Your search keyword '"Thomas Walle"' showing total 230 results

1. PD-L1 as a Urine Biomarker in Renal Cell Carcinoma—A Case Series and Proof-of-Concept Study

Author

Philipp Reimold, Georgi Tosev, Adam Kaczorowski, Jana Friedhoff, Constantin Schwab, Viktoria Schütz, Magdalena Görtz, Niklas Panzer, Martina Heller, Cem Aksoy, Ruth Himmelsbach, Thomas Walle, Stefanie Zschäbitz, Dirk Jäger, Anette Duensing, Albrecht Stenzinger, Markus Hohenfellner, and Stefan Duensing

Subjects

RCC, PD-L1, urine, biomarker, immunotherapy, Medicine (General), R5-920

Abstract

Background: Renal cell carcinoma (RCC) is among the most lethal urologic malignancies once metastatic. Current treatment approaches for metastatic RCC (mRCC) involve immune checkpoint inhibitors (ICIs) that target the PD-L1/PD-1 axis. High PD-L1 expression in tumor tissue has been identified as a negative prognostic factor in RCC. However, the role of PD-L1 as a liquid biomarker has not yet been fully explored. Herein, we analyze urine levels of PD-L1 in mRCC patients before and after either ICI therapy or surgical intervention, as well as in a series of patients with treatment-naïve RCC. Patients and Methods: The mid-stream urine of patients with mRCC (n = 4) or treatment-naïve RCC, i.e., prior to surgery from two centers (cohort I, n = 49: cohort II, n = 29) was analyzed for PD-L1 by ELISA. The results from cohort I were compared to a control group consisting of patients treated for non-malignant urologic diseases (n = 31). In the mRCC group, urine PD-L1 levels were measured before and after tumor nephrectomy (n = 1) or before and after ICI therapy (n = 3). Exosomal PD-L1 in the urine was analyzed in selected patients by immunoblotting. Results: A strong decrease in urine PD-L1 levels was found after tumor nephrectomy or following systemic treatment with ICIs. In patients with treatment-naïve RCC (cohort I), urine PD-L1 levels were significantly elevated in the RCC group in comparison to the control group (median 59 pg/mL vs. 25.7 pg/mL, p = 0.011). PD-L1 urine levels were found to be elevated, in particular, in low-grade RCCs in cohorts I and II. Exosomal PD-L1 was detected in the urine of a subset of patients. Conclusion: In this proof-of-concept study, we show that PD-L1 can be detected in the urine of RCC patients. Urine PD-L1 levels were found to correlate with the treatment response in mRCC patients and were significantly elevated in treatment-naïve RCC patients.

Published

2024

2. eHealth intervention to manage symptoms for patients with cancer on immunotherapy (SOFIA): a study protocol for a randomised controlled external pilot trial

Author

Dirk Jäger, Hans-Christoph Friederich, Georg Martin Haag, Thomas Walle, Stefanie Zschäbitz, Jürgen Krauß, Imad Maatouk, Christina Sauer, Simeon Sauer, and Senta Kiermeier

Subjects

Medicine

Abstract

Introduction Immune checkpoint therapy (ICT) is associated with a distinct pattern of immune-related adverse events (irAEs) caused by inadvertently redirecting immune responses to healthy tissues. IrAEs can occur at any time; however, in most cases, they arise during the first 14 weeks of the beginning of immune checkpoint blockade. In many cases, immunotherapy must be discontinued due to irAEs. Early detection of irAEs triggers the temporary withholding of ICT or initiation of short-term immunosuppressive treatment, is crucial in preventing further aggravation of irAEs and enables safe re-exposure to ICT. This prospective study aims to evaluate the feasibility of an eHealth intervention for patients under immunotherapy (managing symptoms of immunotherapy, SOFIA). The SOFIA-App consists of two components: SOFIA-Monitoring, a tool to rate patient-reported outcomes (PROs) including irAEs, and SOFIA-Coaching, which provides important information about cancer-specific and immunotherapy-specific topics and the counselling services of the National Centre for Tumour Diseases (NCT) Heidelberg.Methods and analysis We outlined a patient-level two-arm randomised controlled pilot trial of the intervention (SOFIA) versus no-SOFIA for patients with cancer beginning an immunotherapy, aged ≥18 years, recruited from the NCT, Heidelberg. Feasibility outcomes include: recruitment rate; drop-out rate; reasons for refusal and drop-out; willingness to be randomised, utilisation rate of SOFIA-Monitoring and utilisation time of SOFIA-Coaching, physicians utilisation rate of the PROs; feasibility of the proposed outcome measures and optimal sample size estimation. The clinical outcomes are measures of quality of life, psychosocial symptoms, self-efficacy, physician-patient communication and medical process data, which are assessed at the beginning of the intervention, postintervention and at 6-month follow-up.Ethics and dissemination This trial protocol was approved by the Ethical Committee of Heidelberg University, Germany (Reference, S-581/2018).Trial registration number We registered the study in the German Clinical Trial Register (Reference: DRKS00021064). Findings will be disseminated broadly via peer-reviewed empirical journals, articles and conference presentations.

Published

2021

3. Community-driven development of a modified progression-free survival ratio for precision oncology

Author

Sebastian Schölch, Benedikt Brors, Albrecht Stenzinger, Ursula Ehmer, Ulrich-Frank Pape, Christoph Springfeld, Dirk Jäger, Felix J Hüttner, Andreas Mock, Christoph E Heilig, Simon Kreutzfeldt, Daniel Huebschmann, Christoph Heining, Evelin Schröck, Richard Schlenk, Hanno Glimm, Stefan Fröhling, Peter Horak, Leonidas Apostolidis, Marinela Augustin, Daniela Aust, Irfan Ahmed Bhatti, Johannes Bloehdorn, Cornelia Brendel, Christian Britschgi, Jan Braess, Stefan Burdach, Elena Busch, Jozefina Casuscelli, Alexander Desuki, Thomas Deutsch, Mareike Dietrich, Thomas J Ettrich, Johanna Falkenhorst, Tanja Fehm, Anne Flörcken, Andrea Forschner, Stefan Fuxius, Maria Gonzales-Carmona, Frank Griesinger, Sabine Grill, Stefan Gröschel, Georg Martin Haag, Ulrich Haag, Niels Halama, Holger Hebart, Nina Heidger, Barbara Hermes, Georg Hess, Simone Hettmer, Manuela Hoechstetter, Martin Hoffmann, Anna L Illert, Maximilian Jenzer, Bernd Kasper, Stefan Kasper-Virchow, Thomas Kindler, Ewa Koscielniak, Jan Krönke, Michael Kühn, Volker Kunzmann, Alois Lang, Jonas Leichsenring, Elisabeth Livingstone, Lucia Liotta, Kim Luley, Elisabeth Mack, Uwe M Martens, Klaus Metzeler, Jan Moritz Middeke, Lino Möhrmann, Roopa Jayarama-Naidu, Lukas Perkhofer, Arne Pfeufer, Constantin Pixberg, Michael Quante, Bernhard Rendenbach, Damian Rieke, Christian Rothermundt, Andre Norbert Sagerer, Martin Salzmann, Dieter Saur, Bastian Schilling, Jan Schleicher, Anke Schlenska-Lange, Thomas Schmidt, Sophia Schmitz, Rajiv Shah, Khalid Shoumariyeh, Alexander Siebenhüner, Martin Singh, Jens Siveke, Helen Starke, Sophia Strobel, Veronica Teleanu, Niklas Thon, Sebastian Wagner, Thomas Walle, Benedikt Westphalen, Bettina Whitlock, Eva Winkler, Naita Maren Wirsik, Lena Woydack, Angelika Zabel-du Bois, and Stefanie Zschäbitz

Subjects

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

Abstract

Objective Measuring the success of molecularly guided therapies is a major challenge in precision oncology trials. A commonly used endpoint is an intra-patient progression-free survival (PFS) ratio, defined as the PFS interval associated with molecularly guided therapy (PFS2) divided by the PFS interval associated with the last prior systemic therapy (PFS1), above 1.3 or, in some studies, above 1.33 or 1.5.Methods To investigate if the concept of PFS ratios is in agreement with actual response evaluations by physicians, we conducted a survey among members of the MASTER (Molecularly Aided Stratification for Tumor Eradication Research) Programme of the German Cancer Consortium who were asked to classify the success of molecularly guided therapies in 194 patients enrolled in the MOSCATO 01 trial based on PFS1 and PFS2 times.Results A comparison of classification profiles revealed three distinct clusters of PFS benefit assessments. Only 29% of assessments were consistent with a PFS ratio threshold of 1.3, whereas the remaining 71% of participants applied a different classification scheme that did not rely on the relation between PFS times alone, but also took into account absolute PFS1 intervals. Based on these community-driven insights, we developed a modified PFS ratio that incorporates the influence of absolute PFS1 intervals on the judgement of clinical benefit by physicians. Application of the modified PFS ratio to outcome data from two recent precision oncology trials, MOSCATO 01 and WINTHER, revealed significantly improved concordance with physician-perceived clinical benefit and identified comparable proportions of patients who benefited from molecularly guided therapies.Conclusions The modified PFS ratio may represent a meaningful clinical endpoint that could aid in the design and interpretation of future precision oncology trials.

Published

2019

4. Radiation effects on antitumor immune responses: current perspectives and challenges

Author

Thomas Walle, Rafael Martinez Monge, Adelheid Cerwenka, Daniel Ajona, Ignacio Melero, and Fernando Lecanda

Subjects

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

Abstract

Radiotherapy (RT) is currently used in more than 50% of cancer patients during the course of their disease in the curative, adjuvant or palliative setting. RT achieves good local control of tumor growth, conferring DNA damage and impacting tumor vasculature and the immune system. Formerly regarded as a merely immunosuppressive treatment, pre- and clinical observations indicate that the therapeutic effect of RT is partially immune mediated. In some instances, RT synergizes with immunotherapy (IT), through different mechanisms promoting an effective antitumor immune response. Cell death induced by RT is thought to be immunogenic and results in modulation of lymphocyte effector function in the tumor microenvironment promoting local control. Moreover, a systemic immune response can be elicited or modulated to exert effects outside the irradiation field (so called abscopal effects). In this review, we discuss the body of evidence related to RT and its immunogenic potential for the future design of novel combination therapies.

