Your search keyword '"Eva Juengel"' showing total 120 results

1. Artesunate Inhibits the Growth Behavior of Docetaxel-Resistant Prostate Cancer Cells

Author

Olesya Vakhrusheva, Holger H. H. Erb, Vitus Bräunig, Sascha D. Markowitsch, Patricia Schupp, Patrick C. Baer, Kimberly Sue Slade, Anita Thomas, Igor Tsaur, Martin Puhr, Zoran Culig, Jindrich Cinatl, Martin Michaelis, Thomas Efferth, Axel Haferkamp, and Eva Juengel

Subjects

prostate cancer (PCa), docetaxel (DX) resistance, artesunate (ART), Traditional Chinese Medicine (TCM), growth inhibition, apoptosis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Novel therapeutic strategies are urgently needed for advanced metastatic prostate cancer (PCa). Phytochemicals used in Traditional Chinese Medicine seem to exhibit tumor suppressive properties. Therefore, the therapeutic potential of artesunate (ART) on the progressive growth of therapy-sensitive (parental) and docetaxel (DX)-resistant PCa cells was investigated. Parental and DX-resistant PCa cell lines DU145, PC3, and LNCaP were incubated with artesunate (ART) [1-100 µM]. ART-untreated and ‘non-cancerous’ cells served as controls. Cell growth, proliferation, cell cycle progression, cell death and the expression of involved proteins were evaluated. ART, dose- and time-dependently, significantly restricted cell growth and proliferation of parental and DX-resistant PCa cells, but not of ‘normal, non-cancerous’ cells. ART-induced growth and proliferation inhibition was accompanied by G0/G1 phase arrest and down-regulation of cell cycle activating proteins in all DX-resistant PCa cells and parental LNCaP. In the parental and DX-resistant PC3 and LNCaP cell lines, ART also promoted apoptotic cell death. Ferroptosis was exclusively induced by ART in parental and DX-resistant DU145 cells by increasing reactive oxygen species (ROS). The anti-cancer activity displayed by ART took effect in all three PCa cell lines, but through different mechanisms of action. Thus, in advanced PCa, ART may hold promise as a complementary treatment together with conventional therapy.

Published

2022

2. Assessment of STAT5 as a potential therapy target in enzalutamide-resistant prostate cancer.

Author

Holger H H Erb, Julia Bodenbender, Florian Handle, Tamara Diehl, Lukas Donix, Igor Tsaur, Martin Gleave, Axel Haferkamp, Johannes Huber, Susanne Fuessel, Eva Juengel, Zoran Culig, and Christian Thomas

Subjects

Medicine, Science

Abstract

Despite enzalutamide's efficacy in delaying the progression of metastatic castration-resistant prostate cancer (CRPC), resistance to this anti-androgen inevitably occurs. Several studies have revealed that the signal transducer and activator of transcription (STAT) 5 plays a role in tumour progression and development of drug resistance such as enzalutamide. Data mining revealed heterogeneous expression of STAT5 in enzalutamide-treated mCRPC patients and enzalutamide-resistant prostate cancer (PCa). Isobologram analysis revealed that the STAT5 inhibitor pimozide combined with enzalutamide has? additive and synergistic inhibitory effects on cell viability in the used models. Functional analysis with siRNA-mediated STAT5 knockdown yielded divergent results. The LNCaP-derived cell line MR49F could be resensitised to enzalutamide by siRNA-mediated STAT5b-knock-down. In contrast, neither STAT5a nor STAT5b knockdown resensitised enzalutamide-resistant LAPC4-EnzaR cells to enzalutamide. In conclusion, our results indicate that STAT5 may be a possible target in a subgroup of enzalutamide-resistant PCa. However, based on the data presented here, a general role of STAT5 in enzalutamide-resistance and its potential as a therapeutic target could not be shown.

Published

2020

3. Antiangiogenic Properties of Axitinib versus Sorafenib Following Sunitinib Resistance in Human Endothelial Cells—A View towards Second Line Renal Cell Carcinoma Treatment

Author

Eva Juengel, Pascal Schnalke, Jochen Rutz, Sebastian Maxeiner, Felix K.-H. Chun, and Roman A. Blaheta

Subjects

renal cell carcinoma, tyrosine kinase inhibitors, endothelial cells, resistance, second-line, Biology (General), QH301-705.5

Abstract

Tyrosine kinase inhibitors (TKIs) and immune checkpoint inhibitors predominate as first-line therapy options for renal cell carcinoma. When first-line TKI therapy fails due to resistance development, an optimal second-line therapy has not yet been established. The present investigation is directed towards comparing the anti-angiogenic properties of the TKIs, sorafenib and axitinib on human endothelial cells (HUVECs) with acquired resistance towards the TKI sunitinib. HUVECs were driven to resistance by continuously exposing them to sunitinib for six weeks. They were then switched to a 24 h or further six weeks treatment with sorafenib or axitinib. HUVEC growth, as well as angiogenesis (tube formation and scratch wound assay), were evaluated. Cell cycle proteins of the CDK-cyclin axis (CDK1 and 2, total and phosphorylated, cyclin A and B) and the mTOR pathway (AKT, total and phosphorylated) were also assessed. Axitinib (but not sorafenib) significantly suppressed growth of sunitinib-resistant HUVECs when they were exposed for six weeks. This axinitib-associated growth reduction was accompanied by a cell cycle block at the G0/G1-phase. Both axitinib and sorafenib reduced HUVEC tube length and prevented wound closure (sorafenib > axitinib) when applied to sunitinib-resistant HUVECs for six weeks. Protein analysis revealed diminished phosphorylation of CDK1, CDK2 and pAKT, accompanied by a suppression of cyclin A and B. Both drugs modulated CDK-cyclin and AKT-dependent signaling, associated either with both HUVEC growth and angiogenesis (axitinib) or angiogenesis alone (sorafenib). Axitinib and sorafenib may be equally applicable as second line treatment options, following sunitinib resistance.

Published

2021

4. Deciphering the Molecular Machinery—Influence of sE-Cadherin on Tumorigenic Traits of Prostate Cancer Cells

Author

Igor Tsaur, Anita Thomas, Eva Juengel, Sebastian Maxeiner, Timothy Grein, Quynh Chi Le, Veronika Muschta, Jochen Rutz, Felix K. H. Chun, and Roman A. Blaheta

Subjects

prostate cancer, sE-cadherin, cell growth, migration, metastasis, Biology (General), QH301-705.5

Abstract

The serum level of soluble (s)E-cadherin is elevated in several malignancies, including prostate cancer (PCa). This study was designed to investigate the effects of sE-cadherin on the behavior of PCa cells in vitro, with the aim of identifying a potential therapeutic target. Growth as well as adhesive and motile behavior were evaluated in PC3, DU-145, and LNCaP cells. Flow cytometry was used to assess cell cycle phases and the surface expression of CD44 variants as well as α and β integrins. Confocal microscopy was utilized to visualize the distribution of CD44 variants within the cells. Western blot was applied to investigate expression of α3 and β1 integrins as well as cytoskeletal and adhesion proteins. Cell growth was significantly inhibited after exposure to 5 µg/mL sE-cadherin and was accompanied by a G0/G1-phase arrest. Adhesion of cells to collagen and fibronectin was mitigated, while motility was augmented. CD44v4, v5, and v7 expression was elevated while α3 and β1 integrins were attenuated. Blocking integrin α3 reduced cell growth and adhesion to collagen but increased motility. sE-cadherin therefore appears to foster invasive tumor cell behavior, and targeting it might serve as a novel and innovative concept to treat advanced PCa.

Published

2021

5. Artesunate Impairs Growth in Cisplatin-Resistant Bladder Cancer Cells by Cell Cycle Arrest, Apoptosis and Autophagy Induction

Author

Fuguang Zhao, Olesya Vakhrusheva, Sascha D. Markowitsch, Kimberly S. Slade, Igor Tsaur, Jindrich Cinatl, Martin Michaelis, Thomas Efferth, Axel Haferkamp, and Eva Juengel

Subjects

bladder cancer (BCa), artesunate (ART), cisplatin resistance, growth inhibition, apoptosis, autophagy, Cytology, QH573-671

Abstract

Cisplatin, which induces DNA damage, is standard chemotherapy for advanced bladder cancer (BCa). However, efficacy is limited due to resistance development. Since artesunate (ART), a derivative of artemisinin originating from Traditional Chinese Medicine, has been shown to exhibit anti-tumor activity, and to inhibit DNA damage repair, the impact of artesunate on cisplatin-resistant BCa was evaluated. Cisplatin-sensitive (parental) and cisplatin-resistant BCa cells, RT4, RT112, T24, and TCCSup, were treated with ART (1–100 µM). Cell growth, proliferation, and cell cycle phases were investigated, as were apoptosis, necrosis, ferroptosis, autophagy, metabolic activity, and protein expression. Exposure to ART induced a time- and dose-dependent significant inhibition of tumor cell growth and proliferation of parental and cisplatin-resistant BCa cells. This inhibition was accompanied by a G0/G1 phase arrest and modulation of cell cycle regulating proteins. ART induced apoptos is by enhancing DNA damage, especially in the resistant cells. ART did not induce ferroptosis, but led to a disturbance of mitochondrial respiration and ATP generation. This impairment correlated with autophagy accompanied by a decrease in LC3B-I and an increase in LC3B-II. Since ART significantly inhibits proliferative and metabolic aspects of cisplatin-sensitive and cisplatin-resistant BCa cells, it may hold potential in treating advanced and therapy-resistant BCa.

Published

2020

6. Levosimendan protects human hepatocytes from ischemia-reperfusion injury.

Author

Stefanie N Brunner, Nicolai V Bogert, Andreas A Schnitzbauer, Eva Juengel, Anton Moritz, Isabella Werner, Angela Kornberger, and Andres Beiras-Fernandez

Subjects

Medicine, Science

Abstract

Ischemia-reperfusion injury (IRI) is a major challenge in liver transplantation. The mitochondrial pathway plays a pivotal role in hepatic IRI. Levosimendan, a calcium channel sensitizer, was shown to attenuate apoptosis after IRI in animal livers. The aim of this study was to investigate the effect of levosimendan on apoptosis in human hepatocytes.Primary human hepatocytes were either exposed to hypoxia or cultured under normoxic conditions. After the hypoxic phase, reoxygenation was implemented and cells were treated with different concentrations of levosimendan (10ng/ml, 100ng/ml, 1000ng/ml). The overall metabolic activity of the cells was measured using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT), and aspartate aminotransferase (AST) levels were determined in order to quantify hepatic injury. Fluorescence-activated cell sorting (FACS) analysis was applied to measure necrosis and apoptosis. Finally, Western blotting was performed to analyze apoptotic pathway proteins.Administration of levosimendan during reperfusion increases the metabolic activity of human hepatocytes and decreases AST levels. Moreover, apoptosis after IRI is reduced in treated vs. untreated hepatocytes, and levosimendan prevents down-regulation of the anti-apoptotic protein Bcl-2 as well as up-regulation of the pro-apoptotic protein BAX.The present study suggests a protective effect of levosimendan on human hepatocytes. Our findings suggest that treatment with levosimendan during reperfusion attenuates apoptosis of human hepatocytes by influencing BAX and Bcl-2 levels.

Published

2017

7. Resistance to the mTOR Inhibitor Temsirolimus Alters Adhesion and Migration Behavior of Renal Cell Carcinoma Cells through an Integrin α5– and Integrin β3–Dependent Mechanism

Author

Eva Juengel, Jasmina Makarević, Michael Reiter, Jens Mani, Igor Tsaur, Georg Bartsch, Axel Haferkamp, and Roman A. Blaheta

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Inhibitors of the mammalian target of rapamycin (mTOR) have improved the treatment of renal cell carcinoma (RCC). However, chronic drug exposure may trigger resistance, limiting the utility of these agents. The metastatic behavior of RCC cells, susceptible (RCCpar) or resistant (RCCres) to the mTOR inhibitor temsirolimus, was investigated. Adhesion to vascular endothelium or immobilized collagen and fibronectin was quantified. Chemotactic motility was evaluated with a modified Boyden chamber assay. Integrin α and β subtype receptors were analyzed by flow cytometry and Western blot analysis. The physiological relevance of the integrins was then determined by blocking studies and small interfering RNA knockdown. Adhesion to endothelial cells and to fibronectin (not to collagen) and chemotaxis were enhanced in RCCres compared to RCCpar. RCCres detached from fibronectin and motile activity further increased under retreatment with low-dosed temsirolimus. α5 integrin was diminished inside the cell and at the cell surface, whereas the β3 subtype was reduced intracellularly but elevated at the plasma membrane. In RCCpar, blocking α5 surface receptors enhanced RCC-collagen but reduced RCC-fibronectin interaction, whereas the opposite was true for RCCres. Chemotaxis of RCCpar but not of RCCres was strongly diminished by the α5 antibody. Blocking β3 significantly lowered chemotaxis with stronger effects on RCCres, compared to RCCpar. Importantly, β3 knockdown reduced chemotaxis of RCCpar but upregulated the motile behavior of RCCres. Temsirolimus resistance is characterized by quantitative alterations of integrin α5 and β3 expression, coupled to functional changes of the integrin molecules, and forces a switch from RCC adhesion to RCC migration.

