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Robert A. Rissman, Wayne W. Poon, Mathew Blurton-Jones, Salvatore Oddo, Reidun Torp, Michael P. Vitek, Frank M. LaFerla, Troy T. Rohn, Carl W. Cotman
Published in Volume 114, Issue 1
J Clin Invest. 2004; 114(1):121–130 doi:10.1172/JCI20640
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Figure 7

ΔTau is present throughout the evolution of NFT pathology. Triple immunofluorescence was used to examine the association of ΔTau (red) with the conformation-sensitive tau antibody MC1 (green) and the tau phosphoepitope antibody PHF-1 (blue) in hippocampal NFT pathology. ΔTau (red) was coincident with MC1 and PHF-1 throughout the evolution of NFT pathology within pretangle neurons (A), diffuse tangle–bearing neurons (B), mature tangle–bearing neurons (C and D), and dystrophic neurites (E and F). Scale bar: 8 μm (A, C, and D), 12 μm (B), 4 μm (E), 10 μm (F).