Feh-1 and apl-1, the Caenorhabditis elegans orthologues of mammalian Fe65 and beta-amyloid precursor protein genes, are involved in the same pathway that controls nematode pharyngeal pumping.
Articolo
Data di Pubblicazione:
2002
Abstract:
The multigenic family of mammalian Fe65s encodes three highly similar
proteins with the same modular organisation: a WW domain and two
phosphotyrosinebinding domains. The PTB2 domain of these proteins binds to
the cytosolic domains of the Alzheimer?s b-amyloid precursor protein APP
and related proteins APLP1 and APLP2, generating a highly redundant system
that is hard to dissect by reverse genetics. By searching potential Fe65-
like genes in the nematode Caenorhabditis elegans, we identified a single
gene, feh-1 (Fe65 homolog-1), encoding a protein with a high sequence
similarity to mammalian Fe65s. FEH-1 is also functionally related to
mammalian orthologues; in fact its PTB2 domain binds to APL-1, the product
of the C. elegans orthologue of APP. Staining with specific antibodies show
that the neuromuscular structures of the pharynx are the sites in which
FEH-1 is present at highest levels. Expression studies with reporters
indicate that the feh-1 gene is also expressed by a subset of the worm
neurons. We generated and isolated a deletion allele of feh-1, and the
corresponding homozygous mutants arrest as late embryos or as L1 larvae,
demonstrating for the first time an essential role for a Fe65-like gene in
vivo. The pharynx of homozygous larvae does not contract and the worms
cannot feed. Analysis of pharyngeal pumping in heterozygous worms and in
feh-1 RNA-interfered worms indicates that dosage of feh-1 function affects
the rate of pharyngeal contraction in C. elegans. Interference with apl-1
double-stranded RNA showed a similar effect on pharyngeal pumping,
suggesting that FEH-1 and APL-1 are involved in the same pathway. The
non-redundant system of the nematode will prove useful for studying the
basic biology of the Fe65-APP interaction and the molecular events
regulated by this evolutionarily conserved system of interacting proteins.
Tipologia CRIS:
01.01 Articolo in rivista
Keywords:
Fe65; B-amiloid precursor; C. elegan; feh-1
Elenco autori:
Bazzicalupo, Paolo; Arbucci, Salvatore
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