional profile of HD disease progression in the well characterized transgenic mouse model, R6/2, and two Knock-in models (KI); zQ175KI (expressing mutant mouse/human chimeric Htt protein) and HdhQ200 HET KI (carrying one allele of expanded mouse CAG repeats). Methods: In this study, we used quantitative PCR (qPCR) to evaluate striatal mRNA levels of markers of neurotransmission, neuroinflammation, and energy metabolism. Results: After analyzing and comparing transcripts from pre-symptomatic and symptomatic stages, markers expressed in the basal ganglia MSNs, which are typically involved in maintaining normal neurotransmission, showed a genotype-specific decrease in mRNA expression in a pattern consistent with human studies. In contrast, transcripts associated with neuroinflammation and energy metabolism were mostly unaffected in these animal models of HD. Conclusion: Our results show that transcripts linked to neurotransmission are significantly reduced and are consistent with disease progression in both zQ175KI and R6/2 transgenic mouse models. [ABSTRACT FROM AUTHOR]

Published

2020

20. In Vivo Cerebral Imaging of Mutant Huntingtin Aggregates Using 11 C-CHDI-180R PET in a Nonhuman Primate Model of Huntington Disease.

Author

Bertoglio D, Weiss AR, Liguore W, Martin LD, Hobbs T, Templon J, Srinivasan S, Dominguez C, Munoz-Sanjuan I, Khetarpal V, Verhaeghe J, Staelens S, Link J, Liu L, Bard JA, and McBride JL

Subjects

Animals, Huntingtin Protein genetics, Positron Emission Tomography Computed Tomography, Macaca mulatta metabolism, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Positron-Emission Tomography, Disease Models, Animal, Huntington Disease metabolism

Abstract

Huntington disease (HD) is a neurodegenerative disorder caused by an expanded polyglutamine (CAG) trinucleotide expansion in the huntingtin ( HTT ) gene that encodes the mutant huntingtin protein (mHTT). Visualization and quantification of cerebral mHTT will provide a proxy for target engagement and a means to evaluate therapeutic interventions aimed at lowering mHTT in the brain. Here, we validated the novel radioligand 11 C-labeled 6-(5-((5-methoxypyridin-2-yl)methoxy)benzo[d]oxazol-2-yl)-2-methylpyridazin-3(2H)-one ( 11 C-CHDI-180R) using PET imaging to quantify cerebral mHTT aggregates in a macaque model of HD. Methods: Rhesus macaques received MRI-guided intrastriatal delivery of a mixture of AAV2 and AAV2.retro viral vectors expressing an HTT fragment bearing 85 CAG repeats (85Q, n = 5), a control HTT fragment bearing 10 CAG repeats (10Q, n = 4), or vector diluent only (phosphate-buffered saline, n = 5). Thirty months after surgery, 90-min dynamic PET/CT imaging was used to investigate 11 C-CHDI-180R brain kinetics, along with serial blood sampling to measure input function and stability of the radioligand. The total volume of distribution was calculated using a 2-tissue-compartment model as well as Logan graphical analysis for regional quantification. Immunostaining for mHTT was performed to corroborate the in vivo findings. Results: 11 C-CHDI-180R displayed good metabolic stability (51.4% ± 4.0% parent in plasma at 60 min after injection). Regional time-activity curves displayed rapid uptake and reversible binding, which were described by a 2-tissue-compartment model. Logan graphical analysis was associated with the 2-tissue-compartment model ( r 2 = 0.96, P < 0.0001) and used to generate parametric volume of distribution maps. Compared with controls, animals administered the 85Q fragment exhibited significantly increased 11 C-CHDI-180R binding was observed between buffer and 10Q animals. The presence of mHTT aggregates in the 85Q animals was confirmed histologically. P < 0.0001). No difference in 11 C-CHDI-180R as a radioligand to visualize and quantify mHTT aggregated species in a HD macaque model. These findings corroborate our previous work in rodent HD models and show that Conclusion: C-CHDI-180R is a promising tool to assess the mHTT aggregate load and the efficacy of therapeutic strategies.11 C-CHDI-180R as a radioligand to visualize and quantify mHTT aggregated species in a HD macaque model. These findings corroborate our previous work in rodent HD models and show that 11 C-CHDI-180R is a promising tool to assess the mHTT aggregate load and the efficacy of therapeutic strategies., (© 2023 by the Society of Nuclear Medicine and Molecular Imaging.)

