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Motor and cognitive deficits in aged tau knockout mice in two background strains.

Molecular neurodegeneration (2014-08-16)
Peng Lei, Scott Ayton, Steve Moon, Qihao Zhang, Irene Volitakis, David I Finkelstein, Ashley I Bush
ZUSAMMENFASSUNG

We recently reported that Parkinsonian and dementia phenotypes emerge between 7-12 months of age in tau-/- mice on a Bl6/129sv mixed background. These observations were partially replicated by another group using pure Bl6 background tau-/- mice, but notably they did not observe a cognitive phenotype. A third group using Bl6 background tau-/- mice found cognitive impairment at 20-months of age. To reconcile the observations, here we considered the genetic, dietary and environmental variables in both studies, and performed an extended set of behavioral studies on 12-month old tau+/+, tau+/-, and tau-/- mice comparing Bl6/129sv to Bl6 backgrounds. We found that tau-/- in both backgrounds exhibited reduced tyrosine hydroxylase-positive nigral neuron and impaired motor function in all assays used, which was ameliorated by oral treatment with L-DOPA, and not confounded by changes in body weight. Tau-/- in the C57BL6/SV129 background exhibited deficits in the Y-maze cognition task, but the mice on the Bl6 background did not. These results validate our previous report on the neurodegenerative phenotypes of aged tau-/- mice, and show that genetic background may impact the extent of cognitive impairment in these mice. Therefore excessive lowering of tau should be avoided in therapeutic strategies for AD.

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Marke
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Salpetersäure, ACS reagent, 70%
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Salpetersäure, 70%, purified by redistillation, ≥99.999% trace metals basis
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Salpetersäure, puriss. p.a., 65.0-67.0%
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Salpetersäure, red, fuming, HNO3 >90 %
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Salpetersäure, ACS reagent, ≥90.0%
Supelco
Salpetersäure-Konzentrat, 0.1 M HNO3 in water (0.1N), eluent concentrate for IC
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Salpeter-14N-Säurelösung, ~10 N in H2O, 99.99 atom % 14N