Design of Novel 3-Pyrimidinylazaindole CDK2/9 Inhibitors with Potent In Vitro and In Vivo Antitumor Efficacy in a Triple-Negative Breast Cancer Model

被引:42
|
作者
Singh, Umed [1 ]
Chashoo, Gousia [2 ]
Khan, Sameer U. [2 ]
Mahajan, Priya [3 ]
Nargotra, Amit [3 ]
Mahajan, Girish [2 ]
Singh, Amarinder [4 ]
Sharma, Anjna [4 ]
Mintoo, Mubashir J. [2 ]
Guru, Santosh Kumar [2 ]
Aruri, Hariprasad [1 ]
Thatikonda, Thanusha [1 ]
Sahu, Promod [4 ]
Chibber, Pankaj [4 ]
Kumar, Vikas [5 ]
Mir, Sameer A. [2 ]
Bharate, Sonali S. [5 ]
Madishetti, Sreedhar [4 ]
Nandi, Utpal [4 ]
Singh, Gurdarshan [4 ]
Mondhe, Dilip Manikrao [2 ]
Bhushan, Shashi [2 ,6 ]
Malik, Fayaz [2 ]
Mignani, Serge [1 ,7 ]
Vishwakarma, Ram A. [1 ]
Singh, Parvinder Pal [1 ]
机构
[1] Acad Sci & Innovat Res, Indian Inst Integrat Med, Med Chem Div, CSIR, Canal Rd, Jammu 180001, Jammu & Kashmir, India
[2] Acad Sci & Innovat Res, Indian Inst Integrat Med, Canc Pharmacol Div, CSIR, Canal Rd, Jammu 180001, Jammu & Kashmir, India
[3] Acad Sci & Innovat Res, Indian Inst Integrat Med, Discovery Informat, CSIR, Canal Rd, Jammu 180001, Jammu & Kashmir, India
[4] Acad Sci & Innovat Res, Indian Inst Integrat Med, Pharmacokinet & Pharmacodynam Div, CSIR, Canal Rd, Jammu 180001, Jammu & Kashmir, India
[5] Acad Sci & Innovat Res, Indian Inst Integrat Med, Preformulat Div, CSIR, Canal Rd, Jammu 180001, Jammu & Kashmir, India
[6] Indian Pharmacopoeia Commiss, Sect 23, Raj Nagar 201002, Ghaziabad, India
[7] Univ Paris 05, PRES Sorbonne Paris Cite, CNRS UMR 860, Lab Chim & Biochim Pharmacol & Toxicol, 45 Rue St Peres, F-75006 Paris, France
来源
JOURNAL OF MEDICINAL CHEMISTRY | 2017年 / 60卷 / 23期
关键词
DEPENDENT KINASE INHIBITOR; DISCOVERY; FLAVOPIRIDOL; MERIOLINS; TARGETS; PROTEIN; CDK4;
D O I
10.1021/acs.jmedchem.7b00663
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
In the present study, a novel series of 3-pyrimidinylazaindoles were designed and synthesized using a bioinformatics strategy as cyclin-dependent kinases CDK2 and CDK9 inhibitors, which play critical roles in the cell cycle control and regulation of cell transcription. The present approach gives new dimensions to the existing SAR and opens a new opportunity for the lead optimizations from comparatively inexpensive starting materials. The study led to the identification of the alternative lead candidate 4ab with a nanomolar potency against CDK2 and CDK9 and potent antiproliferative activities against a panel of tested tumor cell lines along with a better safety ratio of similar to 33 in comparison to reported leads. In addition, the identified lead 4ab demonstrated a good solubility and an acceptable in vivo PK profile. The identified lead 4ab showed an in vivo efficacy in mouse triple-negative breast cancer (TNBC) syngeneic models with a TGI (tumor growth inhibition) of 90% without any mortality growth inhibition in comparison to reported leads.
引用
收藏
页码:9470 / 9489
页数:20
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