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Merck

Targeting the HTLV-I-Regulated BATF3/IRF4 Transcriptional Network in Adult T Cell Leukemia/Lymphoma.

Cancer cell (2018-07-31)
Masao Nakagawa, Arthur L Shaffer, Michele Ceribelli, Meili Zhang, George Wright, Da Wei Huang, Wenming Xiao, John Powell, Michael N Petrus, Yibin Yang, James D Phelan, Holger Kohlhammer, Sigrid P Dubois, Hee Min Yoo, Emmanuel Bachy, Daniel E Webster, Yandan Yang, Weihong Xu, Xin Yu, Hong Zhao, Bonita R Bryant, Joji Shimono, Takashi Ishio, Michiyuki Maeda, Patrick L Green, Thomas A Waldmann, Louis M Staudt
ABSTRAKT

Adult T cell leukemia/lymphoma (ATLL) is a frequently incurable disease associated with the human lymphotropic virus type I (HTLV-I). RNAi screening of ATLL lines revealed that their proliferation depends on BATF3 and IRF4, which cooperatively drive ATLL-specific gene expression. HBZ, the only HTLV-I encoded transcription factor that is expressed in all ATLL cases, binds to an ATLL-specific BATF3 super-enhancer and thereby regulates the expression of BATF3 and its downstream targets, including MYC. Inhibitors of bromodomain-and-extra-terminal-domain (BET) chromatin proteins collapsed the transcriptional network directed by HBZ and BATF3, and were consequently toxic for ATLL cell lines, patient samples, and xenografts. Our study demonstrates that the HTLV-I oncogenic retrovirus exploits a regulatory module that can be attacked therapeutically with BET inhibitors.

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Supelco
1,25-Dihydroxyvitamin D3-13C3 (25,26,27-13C3) solution, 5 μg/mL in ethanol, ampule of 1 mL, certified reference material, Cerilliant®
Sigma-Aldrich
CPI203, ≥98% (HPLC)