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The Journal of Neuroscience, February 1, 1998, 18(3):914-922
Interaction of Presenilins with the Filamin Family
of Actin-Binding Proteins
Wanjiang
Zhang1,
Sang
Woo
Han2,
Daniel W.
McKeel4,
Alison
Goate2, 3, and
Jane Y.
Wu1
Departments of 1 Pediatrics and Molecular Biology and
Pharmacology, 2 Psychiatry, 3 Genetics, and
4 Pathology, Washington University School of Medicine, St.
Louis, Missouri 63110
Mutations in presenilin genes PS1 and PS2 account for ~50% of
early-onset familial Alzheimer's disease (FAD). The PS1 and PS2 genes
encode highly homologous transmembrane proteins related to the
Caenorhabditis elegans sel-12 and spe-4 gene products. A
hydrophilic loop region facing the cytoplasmic compartment is likely to
be functionally important because at least 14 mutations in FAD patients
have been identified in this region. We report here that the loop
regions of PS1 and PS2 interact with nonmuscle filamin (actin-binding
protein 280, ABP280) and a structurally related protein (filamin
homolog 1, Fh1). Overexpression of PS1 appears to modify the
distribution of ABP280 and Fh1 proteins in cultured cells. A monoclonal
antibody recognizing ABP280 and Fh1 binds to blood vessels, astrocytes,
neurofibrillary tangles, neuropil threads, and dystrophic neurites in
the AD brain. Detection of ABP280/Fh1 proteins in these structures
suggests that these presenilin-interacting proteins may be involved in
the development of AD and that interactions between presenilins and
ABP280/Fh1 may be functionally significant. The ABP280 gene is located
on the human X chromosome, whereas the newly identified Fh1 gene maps
to human chromosome 3. These results provide a new basis for
understanding the function of presenilin proteins and further implicate
cytoskeletal elements in AD pathogenesis.
Key words:
Alzheimer's disease; presenilins; protein-protein
interaction; actin-binding protein 280; filamin homolog 1; cytoskeletal
elements
Copyright © 1998 Society for Neuroscience 0270-6474/98/183914-09$05.00/0
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