Establishment and Molecular Characterization of Two Patient-Derived Pancreatic Ductal Adenocarcinoma Cell Lines as Preclinical Models for Treatment Response

Rüdiger Braun; Olha Lapshyna; Jessica Watzelt; Maren Drenckhan; Axel Künstner; Benedikt Färber; Ahmed Ahmed Mohammed Hael; Louisa Bolm; Kim Christin Honselmann; Björn Konukiewitz; Darko Castven; Malte Spielmann; Sivahari Prasad Gorantla; Hauke Busch; Jens-Uwe Marquardt; Tobias Keck; Ulrich Friedrich Wellner; Hendrik Ungefroren

doi:10.3390/cells12040587

Establishment and Molecular Characterization of Two Patient-Derived Pancreatic Ductal Adenocarcinoma Cell Lines as Preclinical Models for Treatment Response

Cells. 2023 Feb 11;12(4):587. doi: 10.3390/cells12040587.

Authors

Rüdiger Braun¹, Olha Lapshyna¹, Jessica Watzelt¹, Maren Drenckhan¹, Axel Künstner^{2

3}, Benedikt Färber¹, Ahmed Ahmed Mohammed Hael⁴, Louisa Bolm¹, Kim Christin Honselmann¹, Björn Konukiewitz⁵, Darko Castven⁴, Malte Spielmann⁶, Sivahari Prasad Gorantla⁷, Hauke Busch^{2

3}, Jens-Uwe Marquardt⁴, Tobias Keck¹, Ulrich Friedrich Wellner¹, Hendrik Ungefroren^{1

4

5}

Affiliations

¹ Department of Surgery, University Medical Center Schleswig-Holstein, Campus Lübeck, 23538 Lübeck, Germany.
² Medical Systems Biology Group, Lübeck Institute of Experimental Dermatology, University of Lübeck, 23538 Lübeck, Germany.
³ Institute for Cardiogenetics, University of Lübeck, 23538 Lübeck, Germany.
⁴ First Medical Department, University Medical Center Schleswig-Holstein, Campus Lübeck, Ratzeburger Allee 160, 23538 Lübeck, Germany.
⁵ Institute of Pathology, University Medical Center Schleswig-Holstein, Campus Kiel, 24105 Kiel, Germany.
⁶ Institute of Human Genetics, University of Lübeck, 23538 Lübeck, Germany.
⁷ Department of Hematology and Oncology, University Medical Center Schleswig-Holstein, Campus Lübeck, 23538 Lübeck, Germany.

Abstract

The prognosis of pancreatic ductal adenocarcinoma (PDAC) is exceedingly poor. Although surgical resection is the only curative treatment option, multimodal treatment is of the utmost importance, as only about 20% of tumors are primarily resectable at the time of diagnosis. The choice of chemotherapeutic treatment regimens involving gemcitabine and FOLFIRINOX is currently solely based on the patient's performance status, but, ideally, it should be based on the tumors' individual biology. We established two novel patient-derived primary cell lines from surgical PDAC specimens. LuPanc-1 and LuPanc-2 were derived from a pT3, pN1, G2 and a pT3, pN2, G3 tumor, respectively, and the clinical follow-up was fully annotated. STR-genotyping revealed a unique profile for both cell lines. The population doubling time of LuPanc-2 was substantially longer than that of LuPanc-1 (84 vs. 44 h). Both cell lines exhibited a typical epithelial morphology and expressed moderate levels of CK7 and E-cadherin. LuPanc-1, but not LuPanc-2, co-expressed E-cadherin and vimentin at the single-cell level, suggesting a mixed epithelial-mesenchymal differentiation. LuPanc-1 had a missense mutation (p.R282W) and LuPanc-2 had a frameshift deletion (p.P89X) in TP53. BRCA2 was nonsense-mutated (p.Q780*) and CREBBP was missense-mutated (p.P279R) in LuPanc-1. CDKN2A was missense-mutated (p.H83Y) in LuPanc-2. Notably, only LuPanc-2 harbored a partial or complete deletion of DPC4. LuPanc-1 cells exhibited high basal and transforming growth factor (TGF)-β1-induced migratory activity in real-time cell migration assays, while LuPanc-2 was refractory. Both LuPanc-1 and LuPanc-2 cells responded to treatment with TGF-β1 with the activation of SMAD2; however, only LuPanc-1 cells were able to induce TGF-β1 target genes, which is consistent with the absence of DPC4 in LuPanc-2 cells. Both cell lines were able to form spheres in a semi-solid medium and in cell viability assays, LuPanc-1 cells were more sensitive than LuPanc-2 cells to treatment with gemcitabine and FOLFIRINOX. In summary, both patient-derived cell lines show distinct molecular phenotypes reflecting their individual tumor biology, with a unique clinical annotation of the respective patients. These preclinical ex vivo models can be further explored for potential new treatment strategies and might help in developing personalized (targeted) therapy regimens.

Keywords: pancreatic cancer; patient-derived cancer model; precision medicine; primary cell line.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antineoplastic Combined Chemotherapy Protocols
Cadherins / metabolism
Carcinoma, Pancreatic Ductal* / pathology
Cell Line, Tumor
Gemcitabine
Humans
Pancreatic Neoplasms* / pathology
Transforming Growth Factor beta1 / metabolism

Substances

Transforming Growth Factor beta1
Gemcitabine
Cadherins

Grants and funding

This work was supported in part by grants from the German Research Foundation (DFG) through the Clinician Scientist School Lübeck (DFG #413535489), the Junior Funding Program of the University of Lübeck, and the Brigitte and Dr. Konstanze Wegener Foundation (project # 81).