CNS Opportunistic Infections:
an update
Paola Cinque
Department of Infectious Diseases
San Raffaele Scientific Institute
Milan, Italy
HANSA Meeting
Goteborg, Sweden, 26-27 May 2011
Frequency of HIV-related CNS-D
at post-mortem examination Milano, 1985-1995
CM
V-E
HIV
-E
To
xo
PC
NS
L
PM
L
HS
V, V
ZV
TB
Cri
pto
NH
L
oth
ers
20%
10%
30%
0
Cinque P and Vago L, AIDS 1997
Incidence of CNS-D in the EuroSIDA cohort
0,01
0,1
1
10
1994 1995 1996 1997 1998 1999 2000 ≥2001
Toxo ADC Crypto
PML PBL FBL
D’Arminio Monforte et al,
Ann Neurol 2004
0,1
1
10
100
Non CNS-D
CNS-D
Positive CSF PCR findings in HIV-infected patientsSan Raffaele Hospital, Milano 1994 - 2001
5
10
15
20
100
75
50
0II/94 I/95 II/95 I/96 II/96 I/97 II/97 I/98
Total patients
EBV+
JCV+
II/98 I/99 II/99
Nu
mb
er
of
po
sit
ive
sa
mp
les
I/00
HAART
CMV
+
II/00 I/01 II/01
Prevalence of HIV-related CNS-D
IRINA cohort, Italy, 2000-2005
0
5
10
15
20
25
30
35
TE HIVE PML Others Crypto EUO PCL TB CMV NHL
P=0.048
P<0.001
P<0.001
P=0.038
naive
experienced
Months from diagnosis
5550454035302520151050
Cu
mu
lativ
e p
rop
ort
ion
su
rviv
ing
1,0
,8
,6
,4
,2
0,0
Log-rank p<0.0001
Survival of HIV-related CNS-DIRINA cohort, 2000-2005
1-year survival prob.
EUO 86%
HIVE 81%
TE 77%
Other 75%
Crypto 73%
TB 65%
PML 48%
PCL 19%
1035 patients
Mortality Hazard Risk
of AIDS-associated events (ADE) during cART
31,620 patients from 15 cohorts
2880 ADE; 377 ADE-related deaths
The Antiretroviral Therapy Cohort Collaboration, CID 2009
Productive JCV infection of the brain: PML
Important progresses in PML
• PML can be (promptly) diagnosed by clinical, neuroimaging and virological assessment
• PML can be monitored by clinical, neuroimaging and virological assessment
0
,2
,4
,6
,8
1
Cu
mu
lative
Su
rviv
al
0 10 20 30 40 50 60
Months
Historical pts
cART
PML can remit following
removal
immunosuppression, i.e.,
by initiating cART
PML: MRI presentation
HIV-related PML with atypical MRI presentation
and fatal fulminant course
March 2007: - Onset of symtpoms
April 2007: - Diagnosis of HIV infection (CD4 122; VL 182,000 c/mL)
- Diagnosis of PML (CSF JCV-DNA 1,520,000 c/mL,
confirmed by brain biopsy)
- Exitus
JCV DNA detection and quantification in CSF
0 25 50 75 100 125 150 175
1
2
3
4
5
6
7
8
9
Diagnostic sensitivity 74%
Diagnostic specificity 99%
Bossolasco et al, Clin Infect Dis 2005
Reduced diagnostic value of JCV-DNA for
PML diagnosis in the cART era
Marzocchetti A. J Clin Microbiol 2005
pre-cART post-cART p
Sensitivity % 17/19 (89.5%) 23/40 (57.5%) 0.014
Specificity % 82/83 (99%) 141/141 (100%) ns
NPV % 98 89 0.05
PPV % 95 100 ns
Diagnostic criteria for PML
In the presence of progressive uni or multifocal neurological
disease and typical MRI lesions:
• Histology-confirmed PML: brain biopsy (or post-mortem
examination) showing typical pathologic features with JCV
confirmed either by IHC or ISH
• Laboratory-confirmed PML: demonstration of JCV DNA in
CSF by nucleic acid amplification methods
• Possible PML: absence of both histological confirmation
and JCV demonstration in CSF
Cinque, Koralnik and Clifford, JNV 2002
Portegies, EJN 2004
CDC, NIH, HMA-IDSA guidelines for HIV-OIs, 2009
2
4
6
8
0 50 100 150 200
Days from first CSF sample
Lo
g C
SF
JC
V D
NA
c/m
L
2
3
4
5
6
0 100 200 300
2
3
4
5
6
0 100 200 300
HAART
progressionNo HAART
HAART
stabilization
Bossolasco et al., CID 2005
JCV-DNA level in CSF
as a marker for monitoring PML activity
August 2005 October 2005 August 2006
JCV-DNA 10,792 c/mL
CD4 495 (11%);
VL 262,000 c/mL
JCV-DNA 335 c/mL
CD4 619 (33%)
VL 4198 c/mL
JCV-DNA nd
CD4 1252 (45%)
VL <50 c/mL
ART
JCV-DNA <100 c/mL
CD4 804 (44%)
VL <50 c/mL
March 2006
JCV-DNA level in CSF in a case with favorable outcome
PML onset
JCV-DNA level in CSF in a PML case
progressing over 2.5 years
ART
onset 1.5 yr later
Some important,
unanswered questions
• Why and how a benign infection will progress
into a fatal CNS disease?
