Post on 15-Apr-2017
Talin/ Radixin, a FERM Family Protein
that Binds Intergrin β2 Cytotail and
Regulates Its Function?
Vascular Biology
Pingtao Tang
• Introduction
• Analysis of protein in lymphocytes
using 2D-electrophoresis
• Integrin β 2 cytoplasmic tail binding protein
1) Talin and Talin F3/ F3S
Interaction between β 2
and Talin
F3
2) ERM family: Radixin
N/C-terminal radixin and β 2
Intergrin
> 20 human intergrins ( αβ heterodimers)
Activation of intergrins is important in many biological processes: cell migration, hemostasis, extracellular matrix assemble, tumor metastasis, and immuune response
The integrin β tail plays a central role in the activation process, by undergoing regulated interations with cytoplasmic proteins
Fb--fibrinogen
FX--factor X
ICAM-1, 2, 3--
intercellular adhesion
molecule-1, 2, 3
The patient: extensive mucosal bleeding,
intercranial hemmorrage, recurrent infection.
Deficiencies: Glanzmann’s Thrombasthenia (GT): failure of Fg
binding to plateles.
Leukocyte Adhesion Deficiency (LAD)
αMβ2 ( neutrophils): NIF binding, but defective adhesion to Fg (PAM)
implicating a defect in the “inside-out” signaling
Lymphocytes: defective adhesion to ICAM-1(αLβ2) and Fn (α4β1).
In contrast, lymphocytes from normal control
adhered to both ligands, and adhesion could be
further enhanced by addition of PAM (a PKC agonist)
Stable cell lines: the Epstein Bar virostransformed lymphocytes.
“Inside-out”
Signaling Conformational Clusterin
changes
The “inside-out” signaling:
Upon activation, intergrins
change their conformation
and/or cluster on the cell
surface. These processes
leads to increase
in ligand affinity
and avidity, and
hence enhanced
ligand binding
and cell adhesion.
Cytohesin-1, a PIP3-regulated
adaptor molecule for LFA-1
(CD11a/CD18, αLβ2) activation
Cytoskeleton (αIIbβ3)
PAK1 Rhok Cytohesin-1 Talin F3
? Lipid (PIP2,PIP3)
rho rac cdc42
PI-3K MAPK
PKC
G-protein
Growth factors CD19 Cytokines
PKC-driven wound
closure response in 2C4
fibrosarcoma cells stably
transfected with GFP–
PKC.
• Wound closure response was
recorded by time-lapse
microscopy
• GFP–PKC-2C4 cells were
wounded after a 30 min
incubation in media
containing LY294002 (10
µM) (+LY294002) PDBu (1
µM) was added to the media
after wounding and the
wound closure response was
monitored.
(EMBO J2001, 20(11): 2723-2741)
AL-500 N-500
pH3 pH10 pH3 pH10
Analysis of Two-Dimensional (2-D) Electrophoresis
of Protein in the Patient’s Lymphocyte Line
(Comsblue)
Empty: Matched, Solid: Unmatched
Blue: AL Red : N ; 4-20% PAGE gel
AL-N-comsblue-Matched Map
pH10 pH3 pH3.0 pH10
AL N
Phosphorylation of 2-D Electrophoresis of Protein
in the Lymphocyte Line
(Western blot with anti- phosphotyrosine antibody)
4 sec
10 sec
• band four-point-one (band4.1)/ezrin/radixin/moesin homology
domain, FERM (173-342aa)
• mediate their interactions with the cytoplasmic domain of
transmembrane protein
F3 , a sandwich of two orthogonal antiparallel b sheets and a helix,
including phosphotyrosine-binding (PTB) and plechstrin homology (PH)
domain.
PTB like F3 subdomain leads to integrin activation.
