The CD8-mediated optimisation of the antigen specific T-cell response
CD8+ T-cells target infected and dysregulated cells for deletion. Failure of this response can result in persistent challenge, such as cancer or chronic infection. CD8+ T-cells recognize peptides in the context of major histocompatibility complex class I (MHCI) molecules on the surface of host cells...
| Main Author: | |
|---|---|
| Published: |
Cardiff University
2017
|
| Online Access: | https://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.742851 |
| id |
ndltd-bl.uk-oai-ethos.bl.uk-742851 |
|---|---|
| record_format |
oai_dc |
| spelling |
ndltd-bl.uk-oai-ethos.bl.uk-7428512019-01-08T03:35:42ZThe CD8-mediated optimisation of the antigen specific T-cell responseDockree, Tamsin2017CD8+ T-cells target infected and dysregulated cells for deletion. Failure of this response can result in persistent challenge, such as cancer or chronic infection. CD8+ T-cells recognize peptides in the context of major histocompatibility complex class I (MHCI) molecules on the surface of host cells. The detection of T-cell antigens involves the binding of two receptors (TCR and CD8) to a single ligand (pMHCI). Individual TCRs cross-react with >106 different peptide antigens to ensure coverage of all possible pMHCI. As a result of this high level of T-cell crossreactivity the TCR/pMHCI interaction is usually suboptimal and significant scope exists in optimization for therapeutic benefit. The CD8 coreceptor enhances T-cell sensitivity through several mechanisms and has a potent ability to tune the antigen specific Tcell response. The pMHCI/CD8 interaction is characterised by very weak affinity. Increasing the strength of the pMHCI/CD8 interaction by 15-fold has been shown to result in complete loss of antigen specificity. In this thesis, I have shown that loss of antigen specificity occurs at a defined pMHCI/CD8 threshold (KD ~ 27 μM). This finding suggests that there is scope to increase the strength of the pMHCI/CD8 interaction for therapeutic benefit without non-specific CD8 T-cell activation. I demonstrated that increasing the strength of the pMHCI/CD8 interaction by engineering a point mutation into cell surface CD8 can result in improved T-cell antigen sensitivity. I have further classified the means by which CD8 can control Tcell crossreactivity and how altering the strength of the pMHCI/CD8 interaction can alter the focus of the TCR. And finally, I demonstrated that the level of CD8 expressed at the surface can have a dramatic effect on T-cell activation. Overall, I have demonstrated that cell surface CD8 can be engineered to enhance the therapeutic efficacy of adoptive T-cell transfer irrespective of antigen specificity.Cardiff Universityhttps://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.742851http://orca.cf.ac.uk/112223/Electronic Thesis or Dissertation |
| collection |
NDLTD |
| sources |
NDLTD |
| description |
CD8+ T-cells target infected and dysregulated cells for deletion. Failure of this response can result in persistent challenge, such as cancer or chronic infection. CD8+ T-cells recognize peptides in the context of major histocompatibility complex class I (MHCI) molecules on the surface of host cells. The detection of T-cell antigens involves the binding of two receptors (TCR and CD8) to a single ligand (pMHCI). Individual TCRs cross-react with >106 different peptide antigens to ensure coverage of all possible pMHCI. As a result of this high level of T-cell crossreactivity the TCR/pMHCI interaction is usually suboptimal and significant scope exists in optimization for therapeutic benefit. The CD8 coreceptor enhances T-cell sensitivity through several mechanisms and has a potent ability to tune the antigen specific Tcell response. The pMHCI/CD8 interaction is characterised by very weak affinity. Increasing the strength of the pMHCI/CD8 interaction by 15-fold has been shown to result in complete loss of antigen specificity. In this thesis, I have shown that loss of antigen specificity occurs at a defined pMHCI/CD8 threshold (KD ~ 27 μM). This finding suggests that there is scope to increase the strength of the pMHCI/CD8 interaction for therapeutic benefit without non-specific CD8 T-cell activation. I demonstrated that increasing the strength of the pMHCI/CD8 interaction by engineering a point mutation into cell surface CD8 can result in improved T-cell antigen sensitivity. I have further classified the means by which CD8 can control Tcell crossreactivity and how altering the strength of the pMHCI/CD8 interaction can alter the focus of the TCR. And finally, I demonstrated that the level of CD8 expressed at the surface can have a dramatic effect on T-cell activation. Overall, I have demonstrated that cell surface CD8 can be engineered to enhance the therapeutic efficacy of adoptive T-cell transfer irrespective of antigen specificity. |
| author |
Dockree, Tamsin |
| spellingShingle |
Dockree, Tamsin The CD8-mediated optimisation of the antigen specific T-cell response |
| author_facet |
Dockree, Tamsin |
| author_sort |
Dockree, Tamsin |
| title |
The CD8-mediated optimisation of the antigen specific T-cell response |
| title_short |
The CD8-mediated optimisation of the antigen specific T-cell response |
| title_full |
The CD8-mediated optimisation of the antigen specific T-cell response |
| title_fullStr |
The CD8-mediated optimisation of the antigen specific T-cell response |
| title_full_unstemmed |
The CD8-mediated optimisation of the antigen specific T-cell response |
| title_sort |
cd8-mediated optimisation of the antigen specific t-cell response |
| publisher |
Cardiff University |
| publishDate |
2017 |
| url |
https://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.742851 |
| work_keys_str_mv |
AT dockreetamsin thecd8mediatedoptimisationoftheantigenspecifictcellresponse AT dockreetamsin cd8mediatedoptimisationoftheantigenspecifictcellresponse |
| _version_ |
1718808478748770304 |