Development of PI3Kγ selective inhibitors: the strategies and application

被引:0
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作者
Dong-yan Gu
Meng-meng Zhang
Jia Li
Yu-bo Zhou
Rong Sheng
机构
[1] Zhejiang University,College of Pharmaceutical Sciences
[2] State Key Laboratory of Drug Research,National Center for Drug Screening
[3] Shanghai Institute of Materia Medica,undefined
[4] Chinese Academy of Sciences,undefined
来源
关键词
PI3K; PI3Kγ inhibitors; isoform selectivity; drug development; rational drug design;
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学科分类号
摘要
The γ isoform of Class I PI3Ks (PI3Kγ) is primarily found in leukocytes and is essential for the function of myeloid cells, as it regulates the migration, differentiation, and activation of myeloid-lineage immune cells. Thus, PI3Kγ has been identified as a promising drug target for the treatment of inflammation, autoimmune disease, and immuno-oncology. Due to the high incidence of serious adverse events (AEs) associated with PI3K inhibitors, in the development of PI3Kγ inhibitors, isoform selectivity was deemed crucial. In this review, an overview of the development of PI3Kγ selective inhibitors in the past years is provided. The isoform selectivity of related drugs was achieved by different strategies, including inducing a specificity pocket by a propeller-shape structure, targeting steric differences in the solvent channel, and modulating the conformation of the Asp-Phe-Gly DFG motif, which have been demonstrated feasible by several successful cases. The insights in this manuscript may provide a potential direction for rational drug design and accelerate the discovery of PI3Kγ selective inhibitors.
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页码:238 / 247
页数:9
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