Published

2014

8. MicroRNA-145 Targets the Metalloprotease ADAM17 and Is Suppressed in Renal Cell Carcinoma Patients

Author

Kai Doberstein, Nico Steinmeyer, Ann-Kathrin Hartmetz, Wolfgang Eberhardt, Michel Mittelbronn, Patrick N. Harter, Eva Juengel, Roman Blaheta, Josef Pfeilschifter, and Paul Gutwein

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

A disintegrin and metalloproteinase 17 (ADAM17) is a metalloprotease that is overexpressed in many cancer types, including renal cancers. However, the regulatory mechanisms of ADAM17 in cancer development and progression are poorly understood. In the present work, we provide evidence using overexpression and inhibition of microRNA 145 (miR-145) that miR-145 negatively regulates ADAM17 expression. Furthermore, we show that ADAM17 negatively regulates miR-145 through tumor necrosis factor-α, resulting in a reciprocal negative feedback loop. In this study, the expression of ADAM17 and miR-145 correlated negatively in renal cancer tumor tissues and cell lines, suggesting an important regulatory mechanism. Additionally, we showed that the regulation of ADAM17 is partly involved in the effects of miR-145 on proliferation and migration, whereas no involvement in chemosensitivity was observed. Importantly, in the healthy kidney, miR-145 was detected in different cell types including tubular cells, which are considered the origin of renal cancer. In renal cancer cell lines, miR-145 expression was strongly suppressed by methylation. In summary, miR-145 is downregulated in renal cancer patients, which leads to the up-regulation of ADAM17 in renal cancer. Importantly, miR-145 and ADAM17 are regulated in a reciprocal negative feedback loop.

Published

2013

9. HDAC Inhibition Counteracts Metastatic Re-Activation of Prostate Cancer Cells Induced by Chronic mTOR Suppression

Author

Jasmina Makarević, Jochen Rutz, Eva Juengel, Sebastian Maxeiner, Jens Mani, Stefan Vallo, Igor Tsaur, Frederik Roos, Felix K.-H. Chun, and Roman A. Blaheta

Subjects

mTOR, histone deacetylase, prostate cancer, integrins, adhesion, invasion, Cytology, QH573-671

Abstract

This study was designed to investigate whether epigenetic modulation by histone deacetylase (HDAC) inhibition might circumvent resistance towards the mechanistic target of rapamycin (mTOR) inhibitor temsirolimus in a prostate cancer cell model. Parental (par) and temsirolimus-resistant (res) PC3 prostate cancer cells were exposed to the HDAC inhibitor valproic acid (VPA), and tumor cell adhesion, chemotaxis, migration, and invasion were evaluated. Temsirolimus resistance was characterized by reduced binding of PC3res cells to endothelium, immobilized collagen, and fibronectin, but increased adhesion to laminin, as compared to the parental cells. Chemotaxis, migration, and invasion of PC3res cells were enhanced following temsirolimus re-treatment. Integrin α and β receptors were significantly altered in PC3res compared to PC3par cells. VPA significantly counteracted temsirolimus resistance by down-regulating tumor cell–matrix interaction, chemotaxis, and migration. Evaluation of integrin expression in the presence of VPA revealed a significant down-regulation of integrin α5 in PC3res cells. Blocking studies demonstrated a close association between α5 expression on PC3res and chemotaxis. In this in vitro model, temsirolimus resistance drove prostate cancer cells to become highly motile, while HDAC inhibition reversed the metastatic activity. The VPA-induced inhibition of metastatic activity was accompanied by a lowered integrin α5 surface level on the tumor cells.

Published

2018

10. Tumor-Endothelium Cross Talk Blocks Recruitment of Neutrophils to Endothelial Cells: A Novel Mechanism of Endothelial Cell Anergy

Author

Roman A. Blaheta, Maciej Powerski, Lukasz Hudak, Eva Juengel, Dietger Jonas, Andreas von Knethen, Hans Willhelm Doerr, and Jindrich Cinatl, Jr

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Tumor cells have evolved effective strategies to escape the host immune response. The objective of this study was to determine whether tumor cells can condition endothelial cells in a specific manner to prevent subsequent adhesion of polymorphonuclear neutrophils (PMNs) and/or peripheral blood lymphocytes (PBLs). Human umbilical vein endothelial cells (HUVECs) and UKF-NB-4 neuroblastoma tumor cells were established in coculture on opposite sides of porous transwell filters. After 24 hours with and without HUVEC conditioning, PMNs or PBLs were added to the HUVEC monolayer. Adhesion to conditioned HUVEC versus adhesion to nonconditioned HUVEC was compared. Effects on endothelial CD44v4, CD44v5, CD44v7, intercellular adhesion molecule 1 (ICAM-1), E-selectin, and vascular cell adhesion molecule 1 (VCAM-1) adhesion receptor expression were analyzed by flow cytometry, intracellular signaling proteins of the mitogen-activated protein kinase pathway and protein kinase C (PKC) subtypes quantified by Western blot analysis. Endothelial conditioning led to a distinct reduction in PMN but not in PBL adhesion to HUVEC. CD44 was significantly reduced, whereas ICAM-1, E-selectin, and VCAM-1 were not altered during HUVEC conditioning. Antibody blockade against CD44v4, CD44v5, and CD44v7 inhibited PMN but not PBL binding. The observed effects were caused by direct tumor cell-HUVEC contact because addition of isolated tumor cell membrane fragments but not of soluble cell culture supernatant to HUVEC induced the CD44 receptor loss. PKCα activity was strongly enhanced in conditioned HUVEC. Blocking PKC prevented the reduction in PMN binding, indicating that this protein is involved in PMN adhesion regulation. A novel tumor escape strategy is presented here. Cell contact-dependent adhesion of tumor cells to the vascular wall promotes down-regulation of endothelial CD44 receptor expression, impairing an effective neutrophil attack.

Published

2009

11. Amygdalin influences bladder cancer cell adhesion and invasion in vitro.

Author

Jasmina Makarević, Jochen Rutz, Eva Juengel, Silke Kaulfuss, Igor Tsaur, Karen Nelson, Jesco Pfitzenmaier, Axel Haferkamp, and Roman A Blaheta

Subjects

Medicine, Science

Abstract

The cyanogenic diglucoside amygdalin, derived from Rosaceae kernels, is employed by many patients as an alternative anti-cancer treatment. However, whether amygdalin indeed acts as an anti-tumor agent is not clear. Metastasis blocking properties of amygdalin on bladder cancer cell lines was, therefore, investigated. Amygdalin (10 mg/ml) was applied to UMUC-3, TCCSUP or RT112 bladder cancer cells for 24 h or for 2 weeks. Tumor cell adhesion to vascular endothelium or to immobilized collagen as well as tumor cell migration was examined. Effects of drug treatment on integrin α and β subtypes, on integrin-linked kinase (ILK) and total and activated focal adhesion kinase (FAK) were also determined. Integrin knock-down was carried out to evaluate integrin influence on migration and adhesion. A 24 h or 2 week amygdalin application distinctly reduced tumor cell adhesion and migration of UMUC-3 and RT112 cells. TCCSUP adhesion was also reduced, but migration was elevated under amygdalin. Integrin subtype expression was significantly and specifically altered by amygdalin depending on the cell line. ILK was moderately, and activated FAK strongly, lost in all tumor cell lines in the presence of amygdalin. Knock down of β1 integrin caused a significant decrease in both adhesion and migration of UMUC-3 cells, but a significant increase in TCCSUP adhesion. Knock down of β4 integrin caused a significant decrease in migration of RT112 cells. Since the different actions of amygdalin on the different cell lines was mirrored by β1 or β4 knock down, it is postulated that amygdalin influences adhesion and migratory properties of bladder cancer cells by modulating β1 or β4 integrin expression. The amygdalin induced increase in TCCSUP migratory behavior indicates that any anti-tumor benefits from amygdalin (seen with the other two cell lines) may depend upon the cancer cell type.

Published

2014

12. Amygdalin blocks bladder cancer cell growth in vitro by diminishing cyclin A and cdk2.

Author

Jasmina Makarević, Jochen Rutz, Eva Juengel, Silke Kaulfuss, Michael Reiter, Igor Tsaur, Georg Bartsch, Axel Haferkamp, and Roman A Blaheta

Subjects

Medicine, Science

Abstract

Amygdalin, a natural compound, has been used by many cancer patients as an alternative approach to treat their illness. However, whether or not this substance truly exerts an anti-tumor effect has never been settled. An in vitro study was initiated to investigate the influence of amygdalin (1.25-10 mg/ml) on the growth of a panel of bladder cancer cell lines (UMUC-3, RT112 and TCCSUP). Tumor growth, proliferation, clonal growth and cell cycle progression were investigated. The cell cycle regulating proteins cdk1, cdk2, cdk4, cyclin A, cyclin B, cyclin D1, p19, p27 as well as the mammalian target of rapamycin (mTOR) related signals phosphoAkt, phosphoRaptor and phosphoRictor were examined. Amygdalin dose-dependently reduced growth and proliferation in all three bladder cancer cell lines, reflected in a significant delay in cell cycle progression and G0/G1 arrest. Molecular evaluation revealed diminished phosphoAkt, phosphoRictor and loss of Cdk and cyclin components. Since the most outstanding effects of amygdalin were observed on the cdk2-cyclin A axis, siRNA knock down studies were carried out, revealing a positive correlation between cdk2/cyclin A expression level and tumor growth. Amygdalin, therefore, may block tumor growth by down-modulating cdk2 and cyclin A. In vivo investigation must follow to assess amygdalin's practical value as an anti-tumor drug.

Published

2014

13. I publish in I edit?--Do editorial board members of urologic journals preferentially publish their own scientific work?

Author

Jens Mani, Jasmina Makarević, Eva Juengel, Hanns Ackermann, Karen Nelson, Georg Bartsch, Axel Haferkamp, and Roman A Blaheta

Subjects

Medicine, Science

Abstract

Scientists who are members of an editorial board have been accused of preferentially publishing their scientific work in the journal where they serve as editor. Reputation and academic standing do depend on an uninterrupted flow of published scientific work and the question does arise as to whether publication mainly occurs in the self-edited journal. This investigation was designed to determine whether editorial board members of five urological journals were more likely to publish their research reports in their own rather than in other journals. A retrospective analysis was conducted for all original reports published from 2001-2010 by 65 editorial board members nominated to the boards of five impact leading urologic journals in 2006. Publications before editorial board membership, 2001-2005, and publications within the period of time as an editorial board member, 2006-2010, were identified. The impact factors of the journals were also recorded over the time period 2001-2010 to see whether a change in impact factor correlated with publication locality. In the five journals as a whole, scientific work was not preferentially published in the journal in which the scientists served as editor. However, significant heterogeneity among the journals was evident. One journal showed a significant increase in the amount of published papers in the 'own' journal after assumption of editorship, three journals showed no change and one journal showed a highly significant decrease in publishing in the 'own' journal after assumption of editorship.

Published

2013

14. Resistance after chronic application of the HDAC-inhibitor valproic acid is associated with elevated Akt activation in renal cell carcinoma in vivo.

