| Literature DB >> 11739631 |
S H Ridley1, N Ktistakis, K Davidson, K E Anderson, M Manifava, C D Ellson, P Lipp, M Bootman, J Coadwell, A Nazarian, H Erdjument-Bromage, P Tempst, M A Cooper, J W Thuring, Z Y Lim, A B Holmes, L R Stephens, P T Hawkins.
Abstract
FENS-1 and DFCP1 are recently discovered proteins containing one or two FYVE-domains respectively. We show that the FYVE domains in these proteins can bind PtdIns3P in vitro with high specificity over other phosphoinositides. Exogenously expressed FENS-1 localises to early endosomes: this localisation requires an intact FYVE domain and is sensitive to wortmannin inhibition. The isolated FYVE domain of FENS-1 also localises to endosomes. These results are consistent with current models of FYVE-domain function in this cellular compartment. By contrast, exogenously expressed DFCP1 displays a predominantly Golgi, endoplasmic reticulum (ER) and vesicular distribution with little or no overlap with FENS-1 or other endosomal markers. Overexpression of DFCP1 was found to cause dispersal of the Golgi compartment defined by giantin and gpp130-staining. Disruption of the FYVE domains of DFCP1 causes a shift to more condensed and compact Golgi structures and overexpression of this mutant was found to confer significant protection to the Golgi against brefeldin-induced dispersal. These properties of DFCP1 are surprising, and suggest FYVE domain-localisation and function may not be exclusively endosomal. Movies available on-lineEntities:
Mesh:
Substances:
Year: 2001 PMID: 11739631 DOI: 10.1242/jcs.114.22.3991
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285