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Development and application of a patient-derived xenograft platform to test anticancer agents

Abstract
Malignant melanoma is the most aggressive form of skin cancer and incidence rates are on the rise. Despite recent improvements in treatment options, the disease still remains lethal. Which calls for expedited solutions. In this thesis I will discuss three studies, which have not only contributed new knowledge to the research community but also led to development of tools used in cancer research. In the first paper we developed a platform of patient-derived xenografts (PDXes) from metastatic melanoma patients. We show that PDXes can accurately predict clinical treatment responses and that the xenografts can be established in time to benefit the patients. Thus, the platform can be used for multiple pre-clinical and clinical purposes. In the second paper we compared the transcriptome of cell line-derived xenografts (CDXes) and PDXes. The initial aim was to investigate if CDXes would be transcriptionally similar to PDXes and could therefore be used as in vitro surrogates for the PDXes. Instead, we identified a significant transcriptional difference between CDXes and PDXes, mainly explained by the pseudo hypoxia experienced by the cell lines once they are transplanted to the physiological environment. In the third paper, we ran a pre-clinical trial in malignant melanoma PDX mouse models with the aim of identifying a predictive biomarker of the MTH1 inhibitor, Karonudib. By comparing the genomic and transcriptomic profiles of the responding and non-responding PDXes we identified that Karonudib has cytotoxic effect independent of those profiles. Also, we discovered that Karonudib causes cytotoxic effect beyond MTH1 inhibition. Taken together, our data shows that PDX models predict clinical responses and can be used to test drugs pre-clinically, and argues that pre-clinical testing in PDX models is superior to cell line based drug testing.
Parts of work
I. Melanoma patient-derived xenografts accurately model the disease and develop fast enough to guide treatment decisions. Berglind O. Einarsdottir, Roger Olofsson Bagge, Joydeep Bhadury, Henrik Jesper-sen, Jan Mattsson, Lisa M. Nilsson, Katarina Truvé, Marcele Dávila López, Peter Naredi, Ola Nilsson, Ulrika Stierner, Lars Ny and Jonas A. Nilsson. Oncotarget 2014; 30;5(20):9609-18. ::PMID::25228592
 
II. Hypoxia-regulated gene expression explains differences between melanoma cell line-derived xenografts and patient-derived xenografts Joydeep Bhadury, Berglind O. Einarsdottir, Agnieszka Podraza, Roger Olofsson Bagge, Ulrika Stierner, Lars Ny, Marcela Dávila López and Jonas A. Nilsson. Oncotarget. 2016 Apr 26;7(17):23801-11 ::PMID::27009863
 
III. TH1579 (Karonudib) inhibits MTH1 and microtubule dynamics and has broad anti-melanoma effects in patient-derived xenografts. Berglind O. Einarsdottir, Joakim Karlsson#, Elin MV Söderberg#, Mattias F. Lind-berg, Lydia C. Green, Elisa Funck-Brentano, Roger Olofsson Bagge, Henrik Jes-persen, Annika Thorsell, Carina Sihlbom, Louise Carstam, Martin Scobie, Tobias Koolmeister, Olof Wallner, Ulrika Stierner, Ulrika Warpman Berglund, Lars Ny, Lisa M. Nilsson, Erik Larsson, Thomas Helleday and Jonas A. Nilsson. #Equal contribution. Manuscript
 
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Clincial Sciences. Department of Surgery
Disputation
Fredagen den 26 Maj 2017, kl. 9.00, Hörsal Arvid Carlsson, Academicum, Medicinaregatan 3, Göteborg
Date of defence
2017-05-26
E-mail
berglind.osk.einarsdottir@gu.se
URI
http://hdl.handle.net/2077/51878
Collections
  • Doctoral Theses / Doktorsavhandlingar Institutionen för kliniska vetenskaper
  • Doctoral Theses from Sahlgrenska Academy
  • Doctoral Theses from University of Gothenburg / Doktorsavhandlingar från Göteborgs universitet
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Thesis frame (42.32Mb)
Abstract (572.7Kb)
Date
2017-05-09
Author
Einarsdottir, Berglind
Keywords
malignant melanoma
patient-derived xenografts
MTH1
pre-clinical trial
Karonudib
Publication type
Doctoral thesis
ISBN
978-91-629-0162-2 (PDF)
978-91-629-0161-5 (PRINT)
Language
eng
Metadata
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