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1. Toward model-informed precision dosing for tamoxifen: A population-pharmacokinetic model with a continuous CYP2D6 activity scale

Author

Bram C. Agema, Sanne M. Buijs, Sebastiaan D.T. Sassen, Thomas E. Mürdter, Mathias Schwab, Birgit C.P. Koch, Agnes Jager, Ron H.N. van Schaik, Ron H.J. Mathijssen, and Stijn L.W. Koolen

Subjects
Tamoxifen, Endoxifen, CYP2D6, Pharmacokinetics, Pharmacometrics, Model-informed precision dosing (MIPD), Therapeutics. Pharmacology, RM1-950
Abstract

Background: Tamoxifen is important in the adjuvant treatment of breast cancer. A plasma concentration of the active metabolite endoxifen of > 16 nM is associated with a lower risk of breast cancer-recurrence. Since inter-individual variability is high and > 20 % of patients do not reach endoxifen levels > 16 nM with the standard dose tamoxifen, therapeutic drug monitoring is advised. However, ideally, the correct tamoxifen dose should be known prior to start of therapy. Our aim is to develop a population pharmacokinetic (POP-PK) model incorporating a continuous CYP2D6 activity scale to support model informed precision dosing (MIPD) of tamoxifen to determine the optimal tamoxifen starting dose. Methods: Data from eight different clinical studies were pooled (539 patients, 3661 samples) and used to develop a POP-PK model. In this model, CYP2D6 activity per allele was estimated on a continuous scale. After inclusion of covariates, the model was subsequently validated using an independent external dataset (378 patients). Thereafter, dosing cut-off values for MIPD were determined. Results: A joint tamoxifen/endoxifen POP-PK model was developed describing the endoxifen formation rate. Using a continuous CYP2D6 activity scale, variability in predicting endoxifen levels was decreased by 37 % compared to using standard CYP2D6 genotype predicted phenotyping. After external validation and determination of dosing cut-off points, MIPD could reduce the proportion of patients with subtherapeutic endoxifen levels at from 22.1 % toward 4.8 %. Conclusion: Implementing MIPD from the start of tamoxifen treatment with this POP-PK model can reduce the proportion of patients with subtherapeutic endoxifen levels at steady-state to less than 5 %.

Published
2023
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2. Perfusion Air Culture of Precision-Cut Tumor Slices: An Ex Vivo System to Evaluate Individual Drug Response under Controlled Culture Conditions

Author

Meng Dong, Kathrin Böpple, Julia Thiel, Bernd Winkler, Chunguang Liang, Julia Schueler, Emma J. Davies, Simon T. Barry, Tauno Metsalu, Thomas E. Mürdter, Georg Sauer, German Ott, Matthias Schwab, and Walter E. Aulitzky

Subjects
precision-cut tumor slices, perfusion culture, tumor microenvironment, ovarian tumor, individual drug responses, mouse xenografts, Cytology, QH573-671
Abstract

Precision-cut tumor slices (PCTS) maintain tissue heterogeneity concerning different cell types and preserve the tumor microenvironment (TME). Typically, PCTS are cultured statically on a filter support at an air–liquid interface, which gives rise to intra-slice gradients during culture. To overcome this problem, we developed a perfusion air culture (PAC) system that can provide a continuous and controlled oxygen medium, and drug supply. This makes it an adaptable ex vivo system for evaluating drug responses in a tissue-specific microenvironment. PCTS from mouse xenografts (MCF-7, H1437) and primary human ovarian tumors (primary OV) cultured in the PAC system maintained the morphology, proliferation, and TME for more than 7 days, and no intra-slice gradients were observed. Cultured PCTS were analyzed for DNA damage, apoptosis, and transcriptional biomarkers for the cellular stress response. For the primary OV slices, cisplatin treatment induced a diverse increase in the cleavage of caspase-3 and PD-L1 expression, indicating a heterogeneous response to drug treatment between patients. Immune cells were preserved throughout the culturing period, indicating that immune therapy can be analyzed. The novel PAC system is suitable for assessing individual drug responses and can thus be used as a preclinical model to predict in vivo therapy responses.

Published
2023
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3. Prediction of Drug–Drug–Gene Interaction Scenarios of (E)-Clomiphene and Its Metabolites Using Physiologically Based Pharmacokinetic Modeling

Author

Christina Kovar, Lukas Kovar, Simeon Rüdesheim, Dominik Selzer, Boian Ganchev, Patrick Kröner, Svitlana Igel, Reinhold Kerb, Elke Schaeffeler, Thomas E. Mürdter, Matthias Schwab, and Thorsten Lehr

Subjects
clomiphene, pharmacokinetics, cytochrome P450 2D6 (CYP2D6) polymorphisms, drug–drug interactions (DDIs), drug–drug–gene interactions (DDGIs), drug–gene interactions (DGIs), Pharmacy and materia medica, RS1-441
Abstract

Clomiphene, a selective estrogen receptor modulator (SERM), has been used for the treatment of anovulation for more than 50 years. However, since (E)-clomiphene ((E)-Clom) and its metabolites are eliminated primarily via Cytochrome P450 (CYP) 2D6 and CYP3A4, exposure can be affected by CYP2D6 polymorphisms and concomitant use with CYP inhibitors. Thus, clomiphene therapy may be susceptible to drug–gene interactions (DGIs), drug–drug interactions (DDIs) and drug–drug–gene interactions (DDGIs). Physiologically based pharmacokinetic (PBPK) modeling is a tool to quantify such DGI and DD(G)I scenarios. This study aimed to develop a whole-body PBPK model of (E)-Clom including three important metabolites to describe and predict DGI and DD(G)I effects. Model performance was evaluated both graphically and by calculating quantitative measures. Here, 90% of predicted Cmax and 80% of AUClast values were within two-fold of the corresponding observed value for DGIs and DD(G)Is with clarithromycin and paroxetine. The model also revealed quantitative contributions of different CYP enzymes to the involved metabolic pathways of (E)-Clom and its metabolites. The developed PBPK model can be employed to assess the exposure of (E)-Clom and its active metabolites in as-yet unexplored DD(G)I scenarios in future studies.

Published
2022
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4. Clinical Trial: CYP2D6 Related Dose Escalation of Tamoxifen in Breast Cancer Patients With Iranian Ethnic Background Resulted in Increased Concentrations of Tamoxifen and Its Metabolites

Author

Zahra Khalaj, Zohreh Baratieh, Parvaneh Nikpour, Matthias Schwab, Elke Schaeffeler, Fariborz Mokarian, Hossein Khanahmad, Rasoul Salehi, Thomas E. Mürdter, and Mansoor Salehi

Subjects
CYP2D6, dose, endoxifen, genotype, metabolite, tamoxifen, Therapeutics. Pharmacology, RM1-950
Abstract

Introduction: The polymorphic enzyme cytochrome P450 2D6 (CYP2D6) catalyzes a major step in the bioactivation of tamoxifen. Genotyping of clinically relevant CYP2D6 alleles and subsequent dose adjustment is a promising approach to individualize breast cancer therapy. The aim of this study was to investigate the relationship between the plasma levels of tamoxifen and its metabolites and different CYP2D6 genotypes under standard (20 mg/day) and dose-adjusted therapy (Registration ID in Iranian Registry of Clinical Trials: IRCT2015082323734N1).Materials and Methods: Using TaqMan® assays common alleles of CYP2D6 (∗1, ∗2, ∗4, ∗5, ∗6, ∗10, ∗17, and ∗41) and gene duplication were identified in 134 breast cancer patients. Based on CYP2D6 genotypes patients with an activity score 1 (n = 15) and 0–0.5 (n = 2) were treated with tamoxifen adjusted dosage of 30 and 40 mg/day, respectively. The concentration of tamoxifen and its metabolites before and after 4 and 8 months of dose adjustment were measured using LC-MS/MS technology.Results: At baseline, (Z)-endoxifen plasma concentrations (33 ± 15.5, 28.1 ± 14, 26.6 ± 23.4, 14.3 ± 8.6, and 10.7 ± 5.5 nmol/l for EM/EM, EM/IM, EM/PM, IM/IM and PM/PM, respectively) and the metabolic ratio (Z)-Endoxifen/N-desmethyltamoxifen (0.0558 ± 0.02, 0.0396 ± 0.0111, 0.0332 ± 0.0222, 0.0149 ± 0.0026, and 0.0169 ± 0.0177 for EM/EM, EM/IM, EM/PM, IM/IM, and PM/PM, respectively) correlated with CYP2D6 genotype (Kruskal–Wallis p = 0.013 and p < 0.0001, respectively). Dose escalation to 30 and 40 mg/day in patients with a CYP2D6 activity score of 1 (n = 15) and 0–0.5 (n = 2) resulted in a significant increase in (Z)-endoxifen plasma levels (22.17 ± 24.42, 34.43 ± 26.54, and 35.77 ± 28.89 nmol/l at baseline, after 4 and 8 months, respectively, Friedman p = 0.0388) along with the plasma concentrations of tamoxifen and its other metabolites. No severe side effects were recorded during dose escalation.Conclusion: For the first time, we show the feasibility of dose escalation of tamoxifen in breast cancer patients with compromised CYP2D6 activity and Iranian ethnic background to increase the plasma concentrations of (Z)-endoxifen.

Published
2019
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5. Simulation-Based Assessment of the Impact of Non-Adherence on Endoxifen Target Attainment in Different Tamoxifen Dosing Strategies

Author

Anna Mueller-Schoell, Lena Klopp-Schulze, Robin Michelet, Madelé van Dyk, Thomas E. Mürdter, Matthias Schwab, Markus Joerger, Wilhelm Huisinga, Gerd Mikus, and Charlotte Kloft

Subjects
tamoxifen, non-adherence, model-informed precision dosing, pharmacokinetics, pharmacometrics, Medicine, Pharmacy and materia medica, RS1-441
Abstract

Tamoxifen is widely used in breast cancer treatment and minimum steady-state concentrations of its active metabolite endoxifen (CSS,min ENDX) above 5.97 ng/mL have been associated with favourable disease outcome. Yet, about 20% of patients do not reach target CSS,min ENDX applying conventional tamoxifen dosing. Moreover, 4–75% of patients are non-adherent, resulting in worse disease outcomes. Assuming complete adherence, we previously showed model-informed precision dosing (MIPD) to be superior to conventional and CYP2D6-guided dosing in minimising the proportion of patients with subtarget CSS,min ENDX. Given the high non-adherence rate in long-term tamoxifen therapy, this study investigated the impact of non-adherence on CSS,min ENDX target attainment in different dosing strategies. We show that MIPD allows to account for the expected level of non-adherence (here: up to 2 missed doses/week): increasing the MIPD target threshold from 5.97 ng/mL to 9 ng/mL (the lowest reported CSS,min ENDX in CYP2D6 normal metabolisers) as a safeguard resulted in the lowest interindividual variability and proportion of patients with subtarget CSS,min ENDX even in non-adherent patients. This is a significant improvement to conventional and CYP2D6-guided dosing. Adding a fixed increment to the originally selected dose is not recommended, since it inflates interindividual variability.

Published
2021
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6. Metabolic Drug Response Phenotyping in Colorectal Cancer Organoids by LC-QTOF-MS

Author

Sylvia K. Neef, Nicole Janssen, Stefan Winter, Svenja K. Wallisch, Ute Hofmann, Marc H. Dahlke, Matthias Schwab, Thomas E. Mürdter, and Mathias Haag

Subjects
metabolomics, lipidomics, metabolic profiling, organoids, colorectal cancer, QTOF, Microbiology, QR1-502
Abstract

As metabolic rewiring is crucial for cancer cell proliferation, metabolic phenotyping of patient-derived organoids is desirable to identify drug-induced changes and trace metabolic vulnerabilities of tumor subtypes. We established a novel protocol for metabolomic and lipidomic profiling of colorectal cancer organoids by liquid chromatography quadrupole time-of-flight mass spectrometry (LC-QTOF-MS) facing the challenge of capturing metabolic information from a minimal sample amount (v/v/v) without ECM removal. To eliminate ECM-derived background signals, we implemented a data filtering procedure based on the p-value and fold change cut-offs, which retained features with signal intensities >120% compared to matrix-derived signals present in blank samples. As a proof-of-concept, the method was applied to examine the early metabolic response of colorectal cancer organoids to 5-fluorouracil treatment. Statistical analysis revealed dose-dependent changes in the metabolic profiles of treated organoids including elevated levels of 2′-deoxyuridine, 2′-O-methylcytidine, inosine and 1-methyladenosine and depletion of 2′-deoxyadenosine and specific phospholipids. In accordance with the mechanism of action of 5-fluorouracil, changed metabolites are mainly involved in purine and pyrimidine metabolism. The novel protocol provides a first basis for the assessment of metabolic drug response phenotypes in 3D organoid models.