Published

2023

21. Role of adenosine pathway on cell growth and stress response in Drosophila

Author

MAAROUFI, Houda Ouns

Subjects

cell growth, stress response, adenosine pathway, cnt1, mHTT, metabolism

Abstract

The thesis surveyed the effects of the adenosine pathway on cell growth and stress response. We described the effects of mutation of the concentrative nucleoside transporter cnt1 on male fertility, particularly spermatogenesis, using a Drosophila melanogaster model. We also described the effects of the adenosine pathway on the cytotoxicity of mHTT.

Published

2022

22. Immunotherapeutic Approaches for the Treatment of Neurodegenerative Diseases: Challenges and Outcomes.

Author

Sushma and Mondal AC

Subjects

Humans, alpha-Synuclein metabolism, tau Proteins, Amyloid beta-Peptides, Immunotherapy, Neurodegenerative Diseases therapy, Neurodegenerative Diseases metabolism, Parkinson Disease

Abstract

Background: Neurodegenerative diseases, being rapidly increasing disorders and the seventh leading cause of death worldwide, have been a great challenge for researchers, affecting cognition, motor activity and other body functioning due to neurodegeneration. Several neurodegenerative diseases are caused by aggregation of proteins which induce the alteration of neuronal function leading to cell death. These proteins are amyloid-β peptide, tau, α-synuclein, and mHTT, which cause Alzheimer's disease, Frontotemporal dementia, Corticobasal degeneration, Progressive supranuclear palsy, Parkinson's disease, Multiple system atrophy, Dementia with Lewy-body and Huntington's disease. Currently available treatments only reduce symptoms and increase life sustainability; however, they possess side effects and are ineffective in curing the diseases., Objective: Literature survey of neurodegenerative diseases and immunotherapeutic approaches is used to evaluate their pharmacological effects and future endeavours., Methods: A literature search was performed to find the relevant articles related to neurodegenerative diseases and immunotherapies. Clinical trials data were analysed from clinicaltrial.com., Results: According to the literature study, it was found that researchers have explored the effect of active and passive vaccines generated against amyloid-β, tau, α-synuclein and mHTT. Few clinical trials have shown severe side effects and terminated, despite that, few of them produced desirable effects for the treatment of AD and PD., Conclusion: Several immunotherapeutic trials have shown promising outcomes against amyloid-β, tau and α-synuclein. In addition, various preclinical studies against mHTT and prion proteins are under scrutinization. These clinical outcomes indicate a promising role of immunotherapies against neurodegenerative diseases., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2023

23. Escins Isolated from

Author

Yueshan, Sun, Xueqin, Jiang, Rong, Pan, Xiaogang, Zhou, Dalian, Qin, Rui, Xiong, Yiling, Wang, Wenqiao, Qiu, Anguo, Wu, and Jianming, Wu

Subjects

Pharmacology, mHtt, autophagy, HT22 cells, Aesculus chinensis Bge, Original Research, Huntington’s disease

Abstract

The pathogenesis of Huntington’s disease (HD), an inherited progressive neurodegenerative disease, is highly associated with the cytotoxicity-inducing mutant huntingtin (mHtt) protein. Emerging evidence indicates that autophagy plays a pivotal role in degrading aggregated proteins such as mHtt to enhance neuronal viability. In this study, by employing preparative high-performance liquid chromatography (pre-HPLC), ultra-high performance liquid chromatography diode-array-detector quadrupole time-of-flight mass spectrometry (UHPLC-DAD-Q-TOF-MS) and nuclear magnetic resonance (NMR), three escins, escin IA (EA), escin IB (EB) and isoescin IA (IEA), were isolated and identified from the seed of Aesculus chinensis Bge. (ACB). After EGFP-HTT74-overexpressing HT22 cells were treated with EA, EB and IEA at safe concentrations, the clearance of mHtt and mHtt-induced apoptosis were investigated by Western blot, immunofluorescence microscopy and flow cytometry methods. In addition, the autophagy induced by these escins in HT22 cells was monitored by detecting GFP-LC3 puncta, P62 and LC3 protein expression. The results showed that EA, EB and IEA could significantly decrease mHtt levels and inhibit its induced apoptosis in HT22 cells. In addition, these three saponins induced autophagic flux by increasing the ratio of RFP-LC3 to GFP-LC3, and by decreasing P62 expression. Among the tested escins, EB displayed the best autophagy induction, which was regulated via both the mTOR and ERK signaling pathways. Furthermore, the degradation of mHtt and the commensurate decrease in its cytotoxic effects by EA, EB and IEA were demonstrated to be closely associated with autophagy induction, which depended on ATG7. In conclusion, we are the first to report that the escins, including EA, EB and IEA are novel autophagy inducers that degrade mHtt and inhibit mHtt-induced apoptosis in vitro and in vivo. As a result of these findings, the triterpenoid saponins in ACB might be considered to be promising candidates for the treatment of HD in the future.

