Post on 04-Jul-2020
Immune Reconstitution :
Quantitative and Qualitative aspects
B.A. Jni07
Pr Brigitte Autran, Hôpital Pitié-Salpétrière, Université Paris -VI
The 3 phases of the ART-induced immune reconstitution : the 1997-2000 years
1. Early Memory CD4 T cell Redistribution : « Fake » quantitative restoration of CD4 counts but no functionnal restoration
2. Decreased activation with virus control : allows functional restoration3. Late Naive T cell regeneration > long term CD4 T cell quantitative
expansion and Restoration of defenses against OI (Autran 97, Pakker 98, Li 98, Lederman 98, Bucy 98, Gorochov 98….)
Months3 6 9 12 18
CD4
Memory CD4+
Naive CD4+
50
100
0
150
Cel
ls/µ
l
HIV
Activation
B.A. Jni07
Quantitative and functional CD4 cell reconstitution with HAART
300 patients treated with HAART, viral loads <200 copies/ml
CD4 counts
0
200
400
600
800
0 8 16 24 32Months
Cel
ls/m
m3
Rapid CD4 counts restoration in end stage disease with high risk of CMV retinitis
0
10
20
30
40
50
60
70
0 1 3 6 9 12%
pos
itive
resp
onse
s
CMV Tuberculin
Months
Restoration of proliferative CD4 responses to CMVin end stage disease(Autran 97, Li 98, Lederman 98, Rinaldo 99,
Similar prognostic significance of CD4 counts during disease and immune reconstitution
Schematic prediction of Time to restore normal CD4 counts acording to CD4 cell depletion at time of ART initiation
(B Autran et al. 1998)
BA/11.98
8 years4
600
200
CD
4 co
unts
Normal1-22 - 3
5 - 67 - 10
> 10
2 4 6 8 10
6 - 84 - 5
HAART
Factors influencing quantitative CD4 T cell reconstitution:• Positively: - amplitude of HIV control at initiation of ART
- rapid CD4 decrease before ART initiation (Renaud et al, 1999)
• Negatively: - outbreaks of virus replication (blips, STI) (Bategay, 2006)
- HCV co-infections (Koziel 2007)
- X4 virus tropism for naive CD4 T cells (Delobel, 2006)BA JNI2007
Schematic prediction of Time to restore normal CD4 counts acording to CD4 cell depletion at time of ART initiation :
Where are we today ?
BA/11.98
8 years4
600
200
CD
4 co
unts
Normal1-22 - 3
5 - 67 - 10
> 10
2 4 6 8 10
6 - 84 - 5
HAART
BA JNI2007
Do drugs influence the quantitative CD4 T cell reconstitution:• Similar Immune restoration with PI sparing and PI
containing regimens (INITIO)(Samri et al. Antiviral Ther. 2007)
• Do new drugs generate a distinct profile of immune restoration ???• entry inhibitors ?• integrase inhibitors ?
Restoration of Immune Defenses against pathogens with ART
Restore defenses to all pathogens (Autran97; Li98, Lederman 98, Rinaldo 99,
Garcia 99, Pontesili99……
Allow arrest of prophylaxis against Opport. Inf (Furrer,99 Reiss 99,Ledereberger 01, Jouan 01..)
Months
50
100
0
150
Opp
ortu
nist
ic P
atho
gens
5
4
3
2
Plas
ma
HIV
RN
A
Memory Cells/ Opportunistic Pathogens
3 6 12 24 48
Naive Cells / Any Pathogens
B.A. Jni07
Recovery of Memory CD4+ T cell reactivity to CMV allows control of CMV viremia with HAART
1
10
100
0 1 2 3 4 5 6 7 8 9 10 11 12 13
Months
Sti
mu
lati
on
ind
ex
anti
-CM
V
2
3
4
5
HIV
RN
A (
log
co
pie
s/m
l)
CMV viremia
HIV viral load
CD4 counts
Stimulation index anti-CMV
Positive CMV viremia
21
206
230
Li et al. AIDS Res. Retrov., 99
Restoration of a CMV-specific T cell reactivity with HAART allows to withdraw prophylaxis against
CMV retinitis in advanced disease
0
20
40
60
80
100
0 4 8 12 16 20Months
% re
spon
ses
to C
MV
0
100
200
300
400
med
ian
CD
4/m
m3
HAART
CMV prevention
47 patients:
Withprior CMV retinitis,
2 relapses after arrest of anti-CMV therapy, Jouan et al, AIDS, 2001
• Benefits from HAART: => Restoration of CD8 T cell-mediated Immune protection
against CMV retinitis:
=> Comparison of the CMV-specific CD8 T cell magnitude, repertoire breadth and differentiation in:
HN: Healthy HIV- (n=11)LTNP : HIV+HCMV+ Long Term Non Progressors (n=10), med CD4: 733/mm3
HIV+ Recovering from CMV retinitis on ART, after stopping GCV :- Short Term Recovery (18 months, n=8) : CD4:357/mm3- Long Term Recovery (>50 months, n=6) :, med CD4: 345/mm3
Acute CMV retinitis : (n=8) : med CD4:50/mm3K Sacre et al. J Exp Med 2005
Restoration of T cell-mediated immune protection against CMV disease
Short Term Recovery of strong responses against the CMV early IE1 antigens after CMV retinitis
