posted on 2016-05-17, 00:00authored byYong Chen, Xiaoyan Wang, Wei Xiang, Lin He, Minghai Tang, Fang Wang, Taijin Wang, Zhuang Yang, Yuyao Yi, Hairong Wang, Ting Niu, Li Zheng, Lei Lei, Xiaobin Li, Hang Song, Lijuan Chen
In the present study, a series of
novel histone deacetylase (HDAC) inhibitors using the morpholinopurine
as the capping group were designed and synthesized. Several compounds
demonstrated significant HDAC inhibitory activities and antiproliferative
effects against diverse human tumor cell lines. Among them, compound 10o was identified as a potent class I and class IIb HDAC
inhibitor with good pharmaceutical profile and druglike properties.
Western blot analysis further confirmed that 10o more
effectively increased acetylated histone H3 than panobinostat (LBH-589)
and vorinostat (SAHA) at the same concentration in vitro. In in vivo efficacy evaluations of HCT116,
MV4-11, Ramos, and MM1S xenograft models, 10o showed
higher efficacy than SAHA or LBH-589 without causing significant loss
of body weight and toxicity. All the results indicated that 10o could be a suitable candidate for treatment of both solid
and hematological cancer.