Post on 16-Jan-2016
1
Cholinergic anti-inflammatory signaling
through α7 nAChR
Talma Brenner Department of Neurology
Hadassah University HospitalJerusalem, Israel
2
Α 7 nicotinic acetylcholine receptor
• The α 7nAChR an anti-inflammatory target in macrophages and T-cells (B-cells)
• α 7nAChR presence on immune cells may explain epidemiological data claiming link between cigarette smoking and several inflammatory disorders (ulcerative colitis, sarcoidosis)
• Animal studies show that nicotine is active in reducing Ab production and in signaling through the TCR
• Involvement of the immune cholinergic system in the regulation of autoimmune responses
33
Non-neuronal immune cholinergic
system
• Synthesis of ACh• Expression of the enzyme cholineacyltransferase (ChAT)• Response to cholinergic signals;
muscarnic and nicotinic• Expression of α7 nicotinic
acetylcholine receptor (AChR)• Termination of cholinergic signals is
mediated by AChE
44
nAChR – structure and function• Neuronal nAChR are pentameric extracellular complexes of α
and β subunits that form a ligand gated ion channel. (9 α and 4 β subunits).
5
Neuro-immune interactionsNeuro-immune interactions
** The nervous The nervous system is a major system is a major producer of ACh, the producer of ACh, the immune cholinergic immune cholinergic system can mediate system can mediate neuro-immune neuro-immune interactions interactions
** or serve as an or serve as an internal regulator of internal regulator of immune responsesimmune responses
** αα7nAChR on 7nAChR on macrophages and T-macrophages and T-cells can be anti-cells can be anti-inflammatory targetinflammatory target
66
Neuroimmune interactionsNeuroimmune interactions((The cholinergic anti-inflammatory The cholinergic anti-inflammatory
surveillance)surveillance)
(Ulloa, 2007)
7
AChE: Termination of cholinergic signalingAChE: Termination of cholinergic signaling
G4
G2 G1
A12 G2 G1
8
AChE Inhibitors (AChEI)AChE Inhibitors (AChEI)
* Clinical indications: Alzheimer’s * Clinical indications: Alzheimer’s Disease (AD) and Myasthenia Gravis Disease (AD) and Myasthenia Gravis (MG).(MG).
* Inhibitors of AChEI enzymatic activity * Inhibitors of AChEI enzymatic activity (Conventional): Donepezil, (Conventional): Donepezil, Rivastigmine, Tacrine, Pyridostigmine Rivastigmine, Tacrine, Pyridostigmine and Edrophonium.and Edrophonium.
* Inhibitors of AChE synthesis: EN101, * Inhibitors of AChE synthesis: EN101, anti-sense targeted to exon 2 of the anti-sense targeted to exon 2 of the AChE mRNA.AChE mRNA.
9
Anti-sense directed to ACHE mRNA Anti-sense directed to ACHE mRNA (EN101) treatment in experimental MG(EN101) treatment in experimental MG
Brenner et al FASEB J.
10
Oral EN101 improves decremental response in EAMG rats
Brenner et al FASEB J.
