2017
DOI: 10.1016/j.neuroscience.2017.08.026
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Tau 45-230 association with the cytoskeleton and membrane-bound organelles: Functional implications in neurodegeneration

Abstract: The dysregulation of posttranslational modifications of the microtubule-associated protein (MAP) tau plays a key role in Alzheimer’s disease (AD) and related disorders. Thus, we have previously shown that beta amyloid (Aβ)-induced neurotoxicity was mediated, at least in part, by tau cleavage into the tau45-230 fragment. However, the mechanisms underlying the toxicity of tau45-230 remain unknown. To get insights into such mechanisms, we first determined the subcellular localization of this tau fragment in hippo… Show more

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Cited by 17 publications
(8 citation statements)
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“…Toxic tau species can interfere with microtubule stability, thus affecting the transport and distribution of organelles and signaling proteins (enzymes, receptors) in cell compartments [118]. An intracellular accumulation of tau was often accompanied by an increase in transport time and the instantaneous velocity of the vesicular cargos [119].…”
Section: Negative Impact Of Tau Oligomers On Microtubule Assembly Nementioning
confidence: 99%
“…Toxic tau species can interfere with microtubule stability, thus affecting the transport and distribution of organelles and signaling proteins (enzymes, receptors) in cell compartments [118]. An intracellular accumulation of tau was often accompanied by an increase in transport time and the instantaneous velocity of the vesicular cargos [119].…”
Section: Negative Impact Of Tau Oligomers On Microtubule Assembly Nementioning
confidence: 99%
“…Tau proteolytic fragments have not been studied to precipitate in up-regulated concentrations from 3R- or 4R-isoforms, and it is unclear whether 3R- or 4R-isoforms more toxic fragments. Reference numbers in parentheses refer to cited articles as follows: (1) Zhang et al (2014) ; (2) Matsumoto et al (2015) ; (3) Ozcelik et al (2016) ; (4) Horowitz et al (2004) ; (5) Horowitz et al (2004) ; (6) Gamblin et al (2003) ; (7) Quintanilla et al (2009) ; (8) Foveau et al (2016) ; (9) Guo et al (2004) ; (10) Zhao et al (2016) ; (11) Amadoro et al (2006) ; (12) Amadoro et al (2012) ; (13) Lang et al (2014) ; (14) Afreen et al (2017) ; (15) Park and Ferreira (2005) ; (16) Garg et al (2010) ; (17) Matthews-Roberson et al (2008) ; (18) Yang and Ksiezak-Reding (1995) ; (19) Arai et al (2005) ; (20) Corsetti et al (2008) ; and (21) Florenzano et al (2017) .…”
Section: Proteases Known To Generate Toxic Tau Fragmentsmentioning
confidence: 99%
“…Alongside the cellular phenotypes, behavioural abnormalities were noted with significantly increased freezing response in the fear conditioning test [ 35 ]. Tau 45 - 230 was also shown to impair both anterograde and retrograde organelle transport, which could help to explain how it exerts its neurotoxic effects [ 36 ]. Which calpain cleaves at R230-T231 in vivo is still unclear, since both calpain-1 and –2 [ 34 ] have been shown to cleave this peptide bond in vitro .…”
Section: Tau Proteasesmentioning
confidence: 99%