Published

2019

24. Passive immunization against phosphorylated tau improves features of Huntington's disease pathology.

Author

Alpaugh M, Masnata M, de Rus Jacquet A, Lepinay E, Denis HL, Saint-Pierre M, Davies P, Planel E, and Cicchetti F

Subjects

Animals, Brain metabolism, Disease Models, Animal, Humans, Huntingtin Protein genetics, Huntingtin Protein metabolism, Immunization, Passive, Mice, Neurons metabolism, Huntington Disease genetics, Huntington Disease metabolism, Huntington Disease therapy, Induced Pluripotent Stem Cells metabolism

Abstract

Huntington's disease is classically described as a neurodegenerative disorder of monogenic aetiology. The disease is characterized by an abnormal polyglutamine expansion in the huntingtin gene, which drives the toxicity of the mutated form of the protein. However, accumulation of the microtubule-associated protein tau, which is involved in a number of neurological disorders, has also been observed in patients with Huntington's disease. In order to unravel the contribution of tau hyperphosphorylation to hallmark features of Huntington's disease, we administered weekly intraperitoneal injections of the anti-tau pS202 CP13 monoclonal antibody to zQ175 mice and characterized the resulting behavioral and biochemical changes. After 12 weeks of treatment, motor impairments, cognitive performance and general health were improved in zQ175 mice along with a significant reduction in hippocampal pS202 tau levels. Despite the lack of effect of CP13 on neuronal markers associated with Huntington's disease pathology, tau-targeting enzymes and gliosis, CP13 was shown to directly impact mutant huntingtin aggregation such that brain levels of amyloid fibrils and huntingtin oligomers were decreased, while larger huntingtin protein aggregates were increased. Investigation of CP13 treatment of Huntington's disease patient-derived induced pluripotent stem cells (iPSCs) revealed a reduction in pS202 levels in differentiated cortical neurons and a rescue of neurite length. Collectively, these findings suggest that attenuating tau pathology could mitigate behavioral and molecular hallmarks associated with Huntington's disease., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2022

25. The Tiny Drosophila Melanogaster for the Biggest Answers in Huntington’s Disease

Author

Argel Estrada-Mondragón, Ricardo Piña, Maite A. Castro, Carola A. Mantellero, and Abraham Rosas-Arellano

Subjects

0301 basic medicine, HD, mHTT, medicine.medical_specialty, Huntingtin, Neurology, huntingtin, Disease, neostriatum, Catalysis, Inorganic Chemistry, polyQ, polyglutamine disorders, lcsh:Chemistry, 03 medical and health sciences, 0302 clinical medicine, Huntington's disease, medicine, neurodegenerative diseases, chorea, Physical and Theoretical Chemistry, Molecular Biology, Drosophila, lcsh:QH301-705.5, Spectroscopy, biology, LOMARS, Organic Chemistry, fruit fly, Chorea, General Medicine, medicine.disease, biology.organism_classification, IT15, Computer Science Applications, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Life expectancy, medicine.symptom, Drosophila melanogaster, HTT, Neuroscience, 030217 neurology & neurosurgery

Abstract

The average life expectancy for humans has increased over the last years. However, the quality of the later stages of life is low and is considered a public health issue of global importance. Late adulthood and the transition into the later stage of life occasionally leads to neurodegenerative diseases that selectively affect different types of neurons and brain regions, producing motor dysfunctions, cognitive impairment, and psychiatric disorders that are progressive, irreversible, without remission periods, and incurable. Huntington’s disease (HD) is a common neurodegenerative disorder. In the 25 years since the mutation of the huntingtin (HTT) gene was identified as the molecule responsible for this neural disorder, a variety of animal models, including the fruit fly, have been used to study the disease. Here, we review recent research that used Drosophila as an experimental tool for improving knowledge about the molecular and cellular mechanisms underpinning HD.

Published

2018

26. The Tiny

Author

Abraham, Rosas-Arellano, Argel, Estrada-Mondragón, Ricardo, Piña, Carola A, Mantellero, and Maite A, Castro

Subjects

HD, mHTT, huntingtin, LOMARS, fruit fly, Review, neostriatum, IT15, polyQ, polyglutamine disorders, Disease Models, Animal, Drosophila melanogaster, Huntington Disease, Animals, Humans, neurodegenerative diseases, chorea, HTT

Abstract

The average life expectancy for humans has increased over the last years. However, the quality of the later stages of life is low and is considered a public health issue of global importance. Late adulthood and the transition into the later stage of life occasionally leads to neurodegenerative diseases that selectively affect different types of neurons and brain regions, producing motor dysfunctions, cognitive impairment, and psychiatric disorders that are progressive, irreversible, without remission periods, and incurable. Huntington’s disease (HD) is a common neurodegenerative disorder. In the 25 years since the mutation of the huntingtin (HTT) gene was identified as the molecule responsible for this neural disorder, a variety of animal models, including the fruit fly, have been used to study the disease. Here, we review recent research that used Drosophila as an experimental tool for improving knowledge about the molecular and cellular mechanisms underpinning HD.

