Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:2.5.1.18 (
glutathione S-transferase
)
22,582
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Phosducin-like protein
(
PhLP
) has recently been identified as a ubiquitous inhibitor of G-protein betagamma-subunit (G betagamma)-mediated signaling, with an affinity about 5-fold lower than that of phosducin. The G betagamma binding site of phosducin has been suggested to be contained in its N-terminus. A region corresponding to this N-terminus is lacking in
PhLP
, suggesting that
PhLP
must utilize a different mode of G betagamma binding. To map the G betagamma binding site in
PhLP
, a series of deletion mutants were constructed, expressed in E. coli as
glutathione S-transferase
(
GST
) fusion proteins, and the purified fusion proteins were examined for their ability to attenuate G(o) GTPase activity. Progressive N-terminal truncations of
PhLP
caused only minor reductions in potency, whereas the complementary N-terminal
PhLP
fragments turned out to be inactive. We further identified a short C-terminal segment comprising residues 168 to 195 that inhibited G0 GTPase activity similar in efficacy and potency to full-length
PhLP
. This C-terminal fragment was also capable of antagonizing a second G betagamma-mediated function, the enhancement of rhodopsin phosphorylation by the beta-adrenergic receptor kinase. Taken together, these data indicate that
PhLP
interacts with G betagamma via a short C-terminal binding site which is distinct from that identified previously in phosducin.
...
PMID:Identification of a C-terminal binding site for G-protein betagamma-subunits in phosducin-like protein. 901 96
Phosducin-like protein
(
PhLP
), a widely expressed ethanol-responsive gene (Miles, M. F., Barhite, S., Sganga, M., and Elliott, M. (1993) Proc. Natl. Acad. Sci. U. S. A. 90, 10831-10835), is a homologue of phosducin, a known major regulator of Gbetagamma signaling in retina and pineal gland. However, although phosducin has a well characterized role in retinal phototransduction, function of the
PhLP
remains unclear. In this study we examine the ability of
PhLP
to bind Gbetagamma dimer in vitro and in vivo. Using
PhLP
glutathione S-transferase
fusion proteins, we show that
PhLP
directly binds Gbetagamma in vitro. Studies with a series of truncated
PhLP
fusion proteins indicate independent binding of Gbetagamma to both the amino- and C-terminal halves of
PhLP
. Protein-protein interactions between Gbetagamma and
PhLP
are inhibited by the alpha subunit of Go and Gi3, suggesting that
PhLP
can bind only free Gbetagamma. Finally, we show that
PhLP
complexes, at least partially, with Gbetagamma in vivo. Following overexpression of epitope-tagged
PhLP
together with Gbeta1gamma2 proteins in COS-7 cells, a
PhLP
-Gbetagamma complex is co-immunoprecipitated by monoclonal antibody directed against the epitope tag. Similarly, polyclonal anti-
PhLP
antibody co-precipitates endogenous
PhLP
and Gbetagamma proteins from NG108-15 cell lysates. These data are consistent with the hypothesis that
PhLP
is a widely expressed modulator of Gbetagamma function. Furthermore, because alternate forms of the
PhLP
transcript are expressed, there may be functional implications for the existence of two Gbetagamma-binding domains on
PhLP
.
...
PMID:Interaction of phosducin-like protein with G protein betagamma subunits. 913 65