Published
2020
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7. Cross‐Ancestry Genome‐Wide Association Study Defines the Extended <scp> CYP2D6 </scp> Locus as the Principal Genetic Determinant of Endoxifen Plasma Concentrations

Author

Chiea Chuen Khor, Stefan Winter, Natalia Sutiman, Thomas E. Mürdter, Sylvia Chen, Joanne Siok Liu Lim, Zheng Li, Jingmei Li, Kar Seng Sim, Boian Ganchev, Diana Eccles, Bryony Eccles, William Tapper, Nathalie K. Zgheib, Arafat Tfayli, Raymond Chee Hui Ng, Yoon Sim Yap, Elaine Lim, Mabel Wong, Nan Soon Wong, Peter Cher Siang Ang, Rebecca Dent, Roman Tremmel, Kathrin Klein, Elke Schaeffeler, Yitian Zhou, Volker M. Lauschke, Michel Eichelbaum, Matthias Schwab, Hiltrud B. Brauch, Balram Chowbay, and Werner Schroth

Subjects
Pharmacology, Pharmacology (medical)
Abstract

The therapeutic efficacy of tamoxifen is predominantly mediated by its active metabolites 4-hydroxy-tamoxifen and endoxifen, whose formation is catalyzed by the polymorphic cytochrome P450 2D6 (CYP2D6). Yet, known CYP2D6 polymorphisms only partially determine metabolite concentrations in vivo. We performed the first cross-ancestry genome-wide association study with well-characterized patients of European, Middle-Eastern, and Asian descent (N = 497) to identify genetic factors impacting active and parent metabolite formation. Genome-wide significant variants were functionally evaluated in an independent liver cohort (N = 149) and in silico. Metabolite prediction models were validated in two independent European breast cancer cohorts (N = 287, N = 189). Within a single 1-megabase (Mb) region of chromosome 22q13 encompassing the CYP2D6 gene, 589 variants were significantly associated with tamoxifen metabolite concentrations, particularly endoxifen and metabolic ratio (MR) endoxifen/N-desmethyltamoxifen (minimal P = 5.4E-35 and 2.5E-65, respectively). Previously suggested other loci were not confirmed. Functional analyses revealed 66% of associated, mostly intergenic variants to be significantly correlated with hepatic CYP2D6 activity or expression (ρ = 0.35 to -0.52), and six hotspot regions in the extended 22q13 locus impacting gene regulatory function. Machine learning models based on hotspot variants (N = 12) plus CYP2D6 activity score (AS) increased the explained variability (~ 9%) compared with AS alone, explaining up to 49% (median R2 ) and 72% of the variability in endoxifen and MR endoxifen/N-desmethyltamoxifen, respectively. Our findings suggest that the extended CYP2D6 locus at 22q13 is the principal genetic determinant of endoxifen plasma concentration. Long-distance haplotypes connecting CYP2D6 with adjacent regulatory sites and nongenetic factors may account for the unexplained portion of variability.

Published
2023

8. Supplementary Figure from Triple Targeting of HER Receptors Overcomes Heregulin-mediated Resistance to EGFR Blockade in Colorectal Cancer

Author

Monilola A. Olayioye, Roland E. Kontermann, Matthias Schwab, Markus Morkel, Christine Sers, Marc-H. Dahlke, Thomas E. Mürdter, Svetlana Kalmykova, Thomas Sell, Lennart Kühl, Nicole Janssen, and Alexander Rau

Abstract

Supplementary Figure from Triple Targeting of HER Receptors Overcomes Heregulin-mediated Resistance to EGFR Blockade in Colorectal Cancer

Published
2023

9. Data from Triple Targeting of HER Receptors Overcomes Heregulin-mediated Resistance to EGFR Blockade in Colorectal Cancer

Author

Monilola A. Olayioye, Roland E. Kontermann, Matthias Schwab, Markus Morkel, Christine Sers, Marc-H. Dahlke, Thomas E. Mürdter, Svetlana Kalmykova, Thomas Sell, Lennart Kühl, Nicole Janssen, and Alexander Rau

Abstract

Current treatment options for patients with advanced colorectal cancers include anti-EGFR/HER1 therapy with the blocking antibody cetuximab. Although a subset of patients with KRAS WT disease initially respond to the treatment, resistance develops in almost all cases. Relapse has been associated with the production of the ligand heregulin (HRG) and/or compensatory signaling involving the receptor tyrosine kinases HER2 and HER3. Here, we provide evidence that triple-HER receptor blockade based on a newly developed bispecific EGFR×HER3-targeting antibody (scDb-Fc) together with the HER2-blocking antibody trastuzumab effectively inhibited HRG-induced HER receptor phosphorylation, downstream signaling, proliferation, and stem cell expansion of DiFi and LIM1215 colorectal cancer cells. Comparative analyses revealed that the biological activity of scDb-Fc plus trastuzumab was sometimes even superior to that of the combination of the parental antibodies, with PI3K/Akt pathway inhibition correlating with improved therapeutic response and apoptosis induction as seen by single-cell analysis. Importantly, growth suppression by triple-HER targeting was recapitulated in primary KRAS WT patient-derived organoid cultures exposed to HRG. Collectively, our results provide strong support for a pan-HER receptor blocking approach to combat anti-EGFR therapy resistance of KRAS WT colorectal cancer tumors mediated by the upregulation of HRG and/or HER2/HER3 signaling.

Published
2023

10. Data from Hyperthermia Synergizes with Chemotherapy by Inhibiting PARP1-Dependent DNA Replication Arrest

Author

Heiko van der Kuip, Walter E. Aulitzky, Georg Sauer, Jens O. Schmid, Thomas E. Mürdter, Simon Heine, Christoph Ulmer, Matthias Schwab, and Lea Schaaf

Abstract

Although hyperthermia offers clinical appeal to sensitize cells to chemotherapy, this approach has been limited in terms of long-term outcome as well as economic and technical burden. Thus, a more detailed knowledge about how hyperthermia exerts its effects on chemotherapy may illuminate ways to improve the approach. Here, we asked whether hyperthermia alters the response to chemotherapy-induced DNA damage and whether this mechanism is involved in its sensitizing effect in BRCA-competent models of ovarian and colon cancer. Notably, we found that hyperthermia delayed the repair of DNA damage caused by cisplatin or doxorubicin, acting upstream of different repair pathways to block histone polyADP-ribosylation (PARylation), a known effect of chemotherapy. Furthermore, hyperthermia blocked this histone modification as efficiently as pharmacologic inhibitors of PARP (PARPi), producing comparable delay in DNA repair, induction of double-strand breaks (DSB), and cell cytotoxicity after chemotherapy. Mechanistic investigations indicated that inhibiting PARylation by either hyperthermia or PARPi induced lethal DSB upon chemotherapy treatment not only by reducing DNA repair but also by preventing replication fork slowing. Overall, our work reveals how PARP blockade, either by hyperthermia or small-molecule inhibition, can increase chemotherapy-induced damage in BRCA-competent cells. Cancer Res; 76(10); 2868–75. ©2016 AACR.

Published
2023

15. Supplementary Figures 1-8 from Hyperthermia Synergizes with Chemotherapy by Inhibiting PARP1-Dependent DNA Replication Arrest

Author

Heiko van der Kuip, Walter E. Aulitzky, Georg Sauer, Jens O. Schmid, Thomas E. Mürdter, Simon Heine, Christoph Ulmer, Matthias Schwab, and Lea Schaaf

Abstract

Supplemental Figures (Supplementary Fig. 1-8): Cell lines are HR proficient (Supplementary Fig. 1); Influence of hyperthermia on the quantity of intra-nuclear Pt-DNA adducts and intracellular doxorubicin concentration (Supplementary Fig. 2); Hyperthermia sensitizes tumor cells to drugs which induce PARylation without altering PARP of PARG protein levels (Supplementary Fig. 3); Hyperthermia leads to a delayed DNA strand break repair capacity in different cell lines from ovarian and colon cancer (Supplementary Fig. 4); HR competence in 14 of 15 samples from PC patients (Supplementary Fig. 5); Gamma-irradiation leads to induction of γH2AX foci in all cells independent of proliferation status (Supplementary Fig. 6); Hyperthermia has no acute effect on cisplatin or doxorubicin induced apoptosis (Supplementary Fig. 7); Combined treatment of cells with hyperthermia and PARPi slightly enhanced the potentiating effect of either treatment alone (Supplementary Fig. 8).

Published
2023

18. Triple Targeting of HER Receptors Overcomes Heregulin-mediated Resistance to EGFR Blockade in Colorectal Cancer

Author

Alexander Rau, Nicole Janssen, Lennart Kühl, Thomas Sell, Svetlana Kalmykova, Thomas E. Mürdter, Marc-H. Dahlke, Christine Sers, Markus Morkel, Matthias Schwab, Roland E. Kontermann, and Monilola A. Olayioye

Subjects
Cancer Research, Receptor, ErbB-3, Receptor, ErbB-2, Neuregulin-1, Trastuzumab, ErbB Receptors, Proto-Oncogene Proteins p21(ras), Phosphatidylinositol 3-Kinases, Oncology, Drug Resistance, Neoplasm, Cell Line, Tumor, Humans, Neoplasm Recurrence, Local, Colorectal Neoplasms
Abstract

Current treatment options for patients with advanced colorectal cancers include anti-EGFR/HER1 therapy with the blocking antibody cetuximab. Although a subset of patients with KRAS WT disease initially respond to the treatment, resistance develops in almost all cases. Relapse has been associated with the production of the ligand heregulin (HRG) and/or compensatory signaling involving the receptor tyrosine kinases HER2 and HER3. Here, we provide evidence that triple-HER receptor blockade based on a newly developed bispecific EGFR×HER3-targeting antibody (scDb-Fc) together with the HER2-blocking antibody trastuzumab effectively inhibited HRG-induced HER receptor phosphorylation, downstream signaling, proliferation, and stem cell expansion of DiFi and LIM1215 colorectal cancer cells. Comparative analyses revealed that the biological activity of scDb-Fc plus trastuzumab was sometimes even superior to that of the combination of the parental antibodies, with PI3K/Akt pathway inhibition correlating with improved therapeutic response and apoptosis induction as seen by single-cell analysis. Importantly, growth suppression by triple-HER targeting was recapitulated in primary KRAS WT patient-derived organoid cultures exposed to HRG. Collectively, our results provide strong support for a pan-HER receptor blocking approach to combat anti-EGFR therapy resistance of KRAS WT colorectal cancer tumors mediated by the upregulation of HRG and/or HER2/HER3 signaling.

Published
2022

20. (Z)-Endoxifen and Early Recurrence of Breast Cancer: An Explorative Analysis in a Prospective Brazilian Study

Author

Thais Almeida, Werner Schroth, Jeanine Nardin, Thomas E. Mürdter, Stefan Winter, Solane Picolotto, Reiner Hoppe, Jenifer Kogin, Elisa Gaio, Angela Dasenbrock, Raquel Cristina Skrsypcsak, Lucia de Noronha, Matthias Schwab, Hiltrud Brauch, and José Claudio Casali-da-Rocha

Subjects
breast cancer, CYP2D6, tamoxifen, (Z)-endoxifen, early recurrence, survival, Brazil, Medicine (miscellaneous)
Abstract

Adherence to treatment and use of co-medication, but also molecular factors such as CYP2D6 genotype, affect tamoxifen metabolism, with consequences for early breast cancer prognosis. In a prospective study of 149 tamoxifen-treated early-stage breast cancer patients from Brazil followed up for 5 years, we investigated the association between the active tamoxifen metabolite (Z)-endoxifen at 3 months and event-free survival (EFS) adjusted for clinico-pathological factors. Twenty-five patients (16.8%) had recurred or died at a median follow-up of 52.3 months. When we applied a putative 15 nM threshold used in previous independent studies, (Z)-endoxifen levels below the threshold showed an association with shorter EFS in univariate analysis (p = 0.045) and after adjustment for stage (HR 2.52; 95% CI 1.13–5.65; p = 0.024). However, modeling of plasma concentrations with splines instead of dichotomization did not verify a significant association with EFS (univariate analysis: p = 0.158; adjusted for stage: p = 0.117). Hence, in our small exploratory study, the link between impaired tamoxifen metabolism and early breast cancer recurrence could not be unanimously demonstrated. This inconsistency justifies larger modeling studies backed up by mechanistic pharmacodynamic analyses to shed new light on this suspected association and the stipulation of an appropriate predictive (Z)-endoxifen threshold.

