High-throughput screening using patient-derived tumor xenografts to predict clinical trial drug response

Gao, Hui; Korn, Joshua M.; Ferretti, Stéphane; Monahan, John E.; Wang, Youzhen; Singh, Mallika; Zhang, Chao; Schnell, Christian; Yang, Guizhi; Zhang, Yun; Balbin, O. Alejandro; Barbé, Stéphanie; Cai, Hongbo; Casey, Fergal; Chatterjee, Susmita; Chiang, Derek Y.; Chuai, Shannon; Cogan, Shawn; Collins, Scott D.; Dammassa, Ernesta; Ebel, Nicolas; Embry, Millicent; Green, John; Kauffmann, Audrey; Kowal, Colleen; Leary, Rebecca J.; Lehár, Joseph; Liang, Ying; Loo, Alice; Lorenzana, Edward; McDonald, Ellice; McLaughlin, Margaret E.; Merkin, Jason J.; Meyer, Ronald A.; Naylor, Tara L.; Patawaran, Montesa; Reddy, Anupama; Röelli, Claudia; Ruddy, David A.; Salangsang, Fernando; Santacroce, Francesca; Singh, Angad; Tang, Yan; Tinetto, Walter; Tobler, Sonja; Velazquez, Roberto; Venkatesan, Kavitha; Arx, Fabian Von; Wang, Hui Qin; Wang, Zongyao; Wiesmann, Marion; Wyss, Daniel F.; Xu, Fiona; Bitter, Hans; Atadja, Peter; Lees, Emma; Hofmann, Francesco; Li, En; Keen, Nicholas; Cozens, Robert; Jensen, Michael Rugaard; Pryer, Nancy; Williams, Juliet; Sellers, William R.

doi:10.1038/nm.3954

Cited by 1,111 publications

(1,265 citation statements)

References 52 publications

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“…7 of these associations could be mapped to independent cell lines in the O'Neil et al 4 data set, with an overall Pearson correlation between DREAM and O'Neil effect sizes of 0.32 ( Figure 6B) showing a trend of reproducibility of synergy markers. Multiple validation criteria for quality and independent and in vivo reproducibility (see Methods) 4,7,8 were then applied to prioritize 13 feature-to-combination associations ( Figure 6C, Supp. Table 3), 7 associated with synergy and 6 with non-synergy.…”

Section: Biomarkers Of Synergy and Clinical Translatabilitymentioning

confidence: 99%

“…A key bottleneck in the development of such models has been a lack of public data sets of sufficient size and variety to train computational approaches 4,7,8 , particularly considering the diversity of biological mechanisms that may influence drug response. We shared with Challenge participants ~11,500 experimentally tested drug combinations on 85 cancer cell lines.…”

Section: Introductionmentioning

confidence: 99%

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A cancer pharmacogenomic screen powering crowd-sourced advancement of drug combination prediction

Wang

Guan

et al. 2017

Preprint

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In the last decade advances in genomics, uptake of targeted therapies, and the advent of personalized treatments have fueled a dramatic change in cancer care. However, the effectiveness of most targeted therapies is short lived, as tumors evolve and develop resistance. Combinations of drugs offer the potential to overcome resistance. The space of possible combinations is vast, and significant advances are required to effectively find optimal treatment regimens tailored to a patient's tumor. DREAM and AstraZeneca hosted a Challenge open to the scientific community aimed at computational prediction of synergistic drug combinations and predictive biomarkers associated to these combinations. We released a data set comprising ~11,500 experimentally tested drug combinations, coupled to deep molecular characterization of the respective 85 cancer cell lines. Among 150 submitted approaches, those that incorporated prior knowledge of putative drug targets showed superior performance predicting drug synergy across independent data. Genomic features of best-performing models revealed putative mechanisms of drug synergy for multiple drugs in combination with PI3K/AKT pathway inhibitors.All rights reserved. No reuse allowed without permission.(which was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.

