| Literature DB >> 33966305 |
Rachel S Fisher1, Rosa Meyo Jimenez1, Elizabeth Soto1, Darin Kalev1, Shana Elbaum-Garfinkle1,2.
Abstract
Huntington's disease is caused by a polyglutamine (polyQ) expansion in the huntingtin protein which results in its abnormal aggregation in the nervous system. Huntingtin aggregates are linked to toxicity and neuronal dysfunction, but a comprehensive understanding of the aggregation mechanism in vivo remains elusive. Here, we examine the morphology of polyQ aggregates in Caenorhabditis elegans mechanosensory neurons as a function of age using confocal and fluorescence lifetime imaging microscopy. We find that aggregates in young worms are mostly spherical with homogenous intensity, but as the worm ages aggregates become substantially more heterogeneous. Most prominently, in older worms we observe an apparent core/shell morphology of polyQ assemblies with decreased intensity in the center. The fluorescence lifetime of polyQ is uniform across the aggregate indicating that the dimmed intensity in the assembly center is most likely not due to quenching or changes in local environment, but rather to displacement of fluorescent polyQ from the central region. This apparent core/shell architecture of polyQ aggregates in aging C. elegans neurons contributes to the diverse landscape of polyQ aggregation states implicated in Huntington's disease.Entities:
Keywords: Caenorhabditis elegans; FLIM; Huntington's disease; Neurodegeneration; aggregate morphology; neural aging; protein aggregation; protein misfolding
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Year: 2021 PMID: 33966305 PMCID: PMC8197433 DOI: 10.1002/pro.4105
Source DB: PubMed Journal: Protein Sci ISSN: 0961-8368 Impact factor: 6.993