Published
2022
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21. Obesity Alters Endoxifen Plasma Levels in Young Breast Cancer Patients

Author

Ellen Copson, Hiltrud Brauch, Robin Michelet, Matthias Schwab, Wilhelm Huisinga, Lena Klopp-Schulze, Patrick Neven, Diana Eccles, Nathalie K. Zgheib, Thomas E. Mürdter, Sylvia Chen, Ron H.J. Mathijssen, Werner Schroth, Arafat Tfayli, Markus Joerger, Balram Chowbay, Anna Mueller-Schoell, Charlotte Kloft, Stijn L.W. Koolen, and Medical Oncology

Subjects
Oncology, obesity, Pharmacogenomic Variants, CYP2D6 GENOTYPE, Overweight, 030226 pharmacology & pharmacy, 0302 clinical medicine, endoxifen plasma, Pharmacology (medical), Pharmacology & Pharmacy, skin and connective tissue diseases, Aged, 80 and over, Endoxifen, Age Factors, WOMEN, PREMENOPAUSAL PATIENTS, Middle Aged, Cytochrome P-450 CYP2D6, 030220 oncology & carcinogenesis, Female, medicine.symptom, Life Sciences & Biomedicine, METABOLITE CONCENTRATIONS, medicine.drug, Adult, medicine.medical_specialty, CYP2D6, Antineoplastic Agents, Hormonal, ADJUVANT TAMOXIFEN, Breast Neoplasms, Young Adult, 03 medical and health sciences, Breast cancer, breast cancer, Pharmacokinetics, SDG 3 - Good Health and Well-being, Internal medicine, medicine, Humans, DOSE-ESCALATION, Computer Simulation, Dosing, EXPOSURE, METAANALYSIS, Aged, Pharmacology, Science & Technology, PHARMACOGENETICS, business.industry, Body Weight, Models, Theoretical, medicine.disease, Obesity, SERUM CONCENTRATIONS, Tamoxifen, 500 Naturwissenschaften und Mathematik::570 Biowissenschaften, Biologie::572 Biochemie, business
Abstract

Endoxifen is one of the most important metabolites of the prodrug tamoxifen. High interindividual variability in endoxifen steady-state concentrations (CSS,min ENDX ) is observed under tamoxifen standard dosing and patients with breast cancer who do not reach endoxifen concentrations above a proposed therapeutic threshold of 5.97 ng/mL may be at a 26% higher recurrence risk compared with patients with endoxifen concentrations exceeding this value. In this investigation, 10 clinical tamoxifen studies were pooled (1,388 patients) to investigate influential factors on CSS,min ENDX using nonlinear mixed-effects modeling. Age and body weight were found to significantly impact CSS,min ENDX in addition to CYP2D6 phenotype. Compared with postmenopausal patients, premenopausal patients had a 30% higher risk for subtarget CSS,min ENDX at tamoxifen 20 mg per day. In treatment simulations for distinct patient subpopulations, young overweight patients had a 3.1-13.8-fold higher risk for subtarget CSS,min ENDX compared with elderly low-weight patients. Considering ever-rising obesity rates and the clinical importance of tamoxifen for premenopausal patients, this subpopulation may benefit most from individualized tamoxifen dosing. ispartof: CLINICAL PHARMACOLOGY & THERAPEUTICS vol:108 issue:3 pages:661-670 ispartof: location:United States status: published

Published
2020

22. Subunits of BK channels promote breast cancer development and modulate responses to endocrine treatment in preclinical models

Author

Dominic Gross, Stephan M. Huber, Stephen F. Madden, Benjamin Stegen, Robert Lukowski, Hiltrud Brauch, Severine Stehling, Alice Dragoi, Werner Schroth, Thomas E. Mürdter, Selina Maier, Corinna J. Mohr, Reiner Hoppe, Friederike A. Steudel, and Peter Ruth

Subjects
0301 basic medicine, BK channel, Cell, Estrogen receptor, Breast Neoplasms, Mice, Transgenic, Context (language use), Membrane Potentials, Mice, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Animals, Humans, Medicine, Large-Conductance Calcium-Activated Potassium Channels, skin and connective tissue diseases, Mice, Knockout, Pharmacology, biology, business.industry, medicine.disease, Tamoxifen, 030104 developmental biology, medicine.anatomical_structure, Cell culture, Cancer cell, biology.protein, Cancer research, Female, business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Background and purpose Pore-forming α subunits of the voltage- and Ca2+ -activated K+ channel with large conductance (BKα) promote malignant phenotypes of breast tumour cells. Auxiliary subunits such as the leucine-rich repeat containing 26 (LRRC26) protein, also termed BKγ1, may be required to permit activation of BK currents at a depolarized resting membrane potential that frequently occur in non-excitable tumour cells. Experimental approach Anti-tumour effects of BKα loss were investigated in breast tumour-bearing MMTV-PyMT transgenic BKα knockout (KO) mice, primary MMTV-PyMT cell cultures, and in a syngeneic transplantation model of breast cancer derived from these cells. The therapeutic relevance of BK channels in the context of endocrine treatment was assessed in human breast cancer cell lines expressing either low (MCF-7) or high (MDA-MB-453) levels of BKα and BKγ1, as well as in BKα-negative MDA-MB-157. Key results BKα promoted breast cancer onset and overall survival in preclinical models. Conversely, lack of BKα and/or knockdown of BKγ1 attenuated proliferation of murine and human breast cancer cells in vitro. At low concentrations, tamoxifen and its major active metabolites stimulated proliferation of BKα/γ1-positive breast cancer cells, independent of the genomic signalling controlled by the oestrogen receptor. Finally, tamoxifen increased the relative survival time of BKα KO but not of wild-type tumour cell recipient mice. Conclusion and implications Breast cancer initiation, progression, and tamoxifen sensitivity depend on functional BK channels thereby providing a rationale for the future exploration of the oncogenic actions of BK channels in clinical outcomes with anti-oestrogen therapy.

Published
2020

23. Abstract P2-11-12: The influences of adherence to tamoxifen and CYP2D6 pharmacogenetics on plasma concentrations of the active metabolite (Z)-endoxifen in breast cancer

Author

Thomas E. Mürdter, Matthias Schwab, Werner Schroth, Jeanine Marie Nardin, Thais Abreu Almeida, Roberto Pecoits-Filho, Silvia Dr Moraes, Hiltrud Brauch, Solange Picolotto, Jenifer Primon Kogin, Evelyn Cl Vendramini, Reiner Hoppe, Diandra Miqueleto, and Jose Claudio Casali da Rocha

Subjects
Oncology, Cancer Research, medicine.medical_specialty, CYP2D6, business.industry, Estrogen receptor, Cancer, medicine.disease, Breast cancer, Selective estrogen receptor modulator, Internal medicine, medicine, skin and connective tissue diseases, Prospective cohort study, business, Tamoxifen, Pharmacogenetics, medicine.drug
Abstract

One-third of early breast cancer patients with estrogen receptor (ER) positive tumors treated with the selective estrogen receptor modulator tamoxifen either relapse or die from the disease in the following decade. Improvement of tamoxifen efficacy requires a better knowledge of factors determining outcome of which the medication-taking behavior, i.e. adherence, is a strong suspect. Discontinuation and non-adherence to tamoxifen are frequent and result in increased mortality. Commonly used methods to assess drug adherence such as prescription-refill patterns infer that the medication is taken exactly as prescribed yet, partial adherence or actual use of the medication cannot be controlled. An objective surrogate of tamoxifen adherence is the monitoring of drug concentrations in the patients’ plasma including the parent drug and its active metabolite (Z)-endoxifen (endoxifen), however individual concentrations depend on pharmacogene polymorphisms particularly those of the liver enzyme cytochrome P450 2D6 (CYP2D6). Patients without CYP2D6 variants have normal enzyme function (extensive metabolizer, EM) and achieve high endoxifen concentrations compared to patients with variants conferring absent activity (poor metabolizer, PM) or reduced activity (intermediate metabolizer, IM) who have significantly lower plasma concentrations of the active metabolite. A putative threshold of 5.9 ng/mL endoxifen has been proposed suggesting that patients with endoxifen concentration above or below threshold have lower or higher risk for recurrence, assuming that low endoxifen exposure in the tumor likely results in incomplete inhibition of ER-dependent growth signaling. During tamoxifen treatment it is therefore important that patients achieve clinically relevant endoxifen levels while at the same time avoid confounders of which adherence is a prime candidate. To this end, we investigated patients’ ability to achieve relevant plasma concentrations during tamoxifen treatment in relation to their CYP2D6 metabolizer status and their tamoxifen adherence behavior. Our prospective study included 192 Brazilian breast cancer patients treated with 20 mg tamoxifen daily. Two-thirds of the patients were premenopausal. Plasma levels of tamoxifen and its metabolites were measured by LC-MS/MS at 3, 6 and 12 months of treatment. Adherence to tamoxifen was evaluated by the questionnaire-based Morisky medication adherence scale. CYP2D6 polymorphisms were determined by MALDI-TOF mass spectrometry and real-time PCR. Adherence to tamoxifen decreased from 74% at month 3 to 64% at month 12, and explained 47% of the variability of tamoxifen plasma concentrations (P Citation Format: Jose Claudio Casali da Rocha, Jeanine M Nardin, Werner Schroth, Thais A Almeida, Thomas Mürdter, Solange Picolotto, Evelyn CL Vendramini, Reiner Hoppe, Jenifer P Kogin, Diandra Miqueleto, Silvia DR Moraes, Matthias Schwab, Roberto F Pecoits-Filho, Hiltrud Brauch. The influences of adherence to tamoxifen and CYP2D6 pharmacogenetics on plasma concentrations of the active metabolite (Z)-endoxifen in breast cancer [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P2-11-12.

Published
2020

24. Raman Imaging and Fluorescence Lifetime Imaging Microscopy for Diagnosis of Cancer State and Metabolic Monitoring

Author

Julia Marzi, Anne T. Nies, Thomas E. Mürdter, Shannon L. Layland, Nicole Janssen, Lucas Becker, and Katja Schenke-Layland

Subjects
Drug, tissue diagnostics, Cancer Research, Fluorescence-lifetime imaging microscopy, media_common.quotation_subject, Review, Raman microspectroscopy, symbols.namesake, In vivo, 3D in vitro models, Medicine, RC254-282, media_common, fluorescence lifetime imaging microscopy, in situ imaging, business.industry, Cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Autofluorescence, Oncology, Cancer research, symbols, tumor metabolism, Personalized medicine, business, Raman spectroscopy
Abstract

Simple Summary In spite of significant improvements in diagnosis and treatment options, cancer treatments still suffer from late detection and patient-specific multidrug resistance causing limited efficacy of systemic drug therapies. This review delineates the pioneering works on current advances in Raman spectroscopy and fluorescence lifetime imaging microscopy and their non-invasive application in in vitro and in vivo cancer identification, early-stage monitoring, drug screening, and metabolic analysis. In addition, the remaining challenges and limitations of the methods will be discussed and important aspects of their application in the clinic, enabling them to be a real asset to clinicians in the future and complementing current gold standard methods, will be explained. Abstract Hurdles for effective tumor therapy are delayed detection and limited effectiveness of systemic drug therapies by patient-specific multidrug resistance. Non-invasive bioimaging tools such as fluorescence lifetime imaging microscopy (FLIM) and Raman-microspectroscopy have evolved over the last decade, providing the potential to be translated into clinics for early-stage disease detection, in vitro drug screening, and drug efficacy studies in personalized medicine. Accessing tissue- and cell-specific spectral signatures, Raman microspectroscopy has emerged as a diagnostic tool to identify precancerous lesions, cancer stages, or cell malignancy. In vivo Raman measurements have been enabled by recent technological advances in Raman endoscopy and signal-enhancing setups such as coherent anti-stokes Raman spectroscopy or surface-enhanced Raman spectroscopy. FLIM enables in situ investigations of metabolic processes such as glycolysis, oxidative stress, or mitochondrial activity by using the autofluorescence of co-enzymes NADH and FAD, which are associated with intrinsic proteins as a direct measure of tumor metabolism, cell death stages and drug efficacy. The combination of non-invasive and molecular-sensitive in situ techniques and advanced 3D tumor models such as patient-derived organoids or microtumors allows the recapitulation of tumor physiology and metabolism in vitro and facilitates the screening for patient-individualized drug treatment options.

