Abstract 318: Enhancing drug discovery and development throughput without sacrificing predictivity: ex vivo 3D drug response profiling (DRP) using patient-derived xenografts (PDX)

Abstract: Background: PDX have become critical elements of preclinical drug development as they better reflect the heterogeneity, molecular and histopathologic signatures of the original tumor than cell lines or genetically engineered mouse models, and their drug response profiles correlate with clinical response. While PDX models have become a powerful tool in drug discovery and development, limitations include low throughput for broad drug screening, lack of dose-response curves, high cost and progressive loss of huma… Show more

“…to phase out NCI-60 panel of 60 cancer cell lines. PDXs are derived by implanting human tumors in mice, and they have proven to mimic the heterogeneity and molecular signatures of the clinical tumor better than cell lines or genetically modified mouse models [78,79]. Similarly, tumor organoids have also been established from patient tumor specimens [80].…”

“…Similarly, tumor organoids have also been established from patient tumor specimens [80]. Although PDX and organoids have become popular in recent times, the limitations of PDX include lack of dose response curve, low throughput for broad drug testing, conducted in mice which lack normal immune response, require optimization of protocol and high cost [79]. Therefore, we believe the proposed 3D spheroid model system in this thesis would provide us with the knowledge and expertise to handle more complex systems like patient-derived organoids and PDXs.…”

Development of a FRET-based 3D in vitro breast tumor model and its application in evaluating drug-induced apoptosis

“…to phase out NCI-60 panel of 60 cancer cell lines. PDXs are derived by implanting human tumors in mice, and they have proven to mimic the heterogeneity and molecular signatures of the clinical tumor better than cell lines or genetically modified mouse models [78,79]. Similarly, tumor organoids have also been established from patient tumor specimens [80].…”

“…Similarly, tumor organoids have also been established from patient tumor specimens [80]. Although PDX and organoids have become popular in recent times, the limitations of PDX include lack of dose response curve, low throughput for broad drug testing, conducted in mice which lack normal immune response, require optimization of protocol and high cost [79]. Therefore, we believe the proposed 3D spheroid model system in this thesis would provide us with the knowledge and expertise to handle more complex systems like patient-derived organoids and PDXs.…”

Development of a FRET-based 3D in vitro breast tumor model and its application in evaluating drug-induced apoptosis