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6 results on '"Fehse, Boris"'

1. The Histogenetic Origin of Malignant Cells Predicts Their Susceptibility towards Synthetic Lethality Utilizing the TK.007 System.

Author

Pallasch, Fabian Bernhard, Freytag, Vera, Kriegs, Malte, Gatzemeier, Dennis, Mair, Thomas, Voss, Hannah, Riecken, Kristoffer, Dawood, Mona, Fehse, Boris, Efferth, Thomas, Schlüter, Hartmut, and Schumacher, Udo

Subjects
MITOGEN-activated protein kinases, GANCICLOVIR, DISEASE vectors, HERPESVIRUSES, GENETIC engineering, CELL proliferation, APOPTOSIS, TREATMENT effectiveness, LYMPHOMAS, DESCRIPTIVE statistics, CELL lines, GENE expression, LEUKEMIA, CANCER chemotherapy, MESSENGER RNA, GENE expression profiling, PROTEOMICS, DISEASE susceptibility, TRANSFERASES, HISTOLOGY, SEQUENCE analysis, SIGNAL peptides, PHARMACODYNAMICS
Abstract

Simple Summary: The efficacy of killing human cancer cells with a modified herpes simplex virus thymidine kinase TK.007/ganciclovir (GCV) system was investigated in malignant cells of different histogenetic origin. The aim was to determine whether different histogenetic origins of cancer cells in themselves influence their reaction towards an approach of synthetic lethality, which theoretically should be toxic in a similar range independently of the cell type. Fifteen malignant human cell lines were transduced with a lentiviral vector to stably express the TK.007 gene and cell proliferation assays under GCV. Among TK.007-expressing cell lines, lymphoma and leukemia cells were more susceptible to killing than solid cancer cells, while osteosarcoma and melanoma cells exhibited an intermediate susceptibility. This study highlights that the histogenetic origin of malignant cells strongly influences their susceptibility towards cytotoxic agents, with leukemias and lymphomas being more sensitive than solid cancer cells. Background: Remarkable differences exist in the outcome of systemic cancer therapies. Lymphomas and leukemias generally respond well to systemic chemotherapies, while solid cancers often fail. We engineered different human cancer cells lines to uniformly express a modified herpes simplex virus thymidine kinase TK.007 as a suicide gene when ganciclovir (GCV) is applied, thus in theory achieving a similar response in all cell lines. Methods: Fifteen different cell lines were engineered to express the TK.007 gene. XTT-cell proliferation assays were performed and the IC50-values were calculated. Functional kinome profiling, mRNA sequencing, and bottom-up proteomics analysis with Ingenuity pathway analysis were performed. Results: GCV potency varied among cell lines, with lymphoma and leukemia cells showing higher susceptibility than solid cancer cells. Functional kinome profiling implies a contribution of the SRC family kinases and decreased overall kinase activity. mRNA sequencing highlighted alterations in the MAPK pathways and bottom-up proteomics showed differences in apoptotic and epithelial junction signaling proteins. Conclusions: The histogenetic origin of cells influenced the susceptibility of human malignant cells towards cytotoxic agents with leukemias and lymphomas being more sensitive than solid cancer cells. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Combined Targeting of AKT and mTOR Inhibits Tumor Formation of EpCAM+ and CD90+ Human Hepatocellular Carcinoma Cells in an Orthotopic Mouse Model

Author

Moustafa, Mohamed, primary, Dähling, Katarzyna-Krystyna, additional, Günther, Armin, additional, Riebandt, Leonie, additional, Smit, Daniel J., additional, Riecken, Kristoffer, additional, Schröder, Carina, additional, Zhuang, Ruimeng, additional, Krech, Till, additional, Kriegs, Malte, additional, Fehse, Boris, additional, Izbicki, Jakob R., additional, Fischer, Lutz, additional, Nashan, Björn, additional, Li, Jun, additional, and Jücker, Manfred, additional

Published
2022
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5. Combined Targeting of AKT and mTOR Inhibits Tumor Formation of EpCAM + and CD90 + Human Hepatocellular Carcinoma Cells in an Orthotopic Mouse Model.

