eprintid: 23529 rev_number: 18 eprint_status: archive userid: 3330 dir: disk0/00/02/35/29 datestamp: 2017-10-06 09:36:36 lastmod: 2018-10-13 08:21:48 status_changed: 2017-10-06 09:36:36 type: doctoralThesis metadata_visibility: show creators_name: Dettling, Steffen title: Identifizierung von Tumor-assoziierten Antigenen in IDH-mutierten Gliomen subjects: ddc-500 divisions: i-140001 adv_faculty: af-14 cterms_swd: Tumor-assoziierte Antigene cterms_swd: IDH mutierte Gliome cterms_swd: Tumorimmunologie abstract: Gliomas are tumors of the central nervous system which are classified by the World Health Organization (WHO) from grade I to grade IV, according to the degree of malignancy as defined by histopathological and molecular criteria. Mutations in the isocitrate dehydrogenase (IDHmut) genes are a common cha- racteristic for lower grade gliomas (LGGs, WHO◦II/◦III) and have been shown to be a prognostic marker for a favorable clinical outcome. The metabolic and biologic consequences by IDHmut-induced epigentic alterations have changed our perceptions of gliomas and demonstrated the demand to consider IDHmut LGGs separately. Despite a favourable prognosis, IDHmut LGGs remain deadly since there is still a lack of effective therapies. For that reason, immunotherapeutic approaches are gaining increasing attention. Due to the limited number of known T cell targets in IDHmut gliomas, we aimed to elucidate the reper- toire of spontaneous T cell responses in IDHmut LGGs by performing an unbiased proteomic approach. We systematically analyzed the proteome of IDHmut LGG samples (n = 4) by fractionating tumor tissue lysates and testing resulting fractions by IFN-γ enzyme linked immunospot (ELISpot) assay for recogni- tion by the patients T cell repertoire. Immunogenic tumor protein fractions were subsequently analyzed by quantitative mass spectrometry resulting in 2897 identified proteins. Based on a thorough filter pro- cess 79 proteins have been selected as potential target antigens and were validated in IFN-γ ELISpots by means of synthetic in silico predicted 50-mer peptides. 26 of these were recognized by autologous T cells and were tested in further IDHmut LGG patients as well as in healthy donors. Tumor-specific T cell responses in up to 50 % of IDHmut LGG patients were observed for CRKII, CFL1, CNTN1, NME2, and TKT. Beside the immunogenicity of the antigens, we further characterized their role in oncogenesis, the antigen-specificity as well as the expression levels in the tumor and on glioma stem-like cells (GSCs). By using immunohistochemistry and gene expression analysis we found that four out of five of the most immunogenic tumor-associated antigens (CRKII, CFL1, CNTN1 and NME2) were expressed in astro- cytic and oligodendroglial tumors as well as in IDHmut GSCs, while being almost absent in normal brain tissues. Finally, we identified HLA-A*02-restricted reactive epitopes for CRKII (ALALEVGEL), NME2 (MVWEGLNVV), and TKT (FLAEAELLNL) which are recognized by up to 1.5 % of antigen-specific pe- ripheral cytotoxic T cells in IDHmut LGG patients. By analyzing the repertoire of T cell target antigens in IDHmut LGG patients, we identified four novel immunogenic antigens and even confirmed their expression on IDHmut GSCs, highlighting their potential as T cell targets for the development of new immunotherapeutic approaches. date: 2018 id_scheme: DOI id_number: 10.11588/heidok.00023529 ppn_swb: 1656524279 own_urn: urn:nbn:de:bsz:16-heidok-235292 date_accepted: 2017-09-19 advisor: HASH(0x558eaa6a4800) language: ger bibsort: DETTLINGSTIDENTIFIZI2018 full_text_status: public citation: Dettling, Steffen (2018) Identifizierung von Tumor-assoziierten Antigenen in IDH-mutierten Gliomen. [Dissertation] document_url: https://archiv.ub.uni-heidelberg.de/volltextserver/23529/1/Dissertation_Steffen%20Dettling%202017.pdf