Author

Eva Juengel, Jasmina Makarević, Igor Tsaur, Georg Bartsch, Karen Nelson, Axel Haferkamp, and Roman A Blaheta

Subjects

Medicine, Science

Abstract

Targeted drugs have significantly improved the therapeutic options for advanced renal cell carcinoma (RCC). However, resistance often develops, negating the benefit of these agents. In the present study, the molecular mechanisms of acquired resistance towards the histone deacetylase (HDAC) inhibitor valproic acid (VPA) in a RCC in vivo model were investigated. NMRI:nu/nu mice were transplanted with Caki-1 RCC cells and then treated with VPA (200 mg/kg/day). Controls remained untreated. Based on tumor growth dynamics, the mice were divided into "responders" and "non-responders" to VPA. Histone H3 and H4 acetylation and expression of cell signaling and cell cycle regulating proteins in the RCC mouse tumors were evaluated by Western blotting. Tumor growth of VPA responders was significantly diminished, whereas that of VPA non-responders even exceeded control values. Cdk1, 2 and 4 proteins were strongly enhanced in the non-responders. Importantly, Akt expression and activity were massively up-regulated in the tumors of the VPA non-responders. Chronic application (12 weeks) of VPA to Caki-1 cells in vitro evoked a distinct elevation of Akt activity and cancer cells no longer responded with cell growth reduction, compared to the short 2 week treatment. We assume that chronic use of an HDAC-inhibitor is associated with (re)-activation of Akt, which may be involved in resistance development. Consequently, combined blockade of both HDAC and Akt may delay or prevent drug resistance in RCC.

Published

2013

15. Publication of original research in urologic journals--a neglected orphan?

Author

Jens Mani, Jasmina Makarević, Eva Juengel, Hanns Ackermann, Karen Nelson, Axel Haferkamp, and Roman A Blaheta

Subjects

Medicine, Science

Abstract

The pathophysiologic mechanisms behind urologic disease are increasingly being elucidated. The object of this investigation was to evaluate the publication policies of urologic journals during a period of progressively better understanding and management of urologic disease. Based on the ISI Web of Knowledge Journal Citation Reports and the PubMed database, the number and percentage of original experimental, original clinical, review or commentarial articles published between 2002-2010 in six leading urologic journals were analyzed. "British Journal of Urology International", "European Urology", "Urologic Oncology-Seminars and Original Investigations" ("Urologic Oncology"), "Urology", "The Journal of Urology", and "World Journal of Urology" were chosen, because these journals publish articles in all four categories. The publication policies of the six journals were very heterogeneous during the time period from 2002 to 2010. The percentage of original experimental and original clinical articles, related to all categories, remained the same in "British Journal of Urology International", "Urologic Oncology", "Urology" and "The Journal of Urology". The percentage of experimental reports in "World Journal of Urology" between 2002-2010 significantly increased from 10 to 20%. A distinct elevation in the percentage of commentarial articles accompanied by a reduction of clinical articles became evident in "European Urology" which significantly correlated with a large increase in the journal's impact factor. No clearly superior policy could be identified with regard to a general increase in the impact factors from all the journals. The publication policy of urologic journals does not expressly reflect the increase in scientific knowledge, which has occurred over the period 2002-2010. One way of increasing the exposure of urologists to research and expand the interface between experimental and clinical research, would be to enlarge the percentage of experimental articles published. There is no indication that such policy would be detrimental to a journal's impact factor.

Published

2012

16. Plant-Derived Sulforaphane Suppresses Growth and Proliferation of Drug-Sensitive and Drug-Resistant Bladder Cancer Cell Lines In Vitro

Author

Hui Xie, Jochen Rutz, Sebastian Maxeiner, Timothy Grein, Anita Thomas, Eva Juengel, Felix K.-H. Chun, Jindrich Cinatl, Axel Haferkamp, Igor Tsaur, and Roman A. Blaheta

Subjects

Cancer Research, Oncology, sulforaphane, bladder cancer, drug resistance, proliferation, AKT/mTOR

Abstract

Combined cisplatin–gemcitabine (GC) application is standard for treating muscle-invasive bladder cancer. However, since rapid resistance to treatment often develops, many patients turn to supplements in the form of plant-based compounds. Sulforaphane (SFN), derived from cruciferous vegetables, is one such compound, and the present study was designed to investigate its influence on growth and proliferation in a panel of drug-sensitive bladder cancer cell lines, as well as their gemcitabine- and cisplatin-resistant counterparts. Chemo-sensitive and -resistant RT4, RT112, T24, and TCCSUP cell lines were exposed to SFN in different concentrations, and tumor growth, proliferation, and clone formation were evaluated, in addition to apoptosis and cell cycle progression. Means of action were investigated by assaying cell-cycle-regulating proteins and the mechanistic target of rapamycin (mTOR)/AKT signaling cascade. SFN significantly inhibited growth, proliferation, and clone formation in all four tumor cell lines. Cells were arrested in the G2/M and/or S phase, and alteration of the CDK–cyclin axis was closely associated with cell growth inhibition. The AKT/mTOR signaling pathway was deactivated in three of the cell lines. Acetylation of histone H3 was up-regulated. SFN, therefore, does exert tumor-suppressive properties in cisplatin- and gemcitabine-resistant bladder cancer cells and could be beneficial in optimizing bladder cancer therapy.

Published

2022

17. MP46-20 INFLUENCE OF RESISTANCE TO CISPLATIN AND OSIMERTINIB ON PATTERNS OF METASTATIC BEHAVIOR OF PENILE CANCER

Author

Anita Thomas, Shirine Huck, Kimberly Slade, Olesya Vakhrusheva, Martin Michaelis, Jaroslav Jinatl, Florian Rothweiler, Axel Haferkamp, Eva Juengel, Jindrich Cinatl, and Igor Tsaur

Subjects

Urology

Published

2022

18. Immunotherapy in prostate cancer: new horizon of hurdles and hopes

Author

Guillaume Ploussard, Maximilian Peter Brandt, Eva Juengel, Igor Tsaur, and Cécile Manceau

Subjects

Male, Oncology, PD-L1, medicine.medical_specialty, Urology, medicine.medical_treatment, 030232 urology & nephrology, Disease, Pembrolizumab, Malignancy, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Internal medicine, PD-1, medicine, Humans, Tumor microenvironment, business.industry, Prostatic Neoplasms, Immunotherapy, medicine.disease, Topic Paper, Radiation therapy, Tumor progression, 030220 oncology & carcinogenesis, Immune checkpoints, business, Vaccine

Abstract

Purpose Prostate cancer (PCa) is the most common malignancy in men and the cause for the second most common cancer-related death in the western world. Despite ongoing development of novel approaches such as second generation androgen receptor targeted therapies, metastatic disease is still fatal. In PCa, immunotherapy (IT) has not reached a therapeutic breakthrough as compared to several other solid tumors yet. We aimed at highlighting the underlying cellular mechanisms crucial for IT in PCa and giving an update of the most essential past and ongoing clinical trials in the field. Methods We searched for relevant publications on molecular and cellular mechanisms involved in the PCa tumor microenvironment and response to IT as well as completed and ongoing IT studies and screened appropriate abstracts of international congresses. Results Tumor progression and patient outcomes depend on complex cellular and molecular interactions of the tumor with the host immune system, driven rather dormant in case of PCa. Sipuleucel-T and pembrolizumab are the only registered immune-oncology drugs to treat this malignancy. A plethora of studies assess combination of immunotherapy with other agents or treatment modalities like radiation therapy which might increase its antineoplastic activity. No robust and clinically relevant prognostic or predictive biomarkers have been established yet. Conclusion Despite immunosuppressive functional status of PCa microenvironment, current evidence, based on cellular and molecular conditions, encourages further research in this field.

Published

2020

19. Value of c-MET and Associated Signaling Elements for Predicting Outcomes and Targeted Therapy in Penile Cancer

Author

Anita Thomas, Kimberly Sue Slade, Roman A. Blaheta, Sascha D. Markowitsch, Philipp Stenzel, Katrin E. Tagscherer, Wilfried Roth, Mario Schindeldecker, Martin Michaelis, Florian Rothweiler, Jaroslav Cinatl, Robert Dotzauer, Olesya Vakhrusheva, Maarten Albersen, Axel Haferkamp, Eva Juengel, Jindrich Cinatl, and Igor Tsaur

Subjects

squamous cell carcinoma, marker, EXPRESSION, Cancer Research, RM, Science & Technology, penile cancer, c-MET, resistant cell lines, targeted therapy, tivantinib, cabozantinib, INHIBITOR, CHEMOTHERAPY, BETA-CATENIN, RECEPTORS, RC0254, Oncology, RENAL-CELL CARCINOMA, GROWTH, PPAR-GAMMA, Life Sciences & Biomedicine, RESISTANCE

Abstract

Whereas the lack of biomarkers in penile cancer (PeCa) impedes the development of efficacious treatment protocols, preliminary evidence suggests that c-MET and associated signaling elements may be dysregulated in this disorder. In the following study, we investigated whether c-MET and associated key molecular elements may have prognostic and therapeutic utility in PeCa. Formalin-fixed, paraffin-embedded tumor tissue from therapy-naïve patients with invasive PeCa was used for tissue microarray (TMA) analysis. Immunohistochemical staining was performed to determine the expression of the proteins c-MET, PPARg, β-catenin, snail, survivin, and n-MYC. In total, 94 PeCa patients with available tumor tissue were included. The median age was 64.9 years. High-grade tumors were present in 23.4%, and high-risk HPV was detected in 25.5%. The median follow-up was 32.5 months. High expression of snail was associated with HPV-positive tumors. Expression of β-catenin was inversely associated with grading. In both univariate COX regression analysis and the log-rank test, an increased expression of PPARg and c-MET was predictive of inferior disease-specific survival (DSS). Moreover, in multivariate analysis, a higher expression of c-MET was independently associated with worse DSS. Blocking c-MET with cabozantinib and tivantinib induced a significant decrease in viability in the primary PeCa cell line UKF-PeC3 isolated from the tumor tissue as well as in cisplatin- and osimertinib-resistant sublines. Strikingly, a higher sensitivity to tivantinib could be detected in the latter, pointing to the promising option of utilizing this agent in the second-line treatment setting. ispartof: CANCERS vol:14 issue:7 ispartof: location:Switzerland status: published

Published

2022

20. Olive Mill Wastewater Inhibits Growth and Proliferation of Cisplatin- and Gemcitabine-Resistant Bladder Cancer Cells In Vitro by Down-Regulating the Akt/mTOR-Signaling Pathway

Author

Blaheta, Jochen Rutz, Sebastian Maxeiner, Eva Juengel, Felix K.-H. Chun, Igor Tsaur, and Roman A.

Subjects

olive mill wastewater (OMWW), bladder cancer, tumor growth, Akt-mTOR signaling, CDK-cyclin axis

Abstract

Bladder cancer patients whose tumors develop resistance to cisplatin-based chemotherapy often turn to natural, plant-derived products. Beneficial effects have been particularly ascribed to polyphenols, although their therapeutic relevance when resistance has developed is not clear. The present study evaluated the anti-tumor potential of polyphenol-rich olive mill wastewater (OMWW) on chemo-sensitive and cisplatin- and gemcitabine-resistant T24, RT112, and TCCSUP bladder cancer cells in vitro. The cells were treated with different dilutions of OMWW, and tumor growth and clone formation were evaluated. Possible mechanisms of action were investigated by evaluating cell cycle phases and cell cycle-regulating proteins. OMWW profoundly inhibited the growth and proliferation of chemo-sensitive as well as gemcitabine- and cisplatin-resistant bladder cancer cells. Depending on the cell line and on gemcitabine- or cisplatin-resistance, OMWW induced cell cycle arrest at different phases. These differing phase arrests were accompanied by differing alterations in the CDK-cyclin axis. Considerable suppression of the Akt-mTOR pathway by OMWW was observed in all three cell lines. Since OMWW blocks the cell cycle through the manipulation of the cyclin-CDK axis and the deactivation of Akt-mTOR signaling, OMWW could become relevant in supporting bladder cancer therapy.

