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CD8+ T cells from a novel T cell receptor transgenic mouse induce liver-stage immunity that can be boosted by blood-stage infection in rodent malaria

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posted on 2014-05-01, 00:00 authored by L S Lau, D Fernandez-Ruiz, V Mollard, A Sturm, M A Neller, A Cozijnsen, J L Gregory, G M Davey, C M Jones, Y H Lin, A Haque, C R Engwerda, C Q Nie, D S Hansen, K M Murphy, A T Papenfuss, J J Miles, S R Burrows, Tania De Koning-WardTania De Koning-Ward, G I McFadden, F R Carbone, B S Crabb, W R Heath
To follow the fate of CD8+ T cells responsive to Plasmodium berghei ANKA (PbA) infection, we generated an MHC I-restricted TCR transgenic mouse line against this pathogen. T cells from this line, termed PbT-I T cells, were able to respond to blood-stage infection by PbA and two other rodent malaria species, P. yoelii XNL and P. chabaudi AS. These PbT-I T cells were also able to respond to sporozoites and to protect mice from liver-stage infection. Examination of the requirements for priming after intravenous administration of irradiated sporozoites, an effective vaccination approach, showed that the spleen rather than the liver was the main site of priming and that responses depended on CD8α+ dendritic cells. Importantly, sequential exposure to irradiated sporozoites followed two days later by blood-stage infection led to augmented PbT-I T cell expansion. These findings indicate that PbT-I T cells are a highly versatile tool for studying multiple stages and species of rodent malaria and suggest that cross-stage reactive CD8+ T cells may be utilized in liver-stage vaccine design to enable boosting by blood-stage infections.

History

Journal

PLoS pathogens

Volume

10

Issue

5

Article number

e1004135

Pagination

1 - 16

Publisher

Public Library of Science

Location

San Francisco, CA

eISSN

1553-7374

Language

eng

Publication classification

C Journal article; C1 Refereed article in a scholarly journal

Copyright notice

2014, PLoS