An Integrated In?Vitro and In?Vivo High-Throughput Screen Identifies Treatment Leads for Ependymoma

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• 作者：Jennifer  ; M. Atkinson¹ ; Anang  ; A. Shelat² ; Angel  ; Montero Carcaboso³ ; Tanya  ; A. Kranenburg¹ ; Leggy A. Arnold² ; Nidal Boulos¹ ; Karen Wright¹ ;   ; ⁴ ; Robert  ; A. Johnson¹ ; Helen Poppleton¹ ; Kumarasamypet  ; M. Mohankumar¹ ; Clementine Fé ; au² ; Timothy Phoenix¹ ; Paul Gibson¹ ; Liqin Zhu¹ ; Yiai Tong¹ ; Chris Eden¹ ; David  ; W. Ellison⁵ ; Waldemar Priebe⁶ ; Dimpy Koul⁷ ; W.  ; K.  ; Alfred Yung⁷ ; Amar Gajjar⁴ ; Clinton  ; F. Stewart³ ; R.  ; Kiplin Guy² ;   ; ^{kip.guy@stjude.org} ; Richard  ; J. Gilbertson¹ ;   ; ⁴ ;   ; ^{richard.gilbertson@stjude.org}
• 刊名：Cancer Cell
• 出版年：2011
• 出版时间：13 September 2011
• 年：2011
• 卷：20
• 期：3
• 页码：384-399
• 全文大小：4359 K

文摘

Summary

Using a mouse model of ependymoma¡ªa chemoresistant brain tumor¡ªwe combined multicell high-throughput screening (HTS), kinome-wide binding assays, and in?vivo efficacy studies, to identify potential treatments with predicted toxicity against neural stem cells (NSC). We identified kinases within the insulin signaling pathway and centrosome cycle as regulators of ependymoma cell proliferation, and their corresponding inhibitors as potential therapies. FDA approved drugs not currently used to treat ependymoma were also identified that posses selective toxicity against ependymoma cells relative to normal NSCs both in?vitro and in?vivo, e.g., 5-fluorouracil. Our comprehensive approach advances understanding of the biology and treatment of ependymoma including the discovery of several treatment leads for immediate clinical translation.