Published
2021

25. The Influences of Adherence to Tamoxifen and CYP2D6 Pharmacogenetics on Plasma Concentrations of the Active Metabolite (Z)‐Endoxifen in Breast Cancer

Author

Jeanine Marie Nardin, José Cláudio Casali-da-Rocha, Jenifer Primon Kogin, Reiner Hoppe, Thomas E. Mürdter, Hiltrud Brauch, Evelyn Castillo Lima Vendramini, Roberto Pecoits-Filho, Thais Abreu Almeida, Solane Picolotto, Werner Schroth, Diandra Miqueleto, Matthias Schwab, and Silvia Dark Robaskievicz de Moraes

Subjects
Oncology, 030213 general clinical medicine, Pharmacogenomic Variants, 030226 pharmacology & pharmacy, 0302 clinical medicine, General Pharmacology, Toxicology and Pharmaceutics, skin and connective tissue diseases, Aged, 80 and over, General Neuroscience, lcsh:Public aspects of medicine, General Medicine, Articles, Middle Aged, 3. Good health, Cytochrome P-450 CYP2D6, Female, Drug Monitoring, Brazil, medicine.drug, Adult, medicine.medical_specialty, CYP2D6, Antineoplastic Agents, Hormonal, Breast Neoplasms, General Biochemistry, Genetics and Molecular Biology, Article, Medication Adherence, 03 medical and health sciences, Young Adult, Breast cancer, Internal medicine, medicine, Humans, Active metabolite, Aged, business.industry, Research, lcsh:RM1-950, lcsh:RA1-1270, medicine.disease, Confidence interval, Pharmacogenomic Testing, Tamoxifen, lcsh:Therapeutics. Pharmacology, Relative risk, Self Report, business, Pharmacogenetics, Drug metabolism
Abstract

Tamoxifen efficacy in breast cancer is suspected to depend on adherence and intact drug metabolism. We evaluated the role of adherence behavior and pharmacogenetics on the formation rate of (Z)-endoxifen. In 192 Brazilian patients, we assessed plasma levels of tamoxifen and its metabolites at 3, 6, and 12 months of treatment (liquid-chromatography tandem mass spectrometry), adherence behavior (Morisky, Green, and Levine medication adherence scale), and cytochrome P450 2D6 (CYP2D6) and other pharmacogene polymorphisms (matrix-assisted laser-desorption-ionization time of flight) mass spectrometry, real-time polymerase chain reaction). Adherence explained 47% of the variability of tamoxifen plasma concentrations (P

Published
2019

26. Computational Treatment Simulations to Assess the Need for Personalized Tamoxifen Dosing in Breast Cancer Patients of Different Biogeographical Groups

Author

Anna Mueller-Schoell, Robin Michelet, Lena Klopp-Schulze, Madelé van Dyk, Thomas E. Mürdter, Matthias Schwab, Markus Joerger, Wilhelm Huisinga, Gerd Mikus, and Charlotte Kloft

Subjects
model-informed precision dosing, tamoxifen, CYP2D6, genotype, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, personalized dosing, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::616 Krankheiten, Article, polymorphism, breast cancer, individualized dosing, otorhinolaryngologic diseases, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::615 Pharmakologie, Therapeutik, skin and connective tissue diseases, RC254-282, hormones, hormone substitutes, and hormone antagonists
Abstract

Tamoxifen is used worldwide to treat estrogen receptor-positive breast cancer. It is extensively metabolized, and minimum steady-state concentrations of its metabolite endoxifen (CSS,min ENDX) &gt, 5.97 ng/mL have been associated with favorable outcome. Endoxifen formation is mediated by the enzyme CYP2D6, and impaired CYP2D6 function has been associated with lower CSS,min&nbsp, ENDX. In the Women’s Healthy Eating and Living (WHEL) study proposing the target concentration, 20% of patients showed subtarget CSS,min ENDX at tamoxifen standard dosing. CYP2D6 allele frequencies vary largely between populations, and as 87% of the patients in the WHEL study were White, little is known about the risk for subtarget CSS,min ENDX in other populations. Applying pharmacokinetic simulations, this study investigated the risk for subtarget CSS,min ENDX at tamoxifen standard dosing and the need for dose individualization in nine different biogeographical groups with distinct CYP2D6 allele frequencies. The high variability in CYP2D6 allele frequencies amongst the biogeographical groups resulted in an up to three-fold difference in the percentages of patients with subtarget CSS,min ENDX. Based on their CYP2D6 allele frequencies, East Asian breast cancer patients were identified as the population for which personalized, model-informed precision dosing would be most beneficial (28% of patients with subtarget CSS,min ENDX).

Published
2021

27. Stress-induced TRAILR2 expression overcomes TRAIL resistance in cancer cell spheroids

Author

Kai Cao, Peter Scheurich, Roland E. Kontermann, Tobias B. Beigl, Thomas E. Mürdter, Cathrin Hagenlocher, Alexandra Mack, Daniela Simone Maichl, Stephen W.G. Tait, Daniela Stöhr, Markus Rehm, Beate Budai, Jens O Schmid, Gavin Fullstone, and Nadine Pollak

Subjects
Cancer microenvironment, Tumour heterogeneity, Cell, Apoptosis, Article, TNF-Related Apoptosis-Inducing Ligand, Cell Line, Tumor, Neoplasms, Spheroids, Cellular, medicine, Humans, Molecular Biology, Cyclooxygenase 2 Inhibitors, Chemistry, Spheroid, Cell Biology, Ligand (biochemistry), Cell biology, Receptors, TNF-Related Apoptosis-Inducing Ligand, medicine.anatomical_structure, Celecoxib, Drug Resistance, Neoplasm, Cancer cell, embryonic structures, Unfolded protein response, Tumor necrosis factor alpha, Trail resistance
Abstract

The influence of 3D microenvironments on apoptosis susceptibility remains poorly understood. Here, we studied the susceptibility of cancer cell spheroids, grown to the size of micrometastases, to tumor necrosis factor-related apoptosis-inducing ligand (TRAIL). Interestingly, pronounced, spatially coordinated response heterogeneities manifest within spheroidal microenvironments: In spheroids grown from genetically identical cells, TRAIL-resistant subpopulations enclose, and protect TRAIL-hypersensitive cells, thereby increasing overall treatment resistance. TRAIL-resistant layers form at the interface of proliferating and quiescent cells and lack both TRAILR1 and TRAILR2 protein expression. In contrast, oxygen, and nutrient deprivation promote high amounts of TRAILR2 expression in TRAIL-hypersensitive cells in inner spheroid layers. COX-II inhibitor celecoxib further enhanced TRAILR2 expression in spheroids, likely resulting from increased ER stress, and thereby re-sensitized TRAIL-resistant cell layers to treatment. Our analyses explain how TRAIL response heterogeneities manifest within well-defined multicellular environments, and how spatial barriers of TRAIL resistance can be minimized and eliminated., Deutsche Forschungsgemeinschaft (German Research Foundation), European Union’s Horizon 2020 research and innovation program, Cluster of Excellence in Simulation Technology, Projekt DEAL

Published
2020

28. Metabolic Drug Response Phenotyping in Colorectal Cancer Organoids by LC-QTOF-MS

Author

Stefan Winter, Ute Hofmann, Mathias Haag, Nicole Janssen, Marc H Dahlke, Thomas E. Mürdter, Matthias Schwab, Svenja K Wallisch, and Sylvia K. Neef

Subjects
0301 basic medicine, Purine, Colorectal cancer, Endocrinology, Diabetes and Metabolism, lcsh:QR1-502, colorectal cancer, Biology, Biochemistry, lcsh:Microbiology, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Metabolomics, Liquid chromatography–mass spectrometry, Lipidomics, Organoid, medicine, Inosine, Molecular Biology, organoids, metabolic profiling, metabolomics, lipidomics, QTOF, LC-MS, medicine.disease, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Pyrimidine metabolism, Cancer research, medicine.drug
Abstract

As metabolic rewiring is crucial for cancer cell proliferation, metabolic phenotyping of patient-derived organoids is desirable to identify drug-induced changes and trace metabolic vulnerabilities of tumor subtypes. We established a novel protocol for metabolomic and lipidomic profiling of colorectal cancer organoids by liquid chromatography quadrupole time-of-flight mass spectrometry (LC-QTOF-MS) facing the challenge of capturing metabolic information from a minimal sample amount (120% compared to matrix-derived signals present in blank samples. As a proof-of-concept, the method was applied to examine the early metabolic response of colorectal cancer organoids to 5-fluorouracil treatment. Statistical analysis revealed dose-dependent changes in the metabolic profiles of treated organoids including elevated levels of 2′-deoxyuridine, 2′-O-methylcytidine, inosine and 1-methyladenosine and depletion of 2′-deoxyadenosine and specific phospholipids. In accordance with the mechanism of action of 5-fluorouracil, changed metabolites are mainly involved in purine and pyrimidine metabolism. The novel protocol provides a first basis for the assessment of metabolic drug response phenotypes in 3D organoid models.

Published
2020

29. Gene Expression Signatures of BRCAness and Tumor Inflammation Define Subgroups of Early-Stage Hormone Receptor-Positive Breast Cancer Patients

Author

Peter Fritz, Matthias Schwab, Werner Schroth, Tanja Fehm, Hiltrud Brauch, Jörg Kumbrink, Thomas E. Mürdter, Diethelm Wallwiener, Florian Büttner, Thomas Kirchner, Peter A. Fasching, Georg Sauer, David Allen Henderson, Siarhei Kandabarau, Reiner Hoppe, Stephen F. Madden, Yuqi Ren, and Heather Ann Brauer

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Receptor, ErbB-2, Estrogen receptor, Breast Neoplasms, 03 medical and health sciences, Basal (phylogenetics), 0302 clinical medicine, Immune system, Breast cancer, Lymphocytes, Tumor-Infiltrating, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Biomarkers, Tumor, Humans, Aromatase, Aged, Retrospective Studies, Aged, 80 and over, BRCA2 Protein, Inflammation, biology, business.industry, BRCA1 Protein, Middle Aged, medicine.disease, Prognosis, Androgen receptor, 030104 developmental biology, Receptors, Estrogen, Hormone receptor, 030220 oncology & carcinogenesis, biology.protein, Female, business, Receptors, Progesterone, Transcriptome, Tamoxifen, medicine.drug, Follow-Up Studies
Abstract

Purpose: Patients with estrogen receptor– and/or progesterone receptor–positive, early breast cancer benefit from hormonal treatment, yet high global death burdens due to high prevalence and long-term recurrence risk call for biomarkers to guide additional treatment approaches. Experimental Design: From a prospective, observational study of postmenopausal early breast cancer patients treated with tamoxifen or aromatase inhibitors, gene expression analyses of 612 tumors was performed using the NanoString Breast Cancer 360 panel to interrogate 23 breast cancer pathways. Candidate signatures associated with disease subtype and event-free survival (EFS) were obtained by cluster analysis, Cox modeling, and conditional inference trees, and were independently tested in 613 patients from BreastMark. Tumor-infiltrating lymphocytes (TIL) were assessed on tissue sections, and mutational burden was assessed in 36 tumors by whole-exome sequencing. Results: PAM50-derived classification distinguished lower-risk (Luminal A) from higher-risk subtypes (Luminal B, P = 0.04; HER2, P = 0.006; Basal, P = 0.008). In higher-risk patients, shorter EFS was associated with low androgen receptor [HR = 3.61; 95% confidence interval (CI), 1.72–7.56; P = 0.001] or high BRCAness signature expression (HR = 3.58; 95% CI, 1.19–10.7; P = 0.023). BRCAness was independently confirmed as a predictor of shorter EFS (HR = 2.64; 95% CI, 1.31–5.34; P = 0.007). About 13%–15% of patients, enriched for high-grade, higher-risk subtypes (P ≤ 0.0001), had strong expression of the Tumor Inflammation Signature (TIS) suggestive of an inhibited antitumor immune response. TIS scores were strongly associated with TIL numbers (P < 1e-30) but not with tumor mutation status. Conclusions: BRCA-related DNA repair deficiency and suppressed tumor immune responses may be clinically relevant predictors of endocrine therapy complementing treatment options in subgroups of hormone-sensitive early breast cancer.