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Section: Biomarkers Of Synergy and Clinical Translatabilitymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A cancer pharmacogenomic screen powering crowd-sourced advancement of drug combination prediction

Wang

Guan

et al. 2017

Preprint

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“…Moreover, such alterations may be over-or underrepresented in cell lines, whereas patient-derived xenografts (PDXs) seem to reproduce the genetic driver mutation landscape in leukemia more closely. [12][13][14] To obtain insight into interpatient drug response heterogeneity, we developed an in vitro platform directly using patient-derived leukemia cells. We hypothesized that drug response profiling of ALL, even without a priori information on genetic lesions or activated pathways, will detect sensitivity that may otherwise be overlooked.…”

Section: Introductionmentioning

confidence: 99%

Ex vivo drug response profiling detects recurrent sensitivity patterns in drug-resistant acute lymphoblastic leukemia

Frismantas

Dobay

Rinaldi

et al. 2017

Blood

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“…FOLFIRINOX. Pancreatic PDX models such as the one used in this study have been shown to be highly predictive of relapse after surgery, reflective of patient outcome, genetics, and RNA tumor subtypes (19,20,24). These results suggest that the iontophoretic delivery of FOLFIRINOX may translate to improved clinical outcomes by enhancing the therapeutic index of this drug mixture, allowing for resection of localized and locally advanced pancreatic cancer.…”

Section: Discussionmentioning

confidence: 63%

“…The aim of our study was to evaluate the iontophoretic delivery of FOLFIRINOX for the treatment of localized pancreatic cancer. We evaluated this therapy in xenografts derived from patients with pancreatic cancer, which have been shown to reflect recently defined RNA tumor subtypes in patients, mirror patient outcome, and be highly predictive of clinical response to many targeted agents (19,20). We report the delivery of high levels of the FOLFIRINOX drugs to the tumor, a reduction in systemic exposure of the drugs, and potent tumor regression.…”

mentioning

confidence: 99%

Iontophoretic device delivery for the localized treatment of pancreatic ductal adenocarcinoma

Byrne

Jajja

Schorzman

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Poor delivery and systemic toxicity of many cytotoxic agents, such as the recent promising combination chemotherapy regimen of folinic acid (leucovorin), fluorouracil, irinotecan, and oxaliplatin (FOLFIRINOX), restrict their full utility in the treatment of pancreatic cancer. Local delivery of chemotherapies has become possible using iontophoretic devices that are implanted directly onto pancreatic tumors. We have fabricated implantable iontophoretic devices and tested the local iontophoretic delivery of FOLFIRINOX for the treatment of pancreatic cancer in an orthotopic patientderived xenograft model. Iontophoretic delivery of FOLFIRINOX was found to increase tumor exposure by almost an order of magnitude compared with i.v. delivery with substantially lower plasma concentrations. Mice treated for 7 wk with device FOLFIRINOX experienced significantly greater tumor growth inhibition compared with i.v. FOLFIRINOX. A marker of cell proliferation, K i -67, was stained, showing a significant reduction in tumor cell proliferation. These data capitalize on the unique ability of an implantable iontophoretic device to deliver much higher concentrations of drug to the tumor compared with i.v. delivery. Local iontophoretic delivery of cytotoxic agents should be considered for the treatment of patients with unresectable nonmetastatic disease and for patients with the need for palliation of local symptoms, and may be considered as a neoadjuvant approach to improve resection rates and outcome in patients with localized and locally advanced pancreatic cancer.iontophoresis | FOLFIRINOX | pancreatic cancer | device delivery | chemotherapy

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High-throughput screening using patient-derived tumor xenografts to predict clinical trial drug response

Cited by 1,111 publications

References 52 publications

A cancer pharmacogenomic screen powering crowd-sourced advancement of drug combination prediction

A cancer pharmacogenomic screen powering crowd-sourced advancement of drug combination prediction

Ex vivo drug response profiling detects recurrent sensitivity patterns in drug-resistant acute lymphoblastic leukemia

Iontophoretic device delivery for the localized treatment of pancreatic ductal adenocarcinoma

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