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Machado-Joseph disease, also known as spinocerebellar ataxia-3, is an autosomal dominant neurologic disorder. Additionally we are shipping Ataxin 3 Antibodies (68) and Ataxin 3 Proteins (14) and many more products for this protein.
The findings reveal ATXN3 to be a novel deubiquitinase of Chk1 (show CHEK1 ELISA Kits), providing a new mechanism of Chk1 (show CHEK1 ELISA Kits) stabilization in genome integrity maintenance.
Segregation patterns and factors influencing instability of expanded ATXN3 CAG transmissions in Machado-Joseph disease have been analyzed.
Our data reveal a previously unrecognized balance between pathogenic and potentially therapeutic properties of the ataxin-3-Rad23 interaction; they highlight this interaction as critical for the toxicity of the SCA3 protein, and emphasize the importance of considering protein context when pursuing suppressive avenues.
the opposing activities of RNF4 (show RNF4 ELISA Kits) and ataxin-3 consolidate robust MDC1 (show MDC1 ELISA Kits)-dependent signaling and repair ofDNA double-strand break.
we demonstrated that neural differentiation in these iPS (show SLC27A4 ELISA Kits) cells was accompanied by autophagy and that rapamycin promoted autophagy through degradation of mutant ATXN3 proteins in neurally differentiated spinocerebellar ataxia-3 (show SCN8A ELISA Kits) human induced pluripotent stem cells (p < 0.05). In conclusion, patient-derived iPS (show SLC27A4 ELISA Kits) cells are a good model for studying the mechanisms of SCA3 and may provide a tool for drug discovery in vitro.
South American cohort did not confirm the effect of the four candidate loci as modifier of onset age: mithocondrial A10398G polymorphism and CAGn at RAI1 (show DOM3Z ELISA Kits), CACNA1A (show CACNA1A ELISA Kits), ATXN3, and ATXN7 (show ATXN7 ELISA Kits) genes
Ataxin-3 phosphorylation decreases neuronal defects in spinocerebellar ataxia type 3 models.
USP19_b up-regulates the protein levels of the polyglutamine (polyQ)-containing proteins, ataxin-3 (Atx3) and huntingtin (Htt (show HTT ELISA Kits)), and thus promotes aggregation of their polyQ-expanded species in cell models
Based on these data and other related studies, we presumed that de novo mutations of ATXN3 emerging from large ANs are at least one survival mechanisms of mutational ATXN3 and we can redefine the range of CAG repeats as: ANs=44, 45 =AIs (show AR ELISA Kits) =49 and AEs (show AES ELISA Kits)>/=50
Results suggest that the aggregation of Josephin proceeds from the monomer state to the formation of spheroidal intermediates with a native structure. Only successively, these intermediates evolve into misfolded aggregates and into the final fibrils.
findings identify a novel molecular link between ATX-3 and p53 (show TP53 ELISA Kits)-mediated cell death and provide an explanation for the direct involvement of p53 (show TP53 ELISA Kits) in SCA3 disease pathogenesis
We show that chronic VPA treatment did not modify the ATXN3 inclusion load and astrogliosis in affected brain regions However, VPA chronic treatment was able to increase GRP78 (show HSPA5 ELISA Kits) protein levels at 30 weeks of age, one of its known neuroprotective effects
work suggests that in Machado-Joseph disease, mutant ataxin-3 drives an abnormal reduction of ataxin-2 (show ATXN2 ELISA Kits) levels, which overactivates poly(A)-binding protein, increases translation of mutant ataxin-3 and other proteins and aggravates Machado-Joseph disease.
SCA3 knockin mice exhibit robust Atxn3 accumulation both in regions known to be affected in human disease; also display altered splicing of the mutant Atxn3 transcript that results in the formation of a previously described alternative ATXN3 transcript
Data support the importance of ATXN3 in neuronal cells and indicate that an expanded polyQ tract leads to a partial loss of the cellular function of ATXN3 that may be relevant to neurodegeneration.
While ataxin-3 may participate in protein quality control pathways, it does not critically regulate the handling of mutant htt (show HTT ELISA Kits) or contribute to major features of disease pathogenesis in Huntington disease (show HTT ELISA Kits).
Results suggest that postnatal nuclear accumulation of mutant ataxin-3 disrupts dendritic differentiation and mGluR-signaling in mouse model spinocerebellar ataxia type 3 Purkinje cells
Lentiviral-based expression of mutant atxn-3 in the mouse cerebellum induces localized neuropathology sufficient to generate a behavioral ataxic phenotype.
Cerebellar soluble mutant ataxin-3 level decreases during disease progression in Spinocerebellar Ataxia Type 3 mice.
the efficacy of gene silencing in blocking the MJD-associated motor-behavior and neuropathological abnormalities
Machado-Joseph disease, also known as spinocerebellar ataxia-3, is an autosomal dominant neurologic disorder. The protein encoded by this gene contains (CAG)n repeats in the coding region, and the expansion of these repeats from the normal 13-36 to 68-79 is one cause of Machado-Joseph disease. There is a negative correlation between the age of onset and CAG repeat numbers. Alternatively spliced transcript variants encoding different isoforms have been described for this gene.
, ataxin 3
, Machado-Joseph disease (spinocerebellar ataxia 3, olivopontocerebellar ataxia 3, autosomal dominant, ataxin 3)
, Machado-Joseph disease protein 1
, ataxin 3 variant h
, ataxin 3 variant m
, ataxin 3 variant ref
, olivopontocerebellar ataxia 3
, spinocerebellar ataxia type 3 protein
, Machado-Joseph disease (spinocerebellar ataxia 3, olivopontocerebellar ataxia 3, autosomal dominant, ataxin 3) homolog
, machado-Joseph disease protein 1 homolog