11
Chronic EN101 Retards EAMG Progression
-15
-10
-5
0
5
10
15
Wei
gh
t ch
ang
e
( g )Saline Mestinon EN101
Body Weight
0
0.5
1
1.52
2.5
3
3.5
4
4.5
Cli
nic
al
sco
re
Before Saline Mestinon EN101
Disease Severity
0
50
100
150
200
250
300
350
Ru
nn
ing
tim
e
( sec
)
Before Saline Mestinon EN101
Stamina
0
20
40
60
80
100
30- d
ay s
urv
ival
(%)
Saline Mestinon EN101
Survival
12
Suppression of Anti-AChR abs and muscle chemokine/chemokine receptor by chronic EN 101 in
EAMG rats
0
20
40
60
80
Saline
0
4
8
12
16
20
0
4
8
12
16
Anti-rat-AChR abs
CXCR3 expression (muscle)
IP10 expression (muscle)
ControlEAMG EAMG+EN101
ControlEAMG
*
*
**
Pmole/ml
EAMG+EN101
AU
Control EAMG EAMG+EN101
*
**
13
EN 101 in phase Ib in MGEN 101 in phase Ib in MG
Baseline
On EN101 500 µg/kg,
day 2
4 wk after treatment
-7
-6
-5
-4
-3
-2
-1
0
3.5hafterfirst
dose
3.5hafter2nddose
3.5hafter3rd
dose
Day 2 Day 3 Day 4 Day 5 Day 6
Day
Mea
n C
han
ge
Mean change in QMG
Argov et al
1414
Our working hypothesis :
Activation of the 7 nAChR has anti-inflammatory effects
7 nAChR
ACh
Cholinergic up-regulation by inhibition of (extra-cellular) AChE can activate the 7 nAChR
7 nAChR
ACh
AChEAChE
AChE
AChE
AChE
AChE
AChEI
15
0.0
0.1
0.2
0.3
0.4
0.5
0.6
0.7
0.8
0.9
1.0
5 10 15 25 30
Minutes in Substrate
Rel
ativ
e A
chE
Act
ivity
(O
.D. 4
05nm
)
PHA
PHA+EN101 1µM
PHA+EN101 2µM
PHA+edrophonium 0.5µM
PHA+edrophonium 1µM
Reduction in AChE activity inthe extracellular medium of
proliferating T-cells by AChEI
7 nAChR is specifically up-regulated during
T-cell activation
1616
7 nAChR involvement in T-cell proliferation
cholinergic up-regulation inhibits T-cell proliferation and can render activated cells to be more sensitive to nicotinic
agonists
Nizri et al Neuropharmacology 2006
17
Attenuation of pro-inflammatory Attenuation of pro-inflammatory cytokine production by cytokine production by 7 nAChR 7 nAChR
activationactivation
Nizri et al Neuropharmacology 2006
18
Expression of α7 nAChR by CD4+ T-cells: increase by stimulation and inhibition by α7
AS
Isolated CD4+ cells stained with FITC αbgtx Nizri et al J. Immunol 2009
19
Cells positive for α-Bgtx are activated cells in replication
20
Up-regulation of α7nAChR in EAMG mice by
Torpedo-AChR
0
0.5
1
1.5
2
2.5
3
3.5
4
ctl torpedo
fold
of
ch
an
ge
2121
What is so special about What is so special about 7 nAChR?7 nAChR? CD3 and 7 nAChRs coimmunoprecipitate
(Razani-Boroujerdi , 2007)
22
23
Treatment control rivastigminerivastigmine+Mecamyl.
Mean severity 3 .4± 0.4 1.7 ± 0.3 * 2.9 ± 0.1
Cumulative score# 70.4 ± 4.8 32.4 ± 2.7 * 50.8 ± 4.2 *
Attenuation of EAE by AChEI Attenuation of EAE by AChEI (rivastigmine)(rivastigmine)
Delivery by mini osmotic pumps
Inhibition of AChE activity: Brain 56%, Muscle 42%
Subcutaneous daily injection
Treatment control rivastigmine
Mean severity 2.2 ± 0.4 0.6 ± 0.1**
Cumulative score# 48.8 ± 5.1 13.5 ± 5.8***
Nizri et al .J Neuroimmunology, 2008
24
Histological preservation of Histological preservation of the CNS following AChEI the CNS following AChEI
treatmenttreatment
Nizri et al J. Neuroimmunology, 2008
25
Quantification of histopathological Quantification of histopathological parametersparameters
Pathologicalparameter
control (n=6) rivastigmine (n=7)
InflammationDemyelinationAxonal damage
2.3 ± 0.491.8 ± 0.471.8 ± 0.37
0.71 ± 0.45*0.71 ± 0.24*0.57 ± 0.35*
26
The inflammatory demyelinating lesions in EAE and MS
27
Reduction of Th1 and Th17 activity by Reduction of Th1 and Th17 activity by AChEI treatmentAChEI treatment in MOG-specific T- in MOG-specific T-
cellscells
28
AChEI treatment affect antigen AChEI treatment affect antigen
presentationpresentation
29
Direct signaling of α7 nAChR by nicotine
3030
Signaling downstream of Signaling downstream of 7 7 nAChRnAChR
3131
Inhibition of Signaling Inhibition of Signaling downstream of downstream of 7 nAChR7 nAChR by nicotine by nicotine
Nizri et al 2009
3232
Direct activation of 7 nAChR by nicotine
control nicotine p
cumulative score 70±8.2 17±7.1* 0.0011
mean severity 3.3±0.4 0.8±0.1* 0.0001
onset 16 15.7 0.02
Nizri et al J. Immunology 2009
33
Improved histophatological parameters under nicotine
treatment Demyelination Microglial activation Axonal damage
PBS
Nicotine
34
Reduced CD4 and CD11b cells in the CNS of
EAE mice treated with nicotine
35
Nicotine treatment was associated with reduced T-cell reactivity
36
Disease Mean severity
WT 3.3±0.4Α7-/- 1.5±0.2Α7 -/- w nicotine 1.4±0.1
Α7 KO mice develop milder EAE without response to nicotine treatment
37
Altered T-cell reactivity in α7 nAChR KO, lack of response to nicotine and reduction in antigen
presentation
38
Does nicotine posses anti-Does nicotine posses anti-inflammatory effectsinflammatory effects??
