BACKGROUND: Efforts to identify novel therapeutic options for human pancreatic ductal adenocarcinoma (PDAC) have failed to result in a clear improvement in patient survival to date. Pancreatic cancer requires efficient therapies that must be designed and assayed in preclinical models with improved predictor ability. Among the available preclinical models, the orthotopic approach fits with this expectation, but its use is still occasional. METHODS: An in vivo platform of 11 orthotopic tumor xenografts has been generated by direct implantation of fresh surgical material. In addition, a frozen tumorgraft bank has been created, ensuring future model recovery and tumor tissue availability. RESULTS: Tissue microarray studies allow showing a high degree of original histology preservation and maintenance of protein expression patterns through passages. The models display stable growth kinetics and characteristic metastatic behavior. Moreover, the molecular diversity may facilitate the identification of tumor subtypes and comparison of drug responses that complement or confirm information obtained with other preclinical models. CONCLUSIONS: This panel represents a useful preclinical tool for testing new agents and treatment protocols and for further exploration of the biological basis of drug responses.
BACKGROUND: Efforts to identify novel therapeutic options for humanpancreatic ductal adenocarcinoma (PDAC) have failed to result in a clear improvement in patient survival to date. Pancreatic cancer requires efficient therapies that must be designed and assayed in preclinical models with improved predictor ability. Among the available preclinical models, the orthotopic approach fits with this expectation, but its use is still occasional. METHODS: An in vivo platform of 11 orthotopic tumor xenografts has been generated by direct implantation of fresh surgical material. In addition, a frozen tumorgraft bank has been created, ensuring future model recovery and tumor tissue availability. RESULTS: Tissue microarray studies allow showing a high degree of original histology preservation and maintenance of protein expression patterns through passages. The models display stable growth kinetics and characteristic metastatic behavior. Moreover, the molecular diversity may facilitate the identification of tumor subtypes and comparison of drug responses that complement or confirm information obtained with other preclinical models. CONCLUSIONS: This panel represents a useful preclinical tool for testing new agents and treatment protocols and for further exploration of the biological basis of drug responses.
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Authors: Helene Damhofer; Eva A Ebbing; Anne Steins; Lieke Welling; Johanna A Tol; Kausilia K Krishnadath; Tom van Leusden; Marc J van de Vijver; Marc G Besselink; Olivier R Busch; Mark I van Berge Henegouwen; Otto van Delden; Sybren L Meijer; Frederike Dijk; Jan Paul Medema; Hanneke W van Laarhoven; Maarten F Bijlsma Journal: J Transl Med Date: 2015-04-11 Impact factor: 5.531
Authors: Ilaria Pergolini; Vicente Morales-Oyarvide; Mari Mino-Kenudson; Kim C Honselmann; Matthew W Rosenbaum; Sabikun Nahar; Marina Kem; Cristina R Ferrone; Keith D Lillemoe; Nabeel Bardeesy; David P Ryan; Sarah P Thayer; Andrew L Warshaw; Carlos Fernández-Del Castillo; Andrew S Liss Journal: PLoS One Date: 2017-08-30 Impact factor: 3.240
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