Juvenile Huntington’s Disease and Other PolyQ Diseases, Update on Neurodevelopmental Character and Comparative Bioinformatic Review of Transcriptomic and Proteomic Data

Polyglutamine (PolyQ) diseases are neurodegenerative disorders caused by the CAG repeat expansion mutation in affected genes resulting in toxic proteins containing a long chain of glutamines. There are nine PolyQ diseases: Huntington’s disease (HD), spinocerebellar ataxias (types 1, 2, 3, 6, 7, and 17), dentatorubral-pallidoluysian atrophy (DRPLA), and spinal bulbar muscular atrophy (SBMA). In general, longer CAG expansions and longer glutamine tracts lead to earlier disease presentations in PolyQ patients. Rarely, cases of extremely long expansions are identified for PolyQ diseases, and they consistently lead to juvenile or sometimes very severe infantile-onset polyQ syndromes. In apparent contrast to the very long CAG tracts, shorter CAGs and PolyQs in proteins seems to be the evolutionary factor enhancing human cognition. Therefore, polyQ tracts in proteins can be modifiers of brain development and disease drivers, which contribute neurodevelopmental phenotypes in juvenile- and adult-onset PolyQ diseases. Therefore we performed a bioinformatics review of published RNAseq polyQ expression data resulting from the presence of polyQ genes in search of neurodevelopmental expression patterns and comparison between diseases. The expression data were collected from cell types reflecting stages of development such as iPSC, neuronal stem cell, neurons, but also the adult patients and models for PolyQ disease. In addition, we extended our bioinformatic transcriptomic analysis by proteomics data. We identified a group of 13 commonly downregulated genes and proteins in HD mouse models. Our comparative bioinformatic review highlighted several (neuro)developmental pathways and genes identified within PolyQ diseases and mouse models responsible for neural growth, synaptogenesis, and synaptic plasticity.

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Juvenile Huntington’s Disease and Other PolyQ diseases, Update on Neurodevelopmental Character and Comparative Bioinformatic Review of Transcriptomic Data

10.1101/2021.02.19.431958 ◽

2021 ◽

Author(s):

Karolina Świtońska-Kurkowska ◽

Bart Krist ◽

Joanna Maria Delimata ◽

Maciej Figiel

Keyword(s):

Huntington's Disease ◽

Huntington’S Disease ◽

Muscular Atrophy ◽

Expression Patterns ◽

Cag Repeat ◽

Human Cognition ◽

Expression Data ◽

Spinocerebellar Ataxias ◽

Neuronal Stem Cell ◽

Polyq Diseases

AbstractPolyglutamine (PolyQ) diseases are neurodegenerative disorders caused by the CAG repeat expansion mutation in affected genes resulting in toxic proteins containing a long chain of glutamines. There are nine PolyQ diseases: Huntington’s disease (HD), spinocerebellar ataxias (types 1, 2, 3, 6, 7, and 17), dentatorubral-pallidoluysian atrophy (DRPLA), and spinal bulbar muscular atrophy (SBMA). In general, longer CAG expansions and longer glutamine tracts lead to earlier disease presentations in PolyQ patients. Rarely, cases of extremely long expansions are identified for PolyQ diseases, and they consistently lead to juvenile or sometimes very severe infantile-onset polyQ syndromes. In apparent contrast to the very long CAG tracts, shorter CAGs and PolyQs in proteins seems to be the evolutionary factor enhancing human cognition. Therefore, polyQ tracts in proteins can be modifiers of brain development and disease drivers, which contribute neurodevelopmental phenotypes in juvenile- and adult-onset PolyQ diseases. Therefore we performed a bioinformatics review of published RNAseq polyQ expression data resulting from the presence of polyQ genes in search of neurodevelopmental expression patterns and comparison between diseases. The expression data were collected from cell types reflecting stages of development such as iPSC, neuronal stem cell, neurons, but also the adult patients and models for PolyQ disease. Our comparative bioinformatic review highlighted several (neuro)developmental pathways and genes identified within PolyQ diseases and mouse models responsible for neural growth, synaptogenesis, and synaptic plasticity.

