Establishment and Molecular Characterization of an In Vitro Model for PARPi-Resistant Ovarian Cancer.

Klotz, Daniel Martin; Buchholz, Frank; Dubrovska, Anna; Theis, Mirko; Krüger, Alexander; Kuhlmann, Jan Dominik; Schuster, Kati; Schwarz, Franziska Maria; Link, Theresa; Kutz, Oliver; Wimberger, Pauline; Drukewitz, Stephan; Thomale, Jürgen

doi:10.3390/cancers15153774

Journal Article

DKFZ-2023-01644

Establishment and Molecular Characterization of an In Vitro Model for PARPi-Resistant Ovarian Cancer.

Klotz, D. M.DKFZ* ; Schwarz, F. M.DKFZ* ; Dubrovska, A.DKFZ* ; Schuster, K.DKFZ* ; Theis, M. ; Krüger, A.DKFZ* ; Kutz, O.DKFZ* ; Link, T.DKFZ* ; Wimberger, P.DKFZ* ; Drukewitz, S.DKFZ* ; Buchholz, F.DKFZ* ; Thomale, J. ; Kuhlmann, J. D.DKFZ*

2023
MDPI Basel

Cancers 15(15), 3774 (2023) [10.3390/cancers15153774]

Abstract: Overcoming PARPi resistance is a high clinical priority. We established and characterized comparative in vitro models of acquired PARPi resistance, derived from either a BRCA1-proficient or BRCA1-deficient isogenic background by long-term exposure to olaparib. While parental cell lines already exhibited a certain level of intrinsic activity of multidrug resistance (MDR) proteins, resulting PARPi-resistant cells from both models further converted toward MDR. In both models, the PARPi-resistant phenotype was shaped by (i) cross-resistance to other PARPis (ii) impaired susceptibility toward the formation of DNA-platinum adducts upon exposure to cisplatin, which could be reverted by the drug efflux inhibitors verapamil or diphenhydramine, and (iii) reduced PARP-trapping activity. However, the signature and activity of ABC-transporter expression and the cross-resistance spectra to other chemotherapeutic drugs considerably diverged between the BRCA1-proficient vs. BRCA1-deficient models. Using dual-fluorescence co-culture experiments, we observed that PARPi-resistant cells had a competitive disadvantage over PARPi-sensitive cells in a drug-free medium. However, they rapidly gained clonal dominance under olaparib selection pressure, which could be mitigated by the MRP1 inhibitor MK-751. Conclusively, we present a well-characterized in vitro model, which could be instrumental in dissecting mechanisms of PARPi resistance from HR-proficient vs. HR-deficient background and in studying clonal dynamics of PARPi-resistant cells in response to experimental drugs, such as novel olaparib-sensitizers.

Keyword(s): PARPi resistance ; cisplatin ; ovarian cancer

Classification:

ddc:610

Contributing Institute(s):

DKTK Koordinierungsstelle Dresden (DD01)

Research Program(s):

899 - ohne Topic (POF4-899) (POF4-899)

Appears in the scientific report 2023

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Medline

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; Article Processing Charges ; BIOSIS Previews ; Biological Abstracts ; Clarivate Analytics Master Journal List ; DOAJ Seal ; Ebsco Academic Search ; Essential Science Indicators ; Fees ; IF >= 5 ; JCR ; PubMed Central ; SCOPUS ; Science Citation Index Expanded ; Web of Science Core Collection

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Record created 2023-08-14, last modified 2024-02-29

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