HCMV-specific SFC/million PBMC per subject
HN LTNP STRR LTRR AHCMV
0
2000
4000
6000
8000
10000
pp65
p=0.02
0
2000
4000
6000
8000
IE1
K Sacre et al, J Exp Med 2005
HealthyCMV+
HIV-negative
HIV infectionHealthy
CMV +CMV
retinitis
Recovery from CMV retinitis
EARLY LATE
Magnitudeof HCMV-specific CD8 T cells
per target antigen
CD4 counts
Repertoire & diversity of CMV-specific CD8 T cells
against pp-65 IE1
Differentiationof HCMV-specific CD8 T cells
% CD27-28-% CD27-/+28+% CD27+28+
Naive
CMV Replication(detection threshold)
Sacre et al. , JEM 2005
Restoration of Immune Protection against CMV retinitis in HAART treated patients
HAART
Sequential Restoration of Immune protection against opportunistic pathogens
• CMV retinitis:– Loss of CD4 responses to HIV => Limited repertoire & diversity of short-
lived anti-CMV CD8 T cells => Loss of CMV control– Gancyclovir: control of CMV replication
BUT no restoration of immunity to CMV
• HAART:– Controls HIV =>Restores CD4 counts
• Restores protective Immunity against CMV:– CD4 responses to CMV– CD8 cells to CMV –IE1 antigens
» Large breadth and diversity» long-lived memory CD8 T cells
=> Restores Long Term control of CMV without gancyclovirB.A. Jni07
Reduction in morbidity / mortality (Hogg, 97, Pallella,98…
Discontinuation of prophylaxis against Opportunistic Infections: PCC. Pneumoniae, CMV retinitis (Furrer,99, Jouan 2001…)
at all stages of the disease : illustrating the lack of definitive immune alterations
BUT Induces the Immune Restoration Syndrome (IRS,.)M French , 98, 2006, Monsuez 99, Breton 2005……….
- during opportunistic infections concommitantly treated with HAART
- reactivation of pathogen-associated symptoms +/- systemic inflamatory
syndrome without microbiological relapse, or of auto-immune diseases
- particularly frequent during mycobacterial infections (MAI, TB : 40%)B.Autran, BA, 01
Rapid restoration of protective memory responses against opportunistic pathogens with HAART
B.A. Jni07
TB and VIH
IFNγ
CD4 CD4-/8-CD8 TgdTNFα
Disparition of Ag-specific responses,
= Anergy to TB antigens
Consequences of CD4 defects in HIV infection:Poor Granuloma, without caseum, poorly functionalsDisseminated pauci-symptomatic Tuberculosis
Activation macrophage
Activation CD4 Th1
IFNγIL12
• Diminution Nb activated macrophages• Diminution of intra-cellular BK lysis
A. Bourgarit 05
IRS: Hypothesis
Activation macrophage
Activation CD4 Th1
IFNγIL12
IFNγ
CD4 CD4-/8-CD8 TgdTNFα
Rapid restoration of TB Ag- spécific Th1 cells???
Rapid Restoration of CD4 counts and function with HAART=> Amplification +++ of the specific CD4 Th1 cells to Mtb => inflammatory Syndrome « cytokine Storm »
A. Bourgarit 05
TBK M0ART M1ART
M3
M6 M12BK
ConfirmationOf inclusion Declaration IRS+
TSRP TSRP+20j
Declaration IRS -
BK+ SRP
ØSRP
ANRS EP-21: PARADOX-TB:A prospective analysis of the Immunological
characteristics of the TB-associated IRS
Bourgarit et al. AIDS, 2006
IRS+ IRS- pn 11 13M/F 6/5 9/2 NSAge 38 (30-56) 36 (26-63) NSPulmonary TB 2/11 4/13 NSDisseminated TB 9/11 9/13 NS
BAAR+ 3/8 4/13 NSHIV Infection CD4 (/mm3) 26 (6-145) 54 (15-267) NS
CV (Log) 6 (4.8-6.5) 5.2 (4.3-8) NS
M0HAART Délai /TBK (j) 36 (7-77) 50 (14-111) NS
IRS Délai / M0 (j) 23 (7-85)CD4 108 (59-430) 163 (9-580)(M1) NS∆CD4 /M0 (/mm3) +54 (-1;+393) +77 (-50;+250) NS
M3 CD4 117 (58-399) 132 (49-410) NS∆CD4 /M0 (/mm3) +86 (-74;+367) +73 (-88;+354) NSCV <200 7/10 8/11 NS
ANRS EP-21: PARADOX-TB : Patients Characteristics
Bourgarit et al. AIDS, 2006
TB-IRS: Acute Exacerbation of a Th1 response to tuberculin but not to live TB (ELISpot IFN-γ) (Bourgarit, AIDS 2006)
IRS+n=11
IRS-n=13
PPD : p =0.005
CMV = NS
T BK M 0 M1 M 3 M6 M120
1000
2000
3000
4000
T BK M 0 T IRS M 3 M 6 M120
1000
2000
3000
4000 PPD CMV
SFC/
106 PB
MC
• N IFN-g producing T cells to PPD significantly stronger in IRS +• No or weak response to to live TB-associated antigens: ESAT-6, CFP-10, 85B• Mediated by CD4 T cells: up to 35% of circulating CD4 T cells
Multiplex Detection of cytokines –Chemokines in culture supernatants (Chimioluminescence)
=> Intense inflammatory response both Ag-specific (PPD) and non specific: cytokines :TNF-a, IL-6, IL-10
chemokines: RANTES, MCP1..