Published

2018

27. Visualization of Mutant Aggregates from Clock Neurons by Agarose Gel Electrophoresis (AGERA) in Drosophila melanogaster.

Author

Delfino L, Campesan S, Fedele G, Green EW, Giorgini F, Kyriacou CP, and Rosato E

Subjects

Animals, Circadian Rhythm physiology, Drosophila metabolism, Electrophoresis, Agar Gel, Neurons metabolism, Drosophila Proteins genetics, Drosophila Proteins metabolism, Drosophila melanogaster metabolism

Abstract

The clock neurons of the fruit fly Drosophila melanogaster have become a useful model for expressing misfolded protein aggregates that accumulate in several human neurodegenerative diseases. One advantage of such an approach is that the behavioral effects can be readily quantified on circadian locomotor rhythms, sleep or activity levels via automated, highly reliable and objective procedures. Therefore, a rapid assay is required to visualize whether these neurons develop aggregates. Here we describe a modified immunoblot method, agarose gel electrophoresis (AGERA) that has been optimized for resolving aggregates from fly clock neurons., (© 2022. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2022

28. Dysregulation of long non-coding RNAs and their mechanisms in Huntington's disease.

Author

Tan X, Liu Y, Liu Y, Zhang T, and Cong S

Subjects

Animals, Brain pathology, Humans, Huntingtin Protein genetics, Huntington Disease genetics, Huntington Disease pathology, RNA, Long Noncoding genetics, Brain metabolism, Gene Regulatory Networks physiology, Huntingtin Protein metabolism, Huntington Disease metabolism, RNA, Long Noncoding metabolism

Abstract

Extensive alterations in gene regulatory networks are a typical characteristic of Huntington's disease (HD); these include alterations in protein-coding genes and poorly understood non-coding RNAs (ncRNAs), which are associated with pathology caused by mutant huntingtin. Long non-coding RNAs (lncRNAs) are an important class of ncRNAs involved in a variety of biological functions, including transcriptional regulation and post-transcriptional modification of many targets, and likely contributed to the pathogenesis of HD. While a number of changes in lncRNAs expression have been observed in HD, little is currently known about their functions. Here, we discuss their possible mechanisms and molecular functions, with a particular focus on their roles in transcriptional regulation. These findings give us a better insight into HD pathogenesis and may provide new targets for the treatment of this neurodegenerative disease., (© 2021 Wiley Periodicals LLC.)

Published

2021

29. Modulation of mTOR and CREB pathways following mGluR5 blockade contribute to improved Huntington's pathology in zQ175 mice.

Author

Abd-Elrahman, Khaled S. and Ferguson, Stephen S. G.

Subjects

HUNTINGTON disease, HUNTINGTON'S chorea treatment, MTOR inhibitors, NEURODEGENERATION, GENETICS, POLYGLUTAMINE, RAPAMYCIN, PHOSPHOINOSITIDES

Abstract

Huntington's disease (HD) is a neurodegenerative disorder caused by a genetic abnormality in the huntingtin gene that leads to a polyglutamine repeat expansion of the huntingtin protein. The cleaved polyglutamine expansion of mutant huntingtin (mHTT) protein can form aggregates strongly correlated with HD progression. We have previously shown that the inhibition of mGluR5 using CTEP, a selective negative allosteric mGluR5 modulator, can delay disease progression and reduce in mHTT aggregates in the zQ175 mouse model of HD. This was paralleled by enhanced catalytic activity of Unc-51-like kinase 1 (ULK1), a kinase modulated by mammalian target of rapamycin (mTOR) and key regulator of autophagy initiation. In the present study, we show that CTEP can correct aberrant phosphoinositide 3-kinase (PI3K)/Akt/mTOR signaling detected in zQ175 mice that may underlie the enhanced ULK1 activity and activation of autophagy. We also show that CTEP can facilitate cAMP response element-binding protein (CREB)-mediated expression of brain-derived neurotrophic factor (BDNF) to foster neuronal survival and reduce apoptosis. Taken together, our findings provide the molecular evidence for how targeting mGluR5 using a well-tolerated selective NAM can mitigate two critical mechanisms of neurodegeneration, autophagy and apoptosis. [ABSTRACT FROM AUTHOR]

Published

2019

30. The Tiny Drosophila Melanogaster for the Biggest Answers in Huntington’s Disease.

Author

Rosas-Arellano, Abraham, Estrada-Mondragón, Argel, Piña, Ricardo, Mantellero, Carola A., and Castro, Maite A.