Published

2018

5. Leder

Author

Elisabeth S. Koren, Birgitte Sauge, Thomas Walle, and Marie-Theres Fojuth

Subjects

Museums. Collectors and collecting, AM1-501

Published

2018

6. What is new for an old molecule? Systematic review and recommendations on the use of resveratrol.

Author

Ole Vang, Nihal Ahmad, Clifton A Baile, Joseph A Baur, Karen Brown, Anna Csiszar, Dipak K Das, Dominique Delmas, Carmem Gottfried, Hung-Yun Lin, Qing-Yong Ma, Partha Mukhopadhyay, Namasivayam Nalini, John M Pezzuto, Tristan Richard, Yogeshwer Shukla, Young-Joon Surh, Thomas Szekeres, Tomasz Szkudelski, Thomas Walle, and Joseph M Wu

Subjects

Medicine, Science

Abstract

BackgroundResveratrol is a natural compound suggested to have beneficial health effects. However, people are consuming resveratrol for this reason without having the adequate scientific evidence for its effects in humans. Therefore, scientific valid recommendations concerning the human intake of resveratrol based on available published scientific data are necessary. Such recommendations were formulated after the Resveratrol 2010 conference, held in September 2010 in Helsingør, Denmark.MethodologyLiterature search in databases as PUBMED and ISI Web of Science in combination with manual search was used to answer the following five questions: (1)Can resveratrol be recommended in the prevention or treatment of human diseases?; (2)Are there observed "side effects" caused by the intake of resveratrol in humans?; (3)What is the relevant dose of resveratrol?; (4)What valid data are available regarding an effect in various species of experimental animals?; (5)Which relevant (overall) mechanisms of action of resveratrol have been documented?Conclusions/significanceThe overall conclusion is that the published evidence is not sufficiently strong to justify a recommendation for the administration of resveratrol to humans, beyond the dose which can be obtained from dietary sources. On the other hand, animal data are promising in prevention of various cancer types, coronary heart diseases and diabetes which strongly indicate the need for human clinical trials. Finally, we suggest directions for future research in resveratrol regarding its mechanism of action and its safety and toxicology in human subjects.

Published

2011

7. Epigenetic plasticity cooperates with cell-cell interactions to direct pancreatic tumorigenesis

Author

Cassandra Burdziak, Direna Alonso-Curbelo, Thomas Walle, José Reyes, Francisco M. Barriga, Doron Haviv, Yubin Xie, Zhen Zhao, Chujun Julia Zhao, Hsuan-An Chen, Ojasvi Chaudhary, Ignas Masilionis, Zi-Ning Choo, Vianne Gao, Wei Luan, Alexandra Wuest, Yu-Jui Ho, Yuhong Wei, Daniela F. Quail, Richard Koche, Linas Mazutis, Ronan Chaligné, Tal Nawy, Scott W. Lowe, and Dana Pe’er

Subjects

Multidisciplinary

Abstract

The response to tumor-initiating inflammatory and genetic insults can vary among morphologically indistinguishable cells, suggesting as yet uncharacterized roles for epigenetic plasticity during early neoplasia. To investigate the origins and impact of such plasticity, we performed single-cell analyses on normal, inflamed, premalignant, and malignant tissues in autochthonous models of pancreatic cancer. We reproducibly identified heterogeneous cell states that are primed for diverse, late-emerging neoplastic fates and linked these to chromatin remodeling at cell-cell communication loci. Using an inference approach, we revealed signaling gene modules and tissue-level cross-talk, including a neoplasia-driving feedback loop between discrete epithelial and immune cell populations that was functionally validated in mice. Our results uncover a neoplasia-specific tissue-remodeling program that may be exploited for pancreatic cancer interception.

Published

2023

8. Tumor ENPP1 (CD203a)/Haptoglobin Axis Exploits Myeloid-Derived Suppressor Cells to Promote Post-Radiotherapy Local Recurrence in Breast Cancer

Author

Borja Ruiz-Fernández de Córdoba, Haritz Moreno, Karmele Valencia, Naiara Perurena, Pablo Ruedas, Thomas Walle, Alberto Pezonaga-Torres, Juan Hinojosa, Elisabet Guruceaga, Antonio Pineda-Lucena, Marta Abengózar-Muela, Denis Cochonneau, Carolina Zandueta, Susana Martínez-Canarias, Álvaro Teijeira, Daniel Ajona, Sergio Ortiz-Espinosa, Xabier Morales, Carlos Ortiz de Solórzano, Marta Santisteban, Luis I. Ramos-García, Laura Guembe, Vratislav Strnad, Dominique Heymann, Sandra Hervás-Stubbs, Rubén Pío, María E. Rodríguez-Ruiz, Carlos E. de Andrea, Silvestre Vicent, Ignacio Melero, Fernando Lecanda, and Rafael Martínez-Monge

Subjects

Haptoglobins, Oncology, Phosphoric Diester Hydrolases, Myeloid-Derived Suppressor Cells, Humans, Breast Neoplasms, Female, Neoplasm Recurrence, Local, Pyrophosphatases, Article

Abstract

Abstract Locoregional failure (LRF) in patients with breast cancer post-surgery and post-irradiation is linked to a dismal prognosis. In a refined new model, we identified ectonucleotide pyrophosphatase/phosphodiesterase 1/CD203a (ENPP1) to be closely associated with LRF. ENPP1hi circulating tumor cells (CTC) contribute to relapse by a self-seeding mechanism. This process requires the infiltration of polymorphonuclear myeloid-derived suppressor cells and neutrophil extracellular trap (NET) formation. Genetic and pharmacologic ENPP1 inhibition or NET blockade extends relapse-free survival. Furthermore, in combination with fractionated irradiation, ENPP1 abrogation obliterates LRF. Mechanistically, ENPP1-generated adenosinergic metabolites enhance haptoglobin (HP) expression. This inflammatory mediator elicits myeloid invasiveness and promotes NET formation. Accordingly, a significant increase in ENPP1 and NET formation is detected in relapsed human breast cancer tumors. Moreover, high ENPP1 or HP levels are associated with poor prognosis. These findings unveil the ENPP1/HP axis as an unanticipated mechanism exploited by tumor cells linking inflammation to immune remodeling favoring local relapse. Significance: CTC exploit the ENPP1/HP axis to promote local recurrence post-surgery and post-irradiation by subduing myeloid suppressor cells in breast tumors. Blocking this axis impairs tumor engraftment, impedes immunosuppression, and obliterates NET formation, unveiling new opportunities for therapeutic intervention to eradicate local relapse and ameliorate patient survival. This article is highlighted in the In This Issue feature, p. 1171

Published

2022

9. Data from Tumor ENPP1 (CD203a)/Haptoglobin Axis Exploits Myeloid-Derived Suppressor Cells to Promote Post-Radiotherapy Local Recurrence in Breast Cancer

Author

Rafael Martínez-Monge, Fernando Lecanda, Ignacio Melero, Silvestre Vicent, Carlos E. de Andrea, María E. Rodríguez-Ruiz, Rubén Pío, Sandra Hervás-Stubbs, Dominique Heymann, Vratislav Strnad, Laura Guembe, Luis I. Ramos-García, Marta Santisteban, Carlos Ortiz de Solórzano, Xabier Morales, Sergio Ortiz-Espinosa, Daniel Ajona, Álvaro Teijeira, Susana Martínez-Canarias, Carolina Zandueta, Denis Cochonneau, Marta Abengózar-Muela, Antonio Pineda-Lucena, Elisabet Guruceaga, Juan Hinojosa, Alberto Pezonaga-Torres, Thomas Walle, Pablo Ruedas, Naiara Perurena, Karmele Valencia, Haritz Moreno, and Borja Ruiz-Fernández de Córdoba

Abstract

Locoregional failure (LRF) in patients with breast cancer post-surgery and post-irradiation is linked to a dismal prognosis. In a refined new model, we identified ectonucleotide pyrophosphatase/phosphodiesterase 1/CD203a (ENPP1) to be closely associated with LRF. ENPP1hi circulating tumor cells (CTC) contribute to relapse by a self-seeding mechanism. This process requires the infiltration of polymorphonuclear myeloid-derived suppressor cells and neutrophil extracellular trap (NET) formation. Genetic and pharmacologic ENPP1 inhibition or NET blockade extends relapse-free survival. Furthermore, in combination with fractionated irradiation, ENPP1 abrogation obliterates LRF. Mechanistically, ENPP1-generated adenosinergic metabolites enhance haptoglobin (HP) expression. This inflammatory mediator elicits myeloid invasiveness and promotes NET formation. Accordingly, a significant increase in ENPP1 and NET formation is detected in relapsed human breast cancer tumors. Moreover, high ENPP1 or HP levels are associated with poor prognosis. These findings unveil the ENPP1/HP axis as an unanticipated mechanism exploited by tumor cells linking inflammation to immune remodeling favoring local relapse.Significance:CTC exploit the ENPP1/HP axis to promote local recurrence post-surgery and post-irradiation by subduing myeloid suppressor cells in breast tumors. Blocking this axis impairs tumor engraftment, impedes immunosuppression, and obliterates NET formation, unveiling new opportunities for therapeutic intervention to eradicate local relapse and ameliorate patient survival.This article is highlighted in the In This Issue feature, p. 1171

Published

2023

10. Supplementary Data from Tumor ENPP1 (CD203a)/Haptoglobin Axis Exploits Myeloid-Derived Suppressor Cells to Promote Post-Radiotherapy Local Recurrence in Breast Cancer

Author

Rafael Martínez-Monge, Fernando Lecanda, Ignacio Melero, Silvestre Vicent, Carlos E. de Andrea, María E. Rodríguez-Ruiz, Rubén Pío, Sandra Hervás-Stubbs, Dominique Heymann, Vratislav Strnad, Laura Guembe, Luis I. Ramos-García, Marta Santisteban, Carlos Ortiz de Solórzano, Xabier Morales, Sergio Ortiz-Espinosa, Daniel Ajona, Álvaro Teijeira, Susana Martínez-Canarias, Carolina Zandueta, Denis Cochonneau, Marta Abengózar-Muela, Antonio Pineda-Lucena, Elisabet Guruceaga, Juan Hinojosa, Alberto Pezonaga-Torres, Thomas Walle, Pablo Ruedas, Naiara Perurena, Karmele Valencia, Haritz Moreno, and Borja Ruiz-Fernández de Córdoba

Abstract

Supplementary Data from Tumor ENPP1 (CD203a)/Haptoglobin Axis Exploits Myeloid-Derived Suppressor Cells to Promote Post-Radiotherapy Local Recurrence in Breast Cancer

Published

2023

11. Supplementary Figure from Tumor ENPP1 (CD203a)/Haptoglobin Axis Exploits Myeloid-Derived Suppressor Cells to Promote Post-Radiotherapy Local Recurrence in Breast Cancer

Author

Rafael Martínez-Monge, Fernando Lecanda, Ignacio Melero, Silvestre Vicent, Carlos E. de Andrea, María E. Rodríguez-Ruiz, Rubén Pío, Sandra Hervás-Stubbs, Dominique Heymann, Vratislav Strnad, Laura Guembe, Luis I. Ramos-García, Marta Santisteban, Carlos Ortiz de Solórzano, Xabier Morales, Sergio Ortiz-Espinosa, Daniel Ajona, Álvaro Teijeira, Susana Martínez-Canarias, Carolina Zandueta, Denis Cochonneau, Marta Abengózar-Muela, Antonio Pineda-Lucena, Elisabet Guruceaga, Juan Hinojosa, Alberto Pezonaga-Torres, Thomas Walle, Pablo Ruedas, Naiara Perurena, Karmele Valencia, Haritz Moreno, and Borja Ruiz-Fernández de Córdoba

Abstract

Supplementary Figure from Tumor ENPP1 (CD203a)/Haptoglobin Axis Exploits Myeloid-Derived Suppressor Cells to Promote Post-Radiotherapy Local Recurrence in Breast Cancer

Published

2023

12. Supervised discovery of interpretable gene programs from single-cell data

Author

Russell Z. Kunes, Thomas Walle, Tal Nawy, and Dana Pe’er

Abstract

Factor analysis can drive biological discovery by decomposing single-cell gene expression data into a minimal set of gene programs that correspond to processes executed by cells in a sample. However, matrix factorization methods are prone to technical artifacts and poor factor interpretability. We have developed Spectra, an algorithm that identifies user-provided gene programs, modifies them to dataset context as needed, and detects novel programs that together best explain expression covariation. Spectra overcomes the dominance of cell-type signals by modeling cell-type-specific programs, and can characterize interpretable cell states along a continuum. We show that it outperforms existing approaches in challenging tumor immune contexts; Spectra finds factors that change under immune checkpoint therapy, disentangles the highly correlated features of CD8+T-cell tumor reactivity and exhaustion, finds a novel program that explains continuous macrophage state changes under therapy, and identifies cell-type-specific immune metabolic programs.

