Functional Diversity and Structural Disorder in the Human Ubiquitination Pathway

A Arrigoni; A Hershko; A Mohan; AE Deffenbaugh; B Bothner; B Hao; B Hess; C Guda; C Haynes; CJ Cox; CM Pickart; D Ekman; D Szklarczyk; D Van Der Spoel; D Vuzman; DM Duda; DM Duda; DW Leung; ES Zimmerman; ET Powers; F Bernassola; F Tama; F. Gisou van der Goot; FU Hartl; G Bussi; G Moncalian; G Swaminathan; G Wu; H Daub; H Dinkel; H Dou; H Shimizu; H Zhu; HC van Leeuwen; HE Niessen; HJ Dyson; HM Berman; I Szymkiewicz; I von Ossowski; J Liu; J Ma; J Prilusky; JC Rosenbaum; JH Fong; JM Huibregtse; K Peng; K Suhre; L Aravind; L Yang; LM Iakoucheva; M Christen; M Cormont; M Fuxreiter; M Fuxreiter; M Guharoy; M Hochstrasser; M Kanehisa; M Kanehisa; M Kanehisa; M Vidal; M Zhao; MA McCoy; Mainak Guharoy; MD Petroski; MD Petroski; ME Sowa; N Foray; N Mathias; N Zheng; P Tompa; P Tompa; P Tompa; P Tompa; P Tompa; Pallab Bhowmick; PE Ryan; PE Wright; Peter Tompa; PW Hildebrand; R Kiss; RG Smock; Rita Pancsa; RJ Deshaies; S Fishbain; S Vucetic; S Wiesner; SC Kales; SJ Demarest; SJ van Wijk; T Hagai; T Inobe; T Mittag; T Ravid; U Emekli; VN Uversky; W Humphrey; W Li; WY Mark; X Zhong; Y Haupt; Y Sheng; Y Xie; Z Dosztanyi; Z Dosztanyi; Z Dosztanyi

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Functional Diversity and Structural Disorder in the Human Ubiquitination Pathway

Authors: A Arrigoni
A Hershko
A Mohan
AE Deffenbaugh
B Bothner
B Hao
B Hess
C Guda
C Haynes
CJ Cox
CM Pickart
D Ekman
D Szklarczyk
D Van Der Spoel
D Vuzman
DM Duda
DM Duda
DW Leung
ES Zimmerman
ET Powers
F Bernassola
F Tama
F. Gisou van der Goot
FU Hartl
G Bussi
G Moncalian
G Swaminathan
G Wu
H Daub
H Dinkel
H Dou
H Shimizu
H Zhu
HC van Leeuwen
HE Niessen
HJ Dyson
HM Berman
I Szymkiewicz
I von Ossowski
J Liu
J Ma
J Prilusky
JC Rosenbaum
JH Fong
JM Huibregtse
K Peng
K Suhre
L Aravind
L Yang
LM Iakoucheva
M Christen
M Cormont
M Fuxreiter
M Fuxreiter
M Guharoy
M Hochstrasser
M Kanehisa
M Kanehisa
M Kanehisa
M Vidal
M Zhao
MA McCoy
Mainak Guharoy
MD Petroski
MD Petroski
ME Sowa
N Foray
N Mathias
N Zheng
P Tompa
P Tompa
P Tompa
P Tompa
P Tompa
Pallab Bhowmick
PE Ryan
PE Wright
Peter Tompa
PW Hildebrand
R Kiss
RG Smock
Rita Pancsa
RJ Deshaies
S Fishbain
S Vucetic
S Wiesner
SC Kales
SJ Demarest
SJ van Wijk
T Hagai
T Inobe
T Mittag
T Ravid
U Emekli
VN Uversky
W Humphrey
W Li
WY Mark
X Zhong
Y Haupt
Y Sheng
Y Xie
Z Dosztanyi
Z Dosztanyi
Z Dosztanyi
Publication date: 1 January 2013
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

The ubiquitin-proteasome system plays a central role in cellular regulation and protein quality control (PQC). The system is built as a pyramid of increasing complexity, with two E1 (ubiquitin activating), few dozen E2 (ubiquitin conjugating) and several hundred E3 (ubiquitin ligase) enzymes. By collecting and analyzing E3 sequences from the KEGG BRITE database and literature, we assembled a coherent dataset of 563 human E3s and analyzed their various physical features. We found an increase in structural disorder of the system with multiple disorder predictors (IUPred - E1: 5.97%, E2: 17.74%, E3: 20.03%). E3s that can bind E2 and substrate simultaneously (single subunit E3, ssE3) have significantly higher disorder (22.98%) than E3s in which E2 binding (multi RING-finger, mRF, 0.62%), scaffolding (6.01%) and substrate binding (adaptor/substrate recognition subunits, 17.33%) functions are separated. In ssE3s, the disorder was localized in the substrate/adaptor binding domains, whereas the E2-binding RING/HECT-domains were structured. To demonstrate the involvement of disorder in E3 function, we applied normal modes and molecular dynamics analyses to show how a disordered and highly flexible linker in human CBL (an E3 that acts as a regulator of several tyrosine kinase-mediated signalling pathways) facilitates long-range conformational changes bringing substrate and E2-binding domains towards each other and thus assisting in ubiquitin transfer. E3s with multiple interaction partners (as evidenced by data in STRING) also possess elevated levels of disorder (hubs, 22.90% vs. non-hubs, 18.36%). Furthermore, a search in PDB uncovered 21 distinct human E3 interactions, in 7 of which the disordered region of E3s undergoes induced folding (or mutual induced folding) in the presence of the partner. In conclusion, our data highlights the primary role of structural disorder in the functions of E3 ligases that manifests itself in the substrate/adaptor binding functions as well as the mechanism of ubiquitin transfer by long-range conformational transitions. © 2013 Bhowmick et al