Published

2022

21. Olive Mill Wastewater Inhibits Growth and Proliferation of Cisplatin- and Gemcitabine-Resistant Bladder Cancer Cells In Vitro by Down-Regulating the Akt/mTOR-Signaling Pathway

Author

Jochen Rutz, Sebastian Maxeiner, Eva Juengel, Felix K.-H. Chun, Igor Tsaur, and Roman A. Blaheta

Subjects

Nutrition. Foods and food supply, CDK-cyclin axis, TOR Serine-Threonine Kinases, Akt-mTOR signaling, olive mill wastewater (OMWW), Polyphenols, Antineoplastic Agents, Apoptosis, Cell Cycle Checkpoints, Wastewater, Deoxycytidine, Gemcitabine, Article, Cyclin-Dependent Kinases, tumor growth, Urinary Bladder Neoplasms, Drug Resistance, Neoplasm, Cell Line, Tumor, Olea, bladder cancer, Humans, TX341-641, Cisplatin, Proto-Oncogene Proteins c-akt, Cell Proliferation

Abstract

Bladder cancer patients whose tumors develop resistance to cisplatin-based chemotherapy often turn to natural, plant-derived products. Beneficial effects have been particularly ascribed to polyphenols, although their therapeutic relevance when resistance has developed is not clear. The present study evaluated the anti-tumor potential of polyphenol-rich olive mill wastewater (OMWW) on chemo-sensitive and cisplatin- and gemcitabine-resistant T24, RT112, and TCCSUP bladder cancer cells in vitro. The cells were treated with different dilutions of OMWW, and tumor growth and clone formation were evaluated. Possible mechanisms of action were investigated by evaluating cell cycle phases and cell cycle-regulating proteins. OMWW profoundly inhibited the growth and proliferation of chemo-sensitive as well as gemcitabine- and cisplatin-resistant bladder cancer cells. Depending on the cell line and on gemcitabine- or cisplatin-resistance, OMWW induced cell cycle arrest at different phases. These differing phase arrests were accompanied by differing alterations in the CDK-cyclin axis. Considerable suppression of the Akt-mTOR pathway by OMWW was observed in all three cell lines. Since OMWW blocks the cell cycle through the manipulation of the cyclin-CDK axis and the deactivation of Akt-mTOR signaling, OMWW could become relevant in supporting bladder cancer therapy.

Published

2022

22. Deciphering the Molecular Machinery—Influence of sE-Cadherin on Tumorigenic Traits of Prostate Cancer Cells

Author

Quynh Chi Le, Veronika Muschta, Felix K.-H. Chun, Anita Thomas, Roman A. Blaheta, Eva Juengel, Jochen Rutz, Sebastian Maxeiner, Igor Tsaur, and Timothy Grein

Subjects

sE-cadherin, General Immunology and Microbiology, biology, Cell growth, Cadherin, QH301-705.5, CD44, Integrin, Motility, Cell cycle, prostate cancer, migration, General Biochemistry, Genetics and Molecular Biology, Article, Cell biology, Fibronectin, LNCaP, biology.protein, cell growth, metastasis, Biology (General), General Agricultural and Biological Sciences

Abstract

Simple Summary Despite recent advances in the therapeutic management of metastasized prostate cancer, disease progression is still inevitable, with often fatal outcomes. Elucidating molecular mechanisms crucial to cancer development and progression is therefore necessary to find ways to interfere in metastatic processes and ultimately improve prognosis. Since soluble (s)E-cadherin is elevated in the serum of patients with prostate cancer, we investigated its influence on prostate cancer cell behavior in vitro. Exposure to sE-cadherin increased the systemic spread of the cells. Thus, targeting sE-cadherin might be a novel and innovative concept to treat advanced PCa. Abstract The serum level of soluble (s)E-cadherin is elevated in several malignancies, including prostate cancer (PCa). This study was designed to investigate the effects of sE-cadherin on the behavior of PCa cells in vitro, with the aim of identifying a potential therapeutic target. Growth as well as adhesive and motile behavior were evaluated in PC3, DU-145, and LNCaP cells. Flow cytometry was used to assess cell cycle phases and the surface expression of CD44 variants as well as α and β integrins. Confocal microscopy was utilized to visualize the distribution of CD44 variants within the cells. Western blot was applied to investigate expression of α3 and β1 integrins as well as cytoskeletal and adhesion proteins. Cell growth was significantly inhibited after exposure to 5 µg/mL sE-cadherin and was accompanied by a G0/G1-phase arrest. Adhesion of cells to collagen and fibronectin was mitigated, while motility was augmented. CD44v4, v5, and v7 expression was elevated while α3 and β1 integrins were attenuated. Blocking integrin α3 reduced cell growth and adhesion to collagen but increased motility. sE-cadherin therefore appears to foster invasive tumor cell behavior, and targeting it might serve as a novel and innovative concept to treat advanced PCa.

Published

2021

23. Systemic treatment of penile squamous cell carcinoma—hurdles and hopes of preclinical models and clinical regimens:a narrative review

Author

Roman A. Blaheta, Anita Thomas, Igor Tsaur, Eva Juengel, Philippe E. Spiess, Silvia Regina Rogatto, Luisa Matos do Canto Alvim, and Cláudia Aparecida Rainho

Subjects

medicine.medical_specialty, business.industry, Penile squamous cell carcinoma, Tumor biology, Urology, Cancer, Translational research, medicine.disease, Penile squamous cell carcinoma (PeSCC), Clinical trial, Copy number alterations (CNAs), Reproductive Medicine, Review Article on Management of Advanced Genitourinary Malignancies, medicine, Etiology, Narrative review, Mutational profiling, Treatment, biomarkers, Disease management (health), business, Intensive care medicine

Abstract

Despite contemporary research efforts, the prognosis of penile squamous cell carcinoma (PeSCC) has not significantly improved over the past decade. Despite frequently encountered patient-related delayed medical consultations impairing outcomes, several other aspects contribute to the lack of advancement in the treatment of this condition. One essential reason is that translational research, a prerequisite for the clinically successful disease management, is still at an early stage in PeSCC as compared to many other malignancies. Preclinical experimental models are indispensable for the evaluation of tumor biology and identification of genomic alterations. However, since neither commercial PeSCC cell lines are available nor xenograft models sustainably established, such analyses are challenging in this field of research. In addition, systemic therapies are less effective and toxic without decisive breakthroughs over recent years. Current systemic management of PeSCC is based on protocols that have been investigated in small series of only up to 30 patients. Thus, there is an unmet medical need for new approaches necessitating research efforts to develop more efficacious systemic strategies. This review aims to highlight the current state of knowledge in the molecular alterations involved in the etiology and ensuing steps for cancer progression, existing preclinical models of translational research, clinically relevant systemic protocols, and ongoing clinical trials.

Published

2021

24. Growth, Proliferation and Metastasis of Prostate Cancer Cells Is Blocked by Low-Dose Curcumin in Combination with Light Irradiation

Author

Blaheta, Jochen Rutz, Aicha Benchellal, Wajdi Kassabra, Sebastian Maxeiner, August Bernd, Stefan Kippenberger, Nadja Zöller, Felix K.-H. Chun, Eva Juengel, and Roman A.

Subjects

curcumin, light irradiation, prostate cancer, growth, proliferation, metastasis

Abstract

Although anti-cancer properties of the natural compound curcumin have been reported, low absorption and rapid metabolisation limit clinical use. The present study investigated whether irradiation with visible light may enhance the inhibitory effects of low-dosed curcumin on prostate cancer cell growth, proliferation, and metastasis in vitro. DU145 and PC3 cells were incubated with low-dosed curcumin (0.1–0.4 µg/mL) and subsequently irradiated with 1.65 J/cm2 visible light for 5 min. Controls remained untreated and/or non-irradiated. Cell growth, proliferation, apoptosis, adhesion, and chemotaxis were evaluated, as was cell cycle regulating protein expression (CDK, Cyclins), and integrins of the α- and β-family. Curcumin or light alone did not cause any significant effects on tumor growth, proliferation, or metastasis. However, curcumin combined with light irradiation significantly suppressed tumor growth, adhesion, and migration. Phosphorylation of CDK1 decreased and expression of the counter-receptors cyclin A and B was diminished. Integrin α and β subtypes were also reduced, compared to controls. Irradiation distinctly enhances the anti-tumor potential of curcumin in vitro and may hold promise in treating prostate cancer.

Published

2021

25. Assessment of PI3K/mTOR/AKT Pathway Elements to Serve as Biomarkers and Therapeutic Targets in Penile Cancer

Author

Jindrich Cinatl, Stephan Macher-Goeppinger, Jaroslav Cinatl, Maarten Albersen, Olesya Vakhrusheva, Katrin E. Tagscherer, Mario Schindeldecker, Florian Rothweiler, Andreas Neisius, Wilfried Roth, Philipp Stenzel, Igor Tsaur, Eva Juengel, Robert Dotzauer, Anita Thomas, Axel Haferkamp, Sascha Reetz, and Martin Michaelis

Subjects

0301 basic medicine, Cancer Research, RM, medicine.medical_treatment, P70-S6 Kinase 1, cell lines, BREAST, Article, Targeted therapy, RC0254, 03 medical and health sciences, 0302 clinical medicine, PROGNOSTIC-FACTORS, PIK3CA GENE, Medicine, Penile cancer, PROSTATE, ddc:610, Viability assay, AKT EXPRESSION, TISSUE MICROARRAY, Protein kinase B, PI3K/AKT/mTOR pathway, RC254-282, HIGH-FREQUENCY, Science & Technology, Akt/PKB signaling pathway, business.industry, MUTATIONS, AKT, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, penile cancer, targeted therapy, 030104 developmental biology, Oncology, MAMMALIAN TARGET, 030220 oncology & carcinogenesis, Cancer research, mTOR, Immunohistochemistry, biomarker, SQUAMOUS-CELL CARCINOMA, business, Life Sciences & Biomedicine

Abstract

Simple Summary: Penile cancer is a rare but aggressive malignancy characterized by rapid tumor growth as well as prompt metastasis in groin lymphatics. While localized diseases can be successfully cured by surgery in most cases, no truly effective treatment options have been established for metastatic diseases as of yet. In the current investigation, we assessed the value of selected members of the PI3K/mTOR/AKT pathway to serve as tumor markers or therapeutic targets for this disease. Higher expression of AKT was significantly more prevalent in high-grade tumors and independently predictive of the worse survival parameters, while increased expression of pmTOR was associated with an inferior prognosis as well. Treatment with the pan-AKT inhibitor capivasertib in PeCa cell lines induced significant reduction of cell viability and movement capacity. These findings might aid in the understanding of the molecular tumor background as well as development of novel treatment options for advanced penile cancer. Abstract: The PI3K/mTOR/AKT pathway might represent an intriguing option for treatment of penile cancer (PeCa). We aimed to assess whether members of this pathway might serve as biomarkers and targets for systemic therapy. Tissue of primary cancer from treatment-naïve PeCa patients was used for tissue microarray analysis. Immunohistochemical staining was performed with antibodies against AKT, pAKT, mTOR, pmTOR, pS6, pPRAS, p4EBP1, S6K1 and pp70S6K. Protein expression was correlated with clinicopathological characteristics as well as overall survival (OS), disease-specific survival (DSS), recurrence-free survival (RFS) and metastasis-free survival (MFS). AKT inhibition was tested in two primarily established, treatment-naïve PeCa cell lines by treatment with capivasertib and analysis of cell viability and chemotaxis. A total of 76 patients surgically treated for invasive PeCa were included. Higher expression of AKT was significantly more prevalent in high-grade tumors and predictive of DSS and OS in the Kaplan–Meier analysis, and an independent predictor of worse OS and DSS in the multivariate regression analysis. Treatment with pan-AKT inhibitor capivasertib in PeCa cell lines induced a significant downregulation of both total AKT and pAKT as well as decreased cell viability and chemotaxis. Selected protein candidates of the mTOR/AKT signaling pathway demonstrate association with histological and survival parameters of PeCa patients, whereas AKT appears to be the most promising one.

Published

2021

26. Abstract 5384: Cell growth of sunitinib-resistant renal cell carcinoma was inhibited by Shikonin through necroptosis induction and Akt/mTOR signaling inhibition

Author

Eva Juengel, Sascha D. Markowitsch, Olesya Vakhrusheva, Yasminn Akele, Jovanna Kitanovic, Patricia Schupp, Kimberly S. Slade, Anita Thomas, Igor Tsaur, Rene Mager, Thomas Efferth, and Axel Haferkamp

Subjects

Cancer Research, Oncology

Abstract

Despite the establishment of new therapy options during the last decades, advanced renal cell carcinoma (RCC) remains an uncurable disease, due to evolving drug-resistance. New, more efficient treatment strategies are still in urgent demand. Shikonin (SHI) from Traditional Chinese Medicine has exhibited anti-tumor properties in several tumor entities. Thus, in the current investigation we evaluated the impact of SHI on progressive growth and metastatic behavior, not only in therapy-sensitive (parental) but also in therapy-resistant RCC cells. Parental and sunitinib-resistant RCC cells, Caki-1, 786-O, KTCTL-26, and A498, were treated with SHI. Tumor cell growth, proliferation, clonogenic capacity, cell cycle phase distribution, induction of cell death (apoptosis and necroptosis) and the expression and activity of regulating and signaling proteins were evaluated. Moreover, the adhesion and chemotactic activity of the RCC cells after exposure to SHI were investigated. SHI did not affect cell motility but led to significant inhibition of progressive tumor cell growth in both therapy-sensitive and therapy-resistant RCC cells. Thereby, SHI significantly inhibited the growth, proliferation and clone formation in parental and sunitinib-resistant RCC cells by G2/M phase arrest through down-regulation of cell cycle activating proteins, blocking cell division. Furthermore, SHI induced apoptosis and necroptosis by activating necrosome complex proteins. Concomitantly, SHI impaired the Akt/mTOR pathway, pivotal for cell survival and growth. Thus, SHI may hold promise as an additive option in treating patients with advanced and therapy-resistant RCC. Citation Format: Eva Juengel, Sascha D. Markowitsch, Olesya Vakhrusheva, Yasminn Akele, Jovanna Kitanovic, Patricia Schupp, Kimberly S. Slade, Anita Thomas, Igor Tsaur, Rene Mager, Thomas Efferth, Axel Haferkamp. Cell growth of sunitinib-resistant renal cell carcinoma was inhibited by Shikonin through necroptosis induction and Akt/mTOR signaling inhibition [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 5384.

