| Literature DB >> 27650389 |
Julia E Gerson1,2, Amrit Mudher3, Rakez Kayed1,2.
Abstract
The culmination of many years of increasing research into the toxicity of tau aggregation in neurodegenerative disease has led to the consensus that soluble, oligomeric forms of tau are likely the most toxic entities in disease. While tauopathies overlap in the presence of tau pathology, each disease has a unique combination of symptoms and pathological features; however, most study into tau has grouped tau oligomers and studied them as a homogenous population. Established evidence from the prion field combined with the most recent tau and amyloidogenic protein research suggests that tau is a prion-like protein, capable of seeding the spread of pathology throughout the brain. Thus, it is likely that tau may also form prion-like strains or diverse conformational structures that may differ by disease and underlie some of the differences in symptoms and pathology in neurodegenerative tauopathies. The development of techniques and new technology for the detection of tau oligomeric strains may, therefore, lead to more efficacious diagnostic and treatment strategies for neurodegenerative disease. [Formula: see text].Entities:
Keywords: Tau; aggregation; amyloid; neurodegeneration; oligomer
Mesh:
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Year: 2016 PMID: 27650389 PMCID: PMC5285467 DOI: 10.1080/10409238.2016.1226251
Source DB: PubMed Journal: Crit Rev Biochem Mol Biol ISSN: 1040-9238 Impact factor: 8.250