Literature DB >> 19200347

Role of caspase-3 in tau truncation at D421 is restricted in transgenic mouse models for tauopathies.

Qipeng Zhang1, Xiaoguang Zhang, Jie Chen, Yanying Miao, Anyang Sun.   

Abstract

Truncated tau is widely detected in Alzheimer's disease brain, and caspase-3 has been considered as a major executioner for tau truncation at aspartate421 (D421), according to its capability of cleaving recombinant tau in vitro. Here we investigated the relationship between D421 truncated tau and caspase-3 in two transgenic mouse models for tauopathies. In adult transgenic mice, activated caspase-3 could not be detected in neurons containing truncated tau, with the exception of a few glia-like cells or neurons in postnatal mice. Caspase-3 expression exhibited a dramatic decrease at the early development stage, and kept at constantly low levels during adult stages in both wild type and transgenic mice. On the other hand, co-incubating brain homogenates from adult tau transgenic mice and ethanol-treated postnatal mice promoted tau truncation at D421, which was mildly reduced by caspase inhibitor, but completely suppressed by phosphatase inhibitor, indicating that hyperphosphorylated tau becomes a poor substrate for truncation at D421. Taken together, our study shows that insufficient caspase-3 expression and hyperphosphorylated status of tau in the adult transgenic mouse brain restrict caspase-3 as an efficient enzyme for tau truncation in vivo. Clearly, there is a caspase-3 independent mechanism responsible for tau truncation at D421 in these models.

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Year:  2009        PMID: 19200347     DOI: 10.1111/j.1471-4159.2009.05959.x

Source DB:  PubMed          Journal:  J Neurochem        ISSN: 0022-3042            Impact factor:   5.372


  11 in total

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6.  A synergic role of caspase-6 and caspase-3 in Tau truncation at D421 induced by H2O 2.

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7.  Tau phosphorylation and cleavage in ethanol-induced neurodegeneration in the developing mouse brain.

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Review 10.  The role of tau in neurodegenerative diseases and its potential as a therapeutic target.

Authors:  Michael S Wolfe
Journal:  Scientifica (Cairo)       Date:  2012-12-19
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