-10 0 10 20 30 40 500
1000
2000
3000
4000 Medium alone CMV PPD
wks
0
10000
20000
30000
40000
50000
IL-6
pg/
ml
TNF-
α an
d IL
-1β
pg/m
l
-10 0 10 20 30 40 500
1000
2000
3000
4000 Medium alone CMV PPD
wks
0
10000
20000
30000
40000
50000
TNF-
α an
d IL
-1β
pg/m
l
IL-6
pg/
ml
IRS+ IRS-
ANRS EP-21: PARADOX-TB :Non PPD-specific pro-inflammatory cytokine storm during IRS
Bourgarit et al. AIDS, 2006
Paradox-TB: A prospective study of the Immune Restoration Syndrome
associated with TB in HIV infection• A frequent syndrome :
– in 40% (9/22) TB-HIV co-infected patients with severe CD4 defects and rapid CD4 restoration within 3 months after treatment initiation
• A brutal explosion of tuberculin-specific T cells– Poorly or undetectable at baseline, – Rapidly restored and exacerbated, within a month– Mediated by activated CD4 Th1 cells + γδ T cells– with specific release of Th1 cytokines and pro-Th1 chemokines
but without deregulated Th2 response– Directed against Antigens present in tuberculin – Associated to an acute non-specific inflammatory response
Bourgarit et al. AIDS, 2006
• Paradox-TB : Pending Questions > BK-VIR-IS– Clonality of the response?– Antigens involved? And role of γ-δ T cells?– Role of regulatory T cells ?– Individual susceptibility?
• Why only 40% IRs if this corresponds to a physiological restoration of tuberculin specific T cells?
– Strains ?– Host Genetic Predisposition?
» HLA» Other Genes: Th1 pathways…,
Immune Restoration Syndrome associated with TB in HIV infection
Bourgarit et al. AIDS, 2006
ANRS and Sidaction PARADOX TB Study group :
Baakili A, Béglé A-M, Besse F, Bollens D, Bouchaud O, Bursachi P, Cadranel J, Camuset J, Chakvetadze C, Delgado J, Diemer M , Dupont B, Elmarsafy S, Fain O, Fonquernie L, Furco A, Girard P-M, Grillot-Courvalin C, Guignet A, Guilleminot MC, Herrmann J-L, Jeantils V, Grivois JF, Joly V, Jouis V, Klutse P, Lacombe K, Lahoulou R, Lavolé A, Lefebvre B, Lefort A, Letellier E, Lortholary O, Metro A TrumeauM, Meynard J-L, Meyohas M-C, Molina J-M, Obenga G , Parrinello M, Pelet O, Pintado C, Ponscarme D, Rami A, Rozenbaum W, Sahli H, Sellier P, Slama L, Courtial S, Tubiana R, Stirnemann J, Tassi S , Taulera O, Touitou H , Vacher I,., Vincent F, Yeni P
Hôpital Saint Louis, Paris FranceIntern. Med.: A Bourgarit, C. Lascoux, D SereniBactériologie: P LagrangeStatistics: V Delcey Institut Pasteur: B Gicquel
Pitié-Salpétrière, Hospital, Immunology : A Bourgarit, G. Carcelain, V Martinez, A. Samri, B. Autran
CHU Pitié-Salpétrière, Univ Pierre et Marie Curie Paris, Immunology, INSERM U543 Infect. Dis. VirologyG. Carcelain, A Samri R. Tubiana V. CalvezB Combadière K Sacre M Jouan AM FilletB. Autran H. Ait Mohand AG Marcellin
C. Katlama H. Agut Statistics : C Dalban, D. Costagliola
and the RESTIMOP study groupANRS , Sidaction and INSERM ATC Immunité anti-virale