Subjects

*DROSOPHILA melanogaster, *HUNTINGTON disease, *NEURODEGENERATION, *ANIMAL models in research, *GENETIC mutation

Abstract

The average life expectancy for humans has increased over the last years. However, the quality of the later stages of life is low and is considered a public health issue of global importance. Late adulthood and the transition into the later stage of life occasionally leads to neurodegenerative diseases that selectively affect different types of neurons and brain regions, producing motor dysfunctions, cognitive impairment, and psychiatric disorders that are progressive, irreversible, without remission periods, and incurable. Huntington’s disease (HD) is a common neurodegenerative disorder. In the 25 years since the mutation of the huntingtin (HTT) gene was identified as the molecule responsible for this neural disorder, a variety of animal models, including the fruit fly, have been used to study the disease. Here, we review recent research that used Drosophila as an experimental tool for improving knowledge about the molecular and cellular mechanisms underpinning HD. [ABSTRACT FROM AUTHOR]

Published

2018

31. Nrf2 Activation by Dimercaptopropanol Attenuates Mutant Huntingtin Toxicity

Author

Dailey, Kyle M

Subjects

Huntington's Disease, mHtt, Dimercaptopropanol, Chemical Actions and Uses, ROS, Prx1, Biology, Nrf2, ARE

Abstract

Huntington’s disease (HD) is a fatal neurodegenerative disorder resulting from the expansion of a trinucleotide repeat within the HD gene. At the cellular level mutant HTT (mHTT) aggregates perturb cellular metabolism, intracellular trafficking and mitochondrial function, resulting in the increased production of reactive oxygen species (ROS) an event closely linked with nerve cell death. Nuclear factor erythroid 2-related factor 2 (NRF2) is a redox-sensitive transcription factor responsible for transcribing neuroprotective genes under the control of the antioxidant response element (ARE), which work to counteract high intracellular ROS levels. I have identified significant increases in cell viability, NRF2 nuclear localization, and ARE-luciferase reporter activity following treatment with the NRF2 activator dimercaptopropanol (DMP). DMP was also found to increase ARE-directed gene expression and maintain a greater proportion of functionally active peroxiredoxin 1 (PRX1) protein levels, resulting in increased neuronal survival. For this reason DMP may serve an important role in treating HD.

Published

2012

32. Investigation of the role of collapsin response mediator 4 in Huntington's disease

Author

Nicoletti, Cecilia

Subjects

Huntington's Disease, mhtt, inclusions, cytoskeleton, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit, CRMP4

