Publications by authors named "Pascale Bouchier"

Article Synopsis
  • * A study tested five spike variants with different stability levels in mice, finding that a highly stable variant (S-closed-2) induced the highest neutralizing antibody response, outperforming less stable proteins by up to 16 times.
  • * However, the most stable variant (S-locked), which prevented the spike from interacting flexibly, produced lower antibody levels against diverse strains, suggesting that further research is needed on spike protein designs to improve vaccine effectiveness.
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For an efficacious vaccine immunogen, influenza hemagglutinin (HA) needs to maintain a stable quaternary structure, which is contrary to the inherently dynamic and metastable nature of class I fusion proteins. In this study, we stabilized HA with three substitutions within its pH-sensitive regions where the refolding starts. An X-ray structure reveals how these substitutions stabilize the intersubunit β-sheet in the base and form an interprotomeric aliphatic layer across the stem while the native prefusion HA fold is retained.

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The trimeric spike (S) protein of SARS-CoV-2 is the primary focus of most vaccine design and development efforts. Due to intrinsic instability typical of class I fusion proteins, S tends to prematurely refold to the post-fusion conformation, compromising immunogenic properties and prefusion trimer yields. To support ongoing vaccine development efforts, we report the structure-based design of soluble S trimers with increased yields and stabilities, based on introduction of single point mutations and disulfide-bridges.

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Article Synopsis
  • Respiratory syncytial virus (RSV) is the primary cause of severe respiratory infections in infants, leading to numerous hospitalizations.* -
  • Researchers have developed new strategies to stabilize the RSV fusion protein (RSV F) in its prefusion state, which enhances its effectiveness as a vaccine antigen.* -
  • The modified RSV F demonstrates high stability and ability to trigger strong immune responses, offering complete protection in lab tests on cotton rats.*
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Model antigens are frequently introduced into pathogens to study determinants that influence T-cell responses to infections. To address whether an antigen's subcellular location influences the nature and magnitude of antigen-specific T-cell responses, we generated Plasmodium berghei parasites expressing the model antigen ovalbumin (OVA) either in the parasite cytoplasm or on the parasitophorous vacuole membrane (PVM). For cytosolic expression, OVA alone or conjugated to mCherry was expressed from a strong constitutive promoter (OVAhsp70 or OVA::mCherryhsp70); for PVM expression, OVA was fused to HEP17/EXP1 (OVA::Hep17hep17).

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The causative agent of tuberculosis (TB), Mycobacterium tuberculosis, remains an important worldwide health threat. Although TB is one of the oldest infectious diseases of man, a detailed understanding of the mycobacterial mechanisms underlying pathogenesis remains elusive. Here, we studied the role of the α(1→2) mannosyltransferase MptC in mycobacterial virulence, using the Mycobacterium marinum zebrafish infection model.

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