Published

2022

13. A simple approach for detecting HLA-A*02 alleles in archival formalin-fixed paraffin-embedded tissue samples and an application example for studying cancer immunoediting

Author

Johannes Witt, Saskia Haupt, Aysel Ahadova, Lena Bohaumilitzky, Vera Fuchs, Alexej Ballhausen, Moritz Jakob Przybilla, Michael Jendrusch, Toni T. Seppälä, Daniel Fürst, Thomas Walle, Elena Busch, Georg Martin Haag, Robert Hüneburg, Jacob Nattermann, Magnus von Knebel Doeberitz, Vincent Heuveline, Matthias Kloor, Tampere University, Clinical Medicine, Department of Gastroenterology, ATG - Applied Tumor Genomics, HUS Abdominal Center, and II kirurgian klinikka

Subjects

Cancer immunoediting, PROGNOSIS, HLA-A Antigens, MICROSATELLITE INSTABILITY, MUTATIONS, Immunology, 3122 Cancers, BIOLOGY, DNA, FREQUENCY, OVARIAN, 3121 Internal medicine, COLORECTAL-CANCER, HLA, formalin-fixed paraffin-embedded tissue samples, HLA typing, Neoplasms, Genetics, Immunology and Allergy, 1182 Biochemistry, cell and molecular biology, Humans, 3111 Biomedicine, Alleles, MSI cancer

Abstract

The HLA system represents a central component of the antigen presentation machinery. As every patient possesses a defined set of HLA molecules, only certain antigens can be presented on the cell surface. Thus, studying HLA type-dependent antigen presentation can improve the understanding of variation in susceptibility to various diseases, including infectious diseases and cancer. In archival formalin-fixed paraffin-embedded (FFPE) tissue, the HLA type is difficult to analyze because of fragmentation of DNA, hindering the application of commonly used assays that rely on long DNA stretches. Addressing these difficulties, we present a refined approach for characterizing presence or absence of HLA-A*02, the most common HLA-A allele in the Caucasian population, in archival samples. We validated our genotyping strategy in a cohort of 90 samples with HLA status obtained by an NGS-based method. 90% (n = 81) of the samples could be analyzed with the approach. For all of them, the presence or absence of HLA-A*02 alleles was correctly determined with the method, demonstrating 100% sensitivity and specificity (95% CI: 91.40%–100% and 91.19%–100%). Furthermore, we provide an example of application in an independent cohort of 73 FFPE microsatellite-unstable (MSI) colorectal cancer samples. As MSI cancer cells encompass a high number of mutations in coding microsatellites, leading to the generation of highly immunogenic frameshift peptide antigens, they are ideally suited for studying relations between the mutational landscape of tumor cells and interindividual differences in the immune system, including the HLA genotype. Overall, our method can help to promote studying HLA type-dependency during the pathogenesis of a wide range of diseases, making archival and historic tissue samples accessible for identifying HLA-A*02 alleles. publishedVersion

Published

2022

14. New atrio-ventricular indices derived from conventional cine MRI correlate with functional capacity in patients with asymptomatic primary mitral regurgitation

Author

Perrine Marsac, Thomas Wallet, Alban Redheuil, Moussa Gueda Moussa, Jérôme Lamy, Vincent Nguyen, Etienne Charpentier, Nadjib Hammoudi, Emilie Bollache, and Nadjia Kachenoura

Subjects

Medicine, Science

Abstract

Abstract Mitral regurgitation (MR) is associated with morphological and functional alterations of left atrium (LA) and ventricle (LV), possibly inducing LA–LV misalignment. We aimed to: (1) characterize angulation between LA and mitral annulus from conventional cine MRI data and feature-tracking (FT) contours, (2) assess their associations with functional capacity in MR patients, as assessed by oxygen consumption (peak-VO2) and minute ventilation to carbon dioxide production (VE/VCO2) slope, in comparison with MRI LA/LV strain indices. Thirty-two asymptomatic primary MR patients (56 [40; 66] years, 12 women) underwent cardiac MRI resulting in LA/LV conventional FT-derived strain indices. Then, end-diastolic angles were derived from FT LA contours: (1) α, centered on the LA centre of mass and defined by mitral valve extremities, (2) γ, centered on the mitral ring anterior/lateral side, and defined by LA centre and the other extremity of the mitral ring. Cardiopulmonary exercise testing with simultaneous echocardiography were also performed; peak-VO2 and VE/VCO2 slope were measured. While peak-VO2 and VE/VCO2 slope were not correlated to LA/LV strains, they were significantly associated with angles (α: r = 0.50, p = 0.003 and r = − 0.52, p = 0.003; γ: r = − 0.53, p = 0.002 and r = 0.52, p = 0.003; respectively), independently of age and gender (R2 ≥ 0.29, p ≤ 0.03). In primary MR, the new LA/mitral annulus angles, computed directly from standard-of-care MRI, are better correlated to exercise tolerance than conventional LA/LV strain.

Published

2024

15. Epigenetic plasticity cooperates with emergent cell-cell interactions to drive neoplastic tissue remodeling in the pancreas

Author

Cassandra Burdziak, Direna Alonso-Curbelo, Thomas Walle, Francisco M. Barriga, José Reyes, Yubin Xie, Zhen Zhao, Chujun Julia Zhao, Hsuan-An Chen, Ojasvi Chaudhary, Ignas Masilionis, Zi-Ning Choo, Vianne Gao, Wei Luan, Alexandra Wuest, Yu-Jui Ho, Yuhong Wei, Daniela Quail, Richard Koche, Linas Mazutis, Tal Nawy, Ronan Chaligné, Scott W. Lowe, and Dana Pe’er

Abstract

The response to tumor-initiating inflammatory and genetic insults can vary amongst morphologically indistinguishable cells, suggesting yet uncharacterized roles for epigenetic plasticity during early neoplasia. To investigate the origins and impact of such plasticity, we perform single-cell analyses on normal, inflamed, pre-malignant and malignant tissues in autochthonous models of pancreatic cancer. We reproducibly identify heterogeneous cell-states that are primed for diverse late-emerging neoplastic fates and link these to chromatin remodeling at cell-cell communication loci. Using a new inference approach, we reveal signaling gene modules and tissue-level crosstalk, including a neoplasia-driving feedback loop between discrete epithelial and immune cell populations that we validate by genetic perturbation in mice. Our results uncover a neoplasia-specific tissue remodeling program that may be exploited for pancreas cancer interception.One-Sentence SummarySingle-cell analysis reveals that enhanced epigenetic plasticity drives pro-neoplastic crosstalk in early pancreatic cancer.

Published

2022

16. The VUB AI-lab RoboCup'99 Small League Team.

Author

Andreas Birk 0002, Thomas Walle, Tony Belpaeme, and Holger Kenn

Published

1999

17. Radiotherapy orchestrates natural killer cell dependent antitumor immune responses through CXCL8

Author

Thomas Walle, Joscha A. Kraske, Boyu Liao, Bénédicte Lenoir, Carmen Timke, Emilia von Bohlen und Halbach, Florian Tran, Paul Griebel, Dorothee Albrecht, Azaz Ahmed, Meggy Suarez-Carmona, Alejandro Jiménez-Sánchez, Tizian Beikert, Alexandra Tietz-Dahlfuß, Ayse Nur Menevse, Gabriele Schmidt, Manuela Brom, Jens H. W. Pahl, Wiebke Antonopoulos, Matthias Miller, Ramon Lopez Perez, Felix Bestvater, Nathalia A. Giese, Philipp Beckhove, Philip Rosenstiel, Dirk Jäger, Oliver Strobel, Dana Pe’er, Niels Halama, Jürgen Debus, Adelheid Cerwenka, and Peter E. Huber

Subjects

Killer Cells, Natural, Mice, Multidisciplinary, Neoplasms, Interleukin-8, Immunity, Animals, Humans, Adoptive Transfer, Xenograft Model Antitumor Assays

Abstract

Radiotherapy is a mainstay cancer therapy whose antitumor effects partially depend on T cell responses. However, the role of Natural Killer (NK) cells in radiotherapy remains unclear. Here, using a reverse translational approach, we show a central role of NK cells in the radiation-induced immune response involving a CXCL8/IL-8–dependent mechanism. In a randomized controlled pancreatic cancer trial, CXCL8 increased under radiotherapy, and NK cell positively correlated with prolonged overall survival. Accordingly, NK cells preferentially infiltrated irradiated pancreatic tumors and exhibited CD56dim-like cytotoxic transcriptomic states. In experimental models, NF-κB and mTOR orchestrated radiation-induced CXCL8 secretion from tumor cells with senescence features causing directional migration of CD56dimNK cells, thus linking senescence-associated CXCL8 release to innate immune surveillance of human tumors. Moreover, combined high-dose radiotherapy and adoptive NK cell transfer improved tumor control over monotherapies in xenografted mice, suggesting NK cells combined with radiotherapy as a rational cancer treatment strategy.

