共 85 条
Beta-arrestins as regulators of signal termination and transduction: How do they determine what to scaffold?
被引:112
作者:

DeFea, Kathryn A.
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h-index: 0
机构:
Univ Calif Riverside, Div Biomed Sci, BIOMED, Riverside, CA 92521 USA Univ Calif Riverside, Div Biomed Sci, BIOMED, Riverside, CA 92521 USA
机构:
[1] Univ Calif Riverside, Div Biomed Sci, BIOMED, Riverside, CA 92521 USA
关键词:
Arrestins;
GPCR;
Signaling;
Chemotaxis;
MAPK;
PI3K;
PDE4;
Ubiquitin;
CAMP-SPECIFIC PHOSPHODIESTERASE;
BETA(2)-ADRENERGIC RECEPTOR;
KINASE ACTIVATION;
PHOSPHATIDYLINOSITOL;
3-KINASE;
CONFORMATIONAL DIFFERENCES;
ERK1/2;
ACTIVATION;
HORMONE RECEPTOR;
BINDING-SITES;
N-DOMAIN;
BETA-ARRESTIN-2;
D O I:
10.1016/j.cellsig.2010.10.004
中图分类号:
Q2 [细胞生物学];
学科分类号:
071009 ;
090102 ;
摘要:
Over the last decade beta-arrestins have emerged as pleiotropic scaffold proteins, capable of mediating numerous diverse responses to multiple agonists. Most well characterized are the G-protein-coupled receptor (GPCR) stimulated beta-arrestin signals, which are sometimes synergistic with, and sometimes independent of, heterotrimeric G-protein signals. beta-arrestin signaling involves the recruitment of downstream signaling moieties to beta-arrestins; in many cases specific sites of interaction between beta-arrestins and the downstream target have been identified. As more information unfolds about the nature of beta-arrestin scaffolding interactions, it is evident that these proteins are capable of adopting multiple conformations which in turn reveal a specific set of interacting domains. Recruitment of beta-arrestin to a specific GPCR can promote formation of a specific subset of available beta-arrestin scaffolds, allowing for a higher level of specificity to given agonists. This review discusses recent advances in beta-arrestin signaling, discussing the molecular details of a subset of known beta-arrestin scaffolds and the significance of specific binding interactions on the ultimate cellular response. (C) 2010 Elsevier Inc. All rights reserved.
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页码:621 / 629
页数:9
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Baillie, George S.
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Li, Xiang
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Lynch, Martin J.
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Herzyk, Pawel
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Mitchell, Lisa High
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McCahill, Angela
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Hundsrucker, Christian
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Klussmann, Enno
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Adams, David R.
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Houslay, Miles D.
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Univ Glasgow, Inst Biomed & Life Sci, Div Biochem & Mol Biol, Mol Pharmacol Grp, Glasgow G12 8QQ, Lanark, Scotland Univ Glasgow, Inst Biomed & Life Sci, Div Biochem & Mol Biol, Mol Pharmacol Grp, Glasgow G12 8QQ, Lanark, Scotland
[10]
Conformational differences between arrestin2 and preactivated mutants as revealed by hydrogen exchange mass spectrometry
[J].
Carter, JM
;
Gurevich, VV
;
Prossnitz, ER
;
Engen, JR
.
JOURNAL OF MOLECULAR BIOLOGY,
2005, 351 (04)
:865-878

Carter, JM
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机构: Univ New Mexico, Dept Chem, Albuquerque, NM 87131 USA

Gurevich, VV
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机构: Univ New Mexico, Dept Chem, Albuquerque, NM 87131 USA

Prossnitz, ER
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Univ New Mexico, Dept Chem, Albuquerque, NM 87131 USA Univ New Mexico, Dept Chem, Albuquerque, NM 87131 USA

Engen, JR
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