A Schematic Representation of Talin
Head F1-3 Rod domain
50 -kDa CalpainII 250-kDa
8d4
139 433 1071
Sequence Alignment of FERM Domains
342
173
Talin F3 Subdomain Adopts
A PTB-like Fold
phosphotyrosine-binding, PTB
(DA. Calderwood 2002)
• GST fusion expression system: pGEX-4T-1
• Histin fusion expression system: pET-32a-c(+), pQE30/pQE31
• Mammalian cell expression: MSCV-IRGFP, pcDNA3.1/myc-His
Head Rod domain
(FERM, F1-3)
8d4 Talin
139 433 1071 2541
210 297 583
Band4.1 ERM
NR CR
Radixin
FERM Domain
Purification of talin F3
Eluted Throbin Talin F3 GST
M 1 2 3 Sup Resin 5 6 11 15 16 17 18 19 20
Ni –NTA Mono HR 5/5
F3
GST
GST-F3
61.3
36.4
24.7
19.2
13.1
9.3 (kDa)
68.8
40.0
28.4
(kDa)
Western bolt SDS-PAGE MW (Anti-His Antibody) (Protein Staning)
Purification of His-talin F3S
Purification of GST-Radixin / Talin L
NR M CR Talin L
68.8
52.5
40.0
(kDa)
(Glutathione Sepharose 4B)
GSH (mM) 5 20 5 20 20
ELISA Assay of Talin/Talin F3
Binding on β2 Cytotail
0
0.4
0.8
1.2 Alpha M
beta2
3 6 3 6 (nM)
Talin Talin F3
His-Talin F3S Subdomain Binds Intergrin β2 Cytotail
0.3 1.2 0.6 1.2 (μg)
0
0.1
0.2
0.3GST-beta2 cytotail (0.31 ug)
GST-alpha M cytotail (0.31 ug)
GST (0.35 ug)
Talin F3S (No. 1) Talin F3 (No. 2)
OD
His-Talin F3S Subdomain Binds
Intergrin β2 Tail (Repeated)
0
0.2
0.4
0.6 GST-beta2 cytotail
GST-alpha M cytotail
GST
0.3 0.6 (μg) Tail F3S
OD
ELISA Assay of Talin / Talin F3
Binding on Intergrin β2 Tail
OD
Concentration of Talin or Talin F3 (nM)
•Coat β2 or
αM cytotail
peptid 21.2
mMol/L
•10% milk and
1% BSA block
•GST-talin/F3
0
0.2
0.4
0.6
0.8
0 2 4 6 8
Talin L+ beta 2
F3 + beta2
Talin + Alpha M
F3 + Alpha M
A
A
C
C
B
Add DDT
0
200
400
600
800
1000
1200
1400
1600
IgM PAC-1 PAC-
1+DDT
Co
un
tes o
f C
ell B
ind
ing
PA
C-1
0
0.2
0.4
0.6
0.8
1 GFP
NM
B
Expression of the N-terminal radixin promotes integrin
aggregation activity
(a) Organization of the
ERM family.
Share a ~300 aa domain involved both in the
morphogenesis of membrance
structure on which they are
concentrated and in cell adhesion
Ezrin, substrate of EGF receptor
tyrosine kinase
Radixin, F-actin barbed end
capping protein
(b) Mapping of binding sites
for ERM-interaction partners.
(Trends in Cell Biology 2003)
Ezrin localization
in human adenocarcinoma
A431cells.
A full-length ezrin–GFP
fusion protein expressed
transiently, appears yellow
in cells that were fixed,
permeabilized and stained
with antibody against ezrin
(red). Ezrin–GFP as well
as endogenous ezrin
localize in actin-rich cell-
surface membrane
structures.