Abstract

Huntington’s disease (HD) is an inherited neurodegenerative disorder characterized by the ac- cumulation in the affected neuronal population of N-terminal huntingtin (htt) fragments bear- ing elongated polyglutamine (polyQ) tracts. Several lines of evidence indicate that the process of htt misfolding and aggregation is associated with cytotoxicity in HD models and patients. Thus, the identification and characterization of proteins that can modulate this process is criti- cal for understanding HD pathogenesis and therapy development. Here, we report a depletion of collapsin response mediator protein 4 (CRMP4) protein levels in a cell culture model of HD. CRMP4 belongs to the collapsin response mediator protein family that mediates many aspects of neuronal development and plasticity by regulating cytoskeleton dynamics. Cell-free and cell-based assays demonstrate that CRMP4 reduces polyQ-mediated htt ag- gregation and toxicity. Furthermore our results show that this effect may be linked to a re- arrangement of Actin cytoskeleton. Indeed both, CRMP4 and filamentous Actin (F-Actin), are recruited into the intracellular inclusions formed by mutant huntingtin (mhtt), while over- expression of CRMP4 partially detached F-Actin from the mhtt aggregates. CRMP4 is cleaved by Calpain-1 when mhtt is expressed. This result links to previous findings showing the same proteolytic cleavage of CRMP4 when cells were subject to excitotoxicity. The proteolysis of CRMP4 may therefore be a marker of neuronal toxicity. This work suggests a functional link between mhtt and CRMP4 and a role for CRMP4 as a new modulator of mhtt. Further stud- ies are important for understanding whether CRMP4 can help deciphering the early cellular pathomechanisms in HD., Chorea Huntington (HD) ist eine vererbte, neurodegenerative Erkrankung. In der Krankheit zeigen die betroffene neuronalen Zellen Einschlusskörperchen von N-terminalen Huntingtin-Fragmenten (htt) mit länglichem Polyglutamin (polyQ). Es gibt Hinweise, dass der Prozess der htt Fehlfaltung und der Aufbau von htt- Einschlusskörperchen zytotoxisch wirkt, sowohl in HD-Modellen als auch in Patienten. Das Identifizieren und Charakterisieren von Proteinen, die diesen Prozess modulieren können, ist deshalb wichtig für das Verständnis der HD Pathogenese und für das Entwickeln von Therapien. Die vorliegende Arbeit berichtet über das Sinken des CRMP4-Spiegels (Collapsin Response Mediator Protein 4) in einem Zellkultur-Modell der HD, eine CRMP4-Depletion. Die Gruppe der CRMPs ist eine Protein-Familie, die in der Zytoskelett-Dynamik wirkt, vor allem in der neuronalen Entwicklung und Plastizität. Sowohl zellfreie als auch zellbasierte Assays zeigen, dass die Zahl der durch mutiertes Huntingtin (mhtt) induzierten Einschlusskörperchen durch CRMP4 verringert wird, und dass CRMP4 auch die Toxizität reduziert. Darüber hinaus zeigen die vorliegenden Untersuchungen, dass das Reduzieren von Einschlusskörperchen und Toxizität mit einer Neuordnung des Aktin-Zytoskeletts verbunden ist. CRMP4 und Aktinfilamente (F-Aktin) wurden in den intrazellulären Einschlusskörperchen von mhtt gehäuft nachgewiesen, dagegen ist F-Aktin nach CRMP4-Überexpression nicht mehr in den mhtt-Einschlusskörperchen nachweisbar. CRMP4 wird unter mhtt-Expression durch Calpain-1 gespalten. Dieses Ergebnis wird durch frühere Befunde gestützt, die die gleiche proteolytische Spaltung von CRMP4 unter Excitotoxizität zeigen. Die Proteolyse von CRMP4 kann daher ein Marker für neuronale Toxizität sein. Diese Arbeit schlägt eine funktionale Beziehung zwischen mhtt und CRMP4, und eine Rolle für CRMP4 als neuer Modulator der mhtt vor. Weitere Untersuchungen könnten zeigen ob CRMP4 zum Entschlüsseln der frühen zellulären Pathogenese in HD beitragen kann.

Published

2011

33. How the manipulation of the Ras homolog enriched in striatum alters the behavioral and molecular progression of Huntington’s disease

Author

Lee, Franklin A

Subjects

Rhes, RasD2, Huntington’s Disease, Huntingtin, mHtt, aggregate, Amino Acids, Peptides, and Proteins, Biological Phenomena, Cell Phenomena, and Immunity, Genetic Processes, Medical Anatomy, Medical Biochemistry, Medical Cell Biology, Medical Genetics, Medical Molecular Biology, Medical Neurobiology, Nervous System, Neurosciences

Abstract

Huntington’s disease is an incurable, progressive neurological disorder characterized by loss of motor control, psychiatric dysfunction, and eventual dystonia leading to death. Despite the fact that this disorder is caused by a mutation in one single gene, there is no cure. The mutant Huntingtin (mHtt) protein is expressed ubiquitously throughout the brain but frank cell death is limited to the striatum. Recent work has suggested that Rhes, Ras homolog enriched in striatum, which is selectively expressed in the striatum, may play a role in Huntington’s disease neuropathology. In vitro studies have shown Rhes to be an E3 ligase for the post-translational modification protein SUMO. Rhes increases binding of SUMO to mHtt which competes for the same binding site as Ubiquitin. SUMOylation of mHtt leads to disaggregation and cellular death, whereas ubiquitination leads to aggregation and cellular protection. In a previous study we showed that deletion of Rhes caused a decrease in the Huntington’s disease phenotype in mice. We hypothesized that mice lacking Rhes would also show increased aggregation in the striatum and this increased aggregation would correlate in a rescue of behavioral symptoms. Despite the prior in vitro and in vivo evidence, deletion of Rhes in vivo did not alter the aggregation of mHtt in the striatum of mice however deletion of Rhes still showed a rescue from the diseased phenotype. This result would indicate that deletion of Rhes alters the neurobehavioral phenotype of Huntington’s disease through a different pathway than promoting aggregation in striatal cells.

Published

2015

34. A Thesis Entitled The Evaluation of Neurotrophic Factor’s Ability to Prevent Induced Cell Death in a PC12 Cell Based Huntington’s Disease Model

Author

Wisner, Alexander S.

