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Dive into the research topics where Jan Endell is active.

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Featured researches published by Jan Endell.


Lab on a Chip | 2012

Macroporous silicon chips for laterally resolved, multi-parametric analysis of epithelial barrier function

Stefanie Michaelis; Christina Rommel; Jan Endell; Petra Göring; Ralf B. Wehrspohn; Claudia Steinem; Andreas Janshoff; Hans-Joachim Galla; Joachim Wegener

This study describes a novel assay to visualize the macromolecular permeability of epithelial and endothelial cell layers with subcellular lateral resolution. Defects within the cell layer and details about the permeation route of the migrating solute are revealed. The assay is based on silicon chips with densely packed, highly ordered, dead-ended pores of μm-diameters on one side. The cells under study are grown on the porous side of the chip such that the pores in the growth surface serve as an array of femtolitre-sized cuvettes in which the permeating probe accumulates at the site of permeation. The pattern of pore filling reveals the permeability characteristics of the cell layer with a lateral resolution in the μm range. Coating of the chip surface with a thin layer of gold allows for impedance analysis of the adherent cells in order to measure their tightness for inorganic ions at the same time. The new assay provides an unprecedented look on epithelial and endothelial barrier function.


Cancer Research | 2016

Abstract 280: Synergistic in vitro activity of MOR209/ES414 in combination with enzalutamide

Toddy Sewell; Michelle Blake; Jane A. Gross; Jan Endell; Johannes Weirather; John W. Blankenship

Metastatic castration-resistant prostate cancer (mCRPC) presents a daunting therapeutic challenge for patients who eventually progress after androgen ablation therapy. Although newer AR antagonists show a survival benefit, these patients ultimately relapse. Thus, it is critical to identify new therapies that will work in combination with AR antagonists or in AR-antagonist resistant settings. MOR209/ES414 is a bispecific ADAPTIR™ (modular protein technology) molecule currently under investigation in a phase 1 clinical trial in mCRPC, including patients that have progressed on enzalutamide. In pre-clinical studies, MOR209/ES414 has previously been shown to redirect T cell cytotoxicity against cells expressing Prostate Specific Membrane Antigen (PSMA). Here, we aimed to determine whether enzalutamide affects PSMA expression on CRPC cells in vitro, and could alter the effectiveness of MOR209/ES414 at inducing T-cell mediated tumor cell death. To address these questions, we utilized a CRPC cell line, 22Rv1, which has low expression of PSMA and is resistant to enzalutamide. Treatment of 22Rv1 cells with 10 μM enzalutamide for 3 weeks resulted in increased PSMA cell surface expression as measured by flow cytometry. 22Rv1 cells exposed to enzalutamide were also more sensitive to MOR209/ES414-mediated T-cell lysis, with a 25% increase in cytotoxicity over a 4 hour chromium release assay compared to 22Rv1 cells that were not exposed to enzalutamide. A concomitant decrease in EC50 for MOR209/ES414-mediated lysis from 0.8 pM to 0.5 pM was also observed in 22Rv1 cells exposed to enzalutamide. MOR209/ES414 and enzalutamide were next tested in combination using a PSMA-positive, enzalutamide-sensitive cell line, LNCaP cultured with primary T cells over several days. Suboptimal doses of MOR209/ES414 and enzalutamide were added to the cultures, and surviving LnCaP cells were quantitated 4 days later. Enzalutamide did not interfere with the ability of MOR209/ES414 to target T cells to LNCaP cells, and Combination Index analysis showed the activity of MOR209/ES414 and enzalutamide to be synergistic in vitro. These studies provide a rationale for further examination of combining MOR209/ES414 with enzalutamide, even in enzalutamide-resistant settings. Citation Format: Toddy Sewell, Michelle Blake, Jane A. Gross, Jan Endell, Johannes Weirather, John W. Blankenship. Synergistic in vitro activity of MOR209/ES414 in combination with enzalutamide. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 280.


Archive | 2011

Anti-cd38 antibody and lenalidomide or bortezomib for the treatment of multiple myeloma and nhl

Lisa Rojkjaer; Rainer Boxhammer; Jan Endell; Mark Winderlich; Christofer Samuelsson


Oncotarget | 2015

α-Radioimmunotherapy with 213 Bi-anti-CD38 immunoconjugates is effective in a mouse model of human multiple myeloma

Katharina Teiluf; Christof Seidl; Birgit Blechert; Florian Gaertner; Klaus-Peter Gilbertz; Vanesa Fernandez; Florian Bassermann; Jan Endell; Rainer Boxhammer; Stephane Leclair; Mario Vallon; Michaela Aichler; Annette Feuchtinger; Frank Bruchertseifer; Alfred Morgenstern; Markus Essler


Journal of Clinical Oncology | 2016

MOR202 alone and in combination with pomalidomide or lenalidomide in relapsed or refractory multiple myeloma: Data from clinically relevant cohorts from a phase I/IIa study.

Marc S. Raab; Manik Chatterjee; Hartmut Goldschmidt; Hermine Agis; Igor Wolfgang Blau; Hermann Einsele; Monika Engelhardt; Barbara Ferstl; Martin Gramatzki; Christoph Röllig; Katja Weisel; Pia Kloepfer; Dominika Weinelt; Jan Endell; Rainer Boxhammer; Christian Peschel


Blood | 2016

Single-Agent MOR208 in Relapsed or Refractory (R-R) Non-Hodgkin's Lymphoma (NHL): Results from Diffuse Large B-Cell Lymphoma (DLBCL) and Indolent NHL Subgroups of a Phase IIa Study

Wojciech Jurczak; Pier Luigi Zinzani; Gianluca Gaidano; Andre Goy; Mariano Provencio; Zsolt Nagy; Tadeusz Robak; Kami Maddocks; Christian Buske; S. Ambarkhane; Mark Winderlich; Maren Dirnberger-Hertweck; Jan Endell; Kristie A. Blum


Journal of Clinical Oncology | 2017

Effect of IMiD compounds on CD38 expression on multiple myeloma cells: MOR202, a human CD38 antibody in combination with pomalidomide.

Rainer Boxhammer; Stefan Steidl; Jan Endell


Journal of Clinical Oncology | 2011

Effect of MOR202, a human CD38 antibody, in combination with lenalidomide and bortezomib, on bone lysis and tumor load in a physiologic model of myeloma.

Jan Endell; C. Samuelsson; Rainer Boxhammer; S. Strauss; Stefan Steidl


Blood | 2014

Synergistic in Vitro Activity of MOR202, a Human CD38 Antibody, in Combination with Pomalidomide

Jan Endell; Rainer Boxhammer; Stefan Steidl


Blood | 2015

MOR202, a Human Anti-CD38 Monoclonal Antibody, Mediates Potent Tumoricidal Activity In Vivo and Shows Synergistic Efficacy in Combination with Different Antineoplastic Compounds

Rainer Boxhammer; Johannes Weirather; Stefan Steidl; Jan Endell

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