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Title
Exploring Mechanisms of Regulatory T cell-mediated Immune Suppression and Development of Anti-PD-L1 CAR T cells
Description
Regulatory T cells (Tregs) suppress adaptive immunity and inflammation. In cancer, Tregs hinder therapeutic responses due to suppression of anti-tumor activity in the tumor microenvironment. Although these cells play a role in suppressing anti-tumor responses, development of therapeutics that target Tregs is limited by their low abundance, heterogeneity, and lack of specific cell surface markers. To study Treg mechanisms of suppression, a human T cell line, MoT, was identified and characterized as a model of human Foxp3+ Tregs. MoT cells express surface markers consistent with PBMC-derived Tregs and inhibit proliferation of CD4+ responder PBMCs in a ratio-dependent manner. Transwell membrane separation prevented suppression of stimulated CD4+ PBMC proliferation by MoT cells, suggesting cell-cell contact is required for suppressive activity. Suppression was found to be independent of soluble cytokines and known immune checkpoint pathways, providing evidence that a Foxp3+ Treg population suppresses immune responses by an unknown cell contact-dependent mechanism. To investigate potential cell surface molecules that mediate suppression, monoclonal antibodies (mAbs) were generated to a known immunosuppressive protein, Galectin-1, and to MoT cell surface proteins. MAbs were identified that bind and functionally block suppressive activity. Another mechanism of immune suppression involves the PD-1/PD-L1 pathway, which is exploited by tumor cells to resist T cell killing and escape immune clearance. Since PD-L1 has emerged as an effective therapeutic target, anti-PD-L1 CAR T cells were generated and demonstrated to kill PD-L1-positive tumor cells. These results expand upon the current knowledge of Treg function and CAR T cell therapy and may lead to enhanced anti-tumor immunity to improve patient responses.
Date Created
2023
Contributors
- Pfeffer, Kirsten (Author)
- Lake, Douglas F (Thesis advisor)
- Ho, Thai H (Committee member)
- Hedin, Karen E (Committee member)
- Rahman, Masmudur M (Committee member)
- Arizona State University (Publisher)
Topical Subject
Resource Type
Extent
202 pages
Language
eng
Copyright Statement
In Copyright
Primary Member of
Peer-reviewed
No
Open Access
No
Handle
https://hdl.handle.net/2286/R.2.N.190799
Level of coding
minimal
Cataloging Standards
Note
Partial requirement for: Ph.D., Arizona State University, 2023
Field of study: Molecular and Cellular Biology
System Created
- 2023-12-14 01:24:29
System Modified
- 2023-12-14 01:24:36
- 11 months 1 week ago
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