Two paralogous complexes, the proteasome lid and the COP9 signalosome (CSN), have diverged from a common ancestor; yet fulfill distinctive roles within the ubiquitin-proteasome sphere. The CSN regulates the largest family of E3 ubiquitin ligases, called CRLs (Cullin-RING ubiquitin Ligases), while the lid is a subcomplex of the 26 S proteasome, a proteolytic machinery responsible for the degradation of ubiquitinated proteins. Remarkably, in many organisms, several subunits of both complexes are duplicated, a circumstance that can hypothetically increase the number of different complexes that can be formed. Duplication, however, is not the only complexity trait within the lid and the CSN, because many of their subunits are not fully committed only to one of the two complexes, but they are able to associate with both. Indeed, their corresponding mutants have features that can be due to the absence of more than one complex. This could be simply explained by the subunits being able to carry an identical function within more than one paralogdus complex or by the subunits having a certain level of promiscuity, i.e. being able to carry more than one function, depending on the complex they are associating with. Recent data show that both options are possible and, although their functional relevance still needs to be fully uncovered, evidence is accumulating, which indicates a promiscuous trading of paralogous subunits, and suggests that this may occur transiently, and/or in response to particular environmental conditions. (C) 2013 Elsevier Ireland Ltd. All rights reserved.

Duplication and familial promiscuity within the proteasome lid and COP9 signalosome kin complexes / Serino, Giovanna; Elah, Pick. - In: PLANT SCIENCE. - ISSN 0168-9452. - STAMPA. - 203:(2013), pp. 89-97. [10.1016/j.plantsci.2012.12.018]

Duplication and familial promiscuity within the proteasome lid and COP9 signalosome kin complexes

SERINO, Giovanna;
2013

Abstract

Two paralogous complexes, the proteasome lid and the COP9 signalosome (CSN), have diverged from a common ancestor; yet fulfill distinctive roles within the ubiquitin-proteasome sphere. The CSN regulates the largest family of E3 ubiquitin ligases, called CRLs (Cullin-RING ubiquitin Ligases), while the lid is a subcomplex of the 26 S proteasome, a proteolytic machinery responsible for the degradation of ubiquitinated proteins. Remarkably, in many organisms, several subunits of both complexes are duplicated, a circumstance that can hypothetically increase the number of different complexes that can be formed. Duplication, however, is not the only complexity trait within the lid and the CSN, because many of their subunits are not fully committed only to one of the two complexes, but they are able to associate with both. Indeed, their corresponding mutants have features that can be due to the absence of more than one complex. This could be simply explained by the subunits being able to carry an identical function within more than one paralogdus complex or by the subunits having a certain level of promiscuity, i.e. being able to carry more than one function, depending on the complex they are associating with. Recent data show that both options are possible and, although their functional relevance still needs to be fully uncovered, evidence is accumulating, which indicates a promiscuous trading of paralogous subunits, and suggests that this may occur transiently, and/or in response to particular environmental conditions. (C) 2013 Elsevier Ireland Ltd. All rights reserved.
2013
arabidopsis thaliana; cop9 signalosome; eif3; elf3; gene duplication; pci complexes; pci complexes cop9 signalosome proteasome lid eif3 arabidopsis thaliana saccharomyces cerevisiae; proteasome lid; protein complexes; saccharomyces cerevisiae; ubiquitin ligase
01 Pubblicazione su rivista::01a Articolo in rivista
Duplication and familial promiscuity within the proteasome lid and COP9 signalosome kin complexes / Serino, Giovanna; Elah, Pick. - In: PLANT SCIENCE. - ISSN 0168-9452. - STAMPA. - 203:(2013), pp. 89-97. [10.1016/j.plantsci.2012.12.018]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/513197
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