Medicinal Chemistry, Oncology, IMED Biotech Unit, AstraZeneca, Cambridge Science Park, Unit 310 Darwin Building, Cambridge CB4 0WG, United Kingdom.
Bioscience, Oncology, IMED Biotech Unit, AstraZeneca, Boston, 35 Gatehouse Drive, Waltham, MA 02451, United States.
Bioorg Med Chem. 2018 Feb 15;26(4):913-924. doi: 10.1016/j.bmc.2018.01.008. Epub 2018 Jan 17.
We have developed a series of orally efficacious IRAK4 inhibitors, based on a scaffold hopping strategy and using rational structure based design. Efforts to tackle low permeability and high efflux in our previously reported pyrrolopyrimidine series (Scott et al., 2017) led to the identification of pyrrolotriazines which contained one less formal hydrogen bond donor and were intrinsically more lipophilic. Further optimisation of substituents on this pyrrolotriazine core culminated with the discovery of 30 as a promising in vivo probe to assess the potential of IRAK4 inhibition for the treatment of MyD88 mutant DLBCL in combination with a BTK inhibitor. When tested in an ABC-DLBCL model with a dual MyD88/CD79 mutation (OCI-LY10), 30 demonstrated tumour regressions in combination with ibrutinib.
我们基于构象跳跃策略和合理的基于结构的设计,开发了一系列口服有效的 IRAK4 抑制剂。为了解决我们之前报道的吡咯并嘧啶系列中低通透性和高外排的问题(Scott 等人,2017),我们鉴定了吡咯并三嗪,它含有一个较少的形式氢键供体,并且内在地更亲脂性。对该吡咯并三嗪核心上取代基的进一步优化,最终发现 30 是一种有前途的体内探针,可用于评估 IRAK4 抑制联合 BTK 抑制剂治疗 MyD88 突变 DLBCL 的潜力。当在具有双重 MyD88/CD79 突变(OCI-LY10)的 ABC-DLBCL 模型中进行测试时,30 与伊布替尼联合显示出肿瘤消退。
