Publications by authors named "N Dereuddre-Bosquet"

Development of new vaccines tailored for difficult-to-target diseases is hampered by a lack of diverse adjuvants for human use, and none of the currently available adjuvants induce Th17 cells. Here, we develop a liposomal adjuvant, CAF®10b, that incorporates Mincle and Toll-like receptor 9 agonists. In parallel mouse and non-human primate studies comparing to CAF® adjuvants already in clinical trials, we report species-specific effects of adjuvant composition on the quality and magnitude of the responses.

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Few therapeutic options are available to treat COVID-19. The KEAP1/NRF2 pathway, the major redox-responsive pathway, has emerged as a potential therapeutic target for COVID-19 as it regulates redox homeostasis and inflammation that are altered during SARS-CoV-2 infection. Here, we characterized the effects of NRF2-agonist Sulfodyne, a stabilized natural Sulforaphane, in cellular and animal models of SARS-CoV-2 infection.

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While most individuals suffer progressive disease following HIV infection, a small fraction spontaneously controls the infection. Although CD8 T-cells have been implicated in this natural control, their mechanistic roles are yet to be established. Here, we combined mathematical modeling and analysis of previously published data from 16 SIV-infected macaques, of which 12 were natural controllers, to elucidate the role of CD8 T-cells in natural control.

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Article Synopsis
  • Early pregnancy Zika virus (ZIKV) infection can cause serious brain damage in fetuses, resulting in conditions like microcephaly, though the exact mechanisms of this damage are still not fully understood.
  • A study using cynomolgus macaque fetuses showed that ZIKV was transmitted from infected fetuses to their mothers, leading to detectable viral levels in blood, brain, and placenta, along with signs of brain size reduction in the infected fetuses.
  • Despite persistent viral genetic material in tissues, the immune response helped clear much of the virus before the delivery, indicating that while short-term brain injury occurs, the body can partially control the infection.
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PARVAX is a genetic vaccine platform based on an adeno-associated vector that has demonstrated to elicit potent, durable, and protective immunity in nonhuman primates (NHPs) after a single dose. Here, we assessed vaccine immunogenicity following a PARVAX prime-boost regimen against SARS-CoV-2. In mice, a low-dose prime followed by a higher-dose boost elicited potent neutralizing antibody responses and distinct cross-reactivity profiles, depending on the antigen used in the booster vaccine.

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