Mol Cell. 2011 Aug 5;43(3):392-405.

Alternative ubiquitin activation/conjugation cascades interact with N-end rule ubiquitin ligases to control degradation of RGS proteins.

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Department of Cell Biology, Harvard Medical School, Boston, MA 02115, USA.

Abstract

Vertebrates express two enzymes for activation of ubiquitin-UBA1, which is responsible for activation of the vast majority of E2 conjugating enzymes, and UBA6, which uses the dedicated E2, USE1. However, targets and E3s for UBA6-USE1 are unknown. Here, we demonstrate that UBA6-USE1 functions with the UBR1-3 subfamily of N-recognin E3s to degrade the N-end rule substrates RGS4, RGS5, and Arg (R)-GFP. This pathway functions in the cytoplasm in parallel with the UBA1-UBE2A/B-UBR2 cascade, which promotes turnover of nuclear RGS4/5 proteins and an apparently phenotypically distinct pool of cytoplasmic RGS4/5. UBR2 promotes Lys48 (K48)-specific ubiquitin discharge from, and RGS4 ubiquitylation by, both USE1 and UBE2A in vitro. This work provides insight into the machinery employed by the UBA6-USE1 cascade to promote protein turnover and suggests that the UBA6 and UBA1 pathways can function in parallel with the same E3 to degrade the same targets in a spatially distinct manner.

PMID:: 21816346; [PubMed - indexed for MEDLINE]
PMCID:: PMC3151487; [Available on 2012/8/5]

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Dual E1 activation systems for ubiquitin differentially regulate E2 enzyme charging. [Nature. 2007]
Dual E1 activation systems for ubiquitin differentially regulate E2 enzyme charging.
Jin J, Li X, Gygi SP, Harper JW. Nature. 2007 Jun 28; 447(7148):1135-8.
RGS4 and RGS5 are in vivo substrates of the N-end rule pathway. [Proc Natl Acad Sci U S A. 2005]
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Cited by 1 PubMed Central article

MEKK1-MKK4-JNK-AP1 Pathway Negatively Regulates Rgs4 Expression in Colonic Smooth Muscle Cells. [PLoS One. 2012]
MEKK1-MKK4-JNK-AP1 Pathway Negatively Regulates Rgs4 Expression in Colonic Smooth Muscle Cells.
Zhang Y, Li F, Liu S, Wang H, Mahavadi S, Murthy KS, Khalili K, Hu W. PLoS One. 2012; 7(4):e35646. Epub 2012 Apr 24.

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