Published

2022

27. Artesunate Inhibits Growth of Sunitinib-Resistant Renal Cell Carcinoma Cells through Cell Cycle Arrest and Induction of Ferroptosis

Author

Rene Mager, Kimberly S. Slade, Axel Haferkamp, Thomas Efferth, Sascha D. Markowitsch, Eva Juengel, Julia Lauckner, Patricia Schupp, and Olesya Vakhrusheva

Subjects

0301 basic medicine, Cancer Research, Traditional Chinese Medicine (TCM), growth inhibition, ferroptosis, reactive oxygen species (ROS), Cell cycle checkpoint, Biology, urologic and male genital diseases, reactive oxygen species (ROS), lcsh:RC254-282, Article, growth inhibition, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, renal cell carcinoma (RCC), medicine, Clonogenic assay, Cytotoxicity, artesunate (ART), Sunitinib, Traditional Chinese Medicine (TCM), Cell cycle, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, ferroptosis, sunitib resistance, 030104 developmental biology, Oncology, chemistry, Cell culture, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Growth inhibition, medicine.drug

Abstract

Although innovative therapeutic concepts have led to better treatment of advanced renal cell carcinoma (RCC), efficacy is still limited due to the tumor developing resistance to applied drugs. Artesunate (ART) has demonstrated anti-tumor effects in different tumor entities. This study was designed to investigate the impact of ART (1&ndash, 100 &micro, M) on the sunitinib-resistant RCC cell lines, Caki-1, 786-O, KTCTL26, and A-498. Therapy-sensitive (parental) and untreated cells served as controls. ART&rsquo, s impact on tumor cell growth, proliferation, clonogenic growth, apoptosis, necrosis, ferroptosis, and metabolic activity was evaluated. Cell cycle distribution, the expression of cell cycle regulating proteins, p53, and the occurrence of reactive oxygen species (ROS) were investigated. ART significantly increased cytotoxicity and inhibited proliferation and clonogenic growth in both parental and sunitinib-resistant RCC cells. In Caki-1, 786-O, and A-498 cell lines growth inhibition was associated with G0/G1 phase arrest and distinct modulation of cell cycle regulating proteins. KTCTL-26 cells were mainly affected by ART through ROS generation, ferroptosis, and decreased metabolism. p53 exclusively appeared in the KTCTL-26 cells, indicating that p53 might be predictive for ART-dependent ferroptosis. Thus, ART may hold promise for treating selected patients with advanced and even therapy-resistant RCC.

Published

2020

28. MP76-07 POTENTIAL ROLE OF PROTEINS OF THE MTOR/AKT SIGNALING PATHWAY TO SERVE AS BIOMARKERS IN PENILE SQUAMOUS CELL CARCINOMA

Author

Maarten Albersen, Joren Vanthoor, Axel Haferkamp, Sascha Reetz, Anita Thomas, Stephan Macher-Goeppinger, Katrin E. Tagscherer, Igor Tsaur, Eva Juengel, Philipp Stenzel, and Silvia Regina Rogatto

Subjects

Lymphatic system, Penile squamous cell carcinoma, business.industry, Akt/PKB signaling pathway, Urology, Cancer research, Medicine, business, Aggressive course, PI3K/AKT/mTOR pathway, Rare disease

Abstract

INTRODUCTION AND OBJECTIVE:Penile squamous cell carcinoma (PSCC) is a rare disease characterized by an aggressive course with an early lymphatic and visceral dissemination. Unfortunately, little is...

Published

2020

29. Shikonin Inhibits Cell Growth of Sunitinib-Resistant Renal Cell Carcinoma by Activating the Necrosome Complex and Inhibiting the AKT/mTOR Signaling Pathway

Author

Sascha D. Markowitsch, Olesya Vakhrusheva, Patricia Schupp, Yasminn Akele, Jovana Kitanovic, Kimberly S. Slade, Thomas Efferth, Anita Thomas, Igor Tsaur, René Mager, Axel Haferkamp, and Eva Juengel

Subjects

Cancer Research, Oncology, 610 Medical sciences, fungi, 610 Medizin, renal cell carcinoma (RCC), sunitinib, therapy resistance, shikonin (SHI), growth, necroptosis, AKT, urologic and male genital diseases

Abstract

Therapy resistance remains a major challenge in treating advanced renal cell carcinoma (RCC), making more effective treatment strategies crucial. Shikonin (SHI) from traditional Chinese medicine has exhibited antitumor properties in several tumor entities. We, therefore, currently investigated SHI’s impact on progressive growth and metastatic behavior in therapy-sensitive (parental) and therapy-resistant Caki-1, 786-O, KTCTL-26, and A498 RCC cells. Tumor cell growth, proliferation, clonogenic capacity, cell cycle phase distribution, induction of cell death (apoptosis and necroptosis), and the expression and activity of regulating and signaling proteins were evaluated. Moreover, the adhesion and chemotactic activity of the RCC cells after exposure to SHI were investigated. SHI significantly inhibited the growth, proliferation, and clone formation in parental and sunitinib-resistant RCC cells by G2/M phase arrest through down-regulation of cell cycle activating proteins. Furthermore, SHI induced apoptosis and necroptosis by activating necrosome complex proteins. Concomitantly, SHI impaired the AKT/mTOR pathway. Adhesion and motility were cell line specifically affected by SHI. Thus, SHI may hold promise as an additive option in treating patients with advanced and therapy-resistant RCC.

Published

2022

30. Acquired resistance to temsirolimus is associated with integrin α7 driven chemotactic activity of renal cell carcinoma in vitro

Author

Igor Tsaur, Frederik Roos, Jochen Rutz, Sorel Fanguen, Sebastian Maxeiner, Wael Khoder, Sebastian Koschade, Eva Juengel, Roman A. Blaheta, and Tobias Engl

Subjects

0301 basic medicine, Integrin, Cell, renal cell cancer, Flow cytometry, resistance, 03 medical and health sciences, 0302 clinical medicine, temsirolimus, medicine, ddc:610, chemotaxis, biology, medicine.diagnostic_test, Chemistry, Chemotaxis, Temsirolimus, Fibronectin, 030104 developmental biology, medicine.anatomical_structure, ITGA7, Oncology, Cell culture, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Intracellular, Research Paper, medicine.drug

Abstract

The mechanistic target of the rapamycin (mTOR) inhibitor, temsirolimus, has significantly improved the outcome of patients with renal cell carcinoma (RCC). However, development of temsirolimus-resistance limits its effect and metastatic progression subsequently recurs. Since integrin α7 (ITGA7) is speculated to promote metastasis, this investigation was designed to investigate whether temsirolimus-resistance is associated with altered ITGA7 expression in RCC cell lines and modified tumor cell adhesion and invasion. Caki-1, KTCTL-26, and A498 RCC cell lines were driven to temsirolimus-resistance by exposing them to temsirolimus over a period of 12 months. Subsequently, adhesion to human umbilical vein endothelial cells, to immobilized fibronectin, or collagen was investigated. Chemotaxis was evaluated with a modified Boyden chamber assay and ITGA7 expression by flow cytometry and western blotting. Chemotaxis significantly decreased in temsirolimus-sensitive cell lines upon exposure to low-dosed temsirolimus, but increased in temsirolimus-resistant tumor cells upon reexposure to the same temsirolimus dose. The increase in chemotaxis was accompanied by elevated ITGA7 at the cell surface membrane with simultaneous reduction of intracellular ITGA7. ITGA7 knock-down significantly diminished motility of temsirolimous-sensitive cells but elevated chemotactic activity of temsirolimus-resistant Caki-1 and KTCTL-26 cells. Therefore, ITGA7 appears closely linked to adhesion and migration regulation in RCC cells. It is postulated that temsirolimus-resistance is associated with translocation of ITGA7 from inside the cell to the outer surface. This switch forces RCC migration forward. Whether ITGA7 can serve as an important target in combatting RCC requires further investigation.

Published

2018

31. Correction to: Immunotherapy in prostate cancer: new horizon of hurdles and hopes

Author

Guillaume Ploussard, Igor Tsaur, Eva Juengel, Maximilian Peter Brandt, and Cécile Manceau

Subjects

Prostate cancer, medicine.medical_specialty, Horizon (archaeology), business.industry, Urology, medicine.medical_treatment, medicine, Medical physics, Immunotherapy, medicine.disease, business

Published

2021

32. Abstract 1423: Shikonin impairs the growth of docetaxel-resistant prostate cancer cells by necroptosis

Author

Eva Juengel, Sascha D. Markowitsch, Martin Michaelis, Kristine Hausschulte, Patricia Schupp, Olesya Vakhrusheva, Thomas Efferth, Kira M. Juetter, Axel Haferkamp, and Jindrich Cinatl

Subjects

Cancer Research, Cell cycle checkpoint, business.industry, Necroptosis, Cancer, Cell cycle, urologic and male genital diseases, medicine.disease, Prostate cancer, Oncology, Docetaxel, DU145, LNCaP, Cancer research, Medicine, business, medicine.drug

Abstract

Introduction: Prostate carcinoma (PCa) is the most common malignancy in men. Androgen-targeted therapy and chemotherapy are currently the treatment of choice for advanced stages. Due to resistance towards these therapies, prognosis remains poor and new treatment options are urgently required. Shikonin (SHI) from Traditional Chinese Medicine (TCM) might be promising, since it induces anti-tumor effects in different tumor entities. However, data on PCa are few, and data on resistant PCa are not existent. Material and Methods: Parental (=sensitive) and docetaxel-resistant PCa cell lines, PC3, DU145, LNCaP, and 22Rv1 were exposed to SHI [0.1 - 1.5 μM] for 24, 48, or 72 hours. Untreated cells served as controls. Tumor cell growth, proliferation, cell cycle, and the expression of cell cycle regulating proteins were assessed. Several cell deaths, like apoptosis, necrosis and necroptosis as well as the metabolic activity were evaluated. Results: Time- and dose-dependent exposure to SHI significantly reduced tumor cell growth and proliferation in parental and docetaxel-resistant PCa cells, compared to the untreated controls. This was accompanied by cell cycle arrest in the G2/M phase in parental PC3 and docetaxel-resistant DU145 and S phase arrest in resistant 22Rv1, associated with modulated expression of cell cycle regulating proteins. Significant apoptotic effects were observed in parental and docetaxel-resistant PC3, DU145, 22Rv1, and resistant LNCaP. Moreover, SHI induced necroptosis in all parental and resistant PCa cells, as shown by additional application to the necroptosis inhibitor necrostatin-1. In line with this, RIP-1 expression enhanced under SHI exposure. In contrast, SHI did not alter the metabolic activity of the PCa cells. Conclusion: Significant anti-tumor effects are apparent in parental but also in docetaxel-resistant PCa cells after SHI application. Thus, adding SHI to standard therapies might be a promising treatment strategy for patients with advanced prostate cancer. Further investigations are necessary to verify our findings. Funding: Friedrich-Spicker-Stiftung (2017). Acknowledgments: The main portion of the results presented here are part of the MD thesis of Kira M. Juetter at the Department of Urology and Pediatric Urology, University Medical Center Mainz, Langenbeckstraße 1, 55131 Mainz, Germany. Citation Format: Sascha D. Markowitsch, Kira M. Juetter, Patricia Schupp, Kristine Hausschulte, Olesya Vakhrusheva, Jindrich Cinatl, Martin Michaelis, Thomas Efferth, Axel Haferkamp, Eva Juengel. Shikonin impairs the growth of docetaxel-resistant prostate cancer cells by necroptosis [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1423.

