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Disease
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Drug
Enzyme
Compound
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Target Concepts:
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Query: EC:1.10.3.1 (
tyrosinase
)
9,065
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Tyrosinase and
tyrosinase
-related proteins (TRPs) are a family of melanosomal membrane proteins involved in mammalian pigmentation. Whereas the melanogenic functions of TRPs are localized in their amino-terminal domains that reside within the lumen of melanosomes, the sorting and targeting of these proteins to melanosomes is mediated by signals in their cytoplasmic domains. To identify proteins that interact with the cytoplasmic tail of gp75 (TRP-1), the most abundant melanosomal membrane protein, we performed yeast two-hybrid screening of a melanocyte cDNA library. Here, we show that the cytoplasmic domain of gp75 interacts with a PDZ domain-containing protein. The gp75-interacting protein is identical to
GIPC
, an RGS (regulator of G protein signaling)/GAIP-interacting protein, and to
SEMCAP
-1, a transmembrane semaphorin-binding protein. Carboxyl-terminal amino acid residues, Ser-Val-Val, of gp75 are necessary and sufficient for interaction of gp75 with the single PDZ domain in
GIPC
. Although endogenous and transfected GIPCs bind efficiently to transiently expressed gp75, only a small amount of
GIPC
is found associated with gp75 at steady state. Using a strategy to selectively synchronize the biosynthesis of endogenous gp75, we demonstrate that only newly synthesized gp75 associates with
GIPC
, primarily in the juxtanuclear Golgi region. Our data suggest that
GIPC
/
SEMCAP
-1 plays a role in biosynthetic sorting of proteins, specifically gp75, to melanosomes.
...
PMID:PDZ domain protein GIPC interacts with the cytoplasmic tail of melanosomal membrane protein gp75 (tyrosinase-related protein-1). 1144 Oct 7
By virtue of the presence of multiple protein-protein interaction and signaling domains, PDZ proteins play important roles in assembling protein complexes that participate in diverse cell biological processes.
GIPC
is a versatile PDZ protein that binds a variety of target proteins in different cell types. In previous studies we showed that, in epidermal melanocytes,
GIPC
interacts with newly synthesized melanosomal protein TRP1 in the Golgi region and proposed that this interaction may facilitate intracellular trafficking of TRP1. However, since
GIPC
contains a single PDZ domain and no other known protein interaction motifs, it is not known how
GIPC
-TRP1 interaction affects melanosome biogenesis and/or melanin pigmentation. Here, we show that in human primary melanocytes
GIPC
interacts with AKT-binding protein APPL (adaptor protein containing pleckstrin homology, leucine zipper and phosphotyrosine binding domains), which readily co-precipitates with newly synthesized TRP1. Knockdown of either
GIPC
or APPL inhibits melanogenesis by decreasing
tyrosinase
protein levels and enzyme activity. In melanocytes, APPL exists in a complex with
GIPC
and phospho-AKT. Inhibition of AKT phosphorylation using a PI3-kinase inhibitor abolishes this interaction and results in retardation TRP1 in the Golgi. These data suggest that interactions between TRP1-
GIPC
and
GIPC
-APPL-AKT provide a potential link between melanogenesis and PI3 kinase signaling.
...
PMID:Interactions between GIPC-APPL and GIPC-TRP1 regulate melanosomal protein trafficking and melanogenesis in human melanocytes. 2129 57