Published
2020

30. Optimized protocol for metabolomic and lipidomic profiling in formalin-fixed paraffin-embedded kidney tissue by LC-MS

Author

Stefan Winter, Elke Schaeffeler, German Ott, Mathias Haag, Thomas E. Mürdter, Falko Fend, Sylvia K. Neef, Axel Walch, Heike Horn, Ute Hofmann, Jörg Hennenlotter, Matthias Schwab, Achim Buck, and Jens Bedke

Subjects
Formalin fixed paraffin embedded, Metabolite, 02 engineering and technology, Kidney, 01 natural sciences, Biochemistry, Analytical Chemistry, chemistry.chemical_compound, Metabolomics, Liquid chromatography–mass spectrometry, Tandem Mass Spectrometry, Formaldehyde, Lipidomics, medicine, Environmental Chemistry, Sample preparation, Spectroscopy, Paraffin Embedding, 010401 analytical chemistry, 021001 nanoscience & nanotechnology, 0104 chemical sciences, medicine.anatomical_structure, chemistry, Non targeted metabolomics, 0210 nano-technology, Chromatography, Liquid
Abstract

Formalin-fixed and paraffin-embedded (FFPE) tissue represents a valuable resource to examine cancer metabolic alterations and to identify potential markers of disease. Protocols commonly used for liquid-chromatography mass spectrometry (LC-MS)-based FFPE metabolomics have not been optimized for lipidomic analysis and pre-analytical factors, that potentially affect metabolite levels, were scarcely investigated. We here demonstrate the assessment and optimization of sample preparation procedures for comprehensive metabolomic and lipidomic profiling in FFPE kidney tissue by LC-QTOF-MS. The optimized protocol allows improved monitoring of lipids including ceramides (Cer), glycosphingolipids (GSL) and triglycerides (TAGs) while the profiling capability for small polar molecules is maintained. Further, repeatable sample preparation (CVs 20%) along with high analytical (CVs 10%) and inter-day precision (CVs 20%) is achieved. As proof of concept, we analyzed a set of clear cell renal cell carcinoma (ccRCC) and corresponding non-tumorous FFPE tissue samples, achieving phenotypic distinction. Investigation of the impact of tissue fixation time (6 h, 30 h and 54 h) on FFPE tissue metabolic profiles revealed metabolite class-dependent differences on their detection abundance. Whereas specific lipids (e.g. phosphatidylinositoles, GSLs, saturated fatty acids and saturated lyso-phosphatidytlethanolamines [LPE]) remained largely unaffected (CVs 20% between groups of fixation time), neutral lipids (e.g. Cer and TAGs) exhibited high variability (CVs 80%). Strikingly, out of the lipid classes assigned as unaffected, fatty acids 18:0, 16:0 and LPE 18:0 were detectable by high-resolution MALDI-FT-ICR MS imaging in an independent cohort of ccRCC tissues (n = 64) and exhibited significant differences between tumor and non-tumor regions.

Published
2020

31. The formation of estrogen-like tamoxifen metabolites and their influence on enzyme activity and gene expression of ADME genes

Author

Michel Eichelbaum, Astrid Nörenberg, Maria Thomas, Ulrich M. Zanger, Werner Schroth, Thomas E. Mürdter, Hiltrud Brauch, Matthias Schwab, Janina Johänning, and Patrick Kröner

Subjects
CYP2B6, Bisphenol, Health, Toxicology and Mutagenesis, Metabolite, Glucuronidation, Estrogen receptor, Gene induction, Pharmacology, Alkenes, Toxicology, 030226 pharmacology & pharmacy, Gene Expression Regulation, Enzymologic, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Glucuronides, Cytochrome P-450 Enzyme System, Phenols, medicine, Humans, Glucuronosyltransferase, skin and connective tissue diseases, ADME, CYP3A4, Estrogens, General Medicine, Tamoxifen, Metabolism, Estrogen-like metabolites, chemistry, 030220 oncology & carcinogenesis, Hepatocytes, Microsomes, Liver, hormones, hormone substitutes, and hormone antagonists, CYP activity, medicine.drug, Toxicokinetics and Metabolism
Abstract

Tamoxifen, a standard therapy for breast cancer, is metabolized to compounds with anti-estrogenic as well as estrogen-like action at the estrogen receptor. Little is known about the formation of estrogen-like metabolites and their biological impact. Thus, we characterized the estrogen-like metabolites tamoxifen bisphenol and metabolite E for their metabolic pathway and their influence on cytochrome P450 activity and ADME gene expression. The formation of tamoxifen bisphenol and metabolite E was studied in human liver microsomes and Supersomes™. Cellular metabolism and impact on CYP enzymes was analyzed in upcyte® hepatocytes. The influence of 5 µM of tamoxifen, anti-estrogenic and estrogen-like metabolites on CYP activity was measured by HPLC MS/MS and on ADME gene expression using RT-PCR analyses. Metabolite E was formed from tamoxifen by CYP2C19, 3A and 1A2 and from desmethyltamoxifen by CYP2D6, 1A2 and 3A. Tamoxifen bisphenol was mainly formed from (E)- and (Z)-metabolite E by CYP2B6 and CYP2C19, respectively. Regarding phase II metabolism, UGT2B7, 1A8 and 1A3 showed highest activity in glucuronidation of tamoxifen bisphenol and metabolite E. Anti-estrogenic metabolites (Z)-4-hydroxytamoxifen, (Z)-endoxifen and (Z)-norendoxifen inhibited the activity of CYP2C enzymes while tamoxifen bisphenol consistently induced CYPs similar to rifampicin and phenobarbital. On the transcript level, highest induction up to 5.6-fold was observed for CYP3A4 by tamoxifen, (Z)-4-hydroxytamoxifen, tamoxifen bisphenol and (E)-metabolite E. Estrogen-like tamoxifen metabolites are formed in CYP-dependent reactions and are further metabolized by glucuronidation. The induction of CYP activity by tamoxifen bisphenol and the inhibition of CYP2C enzymes by anti-estrogenic metabolites may lead to drug–drug-interactions. Electronic supplementary material The online version of this article (10.1007/s00204-017-2147-y) contains supplementary material, which is available to authorized users.

Published
2017

32. Comprehensive Metabolomic and Lipidomic Profiling of Human Kidney Tissue: A Platform Comparison

Author

Ute Hofmann, Judith Wahrheit, Elke Schaeffeler, Jörg Hennenlotter, Florian Büttner, Thomas E. Mürdter, Denise Sonntag, Matthias Schwab, Falko Fend, Jens Bedke, Mathias Haag, Steffen Rausch, Stefan Winter, and Patrick Leuthold

Subjects
0301 basic medicine, Swine, Biology, Kidney, Biochemistry, 03 medical and health sciences, Metabolomics, Liquid chromatography–mass spectrometry, Lipidomics, Animals, Humans, Carcinoma, Renal Cell, Chromatography, Hydrophilic interaction chromatography, Human kidney, General Chemistry, Lipids, Kidney Neoplasms, Chromatographic separation, 030104 developmental biology, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Metabolite profiling, Metabolome, METABOLIC FEATURES, Chromatography, Liquid
Abstract

Metabolite profiling of tissue samples is a promising approach for the characterization of cancer pathways and tumor classification based on metabolic features. Here, we present an analytical method for nontargeted metabolomics of kidney tissue. Capitalizing on different chemical properties of metabolites allowed us to extract a broad range of molecules covering small polar molecules and less polar lipid classes that were analyzed by LC-QTOF-MS after HILIC and RP chromatographic separation, respectively. More than 1000 features could be reproducibly extracted and analyzed (CV30%) in porcine and human kidney tissue, which were used as surrogate matrices for method development. To further assess assay performance, cross-validation of the nontargeted metabolomics platform to a targeted metabolomics approach was carried out. Strikingly, from 102 metabolites that could be detected on both platforms, the majority (90%) revealed Spearman's correlation coefficients ≥0.3, indicating that quantitative results from the nontargeted assay are largely comparable to data derived from classical targeted assays. Finally, as proof of concept, the method was applied to human kidney tissue where a clear differentiation between kidney cancer and nontumorous material could be demonstrated on the basis of unsupervised statistical analysis.

Published
2017

33. Stereoselective quantification of phase 1 and 2 metabolites of clomiphene in human plasma and urine

Author

Svitlana Igel, Thomas E. Mürdter, Reinhold Kerb, Matthias Schwab, Patrick Kröner, and Georg Heinkele

Subjects
Formic acid, Metabolite, 02 engineering and technology, Urine, 01 natural sciences, High-performance liquid chromatography, Clomiphene, Analytical Chemistry, chemistry.chemical_compound, Pharmacokinetics, Biotransformation, Tandem Mass Spectrometry, Humans, Protein precipitation, Chromatography, High Pressure Liquid, Chromatography, 010401 analytical chemistry, Reproducibility of Results, Reference Standards, 021001 nanoscience & nanotechnology, 0104 chemical sciences, chemistry, Female, 0210 nano-technology, Glucuronide, Chromatography, Liquid
Abstract

Clomiphene citrate is first line therapy of female infertility but is also frequently abused by athletes. Human biotransformation of clomiphene results in numerous phase 1 and phase 2 metabolites. The involvement of the polymorphic cytochrome P450 2D6 leads to a high inter-individual variability. To comprehensively investigate clomiphene metabolism in vivo we established a highly sensitive and specific UPLC-MS/MS method for the stereoselective quantification of clomiphene and its phase 1 and phase 2 metabolites in plasma and urine. Reference compounds and stable isotope labelled internal standards were synthesized in-house. High-throughput sample preparation was done by protein precipitation. Analytes were separated by UPLC on a C18 column (1.8 μm, 2.1 * 100 mm) using a gradient of 0.1% formic acid in acetonitrile in 0.1% aqueous formic acid and detected by positive ESI-MS/MS in MRM mode. The lower limit of quantification was below 1 nM for all analytes. The method was validated according to recent guidelines. However, due to absorption effects during sampling the quantification of metabolites in urine was limited to phase 2 metabolites. The method was successfully applied to determine the pharmacokinetic of (E)- and (Z)-clomiphene and 14 metabolites following a single dose of 100 mg clomiphene citrate in 3 healthy subjects and proofed to be an essential tool to comprehensively investigate the human biotransformation of clomiphene.

