Implicating Calpain in Tau-Mediated Toxicity In Vivo

Reinecke, James B.; DeVos, Sarah L.; McGrath, James P.; Shepard, Amanda M.; Goncharoff, Dustin K.; Tait, Don N; Fleming, Samantha; Vincent, Michael; Steinhilb, Michelle Leigh

doi:10.1371/journal.pone.0023865

Cited by 47 publications

(50 citation statements)

References 64 publications

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“…Recently, an additional N-terminal fragment (residues 1-224) was identified in CSF from patients with AD and PSP, and has been hypothesized to be an early marker of disease and particularly pathogenic [35,36]. A similar calpain-cleaved fragment was reported by other groups [37,38].…”

Section: Tau Speciesmentioning

confidence: 71%

Tau immunotherapy for Alzheimer's disease

Pedersen¹,

Sigurdsson²

2015

Trends in Molecular Medicine

233

179

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Section: Tau Speciesmentioning

confidence: 71%

Tau immunotherapy for Alzheimer's disease

Pedersen¹,

Sigurdsson²

2015

Trends in Molecular Medicine

233

179

View full text Add to dashboard Cite

“…In the projection domain, methylation sites K24 and K44 lie adjacent to putative caspase and calpain cleavage sites, respectively. The latter cleavage event is reportedly associated with toxicity in biological models [44, 58– 60]. In the MTBR, where the majority of Lys methylation was found, sites overlapped with three of five reported ubiquitylation sites on AD-derived filamentous tau.…”

Section: Discussionmentioning

confidence: 95%

Lysine methylation is an endogenous post-translational modification of tau protein in human brain and a modulator of aggregation propensity

Funk

Thomas

Schafer

et al. 2014

Biochemical Journal

110

127

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In Alzheimer disease, the microtubule-associated protein tau dissociates from the neuronal cytoskeleton and aggregates to form cytoplasmic inclusions. Although hyper-phosphorylation of tau Ser and Thr residues is an established trigger of tau misfunction and aggregation, tau modifications extend to Lys residues as well, raising the possibility that different modification signatures depress or promote aggregation propensity depending on site occupancy. To identify Lys-residue modifications associated with normal tau function, soluble tau proteins isolated from four cognitively normal human brains were characterized by mass spectrometry methods. The major detectable Lys modification was found to be methylation, which appeared in the form of mono- and di-methyl Lys residues distributed among at least eleven sites. Unlike tau phosphorylation sites, the frequency of Lys methylation was highest in the microtubule binding repeat region that mediates both microtubule binding and homotypic interactions. When purified recombinant human tau was modified in vitro through reductive methylation, its ability to promote tubulin polymerization was retained, whereas its aggregation propensity was greatly attenuated at both nucleation and extension steps. These data establish Lys methylation as part of the normal tau post-translational modification signature in human brain, and suggest that it can function in part to protect against pathological tau aggregation.

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“…Although the role of tau in regulating microtubule dynamics is extensively established, much less is known about the functional role of the N-terminal domain of tau on neuron survival. A 17-kD N-terminal tau fragment generated by calpain cleavage, comprising residues amino acid 45-230, was proposed to mediate Ab-induced toxicity (Park and Ferreira 2005), and mediate tau neurotoxicity in Drosophila tauopathy model (Reinecke et al 2011). However, the toxicity and in vivo relevance of this 17 kD fragment are debated.…”

Section: Introductionmentioning

confidence: 99%

Passive immunization targeting the N-terminal projection domain of tau decreases tau pathology and improves cognition in a transgenic mouse model of Alzheimer disease and tauopathies

et al. 2014

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Intraneuronal accumulation of abnormally hyperphosphorylated tau in the brain is a histopathological hallmark of Alzheimer's disease and a family of related neurodegenerative disorders collectively called tauopathies. At present there is no effective treatment available for these progressive neurodegenerative diseases which are clinically characterized by dementia in mid to old-age. Here we report the treatment of 14-17-months-old 3xTg-AD mice with tau antibodies 43D (tau 6-18) and 77E9 (tau 184-195) to the N-terminal projection domain of tau or mouse IgG as a control by intraperitoneal injection once a week for 4 weeks, and the effects of the passive immunization on reduction of hyperphosphorylated tau, Aβ accumulation and cognitive performance in these animals. We found that treatment with tau antibodies 43D and 77E9 reduced total tau level, decreased tau hyperphosphorylated at Ser199, Ser202/Thr205 (AT8), Thr205, Ser262/356 (12E8), and Ser396/404 (PHF-1) sites, and a trend to reduce Aβ pathology. Most importantly, targeting N-terminal tau especially by 43D (tau 6-18) improved reference memory in the Morris water maze task in 3xTg-AD mice. We did not observe any abnormality in general physical characteristics of the treated animals with either of the two antibodies during the course of this study. Taken together, our studies demonstrate for the first time (1) that passive immunization targeting normal tau can effectively clear the hyperphosphorylated protein and possibly reduce Aβ pathology from the brain and (2) that targeting N-terminal projection domain of tau containing amino acid 6-18 is especially beneficial. Thus, targeting selective epitopes of N-terminal domain of tau may present a novel effective therapeutic opportunity for Alzheimer disease and other tauopathies.

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Implicating Calpain in Tau-Mediated Toxicity In Vivo

Cited by 47 publications

References 64 publications

Tau immunotherapy for Alzheimer's disease

Tau immunotherapy for Alzheimer's disease

Lysine methylation is an endogenous post-translational modification of tau protein in human brain and a modulator of aggregation propensity

Passive immunization targeting the N-terminal projection domain of tau decreases tau pathology and improves cognition in a transgenic mouse model of Alzheimer disease and tauopathies

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