A fluorescent HTS assay for phosphohydrolases based on nucleoside 5′-fluorophosphates: its application in screening for inhibitors of mRNA decapping scavenger and PDE-I

被引:20
作者
Baranowski, M. R. [1 ]
Nowicka, A. [1 ,2 ]
Jemielity, J. [2 ]
Kowalska, J. [1 ]
机构
[1] Univ Warsaw, Inst Expt Phys, Div Biophys, Fac Phys, Zwirki & Wigury 93, PL-02089 Warsaw, Poland
[2] Univ Warsaw, Ctr New Technol, Banacha 2c, PL-02097 Warsaw, Poland
关键词
AQUEOUS FLUORIDE-ION; GAMMA-BUTYROBETAINE HYDROXYLASE; CAP ANALOGS; ENZYMATIC-HYDROLYSIS; NUCLEOTIDE ANALOGS; DCPS; CELLS; PROBE; INFLAMMATION; MECHANISMS;
D O I
10.1039/c6ob00492j
中图分类号
O62 [有机化学];
学科分类号
070303 ; 081704 ;
摘要
Several nucleotide-specific phosphohydrolases can cleave P-F bonds in substrate analogues containing a fluorophosphate moiety to release fluoride ions. In this work, by employing a fluoride-sensitive molecular sensor, we harnessed this cleavage reaction to develop a fluorescence assay to screen for phosphohydrolase inhibitors. The assay is rapid, sensitive, and based on simple and synthetically available reagents. The assay was adapted to the high-throughput screening (HTS) format and its utility was demonstrated by screening an 'in-house' library of small nucleotides against two enzymes: DcpS, a metal-independent mRNA decapping pyrophosphatase of the histidine triad (HIT) family; and PDE-I, a divalent cation-dependent nuclease. Our screening results agreed with the known specificities of DcpS and PDE-I, and led to the selection of several inhibitors featuring low-micromolar IC50 values. For DcpS, we also verified the results by using an alternative method with the natural substrate. Notably, the assay presented here is the first fluorescence-based HTS-adaptable assay for DcpS, an established therapeutic target for spinal muscular atrophy. The assay should be useful for phosphohydrolase specificity profiling and inhibitor discovery, particularly in the context of DcpS and other HIT-family enzymes, which play key roles in maintaining cellular functions and have been linked to disease development.
引用
收藏
页码:4595 / 4604
页数:10
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