Published

2022

18. The Small League RoboCup Team of the VUB AI-Lab.

Author

Andreas Birk 0002, Thomas Walle, Tony Belpaeme, Johan Parent, Tom De Vlaminck, and Holger Kenn

Published

1998

19. RoboCube a 'universal' 'special purpose' Hardware for the RoboCup small robots league.

Author

Andreas Birk 0002, Holger Kenn, and Thomas Walle

Published

1998

20. HPP: A High Performance PRAM.

Author

Arno Formella, Jörg Keller 0001, and Thomas Walle

Published

1996

21. Cytokine release syndrome-like serum responses after COVID-19 vaccination are frequent and clinically inapparent under cancer immunotherapy

Author

Thomas, Walle, Sunanjay, Bajaj, Joscha A, Kraske, Thomas, Rösner, Christiane S, Cussigh, Katharina A, Kälber, Lisa Jasmin, Müller, Sophia Boyoung, Strobel, Jana, Burghaus, Stefan M, Kallenberger, Christoph K, Stein-Thöringer, Maximilian, Jenzer, Antonia, Schubert, Steffen, Kahle, Anja, Williams, Birgit, Hoyler, Lin, Zielske, Renate, Skatula, Stefanie, Sawall, Mathias F, Leber, Russell Z, Kunes, Johannes, Krisam, Carlo, Fremd, Andreas, Schneeweiss, Jürgen, Krauss, Leonidas, Apostolidis, Anne Katrin, Berger, Georg M, Haag, Stefanie, Zschäbitz, Niels, Halama, Christoph, Springfeld, Romy, Kirsten, Jessica C, Hassel, and Dirk, Jäger

Subjects

Cohort Studies, COVID-19 Vaccines, Interleukin-6, Neoplasms, Vaccination, COVID-19, Cytokines, Humans, Immunotherapy, Cytokine Release Syndrome, Immune Checkpoint Inhibitors

Abstract

Patients with cancer frequently receive immune-checkpoint inhibitors (ICIs), which may modulate immune responses to COVID-19 vaccines. Recently, cytokine release syndrome (CRS) was observed in a patient with cancer who received BTN162b2 vaccination under ICI treatment. Here, we analyzed adverse events and serum cytokines in patients with 23 different tumors undergoing (n = 64) or not undergoing (n = 26) COVID-19 vaccination under ICI therapy in a prospectively planned German single-center cohort study (n = 220). We did not observe clinically relevant CRS (≥grade 2) after vaccination (95% CI 0-5.6%; Common Terminology of Adverse Events v.5.0) in this small cohort. Within 4 weeks after vaccination, serious adverse events occurred in eight patients (12.5% 95% CI 5.6-23%): six patients were hospitalized due to events common under cancer therapy including immune related adverse events and two patients died due to conditions present before vaccination. Despite absence of CRS symptoms, a set of pairwise-correlated CRS-associated cytokines, including CXCL8 and interleukin-6 was1.5-fold upregulated in 40% (95% CI 23.9-57.9%) of patients after vaccination. Hence, elevated cytokine levels are common and not sufficient to establish CRS diagnosis.

Published

2021

22. Pregnancy and cardiac maternal outcomes in women with inherited cardiomyopathy: interest of the CARPREG II risk score

Author

Thomas Wallet, Lise Legrand, Richard Isnard, Estelle Gandjbakhch, Françoise Pousset, Julie Proukhnitzky, Marc Dommergues, Jacky Nizard, and Philippe Charron

Subjects

Cardiomyopathy, Pregnancy, Prognosis, Risk score, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Aims Inherited cardiomyopathies are relatively rare but carry a high risk of cardiac maternal morbidity and mortality during pregnancy and postpartum. However, data for risk stratification are scarce. The new CARPREG II score improves prediction of prognosis in pregnancies associated with heart disease, though its role in inherited cardiomyopathies is unclear. We aim to describe characteristics and cardiac maternal outcomes in patients with inherited cardiomyopathy during pregnancy, and to evaluate the interest of the CARPREG II risk score in this population. Methods and results In this retrospective single‐centre study, 90 consecutive pregnancies in 74 patients were included (mean age 32 ± 5 years), including 28 cases of dilated cardiomyopathy (DCM), 46 of hypertrophic cardiomyopathy, 11 of arrhythmogenic right ventricular cardiomyopathy and 5 of left ventricular noncompaction, excluding peripartum cardiomyopathy. The discriminatory power of several risk scores was assessed by the area under the receiver‐operating characteristic curve (AUC). Median CARPREG II score was 2 [0;3] and was higher in the DCM subgroup. A severe cardiac maternal complication was observed in 18 (20%) pregnancies, mainly driven by arrhythmia and heart failure (each event in 10 pregnancies), with 3 cardiovascular deaths. Forty‐three pregnancies (48%) presented foetal/neonatal complications (18 premature delivery, 3 foetal/neonatal death). CARPREG II was significantly associated with cardiac maternal complications (P

Published

2024

23. Signatures of plasticity, metastasis, and immunosuppression in an atlas of human small cell lung cancer

Author

Umesh Bhanot, David R. Jones, Thomas Walle, Ojasvi Chaudhary, Triparna Sen, Besnik Qeriqi, Linas Mazutis, Ignas Masilionis, Elisa de Stanchina, Dana Pe'er, W. Victoria Lai, Marissa Mattar, Dig Vijay Kumar Yarlagadda, Andrew Chow, Marina K. Baine, Fathema Uddin, Arvin Ruiz, Yanyun Li, Álvaro Quintanal-Villalonga, Natasha Rekhtman, Jacklynn V. Egger, Tal Nawy, Joseph M. Chan, John T. Poirier, Charles M. Rudin, Matthew J. Bott, Michael Offin, Amber Bahr, Viola Allaj, Travis J. Hollmann, Metamia Ciampricotti, James L. Wang, Vianne R. Gao, and Yubin Xie

Subjects

Cancer Research, Myeloid, Lung Neoplasms, medicine.medical_treatment, Cell Plasticity, Biology, Malignancy, Article, Metastasis, Immune system, medicine, Humans, Neoplasm Metastasis, neoplasms, Lung, Phospholipase C gamma, Sequence Analysis, RNA, Gene Expression Profiling, Immunosuppression, medicine.disease, Prognosis, Phenotype, Small Cell Lung Carcinoma, Survival Analysis, humanities, respiratory tract diseases, metastasis, myeloid, PLCG2, SCLC, scRNA-seq, single cell, tumor atlas, medicine.anatomical_structure, Oncology, Cancer research, Adenocarcinoma, Single-Cell Analysis

Abstract

Summary Small cell lung cancer (SCLC) is an aggressive malignancy that includes subtypes defined by differential expression of ASCL1, NEUROD1, and POU2F3 (SCLC-A, -N, and -P, respectively). To define the heterogeneity of tumors and their associated microenvironments across subtypes, we sequenced 155,098 transcriptomes from 21 human biospecimens, including 54,523 SCLC transcriptomes. We observe greater tumor diversity in SCLC than lung adenocarcinoma, driven by canonical, intermediate, and admixed subtypes. We discover a PLCG2-high SCLC phenotype with stem-like, pro-metastatic features that recurs across subtypes and predicts worse overall survival. SCLC exhibits greater immune sequestration and less immune infiltration than lung adenocarcinoma, and SCLC-N shows less immune infiltrate and greater T cell dysfunction than SCLC-A. We identify a profibrotic, immunosuppressive monocyte/macrophage population in SCLC tumors that is particularly associated with the recurrent, PLCG2-high subpopulation.

Published

2021

24. On-board control in the RoboCup small robots league.

Author

Andreas Birk 0002, Holger Kenn, and Thomas Walle

Published

2000

25. Ketotifen is a Prodrug. Norketotifen is the active metabolite

Author

Nada Arulnesan, Axel Karl Gunnar Aberg, Thomas Walle, Gordon T. Bolger, Vincent B. Ciofalo, Kresimir Pucaj, and Kristina Walle

Subjects

Ketotifen, Metabolite, Buffy coat, Prodrug, Pharmacology, chemistry.chemical_compound, medicine.anatomical_structure, Dogs, chemistry, Hepatocyte, Drug Discovery, medicine, Microsome, Animals, Hypnotics and Sedatives, Tumor necrosis factor alpha, Prodrugs, Active metabolite, medicine.drug

Abstract

Evaluation of the in vitro human liver microsome and hepatocyte metabolism of ketotifen demonstrated that norketotifen (NK) is the major demethylated hepatic metabolite of ketotifen. It is here reported that NK is completely devoid of the severe and dose-limiting sedative effects of ketotifen. Thus, while ketotifen is clinically dose-limited to 1 mg, bid, there are no dose-limiting sedative effects elicited by NK, even after the highest single-dose (16 mg) or after repeat-doses (8 mg × 7 days) in humans or after the highest doses given to dogs in repeat-dose toxicological studies (40 mg/kg × 14 days). In addition, NK-but not ketotifen-was found to express potent and dose-dependent inhibition of the release of the pro-inflammatory cytokine TNFα from activated human buffy coat preparations. Thus, when used as an anti-inflammatory drug, ketotifen is the sedating prodrug which is converted to NK a nonsedating metabolite with anti-inflammatory activity.

Published

2021

26. eHealth intervention to manage symptoms for patients with cancer on immunotherapy (SOFIA): a study protocol for a randomised controlled external pilot trial

Author

Simeon Sauer, Dirk Jäger, Thomas Walle, Georg Martin Haag, Imad Maatouk, Jürgen Krauß, Hans-Christoph Friederich, Christina Sauer, Senta Kiermeier, and Stefanie Zschäbitz

Subjects

Adult, medicine.medical_specialty, Adolescent, Pilot Projects, 03 medical and health sciences, 0302 clinical medicine, Quality of life, Intervention (counseling), Germany, Neoplasms, medicine, eHealth, Humans, 030212 general & internal medicine, Prospective Studies, Prospective cohort study, Adverse effect, Intensive care medicine, Randomized Controlled Trials as Topic, business.industry, General Medicine, Mental health, Telemedicine, adverse events, Clinical trial, Oncology, 030220 oncology & carcinogenesis, Quality of Life, Medicine, Immunotherapy, business, Psychosocial, mental health

Abstract

IntroductionImmune checkpoint therapy (ICT) is associated with a distinct pattern of immune-related adverse events (irAEs) caused by inadvertently redirecting immune responses to healthy tissues. IrAEs can occur at any time; however, in most cases, they arise during the first 14 weeks of the beginning of immune checkpoint blockade. In many cases, immunotherapy must be discontinued due to irAEs. Early detection of irAEs triggers the temporary withholding of ICT or initiation of short-term immunosuppressive treatment, is crucial in preventing further aggravation of irAEs and enables safe re-exposure to ICT. This prospective study aims to evaluate the feasibility of an eHealth intervention for patients under immunotherapy (managing symptoms of immunotherapy, SOFIA). The SOFIA-App consists of two components: SOFIA-Monitoring, a tool to rate patient-reported outcomes (PROs) including irAEs, and SOFIA-Coaching, which provides important information about cancer-specific and immunotherapy-specific topics and the counselling services of the National Centre for Tumour Diseases (NCT) Heidelberg.Methods and analysisWe outlined a patient-level two-arm randomised controlled pilot trial of the intervention (SOFIA) versus no-SOFIA for patients with cancer beginning an immunotherapy, aged ≥18 years, recruited from the NCT, Heidelberg. Feasibility outcomes include: recruitment rate; drop-out rate; reasons for refusal and drop-out; willingness to be randomised, utilisation rate of SOFIA-Monitoring and utilisation time of SOFIA-Coaching, physicians utilisation rate of the PROs; feasibility of the proposed outcome measures and optimal sample size estimation. The clinical outcomes are measures of quality of life, psychosocial symptoms, self-efficacy, physician-patient communication and medical process data, which are assessed at the beginning of the intervention, postintervention and at 6-month follow-up.Ethics and disseminationThis trial protocol was approved by the Ethical Committee of Heidelberg University, Germany (Reference, S-581/2018).Trial registration numberWe registered the study in the German Clinical Trial Register (Reference: DRKS00021064). Findings will be disseminated broadly via peer-reviewed empirical journals, articles and conference presentations.

