Your search keyword '"Breningstall G"' showing total 8 results

1. In vivo analysis of cerebellar Purkinje cell activity in SCA2 transgenic mouse model.

Author

Egorova, Polina A., Zakharova, Olga A., Vlasova, Olga L., and Bezprozvanny, Ilya B.

Subjects

PURKINJE cells, SPINOCEREBELLAR ataxia, ELECTROPHYSIOLOGY, NEURODEGENERATION, POLYGLUTAMINE, TRANSGENIC mice, LABORATORY mice

Abstract

Cerebellar Purkinje cells (PCs) are primarily affected in many spinocerebellar ataxias (SCA). In this study we investigated functional activity of PCs in transgenic mouse model of SCA2, a polyglutamine neurodegenerative hereditary disorder. In our studies we used extracellular single-unit recording method to compare spontaneous activity of PCs in agematched wild-type mice and SCA2-58Q transgenic mice. We discovered that the fraction of PCs with bursting and an irregular pattern of spontaneous activity dramatically increases in aged SCA2-58Q mice compared with wild-type littermates. Small-conductance calciumactivated potassium (SK) channels play an important role in determining firing rate of PCs. Indeed, we demonstrated that intraperitoneal (IP) injection of SK channel inhibitor NS8593 induces an irregular pattern of PC activity in wild-type mice. Furthermore, we demonstrated that IP injection of SK channel-positive modulator chlorzoxazone (CHZ) decreases spontaneous firing rate of cerebellar PCs. Finally, we have shown that IP injections with CHZ normalize firing activity of cerebellar PCs from aging SCA2-58Q mice. We propose that alterations in PC firing patterns is one of potential causes of ataxic symptoms in SCA2 and in other SCAs and that positive modulators of SK channels can be used to normalize activity of PCs and alleviate ataxic phenotype in patients with SCA. [ABSTRACT FROM AUTHOR]

Published

2016

2. Spinocerebellar ataxia 2 (SCA2).

Author

Lastres-Becker, Isabel, Rüb, Udo, and Auburger, Georg

Subjects

FRIEDREICH'S ataxia, NEURODEGENERATION, ATAXIA, MUSCULAR atrophy, SYMPTOMS, GENETICS, THERAPEUTICS

Abstract

Spinocerebellar ataxia type 2 (SCA2) is an autosomal dominantly inherited, neurodegenerative disease. It can manifest either with a cerebellar syndrome or as Parkinson’s syndrome, while later stages involve mainly brainstem, spinal cord and thalamus. This particular atrophy pattern resembles sporadic multi-system-atrophy (MSA) and results in some clinical features indicative of SCA2, such as early saccade slowing, early hyporeflexia, severe tremor of postural or action type, and early myoclonus. For treatment, levodopa is temporarily useful for rigidity/bradykinesia and for tremor, magnesium for muscle cramps, but neuroprotective therapy will depend on the elucidation of pathogenesis. The disease cause lies in the polyglutamine domain of the protein ataxin-2, which can expand in families over successive generations resulting in earlier onset age and faster progression. Genetic testing in SCA2 and other polyglutamine disorders like the well-studied Huntington’s disease is now readily available for family planning. Although these disorders differ clinically and in the affected neuron populations, it is not understood how the different polyglutamine proteins mediate such tissue specificity. The neuronal intranuclear inclusion bodies described in other polyglutamine disorders are not frequent in SCA2. For the quite ubiquitously expressed ataxin-2, a subcellular localization at the Golgi, the endoplasmic reticulum and the plasma membrane, in interaction with proteins of mRNA translation and of endocytosis have been observed. As a first victim of SCA2 degeneration, cerebellar Purkinje neurons may be preferentially susceptible to alterations of these subcellular pathways, and therefore our review aims to portray the particular profile of the SCA2 disease process and correlate it to the specific features of ataxin-2. [ABSTRACT FROM AUTHOR]