• Why will some treated HIV-infected patients
develop PML? Why only half of treated
patients will respond to cART?
• When will we have a specific treatment for
JCV infection and PML?
CNS-OIs and CNS HIV replication
Hagberg L. et al., AIDS Res Ther 2010
JCV replication
in CNS - PML
Immune
competence
Natural history of JCV infection and PML
- Urinary tract
- Bone marrow ?
- CNS ?
Loss of
immune control
JCV
reactivation
Primary
JCV infection
Persistent
JCV infection
CNS seeding ?
50-70% JCV
seroprevalence in
healthy adults
20% JCV DNA
excretion in urine in
healthy adults
• Critical for virus entry in the host cell - interaction with
sialic acid on cell receptor
• Main target for both B-cell and T-cell immune response
JCV capside viral protein-1 (VP-1)
PML-specific JCV VP-1 mutations in CSF
37/40 patients had one of 12 different PML-
specific mutations or deletions in CSF
Gorelik L. et al, JID, in press
L55, K60, S267, S269, S61, P51, H122
S61
S269
K60
S267
H122
L55
Intra-Patient Appearance of PML-Specific
VP1 Mutations
Pt Lab ID SAMPLE mutation mt clone # total clone# type
5067 CSF 122R 25 25 1A
5067 PLASMA 122R 26 26 1A
5067 URINE 0 na 11 1A
5166 CSF 269F 11 11 1Av75R
5166 PLASMA 269F 13 16 1Av75R
5166 URINE 0 na 26 1Av75R
5174 CSF 269F 27 27 1B
5174 PLASMA 269F 37 38 1B
5174 URINE 0 na 13 1B
Gorelik L. et al, JID, in press
PML onset or progression despite
succesful cART: why?
• cART immunereconstitution insufficient
or too slow?
• cART immunereconstitution
exaggerated or too fast?
• Other mechanisms?
Increased frequency of Gd-enhancing MRI PML lesions
paralleles increased ART potency
Sighinolfi et al. 2008
PML survival in the cART periodSan Raffaele Hospital, Milano 1995-2001
(n=108)
Unpublished data
Anti-JCV CD4 T cell proliferative assay
47%
32%
4%
23%
0%
20%
40%
60%
80%
100%
Bas eline W6 M3 M6
% p
ati
en
ts w
ith
po
sit
ive
re
spo
nse
P24 JCV SEB PHA
Gasnault J et al., CROI2007, Poster 379
17%
23%
27%
37%
0%
10%
20%
30%
40%
50%
Bas eline W6 M3 M6
% p
ati
en
ts w
ith
po
sit
ive
re
sp
on
se
Ove r lapping JCV VP1 - peptide s
IFN-gamma CD8 T cell ELISPOT
JCV-specific T-cell responses
in cART-treated patients with PML
Longitudinal assessment of T-cell responses
against JCV VP1-p261 in patients with active PML
cART Plex Stop IS
cART cART ongoing
Days from 1st sampling
Remission
Progression
PML onset or progression despite
succesful cART: why?