Author

Moustafa, Mohamed, Dähling, Katarzyna-Krystyna, Günther, Armin, Riebandt, Leonie, Smit, Daniel J., Riecken, Kristoffer, Schröder, Carina, Zhuang, Ruimeng, Krech, Till, Kriegs, Malte, Fehse, Boris, Izbicki, Jakob R., Fischer, Lutz, Nashan, Björn, Li, Jun, and Jücker, Manfred

Subjects
IN vitro studies, XENOGRAFTS, ANIMAL experimentation, SIGNAL peptides, TRANSFERASES, CELL adhesion molecules, CELL proliferation, HEPATOCELLULAR carcinoma, MICE, DRUG resistance in cancer cells
Abstract

Simple Summary: Cancer stem cells are a distinct tumor subpopulation associated with poor outcome. The epithelial cell adhesion molecule (EpCAM) and Thy-1 cell surface antigen (CD90) have been implicated as cancer stem cell (CSC) markers in hepatocellular carcinoma (HCC). Eradication of those CSCs is of high importance with respect to the outcome of treatment. We aimed to verify the impact of targeting HCC cells expressing the CSC marker CD90 and EpCAM with combined therapy of AKT and mTOR inhibitors. Our data demonstrated that combined targeting of AKT and mTOR is highly synergistic in vitro but leads to treatment resistance of xenograft tumors in an orthotopic mouse model in vivo. The development of resistance was observed in large numbers of MK2206/RAD001 treated cells. Restoration of phosphorylated AKT was observed in most tumors during AKT/mTOR therapy underlining the importance of restored AKT signaling as a resistance mechanism. Further work is required to verify the molecular mechanisms of HCC treatment resistance. The epithelial cell adhesion molecule (EpCAM) and Thy-1 cell surface antigen (CD90) have been implicated as cancer stem cell (CSC) markers in hepatocellular carcinoma (HCC). Expression of EpCAM and CD90 on HCC cells is associated with increased tumorigenicity, metastasis and poor prognosis. In this study, we demonstrate that combined treatment with AKT and mTOR inhibitors—i.e., MK2206 and RAD001—results in a synergistic reduction in proliferation of EpCAM+ and CD90+ HCC cells cultured either as adherent cells or as tumoroids in vitro. In addition, tumor growth was reduced by combined treatment with AKT and mTOR inhibitors in an orthotopic xenograft mouse model of an EpCAM+ HCC cell line (Huh7) and primary patient-derived EpCAM+ HCC cells (HCC1) as well as a CD90+ HCC-related cell line (SK-HEP1) in vivo. However, during AKT/mTOR treatment, outgrowth of therapy-resistant tumors was observed in all mice analyzed within a few weeks. Resistance was associated in most cases with restoration of AKT signaling in the tumors, intrahepatic metastases and distant metastases. In addition, an upregulation of the p38 MAPK pathway was identified in the AKT/mTOR inhibitor-resistant tumor cells by kinome profiling. The development of resistant cells during AKT/mTOR therapy was further analyzed by red-green-blue (RGB) marking of HCC cells, which revealed an outgrowth of a large number of Huh7 cells over a period of 6 months. In summary, our data demonstrate that combined treatment with AKT and mTOR inhibitors exhibits synergistic effects on proliferation of EpCAM+ as well as CD90+ HCC cells in vitro. However, the fast development of large numbers of resistant clones under AKT/mTOR therapy observed in vitro and in the orthotopic xenotransplantation mouse model in vivo strongly suggests that this therapy alone will not be sufficient to eliminate EpCAM+ or CD90+ cancer stem cells from HCC patients. [ABSTRACT FROM AUTHOR]

Published
2022
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