Published

2008

3. Huntington's disease. Part 2: treatment and management issues in juvenile HD.

Author

Aubeeluck, Aimee and Brewer, Helen

Subjects

HUNTINGTON disease, THERAPEUTICS, NEURODEGENERATION, NURSING, NEUROSCIENCES

Abstract

Juvenile Huntington's disease (JHD) is a rare condition, with only about 5-10% of Huntington's disease cases occurring in individuals under the age of 20 years. Symptoms of JHD include, for example, rigidity, stiffness, awkawrdness in walking, and speech difficulty. JHD is caused by an inherited gene mutation that is localized to the short arm of chromosome 4. There is no cure for the condition, and it is currently managed through symptomatic treatment and supportive care. Being an inherited condition, those involved in the care of a child with JHD need to be aware of the impact that the disorder have on the whole family. [ABSTRACT FROM AUTHOR]

Published

2008

4. Huntington Disease in a 9-Year-Old Boy: Clinical Course and Neuropathologic Examination.

Author

Wojaczyńska-Stanek, Katarzyna, Adamek, Dariusz, Marszal, Elżbieta, and Hoffman-Zacharska, Dorota

Subjects

HUNTINGTON disease, JUVENILE diseases, GENETIC disorders, NEURODEGENERATION, PARKINSON'S disease, MYOCLONUS, GENETIC counseling, DIAGNOSIS, CLINICAL medicine

Abstract

Huntington disease is a dominantly inherited, neurodegenerative disorder, usually with onset in the fourth to fifth decade of life but in a small proportion of patients before the age of 20 years. The early-onset form, juvenile Huntington disease, is clinically different from that of more common adult-onset forms and includes cognitive decline, parkinsonism, myoclonus, and seizures. We report a case of a boy with juvenile Huntington disease with a very early age at disease onset (3 years). The suspected clinical diagnosis was confirmed by DNA analysis, which revealed (CAG)n expansion into the range characteristic of juvenile Huntington disease (95 repeats). The clinical course of the disease was typical for the juvenile form of Huntington disease, but the diagnosis was not so obvious because there was no history of any neurodegenerative disorder in the family. The child died at the age of 11 years. The detailed neuropathologic investigations performed postmortem showed the characteristic features of Huntington disease. As the patient's de novo mutation was very unlikely to occur, genetic counseling and the possibility of predictive testing were proposed to the family. Indirect molecular data indicate the familial character of the disease, with strong anticipation of transmission. [ABSTRACT FROM AUTHOR]

Published

2006

5. A new model for prediction of the age of onset and penetrance for Huntington's disease based on CAG length.

Author

Langbehn, D.R., Brinkman, R.R., Falush, D., Paulsen, J.S., and Hayden, M.R.

Subjects

HUNTINGTON disease, NEURODEGENERATION, CONFIDENCE intervals, DISEASE risk factors, PATIENTS, PROBABILITY theory

Abstract

Langbehn DR, Brinkman RR, Falush D, Paulsen JS, Hayden MR on behalf of an International Huntington's Disease Collaborative Group. A new model for prediction of the age of onset and penetrance for Huntington's disease based on CAG length. Huntington's disease (HD) is a neurodegenerative disorder caused by an unstable CAG repeat. For patients at risk, participating in predictive testing and learning of having CAG expansion, a major unanswered question shifts from “Will I get HD?” to “When will it manifest?” Using the largest cohort of HD patients analyzed to date (2913 individuals from 40 centers worldwide), we developed a parametric survival model based on CAG repeat length to predict the probability of neurological disease onset (based on motor neurological symptoms rather than psychiatric onset) at different ages for individual patients. We provide estimated probabilities of onset associated with CAG repeats between 36 and 56 for individuals of any age with narrow confidence intervals. For example, our model predicts a 91% chance that a 40-year-old individual with 42 repeats will have onset by the age of 65, with a 95% confidence interval from 90 to 93%. This model also defines the variability in HD onset that is not attributable to CAG length and provides information concerning CAG-related penetrance rates. [ABSTRACT FROM AUTHOR]