Published

2021

27. Mirroring: a technique for pipelining semi-systolic and systolic arrays.

Author

Michael Braun 0002, Guy Even, and Thomas Walle

Published

1997

28. A Note on Implementing Combining Networks.

Author

Jörg Keller 0001 and Thomas Walle

Published

1995

29. Abstract LB116: CXCL8/Interleukin-8 orchestrates radiation-induced immune responses in pancreatic adenocarcinoma

Author

Thomas Walle, Joscha A. Kraske, Boyu Liao, Carmen Timke, Benedicte Lenoir, Niels Halama, and Peter E. Huber

Subjects

Cancer Research, Oncology

Abstract

The role of radiotherapy in the treatment of pancreatic adenocarcinoma (PDAC) is controversial. In many other tumor types, radiotherapy is a mainstay therapy whose anti-tumor effects have partially been ascribed to T cell responses. The role of Natural Killer (NK) cells in radiotherapy tumor responses remains unclear. Here, we focused on the role of NK cells in radiotherapy of pancreatic cancer. In a randomized controlled pancreatic cancer trial, we found that CXCL8 serum levels increased under radiotherapy and NK cells positively correlated with prolonged overall patient survival. Accordingly, NK cells preferentially infiltrated irradiated tumors and exhibited CD56dim like cytotoxic transcriptomic states. In preclinical experimental systems in mice and tumor cells, NF-κB and mTOR signaling prompted radiation-induced CXCL8 secretion from senescent tumor cells causing directional migration of CD56dim NK cells into tumors. Thus, we link senescence-associated CXCL8 release to innate immune surveillance of human tumors. Moreover, combined radiotherapy and adoptive NK cell transfer improved tumor control over monotherapies in xenografted mice suggesting NK cells combined with radiotherapy as a rational cancer treatment strategy which may be integrated into PDAC treatment algorithms. Citation Format: Thomas Walle, Joscha A. Kraske, Boyu Liao, Carmen Timke, Benedicte Lenoir, Niels Halama, Peter E. Huber. CXCL8/Interleukin-8 orchestrates radiation-induced immune responses in pancreatic adenocarcinoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr LB116.

Published

2022

30. Single cell profiling reveals novel tumor and myeloid subpopulations in small cell lung cancer

Author

Marissa Mattar, James L. Wang, Vianne R. Gao, Yubin Xie, Linas Mazutis, Charles M. Rudin, Dig Vk Yarlagadda, Jacklynn V. Egger, Thomas Walle, John T. Poirier, David R. Jones, Tal Nawy, Umesh Bhanot, Ignas Masilionis, Arvin Ruiz, Ojasvi Chaudhary, Triparna Sen, Dana Pe'er, Matthew J. Bott, Michael Offin, Joseph M. Chan, W. Victoria Lai, Viola Allaj, Fathema Uddin, Andrew Chow, Travis J. Hollmann, Metamia Ciampricotti, and Álvaro Quintanal-Villalonga

Subjects

Myeloid, Cell, Biology, medicine.disease, Malignancy, respiratory tract diseases, Metastasis, Transcriptome, ASCL1, medicine.anatomical_structure, medicine, Cancer research, Adenocarcinoma, CD8

Abstract

Small cell lung cancer (SCLC) is an aggressive malignancy that includes subtypes defined by differential expression of ASCL1, NEUROD1, and POU2F3 (SCLC-A, -N, and -P, respectively), which are associated with distinct therapeutic vulnerabilities. To define the heterogeneity of tumors and their associated microenvironments across subtypes, we sequenced 54,523 cellular transcriptomes from 21 human biospecimens. Our single-cell SCLC atlas reveals tumor diversity exceeding lung adenocarcinoma, driven by canonical, intermediate, and admixed subtypes. We discovered a PLCG2-high tumor cell population with stem-like, pro-metastatic features that recurs across subtypes and predicts worse overall survival, and manipulation of PLCG2 expression in cells confirms correlation with key metastatic markers. Treatment and subtype are associated with substantial phenotypic changes in the SCLC immune microenvironment, with greater T-cell dysfunction in SCLC-N than SCLC-A. Moreover, the recurrent, PLCG2-high subclone is associated with exhausted CD8+ T-cells and a pro-fibrotic, immunosuppressive monocyte/macrophage population, suggesting possible tumor-immune coordination to promote metastasis.

Published

2020

31. Feasibility and sociopsychological impact of video consultations in medical oncology - a randomized controlled open label trial

Author

Barbara Gruen, Constantin Pixberg, Jakob Nikolas Kather, Hans Martin Singh, Editha Gnutzmann, Mareike Dietrich, Bruno Christian Koehler, Niels Steinebrunner, Helen Starke, Andreas Mock, Andreas Schneeweiss, Eva C. Winkler, Lena Woydack, Athanasios Mavratzas, Helene Hofmann, Erkin Erdal, David Schult, Johannes Krisam, Leon Muehlsteffen, Felix Korell, Thomas Walle, Alexandra Ivanova, and Dirk Jaeger

Subjects

Clinical trial, medicine.medical_specialty, Indirect costs, Patient satisfaction, business.industry, Mobile phone, Consulting Physician, Cohort, Physical therapy, medicine, Outpatient clinic, Open label, business

Abstract

BackgroundMobile phone video call applications generally did not undergo testing in randomized controlled clinical trials prior to their implementation in patient care regarding the rate of successful patient visits and impact on the physician-patient relationship.MethodsThe NCT MOBILE trial was a monocentric open-label randomized controlled clinical trial of patients with solid tumors undergoing systemic cancer therapy with need of a follow-up visit with their consulting physician at outpatient clinics. 66 patients were 1:1 randomized to receive either a standard in-person follow-up visit at outpatient clinics or a video callviaa mobile phone application. The primary outcome was feasibility defined as the number of successful appointments at the first follow up visit. Secondary outcomes included success rate of further video calls, time spent by patient and physician, patient satisfaction, and quality of physician-patient relationship.FindingsSuccess rate of the first follow up visit in the intention-to-treat cohort was 87.8% for in-person visits and 78.7% for video calls (p=0.51, RR=0.88-1.43 95%CI). The most common reasons for failure were software incompatibility (12%) in the video call and no-show (6%) in the in-person visit arm. The success rate for further video visits was 91.6% (11 of 12 calls). Standardized patient questionnaires showed significantly decreased total time spent and less direct costs for patients (Δ95 to 246min 95%CI, Δ4.8 to 23.9€ 95%CI) and comparable time spent for physicians in the video call arm (Δ-6.4 to 5.4min, 95%CI). Doctor-patient relationship quality mean scores assessed by the validated standardized “questionnaire on quality of physician-patient interaction”(QQPPI) were higher in the video call arm (video call/in-person = 1.12 fold, p=0.02).InterpretationFollow-up visits with the tested mobile phone video call application were feasible but software compatibility should be critically evaluated.Trial registrationRetrospectively registered in the German Clinical Trials Register DRKS00015788, 26thOctober 2018

Published

2020

32. Surrogates for Liquid–Liquid Extraction

Author

Maximilian Neubauer, Georg Lenk, Nikolai Josef Schubert, Susanne Lux, and Thomas Wallek

Subjects

Chemistry, QD1-999

Published

2023

33. OA07.01 Signatures of Plasticity and Immunosuppression in a Single-Cell Atlas of Human Small Cell Lung Cancer

Author

Vianne R. Gao, Linas Mazutis, Travis J. Hollmann, Yubin Xie, Joseph M. Chan, Dana Pe'er, Metamia Ciampricotti, Tal Nawy, V. Lai, Ignas Masilionis, David R. Jones, Matthew J. Bott, Ojasvi Chaudhary, Thomas Walle, Michael Offin, Triparna Sen, Andrew Chow, Álvaro Quintanal-Villalonga, Jacklynn V. Egger, Charles M. Rudin, and Viola Allaj

Subjects

Pulmonary and Respiratory Medicine, medicine.anatomical_structure, Oncology, Atlas (topology), business.industry, medicine.medical_treatment, Cell, Cancer research, medicine, Immunosuppression, Non small cell, business

Published

2021

34. Completion rate and impact on physician-patient relationship of video consultations in medical oncology: a randomised controlled open-label trial

Author

Barbara Grün, Alexandra Ivanova, Constantin Pixberg, David Schult, Niels Steinebrunner, Athanasios Mavratzas, Helene Hofmann, Editha Gnutzmann, Lena Woydack, Thomas Walle, Leon Mühlsteffen, Erkin Erdal, Andreas Schneeweiss, Dirk Jäger, Eva C. Winkler, Mareike Dietrich, Felix Korell, Jakob Nikolas Kather, Johannes Krisam, Helen Starke, Hans Martin Singh, Bruno Köhler, and Andreas Mock

Subjects

Cancer Research, Telemedicine, medicine.medical_specialty, digital health, Medical Oncology, smartphone, lcsh:RC254-282, Indirect costs, physician-patient relationship, Patient satisfaction, Consulting Physician, Physicians, Outpatient clinic, Medicine, Humans, Referral and Consultation, Original Research, business.industry, shared decision-making, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Clinical trial, Oncology, Patient Satisfaction, Relative risk, Cohort, Physical therapy, telemedicine, business

Abstract

ESMO open 5(6), e000912 (2020). doi:10.1136/esmoopen-2020-000912, Published by BMJ, London

Published

2020

35. Signatures of plasticity and immunosuppression in a single-cell atlas of human small cell lung cancer

Author

Charles M. Rudin, Jacklynn V. Egger, Thomas Walle, Travis Hollman, Matthew J. Bott, Marissa Mattar, Tal Nawy, Michael Offin, Dana Pe'er, Vianne R. Gao, Linas Mazutis, W. Victoria Victoria Lai, Ojasvi Chaudhary, Triparna Sen, Andrew Chow, Álvaro Quintanal-Villalonga, Joseph M. Chan, Viola Allaj, and Ignas Masilionis

Subjects

Cancer Research, Atlas (topology), business.industry, medicine.medical_treatment, Cell, Immunosuppression, Malignancy, medicine.disease, respiratory tract diseases, ASCL1, medicine.anatomical_structure, Oncology, NEUROD1, medicine, Cancer research, Non small cell, Differential expression, business, neoplasms

