Constructing Hybrid Cytokine Receptors to Amplify CAR T Cell Anti-Tumor Potency

dc.contributor.advisorJensen, Michael C
dc.contributor.authorSaxby, Christopher
dc.date.accessioned2023-08-14T17:02:09Z
dc.date.available2023-08-14T17:02:09Z
dc.date.issued2023-08-14
dc.date.submitted2023
dc.descriptionThesis (Ph.D.)--University of Washington, 2023
dc.description.abstractChimeric antigen receptors (CARs) have achieved remarkable therapeutic efficacy against cancer by linking natural circuits of T cell activation to the recognition of tumor-associated antigens, but optimal anti-tumor responses require an additional input: cytokine stimulation. Here, we explored cellular engineering approaches to deliver cytokine signals directly to CAR T cells to enhance T cell expansion and functional durability. First, we compared a set of engineered receptors providing constitutive gamma chain cytokine signaling (Ch. 1) and found that cytokine inputs promote distinct and potentially complementary behavior in CAR T cells. To investigate combinatorial cytokine signaling, we developed a hybrid IL-7 and IL-21 receptor platform (Ch. 2), which amplified CAR T cell anti-tumor potency and yielded insights into the roles of cytokine signaling outputs (Ch. 3). In some cases, cytokine-driven improvements in CAR T cell efficacy were accompanied by unrestricted T cell growth and subsequent toxicity in vivo. Therefore, we implemented strategies to safely deploy cytokine signaling technology, including drug-responsive molecular switches (Ch. 4) and a synthetic T cell activation-dependent promoter (Ch. 5).
dc.embargo.termsOpen Access
dc.format.mimetypeapplication/pdf
dc.identifier.otherSaxby_washington_0250E_25865.pdf
dc.identifier.urihttp://hdl.handle.net/1773/50219
dc.language.isoen_US
dc.rightsnone
dc.subjectCancer
dc.subjectCAR T
dc.subjectCytokine
dc.subjectImmunotherapy
dc.subjectProtein Engineering
dc.subjectSynthetic Biology
dc.subjectBioengineering
dc.subject.otherBioengineering
dc.titleConstructing Hybrid Cytokine Receptors to Amplify CAR T Cell Anti-Tumor Potency
dc.typeThesis

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