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Deep Immune Phenotyping and Single-Cell Transcriptomics Allow Identification of Circulating TRM-Like Cells Which Correlate With Liver-Stage Immunity and Vaccine-Induced Protection From Malaria. | LitMetric

AI Article Synopsis

  • Protection against liver-stage malaria requires CD8+ T cells to target infected cells, and a new vaccination strategy called prime-target vaccination enhances this immune response.
  • This study involved advanced techniques like single-cell RNA sequencing to analyze liver and blood samples for CD8+ T cells, identifying differences and similarities between liver-resident memory (TRM) cells and their circulating counterparts.
  • The findings suggest that TRM-like cells could serve as reliable indicators of vaccine effectiveness, providing valuable insights for large-scale trials of liver-stage malaria vaccines, especially in African infants.

Article Abstract

Protection from liver-stage malaria requires high numbers of CD8+ T cells to find and kill -infected cells. A new malaria vaccine strategy, prime-target vaccination, involves sequential viral-vectored vaccination by intramuscular and intravenous routes to target cellular immunity to the liver. Liver tissue-resident memory (TRM) CD8+ T cells have been shown to be necessary and sufficient for protection against rodent malaria by this vaccine regimen. Ultimately, to most faithfully assess immunotherapeutic responses by these local, specialised, hepatic T cells, periodic liver sampling is necessary, however this is not feasible at large scales in human trials. Here, as part of a phase I/II challenge study of prime-target vaccination, we performed deep immune phenotyping, single-cell RNA-sequencing and kinetics of hepatic fine needle aspirates and peripheral blood samples to study liver CD8+ TRM cells and circulating counterparts. We found that while these peripheral 'TRM-like' cells differed to TRM cells in terms of previously described characteristics, they are similar phenotypically and indistinguishable in terms of key T cell residency transcriptional signatures. By exploring the heterogeneity among liver CD8+ TRM cells at single cell resolution we found two main subpopulations that each share expression profiles with blood T cells. Lastly, our work points towards the potential for using TRM-like cells as a correlate of protection by liver-stage malaria vaccines and, in particular, those adopting a prime-target approach. A simple and reproducible correlate of protection would be particularly valuable in trials of liver-stage malaria vaccines as they progress to phase III, large-scale testing in African infants. We provide a blueprint for understanding and monitoring liver TRM cells induced by a prime-target malaria vaccine approach.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8859435PMC
http://dx.doi.org/10.3389/fimmu.2022.795463DOI Listing

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