Published

2021

33. HDAC inhibition as a treatment concept to combat temsirolimus-resistant bladder cancer cells

Author

Ramin Najafi, Jasmina Makarević, Sebastian Maxeiner, Roman A. Blaheta, Igor Tsaur, Frederik Roos, Axel Haferkamp, Eva Juengel, and Jochen Rutz

Subjects

0301 basic medicine, Cyclin A, HDAC inhibition, 03 medical and health sciences, 0302 clinical medicine, medicine, temsirolimus-resistance, Mechanistic target of rapamycin, PI3K/AKT/mTOR pathway, Cyclin-dependent kinase 1, Bladder cancer, biology, business.industry, valproic acid (VPA), Cell cycle, medicine.disease, Temsirolimus, tumor growth, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, bladder cancer, Histone deacetylase, business, Research Paper, medicine.drug

Abstract

// Eva Juengel 1, 2 , Ramin Najafi 1 , Jochen Rutz 1 , Sebastian Maxeiner 1 , Jasmina Makarevic 1 , Frederik Roos 1, 2 , Igor Tsaur 1, 2 , Axel Haferkamp 1, 2 and Roman A. Blaheta 1 1 Department of Urology, Goethe-University, Frankfurt am Main, Germany 2 Current address: Department of Urology and Pediatric Urology, Mainz University Medical Center, Mainz, Germany Correspondence to: Eva Juengel, email: eva.juengel@unimedizin-mainz.de Keywords: bladder cancer; temsirolimus-resistance; HDAC inhibition; valproic acid (VPA); tumor growth Received: June 01, 2017 Accepted: October 12, 2017 Published: November 06, 2017 ABSTRACT Introduction: Although the mechanistic target of rapamycin (mTOR) might be a promising molecular target to treat advanced bladder cancer, resistance develops under chronic exposure to an mTOR inhibitor (everolimus, temsirolimus). Based on earlier studies, we proposed that histone deacetylase (HDAC) blockade might circumvent resistance and investigated whether HDAC inhibition has an impact on growth of bladder cancer cells with acquired resistance towards temsirolimus. Results: The HDAC inhibitor valproic acid (VPA) significantly inhibited growth, proliferation and caused G0/G1 phase arrest in RT112 res and UMUC-3 res . cdk1, cyclin B, cdk2, cyclin A and Skp1 p19 were down-regulated, p27 was elevated. Akt-mTOR signaling was deactivated, whereas acetylation of histone H3 and H4 in RT112 res and UMUC-3 res increased in the presence of VPA. Knocking down cdk2 or cyclin A resulted in a significant growth blockade of RT112 res and UMUC-3 res . Materials And Methods: Parental (par) and resistant (res) RT112 and UMUC-3 cells were exposed to the HDAC inhibitor VPA. Tumor cell growth, proliferation, cell cycling and expression of cell cycle regulating proteins were then evaluated. siRNA blockade was used to investigate the functional impact of the proteins. Conclusions: HDAC inhibition induced a strong response of temsirolimus-resistant bladder cancer cells. Therefore, the temsirolimus-VPA-combination might be an innovative strategy for bladder cancer treatment.

Published

2017

34. Amygdalin Modulates Prostate Cancer Cell Adhesion and Migration In Vitro

Author

Jens Neuschäfer, Christian Resch, Eva Juengel, Felix K.-H. Chun, Jochen Rutz, Frederik Roos, Roman A. Blaheta, Sebastian Maxeiner, and Jens Mani

Subjects

0301 basic medicine, Male, Cancer Research, Integrins, Integrin, Amygdalin, Integrin alpha2, Medicine (miscellaneous), Integrin alpha6, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 0302 clinical medicine, Downregulation and upregulation, Cell Movement, Cell Line, Tumor, medicine, Cell Adhesion, Humans, 030109 nutrition & dietetics, Nutrition and Dietetics, biology, Chemotaxis, Integrin beta1, Prostatic Neoplasms, medicine.disease, Antineoplastic Agents, Phytogenic, In vitro, Oncology, chemistry, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, biology.protein, Collagen

Abstract

The natural compound, amygdalin, is notably popular with prostate cancer patients as an alternative or complementary treatment option. However, knowledge about its mode of action is sparse. We investigated amygdalin's impact on prostate cancer adhesion and motile behavior. DU-145 and PC3 cancer cells were exposed to amygdalin. Adhesion to human vascular endothelium or immobilized collagen was then explored. The influence of amygdalin on chemotaxis and migration was also investigated, as well as amygdalin induced alteration to surface and total cellular α and β integrin expression. Integrin knockdown was performed to evaluate the integrin influence on chemotaxis and adhesion. Amygdalin significantly reduced chemotactic activity, migration, and adhesion of DU-145 but not of PC3 cells. Amygdalin elevated integrin α2 in both cell lines. Integrin α6 was reduced by amygdalin only in DU-145 cells, whereas β1 increased only in PC3 cells. Functional blocking revealed a negative association of α2 with PC3 and DU-145 chemotaxis. The β1 increase correlated with enhanced chemotaxis, the diminished α6 expression with reduced chemotaxis. Amygdalin acted on prostate cancer cells in vitro. It induced downregulation of α6 integrin in DU-145 but not in PC3 cells, suggesting that exposing certain prostate cancer cells to amygdalin might inhibit metastatic spread promoted by this particular integrin.

Published

2019

35. Influence of the HDAC Inhibitor Valproic Acid on the Growth and Proliferation of Temsirolimus-Resistant Prostate Cancer Cells In Vitro

Author

Jasmina Makarević, Jochen Rutz, Eva Juengel, Sebastian Maxeiner, Igor Tsaur, Felix K.-H. Chun, Jürgen Bereiter-Hahn, Roman A. Blaheta, and Nelson, Karen

Subjects

resistance, HDAC, cdk, valproic acid, mtor, temsirolimus, cell growth, ddc:610, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, prostate cancer, lcsh:RC254-282, cyclins, Article

Abstract

The mechanistic target of rapamycin (mTOR) is elevated in prostate cancer, making this protein attractive for tumor treatment. Unfortunately, resistance towards mTOR inhibitors develops and the tumor becomes reactivated. We determined whether epigenetic modulation by the histone deacetylase (HDAC) inhibitor, valproic acid (VPA), may counteract non-responsiveness to the mTOR inhibitor, temsirolimus, in prostate cancer (PCa) cells. Prostate cancer cells, sensitive (parental) and resistant to temsirolimus, were exposed to VPA, and tumor cell growth behavior compared. Temsirolimus resistance enhanced the number of tumor cells in the G2/M-phase, correlating with elevated cell proliferation and clonal growth. The cell cycling proteins cdk1 and cyclin B, along with Akt-mTOR signaling increased, whereas p19, p21 and p27 decreased, compared to the parental cells. VPA significantly reduced cell growth and up-regulated the acetylated histones H3 and H4. Cdk1 and cyclin B decreased, as did phosphorylated mTOR and the mTOR sub-complex Raptor. The mTOR sub-member Rictor and phosphorylated Akt increased under VPA. Knockdown of cdk1, cyclin B, or Raptor led to significant cell growth reduction. HDAC inhibition through VPA counteracts temsirolimus resistance, probably by down-regulating cdk1, cyclin B and Raptor. Enhanced Rictor and Akt, however, may represent an undesired feedback loop, which should be considered when designing future therapeutic regimens.

Published

2019

36. Growth and proliferation of renal cell carcinoma cells is blocked by low curcumin concentrations combined with visible light irradiation

Author

Jochen Rutz, Sebastian Maxeiner, Eva Juengel, August Bernd, Stefan Kippenberger, Nadja Zöller, Felix K.-H. Chun, and Roman A. Blaheta

Subjects

Curcumin, Light, Cell Survival, Cell Cycle, cell cycling, Antineoplastic Agents, Apoptosis, renal cell cancer, Article, lcsh:Chemistry, tumor growth, lcsh:Biology (General), lcsh:QD1-999, Cell Line, Tumor, Gene Knockdown Techniques, Humans, ddc:610, tumor proliferation, lcsh:QH301-705.5, Carcinoma, Renal Cell, Cell Proliferation

Abstract

The anti-cancer properties of curcumin in vitro have been documented. However, its clinical use is limited due to rapid metabolization. Since irradiation of curcumin has been found to increase its anti-cancer effect on several tumor types, this investigation was designed to determine whether irradiation with visible light may enhance the anti-tumor effects of low-dosed curcumin on renal cell carcinoma (RCC) cell growth and proliferation. A498, Caki1, and KTCTL-26 cells were incubated with curcumin (0.1–0.4 µg/mL) and irradiated with 1.65 J/cm2 visible light for 5 min. Controls were exposed to curcumin or light alone or remained untreated. Curcumin plus light, but not curcumin or light exposure alone altered growth, proliferation, and apoptosis of all three RCC tumor cell lines. Cells were arrested in the G0/G1 phase of the cell cycle. Phosphorylated (p) CDK1 and pCDK2, along with their counter-receptors Cyclin B and A decreased, whereas p27 increased. Akt-mTOR-signaling was suppressed, the pro-apoptotic protein Bcl-2 became elevated, and the anti-apoptotic protein Bax diminished. H3 acetylation was elevated when cells were treated with curcumin plus light, pointing to an epigenetic mechanism. The present findings substantiate the potential of combining low curcumin concentrations and light as a new therapeutic concept to increase the efficacy of curcumin in RCC.

Published

2019

37. Cyanide and lactate levels in patients during chronic oral amygdalin intake followed by intravenous amygdalin administration

Author

Jens Mani, Jochen Rutz, Dimitra Bon, Frederik Roos, Eva Juengel, Sebastian Maxeiner, Roman A. Blaheta, and Felix K.-H. Chun

Subjects

Complementary and Manual Therapy, Adult, Male, Cyanide, Amygdalin, Administration, Oral, Pharmacology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Oral administration, Lactate dehydrogenase, Neoplasms, Blood plasma, medicine, Humans, 030212 general & internal medicine, Acidosis, Aged, Retrospective Studies, Advanced and Specialized Nursing, Aged, 80 and over, Cyanides, business.industry, Metabolic acidosis, Middle Aged, medicine.disease, Antineoplastic Agents, Phytogenic, Complementary and alternative medicine, chemistry, Lactic acidosis, Lactates, Administration, Intravenous, Female, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

The natural compound amygdalin has gained high popularity among tumor patients as a complementary or alternative treatment option. However, due to metabolization of amygdalin to cyanide (HCN) following oral consumption, there could be a high risk of lactic acidosis caused by cyanide intoxication. The present retrospective study was undertaken to evaluate cyanide blood and lactate plasma levels of tumor patients (n = 55) before and after intravenous (i.v.) amygdalin infusion. All patients had also continuously ingested amygdalin tablets (3 x 500 mg/day), excepting on the days of i.v. administration. Each patient received one to five intravenous amygdalin treatments. The time period between each i.v. application ranged between 4–6 days. The initial i.v. dose was 6 mg (n = 28), 9 mg (n = 1), 15 mg (n = 1) or 18 mg (n = 25). The mean cyanide blood level before i.v. amygdalin administration was 34.74 μg/L, which increased significantly to a mean value of 66.20 μg/L after i. v. amygdalin application. In contrast, lactate decreased significantly from 1266 μmol/L pre-infusion to 868 μmol/L post-infusion. Increasing i.v. amygdalin by 1 mg was also associated with a significant increase in the cyanide level, while the lactate blood level significantly decreased. This is the first study evaluating cyanide levels under conditions employed by amygdalin administrators, i.e. after chronic oral amygdalin intake and then again after a closely subsequent intravenous amygdalin administration. Since lactate decreased, whilst cyanide increased, it is concluded that elevation of cyanide does not induce metabolic acidosis in terms of an increased lactate level.

