Systematic Screening Identifies Dual PI3K and mTOR Inhibition as a Conserved Therapeutic Vulnerability in Osteosarcoma

被引:61
作者
Gupte, Ankita [1 ,2 ]
Baker, Emma K. [1 ,2 ]
Wan, Soo-San [3 ,4 ]
Stewart, Elizabeth [5 ]
Loh, Amos [5 ]
Shelat, Anang A. [6 ]
Gould, Cathryn M. [7 ]
Chalk, Alistair M. [1 ,2 ]
Taylor, Scott [1 ,2 ]
Lackovic, Kurt [3 ,4 ]
Karlstroem, Asa [5 ]
Mutsaers, Anthony J. [1 ,2 ,8 ]
Desai, Jayesh [9 ,10 ]
Madhamshettiwar, Piyush B. [5 ]
Zannettino, Andrew C. W. [11 ,12 ]
Burns, Chris [3 ,4 ]
Huang, David C. S. [3 ,4 ]
Dyer, Michael A. [5 ,13 ]
Simpson, Kaylene J. [7 ,14 ]
Walkley, Carl R. [1 ,2 ,15 ]
机构
[1] St Vincents Inst Med Res, Fitzroy, Vic 3065, Australia
[2] Univ Melbourne, St Vincents Hosp, Dept Med, Fitzroy, Vic 3065, Australia
[3] Royal Melbourne Hosp, Walter & Eliza Hall Inst Med Res, Parkville, Vic 3050, Australia
[4] Univ Melbourne, Dept Med Biol, Parkville, Vic 3052, Australia
[5] St Jude Childrens Res Hosp, Dept Dev Neurobiol, Memphis, TN 38105 USA
[6] St Jude Childrens Res Hosp, Dept Chem Biol & Therapeut, Memphis, TN 38105 USA
[7] Peter MacCallum Canc Ctr, Victorian Ctr Funct Genom, East Melbourne, Vic, Australia
[8] Univ Guelph, Ontario Vet Coll, Guelph, ON N1G 2W1, Canada
[9] Royal Melbourne Hosp, Dept Med Oncol, Melbourne, Vic, Australia
[10] Peter MacCallum Canc Ctr, Melbourne, Vic, Australia
[11] Univ Adelaide, Fac Hlth Sci, Sch Med Sci, Myeloma Res Lab, Adelaide, SA, Australia
[12] South Australian Hlth & Med Res Inst, Canc Theme, Adelaide, SA, Australia
[13] Howard Hughes Med Inst, Chevy Chase, MD USA
[14] Univ Melbourne, Sir Peter MacCallum Dept Oncol, Parkville, Vic 3052, Australia
[15] St Vincents Inst Med Res, ACRF Rat Drug Discovery Ctr, Fitzroy, Vic 3065, Australia
基金
澳大利亚国家健康与医学研究理事会;
关键词
PRECLINICAL TESTING PROGRAM; MAMMALIAN TARGET; MESSENGER-RNA; CELL-LINES; IN-VIVO; STAGE; RAPAMYCIN; P53; RB; SEGMENTATION;
D O I
10.1158/1078-0432.CCR-14-3026
中图分类号
R73 [肿瘤学];
学科分类号
100214 [肿瘤学];
摘要
Purpose: Osteosarcoma is the most common cancer of bone occurring mostly in teenagers. Despite rapid advances in our knowledge of the genetics and cell biology of osteosarcoma, significant improvements in patient survival have not been observed. The identification of effective therapeutics has been largely empirically based. The identification of new therapies and therapeutic targets are urgently needed to enable improved outcomes for osteosarcoma patients. Experimental Design: We have used genetically engineered murine models of human osteosarcoma in a systematic, genome-wide screen to identify new candidate therapeutic targets. We performed a genome-wide siRNA screen, with or without doxorubicin. In parallel, a screen of therapeutically relevant small molecules was conducted on primary murine-and primary human osteosarcoma-derived cell cultures. All results were validated across independent cell cultures and across human and mouse osteosarcoma. Results: The results from the genetic and chemical screens significantly overlapped, with a profound enrichment of pathways regulated by PI3K and mTOR pathways. Drugs that concurrently target both PI3K and mTOR were effective at inducing apoptosis in primary osteosarcoma cell cultures in vitro in both human and mouse osteosarcoma, whereas specific PI3K or mTOR inhibitors were not effective. The results were confirmed with siRNA and small molecule approaches. Rationale combinations of specific PI3K and mTOR inhibitors could recapitulate the effect on osteosarcoma cell cultures. Conclusions: The approaches described here have identified dual inhibition of the PI3K-mTOR pathway as a sensitive, druggable target in osteosarcoma, and provide rationale for translational studies with these agents. (C) 2015 AACR.
引用
收藏
页码:3216 / 3229
页数:14
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