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Literature DB >> 24012956

Rapid degeneration of rod photoreceptors expressing self-association-deficient arrestin-1 mutant.

Xiufeng Song¹, Jungwon Seo, Faiza Baameur, Sergey A Vishnivetskiy, Qiuyan Chen, Seunghyi Kook, Miyeon Kim, Evan K Brooks, Christian Altenbach, Yuan Hong, Susan M Hanson, Maria C Palazzo, Jeannie Chen, Wayne L Hubbell, Eugenia V Gurevich, Vsevolod V Gurevich.

Abstract

Arrestin-1 binds light-activated phosphorhodopsin and ensures timely signal shutoff. We show that high transgenic expression of an arrestin-1 mutant with enhanced rhodopsin binding and impaired oligomerization causes apoptotic rod death in mice. Dark rearing does not prevent mutant-induced cell death, ruling out the role of arrestin complexes with light-activated rhodopsin. Similar expression of WT arrestin-1 that robustly oligomerizes, which leads to only modest increase in the monomer concentration, does not affect rod survival. Moreover, WT arrestin-1 co-expressed with the mutant delays retinal degeneration. Thus, arrestin-1 mutant directly affects cell survival via binding partner(s) other than light-activated rhodopsin. Due to impaired self-association of the mutant its high expression dramatically increases the concentration of the monomer. The data suggest that monomeric arrestin-1 is cytotoxic and WT arrestin-1 protects rods by forming mixed oligomers with the mutant and/or competing with it for the binding to non-receptor partners. Thus, arrestin-1 self-association likely serves to keep low concentration of the toxic monomer. The reduction of the concentration of harmful monomer is an earlier unappreciated biological function of protein oligomerization.

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: Arrestin; Cell death; G protein-coupled receptor; G protein-coupled receptor kinase; GPCR; GRK; Monomer; P-Ops; P-Rh; P-Rh*; Retina; Rh; Rh*; Rhodopsin; Self-association; WT; dark phosphorylated rhodopsin; dark unphosphorylated rhodopsin; light-activated phosphorylated rhodopsin; light-activated unphosphorylated rhodopsin; phospho-opsin; wild type

Mesh：

Substances：

Year: 2013 PMID： 24012956 PMCID： PMC3833262 DOI： 10.1016/j.cellsig.2013.08.022

Source DB: PubMed Journal: Cell Signal ISSN： 0898-6568 Impact factor: 4.315

77 in total

1. Visual arrestin activity may be regulated by self-association.

Authors: C Schubert; J A Hirsch; V V Gurevich; D M Engelman; P B Sigler; K G Fleming
Journal: J Biol Chem Date: 1999-07-23 Impact factor: 5.157

2. The 2.8 A crystal structure of visual arrestin: a model for arrestin's regulation.

Authors: J A Hirsch; C Schubert; V V Gurevich; P B Sigler
Journal: Cell Date: 1999-04-16 Impact factor: 41.582

3. The selectivity of visual arrestin for light-activated phosphorhodopsin is controlled by multiple nonredundant mechanisms.

Authors: V V Gurevich
Journal: J Biol Chem Date: 1998-06-19 Impact factor: 5.157

Review 4. Caspases: enemies within.

Authors: N A Thornberry; Y Lazebnik
Journal: Science Date: 1998-08-28 Impact factor: 47.728

5. Mechanism of quenching of phototransduction. Binding competition between arrestin and transducin for phosphorhodopsin.

Authors: J G Krupnick; V V Gurevich; J L Benovic
Journal: J Biol Chem Date: 1997-07-18 Impact factor: 5.157

6. Arrestin with a single amino acid substitution quenches light-activated rhodopsin in a phosphorylation-independent fashion.

Authors: M P Gray-Keller; P B Detwiler; J L Benovic; V V Gurevich
Journal: Biochemistry Date: 1997-06-10 Impact factor: 3.162

Rapid degeneration of rod photoreceptors expressing self-association-deficient arrestin-1 mutant.

1. Visual arrestin activity may be regulated by self-association.

2. The 2.8 A crystal structure of visual arrestin: a model for arrestin's regulation.

3. The selectivity of visual arrestin for light-activated phosphorhodopsin is controlled by multiple nonredundant mechanisms.

Review 4. Caspases: enemies within.

5. Mechanism of quenching of phototransduction. Binding competition between arrestin and transducin for phosphorhodopsin.

6. Arrestin with a single amino acid substitution quenches light-activated rhodopsin in a phosphorylation-independent fashion.

7. How does arrestin respond to the phosphorylated state of rhodopsin?

8. Abnormal photoresponses and light-induced apoptosis in rods lacking rhodopsin kinase.

9. Arrestin2 expression selectively increases during neural differentiation.

10. Prolonged photoresponses in transgenic mouse rods lacking arrestin.

Review 1. Beyond traditional pharmacology: new tools and approaches.

Review 2. The Diverse Roles of Arrestin Scaffolds in G Protein-Coupled Receptor Signaling.

3. Arrestin expression in E. coli and purification.

Review 4. Overview of different mechanisms of arrestin-mediated signaling.

5. Differential manipulation of arrestin-3 binding to basal and agonist-activated G protein-coupled receptors.

6. Enhanced phosphorylation-independent arrestins and gene therapy.

7. Arrestins in apoptosis.

8. Self-association of arrestin family members.

Review 9. Analyzing the roles of multi-functional proteins in cells: The case of arrestins and GRKs.

10. Requirements for Neurogenin2 during mouse postnatal retinal neurogenesis.