Subjects

Pharmacology, Huntingtin, neurotrophic, huntington disease, PC12, htt, mhtt, Colivelin, D-NAP, D-SAL

Abstract

Huntington’s disease (HD) is caused by a genetic mutation of the IT-15 gene resulting in the expansion of the trinucleotide CAG in the huntingtin protein (MacDonald et al., 2003). The mechanism(s) by which this expanded protein causes the disease remains unknown, and there is currently no treatment to halt or prevent development of the disease. An assay was designed to measure the ability of three neurotrophic peptides (Colivelin, D-SAL, D-NAP) to protect cultured PC12 cells from death caused by an expanded form of human huntingtin exon 1. Each neurotrophic peptide was tested at six concentrations for its ability to protect cells against huntingtin-induced cell death. Cell viability was determined by an LDH activity assay that measured the change in absorbance over time. Neurotrophic peptides Colivelin and D-SAL promoted cell viability in both treatment types tested whereas D-NAP only promoted cell viability in the twenty-four hour pre-incubation treatment type.

Published

2015

35. Amitriptyline improves motor function via enhanced neurotrophin signaling and mitochondrial functions in the murine N171-82Q Huntington disease model.

Author

Cong WN, Chadwick W, Wang R, Daimon CM, Cai H, Amma J, Wood WH 3rd, Becker KG, Martin B, and Maudsley S

Subjects

Animals, Brain-Derived Neurotrophic Factor, Computational Biology, Disease Models, Animal, Female, Huntington Disease metabolism, Male, Mice, Mitochondria drug effects, Amitriptyline therapeutic use, Huntington Disease drug therapy, Huntington Disease physiopathology, Mitochondria metabolism, Nerve Growth Factors metabolism

Abstract

Huntington disease (HD) is a neurodegenerative disorder characterized by progressive motor impairment and cognitive alterations. Hereditary HD is primarily caused by the expansion of a CAG trinucleotide repeat in the huntingtin (Htt) gene, which results in the production of mutant huntingtin protein (mHTT) with an expanded amino-terminal polyglutamine (poly(Q)) stretch. Besides pathological mHTT aggregation, reduced brain-derived neurotrophic factor (BDNF) levels, impaired neurotrophin signaling, and compromised mitochondrial functions also contribute to the deleterious progressive etiology of HD. As a well tolerated Food and Drug Administration-approved antidepressant, amitriptyline (AMI) has shown efficacy in treating neurodegenerative murine models via potentiation of BDNF levels and amelioration of alterations in neurotrophin signaling pathways. In this study, we observed profound improvements in the motor coordination of AMI-treated N171-82Q HD model mice. The beneficial effects of AMI treatment were associated with its ability to reduce mHTT aggregation, potentiation of the BDNF-TrkB signaling system, and support of mitochondrial integrity and functionality. Our study not only provides preclinical evidence for the therapeutic potency of AMI in treating HD, but it also represents an important example of the usefulness of additional pharmacogenomic profiling of pre-existing drugs for novel therapeutic effects with often intractable pathological scenarios., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

36. Dynamic recruitment of active proteasomes into polyglutamine initiated inclusion bodies.

Author

Schipper-Krom S, Juenemann K, Jansen AH, Wiemhoefer A, van den Nieuwendijk R, Smith DL, Hink MA, Bates GP, Overkleeft H, Ovaa H, and Reits E

Subjects

Animals, Blotting, Western, Brain metabolism, Brain pathology, Cell Line, Tumor, Disease Models, Animal, Female, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, HEK293 Cells, HeLa Cells, Humans, Huntingtin Protein, Huntington Disease genetics, Huntington Disease pathology, Inclusion Bodies genetics, Male, Mice, Mice, Inbred C57BL, Mice, Inbred CBA, Mice, Transgenic, Microscopy, Confocal, Mutation, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Peptides genetics, Proteasome Endopeptidase Complex genetics, Protein Binding, Trinucleotide Repeat Expansion genetics, Huntington Disease metabolism, Inclusion Bodies metabolism, Peptides metabolism, Proteasome Endopeptidase Complex metabolism

Abstract

Neurodegenerative disorders such as Huntington's disease are hallmarked by neuronal intracellular inclusion body formation. Whether proteasomes are irreversibly recruited into inclusion bodies in these protein misfolding disorders is a controversial subject. In addition, it has been proposed that the proteasomes may become clogged by the aggregated protein fragments, leading to impairment of the ubiquitin-proteasome system. Here, we show by fluorescence pulse-chase experiments in living cells that proteasomes are dynamically and reversibly recruited into inclusion bodies. As these recruited proteasomes remain catalytically active and accessible to substrates, our results challenge the concept of proteasome sequestration and impairment in Huntington's disease, and support the reported absence of proteasome impairment in mouse models of Huntington's disease., (Copyright © 2013 Federation of European Biochemical Societies. All rights reserved.)

