Walz, Michael (2023)
Development of the first selective proteolysis targeting chimera for the FK506-binding protein 51.
Technische Universität Darmstadt
doi: 10.26083/tuprints-00024051
Dissertation, Erstveröffentlichung, Verlagsversion
Kurzbeschreibung (Abstract)
Because of its various potential applications, FKBP51 emerged as an interesting target protein for pharmacological research. In spite of many attempts, however, no conventional ligand with a sufficient pharmacological profile has yet been developed. Since the synthesis of such a ligand proved to be challenging and moreover it is still not exactly explored which domain is responsible for which function of the protein, the recently developed concept of PROTACs seemed to be an interesting possibility to investigate these problems. Moreover, due to the recently clarified interactions of FKBP51 with GR by Baischew et al.1, PROTACs prove to be a highly interesting target for the treatment of GR-mediated stress-related disorders. In her doctoral thesis2, Dr. Tianqi Mao was able to show that the degradation of FKBP51 by the use of a PROTAC is feasible in general. However, no PROTAC synthesized in the course of her work showed sufficient activity or selectivity. Therefore, the PROTAC library synthesized by Dr. Mao should be extended and screened for potential hits within the scope of this work. If possible, conclusions about structure-activity relationships should be drawn and then used for optimization of the PROTACs. The aim was to develop a highly active and selective PROTAC for FKBP51.
Typ des Eintrags: | Dissertation | ||||
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Erschienen: | 2023 | ||||
Autor(en): | Walz, Michael | ||||
Art des Eintrags: | Erstveröffentlichung | ||||
Titel: | Development of the first selective proteolysis targeting chimera for the FK506-binding protein 51 | ||||
Sprache: | Englisch | ||||
Referenten: | Hausch, Prof. Dr. Felix ; Immel, PD Dr. Stefan | ||||
Publikationsjahr: | 2023 | ||||
Ort: | Darmstadt | ||||
Kollation: | 7, 460 Seiten | ||||
Datum der mündlichen Prüfung: | 8 Mai 2023 | ||||
DOI: | 10.26083/tuprints-00024051 | ||||
URL / URN: | https://tuprints.ulb.tu-darmstadt.de/24051 | ||||
Kurzbeschreibung (Abstract): | Because of its various potential applications, FKBP51 emerged as an interesting target protein for pharmacological research. In spite of many attempts, however, no conventional ligand with a sufficient pharmacological profile has yet been developed. Since the synthesis of such a ligand proved to be challenging and moreover it is still not exactly explored which domain is responsible for which function of the protein, the recently developed concept of PROTACs seemed to be an interesting possibility to investigate these problems. Moreover, due to the recently clarified interactions of FKBP51 with GR by Baischew et al.1, PROTACs prove to be a highly interesting target for the treatment of GR-mediated stress-related disorders. In her doctoral thesis2, Dr. Tianqi Mao was able to show that the degradation of FKBP51 by the use of a PROTAC is feasible in general. However, no PROTAC synthesized in the course of her work showed sufficient activity or selectivity. Therefore, the PROTAC library synthesized by Dr. Mao should be extended and screened for potential hits within the scope of this work. If possible, conclusions about structure-activity relationships should be drawn and then used for optimization of the PROTACs. The aim was to develop a highly active and selective PROTAC for FKBP51. |
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Alternatives oder übersetztes Abstract: |
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Status: | Verlagsversion | ||||
URN: | urn:nbn:de:tuda-tuprints-240514 | ||||
Sachgruppe der Dewey Dezimalklassifikatin (DDC): | 500 Naturwissenschaften und Mathematik > 540 Chemie | ||||
Fachbereich(e)/-gebiet(e): | 07 Fachbereich Chemie 07 Fachbereich Chemie > Clemens-Schöpf-Institut > Fachgebiet Biochemie 07 Fachbereich Chemie > Clemens-Schöpf-Institut > Fachgebiet Organische Chemie |
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Hinterlegungsdatum: | 29 Aug 2023 14:37 | ||||
Letzte Änderung: | 30 Aug 2023 05:20 | ||||
PPN: | |||||
Referenten: | Hausch, Prof. Dr. Felix ; Immel, PD Dr. Stefan | ||||
Datum der mündlichen Prüfung / Verteidigung / mdl. Prüfung: | 8 Mai 2023 | ||||
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