Presenilin-1 Mutations Reduce Cytoskeletal Association, Deregulate Neurite Growth, and Potentiate Neuronal Dystrophy and Tau Phosphorylation

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The Journal of Neuroscience, February 1, 2001, 21(3):834-842

Presenilin-1 Mutations Reduce Cytoskeletal Association, Deregulate Neurite Growth, and Potentiate Neuronal Dystrophy and Tau Phosphorylation
Gustavo Pigino¹, Alejandra Pelsman¹, Hiroshi Mori², and Jorge Busciglio¹
¹ Department of Neuroscience, University of Connecticut Health Center, Farmington, Connecticut 06030, and ² Department of Neuroscience, Osaka City University Medical School, Osaka 545-8585, Japan
Mutations in presenilin genes are linked to early onset familial Alzheimer's disease (FAD). Previous work in non-neuronalcells indicates that presenilin-1 (PS1) associates with cytoskeletalelements and that it facilitates Notch1 signaling. Because Notch1participates in the control of neurite growth, cultured hippocampalneurons were used to investigate the cytoskeletal associationof PS1 and its potential role during neuronal development. Wefound that PS1 associates with microtubules (MT) and microfilaments(MF) and that its cytoskeletal association increases dramaticallyduring neuronal development. PS1 was detected associated withMT in the central region of neuronal growth cones and with MFin MF-rich areas extending into filopodia and lamellipodia. Indifferentiated neurons, PS1 mutations reduced the interactionof PS1 with cytoskeletal elements, diminished the nuclear translocationof the Notch1 intracellular domain (NICD), and promoted a markedincrease in total neurite length. In developing neurons, PS1 overexpressionincreased the nuclear translocation of NICD and inhibited neuritegrowth, whereas PS1 mutations M146V, I143T, and deletion of exon9 (D9) did not facilitate NICD nuclear translocation and had noeffect on neurite growth. In cultures that were treated with amyloid $beta$ (A $beta$ ), PS1 mutations significantly increased neuritic dystrophyand AD-like changes in tau such as hyperphosphorylation, releasefrom MT, and increased tau protein levels. We conclude that PS1participates in the regulation of neurite growth and stabilizationin both developing and differentiated neurons. In the Alzheimer'sbrain PS1 mutations may promote neuritic dystrophy and tangleformation by interfering with Notch1 signaling and enhancing pathologicalchanges intau.

Key words: Alzheimer's disease; presenilin; cytoskeleton; Notch1; amyloid $beta$ ; tau; neuronal dystrophy
Copyright © 2001 Society for Neuroscience 0270-6474/01/213834-09$05.00/0

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