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An mRNA vaccine induces antimycobacterial immunity by activating DNA damage repair and autophagy. | LitMetric

AI Article Synopsis

  • A new mRNA vaccine for tuberculosis (TB) shows strong effectiveness in a zebrafish model, offering both prevention and treatment benefits.
  • Zebrafish that received the mRNA vaccine lived longer after being exposed to TB and showed significantly reduced bacterial levels when treated after infection.
  • The vaccine not only activates important DNA repair systems for immune function but also promotes cell survival and bacterial killing without triggering harmful cell death responses.

Article Abstract

Effective vaccines are urgently needed for the control of tuberculosis (TB). Here, we report that an mRNA TB vaccine is highly effective and exhibits both prophylactic and therapeutic activity in the zebrafish model of TB. Adult zebrafish immunized with the mRNA vaccine survived significantly longer after challenge compared to those immunized with the DNA vaccine. Furthermore, post-infection treatment with the mRNA vaccine drastically reduced the bacterial burden. The mRNA vaccine activated multiple DNA break repair systems that are essential for the normal development and function of adaptive immunity, but did not activate the canonical DNA damage responses that promote cell death. This highlights a profound connection between DNA damage repair and the activation of immune responses under physiological processes of immunization. Remarkably, the mRNA vaccine induced autophagy in granulomas, coinciding with bacterial killing and cell survival. Collectively, these findings demonstrate that the mRNA vaccine elicits potent innate and adaptive immunity, providing effective host protection against mycobacterial challenge.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11700299PMC
http://dx.doi.org/10.1016/j.omtn.2024.102402DOI Listing

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