| Literature DB >> 26704708 |
YoungDoo Kim1, Hyunwoo Choi1, WonJae Lee1, Hyejin Park1, Tae-In Kam1, Se-Hoon Hong1, Jihoon Nah1, Sunmin Jung1, Bora Shin1, Huikyong Lee1, Tae-Yong Choi2, Hyosun Choo1, Kyung-Keun Kim3, Se-Young Choi2, Rakez Kayed4, Yong-Keun Jung5.
Abstract
In neurodegenerative diseases like AD, tau forms neurofibrillary tangles, composed of tau protein. In the AD brain, activated caspases cleave tau at the 421th Asp, generating a caspase-cleaved form of tau, TauC3. Although TauC3 is known to assemble rapidly into filaments in vitro, a role of TauC3 in vivo remains unclear. Here, we generated a transgenic mouse expressing human TauC3 using a neuron-specific promoter. In this mouse, we found that human TauC3 was expressed in the hippocampus and cortex. Interestingly, TauC3 mice showed drastic learning and spatial memory deficits and reduced synaptic density at a young age (2-3months). Notably, tau oligomers as well as tau aggregates were found in TauC3 mice showing memory deficits. Further, i.p. or i.c.v. injection with methylene blue or Congo red, inhibitors of tau aggregation in vitro, and i.p. injection with rapamycin significantly reduced the amounts of tau oligomers in the hippocampus, rescued spine density, and attenuated memory impairment in TauC3 mice. Together, these results suggest that TauC3 facilitates early memory impairment in transgenic mice accompanied with tau oligomer formation, providing insight into the role of TauC3 in the AD pathogenesis associated with tau oligomers and a useful AD model to test drug candidates.Entities:
Keywords: AD mice; Alzheimer's disease; Caspase-cleaved tau; Tau oligomers; Tauopathy
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Year: 2015 PMID: 26704708 DOI: 10.1016/j.nbd.2015.12.006
Source DB: PubMed Journal: Neurobiol Dis ISSN: 0969-9961 Impact factor: 5.996