Abstract

8509 Background: Small cell lung cancer (SCLC) is an aggressive malignancy that includes subtypes defined by differential expression of ASCL1, NEUROD1, and POU2F3 (SCLC-A, -N, and -P, respectively), which are associated with distinct therapeutic vulnerabilities. The emerging consensus on SCLC subtypes has led to new questions, such as whether subtypes are associated with different disease stages, metastatic potential, or immune microenvironments; whether there is plasticity between subtypes; and whether novel SCLC phenotypes exist. Single cell RNA sequencing (scRNA-seq) offers a unique opportunity to address these questions by dissecting intratumoral transcriptional heterogeneity and the surrounding tumor microenvironment (TME). However, efforts to apply this technology to human SCLC tumors have been limited, as these tumors are infrequently resected. Methods: We have optimized protocols to process both surgical resections and biopsies to construct the first single-cell atlas of SCLC patient tumors (N = 21), with comparative lung adenocarcinoma (LUAD) and normal lung data. We leverage computational methods including diffusion maps and non-negative matrix factorization to perform a deep annotation of SCLC phenotypes and the surrounding immune TME. We perform validation experiments using flow cytometry, Vectra, and immunohistochemistry in independent SCLC cohorts, as well as genetic manipulation in preclinical SCLC models. Results: Our data reveals substantial transcriptional heterogeneity in SCLC both within and across tumors and confirms a pro-metastatic gene program in SCLC-N subtype characterized by epithelial-mesenchymal transformation and axonogenesis. Beyond known subtypes, we discover a PLCG2-high tumor cell population with stem-like, pro-metastatic features that recurs across subtypes and predicts significantly worse overall survival. Manipulation of PLCG2 expression in cells confirms correlation with key metastatic markers. Treatment and subtype are associated with substantial phenotypic changes in the SCLC immune microenvironment, with greater T-cell dysfunction in SCLC-N than SCLC-A. Moreover, the recurrent, PLCG2-high subclone is associated with exhausted CD8+ T-cells and a pro-fibrotic, immunosuppressive monocyte/macrophage population, suggesting possible tumor-immune coordination to promote metastasis. Conclusions: This atlas of SCLC illustrates how canonical subtypes and a novel PLCG2-high recurrent tumor subclone enlist diverse gene programs to create tumor heterogeneity and facilitate metastasis in a profoundly immunosuppressed TME. Our dataset provides further insight into tumor and immune biology in SCLC at single-cell resolution, with potential implications for design of novel targeted therapies and immunotherapeutic approaches.

Published

2021

36. Community-driven development of a modified progression-free survival ratio for precision oncology

Author

Andreas Mock, Christoph E Heilig, Simon Kreutzfeldt, Daniel Huebschmann, Christoph Heining, Evelin Schröck, Benedikt Brors, Albrecht Stenzinger, Dirk Jäger, Richard Schlenk, Hanno Glimm, Stefan Fröhling, Peter Horak, Leonidas Apostolidis, Marinela Augustin, Daniela Aust, Irfan Ahmed Bhatti, Johannes Bloehdorn, Cornelia Brendel, Christian Britschgi, Jan Braess, Stefan Burdach, Elena Busch, Jozefina Casuscelli, Alexander Desuki, Thomas Deutsch, Mareike Dietrich, Ursula Ehmer, Thomas J Ettrich, Johanna Falkenhorst, Tanja Fehm, Anne Flörcken, Andrea Forschner, Stefan Fuxius, Maria Gonzales-Carmona, Frank Griesinger, Sabine Grill, Stefan Gröschel, Georg Martin Haag, Ulrich Haag, Niels Halama, Holger Hebart, Nina Heidger, Barbara Hermes, Georg Hess, Simone Hettmer, Manuela Hoechstetter, Martin Hoffmann, Felix J Hüttner, Anna L Illert, Maximilian Jenzer, Bernd Kasper, Stefan Kasper-Virchow, Thomas Kindler, Ewa Koscielniak, Jan Krönke, Michael Kühn, Volker Kunzmann, Alois Lang, Jonas Leichsenring, Elisabeth Livingstone, Lucia Liotta, Kim Luley, Elisabeth Mack, Uwe M Martens, Klaus Metzeler, Jan Moritz Middeke, Lino Möhrmann, Roopa Jayarama-Naidu, Ulrich-Frank Pape, Lukas Perkhofer, Arne Pfeufer, Constantin Pixberg, Michael Quante, Bernhard Rendenbach, Damian Rieke, Christian Rothermundt, Andre Norbert Sagerer, Martin Salzmann, Dieter Saur, Bastian Schilling, Jan Schleicher, Anke Schlenska-Lange, Thomas Schmidt, Sophia Schmitz, Sebastian Schölch, Rajiv Shah, Khalid Shoumariyeh, Alexander Siebenhüner, Martin Singh, Jens Siveke, Christoph Springfeld, Helen Starke, Sophia Strobel, Veronica Teleanu, Niklas Thon, Sebastian Wagner, Thomas Walle, Benedikt Westphalen, Bettina Whitlock, Eva Winkler, Naita Maren Wirsik, Lena Woydack, Angelika Zabel-du Bois, Stefanie Zschäbitz, University of Zurich, and Fröhling, Stefan

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Concordance, 610 Medicine & health, Classification scheme, Medical Oncology, Systemic therapy, lcsh:RC254-282, PFS, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Outcome Assessment, Health Care, Clinical endpoint, Medicine, Humans, 1306 Cancer Research, Progression-free survival, Precision Medicine, Societies, Medical, 030304 developmental biology, Original Research, Oncologists, 0303 health sciences, Clinical Trials as Topic, business.industry, High-Throughput Nucleotide Sequencing, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, personalized oncology, Progression-Free Survival, 3. Good health, Precision oncology, Research Design, 030220 oncology & carcinogenesis, 10032 Clinic for Oncology and Hematology, Personalized oncology, N-of-1 clinical trials, 2730 Oncology, Outcome data, business

Abstract

Objective Measuring the success of molecularly guided therapies is a major challenge in precision oncology trials. A commonly used endpoint is an intra-patient progression-free survival (PFS) ratio, defined as the PFS interval associated with molecularly guided therapy (PFS2) divided by the PFS interval associated with the last prior systemic therapy (PFS1), above 1.3 or, in some studies, above 1.33 or 1.5. Methods To investigate if the concept of PFS ratios is in agreement with actual response evaluations by physicians, we conducted a survey among members of the MASTER (Molecularly Aided Stratification for Tumor Eradication Research) Programme of the German Cancer Consortium who were asked to classify the success of molecularly guided therapies in 194 patients enrolled in the MOSCATO 01 trial based on PFS1 and PFS2 times. Results A comparison of classification profiles revealed three distinct clusters of PFS benefit assessments. Only 29% of assessments were consistent with a PFS ratio threshold of 1.3, whereas the remaining 71% of participants applied a different classification scheme that did not rely on the relation between PFS times alone, but also took into account absolute PFS1 intervals. Based on these community-driven insights, we developed a modified PFS ratio that incorporates the influence of absolute PFS1 intervals on the judgement of clinical benefit by physicians. Application of the modified PFS ratio to outcome data from two recent precision oncology trials, MOSCATO 01 and WINTHER, revealed significantly improved concordance with physician-perceived clinical benefit and identified comparable proportions of patients who benefited from molecularly guided therapies. Conclusions The modified PFS ratio may represent a meaningful clinical endpoint that could aid in the design and interpretation of future precision oncology trials.

Published

2019

37. Targeting CD73 May Improve Immunotherapy Efficacy in Glioblastoma

Author

Thomas Walle, Luis M Vence, Irina Fernandez, Swetha Anandhan, A. E. Cornish, Sangeeta Goswami, and Sreyashi Basu

Subjects

Oncology, business.industry, medicine.medical_treatment, Cancer research, Medicine, Immunotherapy, business, medicine.disease, Glioblastoma

Abstract

CD73hi macrophages are enriched in glioblastoma and may contribute to immunotherapy resistance.

Published

2020

38. CMR Left Atrial Flow Indices and Mitral Annulus Angulation in Patients with Asymptomatic Primary Mitral Regurgitation

Author

Perrine Marsac, MSc, Thomas Wallet, MD, Alban Redheuil, MD, PhD, Moussa Gueda, MSc, Jérôme Lamy, PhD, Vincent Nguyen, MSc, Etienne Charpentier, MD, Emilie Bollache, PhD, Nadjib Hammoudi, MD, PhD, and Nadjia Kachenoura, PhD

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Published

2024

39. Radiation effects on antitumor immune responses: current perspectives and challenges

Author

Adelheid Cerwenka, Ignacio Melero, Daniel Ajona, Fernando Lecanda, Thomas Walle, and Rafael Martinez Monge

Subjects

0301 basic medicine, Abscopal, medicine.medical_treatment, Lymphocyte, brachytherapy, Brachytherapy, Review, abscopal, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immune system, immunogenic cell death, PD-1, medicine, radiotherapy, Tumor microenvironment, Radiotherapy, business.industry, Cancer, Immunotherapy, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Radiation therapy, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Immunogenic cell death, immunotherapy, business, Adjuvant, checkpoint inhibitors, Checkpoint inhibitors

Abstract

Radiotherapy (RT) is currently used in more than 50% of cancer patients during the course of their disease in the curative, adjuvant or palliative setting. RT achieves good local control of tumor growth, conferring DNA damage and impacting tumor vasculature and the immune system. Formerly regarded as a merely immunosuppressive treatment, pre- and clinical observations indicate that the therapeutic effect of RT is partially immune mediated. In some instances, RT synergizes with immunotherapy (IT), through different mechanisms promoting an effective antitumor immune response. Cell death induced by RT is thought to be immunogenic and results in modulation of lymphocyte effector function in the tumor microenvironment promoting local control. Moreover, a systemic immune response can be elicited or modulated to exert effects outside the irradiation field (so called abscopal effects). In this review, we discuss the body of evidence related to RT and its immunogenic potential for the future design of novel combination therapies.

Published

2018

40. Bioavailability of resveratrol

Author

Thomas Walle

Subjects

chemistry.chemical_classification, endocrine system diseases, organic chemicals, General Neuroscience, Sulfatase, Microbial metabolism, food and beverages, Metabolism, Absorption (skin), Urine, Pharmacology, Resveratrol, General Biochemistry, Genetics and Molecular Biology, Bioavailability, chemistry.chemical_compound, Enzyme, History and Philosophy of Science, chemistry, skin and connective tissue diseases, hormones, hormone substitutes, and hormone antagonists

Abstract

This paper reviews our current understanding of the absorption, bioavailability, and metabolism of resveratrol, with an emphasis on humans. The oral absorption of resveratrol in humans is about 75% and is thought to occur mainly by transepithelial diffusion. Extensive metabolism in the intestine and liver results in an oral bioavailability considerably less than 1%. Dose escalation and repeated dose administration of resveratrol does not appear to alter this significantly. Metabolic studies, both in plasma and in urine, have revealed major metabolites to be glucuronides and sulfates of resveratrol. However, reduced dihydroresveratrol conjugates, in addition to highly polar unknown products, may account for as much as 50% of an oral resveratrol dose. Although major sites of metabolism include the intestine and liver (as expected), colonic bacterial metabolism may be more important than previously thought. Deconjugation enzymes such as β-glucuronidase and sulfatase, as well as specific tissue accumulation of resveratrol, may enhance resveratrol efficacy at target sites. Resveratrol analogs, such as methylated derivatives with improved bioavailability, may be important in future research.

