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dc.rights.licenseCC-BY-NC-ND
dc.contributor.advisorBoxtel, Ruben van
dc.contributor.authorBlijleven, Kees
dc.date.accessioned2022-07-01T00:00:37Z
dc.date.available2022-07-01T00:00:37Z
dc.date.issued2022
dc.identifier.urihttps://studenttheses.uu.nl/handle/20.500.12932/41682
dc.description.abstractThe treatment of Hodgkin lymphoma (HL) is considered a success story: cure rates surpass 80%. However, the successful treatment of HL can result in adverse side-effects later in life. Thus, there remains a need for novel therapies that result in a better quality-of-life after treatment. The tumor microenvironment (TME) affects tumor proliferation and progression. Interactions between tumor cells and their TME are being targeted as novel treatment options. A well-known inhibitory interaction in HL is PD-1 mediated inhibition of cytotoxic T-cell activity, which renders the immune system in the TME inactive and lets Hodgkin cancer cells escape immune detection. To study HL TME composition in pediatric patients, samples were analysed on a single cell level. A T-cell dominant TME marked with exhaustion markers CTLA4 and LAG3 was identified. Tumor cells were identified for seven out of eight patients using a SORT-seq strategy. Interactions between tumor cells and their TME were studied with CellChat, a method that reconstructs cell-cell interaction by computing a probability score based on scRNA-seq data. Finally, identified interactions were compared to previously published results. Both similarities and discrepancies were found, indicating that there is a likely biological difference between published Hodgkin protein data focussing on adults and pediatric scRNA-seq data that has been described here.
dc.description.sponsorshipUtrecht University
dc.language.isoEN
dc.subjectHodgkin Lymphoma (HL) tumors contain few malignant cells and many immune infiltrate cells. However, these immune cells do not seem to function as regular immune cells and fail to detect the malignant cells in HL. To improve treatment of pediatric HL, interactions between malignant cells and cells in their microenvironment were studied on single cell level. The results are described in this report.
dc.titleStudying the tumor microenvironment of Hodgkin Lymphoma with scRNA-seq
dc.type.contentMaster Thesis
dc.rights.accessrightsOpen Access
dc.subject.courseuuCancer, Stem Cells and Developmental Biology
dc.thesis.id494


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