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A SUMO-Dependent Protein Network Regulates Chromosome Congression during Oocyte Meiosis

Author(s)
Pelisch, FedericoTammsalu, TriinWang, BinJaffray, Ellis G.Gartner, AntonHay, Ronald T.
Issued Date
2017-01
DOI
10.1016/j.molcel.2016.11.001
URI
https://scholarworks.unist.ac.kr/handle/201301/27444
Fulltext
https://www.sciencedirect.com/science/article/pii/S1097276516307092?via%3Dihub
Citation
MOLECULAR CELL, v.65, no.1, pp.66 - 77
Abstract
During Caenorhabditis elegans oocyte meiosis, a multi-protein ring complex (RC) localized between homologous chromosomes, promotes chromosome congression through the action of the chromokinesin KLP-19. While some RC components are known, the mechanism of RC assembly has remained obscure. We show that SUMO E3 ligase GEI-17/PIAS is required for KLP-19 recruitment to the RC, and proteomic analysis identified KLP-19 as a SUMO substrate in vivo. In vitro analysis revealed that KLP-19 is efficiently sumoylated in a GEI-17-dependent manner, while GEI-17 undergoes extensive auto-sumoylation. GEI-17 and another RC component, the kinase BUB-1, contain functional SUMO interaction motifs (SIMs), allowing them to recruit SUMO modified proteins, including KLP-19, into the RC. Thus, dynamic SUMO modification and the presence of SIMs in RC components generate a SUMO-SIM network that facilitates assembly of the RC. Our results highlight the importance of SUMO-SIM networks in regulating the assembly of dynamic protein complexes.
Publisher
CELL PRESS
ISSN
1097-2765
Keyword
C-ELEGANSIDENTIFICATIONSEGREGATIONPATHWAYSUMOYLATIONPROGRESSIONMODIFIERBODY

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