Published

2011

41. Methylation of Dietary Flavones Increases Their Metabolic Stability and Chemopreventive Effects

Author

Thomas Walle

Subjects

Cell Membrane Permeability, Review, Flavones, Catalysis, Intestinal absorption, lcsh:Chemistry, Inorganic Chemistry, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Animals, Humans, Physical and Theoretical Chemistry, Aromatase, lcsh:QH301-705.5, Molecular Biology, Spectroscopy, 030304 developmental biology, 2. Zero hunger, chemistry.chemical_classification, 0303 health sciences, cancer prevention, biology, Organic Chemistry, General Medicine, Methylation, methoxyflavones, Diet, 3. Good health, Computer Science Applications, Bioavailability, lcsh:Biology (General), lcsh:QD1-999, chemistry, Biochemistry, 030220 oncology & carcinogenesis, flavonoids, Toxicity, Cancer cell, Microsomes, Liver, biology.protein, Chemoprotective, methylation, Half-Life

Abstract

Dietary flavones have promising chemoprotective properties, in particular with regard to cancer, but problems with low oral bioavailability and sometimes unacceptable toxicity have made their use as protective additives to normal diets questionable. However, methylation of free phenolic hydroxyl groups leads to derivatives not susceptible to glucuronic acid or sulfate conjugation, resulting in increased metabolic stability. Methylation also leads to greatly improved transport through biological membranes, such as in intestinal absorption, and much increased oral bioavailability. Recent studies also indicate that methylation results in derivatives with increasing potency to kill cancer cells. They also show high potency towards inhibition of hormone-regulating enzymes, e.g., aromatase, important in the causation of breast cancer. Methylation of the flavones may also result in derivatives with diminished toxic side-effects and improved aqueous solubility. In conclusion, it appears that methylation of dietary flavones as well as of other food products may produce derivatives with much improved health effects.

Published

2009

42. Cytotoxic effects of the dietary flavones chrysin and apigenin in a normal trout liver cell line

Author

Petra A. Tsuji and Thomas Walle

Subjects

Cell Survival, Trout, Toxicology, medicine.disease_cause, Flavones, Article, Cell Line, chemistry.chemical_compound, Cell Line, Tumor, Cell Adhesion, medicine, Animals, Humans, Chrysin, Apigenin, Cell Proliferation, Peroxidase, Flavonoids, chemistry.chemical_classification, Molecular Structure, Chemistry, Liver cell, Hydrogen Peroxide, General Medicine, Oxidants, Biochemistry, Toxicity, Hepatocytes, Quercetin, Oxidation-Reduction, Luteolin, Oxidative stress

Abstract

Many flavonoids have been shown to possess prooxidant properties, capable of causing oxidative stress, especially at larger doses. Here, we examined the potential cell toxicity caused by exposure to the hydroxylated flavones chrysin, apigenin, luteolin and quercetin in comparison to the methylated flavones 5,7-dimethoxyflavone and 3',4'-dimethoxyflavone in normal Rainbow trout hepatocytes. The hydroxylated flavones, especially chrysin, demonstrated cell toxicity and inhibition of DNA synthesis at very low (2 microM) concentrations. The cytotoxicity of chrysin may partially be due to its metabolism by myeloperoxidase, which was shown to be present in these normal trout liver cells (164pmol/(min mg protein)). In contrast, methylated flavones showed no significant metabolism by myeloperoxidase and no signs of toxicity, even at much higher concentrations. These results may be useful for further investigations of cytotoxicity of dietary flavonoids.

Published

2008

43. Methylation of Dietary Flavones Greatly Improves Their Hepatic Metabolic Stability and Intestinal Absorption

Author

Thomas Walle

Subjects

chemistry.chemical_classification, Chemistry, Biological Availability, Pharmaceutical Science, Metabolism, Methylation, Flavones, Glucuronic acid, Intestinal absorption, Diet, Bioavailability, chemistry.chemical_compound, Intestinal Absorption, Liver, S9 fraction, Biochemistry, In vivo, Drug Discovery, Animals, Humans, Molecular Medicine, Tissue Distribution, Cell Proliferation

Abstract

Dietary flavonoids and other polyphenols have many biological properties that could make them useful as chemopreventive agents. However, very poor oral bioavailability makes them largely ineffective in vivo. The low bioavailability is mainly due to highly efficient glucuronic acid and sulfate conjugation of these mono- or polyhydroxylated agents in the intestinal/hepatic barrier. This review describes how the methyl capping of all free hydroxyl groups of flavones results in dramatically increased metabolic stability, as the metabolism is shifted to less efficient CYP-mediated oxidation. This was demonstrated best by using the human liver S9 fraction with an appropriate selection of cofactors. In addition, the intestinal transport of flavones was much improved through methylation, as shown in Caco-2 cell Transwell experiments. In vivo in the rat, oral administration of one methylated flavone resulted in high bioavailability and tissue distribution with no detectable levels of its unmethylated analogue. In addition to increased metabolic stability, methylation resulted in markedly increased inhibition of cancer cell proliferation. Thus, methylation appears to be a simple and effective way of increasing both metabolic resistance and transport of the flavonoids and, most important, some of their major biological activities.

Published

2007

44. Methoxylated flavones, a superior cancer chemopreventive flavonoid subclass?

Author

Thomas Walle

Subjects

Flavonoids, chemistry.chemical_classification, Cancer Research, Cancer prevention, Flavonoid, Cell cycle, Pharmacology, Membrane transport, Flavones, Chemoprevention, Methylation, Article, Nobiletin, chemistry.chemical_compound, Cell Transformation, Neoplastic, Biochemistry, chemistry, Neoplasms, Cancer cell, Animals, Anticarcinogenic Agents, Humans, Carcinogen

Abstract

Dietary flavonoids and other polyphenols show great potential as cancer chemopreventive agents in cell culture studies. This does not translate well into in vivo activity, because of extensive conjugative metabolism of these compounds in the intestine and liver. This paper presents a review of a flavonoid subclass in which all hydroxyl groups are capped by methylation. This results in dramatically increased metabolic stability and membrane transport in the intestine/liver, thus improving oral bioavailability. The methoxyflavones also show increased cancer chemopreventive properties. At the cancer initiation stage, bioactivation of polyaromatic hydrocarbon carcinogens and binding to DNA are markedly diminished through effects on CYP1A1/1B1 transcription but also through direct interactions with the proteins. At the cancer promotion stage, the proliferation of cancer cells, but not normal cells, is inhibited with greater potency than with the unmethylated flavones. Limited mechanistic experiments, such as of effects on cell cycle regulation, indicate that the mechanisms of methoxyflavone activities are unique, including aromatase inhibition. The cancer preventive effects and mechanisms of the polymethoxyflavones, such as tangeretin and nobiletin, are discussed in comparison. It is concluded that the methoxyflavones have properties that may make them particularly useful as cancer chemopreventive agents.

Published

2007

45. Bioavailable Flavonoids: Cytochrome P450-Mediated Metabolism of Methoxyflavones

Author

U. Kristina Walle and Thomas Walle

Subjects

Stereochemistry, Flavonoid, Glucuronidation, Pharmaceutical Science, Flavones, chemistry.chemical_compound, Sulfation, Cytochrome P-450 Enzyme System, Cytochrome P-450 CYP1A2, Cytochrome P-450 CYP1A1, Cytochrome P-450 CYP3A, Humans, Phenols, Kaempferols, Cytochrome P-450 CYP2C9, Flavonoids, Pharmacology, chemistry.chemical_classification, Molecular Structure, CYP1A2, Recombinant Proteins, Cytochrome P-450 CYP2D6, Liver, S9 fraction, chemistry, Biochemistry, Microsomes, Liver, Microsome, Aryl Hydrocarbon Hydroxylases, Subcellular Fractions

Abstract

Methoxylated flavones were recently shown to be promising cancer chemopreventive agents. Their high metabolic stability compared with the hydroxylated analogs was shown in our laboratory using the human hepatic S9 fraction with cofactors for glucuronidation, sulfation, and oxidation. In the present study, the resistance of methoxylated flavones toward oxidative metabolism was investigated with human liver microsomes and recombinant cytochrome P450 (P450) isoforms. Among 15 methoxylated flavones investigated, the two partially methylated compounds, tectochrysin and kaempferide, were among the most susceptible to microsomal oxidation (Cl(int) 283 and 82 ml/min/kg). Of the fully methylated compounds, 5,7-dimethoxyflavone and 5-methoxyflavone were the most stable (Cl(int) 13 and 18 ml/min/kg, respectively), whereas 4'-methoxyflavone, 3'-methoxyflavone, 5,4'-dimethoxyflavone, and 7,3'-dimethoxyflavone were the least stable (Cl(int) 161, 140, 119, and 92 ml/min/kg, respectively), emphasizing the importance of the positions of the methoxy substituents in the flavone ring system. Among the five P450 isoforms tested, CYP1A1 showed the highest rate of metabolism of fully methylated compounds, followed by CYP1A2 and CYP3A4. CYP2C9 and CYP2D6 gave minimal disappearance of the parent compound. Finally, in incubations with hepatic S9 fraction with cofactors for oxidation and both conjugation reactions, partially methylated flavones, as expected, were much less metabolically stable than fully methylated flavones, confirming that oxidative demethylation is the rate-limiting metabolic reaction for fully methylated flavones only. In summary, the rate of oxidative metabolism of methoxylated flavones, mainly involving CYP1A1 and CYP1A2, varied widely, even between compounds with very similar structures.

