Simultaneous evaluation of anti-EGFR-induced tumour and adverse skin effects in a microfluidic human 3D co-culture model

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作者
Juliane Hübner
Marian Raschke
Isabel Rütschle
Sarah Gräßle
Tobias Hasenberg
Kerstin Schirrmann
Alexandra Lorenz
Susanne Schnurre
Roland Lauster
Ilka Maschmeyer
Thomas Steger-Hartmann
Uwe Marx
机构
[1] Technische Universität Berlin,
[2] Institute of Biotechnology,undefined
[3] Department Medical Biotechnology,undefined
[4] TissUse GmbH,undefined
[5] Bayer AG,undefined
[6] Investigational Toxicology,undefined
[7] The University of Manchester,undefined
[8] Manchester Centre for Nonlinear Dynamics,undefined
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关键词
Epithelial Growth Factor Receptor (EGFR); Tissue Micro; Culture Compartment; EGFR Inhibitors; Skin Equivalents;
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摘要
Antibody therapies targeting the epithelial growth factor receptor (EGFR) are being increasingly applied in cancer therapy. However, increased tumour containment correlates proportionally with the severity of well-known adverse events in skin. The prediction of the latter is not currently possible in conventional in vitro systems and limited in existing laboratory animal models. Here we established a repeated dose “safficacy” test assay for the simultaneous generation of safety and efficacy data. Therefore, a commercially available multi-organ chip platform connecting two organ culture compartments was adapted for the microfluidic co-culture of human H292 lung cancer microtissues and human full-thickness skin equivalents. Repeated dose treatment of the anti-EGFR-antibody cetuximab showed an increased pro-apoptotic related gene expression in the tumour microtissues. Simultaneously, proliferative keratinocytes in the basal layer of the skin microtissues were eliminated, demonstrating crucial inhibitory effects on the physiological skin cell turnover. Furthermore, antibody exposure modulated the release of CXCL8 and CXCL10, reflecting the pattern changes seen in antibody-treated patients. The combination of a metastatic tumour environment with a miniaturized healthy organotypic human skin equivalent make this “safficacy” assay an ideal tool for evaluation of the therapeutic index of EGFR inhibitors and other promising oncology candidates.
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