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1. Modified Vaccinia Virus Ankara Can Induce Optimal CD8+T Cell Responses to Directly Primed Antigens Depending on Vaccine Design

2. Modified Vaccinia Virus Ankara Can Induce Optimal CD8 + T Cell Responses to Directly Primed Antigens Depending on Vaccine Design.

3. Heightened self-reactivity associated with selective survival, but not expansion, of naïve virus-specific CD8+ T cells in aged mice.

4. Paired TCRαβ analysis of virus-specific CD8(+) T cells exposes diversity in a previously defined 'narrow' repertoire.

5. The influenza virus-specific CTL immunodominance hierarchy in mice is determined by the relative frequency of high-avidity T cells.

6. Reproducible selection of high avidity CD8+ T-cell clones following secondary acute virus infection.

7. Multiplexed combinatorial tetramer staining in a mouse model of virus infection.

8. Primary CTL response magnitude in mice is determined by the extent of naive T cell recruitment and subsequent clonal expansion.

9. Diversity and clonotypic composition of influenza-specific CD8+ TCR repertoires remain unaltered in the absence of Aire.

10. Altered CD8(+) T cell immunodominance after vaccinia virus infection and the naive repertoire in inbred and F(1) mice.

11. Narrowed TCR diversity for immunised mice challenged with recombinant influenza A-HIV Env(311-320) virus.

12. Epitope-specific TCRbeta repertoire diversity imparts no functional advantage on the CD8+ T cell response to cognate viral peptides.

13. His1 and His2 are distantly related, spindle-shaped haloviruses belonging to the novel virus group, Salterprovirus.

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