Improved Binding Affinity and Pharmacokinetics Enable Sustained Degradation of BCL6 In Vivo

提高结合亲和力和药代动力学可实现体内BCL6的持续降解

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作者：Huckvale,Rosemary,Harnden,Alice C,Cheung,Kwai-Ming J,Pierrat,Olivier A,Talbot,Rachel,Box,Gary M,Henley,Alan T,de Haven Brandon,Alexis K,Hallsworth,Albert E,Bright,Michael D,Akpinar,Hafize Aysin,Miller,Daniel S J,Tarantino,Dalia,Gowan,Sharon,Hayes,Angela,Gunnell,Emma A,Brennan,Alfie,Davis,Owen A,Johnson,Louise D,de Klerk,Selby,McAndrew,Craig,Le Bihan,Yann-Vaï,Meniconi,Mirco,Burke,Rosemary,Kirkin,Vladimir,van Montfort,Rob L M,Raynaud,Florence I,Rossanese,Olivia W,Bellenie,Benjamin R,Hoelder,Swen

期刊：	Journal of Medicinal Chemistry	影响因子：	6.800
时间：	2022	起止号：	2022 Jun 23;65(12):8191-8207
doi：	10.1021/acs.jmedchem.1c02175	靶点：	BCL6

Abstract

The transcriptional repressor BCL6 is an oncogenic driver found to be deregulated in lymphoid malignancies. Herein, we report the optimization of our previously reported benzimidazolone molecular glue-type degrader CCT369260 to CCT373566, a highly potent probe suitable for sustained depletion of BCL6 in vivo. We observed a sharp degradation SAR, where subtle structural changes conveyed the ability to induce degradation of BCL6. CCT373566 showed modest in vivo efficacy in a lymphoma xenograft mouse model following oral dosing.

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