RGSZ1 interacts with protein kinase C interacting protein PKCI-1 and modulates mu opioid receptor signaling

被引:53
作者
Ajit, Seena K. [1 ]
Ramineni, Suneela
Edris, Wade
Hunt, Rachel A.
Hum, Wah-Tung
Hepler, John R.
Young, Kathleen H.
机构
[1] Wyeth Res CN 8000, Neurosci Discovery, Princeton, NJ 08543 USA
[2] Emory Univ, Sch Med, Dept Pharmacol, Atlanta, GA 30322 USA
关键词
RGSZl; PKCI-1; yeast two hybrid; 14-3-3; phosphorylation; cAMP;
D O I
10.1016/j.cellsig.2006.09.008
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Protein kinase C interacting protein (PKCI-1) was identified among the potential interactors from a yeast two hybrid screen of human brain library using N terminal of RGSZ1 as a bait. The cysteine string region, unique to the RZ subfamily, contributes to the observed interaction because PKCI-1 interacted with N-terminus of RGS17 and GAIP, but not with that of RGS2 or RGS7 where cysteine string motif is absent. The interaction between RGSZ1 and PKCI-1 was confirmed by coinummoprecipitation and immuno fluorescence. PKCI-1 and RGSZ1 could be detected by coimmunoprecipitation using 14-3-3 antibody in cells transfected with PKCI-1 or RGSZ1 respectively, but when transfected with PKCI-1 and RGSZ1 together, only RGSZ1 could be detected. Phosphorylation of G alpha z by protein kinase C (PKC) reduces the ability of the RGS to effectively function as GTPase accelerating protein for G alpha z, and interferes with ability of Getz to interact with beta gamma complex. We investigated the roles of 14-3-3 and PKCI-1 in phosphorylation of G alpha z. Phosphorylation of G alpha z by PKC was inhibited by 14-3-3 and the presence of PKCI-1 did not provide any further inhibition. PKCI-1 interacts with mu opioid receptor and suppresses receptor desensitization and PKC related mu opioid receptor phosphorylation [W. Guang, H. Wang, T. Su, I.B. Weinstein, J.B. Wang, Mol. Pharmacol. 66 (2004) 1285.]. Previous studies have also shown that mu opioid receptor co-precipitates with RGSZ1 and influence mu receptor signaling by acting as effector antagonists [J. Garzon, M. Rodriguez-Munoz, P. Sanchez-Blazquez, Neurophannacology 48 (2005) 853., J. Garzon, M. Rodriguez-Munoz, A. Lopez-Fando, P. Sanchez-Blazquez Neuropsychopharmacology 30 (2005) 1632.]. Inhibition of cAMP by mu opioid receptor was significantly reduced by RGSZ1 and this effect was enhanced in combination with PKCI-1. Our studies thus provide a link between the previous observations mentioned above and indicate that the major function of PKCI-I is to modulate mu opioid receptor signaling pathway along with RGSZ1, rather than directly mediating the G alpha z RGSZ1 interaction. (c) 2006 Elsevier Inc. All rights reserved.
引用
收藏
页码:723 / 730
页数:8
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