Structural and biological characterization of new hybrid drugs joining an HDAC inhibitor to different NO-donors

被引:16
作者
Atlante, Sandra [1 ]
Chegaev, Konstantin [2 ]
Cencioni, Chiara [1 ,3 ]
Guglielmo, Stefano [2 ]
Marini, Elisabetta [2 ]
Borretto, Emily [2 ]
Gaetano, Carlo [1 ]
Fruttero, Roberta [2 ]
Spallotta, Francesco [1 ]
Lazzarato, Loretta [2 ]
机构
[1] Goethe Univ, Dept Cardiol, Div Cardiovasc Epigenet, D-60596 Frankfurt, Germany
[2] Univ Turin, Dipartimento Sci & Tecnol Farmaco, I-10125 Turin, Italy
[3] CNR, IBCN, I-00143 Rome, Italy
关键词
Histone deacetylases; Nitric oxide; Multitarget drugs; Muscle differentiation; Vasodilatation; DUCHENNE MUSCULAR-DYSTROPHY; HISTONE DEACETYLASE INHIBITOR; SUBEROYLANILIDE HYDROXAMIC ACID; NITRIC-OXIDE RELEASE; VASODILATOR ACTIVITIES; MOUSE MODEL; CELLS; CANCER; MICE; ACTIVATION;
D O I
10.1016/j.ejmech.2017.12.047
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
HDAC inhibitors and NO donors have already revealed independently their broad therapeutic potential in pathologic contexts. Here we further investigated the power of their combination in a single hybrid molecule. Nitrooxy groups or substituted furoxan derivatives were joined to the alpha-position of the pyridine ring of the selective class I HDAC inhibitor MS-275. Biochemical analysis showed that the association with the dinitrooxy compound 31 or the furoxan derivative 16 gives hybrid compounds the ability to preserve the single moiety activities. The two new hybrid molecules were then tested in a muscle differentiation assay. The hybrid compound bearing the moiety 31 promoted the formation of large myotubes characterized by highly multinucleated fibers, possibly due to a stimulation of myoblast fusion, as implicated by the strong induction of myomaker expression. Thanks to their unique biological features, these compounds may represent new therapeutic tools for cardiovascular, neuromuscular and inflammatory diseases. (C) 2017 Elsevier Masson SAS. All rights reserved.
引用
收藏
页码:612 / 625
页数:14
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