Published

2014

37. Autophagy and apoptosis dysfunction in neurodegenerative disorders.

Author

Ghavami S, Shojaei S, Yeganeh B, Ande SR, Jangamreddy JR, Mehrpour M, Christoffersson J, Chaabane W, Moghadam AR, Kashani HH, Hashemi M, Owji AA, and Łos MJ

Subjects

Animals, Brain pathology, Brain Diseases pathology, Humans, Neurodegenerative Diseases pathology, Peripheral Nervous System Diseases pathology, Apoptosis, Autophagy, Brain physiopathology, Brain Diseases physiopathology, Neurodegenerative Diseases physiopathology, Neurons pathology, Peripheral Nervous System Diseases physiopathology

Abstract

Autophagy and apoptosis are basic physiologic processes contributing to the maintenance of cellular homeostasis. Autophagy encompasses pathways that target long-lived cytosolic proteins and damaged organelles. It involves a sequential set of events including double membrane formation, elongation, vesicle maturation and finally delivery of the targeted materials to the lysosome. Apoptotic cell death is best described through its morphology. It is characterized by cell rounding, membrane blebbing, cytoskeletal collapse, cytoplasmic condensation, and fragmentation, nuclear pyknosis, chromatin condensation/fragmentation, and formation of membrane-enveloped apoptotic bodies, that are rapidly phagocytosed by macrophages or neighboring cells. Neurodegenerative disorders are becoming increasingly prevalent, especially in the Western societies, with larger percentage of members living to an older age. They have to be seen not only as a health problem, but since they are care-intensive, they also carry a significant economic burden. Deregulation of autophagy plays a pivotal role in the etiology and/or progress of many of these diseases. Herein, we briefly review the latest findings that indicate the involvement of autophagy in neurodegenerative diseases. We provide a brief introduction to autophagy and apoptosis pathways focusing on the role of mitochondria and lysosomes. We then briefly highlight pathophysiology of common neurodegenerative disorders like Alzheimer's diseases, Parkinson's disease, Huntington's disease and Amyotrophic lateral sclerosis. Then, we describe functions of autophagy and apoptosis in brain homeostasis, especially in the context of the aforementioned disorders. Finally, we discuss different ways that autophagy and apoptosis modulation may be employed for therapeutic intervention during the maintenance of neurodegenerative disorders., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2014

38. An integrative approach to elucidate the mechanisms and dynamics of Huntingtin aggregation and inclusion formation in neuronal models of Huntington's Disease

Author

Riguet, Nathan Alain Denis and Lashuel, Hilal

Subjects

Huntington's Disease, mHtt, Httex1, correlative light electron microscopy, aggregation, Huntingtin protein, cellular inclusions, confocal microscopy, polyglutamine, proteomic

Abstract

Despite the fact that the gene responsible for Huntington's disease (HD) is known, we still do not understand the underlying mechanisms leading to neurodegeneration and death. Identifying and understanding the mechanisms controlling mutant huntingtin (mHtt) aggregation and inclusion formation using different cellular and animal models is crucial to elucidate the molecular mechanisms underpinning the disease and to develop effective treatments to prevent or slow the progression of HD. At the mechanistic level, our work shows that mHtt aggregation and inclusion formation in the cytosol and nucleus occur via different mechanisms and lead to the formation of inclusions with distinct biochemical and ultrastructural properties. We show that mHtt cytoplasmic inclusion formation occurs via two phases: 1) a first phase involves the rapid formation of a dense fibrillar core and is driven predominantly by intermolecular interactions involving the polyQ domain via phase separation-like mechanisms; 2) a second phase is associated with the recruitment of soluble mHtt, fibril growth, and the active recruitment and sequestration of lipids, proteins, and membranous organelles. Our work points to this second phase as an important contributor to mHtt toxicity and suggests that targeting inclusion growth and maturation represent a promising therapeutic strategy. These observations suggest that the two types of inclusions may exert their toxicity via different mechanisms and may require different strategies to interfere with their formation, maturation and toxicity. Using primary neurons, we demonstrated that neuronal intranuclear inclusions evolve over time from small aggregates to large granulo-filamentous inclusions associated with cellular toxicity. In addition, our work underscores the failure of the cellular degradation machineries to clear mHtt inclusions, as well as the sequestration of other proteins, lipids and organelles. Finally, we would like to emphasize that our comparative analysis of tag-free and GFP-tagged mutant mHtt aggregation and inclusions formation will inform future efforts to develop models that reproduce HD pathology more faithfully and underscore the need for developing label-free techniques to investigate disease-relevant mechanisms that underpin inclusion formation.