• Invasive pneumococcal disease is more prevalent in smokers (Nuorti, 2000). Nicotine increases intracellular replication of Legionella (Matsunaga, 2001).
• Smoking AD patients have reduced levels of Aβ 40 and Aβ 42 (Hellstrom-Lindahl, 2004).
• Smoking protects against UC (Rubin and Hanauer, 2000). Clinical trials with nicotine in TDP reduced UC severity (Van Assche, 2005).
39
History may be revealingHistory may be revealing……
40
Inhibition of AChE by Rivastigmine Inhibition of AChE by Rivastigmine reversed cognitive impairment reversed cognitive impairment
associated with EAEassociated with EAE
clinical signs
0 7 14
Assay periodinduction
41
EAE is associated with inflammatory infiltrates near the
hippocampus
4242
Cognitive dysfunction in MS
• Most MS patients develop cognitive dysfunction (memory, attention, information processing and verbal fluency).
• These patients are more prone to develop affective disorders (Gilchrist and Creed, 1994).
• Immunmodulatory treatment can slow the cognitive decline in MS, there’s still a need for symptomatic treatment (Henze, 2006).
• AChEI are prescribed for cognitive dysfunction in AD. Recent evidence pointed to their efficacy in MS patients (Krupp 2004).
43
44
Conclusions IConclusions IThe immune cholinergic system can The immune cholinergic system can be harnessed for immunomodulationbe harnessed for immunomodulationProposed mechanism involves Proposed mechanism involves activation of activation of αα7 nAChR7 nAChRCholinergic up-regulation by AChEI Cholinergic up-regulation by AChEI treatment results in reduction of treatment results in reduction of neuroinflammation, amelioration of neuroinflammation, amelioration of EAE and improvement of cognitive EAE and improvement of cognitive deficit deficit AChEI mediate anti-inflammatory AChEI mediate anti-inflammatory effects; Suppression of T-cell effects; Suppression of T-cell activities, proliferation, pro-activities, proliferation, pro-inflammatory cytokine productioninflammatory cytokine production
45
Conclusions IIConclusions II
αα7 nAChR is expressed on CD47 nAChR is expressed on CD4++ cell surface. cell surface. Expression increases following stimulationExpression increases following stimulation
Nicotine treatment suppressed EAENicotine treatment suppressed EAE
Nicotine treatment reduced T-cell reactivity, Th1 Nicotine treatment reduced T-cell reactivity, Th1 and Th17 activity and implicated a skew towards and Th17 activity and implicated a skew towards Th2 with inhibition of NFkb induced signalingTh2 with inhibition of NFkb induced signaling
Effects of nicotine are Effects of nicotine are αα7 nAChR dependent 7 nAChR dependent
Differential responses of Differential responses of αα7 nAChR7 nAChR-/--/-cells; cells; impairment in antigen presentation and impairment in antigen presentation and increased T-cell proliferation increased T-cell proliferation
46
Thanks Lab members • Eran Nizri• Michal Irony-Tur-
Sinai• Yasmine Hamra-
Amitay• Neli Boneva• Camille Sicsic• Omer Lori• Hodaya Hadad
Collaborators • M. Rosin• E. Lavi• S. Berrih-Aknin• H. Soreq• O. Abramsky
• Ester\ Neuroscience
• AFM• Israeli Ministry of
Health chief scientist fund