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1: Mol Cell Neurosci. 2008 Mar;37(3):559-67. Epub 2007 Dec 15.Click here to read Links

Tau kinase inhibitors protect hippocampal synapses despite of insoluble tau accumulation.

KeyNeurotek Pharmaceuticals AG, ZENIT-Technologie Park, Leipziger Strasse 44, D-39120 Magdeburg, Germany. ina.hinners@keyneurotek.de

A better understanding of the cellular and molecular pathomechanisms of Alzheimer's disease (AD) is a prerequisite for the development of efficient treatments. We have used a novel assay system based on virus-transduced organotypic hippocampal slice cultures that mimics important aspects of tau-driven AD pathology in a short time frame. Human tau P301L, when expressed in pyramidal neurons of hippocampal slice cultures, was increasingly phosphorylated at several disease-relevant epitopes, leading to progressive neuronal dystrophy and formation of RIPA-insoluble tau. AD-like tau hyperphosphorylation was reduced by the tau kinase inhibitors lithium and SRN-003-556, but RIPA-insoluble tau remained unaffected after treatment with any of these substances. Only SRN-003-556 was able to protect hippocampal neurons from synaptic damage that was presumably caused by a toxic soluble tau fraction. These data provide first mechanistic insights towards the functional benefits of SRN-003-556 that have been observed in vivo.

PMID: 18201898 [PubMed - indexed for MEDLINE]

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