Litcius/Paper detail

Analysis of mutant and total huntingtin expression in Huntington’s disease murine models

Valentina Fodale, Roberta Pintauro, Manuel Daldin, Roberta Altobelli, Maria Carolina Spiezia, Monica Bisbocci, Douglas Macdonald, Alberto Bresciani

2020Scientific Reports30 citationsDOIOpen Access PDF

Abstract

Huntington's disease (HD) is a monogenetic neurodegenerative disorder that is caused by the expansion of a polyglutamine region within the huntingtin (HTT) protein, but there is still an incomplete understanding of the molecular mechanisms that drive pathology. Expression of the mutant form of HTT is a key aspect of diseased tissues, and the most promising therapeutic approaches aim to lower expanded HTT levels. Consequently, the investigation of HTT expression in time and in multiple tissues, with assays that accurately quantify expanded and non-expanded HTT, are required to delineate HTT homeostasis and to best design and interpret pharmacodynamic readouts for HTT lowering therapeutics. Here we evaluate mutant polyglutamine-expanded (mHTT) and polyglutamine-independent HTT specific immunoassays for validation in human HD and control fibroblasts and use to elucidate the CSF/brain and peripheral tissue expression of HTT in preclinical HD models.

Topics & Concepts

HuntingtinHuntington's diseaseHuntingtin ProteinMutantBiologyTrinucleotide repeat expansionPhenotypeNeuroscienceCell biologyDiseaseMedicineGeneticsPathologyGeneAlleleGenetic Neurodegenerative DiseasesMuscle Physiology and DisordersMitochondrial Function and Pathology