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Pneumococcal sialidase promotes bacterial survival by fine-tuning of pneumolysin-mediated membrane disruption. | LitMetric

AI Article Synopsis

  • Pneumolysin (Ply) is a critical protein for the infection process of pneumococci, but its effectiveness can also harm bacterial survival by causing excessive disruptions in host cells.
  • A novel assay using NanoBiT-Nanobody was developed to measure the endosomal disruption effects of Ply, revealing that the pneumococcal sialidase NanA regulates Ply activity by modifying cell membrane sugars.
  • Also, the sialidase inhibitor oseltamivir amplifies Ply's destructive effects in vitro and increases tissue damage and bacterial clearance in vivo, suggesting new treatment approaches for severe pneumococcal infections that leverage Ply’s dual role.

Article Abstract

Pneumolysin (Ply) is an indispensable cholesterol-dependent cytolysin for pneumococcal infection. Although Ply-induced disruption of pneumococci-containing endosomal vesicles is a prerequisite for the evasion of endolysosomal bacterial clearance, its potent activity can be a double-edged sword, having a detrimental effect on bacterial survivability by inducing severe endosomal disruption, bactericidal autophagy, and scaffold epithelial cell death. Thus, Ply activity must be maintained at optimal levels. We develop a highly sensitive assay to monitor endosomal disruption using NanoBiT-Nanobody, which shows that the pneumococcal sialidase NanA can fine-tune Ply activity by trimming sialic acid from cell-membrane-bound glycans. In addition, oseltamivir, an influenza A virus sialidase inhibitor, promotes Ply-induced endosomal disruption and cytotoxicity by inhibiting NanA activity in vitro and greater tissue damage and bacterial clearance in vivo. Our findings provide a foundation for innovative therapeutic strategies for severe pneumococcal infections by exploiting the duality of Ply activity.

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Source
http://dx.doi.org/10.1016/j.celrep.2024.113962DOI Listing

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