Published
2021

34. Oncogenic Ras triggers hyperproliferation and impairs polarized colonic morphogenesis by autocrine ErbB3 signaling

Author

Simone Schmid, Christine Sers, Michaela Strotbek, Yvonne Möller, Thomas E. Mürdter, Roland E. Kontermann, Lisa C. Schmitt, Pamela Riemer, Janina Hendrick, Sven Beyes, Markus Morkel, Monilola A. Olayioye, Jens O Schmid, and Matthias Schwab

Subjects
0301 basic medicine, 3D culture, Receptor, ErbB-3, Morphogenesis, Tumor initiation, Biology, Receptor tyrosine kinase, 03 medical and health sciences, oncogenic Ras, Cell Line, Tumor, Humans, ERBB3, Intestinal Mucosa, Autocrine signalling, apical-basolateral polarity, Cell Proliferation, Cell Polarity, Cell Dedifferentiation, Tumor Pathology, Molecular medicine, Autocrine Communication, 030104 developmental biology, Cell Transformation, Neoplastic, Oncology, intestinal organoids, Immunology, Cancer research, biology.protein, ras Proteins, Neuregulin, Colorectal Neoplasms, ErbB3/HER3, Research Paper
Abstract

// Yvonne Moller 1 , Markus Morkel 2 , Jens Schmid 3 , Sven Beyes 1, 8 , Janina Hendrick 1 , Michaela Strotbek 1 , Pamela Riemer 2, 4 , Simone Schmid 1 , Lisa C. Schmitt 1 , Roland Kontermann 1, 5 , Thomas Murdter 3 , Matthias Schwab 3, 6, 7 , Christine Sers 2, 4 , Monilola A. Olayioye 1, 5 1 Institute of Cell Biology and Immunology, University of Stuttgart, Stuttgart, Germany 2 Laboratory of Molecular Tumor Pathology and Systems Biology, Institute of Pathology, Charite Universitatsmedizin Berlin, Berlin, Germany 3 Dr. Margarete Fischer-Bosch Institute of Clinical Pharmacology and University of Tubingen, Stuttgart, Germany 4 DKTK, German Cancer Consortium, Partner site Charite, Berlin, Germany 5 Stuttgart Research Center Systems Biology (SRCSB), University of Stuttgart, Stuttgart, Germany 6 Department of Clinical Pharmacology, University Hospital, Tubingen, Germany 7 Department of Biochemistry and Pharmacy, University of Tubingen, Tubingen, Germany 8 Current address: Institute of Molecular Medicine and Cell Research, Faculty of Biology, Albert-Ludwigs-University, Freiburg, Germany Correspondence to: Monilola A. Olayioye, email: monilola.olayioye@izi.uni-stuttgart.de Keywords: oncogenic Ras, ErbB3/HER3, 3D culture, intestinal organoids, apical-basolateral polarity Received: January 31, 2016 Accepted: July 09, 2016 Published: July 18, 2016 ABSTRACT Here we study the effects of inducible oncogenic K-Ras (G12V) expression on the polarized morphogenesis of colonic epithelial cells. We provide evidence that the autocrine production of heregulins, ligands for the ErbB3 receptor tyrosine kinase, is responsible for the hyperproliferation and aberrant 3D morphogenesis upon oncogenic K-Ras expression. This is in line with results obtained in primary intestinal organoid cultures, in which exogenous heregulin is shown to interfere with normal tissue architecture. Importantly, ErbB3 inhibition and heregulin gene silencing rescued K-Ras G12V -induced features of cell transformation. Together with the increased ErbB3 positivity detected in human high-grade primary colorectal cancers, our findings provide support for an autocrine signaling loop engaged by oncogenic K-Ras involving ErbB3 that contributes to the dedifferentiation of the intestinal epithelium during tumor initiation and progression.

Published
2016

35. Hyperthermia Synergizes with Chemotherapy by Inhibiting PARP1-Dependent DNA Replication Arrest

Author

Lea Schaaf, Thomas E. Mürdter, Walter E. Aulitzky, Christoph Ulmer, Jens O Schmid, Heiko van der Kuip, Georg Sauer, Matthias Schwab, and Simon Heine

Subjects
DNA Replication, 0301 basic medicine, Hyperthermia, Cancer Research, DNA Repair, DNA repair, DNA damage, Poly ADP ribose polymerase, medicine.medical_treatment, Blotting, Western, Poly (ADP-Ribose) Polymerase-1, Fluorescent Antibody Technique, Antineoplastic Agents, Apoptosis, Biology, Real-Time Polymerase Chain Reaction, 03 medical and health sciences, 0302 clinical medicine, PARP1, Tumor Cells, Cultured, medicine, Humans, Doxorubicin, RNA, Messenger, Peritoneal Neoplasms, Cell Proliferation, Ovarian Neoplasms, Cisplatin, Chemotherapy, Antibiotics, Antineoplastic, Reverse Transcriptase Polymerase Chain Reaction, Hyperthermia, Induced, medicine.disease, Combined Modality Therapy, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Colonic Neoplasms, Immunology, Cancer research, Female, DNA Damage, medicine.drug
Abstract

Although hyperthermia offers clinical appeal to sensitize cells to chemotherapy, this approach has been limited in terms of long-term outcome as well as economic and technical burden. Thus, a more detailed knowledge about how hyperthermia exerts its effects on chemotherapy may illuminate ways to improve the approach. Here, we asked whether hyperthermia alters the response to chemotherapy-induced DNA damage and whether this mechanism is involved in its sensitizing effect in BRCA-competent models of ovarian and colon cancer. Notably, we found that hyperthermia delayed the repair of DNA damage caused by cisplatin or doxorubicin, acting upstream of different repair pathways to block histone polyADP-ribosylation (PARylation), a known effect of chemotherapy. Furthermore, hyperthermia blocked this histone modification as efficiently as pharmacologic inhibitors of PARP (PARPi), producing comparable delay in DNA repair, induction of double-strand breaks (DSB), and cell cytotoxicity after chemotherapy. Mechanistic investigations indicated that inhibiting PARylation by either hyperthermia or PARPi induced lethal DSB upon chemotherapy treatment not only by reducing DNA repair but also by preventing replication fork slowing. Overall, our work reveals how PARP blockade, either by hyperthermia or small-molecule inhibition, can increase chemotherapy-induced damage in BRCA-competent cells. Cancer Res; 76(10); 2868–75. ©2016 AACR.

Published
2016

36. Clinical Trial

Author

Zahra, Khalaj, Zohreh, Baratieh, Parvaneh, Nikpour, Matthias, Schwab, Elke, Schaeffeler, Fariborz, Mokarian, Hossein, Khanahmad, Rasoul, Salehi, Thomas E, Mürdter, and Mansoor, Salehi

Subjects
Pharmacology, tamoxifen, CYP2D6, genotype, metabolite, dose, endoxifen, skin and connective tissue diseases, Clinical Trial
Abstract

Introduction: The polymorphic enzyme cytochrome P450 2D6 (CYP2D6) catalyzes a major step in the bioactivation of tamoxifen. Genotyping of clinically relevant CYP2D6 alleles and subsequent dose adjustment is a promising approach to individualize breast cancer therapy. The aim of this study was to investigate the relationship between the plasma levels of tamoxifen and its metabolites and different CYP2D6 genotypes under standard (20 mg/day) and dose-adjusted therapy (Registration ID in Iranian Registry of Clinical Trials: IRCT2015082323734N1). Materials and Methods: Using TaqMan® assays common alleles of CYP2D6 (∗1, ∗2, ∗4, ∗5, ∗6, ∗10, ∗17, and ∗41) and gene duplication were identified in 134 breast cancer patients. Based on CYP2D6 genotypes patients with an activity score 1 (n = 15) and 0–0.5 (n = 2) were treated with tamoxifen adjusted dosage of 30 and 40 mg/day, respectively. The concentration of tamoxifen and its metabolites before and after 4 and 8 months of dose adjustment were measured using LC-MS/MS technology. Results: At baseline, (Z)-endoxifen plasma concentrations (33 ± 15.5, 28.1 ± 14, 26.6 ± 23.4, 14.3 ± 8.6, and 10.7 ± 5.5 nmol/l for EM/EM, EM/IM, EM/PM, IM/IM and PM/PM, respectively) and the metabolic ratio (Z)-Endoxifen/N-desmethyltamoxifen (0.0558 ± 0.02, 0.0396 ± 0.0111, 0.0332 ± 0.0222, 0.0149 ± 0.0026, and 0.0169 ± 0.0177 for EM/EM, EM/IM, EM/PM, IM/IM, and PM/PM, respectively) correlated with CYP2D6 genotype (Kruskal–Wallis p = 0.013 and p < 0.0001, respectively). Dose escalation to 30 and 40 mg/day in patients with a CYP2D6 activity score of 1 (n = 15) and 0–0.5 (n = 2) resulted in a significant increase in (Z)-endoxifen plasma levels (22.17 ± 24.42, 34.43 ± 26.54, and 35.77 ± 28.89 nmol/l at baseline, after 4 and 8 months, respectively, Friedman p = 0.0388) along with the plasma concentrations of tamoxifen and its other metabolites. No severe side effects were recorded during dose escalation. Conclusion: For the first time, we show the feasibility of dose escalation of tamoxifen in breast cancer patients with compromised CYP2D6 activity and Iranian ethnic background to increase the plasma concentrations of (Z)-endoxifen.

Published
2018

37. Is Mistletoe Treatment Beneficial in Invasive Breast Cancer? A New Approach to an Unresolved Problem

Author

Sven Goletz, German Ott, Stefan Winter, Christian Trautmann, Godehard Friedel, Susanne Rössle, Peter Fritz, Andreas Gerteis, Thomas E. Mürdter, Simone Faisst, Matthias Schwab, Jürgen Dippon, Friedhelm Brinkmann, Xenophon Pappas, Hiltrud Brauch, and Simon Müller

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Breast Neoplasms, Disease-Free Survival, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Quality of life, Internal medicine, Recurrence free survival, medicine, Overall survival, Humans, Neoplasm Invasiveness, Stage (cooking), Aged, Retrospective Studies, Toxins, Biological, business.industry, Proportional hazards model, Standard treatment, Retrospective cohort study, General Medicine, Middle Aged, medicine.disease, Ribosome Inactivating Proteins, Type 2, Treatment Outcome, 030104 developmental biology, 030220 oncology & carcinogenesis, Quality of Life, business
Abstract

Background/aim In this retrospective study, we compared breast cancer patients treated with and without mistletoe lectin I (ML-I) in addition to standard breast cancer treatment in order to determine a possible effect of this complementary treatment. Patients and methods This study included 18,528 patients with invasive breast cancer. Data on additional ML-I treatments were reported for 164 patients. We developed a "similar case" method with a distance measure retrieved from the beta variable in Cox regression to compare these patients, after stage adjustment, with their non-ML-1 treated counterparts in order to answer three hypotheses concerning overall survival, recurrence free survival and life quality. Results Raw data analysis of an additional ML-I treatment yielded a worse outcome (p=0.02) for patients with ML treatment, possibly due to a bias inherent in the ML-I-treated patients. Using the "similar case" method (a case-based reasoning approach) we could not confirm this harm for patients using ML-I. Analysis of life quality data did not demonstrate reliable differences between patients treated with ML-I treatment and those without proven ML-I treatment. Conclusion Based on a "similar case" model we did not observe any differences in the overall survival (OS), recurrence-free survival (RFS), and quality of life data between breast cancer patients with standard treatment and those who in addition to standard treatment received ML-I treatment.

Published
2018

38. A Temperature of 40 °C Appears to be a Critical Threshold for Potentiating Cytotoxic Chemotherapy In Vitro and in Peritoneal Carcinomatosis Patients Undergoing HIPEC

Author

Christoph Ulmer, Thomas E. Mürdter, Heiko van der Kuip, Stefan Winter, Marina Münch, Wolfgang Steurer, Waltraud Zopf, Lea Schaaf, Walter E. Aulitzky, and KP Thon

Subjects
Hyperthermia, medicine.medical_specialty, medicine.medical_treatment, Urology, Fluorescent Antibody Technique, Apoptosis, In Vitro Techniques, Immunoenzyme Techniques, Peritoneal cavity, Peritoneal Neoplasm, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, medicine, Humans, Doxorubicin, Peritoneal Neoplasms, Cell Proliferation, Neoplasm Staging, Retrospective Studies, Cisplatin, Chemotherapy, business.industry, Carcinoma, Temperature, Cytoreduction Surgical Procedures, Hyperthermia, Induced, Prognosis, medicine.disease, Combined Modality Therapy, medicine.anatomical_structure, Oncology, Chemotherapy, Adjuvant, Chemotherapy, Cancer, Regional Perfusion, Anesthesia, Peritoneal Cancer Index, Surgery, Hyperthermic intraperitoneal chemotherapy, business, Follow-Up Studies, medicine.drug
Abstract

Hyperthermic intraperitoneal chemotherapy (HIPEC) following cytoreductive surgery is a radical but effective treatment option for patients with peritoneal carcinomatosis (PC). Unfortunately, a standardized HIPEC protocol is missing impeding systematic comparisons with regard to minimal effective temperatures. The purpose of the present study was to systematically analyse the precise minimal temperature needed for potentiation of chemotherapy effects in vitro and for patient survival. We established a cell line-based model to mimic HIPEC conditions used in clinical practice, and evaluated intracellular drug concentrations and long-term survival using different temperatures ranging from 38 to 42 °C combined with cisplatin or doxorubicin. In parallel, we evaluated the temperature reached in the clinical setting by measuring inflow and outflow, as well as in two locations in the peritoneal cavity in 34 patients. Finally, we determined the influence of different HIPEC temperatures on survival. Long-term survival of cells treated with either cisplatin or doxorubicin was further improved only at temperatures above 40 °C. In patients, during HIPEC, constant temperatures were reached after 10 min in the peritoneal cavity. A temperature above 40 °C for at least 40 min was achieved in 68 % of patients over the 60 min duration of HIPEC. Importantly, we observed a significantly enhanced overall survival (OS) and progression-free survival (PFS) in those patients reaching temperatures above 40 °C. Hyperthermia significantly potentiated the chemotherapy effects only at temperatures above 40 °C in vitro. Importantly, this temperature threshold was also critical for OS and PFS of PC patients.

