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![Page 1: Activation of the Interferon Regulatory Factors: Crystal Structure of Dimeric IRF-5 Bill Royer, Weijun Chen, Suvana Lam, Hema Srinath, Celia Schiffer,](https://reader034.fdocuments.us/reader034/viewer/2022051116/56649f2b5503460f94c454d0/html5/thumbnails/1.jpg)
Activation of the Interferon Regulatory Factors: Crystal Structure of Dimeric IRF-5
Bill Royer, Weijun Chen, Suvana Lam, Hema Srinath, Celia Schiffer, Kate Fitzgerald and Kai Lin
University of MassachusettsWorcester (not Amherst)
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Immediate and Delayed Anti-Viral Responses
IFN- IFN-
IFNAR
Jak1Tyk2
Stat2
Stat1
IRF-9 (ISGF3)
other cytokines,anti-viral genes
IFN-/
virus
IRF3
IRF3IRF3
IRF3
IRF3
IRF3
IFN- genes
PP
IFN- gene
IRF3
IRF3IRF3
P
IRF3P
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TLR7,TLR8
ssRNA
MyD88
TBK1
IKK
IRF7
IRAK4
IRAK1TRAF6
Ub
TABs
1
TAK1
23
IKK
IKK
IKK
P
MAPKsNF-B
IBs
P
Ub
P
IBs
26Sproteasome
NF-BIRF7 ATF2/c-Jun
IFN
IRF5NF-B
Inflammatorycytokines
Cytoplasm
Endosome
Nucleus
IFNs
IRF7
TLR9
dsDNA
virus
MyD88
TRAF6Ub
IRF5Ub
IRF5
?
P
Innate immunity is triggered by the recognition of “pathogen-associated molecular patterns” such as viral nucleic acids by Toll-like receptors (TLR) or cytoplasmic receptors.
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IRFs are activated by phosphorylation in the C-terminal domain
P
P P
Cytoplasm
Nucleus
C
N
CBP
P P
DD
P P
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Serine PO4 sites
B.Y. Qin, et al. K. Lin (2003) Nat. Struct. Biol. 10, 913 -921K. Takahashi, et al. F. Inagaki (2003) Nat. Struct. Biol. 10, 922-927
Domain structure of human IRF-3
110 427
NES
DBD1
NLS
200
IAD
IAD173 427
AUD
RVGGASSLENTVDLHISNSHPLSLTS
380
380
IRF-3 transactivation domain construct
IRF-3 acts as a molecular sentry for viral infection in all cell types.
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N
C
IRF-3 (residues 173-427)
Structure of IRF-3 transactivation domain in complex with CBP supports the hypothesis that the autoinhibitory region masks CBP binding site
B.Y. Qin, et al. K. Lin (2005) Structure 13, 1269-1277
IRF-3 (residues 173-394)
CBP (2067-2112)
N
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IRF-5
The autoinhibition of IRF-5 is less tight than that for the ubiquitously expressed IRF-3.
IRF-5 is activated by:• viral expression • type I interferon• tumor suppressor p53
IRF-5 activates• type I interferon• inflammatory cytokines• tumor suppressors
Human mutations of IRF-5 have been implicated in• systemic lupus erythematosis• multiple sclerosis• Sjogrens syndrome• Inflamatory bowel disease
IRF-5 k.o. mice show• susceptibility to viral infection• susceptibility to tumors
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110 427
NES
DBD1
NLS
200
405
IAD
IAD173 427
AUD
Domain structure of Human IRF-3 and IRF-5
RVGGASSLENTVDLHISNSHPLSLTS
SGELSWSADSIRLQISNPDIKDRMV
NES
DBD
NLS
IAD
380
380
IRF-3
IRF-3 transactivation domain construct
IRF-5 (variant 4)
IRF-5 transactivation domain construct
IAD
222 467
NLS
421 455
421 4672331401
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Interactions of CBP (2067-2112) with IRF-5 (222-467) and phosphomimetic mutants based on ITC data
Complex Kd Change in affinity
CBP – IRF-5 1.64M 1.0 foldCBP – IRF-5 (S427D) 0.96M 1.7 foldCBP – IRF-5 (S425D) 0.71M 2.3 foldCBP – IRF-5 (S436D) 0.67M 2.4 foldCBP – IRF-5 (S430D) 0.56M 2.9 fold
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0
200
400
600
mAU(280 nm)
12.0 13.0 14.0 15.0 16.0 17.0 18.0 19.0
Volume (ml)
IRF-5
IRF-5 + CBP
CBP 200
400
600
800
mAU (280 nm)13.0 14.0 15.0 16.0 17.0
Volume (ml)
0
250 µM
IRF-5 WT
100 µM
50 µM
450 µM
0
200
400
600
800
mAU (280 nm)
13.0 14.0 15.0 16.0 17.0Volume (ml)
IRF-5 S430D450 µM
250 µM
100 µM
50 µM
mAU (280 nm)
0
200
400
600
12.0 13.0 14.0 15.0 16.0 17.0 18.0 19.0Volume (ml)
IRF-5 S430DIRF-5 S430D + CBP
CBP
Size exclusion chromatography to investigate oligomerization of IRF-5 (222-467) and IRF-5 S430D
Monomer
Dimer
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IRF-3 complex with CBP
C
N
IRF-5 dimeric subunit
C
N
Helix 2
Hel
ix 5
Helix 4
Helix 3 Helix 1
IRF-3 autoinhibited monomer
C
N
Helix 5
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IRF-5 dimeric subunitIRF-3 autoinhibited monomer IRF-3 complex with CBP
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IRF-5 (222-467) S430D Dimer
Hel
ix 5
Hel
ix 5
N
N
C
C
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IRF-5 (222-467) S430D Dimer
Hel
ix 5
Hel
ix 5
N
N
C
C
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Helix 5 plays key alternate roles in IRF autoinhibition and dimerization.
