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1. The immunogenicity of a viral cytotoxic T cell epitope is controlled by its MHC-bound conformation

2. T cell receptor recognition of a 'super-bulged' major histocompatibility complex class I-bound peptide

3. The crystal structure of myelin oligodendrocyte glycoprotein, a key autoantigen in multiple sclerosis

4. Hard wiring of T cell receptor specificity for the major histocompatibility complex is underpinned by TCR adaptability.

5. T cell allorecognition via molecular mimicry.

6. Impact of clonal competition for peptide-MHC complexes on the CD8+ T-cell repertoire selection in a persistent viral infection.

7. The impact of HLA-B micropolymorphism outside primary peptide anchor pockets on the CTL response to CMV.

8. A T cell receptor flattens a bulged antigenic peptide presented by a major histocompatibility complex class I molecule.

9. TCR alpha genes direct MHC restriction in the potent human T cell response to a class I-bound viral epitope.

10. Two distinct regions of the large serine recombinase TnpX are required for DNA binding and biological function.

11. The immunogenicity of a viral cytotoxic T cell epitope is controlled by its MHC-bound conformation.

12. T cell receptor recognition of a 'super-bulged' major histocompatibility complex class I-bound peptide.

13. CTL recognition of a bulged viral peptide involves biased TCR selection.

14. High resolution structures of highly bulged viral epitopes bound to major histocompatibility complex class I. Implications for T-cell receptor engagement and T-cell immunodominance.

15. Identification of the structural and functional domains of the large serine recombinase TnpX from Clostridium perfringens.

16. The crystal structure of myelin oligodendrocyte glycoprotein, a key autoantigen in multiple sclerosis.

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