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BACKGROUND • Mature dendritic cells (DCs) express high levels of peptide-MHC complexes, costimulators, and cytokines making them the most efficient antigen-presenting cells for T cell responses. (Abbas 2012) • DCs have been shown to enhance CD8+ T cell responses to consensus HIV-1 Gag peptides. (Huang 2010) Furthermore, mature DCs loaded with HIV-1 IIIb-superinfected apoptotic cells resulted in the highest IFNγ production by autologous PBMCs. (Zhao 2002) • We evaluated the safety and tolerability of a therapeutic HIV vaccine composed on autologous DCs pulsed with autologous, inactivated, HIV-1 infected apoptotic cells (DC-HIV vaccine). We also evaluated the effect of the vaccine of viral load setpoint 12 wks after treatment interruption.
DC-HIV VACCINE PRODUCTION
• Three of the ten subjects had a ≥0.4 log10 decrease in plasma HIV-1 RNA compared to their pre-treatment baseline.
21st Conference on Retroviruses and Opportunistic Infections, Boston , March 3 – 6, 2014
INCREASE IN T CELL ACTIVATION AND MDSC FREQUENCIES
CONCLUSIONS • DC-HIV vaccine was safe and well-tolerated . It did not prevent viral rebound during treatment interruption but was associated with a modest decrease in viral load setpoint 12 weeks after treatment interruption in 3/10 subjects. • Post-vaccine increase in polyfunctional CD8+ T cell response to Gag peptide was observed in only 4/10 subjects and only 1 of the 4 had a decreased viral load setpoint at primary endpoint compared to the pre-ART baseline. • Vaccination led to a modest and transient increase in T cell activation as well as in the frequency of MDSC.
ACKNOWLEDGMENTS: We would like to thank Sarah Read and Sandra Bridges from NIAID/NIH, Carol Oriss, Renee Weinman, and Chris Tripoli from the Pitt Treatment and Evaluation Unit, Patricia Peters, the staff of IMCPL at the Hillman Cancer Center, and all the study participants. This study was funded by NIH/NIAID Grant U19 AI055794.
VIRAL REBOUND FOLLOWING TREATMENT INTERRUPTION
POLYFUNCTIONAL RESPONSE TO HIV-1 GAG PEPTIDE BEFORE (LP) AND AFTER VACCINATION (ATI) AND AT 1o ENDPOINT (Endpt)
• 4/10 subjects had an increase in CD8+ T cell polyfunctional response to HIV-1 Gag after vaccination. Of these 4, only 1 had a decrease in HIV-1 RNA setpoint at primary endpoint.
STUDY SCHEMA AND DEMOGRAPHICS
DC-HIV Vaccine
Co-culture and Maturation TNFα IL1β IFNγ Poly I:C.
HIV-1 RNA 12 WEEKS AFTER TREATMENT INTERRUPTION (1o ENDPOINT)
-‐0.700
-‐0.600
-‐0.500
-‐0.400
-‐0.300
-‐0.200
-‐0.100
0.000
0.100
0.200
0.300
1 2 3 4 5 6 7 8 9 10
Log Change from Baseline
0.000 0.500 1.000 1.500 2.000 2.500 3.000 3.500 4.000 4.500 5.000 5.500 6.000
Subj 7
Subj 8
Subj 9
Subj 10
0.000 0.500 1.000 1.500 2.000 2.500 3.000 3.500 4.000 4.500 5.000 5.500 6.000
Subj 4
Subj 5
Subj 6
0.000 0.500 1.000 1.500 2.000 2.500 3.000 3.500 4.000 4.500 5.000 5.500 6.000
Subj 1
Subj 2
Subj 3
On ART
ART stopped
LP ATI Endpt Subj LP Endpt ATI
monofunctional
polyfunctional: IFNγ, TNFα, IL2, MIP1B, CD107a
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Subj
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI Timepoint: Endpt
Timepoint: LP Timepoint: ATI Timepoint: Endpt
1
2
3
4
5
6
7
8
9
10
LP – leukapheresis ATI – analytic treatment interruption see study schema for timeline
• 2/10 subjects had detectable plasma viremia (using a commercial assay) as early as 2 weeks after treatment interruption. • At 6 weeks after treatment interruption, all subjects had detectable plasma viremia.
p=0.006
p=0.09
p=0.02
p=0.007
p=1.0
p=0.03
• CD4+ and CD8+ T cell activation levels increased after the first vaccine dose. These returned to baseline by the time of treatment interruption (ATI) • There was a modest increase in myeloid-derived suppressor cells (MDSC) frequency after the three vaccine doses (ATI).
Vaccination with Autologous Dendritic Cells Pulsed with Autologous HIV-Infected Apoptotic Cells
Bernard JC Macatangay1, Sharon A Riddler1, Nicole D Wheeler1, Mary J Buffo2, Aarika Yates3, Luann Borowski3, Theresa L Whiteside2 and Charles R Rinaldo3
1University of Pittsburgh School of Medicine, 2Hillman Cancer Center, University of Pittsburgh 3University of Pittsburgh Graduate School of Public Health
p=0.04
p=0.43
p=0.13
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