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J. Biol. Chem., Vol. 277, Issue 22, 19783-19791, May 31, 2002
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From the Centro de Biología Molecular Severo Ochoa, Consejo
Superior de Investigaciones Científicas, Universidad
Autónoma de Madrid, Madrid 28049, Spain
In this study we have used the yeast two-hybrid
system to identify proteins that interact with the carboxyl-cytoplasmic
domain (residues 464-509) of the insulin-sensitive glucose transporter GLUT4 (C-GLUT4). Using as bait C-GLUT4, we have isolated the carboxyl domain of Daxx (C-Daxx), the adaptor protein associated with the Fas
and the type II TGF-
The Insulin-sensitive Glucose Transporter, GLUT4,
Interacts Physically with Daxx
TWO PROTEINS WITH CAPACITY TO BIND Ubc9 AND CONJUGATED TO
SUMO1*
,
(TRII) receptors (1, 2). The two-hybrid
interaction between C-GLUT4 and C-Daxx is validated by the ability of
in vitro translated C-GLUT4 to interact with in
vitro translated full-length Daxx and C-Daxx. C-Daxx does not interact with the C-cytoplasmic domain of GLUT1, the ubiquitous glucose
transporter homologous to GLUT4. Replacement of alanine and serine for
the dileucine pair (Leu489-Leu490)
critical for targeting GLUT4 from the trans-Golgi network to the
perinuclear intracellular store as well as for its surface internalization by endocytosis inhibits 2-fold the interaction of
C-GLUT4 with Daxx. Daxx is pulled down with GLUT4 immunoprecipitated from lysates of 3T3-L1 fibroblasts stably transfected with GLUT4 and
3T3-L1 adipocytes expressing physiological levels of the two proteins.
Similarly, GLUT4 is recovered with anti-Daxx immunoprecipitates. Using
an established cell fractionation procedure we present evidence for the
existence of two distinct intracellular Daxx pools in the nucleus and
low density microsomes. Confocal immunofluorescence microscopy studies
localize Daxx to promyelocytic leukemia nuclear bodies and
punctate cytoplasmic structures, often organized in strings and
underneath the plasma membrane. Daxx and GLUT4 are SUMOlated as shown
by their reaction with an anti-SUMO1 antibody and by the ability of
this antibody to pull down Daxx and GLUT4.
*
This work was supported by Grant PB94-0035 from the
Ministerio Español de Educación y Ciencia and the European
Commission Grants ERB4061PL95-0924 and FMRX-CT96-0058.The costs of publication of this
article were defrayed in part by the
payment of page charges. The article
must therefore be hereby marked
"advertisement" in accordance with 18 U.S.C. Section
1734 solely to indicate this fact.
Supported by Fellowship AP2000-3212 from the Ministerio
Español de Educación, Cultura y Deporte.
§
To whom correspondence should be addressed: Centro de
Biología Molecular Severo Ochoa, Consejo Superior de
Investigaciones Científicas, Universidad Autónoma de
Madrid, Cantoblanco, Madrid 28049, Spain. Tel.: 34-91-397-8455;
Fax: 34-91-397-4799; E-mail: isandoval@cbm.uam.es.
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