Published

2019

38. The Antitumor Effect of Curcumin in Urothelial Cancer Cells Is Enhanced by Light Exposure In Vitro

Author

August Bernd, Jochen Rutz, Felix K.-H. Chun, Eva Juengel, Stefan Kippenberger, Roman A. Blaheta, Sebastian Maxeiner, Katherina Binder, Frederik Roos, Nadja Zöller, and Solano, Francisco

Subjects

0303 health sciences, Article Subject, Chemistry, Cell growth, Cell, lcsh:Other systems of medicine, Cell cycle, lcsh:RZ201-999, In vitro, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine.anatomical_structure, Complementary and alternative medicine, Cell culture, Acetylation, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Curcumin, medicine, ddc:610, 030304 developmental biology, Research Article

Abstract

The natural compound curcumin exerts antitumor properties in vitro, but its clinical application is limited due to low bioavailability. Light exposure in skin and skin cancer cells has been shown to improve curcumin bioavailability; thus, the object of this investigation was to determine whether light exposure might also enhance curcumin efficacy in bladder cancer cell lines. RT112, UMUC3, and TCCSUP cells were preincubated with low curcumin concentrations (0.1-0.4μg/ml) and then exposed to 1.65 J/cm2visible light for 5 min. Cell growth, cell proliferation, apoptosis, cell cycle progression, and cell cycle regulating proteins along with acetylation of histone H3 and H4 were investigated. Though curcumin alone did not alter cell proliferation or apoptosis, tumor cell growth and proliferation were strongly blocked when curcumin was combined with visible light. Curcumin-light caused the bladder cancer cells to become arrested in different cell phases: G0/G1 for RT112, G2/M for TCCSUP, and G2/M- and S-phase for UMUC3. Proteins of the Cdk-cyclin axis were diminished in RT112 after application of 0.1 and 0.4μg/ml curcumin. Cell cycling proteins were upregulated in TCCSUP and UMUC3 in the presence of 0.1μg/ml curcumin-light but were partially downregulated with 0.4μg/ml curcumin. 0.4μg/ml (but not 0.1μg/ml) curcumin-light also evoked late apoptosis in TCCSUP and UMUC3 cells. H3 and H4 acetylation was found in UMUC3 cells treated with 0.4μg/ml curcumin alone or with 0.1μg/ml curcumin-light, pointing to an epigenetic mechanism. Light exposure enhanced the antitumor potential of curcumin on bladder cancer cells but by different molecular action modes in the different cell lines. Further studies are necessary to evaluate whether intravesical curcumin application, combined with visible light, might become an innovative tool in combating bladder cancer.

Published

2019

39. Elements of Wnt/β-catenin signaling pathway as prognostic biomarkers and therapeutic targets in penile squamous cell carcinoma

Author

Eva Juengel, Anita Thomas, O. Vakhrusheva, M. Schindeldecker, K. Tagscherer, Igor Tsaur, Maarten Albersen, A. Haferkamp, Philipp Stenzel, and Wilfried Roth

Subjects

Penile squamous cell carcinoma, business.industry, Urology, Cancer research, Wnt β catenin signaling, Medicine, business

Published

2021

40. Patterns and mechanisms of resistance to cisplatin and osimertinib in penile squamous cell carcinoma

Author

O. Vakhrusheva, Igor Tsaur, A. Haferkamp, Eva Juengel, M. Michaelis, Maarten Albersen, F. Rothweiler, J. Cinatl, and Anita Thomas

Subjects

Cisplatin, business.industry, Penile squamous cell carcinoma, Urology, Cancer research, Medicine, Osimertinib, business, medicine.drug

Published

2021

41. Sulforaphane inhibits proliferation and invasive activity of everolimus-resistant kidney cancer cells in vitro

Author

Jochen Rutz, Karen Nelson, Saira Justin, Axel Haferkamp, Igor Tsaur, Frederik Roos, Wolf O. Bechstein, Roman A. Blaheta, Sebastian Maxeiner, Wael Khoder, and Eva Juengel

Subjects

0301 basic medicine, renal cell carcinoma, proliferation, Integrin, Cyclin B, sulforaphane, Antineoplastic Agents, Apoptosis, Integrin alpha5, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Isothiocyanates, Cell Line, Tumor, CDC2 Protein Kinase, Cell Adhesion, Humans, Medicine, Everolimus, ddc:610, RNA, Small Interfering, Cell adhesion, Mechanistic target of rapamycin, PI3K/AKT/mTOR pathway, Cell Proliferation, Cyclin-dependent kinase 1, biology, business.industry, Cell growth, TOR Serine-Threonine Kinases, Cell Cycle, Cell cycle, invasion, Kidney Neoplasms, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, Sulfoxides, 030220 oncology & carcinogenesis, Immunology, biology.protein, Cancer research, business, Research Paper, complementary and alternative medicine

Abstract

Although the mechanistic target of rapamycin (mTOR) inhibitor, everolimus, has improved the outcome of patients with renal cell carcinoma (RCC), improvement is temporary due to the development of drug resistance. Since many patients encountering resistance turn to alternative/complementary treatment options, an investigation was initiated to evaluate whether the natural compound, sulforaphane (SFN), influences growth and invasive activity of everolimus-resistant (RCCres) compared to everolimus-sensitive (RCCpar) RCC cell lines in vitro. RCC cells were exposed to different concentrations of SFN and cell growth, cell proliferation, apoptosis, cell cycle, cell cycle regulating proteins, the mTOR-akt signaling axis, adhesion to human vascular endothelium and immobilized collagen, chemotactic activity, and influence on surface integrin receptor expression were investigated. SFN caused a significant reduction in both RCCres and RCCpar cell growth and proliferation, which correlated with an elevation in G2/M- and S-phase cells. SFN induced a marked decrease in the cell cycle activating proteins cdk1 and cyclin B and siRNA knock-down of cdk1 and cyclin B resulted in significantly diminished RCC cell growth. SFN also modulated adhesion and chemotaxis, which was associated with reduced expression of the integrin subtypes α5, α6, and β4. Distinct differences were seen in RCCres adhesion and chemotaxis (diminished by SFN) and RCCpar adhesion (enhanced by SFN) and chemotaxis (not influenced by SFN). Functional blocking of integrin subtypes demonstrated divergent action on RCC binding and invasion, depending on RCC cell sensitivity to everolimus. Therefore, SFN administration could hold potential for treating RCC patients with established resistance towards everolimus.

Published

2016

42. Amygdalin, quackery or cure?

Author

Axel Haferkamp, Roman A. Blaheta, Karen Nelson, and Eva Juengel

Subjects

0301 basic medicine, medicine.medical_specialty, Evidence-based practice, Quackery, Amygdalin, Alternative medicine, MEDLINE, Pharmaceutical Science, Disease, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Drug Discovery, medicine, Humans, Intensive care medicine, Rosaceae, Pharmacology, Cyanides, Traditional medicine, Plant Extracts, business.industry, Cancer, medicine.disease, Antineoplastic Agents, Phytogenic, 030104 developmental biology, Complementary and alternative medicine, chemistry, Prunasin, 030220 oncology & carcinogenesis, Molecular Medicine, business, Phytotherapy

Abstract

Background The cyanogenic diglucoside, amygdalin, has gained high popularity among cancer patients together with, or in place of, conventional therapy. Still, evidence based research on amygdalin is sparse and its benefit controversial. Purpose Since so many cancer patients consume amygdalin, and many clinicians administer it without clear knowledge of its mode of action, current knowledge has been summarized and the pros and cons of its use weighed. Methods A retrospective analysis was conducted for amygdalin relevant reports using the PubMed database with the main search term “Amygdalin” or “laetrile”, at times combined with “cancer”, “patient”, “cyanide” or “toxic”. We did not exclude any “unwanted” articles. Additionally, internet sources authorized by governmental or national institutions have also been included. Sections Individual chapters summarize pharmacokinetics, preclinical and clinical studies and toxicity. Conclusion No convincing evidence showing that amygdalin induces rapid, distinct tumor regression in cancer patients, particularly in those with late-stage disease, is apparent. However, there is also no evidence that purified amygdalin, administered in "therapeutic" dosage, causes toxicity. Multiple aspects of amygdalin administration have not yet been adequately explored, making further investigation necessary to evaluate its actual therapeutic potential.

Published

2016

43. Amygdalin delays cell cycle progression and blocks growth of prostate cancer cells in vitro

Author

Axel Haferkamp, Igor Tsaur, Georg Bartsch, Karen Nelson, Hendrik Borgmann, Eva Juengel, Jasmina Makarević, Christian Thomas, and Roman A. Blaheta

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Time Factors, Amygdalin, Blotting, Western, Cyclin A, Cyclin B, Apoptosis, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Cyclin-dependent kinase, Cell Line, Tumor, Internal medicine, LNCaP, medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, Clonogenic assay, Cyclin D3, Dose-Response Relationship, Drug, biology, Cell growth, Cell Cycle, Prostatic Neoplasms, General Medicine, Cell cycle, Flow Cytometry, Antineoplastic Agents, Phytogenic, Prostatic Neoplasms, Castration-Resistant, 030104 developmental biology, Endocrinology, 030220 oncology & carcinogenesis, biology.protein, Cancer research

Abstract

Aims Despite impressive survival benefits from new agents to treat metastasized prostate cancer (PCa), progressive drug resistance hinders long-term response and restricts the efficacy of subsequent therapy. Due to reported antitumor activity of amygdalin and growing popularity for complementary and alternative medicine the potential of this natural, widely used substance to exert antineoplastic effects on prostate cancer cells has been assessed. Main methods LNCaP (castration-sensitive), DU-145 and PC3 cells (castration-resistant) were exposed to different concentrations of amygdalin for 24 h or 2 weeks. Cell growth was measured by the MTT test, clonal formation by the clonogenic assay. Flow cytometry served to investigate apoptosis and cell cycle phases. Cell cycle regulating proteins and the mTOR–akt signaling axis were analyzed by western blotting. Key findings Amygdalin dose-dependently diminished tumor cell growth with maximum effects at 10 mg/ml. Apoptosis of PC3 and LNCaP but not of DU-145 cells was reduced, whereas colony formation was suppressed in all cell lines. A decrease in the number of G2/M- and S-phase cells along with an elevated number of G0/G1-phase cells was recorded. The cell cycle proteins cdk 1, cdk 2 and cdk 4 as well as cyclin A, cyclin B and cyclin D3 were modulated by amygdalin after both 24 h and 2 weeks. Distinct effects on p19 and p27 expression and on Akt, Rictor and Raptor activation became evident only after 2 weeks. Significance Amygdalin exhibits significant antitumor activity in both castration-sensitive and castration-resistant PCa cell lines and merits further evaluation for therapeutic purposes.

Published

2016

44. Abstract 6327: Artesunate reduces tumor growth and induces different kinds of cell death in docetaxel-resistant prostate carcinoma cells

Author

Holger H.H. Erb, Vitus Braeunig, Axel Haferkamp, Sascha D. Markowitsch, Thomas Efferth, Patricia Schupp, Olesya Vakhrusheva, and Eva Juengel

Subjects

Cancer Research, Cell cycle checkpoint, business.industry, Cell, Cancer, Cell cycle, urologic and male genital diseases, medicine.disease, Prostate cancer, medicine.anatomical_structure, Oncology, DU145, Apoptosis, LNCaP, medicine, Cancer research, business

Abstract

Introduction: Prostate carcinoma (PCa) is the most common cancer in men. The therapeutic effect of approved compounds, such as docetaxel, is limited due to the development of therapy resistance, making new treatment options essential. Artesunate (ART), used in Traditional Chinese Medicine, has shown anti-tumor activity in several tumor types. However, little is known about the efficacy of ART on therapy-resistant PCa. Therefore, the impact of ART on docetaxel-resistant PCa cells was investigated. Material and Methods: Parental (=sensitive) and docetaxel-resistant PCa cell lines, PC3, DU145, and LNCaP, were exposed to ART [1-100 µM] for 24, 48, or 72 hours. Cells not exposed to ART served as controls. Tumor cell growth, proliferation, cell cycling, and the expression of cell cycle regulating proteins were assessed. Apoptotic, ferroptotic, and necrotic effects were also evaluated. Results: Exposure to ART significantly reduced tumor cell growth and proliferation of parental and docetaxel-resistant PCa cells in a time- and dose-dependent manner. Cell cycle arrest in the G0/G1 phase after 48h exposure to 37.5 µM ART was observed in parental LNCaP and in all three resistant cell lines. The observed changes in cell growth and cell cycle phases were accompanied by marked modulation of cell cycle regulating proteins. Significant apoptotic effects were observed in parental PC3 and both parental and resistant LNCaP, whereas ferroptosis was apparent in parental and resistant DU145 after exposure to ART. Necrotic events were not detectable in the PCa cells after ART exposure. Conclusion: ART induced anti-tumor effects, though differing according to the cell line, were apparent in not only parental but also in docetaxel-resistant PCa cells. Thus, adding ART to standard therapies might be a promising treatment strategy for patients with advanced prostate cancer. Further investigations are necessary to verify our findings. Citation Format: Vitus Braeunig, Patricia Schupp, Sascha Markowitsch, Olesya Vakhrusheva, Holger Erb, Thomas Efferth, Axel Haferkamp, Eva Juengel. Artesunate reduces tumor growth and induces different kinds of cell death in docetaxel-resistant prostate carcinoma cells [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 6327.