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Skeletal muscle regeneration is altered in the R6/2 mouse model of Huntington's disease

10.1101/2022.01.11.475914 ◽

2022 ◽

Author(s):

Sanzana Hoque ◽

Marie Sjogren ◽

Valerie Allamand ◽

Kinga Gawlik ◽

Naomi Franke ◽

...

Keyword(s):

Skeletal Muscle ◽

Huntington's Disease ◽

Huntington’S Disease ◽

Muscle Damage ◽

Satellite Cell ◽

Mouse Models ◽

Satellite Cells ◽

Muscle Fibers ◽

Cag Repeat ◽

Skeletal Muscle Regeneration

Huntington's disease (HD) is caused by CAG repeat expansion in the huntingtin (HTT) gene. Skeletal muscle wasting alongside central pathology is a well-recognized phenomenon seen in patients with HD and HD mouse models. HD muscle atrophy progresses with disease and affects prognosis and quality of life. Satellite cells, progenitors of mature skeletal muscle fibers, are essential for proliferation, differentiation, and repair of muscle tissue in response to muscle injury or exercise. In this study, we aim to investigate the effect of mutant HTT on the differentiation and regeneration capacity of HD muscle by employing in vitro mononuclear skeletal muscle cell isolation and in vivo acute muscle damage model in R6/2 mice. We found that, similar to R6/2 adult mice, neonatal R6/2 mice also exhibit a significant reduction in myofiber width and morphological changes in gastrocnemius and soleus muscles compared to WT mice. Cardiotoxin (CTX)-induced acute muscle damage in R6/2 and WT mice showed that the Pax7+ satellite cell pool was dampened in R6/2 mice at 4 weeks post-injection, and R6/2 mice exhibited an altered inflammatory profile in response to acute damage. Our results suggest that, in addition to the mutant HTT degenerative effects in mature muscle fibers, expression of mutant HTT in satellite cells might alter developmental and regenerative processes to contribute to the progressive muscle mass loss in HD. Taken together, the results presented here encourage further studies evaluating the underlying mechanisms of satellite cell dysfunction in HD mouse models.

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Partial resistance to malonate-induced striatal cell death in transgenic mouse models of Huntington's disease is dependent on age and CAG repeat length

Journal of Neurochemistry ◽

10.1046/j.1471-4159.2001.00482.x ◽

2001 ◽

Vol 78 (4) ◽

pp. 694-703 ◽

Cited By ~ 42

Author(s):

Oskar Hansson ◽

Roger F. Castilho ◽

Laura Korhonen ◽

Dan Lindholm ◽

Gillian P. Bates ◽

...

Keyword(s):

Cell Death ◽

Huntington's Disease ◽

Huntington’S Disease ◽

Transgenic Mouse ◽

Mouse Models ◽

Partial Resistance ◽

Repeat Length ◽

Cag Repeat ◽

Transgenic Mouse Models

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Striatal Circuit Development and Its Alterations in Huntington’s Disease

10.20944/preprints202005.0488.v1 ◽

2020 ◽

Author(s):

Margaux Lebouc ◽

Quentin Richard ◽

Maurice Garret ◽

Jérôme Baufreton

Keyword(s):

Huntington's Disease ◽

Huntington’S Disease ◽

Mouse Models ◽

Neurodegenerative Disorder ◽

Repeat Expansion ◽

Cag Repeat ◽

Rodent Models ◽

Network Development ◽

Cag Repeat Expansion ◽

Circuit Development

Huntington's disease (HD) is an inherited neurodegenerative disorder that usually starts during midlife with progressive alterations of motor and cognitive functions. The disease is caused by a CAG repeat expansion within the huntingtin gene leading to severe striatal neurodegeneration. Recent studies conducted on pre-HD children highlight early striatal developmental alterations starting as soon as 6 years old, the earliest age assessed. These findings, in line with data from mouse models of HD, raise the question of when during development do the first disease-related striatal alterations emerge or whether they contribute to the later appearance of the neurodegenerative features of the disease. In this review we will describe the different stages of striatal network development and then discuss recent evidence for its alterations in rodent models of the disease. We argue that a better understanding of the striatum’s development should help in assessing aberrant neurodevelopmental processes linked to the HD mutation.