Published
2015

39. Highly sensitive simultaneous quantification of estrogenic tamoxifen metabolites and steroid hormones by LC-MS/MS

Author

Georg Heinkele, Jana C. Precht, Matthias Schwab, Michel Eichelbaum, Hiltrud Brauch, Werner Schroth, Janina Johänning, and Thomas E. Mürdter

Subjects
Antineoplastic Agents, Hormonal, Bisphenol, medicine.drug_class, medicine.medical_treatment, Breast Neoplasms, Estrone, Biochemistry, Analytical Chemistry, Steroid, chemistry.chemical_compound, Limit of Detection, Tandem Mass Spectrometry, medicine, Humans, Androstenedione, Solid phase extraction, Chromatography, Chemistry, Selected reaction monitoring, Postmenopause, Tamoxifen, Estrogen, Female, hormones, hormone substitutes, and hormone antagonists, Chromatography, Liquid, medicine.drug
Abstract

Tamoxifen is a mainstay in the treatment of estrogen receptor-positive breast cancer and is metabolized to more than 30 different compounds. Little is known about in vivo concentrations of estrogenic metabolites E-metabolite E, Z-metabolite E, and bisphenol and their relevance for tamoxifen efficacy. Therefore, we developed a highly sensitive HPLC-ESI-MS/MS quantification method for tamoxifen metabolites bisphenol, E-metabolite E, and Z-metabolite E as well as for the sex steroid hormones estradiol, estrone, testosterone, androstenedione, and progesterone. Plasma samples were subjected to protein precipitation followed by solid phase extraction. Upon derivatization with 3-[(N-succinimide-1-yl)oxycarbonyl]-1-methylpyridinium iodide, all analytes were separated on a sub-2-μm column with a gradient of acetonitrile in water with 0.1 % of formic acid. Analytes were detected on a triple-quadrupole mass spectrometer with positive electrospray ionization in the multiple reaction monitoring mode. Our method demonstrated high sensitivity, accuracy, and precision. The lower limits of quantification were 12, 8, and 25 pM for bisphenol, E-metabolite E, and Z-metabolite E, respectively, and 4 pM for estradiol and estrogen, 50 pM for testosterone and androstenedione, and 25 pM for progesterone. The method was applied to plasma samples of postmenopausal patients taken at baseline and under tamoxifen therapy. Graphical Abstract Sample preparation and derivatization for highly sensitive quantification of estrogenic tamoxifen metabolites and steroid hormones by HPLC-MS/MS.

Published
2015

40. Quantitative bile acid profiling by liquid chromatography quadrupole time-of-flight mass spectrometry: monitoring hepatitis B therapy by a novel Na+-taurocholate cotransporting polypeptide inhibitor

Author

Stephan Urban, Thomas E. Mürdter, Georg Heinkele, Ute Hofmann, Matthias Schwab, A. Alexandrov, Walter E. Haefeli, Mathias Haag, Antje Blank, and Patrick Leuthold

Subjects
Adult, Male, Spectrometry, Mass, Electrospray Ionization, Analyte, medicine.drug_class, Ion suppression in liquid chromatography–mass spectrometry, Mass spectrometry, Sensitivity and Specificity, Biochemistry, Analytical Chemistry, Bile Acids and Salts, chemistry.chemical_compound, medicine, Glycochenodeoxycholic acid, Humans, History, Ancient, Chromatography, Bile acid, Reproducibility of Results, Tauroursodeoxycholic acid, Hepatitis B, medicine.disease, Blood proteins, Hepatitis D, Treatment Outcome, chemistry, Female, Drug Monitoring, Biomarkers
Abstract

A novel analytical approach for the targeted profiling of bile acids (BAs) in human serum/plasma based on liquid chromatography quadrupole time-of-flight mass spectrometry (LC-QTOF-MS) is presented. Reversed-phase chromatography enabled the baseline separation of 15 human BA species which could be readily detected by accurate mass analysis in negative ion mode. Blood proteins were removed by methanol precipitation in the presence of deuterium-labeled internal standards which allowed BA quantification in 50 μl plasma/serum. The assay was validated according to FDA guidance achieving quantification limits from 7.8 to 156 nM. Calibration curves prepared in charcoal-stripped serum/plasma showed excellent regression coefficients (R 2 > 0.997) and covered quantities from 7.8 to 10,000 nM depending on the analyzed species. Intra- and inter-day accuracy and precision were below 15 % for all analytes. Apparent extraction recoveries were above 97 %, and ion suppression rates were between 4 and 53 %. Mean BA level in serum/plasma from healthy volunteers ranged from 11 ± 4 nM (tauroursodeoxycholic acid) to 1321 ± 1442 nM (glycochenodeoxycholic acid). As a proof of concept, the assay was applied to plasma samples derived from a clinical phase I study of myrcludex B, a novel first-in-class virus entry inhibitor for the treatment of chronic hepatitis B and D. The results demonstrate that myrcludex-induced inhibition of the hepatic BA transporter Na+-taurocholate cotransporting polypeptide (NTCP) significantly affects plasma BA level. These observations provide novel insights into drug-induced metabolic responses and will be indispensable for the assessment of side effects and dose-finding processes during future clinical trials.

Published
2015

41. Simulation with cellsin vitroof tamoxifen treatment in premenopausal breast cancer patients with different CYP2D6 genotypes

Author

Puspanjali Bhatta, Thomas E. Mürdter, Russell E. McDaniel, V. Craig Jordan, David A. Flockhart, Philipp Y. Maximov, Daphne J. Fernandes, and Valeriy R. Korostyshevskiy

Subjects
Pharmacology, CYP2D6, Metabolite, Primary metabolite, Prodrug, Secondary metabolite, Biology, medicine.disease, chemistry.chemical_compound, Breast cancer, chemistry, medicine, Adenocarcinoma, skin and connective tissue diseases, Tamoxifen, medicine.drug
Abstract

Background and Purpose Tamoxifen is a prodrug that is metabolically activated by 4-hydroxylation to the potent primary metabolite 4-hydroxytamoxifen (4OHT) or via another primary metabolite N-desmethyltamoxifen (NDMTAM) to a biologically active secondary metabolite endoxifen through a cytochrome P450 2D6 variant system (CYP2D6). To elucidate the mechanism of action of tamoxifen and the importance of endoxifen for its effect, we determined the anti-oestrogenic efficacy of tamoxifen and its metabolites, including endoxifen, at concentrations corresponding to serum levels measured in breast cancer patients with various CYP2D6 genotypes (simulating tamoxifen treatment). Experimental Approach The biological effects of tamoxifen and its metabolites on cell growth and oestrogen-responsive gene modulation were evaluated in a panel of oestrogen receptor-positive breast cancer cell lines. Actual clinical levels of tamoxifen metabolites in breast cancer patients were used in vitro along with actual levels of oestrogens observed in premenopausal patients taking tamoxifen. Key Results Tamoxifen and its primary metabolites (4OHT and NDMTAM) only partially inhibited the stimulant effects of oestrogen on cells. The addition of endoxifen at concentrations corresponding to different CYP2D6 genotypes was found to enhance the anti-oestrogenic effect of tamoxifen and its metabolites with an efficacy that correlated with the concentration of endoxifen; at concentrations corresponding to the extensive metabolizer genotype it further inhibited the actions of oestrogen. In contrast, lower concentrations of endoxifen (intermediate and poor metabolizers) had little or no anti-oestrogenic effects. Conclusions and Implications Endoxifen may be a clinically relevant metabolite in premenopausal patients as it provides additional anti-oestrogenic actions during tamoxifen treatment.

Published
2014

42. A new [2H]-labelledα-trichloroimidate glucuronic ester for the synthesis of deuterated drug conjugates

Author

Thomas E. Mürdter, Reinhold Kerb, Georg Heinkele, Boian Ganchev, Mirjam C. K. Geditz, and Ute Hofmann

Subjects
chemistry.chemical_compound, chemistry, Organic Chemistry, Drug Discovery, Glucuronidation, Organic chemistry, Radiology, Nuclear Medicine and imaging, Deuterated drug, Biochemistry, Quantitative analysis (chemistry), Spectroscopy, Analytical Chemistry, Conjugate
Abstract

A new reaction pathway for the synthesis of a [(2)H]-labelled trichloroacetimidate precursor for the preparation of glucuronides is described. Therewith, stable isotope-labelled drug glucuronides become accessible on a preparative scale, which can further be used as internal standards for quantitative analysis.

Published
2014

43. Bile acid monitoring to support safety and efficacy of Myrcludex B in combination with Tenofovir in patients with chronic HBV/HDV co-infection

Author

Katrin Schöneweis, Matthias Schwab, A. Alexandrov, Thomas E. Mürdter, Ute Hofmann, Mathias Haag, Pavel O. Bogomolov, Stephan Urban, Antje Blank, Georg Heinkele, H. Wedemeyer, and Walter-Emil Haefeli

Subjects
0301 basic medicine, medicine.medical_specialty, Hepatology, Bile acid, Tenofovir, medicine.drug_class, business.industry, Myrcludex B, Gastroenterology, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Internal medicine, medicine, 030211 gastroenterology & hepatology, In patient, business, medicine.drug, Co infection
Published
2018

44. Intraperitoneal Chemotherapy of Peritoneal Carcinomatosis Using Pressurized Aerosol as an Alternative to Liquid Solution: First Evidence for Efficacy

Author

Clemens B. Tempfer, Wiebke Solass, Urs Giger-Pabst, Dirk Strumberg, Reinhold Kerb, Thomas E. Mürdter, Jürgen Zieren, Marc A. Reymond, and Matthias Schwab

Subjects
Adult, Male, medicine.medical_specialty, Treatment outcome, Urology, Peritoneal Neoplasm, Stomach Neoplasms, Surgical oncology, Antineoplastic Combined Chemotherapy Protocols, Pressure, medicine, Humans, Survival rate, Peritoneal Neoplasms, Aged, Neoplasm Staging, Aerosols, Ovarian Neoplasms, Gastrointestinal Oncology, Systemic chemotherapy, business.industry, Intraperitoneal chemotherapy, Middle Aged, Surgery, Peritoneal carcinomatosis, Survival Rate, Treatment Outcome, Appendiceal Neoplasms, Oncology, Female, Neoplasm staging, business, Injections, Intraperitoneal
Abstract

Background Peritoneal carcinomatosis (PC) is an unmet medical need. Despite recent improvements, systemic chemotherapy has limited efficacy. We report the first application of intraperitoneal chemotherapy as a pressurized aerosol in human patients. Methods Three end-stage patients with advanced PC from gastric, appendiceal, and ovarian origin were treated as a compassionate therapy. All patients had received previous systemic chemotherapy. A pressurized aerosol of CO2 loaded with doxorubicin 1.5 mg/m2 and cisplatin 7.5 mg/m2 (pressurized intraperitoneal aerosol chemotherapy, PIPAC) was applied into the abdomen for 30 min at a pressure of 12 mmHg and a temperature of 37 °C. Results No side-effects >2 CTCAE were observed, and the procedures were well tolerated. Early hospital discharge was possible (days 2–5). Nuclear presence of doxorubicin was documented throughout the peritoneum, reaching high local concentration (≤4.1 μmol/g) and plasma concentration was low (4.0–6.2 ng/ml). PIPAC created no significant adhesions, could be repeated, and was applied 6×, 4×, and 2×. Two patients showed a complete and one a partial histological remission. Mean survival after the first PIPAC was 288 days. One patient is alive after 567 days. Conclusions PIPAC shows superior pharmacological properties with high local concentration and low systemic exposure. PIPAC can induce regression of PC in chemoresistant tumors, using 10 % of a usual systemic dose. Electronic supplementary material The online version of this article (doi:10.1245/s10434-013-3213-1) contains supplementary material, which is available to authorized users.