• cART immunereconstitution insufficient
or too slow?
• cART immunereconstitution
exaggerated or too fast?
• Other mechanisms?
PML, cART and
immunoreconstitution
No evidenceof PML
cART‘Unmasking’
PML-IRIS
PML diagnosedand treated
cART‘Paradoxical’
PML-IRIS
Paradoxical worsening of PML following cART
Courtesy of
Pilar Miralles, Madrid, Spain
After 12 weeks
of cARTPML onset
5-Oct-07 31-Jan-0825-Oct-07 15-Nov-07
JCV DNA n.d.
CD4 31 (3.8%);
VL <50 c/mL
JCV-DNA <100 c/mL
CD4 37
VL <50 c/mL
JCV-DNA 455 c/mL
CD4 79
VL <50 c/mL
JCV-DNA 2320 c/mL
CD4 9
VL 2930 c/mL
June ‘07
ART
HD IV
steroids
Paradoxical worsening of PML following cART and
response to corticosteroids
PML onset or progression despite
succesful cART: why?
• cART immunereconstitution insufficient
or too slow?
• cART immunereconstitution
exaggerated or too fast?
• Other mechanisms?
PML-specific treatments
• Non-recommended* – Cytarabine (AII)
– Cidofovir (AII)
– IFN (BIII)
– Topotecan (BIII)
• Use not justified in routine* – 5HT2a Inhibitors (BIII)
• Clinical trial on Mefloquine: terminated
• CMX-001 ??? (Patel A, JAC 2010)
• Immune-based interventions – Adoptive JCV-specific T-cell transfer ??? (Balduzzi A, BMT 2010)
– IL-7 ??? (Patel A, JAC 2010)
CDC, NIH, HMA-IDSA
guidelines for HIV-OIs, 2009
High CSF HIV RNA level in CNS-OIs
Hagberg L. et al., AIDS Res Ther 2010
2
3
4
5
6
Lo
g10
HIV
-1 R
NA
co
pie
s/m
l
2
3
4
5
6
2
3
4
5
6
Toxoplasmosis Cryptococcosis CMV encephalitis
Onset Onset OnsetPost-tx Post-tx Post-tx
Changes of CSF HIV RNA level
in patients with CNS-Ois
No cART, CNS OI treatment only
CNS-OIs and CNS HIV replication
• May CNS-OIs favor HIV replication?
– High CSF level due to brain barriers
dysruption?
– Other mechanisms?
• May HIV replication favor onset or
progression of CNS-OI?
Origin of high CSF HIV RNA level in CNS-Ois
(peripheral vs. intrathecal)
• CSF HIV infection seems to be compartmentalized in
a significant number of CNS-OI cases
% diversity between CSF and plasma RT sequences
Lower rate of death in treated patients
with CPE score >1.5
9932 pts with first neurological AIDS-defining event
FHDH-ANRS CO4
Lenoy et al, Neurology 2011
But loss of association if model adjusted for plasma VL
Non significantly higher incidence of CNS-D in
patients with higher CPE score
251/22356 patients who started ART (1996-2008)
UK CollaborativeHIV Cohort (CHIC) Study
Lenoy et al, Neurology 2011
CNS-OIs and HIV replication
• High CSF HIV RNA levels in CNS-OIs
• Possible synergistic effect of HIV and
opportunistic agents on the CNS
• Whether treatment of HIV CNS infection
is beneficial for care or prevention of
CNS OIs is unknown
Acknowledgements
Neurovirology Unit, ID Dept. San Raffaele Sci. Inst., Milan
• Arabella Bestetti
• Simona Bossolasco
• Manuela Testa
• Francesca Ferretti
• Annamaria Pazzi
• Ester Tuveri
• Adriano Lazzarin and colleagues from the ID Dept.
• Simonetta Gerevini (Neuroradiology)
• Manuela Nebuloni and Luca Vago, University of Milan
• Magnus Gisslen and Lars Hagberg, University of Goteborg, Sweden
• Dick Price, University of San Francisco California
• Andrea Antinori and colleagues, L. Spallanzani ID Institute, Rome, Italy
• Leonid Gorelik and staff at Biogen Idec, Cambridge, MS