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Lack of RAN-mediated toxicity in Huntington’s disease knock-in mice

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1919197117 ◽

2020 ◽

Vol 117 (8) ◽

pp. 4411-4417 ◽

Cited By ~ 1

Author(s):

Su Yang ◽

Huiming Yang ◽

Luoxiu Huang ◽

Luxiao Chen ◽

Zhaohui Qin ◽

...

Keyword(s):

Huntington's Disease ◽

Huntington’S Disease ◽

Genome Editing ◽

Mouse Models ◽

Cag Repeat ◽

Cag Repeats ◽

Behavioral Phenotypes ◽

Endogenous Level ◽

Ran Translation

Identification of repeat-associated non-AUG (RAN) translation in trinucleotide (CAG) repeat diseases has led to the emerging concept that CAG repeat diseases are caused by nonpolyglutamine products. Nonetheless, the in vivo contribution of RAN translation to the pathogenesis of CAG repeat diseases remains elusive. Via CRISPR/Cas9-mediated genome editing, we established knock-in mouse models that harbor expanded CAG repeats in the mouse huntingtin gene to express RAN-translated products with or without polyglutamine peptides. We found that RAN translation is not detected in the knock-in mouse models when expanded CAG repeats are expressed at the endogenous level. Consistently, the expanded CAG repeats that cannot be translated into polyglutamine repeats do not yield the neuropathological and behavioral phenotypes that were found in knock-in mice expressing expanded polyglutamine repeats. Our findings suggest that RAN-translated products do not play a major role in the pathogenesis of CAG repeat diseases and underscore the importance in targeting polyglutamine repeats for therapeutics.

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Repeat expansion and autosomal dominant neurodegenerative disorders: consensus and controversy

Expert Reviews in Molecular Medicine ◽

10.1017/s1462399403006598 ◽

2003 ◽

Vol 5 (21) ◽

pp. 1-24 ◽

Cited By ~ 7

Author(s):

Dobrila D. Rudnicki ◽

Russell L. Margolis

Keyword(s):

Calcium Channel ◽

Huntington's Disease ◽

Huntington’S Disease ◽

Neurodegenerative Disorders ◽

Autosomal Dominant ◽

Muscular Atrophy ◽

Early Stage ◽

Repeat Expansion ◽

Cag Repeat ◽

Cag Repeat Expansion

Repeat-expansion mutations cause 13 autosomal dominant neurodegenerative disorders falling into three groups. Huntington's disease (HD), dentatorubral pallidoluysian atrophy (DRPLA), spinal and bulbar muscular atrophy (SBMA), and spinocerebellar ataxias (SCAs) types 1, 2, 3, 7 and 17 are each caused by a CAG repeat expansion that encodes polyglutamine. Convergent lines of evidence demonstrate that neurodegeneration in these diseases is a consequence of the neurotoxic effects of abnormally long stretches of glutamines. How polyglutamine induces neurodegeneration, and why neurodegeneration occurs in only select neuronal populations, remains a matter of intense investigation. SCA6 is caused by a CAG repeat expansion in CACNA1A, a gene that encodes a subunit of the P/Q-type calcium channel. The threshold length at which the repeat causes disease is much shorter than in the other polyglutamine diseases, and neurodegeneration may arise from expansion-induced change of function in the calcium channel. Huntington's disease-like 2 (HDL2) and SCAs 8, 10 and 12 are rare disorders in which the repeats (CAG, CTG or ATTCT) are not in protein-coding regions. Investigation into these diseases is still at an early stage, but it is now reasonable to hypothesise that the net effect of each expansion is to alter gene expression. The different pathogenic mechanisms in these three groups of diseases have important implications for the development of rational therapeutics.

