Different adjuvanted pediatric HIV envelope vaccines induced distinct plasma antibody responses despite similar B cell receptor repertoires in infant rhesus macaques

Berendam, Stella J.; Morgan-Asiedu, Papa K; Mangan, Riley J.; Li, Shuk Hang; Heimsath, Holly; Luo, Kan; Curtis, Alan D.; Eudailey, Joshua; Fox, Christopher B.; Tomai, Mark A.; Phillips, Bonnie; Itell, Hannah L.; Hudgens, Michael G.; Cronin, Kenneth; Wiehe, Kevin; Alam, S. Munir; Rompay, Koen K. A. Van; Paris, Kristina De; Permar, Sallie R.; Moody, M. Anthony; Fouda, Genevieve G.

doi:10.1371/journal.pone.0256885

Cited by 2 publications

(1 citation statement)

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“…Innate immunity is a crucial part of the infant immune system since, given the limited exposures to antigens in utero, infants must rely on their innate responses for their protection [31][32][33][34]. Innate immune cells in early life exhibit distinctive cytokine profiles, characterized by lower levels of proinflammatory cytokines and higher levels of immunoregulatory and anti-inflammatory cytokines, fostering a tolerogenic environment [35]. Neonatal NK cell frequencies are comparable to those in adults [13,36].…”

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confidence: 99%

Comparative Analysis of Within-Host Dynamics of Acute Infection and Viral Rebound Dynamics in Postnatally SHIV-Infected ART-Treated Infant Rhesus Macaques

Mainou,

Berendam,

Obregon-Perko

et al. 2024

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Viral dynamics of acute HIV infection and HIV rebound following suspension of antiretroviral therapy may be qualitatively similar but must differ given, for one, development of adaptive immune responses. Understanding the differences of acute HIV infection and viral rebound dynamics in pediatric populations may provide insights into the mechanisms of viral control with potential implications for vaccine design and the development of effective targeted therapeutics for infants and children. Mathematical models have been a crucial tool to elucidate the complex processes driving viral infections within the host. Traditionally, acute HIV infection has been modeled with a standard model of viral dynamics initially developed to explore viral decay during treatment, while viral rebound has necessitated extensions of that standard model to incorporate explicit immune responses. Previous efforts to fit these models to viral load data have underscored differences between the two infection stages, such as increased viral clearance rate and increased death rate of infected cells during rebound. However, these findings have been predicated on viral load measurements from disparate adult individuals. In this study, we aim to bridge this gap, in infants, by comparing the dynamics of acute infection and viral rebound within the same individuals by leveraging an infant nonhuman primate Simian/Human Immunodeficiency Virus (SHIV) infection model. Ten infant Rhesus macaques (RMs) orally challenged with SHIV.C.CH505 375H dCT and given ART at 8 weeks post-infection. These infants were then monitored for up to 60 months post-infection with serial viral load and immune measurements. We use the HIV standard viral dynamics model fitted to viral load measurements in a nonlinear mixed effects framework. We find that the primary difference between acute infection and rebound is the increased death rate of infected cells during rebound. We use these findings to generate hypotheses on the effects of adaptive immune responses. We leverage these findings to formulate hypotheses to elucidate the observed results and provide arguments to support the notion that delayed viral rebound is characterized by a stronger CD8+ T cell response.

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