Dengue vaccine–induced CD8+ T cell immunity confers protection in the context of enhancing, interfering maternal antibodies
Jian Hang Lam, Yen Leong Chua, Pei Xuan Lee, Julia María Martínez Gómez, Eng Eong Ooi, Sylvie Alonso
Jian Hang Lam, Yen Leong Chua, Pei Xuan Lee, Julia María Martínez Gómez, Eng Eong Ooi, Sylvie Alonso
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Research Article Infectious disease Vaccines

Dengue vaccine–induced CD8+ T cell immunity confers protection in the context of enhancing, interfering maternal antibodies

Abstract

Declining levels of maternal antibodies were shown to sensitize infants born to dengue-immune mothers to severe disease during primary infection, through the process of antibody-dependent enhancement of infection (ADE). With the recent approval for human use of Sanofi-Pasteur’s chimeric dengue vaccine CYD-TDV and several vaccine candidates in clinical development, the scenario of infants born to vaccinated mothers has become a reality. This raises 2 questions: will declining levels of maternal vaccine-induced antibodies cause ADE; and, will maternal antibodies interfere with vaccination efficacy in the infant? To address these questions, the above scenario was modeled in mice. Type I IFN–deficient female mice were immunized with live attenuated DENV2 PDK53, the core component of the tetravalent DENVax candidate currently under clinical development. Pups born to PDK53-immunized dams acquired maternal antibodies that strongly neutralized parental strain 16681, but not the heterologous DENV2 strain D2Y98P-PP1, and instead caused ADE during primary infection with this strain. Furthermore, pups failed to seroconvert after PDK53 vaccination, owing to maternal antibody interference. However, a cross-protective multifunctional CD8+ T cell response did develop. Thus, our work advocates for the development of dengue vaccine candidates that induce protective CD8+ T cells despite the presence of enhancing, interfering maternal antibodies.

Authors

Jian Hang Lam, Yen Leong Chua, Pei Xuan Lee, Julia María Martínez Gómez, Eng Eong Ooi, Sylvie Alonso

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Figure 4

Disease outcome upon challenge with D2Y98P-PP1 of pups born to PDK53-immunized dams and vaccinated with PDK53 or passively transferred with CD4+ or CD8+ T cells.

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Disease outcome upon challenge with D2Y98P-PP1 of pups born to PDK53-imm...
Three-wko A129 pups born to PDK53-immunized or naive dams were vaccinated, or not, with PDK53 and challenged at 6 weeks of age with 107 PFU of D2Y98P-PP1 strain. (A and B) Clinical scores. Euthanasia was performed at a clinical score of 4. Medians and interquartile ranges of 5–6 mice per group are shown. (C) D2Y98P-PP1 viremia and organ viral loads. Nominal values were assigned to viral loads below limit of detection. Mann-Whitney test was performed to compare viral loads between the nonvaccinated groups. (D and E) Five- to 7-wko mice born to PDK53-immune or DENV-naive dams were transferred with 1.5 × 107 naive or PDK53-primed CD4+ (D) or CD8+ (E) T cells and challenged with 107 PFU of D2Y98P-PP1 one day later. Medians and interquartile ranges of 7–8 (D) and 5 (E) mice per group are shown. Euthanasia was performed at a clinical score of 4. Data are representative of 2 independent experiments. (F) Clinical scores of 6-wko A129 mice (n = 8) born to PDK53-immunized dams, and adoptively transferred with 6 × 106 CD8+ T cells 1 day prior to D2Y98P-PP1 challenge (106 PFU). The CD8+ T cells transferred were either nonspecifically activated or PDK53-primed. (G) D2Y98P-PP1 viremia at day 4 after challenge (n = 4) in mice transferred with either nonspecifically activated CD8+ T cells or PDK53-primed CD8+ T cells. Kruskal-Wallis test with Dunn’s multiple comparison was performed. *P ≤ 0.05; ns, P > 0.05. Data are representative of 2 independent experiments.