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Papers In Press, published online ahead of print March 6, 2003
Department of Biochemistry, Shanghai Medical Center of Fudan University, Shanghai 200032
Corresponding Author: jxgu{at}shmu.edu.cn
The PITSLRE protein kinases are parts of the large family of p34cdc2-related kinases. During apoptosis induced by some stimuli, specific PITSLRE isoforms are cleaved by caspase to produce a protein that contains C-terminal kinase domain of the PITSLRE proteins (p110C). The p110C could induce apoptosis when it was ectopically expressed in CHO cells. In our study, similar induction of this p110C was observed during anoikis in NIH3T3 cells. To investigate the molecular mechanism of apoptosis mediated by p110C, we used the yeast two-hybrid system to screen a human fetal liver cDNA library, and identified p21-activated kinase 1 (PAK1) as an interacting partner of p110C. The association of p110C with PAK1 was further confirmed by in vitro binding assay, in vivo coimmunoprecipitation, and confocal microscope analysis. The interaction of p110C with PAK1 was through the residues 210-332 within PAK1. Neither association between p58PITSLRE or p110PITSLRE and PAK1 nor association between p110C and PAK2 or PAK3 was observed. Anoikis was increased and PAK1 activity was inhibited when NIH3T3 cells were transfected with p110C. Furthermore, the binding of p110C with PAK1 and inhibition of PAK1 activity were also observed during anoikis. Taken together, these data suggested that PAK1 might participate in the apoptotic pathway mediated by p110C.
J. Biol. Chem, 10.1074/jbc.M300818200
Submitted on January 24, 2003
Revised on March 6, 2003
Accepted on March 6, 2003
C-terminal kinase domain of the p34cdc2 related PITSLRE protein kinase (p110C) associates with p21-activated kinase 1 and inhibits its activity during Anoikis
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