Published

2007

46. Site-specific accumulation of the cancer preventive dietary polyphenol ellagic acid in epithelial cells of the aerodigestive tract

Author

Douglas H. Sweet, A.C. Whitley, and Thomas Walle

Subjects

Male, Organic anion transporter 1, Colon, Pharmaceutical Science, 4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid, Organic Anion Transporters, Sodium-Independent, Sulfobromophthalein, chemistry.chemical_compound, Esophagus, Organic Anion Transport Protein 1, Ellagic Acid, Intestine, Small, medicine, Animals, Humans, Tissue Distribution, Large intestine, RNA, Messenger, Intubation, Gastrointestinal, Pharmacology, biology, Epithelial Cells, Transporter, Hydrogen-Ion Concentration, Antineoplastic Agents, Phytogenic, Molecular biology, Rats, Inbred F344, Small intestine, Rats, Gastrointestinal Tract, medicine.anatomical_structure, Biochemistry, chemistry, Polyphenol, Paracellular transport, Injections, Intravenous, biology.protein, Organic anion transport, Caco-2 Cells, Ellagic acid

Abstract

Ellagic acid (EA), a polyphenol present in berries, has been demonstrated to prevent oesophageal and colon cancer in animals. To better understand the site-specificity of these effects, we studied the accumulation and transport of [14C]EA in rat aerodigestive epithelial cells in-vivo and in cultured human cells. When [14C]EA was administered to rats by gavage, a high content of EA was found in the oesophagus and small intestine at 0.5h after oral administration and in the colon at 12h, with very low amounts in plasma and peripheral tissues. Studies in human intestinal Caco-2 and human oesophageal HET-1A cells found very limited transcellular transport (Caco-2) of EA but high accumulation (Caco-2 and HET-1A) in the cells. In more detailed studies in the Caco-2 cells, accumulation of EA displayed ATP- and Na+-dependency. Multiple interventions permitted the exclusion of a number of transporters as mediators of this uptake. A dramatically reduced transport of EA at low pH (5.5) compared with high pH (7.4) suggested an important role for the negative charge of EA. This was supported by the organic anion transport inhibitors 4,4′-diisothiocyanatostilbene-2,2′-disulfonic acid and bromosulfophthalein. The latter produced as much as 78% inhibition at the 100 μm concentration. Finally, Caco-2 cells were shown to express organic anion transporter 4 (OAT4) mRNA, as was the human large intestine. EA appears to be accumulated along the aerodigestive tract using OATlike transporters, one of which might be OAT4.

Published

2006

47. BENZO[A]PYRENE-INDUCED ORAL CARCINOGENESIS AND CHEMOPREVENTION: STUDIES IN BIOENGINEERED HUMAN TISSUE

Author

Thomas Walle, David Sedmera, U. Kristina Walle, and Mitch Klausner

Subjects

Pharmaceutical Science, Resveratrol, Biology, medicine.disease_cause, Models, Biological, DNA Adducts, chemistry.chemical_compound, Organ Culture Techniques, Cytochrome P-450 Enzyme System, Phenols, Oral administration, Benzo(a)pyrene, medicine, Anticarcinogenic Agents, Humans, Carcinogen, Leukoplakia, Flavonoids, Pharmacology, Tissue Engineering, Mouth Mucosa, Polyphenols, medicine.disease, Epithelium, medicine.anatomical_structure, chemistry, Biochemistry, Carcinogens, Cancer research, Mouth Neoplasms, Carcinogenesis, Quercetin

Abstract

Oral cancer, originating from smoking-induced lesions of the basal cells in the complex stratified oral epithelium, is difficult to treat. Early detection of premalignant lesions, e.g., leukoplakia, has suggested the possibility of chemopreventive measures, such as topical application of antimutagenic/antiproliferative dietary or pharmaceutical agents. As an extension of a study in human oral epithelial cell monolayers, we determined the carcinogen, i.e., benzo[a]pyrene (BaP), transport, bioactivation, and DNA binding in a bioengineered human gingival epithelial tissue construct and the chemopreventive effects of dietary polyphenols. Short-term experiments showed that both types of compounds can traverse this tissue as well as be effectively taken up by the tissue. The model cigarette smoke carcinogen BaP very slowly, but to a great extent, accumulated in the tissue with maximal uptake at 24 h. Such exposure clearly resulted in DNA binding of BaP by the tissue. This DNA binding was associated with BaP-induced CYP1B1 as well as CYP1A1 expression, as evidenced by mRNA measurements. Cotreatment of the oral tissue with dietary polyphenols, including resveratrol and quercetin, and BaP, resulted in significant inhibition of the BaP-DNA binding. Using fluorescence microscopy as well as simultaneous autoradiography, we also demonstrated that quercetin indeed penetrates the entire stratified tissue layer, but that quercetin was also oxidized within the cells. Thus, this bioengineered oral tissue construct opens up improved ways of understanding and preventing/treating smoking-induced oral cancer.

Published

2005

48. S-adenosyl-l-methionine: transcellular transport and uptake by Caco-2 cells and hepatocytes

Author

U K Walle, J. M. McMillan, and Thomas Walle

Subjects

Male, Absorption (pharmacology), S-Adenosylmethionine, Cell type, Time Factors, Enterocyte, Cell, Cell Culture Techniques, Pharmaceutical Science, Intestinal mucosa, medicine, Animals, Humans, Rats, Long-Evans, Chromatography, High Pressure Liquid, Pharmacology, Chemistry, Biological Transport, Membrane transport, Culture Media, Rats, medicine.anatomical_structure, Biochemistry, Caco-2, Paracellular transport, Hepatocytes, Biophysics, Caco-2 Cells

Abstract

S-adenosyl-l-methionine (SAMe) is an endogenous molecule that is known to be protective against hepatotoxic injury. Although oral SAMe appears to be absorbed across the intestinal mucosa, its systemic bioavailability is low. The reason for this is unknown. Using the Caco-2 cell culture model for enterocyte absorption, we determined the mode by which SAMe is transported across this cell monolayer. We also determined the extent it is taken up by both Caco-2 cells and hepatocytes. In Caco-2 cells transport was observed in both apical to basolateral and basolateral to apical directions. The apparent permeability coefficients (Papp) appeared to be concentration independent and were similar in both directions (0.7 times 10−6 and 0.6 times 10−6 cms−1, respectively), i.e. identical to that of the paracellular transport marker mannitol (0.9 times 10−6 and 0.7 times 10−6 cms−1). This mode of transport was supported by a four-fold increase in the Papp for SAMe transport in Ca++-free buffer. Cellular uptake of SAMe was examined in both Caco-2 cells and cultured rat hepatocytes. Uptake by hepatocytes was not saturable in a concentration range of 0.001–100 μm. Accumulation by both cell types was very low, with a cell:medium ratio at equilibrium of only 0.2–0.5. This low cell accumulation supports the finding of paracellular transport as the only mode of cell membrane transport. Increased hepatocellular protection for SAMe may be accomplished by converting SAMe to a more lipid-soluble prodrug.

Published

2005

49. 5,7-Dimethoxyflavone downregulates CYP1A1 expression and benzo[a]pyrene-induced DNA binding in Hep G2 cells

Author

Xia Wen, Thomas Walle, and U. Kristina Walle

Subjects

Cancer Research, Carcinoma, Hepatocellular, Down-Regulation, Catalysis, Gene Expression Regulation, Enzymologic, law.invention, DNA Adducts, chemistry.chemical_compound, Phenols, Cytochrome P-450 CYP1A2, law, Benzo(a)pyrene, Cytochrome P-450 CYP1A1, Tumor Cells, Cultured, polycyclic compounds, Humans, RNA, Messenger, Binding site, IC50, Flavonoids, chemistry.chemical_classification, Binding Sites, biology, Reverse Transcriptase Polymerase Chain Reaction, Liver Neoplasms, Polyphenols, Cytochrome P450, DNA, Neoplasm, General Medicine, Molecular biology, Hep G2, Enzyme, chemistry, Biochemistry, Cytochrome P-450 CYP1B1, Recombinant DNA, biology.protein, Aryl Hydrocarbon Hydroxylases, DNA

Abstract

The objective of this study was to examine the ability of dietary polyphenols to inhibit cytochrome P450 (CYP) 1A1 expression and activity and benzo[a]pyrene (BaP) DNA binding, with the main emphasis on prevention of chemical-induced hepatic carcinogenesis. For this purpose we used Hep G2 cells, a good model of the normal human hepatocyte for CYP1A1 cell signaling. First, when these cells were exposed to a low concentration (1 microM) of BaP, DNA binding occurred, which dramatically increased after 6 h of treatment. BaP also dramatically induced CYP1A1 activity, protein expression and mRNA levels, the likely reason for the marked increase in DNA binding. Second, we screened 25 polyphenols with highly varying chemical structures for maximum ability to inhibit CYP1A1 activity in the Hep G2 cells. Highly varying responses were obtained, ranging from a 10-fold induction by some polyphenols to almost complete inhibition, in particular by 5,7-dimethoxyflavone (DMF), a flavonoid found in some tropical plants. Third, we examined the ability of DMF to inhibit DNA binding of BaP and the mechanisms involved. DMF (2-20 microM) inhibited BaP-induced DNA binding. DMF also inhibited BaP-induced CYP1A1 activity, CYP1A1 protein expression and mRNA levels. Moreover, DMF directly inhibited the catalytic activity of recombinant CYP1A1 with an IC50 of 0.8 microM. In conclusion, DMF was a highly potent inhibitor of BaP-induced DNA binding and CYP1A1 protein expression and activity in the Hep G2 cells. These properties may make DMF an effective chemoprotectant in chemical-induced liver cancer.

Published

2005

50. Flavonoid Glucosides Are Hydrolyzed and Thus Activated in the Oral Cavity in Humans

Author

U. Kristina Walle, Alyson M. Browning, Lisa L. Steed, Thomas Walle, and Susan G. Reed

Subjects

Saliva, Flavonoid, Medicine (miscellaneous), Genistein, Antineoplastic Agents, Rutin, chemistry.chemical_compound, Glucosides, Cell Line, Tumor, Humans, heterocyclic compounds, Flavonoids, chemistry.chemical_classification, Mouth neoplasm, Nutrition and Dietetics, Chemistry, Hydrolysis, food and beverages, Glycoside, Isoflavones, Quercitrin, Biochemistry, Flavanones, Carcinoma, Squamous Cell, Mouth Neoplasms, Quercetin, Cell Division

Abstract

Increasing epidemiological evidence supports the view that dietary flavonoids have protective roles in oral diseases, including cancer. However, the dietary forms of flavonoids, the flavonoid glycosides, must first be hydrolyzed to the aglycones, which is thought to occur mainly in the intestine. In the present study we tested whether this hydrolytic activity occurs in the oral cavity. Saliva was collected from human subjects, incubated with flavonoid glycosides, and analyzed for aglycone formation by HPLC. When quercetin 4'-glucoside or genistein 7-glucoside was incubated with human saliva, hydrolysis to quercetin and genistein, respectively, was detected within minutes. Studies of additional flavonoid glycosides demonstrated that glucose conjugates were rapidly hydrolyzed, but not conjugates with other sugars, i.e., rutin, quercitrin, and naringin. In a limited study of 17 subjects, the interindividual variability in the hydrolysis of genistein 7-glucoside was >20-fold. This supports the contention that salivary hydrolysis of certain flavonoid glucosides may be important in some individuals but not in others. Support for a bacterial contribution to this hydrolysis was obtained from the inhibitory effect of antibacterials in vivo and in vitro and from experiments with subcultured oral bacterial colonies. However, cytosol isolated from oral epithelial cells was also capable of effective hydrolysis. Dietary flavonoid glucosides may thus be hydrolyzed in the oral cavity by both bacteria and shedded epithelial cells to deliver the biologically active aglycones at the surface of the epithelial cells. The aglycones quercetin and genistein both potently inhibited proliferation of oral cancer cells. The large interindividual variability in this hydrolytic activity may be a factor that should be taken into consideration in future studies.

Published

2005