Investigation of Immune Interventions in SIV-Infected, ART-Treated Infant Rhesus Macaques Öffentlichkeit

Abstract

The latent viral reservoir is composed of a small subset of infected CD4+ T cells that persist during antiretroviral therapy (ART) and constitute the major barrier to HIV-1 cure. Strategies to reduce or eliminate this reservoir would be highly beneficial to the 1.7 million children living with HIV-1. Here, we used a non-human primate (NHP) model of postnatal oral SIVmac251 transmission and ART suppression to investigate potential cure interventions in a preclinical pediatric model of HIV-1 infection.

First, we evaluated safety and immunogenicity of the toll-like receptor (TLR)-7 agonist, GS-986, in 2 SIV-infected, ART-treated infant rhesus macaques (RMs). We found that oral administration of GS-986 at both tested concentrations was tolerable and resulted in a dose-dependent pharmacodynamic response detectable through increased concentrations of plasma cytokines and chemokines, such as IFN-𝛾 and increased circulating nonclassical monocytes (CD14+CD16+) and circulating macrophages (CD14+CD169+) at 24 hours post-administration.

We next combined GS-986 with an Ad48-prime, MVA-boost therapeutic vaccine in 8 SIV-infected, ART-treated infant RMs. Immunized infants had augmented anti-SIV cellular and humoral immunity. Repeated oral GS-986 induced the expected pharmacodynamic response with activation of monocytes and T cells in the periphery 24-hours post-dose. Despite the vaccine-induced immune responses, vaccination did not result in reductions to the viral reservoir through cell-associated SIV DNA or rebound kinetics following the removal of ART.

Finally, we examined the effect of a newly identified latency reversing agent (LRA), the mimetic of second mitochondrial activator of caspases (SMACm) AZD5582, in 8 SIV-infected, ART-suppressed infant RMs. Latency reversal, measured by on-ART viremia, was observed in 63% of infants. Immunogenicity of AZD5582 was demonstrated through T cell activation and increased transcription of ncNF-kB genes, such as BIRC3. Quantification of plasma AZD5582 revealed a lower Cmax in infants compared to adult RMs which may, in part, explain the dampened viremia.

Taken together, these findings hold promise for pediatric HIV-1 cure strategies and inform future pediatric clinical trials. Additionally, these studies highlight the importance of studying HIV-1 cure in a pediatric setting as unique features of the pediatric reservoir and/or the developing immune system may influence the efficacy of HIV-1 cure interventions.

Table of Contents

Table of Contents

Chapter One: Introduction        1

Discovery and Origins of HIV-1/AIDS  1

Virology and HIV-1 Life Cycle 2

Transmission and Pathogenesis of HIV-1          5

The Immune Response to HIV-1           8

Non-human Primate Models     10

Antiretroviral Therapy  12

The Viral Reservoir      14

Strategies for HIV-1 Cure         16

Pediatric HIV-1 21

Chapter 1 Summary     29

Chapter 1 Figures         31

Chapter Two: Oral TLR7 Agonist Administration Induces an Immunostimulatory Response in SIV-Infected ART-Suppressed Infant Rhesus Macaques     32

Abstract           33

Author Summary         34

Introduction     35

Results 38

Discussion       43

Materials and Methods 45

Chapter Two Figures    50

Chapter Three: Therapeutic vaccination of SIV-infected, ART-treated infant rhesus macaques using Ad48/MVA in combination with TLR-7 stimulation   57

Abstract           58

Author summary          60

Introduction     61

Results 64

Discussion       74

Materials and Methods 80

Chapter 3 Figures         89

Chapter Four: Altered response patterns following non-canonical NF-B activation in SIV-infected, ART-suppressed rhesus macaque infants       112

Abstract           113

Author Summary         114

Introduction     115

Results 118

Discussion       126

Materials and Methods 131

Chapter 4 Figures         140

Chapter Five: Discussion          153

List of Abbreviations    165

References       166

About this Dissertation

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School	Laney Graduate School
Department	Biological and Biomedical Sciences
Subfield / Discipline	Immunology and Molecular Pathogenesis
Degree	Ph.D.
Submission	Dissertation
Language	English
Research Field	Health Sciences, Immunology
Stichwort	HIV-1 pediatric HIV nonhuman primates
Committee Chair / Thesis Advisor	Ann Chahroudi, Emory University
Committee Members	Jens Wrammert, Emory University Cynthia Derdeyn, Emory University Rama Amara, Emory University Mirko Paiardini, Emory University

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