Published
2013

45. The Letrozole Phase 1 Metabolite Carbinol as a Novel Probe Drug for UGT2B7

Author

Kathrin Klein, Matthias Schwab, Evgeny Krynetskiy, Werner Schroth, Thomas E. Mürdter, Jana C. Precht, and Hiltrud Brauch

Subjects
medicine.drug_class, Metabolite, Glucuronidation, Pharmaceutical Science, Pharmacology, chemistry.chemical_compound, In vivo, Nitriles, medicine, Humans, Glucuronosyltransferase, chemistry.chemical_classification, Polymorphism, Genetic, Aromatase inhibitor, Methanol, Triazoles, Recombinant Proteins, In vitro, UGT2B7, Kinetics, Enzyme, Liver, chemistry, Letrozole, Microsomes, Liver, Microsome, Metabolic Detoxication, Phase I
Abstract

Carbinol [4,4'-(hydroxymethylene)dibenzonitrile] is the main phase 1 metabolite of letrozole, a nonsteroidal aromatase inhibitor used for endocrine therapy in postmenopausal breast cancer. We elucidated the contribution of UDP-glucuronosyltransferase (UGT) isoforms on the glucuronidation of carbinol. Identification of UGT isoforms was performed using a panel of recombinant human UGT enzymes. Kinetic studies were done in recombinant human UGT2B7 and pooled human liver microsomes (HLMs). A liquid chromatography-tandem mass spectrometry method was used for detection of metabolites. To assess the impact of UGT2B7*2, we determined the carbinol glucuronidation activity using HLM as well as UGT2B7 protein expression in 148 human livers. Moreover, we analyzed the plasma concentrations of 60 letrozole-treated breast cancer patients. We identified UGT2B7 as the predominant UGT isoform involved in carbinol glucuronidation. In HLMs and recombinant UGT2B7, we determined K(m) values (9.99 and 9.56 µM) and V(max) values (3430 and 2399 pmol/min per milligram of protein), respectively. In the set of 148 human livers, carbinol glucuronidation activity significantly correlated with UGT2B7 protein as determined by Western blotting (r(s) = 0.5088, P < 0.0001). Neither carbinol glucuronidation activity (*1/*1: n = 25, 2434 ± 1018; *1/*2: n = 80, 2356 ± 1372; *2/*2: n = 43, 2251 ± 1421 pmol/min per milligram of protein) nor UGT2B7 protein expression was altered by the UGT2B7*2 genotype. No impact of UGT2B7*2 on plasma levels of carbinol and carbinol-gluc [bis(4-cyanophenyl)methyl hexopyranosiduronic acid] in 60 letrozole-treated patients was found. Taken together, these findings suggest carbinol as a novel in vitro probe substrate for UGT2B7. In vitro and in vivo data suggest a lack of influence of the UGT2B7*2 polymorphism on carbinol glucuronidation.

Published
2013

46. Tamoxifen Use in Postmenopausal Breast Cancer: CYP2D6 Matters

Author

Stefan Winter, Thomas E. Mürdter, James N. Ingle, Hiltrud Brauch, Werner Schroth, Matthew P. Goetz, Matthias Schwab, and Michel Eichelbaum

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Antineoplastic Agents, Hormonal, Breast Neoplasms, digestive system, Loss of heterozygosity, Breast cancer, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Genotype, medicine, Humans, skin and connective tissue diseases, Genotyping, Gynecology, Polymorphism, Genetic, business.industry, Saponins, medicine.disease, Genotype frequency, Postmenopause, Comments and Controversies, Cardenolides, Tamoxifen, Cytochrome P-450 CYP2D6, Allelic Imbalance, Female, business, Pharmacogenetics, medicine.drug
Abstract

The question of whether genetic polymorphisms of CYP2D6 can affect treatment outcome in patients with early postmenopausal breast cancer has been a matter of debate. With the recent negative results with regard to CYP2D6 genotyping from the Breast International Group (BIG) 1-98 and Arimidex, Tamoxifen, Alone or in Combination (ATAC) studies, the study investigators suggest that testing for CYP2D6 has no value in clinical practice.1,2 The authors of the accompanying editorial conclude that this matter can be likely laid to rest.3 However, pharmacogenetic experts demanded the retraction of the BIG 1-98 CYP2D6 study4 on the basis of massive departures from Hardy-Weinberg equilibrium (HWE; Table 1), possibly because of the bias that may result when the CYP2D6 genotype is obtained from the tumor (somatic) genome and not the host genome (germline DNA). Various authors in their letters attribute the highly distorted genotype frequencies to allelic imbalance associated with loss of heterozygosity (LOH) in breast tumor tissue,4,5 deviation from the standard genotyping assay protocol,5 or the presence of pseudogenes neighboring the CYP2D6 locus.6 Because the BIG 1-98 and ATAC pharmacogenetic studies may be considered sufficient to settle the issue of the value of CYP2D6 in decision making regarding endocrine therapy in postmenopausal women with breast cancer, we revisit the hypothesis, comment on the complementary evidence, and discuss pros and cons of the validity of CYP2D6 tamoxifen pharmacogenetics.

Published
2013

47. Cancer Cells Cue the p53 Response of Cancer-Associated Fibroblasts to Cisplatin

Author

Jens O Schmid, Walter E. Aulitzky, Silke Haubeiss, Heiko van der Kuip, Sabine Bode, German Ott, Moshe Oren, Godehard Friedel, Meng Dong, Thomas E. Mürdter, and Andreas Grabner

Subjects
Cancer Research, Cell type, Lung Neoplasms, Cell, Antineoplastic Agents, Biology, Tissue culture, Tumor Microenvironment, medicine, Humans, Lung cancer, Cisplatin, Tumor microenvironment, Fibroblasts, medicine.disease, Immunohistochemistry, Ki-67 Antigen, medicine.anatomical_structure, Oncology, Cancer cell, Cancer research, Cancer-Associated Fibroblasts, Tumor Suppressor Protein p53, DNA Damage, medicine.drug
Abstract

Current understanding of the p53 response is based mainly upon in vitro studies of homogeneous cell populations. However, there is little information on whether the same principles operate within heterogeneous tumor tissues that are comprised of cancer cells and other cell types, including cancer-associated fibroblasts (CAF). Using ex-vivo tissue cultures, we investigated p53 status and responses to cisplatin in tumor cells and CAFs from tissue specimens isolated from 32 lung cancer patients. By comparing cultivated tissue slices with the corresponding tumor tissues fixed immediately after surgery, we found that morphology, proliferation, and p53 staining pattern were preserved during cultivation. Unexpectedly, when CAFs were analyzed, p53 accumulation and induction of p21 was observed only in tumors with constitutively low p53 protein and accumulation upon cisplatin treatment. In contrast, in tumors with no p53 accumulation in cancer cells there was also no p53 accumulation or p21 induction in adjacent CAFs. Furthermore, induction of cisplatin-induced apoptosis in CAFs was selectively observed in tumors characterized by a parallel induction of cancer cell death. Our findings reveal an interdependence of the p53 response in cancer cells and adjacent CAFs within tumor tissues, arguing that cancer cells control the response of their microenvironment to DNA damage. Cancer Res; 72(22); 5824–32. ©2012 AACR.

Published
2012

48. Pulmonary delivery and tissue distribution of aerosolized antisense 2′-O-Methyl RNA containing nanoplexes in the isolated perfused and ventilated rat lung

Author

Matthias Schwab, Claudia Philippi, Ulrich F. Schaefer, Meng Dong, Claus-Michael Lehr, Thomas E. Mürdter, Brigitta Loretz, and Susanne Ammon-Treiber

Subjects
Male, Genetic enhancement, Pharmaceutical Science, Context (language use), Treatment of lung cancer, Pharmacology, Polylactic Acid-Polyglycolic Acid Copolymer, medicine, Animals, RNA, Antisense, Tissue Distribution, Lactic Acid, Rats, Wistar, Lung, Aerosols, Chitosan, Inhalation, business.industry, General Medicine, respiratory system, Rats, medicine.anatomical_structure, Tolerability, Drug delivery, Nanoparticles, Respiratory epithelium, business, Polyglycolic Acid, Biotechnology
Abstract

Pulmonary delivery of drugs, particularly in the treatment of lung cancer, is an attractive strategy for future targeted therapy. In this context, inhalation of nanoplexes might offer a new mode for drug delivery in gene therapy. However, limited data are currently available demonstrating pulmonary delivery, cellular uptake as well as local tolerability in lung tissue. The aim of this study was to elucidate the pulmonary delivery, tissue distribution and local tolerability of aerosolized chitosan-coated poly(lactide-co-glycolide) based nanoplexes containing antisense 2'-O-Methyl RNA (OMR). Therefore, an aerosol of OMR-nanoplexes or OMR alone was administered intra-tracheally using the model of the isolated perfused and ventilated rat lung. Localization of OMR in rat lung tissue was examined by immunohistochemistry. Administration of the OMR-nanoplex formulation resulted in significantly higher cellular OMR uptake of the respiratory epithelium in contrast to the administration of OMR alone, indicating that drug administration via aerosolized nanoplexes is able to target lung tissue. No prominent changes in lung physiology parameters were observed following inhalation, suggesting good local tolerability of OMR-nanoplex formulation.

Published
2012

49. Determination of content uniformity of busulfan capsules by liquid chromatography–mass spectrometry

Author

Thomas E. Mürdter, Matthias Schwab, Dorothea U Schulze, and Siegfried Klumpp

Subjects
Transplantation, medicine.medical_specialty, Chromatography, Liquid chromatography–mass spectrometry, business.industry, medicine, Plasma levels, General Pharmacology, Toxicology and Pharmaceutics, business, Busulfan, medicine.drug, Surgery
Abstract

Study objectives Oral high dose busulfan (1,4-butanediol dimethanesulfonate) is frequently used in conditioning regimens prior to haematopoietic stem cell transplantation. As tablets with high dose busulfan are not commercially available, it is common practice to extemporaneously prepare capsules in hospital pharmacies. However, proper content uniformity assays are lacking. Methods An HPLC–mass spectrometry (MS) method that was previously validated for quantification of plasma levels of busulfan was adapted for determination of the content uniformity of capsules comprising 50 mg of busulfan for high dose regimens. Results Intraday and interday variability and imprecision were less than 2.2%. Conclusions The data indicate high specificity and sensitivity of this novel assay.

Published
2012

50. TKTL-1 expression in lung cancer

Author

German Ott, Johannes F. Coy, Godehard Friedel, Thomas E. Mürdter, Peter Fritz, and Mark Dominik Alscher

Subjects
Adult, Male, medicine.medical_specialty, Lung Neoplasms, Glucose uptake, Biology, medicine.disease_cause, Pathology and Forensic Medicine, Malignant transformation, Carcinoma, Non-Small-Cell Lung, Germany, Internal medicine, Biomarkers, Tumor, medicine, Carcinoma, Humans, Lung cancer, Lung, Survival rate, Aged, Neoplasm Staging, Aged, 80 and over, Cell Biology, Middle Aged, medicine.disease, Immunohistochemistry, Small Cell Lung Carcinoma, Warburg effect, Survival Rate, Endocrinology, Anaerobic glycolysis, Cancer research, Female, Transketolase, Carcinogenesis
Abstract

Study of the physiological changes associated with the development of malignancy demonstrates a metabolic signature for the different stages of tumorigenesis. Increased glucose uptake and lactate production have been detected during malignant transformation. Based on energy production, malignancies can be divided into two subclasses: (a) tumor cells which use the mitochondrial machinery for ATP synthesis, and (b) tumor cells which generate ATP by glucose fermentation and lactate production even in the presence of oxygen (aerobic glycolysis). Recently, transketolase-like protein 1 (TKTL1) gene expression has been shown to contribute to carcinogenesis through increased aerobic glycolysis and hypoxia-inducible factor alpha stabilization. In the present study, 197 patients suffering from lung cancer were investigated by immunohistochemistry for the presence of TKTL1 protein expression. We detected: (1) moderate to strong TKTL1 expression (immune reactive score>100) in 39.1% of the investigated lung cancer patients; (2) a complete lack of TKTL1 by immunohistochemistry in 12.7% of lung cancer cases, with small cell lung cancer (SCLC) being most frequent in this subgroup; (3) no correlation of TKTL1 with overall survival, disease-free survival, any of the established variables of the TNM system, grading, stage, smoking status, or gender. Based on this data, we conclude that TKTL1 could be a target protein for improved therapeutic strategies in some cases of lung cancer.

Published
2012

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