AI Article Synopsis

  • Malaria remains a significant health threat despite advancements in treatment, highlighting the urgent need for an effective vaccine targeting its life cycle stages, particularly the liver.
  • A new "prime and target" vaccination strategy shows promise in inducing high levels of tissue-resident memory T cells in the liver, which improves the effectiveness of liver-stage malaria vaccines without relying solely on high circulating T cell counts.
  • Early human trials using this innovative vaccination approach demonstrate safety and potential effectiveness, suggesting it could be a viable method for not only malaria but also other liver-related infections and diseases.

Article Abstract

Despite recent advances in treatment and vector control, malaria is still a leading cause of death, emphasizing the need for an effective vaccine. The malaria life cycle can be subdivided into three stages: the invasion and growth within liver hepatocytes (pre-erythrocytic stage), the blood stage (erythrocytic stage), and, finally, the sexual stage (occurring within the mosquito vector). Antigen (Ag)-specific CD8 T cells are effectively induced by heterologous prime-boost viral vector immunization and known to correlate with liver-stage protection. However, liver-stage malaria vaccines have struggled to generate and maintain the high numbers of -specific circulating T cells necessary to confer sterile protection. We describe an alternative "prime and target" vaccination strategy aimed specifically at inducing high numbers of tissue-resident memory T cells present in the liver at the time of hepatic infection. This approach bypasses the need for very high numbers of circulating T cells and markedly increases the efficacy of subunit immunization against liver-stage malaria with clinically relevant Ags and clinically tested viral vectors in murine challenge models. Translation to clinical use has begun, with encouraging results from a pilot safety and feasibility trial of intravenous chimpanzee adenovirus vaccination in humans. This work highlights the value of a prime-target approach for immunization against malaria and suggests that this strategy may represent a more general approach for prophylaxis or immunotherapy of other liver infections and diseases.

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Source
http://dx.doi.org/10.1126/scitranslmed.aap9128DOI Listing

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