Published

2004

6. Unusual Early-Onset Hungtington's Disease.

Author

Vargas, Antonio P., Carod-Artal, Francisco J., Bomfim, Denise, Vázquez-Cabrera, Carolina, and Dantas-Barbosa, Carmela

Subjects

HUNTINGTON disease, JUVENILE diseases, NEURODEGENERATION, BEHAVIOR disorders in children

Abstract

Huntington's disease is an autosomal dominant progressive neurodegenerative disorder characterized by involuntary movements, cognitive decline, and behavioral disorders leading to functional disability. In contrast to patients with adult onset, in which chorea is the major motor abnormality, children often present with spasticity, rigidity, and significant intellectual decline associated with a more rapidly progressive course. An unusual early-onset Huntington's disease case of an 11-year-old boy with severe hypokinetic/rigid syndrome appearing at the age of 2.5 years is presented in the article. Clinical diagnosis was confirmed by polymerase chain reaction study of the expanded IT-15 allele with a compatible size of 102 cytosine-adenosine-guanosine repeats. L-Dopa mildly ameliorated rigidity, bradykinesia, and dystonia. The authors conclude that Huntington's disease should be included in the differential diagnoses of regressive syndromes of early childhood. [ABSTRACT FROM AUTHOR]

Published

2003

7. Juvenile onset Huntington's disease—clinical and research perspectives.

Author

Nance, Martha A. and Myers, Richard H.

Subjects

HUNTINGTON disease, GENETIC disorders, NEURODEGENERATION, TRINUCLEOTIDE repeats, ETIOLOGY of diseases, HEREDITY

Abstract

Huntington's disease (HD) is an inherited neurodegenerative disorder. The mutation which causes the disease is an expansion in the number of repetitions of three nucleotides, C, A, and G in exon 1 of the huntingtin gene. The gene normally has 15 to 30 repeats and an expansion to 40 or more is associated with HD. HD usually has a mid-life onset, but a juvenile form, defined by onset of symptoms before the age of 21 years, is present in about 7% of HD cases. Juvenile HD is characterized by (1) transmission from an HD affected father, (2) an unusually large repeat size, usually of 60 or more units, and (3) unique clinical features, including rigidity and seizure disorder. Although juvenile onset is associated with a more severe neuropathological involvement, the neuropathological characteristics of juvenile HD are similar to those seen in the adult form in that the striatum bears the brunt of the illness. Clumps of protein, termed inclusion bodies, which stain positive for huntingtin and ubiquitin, are found primarily in the nucleus but also in the cytoplasm and axons in HD neurons. Research suggests that these inclusion bodies sequester a deleterious protein fragment and prolong cell life during the degenerative process of the disease. MRDD Research Reviews 2001;7:153–157. © 2001 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2001

8. Molecular genetics: unmasking polyglutamine triggers in neurodegenerative disease.

Author

Gusella, James F., MacDonald, Marcy E., Gusella, J F, and MacDonald, M E

Subjects

GENETIC mutation, NEURODEGENERATION, MEDICAL genetics, HUNTINGTON disease, PATHOLOGY, DRUG development

Abstract

Two decades ago, molecular genetic analysis provided a new approach for defining the roots of inherited disorders. This strategy has proved particularly powerful because, with only a description of the inheritance pattern, it can uncover previously unsuspected mechanisms of pathogenesis that are not implicated by known biological pathways or by the disease manifestations. Nowhere has the impact of molecular genetics been more evident than in the dominantly inherited neurodegenerative disorders, where eight unrelated diseases have been revealed to possess the same type of mutation--an expanded polyglutamine encoding sequence--affecting different genes. [ABSTRACT FROM AUTHOR]

Published

2000