Moesin and radixin
localize similarly, ERM
bind to the plasma
membrane through the
FERM domain
(Paul M, et al. 2003)
Possible conformations of ERM
Single phosphorylation of a conserved C-terminal Thr residue
Dimers and oligomers are physiological forms of ERM molecules found associated at the membrane level
The activation ERM resulting in unfolding and subsequent N–C ERMAD association
A fold cytosolic
ERM is unable
to associate
with membrane
and
microfilaments
C-terminal Thr- P
Activated forms of
ERM might contol
assemble of actin
microfilaments
Radixin recognizes the membrane-proximal region
of the integrin b2 cytoplasmic tail
sb2CTD31:
Bo
un
d r
ad
ixin
N-E
RM
AD
(A
550)
0.0
0.2
0.4
0.6
0.8
1.0
1.2
1.4
WT CTD19 CTD sCTD BSA
Peptide added (M)
0 100 200 300 400
Bo
un
d r
ad
ixin
N-E
RM
AD
(A
550)
0.0
0.5
1.0
1.5
2.0
DMSO
b2CTD31
GST
sb2CTD31
CWKALIHLSDLREYRRFEKEKLKSQWNNDNPLFKSATTTV M N PKFAES WT b2CT:
CWKALIHLSDLREYRRFEKEKLKSQWNND b2CTD19:
CLYRLEWFHAILRSRKD CWKALIHLSDLREYRRF b2CTD31:
723
|
750
|
738
| I II III
A
B C
Radixin Binding on Integrin β2 Cytotail
0
0.2
0.4
0.6
0.8
1
1.2 NR + beta 2 tail
CR + beta 2 tail
NR + alpha M tail
CR + alpha M tail
21 11 5 2.5
Concentration of β2/αM cytotail (nM)
Interaction of N, C-terminal Radixin with
Integrin β2 Cytotail
2
Radixin(nM) vs NR(aMtail) Kd=1.4*10
Radixin(nM) vs 5CR(aMtail) Kd=5*10
Radixin(nM) vs NR(b2tail) Kd=3.2*10
Radixin(nM) vs CR(b2tail) Kd=3.2*10
2
6
Radixin fragment added (nM)
0 50 100 150 200 250
Bo
un
d r
ad
ixin
fra
gm
en
ts (
A550
)
0.0
0.2
0.4
0.6
0.8
1.0
1.2
1.4
Effect of C-radixin on interaction of
N-radixin with integrin tail
Bo
un
d r
ad
ixin
N-E
RM
AD
(A
550
)
0.0
0.1
0.2
0.3
0.4
0.5
0.6
C/N Ratio: 0:1 2:1 4:1
the b2 peptide
the M
peptide
F
N-ERMAD (1-297) C-ERMAD (281-583)
FERM -helix CTD F
Radixin N-ERMAD interacts with the integrin b cytoplasmic tail.
Expression of the N-terminal radixin promotes integrin
adhesive activity
Ce
ll a
dh
es
ion
(A
57
0)
0
1
2
3
4
5
GFP N-CRMAD
clone 6
N-CRMAD
pool
C-CRMAD
pool
N-CRMAD
pool +EDTA
A B
Expression
of the N-
terminal
radixin
promotes
integrin
adhesive
activity
Cytohesin-1 and radixin N-ERMAD recognize overlapping
regions of the b2 cytoplasmic tail
Peptide added (M)
0 20 40 60 80 100
Bo
un
d c
yto
hesin
-1 (
A550)
0.0
0.5
1.0
1.5
2.0
2.5DMSO
b2CTD31
GST
sb2CTD31
SW63
Cytohesin-1 (M)
0 2 4 6 8 10 12
Bo
un
d r
ad
ixin
N-E
RM
AD
(A
550)
0.0
0.1
0.2
0.3
0.4
0.5
0.6
A B
The integrin β tail plays a central role in
the activation process, by undergoing
regulated interations with cytoplasmic
proteins
“Inside-out”
Signaling Conformational Clusterin
changes
Cytohesin-1, a PIP3-
regulated adaptor molecule
for LFA-1 (CD11a/CD18, αLβ2)
activation
Cytoskeleton (αIIbβ3)
PAK1 Rhok Cytohesin-1 Talin F3
?
GTP (active) Lipid (PIP2,PIP3)
rho rac cdc42 GDP
PI-3K MAPK
PKC G-protein
Growth factors CD19
Cytokines
N-Radixin
Rho GDI
ACKNOWLEDGEMENT
Li Zhang
Yumei Xiong
Min Xu
Driss Ehirchiou
Ying Xiong
Yasuo Miura