IRF-5 dimerIRF-3 monomer
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R353
I431’
L433’
I435’
S430’(D) S427’S425
S436’
K449’
V445’
D442’
R328
L403
Y303
L307
V310D312
F279
Helix 5
Hel
ix 2
Hel
ix 4
Key interface residues in the IRF-5 dimer
R328
D442’
R353
S436’
Helix 5
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R353
I431’
L433’
I435’
S430’(D) S427’S425
S436’
K449’
V445’
D442’
R328
L403
Y303
L307
V310D312
F279
Helix 5
Hel
ix 2
Hel
ix 4
V391
L393
S396
I395 Hel
ix 1
Hel
ix 4
IRF-5 Dimer IRF-3 Monomer
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R353
I431’
L433’
I435’
S430’(D) S427’S425
S436’
K449’
V445’
D442’
R328
L403
Y303
L307
V310D312
F279
Helix 5
Hel
ix 2
Hel
ix 4
Key interface residues in the IRF-5 dimer
R328
D442’
R353
S436’
Helix 5
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IRF5-S430D & CBP
IRF5-S430D/R353D & CBP IRF5-S430D/D442R & CBP
IRF5-S430D/V310D & CBP IRF5-S430D/R328E & CBP IRF5-S436D/R328E & CBP
0
100
200
300
400
500
600
mAU (280 nm)
13 14 15 16 17 18 19 20
Volume (ml)
Dimer
Monomer
CBP
Mutation of interface residues disrupt dimer formation of IRF-5 in solution
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Disruption of dimerization by mutation of interface residues inhibits IRF-5 activation
HEK293 Cells
IFN
luce
rfer
ase
(F
old
In
du
ctio
n)
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I431’
L433’
I435’
S430’(D) S427’S425
S436’
K449’
V445’
D442’
R353
R328
L403
Y303
L307
V310D312
F279
Helix 5H
elix
2
(homologous IRF3 residue number for absolutely conserved residues)(L362)
(R285)
Hel
ix 5
R328
D442’
R353
S436’
Helix 5
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IRF3-S386D/S396D/L362D & CBP IRF3-S386D/S396D/R285E & CBP IRF3-S386D/396D & CBP
0
100
200
300
400
mAU (280 nm)
Volume (ml)
12.0 13.0 14.0 15.0 16.0 17.0 18.0 19.0 20.0
Dimer
Monomer
CBP
Mutation of IRF-3 residues homologous to IRF-5 dimeric interface residues disrupts formation of the IRF-3 dimer in solution
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Disruption of IRF-3 dimerization inhibits its activationIF
N
luc
erf
era
se
(F
old
In
du
cti
on)
HEK293 Cells
Published IRF-3 mutants reinterpreted in light of our structure also support the crystallographically observed IRF-
5 dimer as representing the active state of IRF-3
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Relationship of the IRF-5 transactivation domain dimer with IRF-3 DNA binding Domains
D. Panne, T. Maniatis & S.C. Harrison (2007) Cell 129, 1111-1123
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(Morphing CNS script from the Yale Morph Server, http://molmovdb.org)
Phosphorylation
IRF activation, dimerization and CBP binding
C-term
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(Morphing CNS script from the Yale Morph Server, http://molmovdb.org)
Phosphorylation
IRF activation, dimerization and CBP binding
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P
PP
PP
Hel
ix 5
Helix 5DBD
CBP
bindingsite
DBDCBP
bindingsite
DBD
DBD
Helix 5
Helix 5
Nucleus
Cytoplasm
DBD
DB
D
PP
PP
Hel
ix 5
CBP
binding
site
DBDCBP
binding
site
Helix 5
PP
PP
Hel
ix 5
Helix 5DBD
CBP
bindingsite
DBDCBP
bindingsite
CBP
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University of Massachusetts, Worcester
Dept. of Biochemistry and Molecular Pharmacology
Kai Lin
Weijun ChenSuvana Lam
Hema SrinathBrendan Hilbert
Celia Schiffer
Department of Medicine
Kate FitzgeraldZhaozhao Jiang
$ - NIH
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Sequence alignment of the C-terminal transactivation domains of human IRF family members
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The IFN Enhanceosome
IRF3 IRF7
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D. Panne, T. Maniatis & S.C. Harrison (2007) Cell 129, 1111-1123
Binding of four N-terminal DNA Binding Domains of IRF-3 to promoter as part of IFN- enhanceosome
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