Published

2020

45. Elements of mTOR/akt signaling pathway exhibit biomarker potential in penile squamous cell carcinoma

Author

K. Tagscherer, S.R. Rogatto, S. Reetz, S. Macher-Goeppinger, Eva Juengel, A. Haferkamp, I. Tsaur, Philipp Stenzel, Maarten Albersen, J. Vanthoor, Anita Thomas, and W. Roth

Subjects

business.industry, Akt/PKB signaling pathway, Penile squamous cell carcinoma, Urology, Cancer research, Medicine, Biomarker (medicine), lcsh:Diseases of the genitourinary system. Urology, lcsh:RC870-923, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, business, lcsh:RC254-282, PI3K/AKT/mTOR pathway

Published

2020

46. Chronic Sulforaphane Application Does Not Induce Resistance in Renal Cell Carcinoma Cells

Author

Frederik Roos, Sebastian Maxeiner, Stephanie Euler, Saira Justin, Jochen Rutz, Felix K.-H. Chun, Roman A. Blaheta, and Eva Juengel

Subjects

0301 basic medicine, Cancer Research, Time Factors, Cell Survival, Cell Cycle Proteins, 03 medical and health sciences, chemistry.chemical_compound, Isothiocyanates, Cell Line, Tumor, Anticarcinogenic Agents, Humans, Phosphorylation, Protein kinase B, Carcinoma, Renal Cell, Cell Proliferation, Cyclin-dependent kinase 1, biology, Cell growth, Cyclin-dependent kinase 2, General Medicine, Cell cycle, Kidney Neoplasms, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, chemistry, Cell culture, A549 Cells, Drug Resistance, Neoplasm, Sulfoxides, Cancer research, biology.protein, Signal transduction, Drug Screening Assays, Antitumor, Sulforaphane, Signal Transduction

Abstract

Background/aim Since the natural compound sulforaphane (SFN) has been shown to stop tumor growth, renal cell carcinoma (RCC) patients often use this drug in addition to their prescribed oncotherapy. The aim of this study was to examine whether resistance to SFN may develop after long-term application. Materials and methods Several RCC cell lines were incubated with SFN for short periods of time (24-72 h) or long periods of time (8 weeks) and cell growth, proliferation, and cell-cycle proteins were analyzed. Results Both short- and long-term application of SFN distinctly reduced RCC cell growth and proliferation. However, differences in the distribution of cells in each phase of the cell cycle and in the expression of cell-cycle proteins were apparent. Short-term treatment induced S-phase arrest, whereas long-term treatment induced G0/G1-phase arrest. Expression of Cdk1 and Cdk2 increased over short-term incubation, but decreased long-term. Expression of pCdk2, Akt, and Raptor were reduced following long-term SFN-exposure, but remained unchanged when SFN was applied for short periods of time. Conclusion Chronic use of SFN did not evoke resistance, but differentially altered signaling pathways, compared to short-term use.

Published

2018

47. Relevance of the natural HDAC inhibitor sulforaphane as a chemopreventive agent in urologic tumors

Author

Roman A. Blaheta, Holger H.H. Erb, Eva Juengel, Jochen Rutz, Felix K.-H. Chun, and Axel Haferkamp

Subjects

0301 basic medicine, Cancer Research, Urologic Neoplasms, Apoptosis, Disease, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Isothiocyanates, Cell Line, Tumor, HDAC inhibitor, Medicine, Anticarcinogenic Agents, Humans, Epigenetics, Mode of action, Biological Products, Molecular Structure, business.industry, Cruciferous vegetables, Cancer, medicine.disease, Histone Deacetylase Inhibitors, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Sulfoxides, Brassicaceae, Cancer research, business, Sulforaphane

Abstract

Due to an increased understanding of molecular biology and the genomics of cancer, new and potent agents have been approved by the Food and Drug Administration (FDA) to fight this disease. However, all of these drugs cause severe side effects and resistance inevitably develops, re-activating tumor growth and dissemination. For this reason, patients turn to natural compounds as alternative or complementary treatment options, since it has been found that natural plant products may block, inhibit, or reverse cancer development. The present review focusses on the role of the natural compound sulforaphane (SFN) as an anti-tumor agent in urologic cancer. SFN is a natural compound found in cruciferous vegetables from the Brassicaceae family such as broccoli, cauliflower and cabbage. Several epidemiologic and clinical studies have documented chemopreventive properties of SFN, making it an interesting candidate for additive cancer treatment. SFN shows remarkable anti-tumor effects in vitro and in vivo without exerting toxicity. The review summarizes the current understanding of SFN and provides insights into its molecular mode of action with particular emphasis on epigenetic tumor control.

Published

2018

48. Amygdalin: Nutzen oder Risiko?

Author

Roman A. Blaheta, Rene Mager, Axel Haferkamp, and Eva Juengel

Subjects

Gynecology, Cancer Research, medicine.medical_specialty, business.industry, Medicine, business

Abstract

Die Komplementar- und Alternativmedizin (CAM) ist oftmals in die Behandlung von Tumorerkrankungen eingebunden. Tatsachlich ist ihre Popularitat in den letzten Jahrzehnten stetig angestiegen. 80 % der amerikanischen und 50 % der europaischen Tumorpatienten wenden CAM begleitend oder anstelle der konventionellen Therapie an. Dennoch ist das Wissen uber die Wirkeffektivitat von CAM durftig. Die Diskrepanz zwischen Anwendung und tatsachlichem Benefit wird insbesondere beim cyanogenen Diglucosid Amygdalin deutlich, das in den Kernen der Spezies Rosaceae angereichert vorliegt. In den 1970er-Jahren reprasentierte Amygdalin eines der popularsten nicht-konventionellen Antitumor-Verfahren. Alleine im Jahr 1978 konsumierten 70.000 amerikanische Krebspatienten diese Substanz. Ob Amygdalin aber uberhaupt als antitumorales Agens angesprochen werden kann, ist unklar. Befurworter betrachten Amygdalin als naturliches Heilmittel, Gegner hingegen verneinen diese Eigenschaft und warnen vor toxischen Nebeneffekten. Der Ubersichtsartikel fasst das Wissen um diese Substanz zusammen.

Published

2015

49. Use of complementary and alternative medicine before and after organ removal due to urologic cancer

Author

Hanns Ackermann, Ilhan Arslan, Tobias Engl, Roman A. Blaheta, Axel Haferkamp, Natalie Filmann, Eva Juengel, Jens Mani, Karen C Nelson, and Georg Bartsch

Subjects

medicine.medical_specialty, Pathology, Bladder cancer, animal structures, business.industry, Health Policy, Alternative medicine, Medicine (miscellaneous), Patient counseling, medicine.disease, Urological surgery, Urogenital organ, surgery, urologic cancer, Symptom relief, Patient Preference and Adherence, Internal medicine, Urologic cancer, Surgical removal, Medicine, business, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Social Sciences (miscellaneous), Original Research, complementary and alternative medicine

Abstract

Jens Mani,1 Eva Juengel,1 Ilhan Arslan,1 Georg Bartsch,1 Natalie Filmann,2 Hanns Ackermann,2 Karen Nelson,3 Axel Haferkamp,1 Tobias Engl,1,* Roman A Blaheta1,* 1Department of Urology, 2Institute of Biostatistics and Mathematical Modeling, 3Department of Vascular and Endovascular Surgery, Johann Wolfgang Goethe-University, Frankfurt am Main, Germany *These authors contributed equally to this work Objective: Many patients use complementary and alternative medicine (CAM) as primary treatment or symptom relief for a variety of illnesses. This study was designed to investigate the influence of surgical removal of a tumor-bearing urogenital organ on CAM use.Methods: From 2007 to 2011, 350 patients underwent major urological surgery for kidney, prostate, or bladder cancer at the Goethe-University Hospital, Frankfurt, Germany. Data from 172 patients (49%), who returned a questionnaire, were retrospectively evaluated using the hospital information system along with the questionnaire to objectify CAM use 2 years before and after surgery.Results: From the 172 patients returning questionnaires, 56 (33%) used CAM before and/or after surgery and 116 (67%) never used CAM. Of the 56 CAM users, 30 (54%) used CAM presurgery and 53 (95%) used CAM postsurgery, indicating a significant change of mind about CAM use. Patients of German nationality used CAM significantly more than patients of other nationalities. Higher educational status (high-school diploma or higher) was a significant factor in favor of CAM use. The most common type of CAM used before/after surgery was an alternative medical system (63/49%), a manipulative and body-based method (50/19%), and a biological-based therapy (37/32%). Information about CAM, either provided by medical professionals or by other sources, was the main reason determining whether patients used CAM or not.Conclusion: The number of patients using CAM almost doubled after surgical removal of a cancer-bearing organ. Better awareness and understanding of CAM use by medical professionals could improve patient counseling. Keywords: complementary and alternative medicine, surgery, urologic cancer

Published

2015

50. Levosimendan protects human hepatocytes from ischemia-reperfusion injury

Author

Anton Moritz, Angela Kornberger, Andreas A. Schnitzbauer, I. Werner, Eva Juengel, N. Bogert, Stefanie N. Brunner, Andres Beiras-Fernandez, and Gallyas, Ferenc

Subjects

0301 basic medicine, Necrosis, Critical Care and Emergency Medicine, lcsh:Medicine, Apoptosis, 030204 cardiovascular system & hematology, Biochemistry, 0302 clinical medicine, Animal Cells, Medicine and Health Sciences, Enzyme assays, Colorimetric assays, lcsh:Science, Bioassays and physiological analysis, Cells, Cultured, Energy-Producing Organelles, bcl-2-Associated X Protein, Multidisciplinary, MTT assay, biology, Cell Death, Mitochondria, Pyridazines, Liver, Cell Processes, Reperfusion Injury, medicine.symptom, Cellular Types, Anatomy, Cellular Structures and Organelles, medicine.drug, Research Article, medicine.medical_specialty, Cell Physiology, Ischemia, Cardiology, Surgical and Invasive Medical Procedures, Bioenergetics, 03 medical and health sciences, Digestive System Procedures, Bcl-2-associated X protein, Internal medicine, medicine, Humans, ddc:610, Simendan, Heart Failure, Transplantation, business.industry, lcsh:R, Hydrazones, Biology and Life Sciences, Levosimendan, Cell Biology, Organ Transplantation, Hypoxia (medical), medicine.disease, Liver Transplantation, Cell Metabolism, Research and analysis methods, 030104 developmental biology, Endocrinology, Reperfusion, Biochemical analysis, biology.protein, Hepatocytes, lcsh:Q, business, Reperfusion injury

Abstract

Background Ischemia-reperfusion injury (IRI) is a major challenge in liver transplantation. The mitochondrial pathway plays a pivotal role in hepatic IRI. Levosimendan, a calcium channel sensitizer, was shown to attenuate apoptosis after IRI in animal livers. The aim of this study was to investigate the effect of levosimendan on apoptosis in human hepatocytes. Methods Primary human hepatocytes were either exposed to hypoxia or cultured under normoxic conditions. After the hypoxic phase, reoxygenation was implemented and cells were treated with different concentrations of levosimendan (10ng/ml, 100ng/ml, 1000ng/ml). The overall metabolic activity of the cells was measured using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT), and aspartate aminotransferase (AST) levels were determined in order to quantify hepatic injury. Fluorescence-activated cell sorting (FACS) analysis was applied to measure necrosis and apoptosis. Finally, Western blotting was performed to analyze apoptotic pathway proteins. Results Administration of levosimendan during reperfusion increases the metabolic activity of human hepatocytes and decreases AST levels. Moreover, apoptosis after IRI is reduced in treated vs. untreated hepatocytes, and levosimendan prevents down-regulation of the anti-apoptotic protein Bcl-2 as well as up-regulation of the pro-apoptotic protein BAX. Conclusion The present study suggests a protective effect of levosimendan on human hepatocytes. Our findings suggest that treatment with levosimendan during reperfusion attenuates apoptosis of human hepatocytes by influencing BAX and Bcl-2 levels.

Published

2017