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Molecular Mechanisms of Polyglutamine Pathology and Lessons Learned from Huntington’s Disease

Neurodegenerative Diseases - Molecular Mechanisms and Current Therapeutic Approaches ◽

10.5772/intechopen.93508 ◽

2021 ◽

Author(s):

Nagehan Ersoy Tunalı

Keyword(s):

Huntington's Disease ◽

Huntington’S Disease ◽

Molecular Mechanisms ◽

Lessons Learned ◽

Trinucleotide Repeats ◽

Cag Repeat ◽

Cag Repeats ◽

Disease Genes ◽

Polyq Diseases ◽

Dynamic Mutations

Identification of polymorphic repeating units on DNA as a cause of many neurological disorders has introduced a new concept in molecular biology: Dynamic mutations. Many of the identified dynamic mutations involve expansion of trinucleotide repeats within disease genes. Nine neurodegenerative disorders are currently known to be caused by expanding CAG trinucleotide repeats. These are Huntington’s Disease (HD), Dentato-Rubral Pallidoluysian Atrophy (DRPLA), Spinal and Bulbar Muscular Atrophy (SBMA), and Spinocerebellar Ataxia (SCA) Type 1, 2, 3, 6, 7 and 17. All are inherited in an autosomal dominant fashion except for SBMA, which is X-linked recessive. In all polyQ diseases, the disease mutation involves an increase in the number of CAG repeats within the coding regions of the respective genes. Since CAG triplets encode glutamine in the proteins, diseases caused by CAG repeat expansions are known as “Polyglutamine (polyQ) Diseases”. PolyQ diseases share certain clinical, neuropathological and molecular findings. The most widely studied polyQ disease is HD. In HD and other polyQ diseases, conformational change in the mutant protein causes abnormal folding and proteolysis of the protein, leading to the formation of a toxic polyQ fragment, which aggregates and causes neuronal dysfunction and selective neuronal death in the brain.

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Modifiers of Somatic Repeat Instability in Mouse Models of Friedreich Ataxia and the Fragile X-Related Disorders: Implications for the Mechanism of Somatic Expansion in Huntington’s Disease

Journal of Huntington s Disease ◽

10.3233/jhd-200423 ◽

2021 ◽

Vol 10 (1) ◽

pp. 149-163

Author(s):

Xiaonan Zhao ◽

Daman Kumari ◽

Carson J. Miller ◽

Geum-Yi Kim ◽

Bruce Hayward ◽

...

Keyword(s):

Huntington's Disease ◽

Huntington’S Disease ◽

Mouse Models ◽

Fragile X ◽

Friedreich Ataxia ◽

Disease Onset ◽

Neuronal Cell ◽

Repeat Expansion ◽

Cag Repeat ◽

Dna Repeats

Huntington’s disease (HD) is one of a large group of human disorders that are caused by expanded DNA repeats. These repeat expansion disorders can have repeat units of different size and sequence that can be located in any part of the gene and, while the pathological consequences of the expansion can differ widely, there is evidence to suggest that the underlying mutational mechanism may be similar. In the case of HD, the expanded repeat unit is a CAG trinucleotide located in exon 1 of the huntingtin (HTT) gene, resulting in an expanded polyglutamine tract in the huntingtin protein. Expansion results in neuronal cell death, particularly in the striatum. Emerging evidence suggests that somatic CAG expansion, specifically expansion occurring in the brain during the lifetime of an individual, contributes to an earlier disease onset and increased severity. In this review we will discuss mouse models of two non-CAG repeat expansion diseases, specifically the Fragile X-related disorders (FXDs) and Friedreich ataxia (FRDA). We will compare and contrast these models with mouse and patient-derived cell models of various other repeat expansion disorders and the relevance of these findings for somatic expansion in HD. We will also describe additional genetic factors and pathways that modify somatic expansion in the FXD mouse model for which no comparable data yet exists in HD mice or humans. These additional factors expand the potential druggable space for diseases like HD where somatic expansion is a significant contributor to disease impact.

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