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A novel combination approach targeting an enhanced protein synthesis pathway in MYC-driven (Group 3) medulloblastoma
Journal article

A novel combination approach targeting an enhanced protein synthesis pathway in MYC-driven (Group 3) medulloblastoma

N. K. Chaturvedi, M. J. Kling, C. N. Griggs, V. Kesherwani, M. Shukla, E. M. McIntyre, S. Ray, Y. Liu, T. R. McGuire, J. G. Sharp, …
Molecular Cancer Therapeutics, Vol.19(6)
2020

Abstract

4 (4 chlorophenyl) 2,3,9 trimethyl 6h thieno[3,2 f][1,2,4]triazolo[4,3 a][1,4]diazepine 6 acetic acid tert butyl ester birabresib cisplatin dactolisib mammalian target of rapamycin Myc protein RNA temsirolimus (+)-JQ1 compound antineoplastic agent azepine derivative imidazole derivative MTOR protein, human quinoline derivative target of rapamycin kinase triazole derivative animal cell animal experiment animal model antineoplastic activity apoptosis Article cancer combination chemotherapy cancer growth cancer resistance cancer survival chemoradiotherapy controlled study down regulation drug potentiation drug targeting female G1 phase cell cycle checkpoint IC50 in vivo study medulloblastoma medulloblastoma cell line mouse mTOR signaling nonhuman priority journal protein expression protein synthesis inhibition RNA sequencing signal transduction tumor xenograft animal cell cycle cell proliferation cerebellum tumor drug effect drug screening gene expression regulation genetics human metabolism nonobese diabetic mouse pathology protein synthesis SCID mouse tumor cell culture Animals Antineoplastic Agents Azepines Cerebellar Neoplasms Gene Expression Regulation, Neoplastic Humans Imidazoles Mice Mice, Inbred NOD Mice, SCID Protein Biosynthesis Proto-Oncogene Proteins c-myc Quinolines TOR Serine-Threonine Kinases Triazoles Tumor Cells, Cultured Xenograft Model Antitumor Assays

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