4.7 Article

Phosphate-modified analogues of m7GTP and m7Gppppm7G-Synthesis and biochemical properties

Journal

BIOORGANIC & MEDICINAL CHEMISTRY
Volume 23, Issue 17, Pages 5369-5381

Publisher

PERGAMON-ELSEVIER SCIENCE LTD
DOI: 10.1016/j.bmc.2015.07.052

Keywords

Bioorganic chemistry; Nucleotides; mRNA cap; Phosphorothioates; Boranophosphates

Funding

  1. National Science Centre (Poland) [UMO-2011/01/N/NZ1/04326, UMO-2014/12/T/NZ1/00528, UMO-2012/07/B/NZ1/00118, UMO-2013/08/A/NZ1/00866, UMO-2013/09/B/ST5/01341]
  2. Foundation for Polish Science International Ph.D. Projects Programme
  3. EU European Regional Development Fund

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The synthesis and biochemical properties of 17 new mRNA cap analogues are reported. Six of these nucleotides are m(7)GTP derivatives, whereas 11 are 'two headed' tetraphosphate dinucleotides based on a m(7)Gppppm(7)G structure. The compounds contain either a boranophosphate or phosphorothioate moiety in the nucleoside neighbouring position(s) and some of them possess an additional methylene group between beta and gamma phosphorus atoms. The compounds were prepared by divalent metal chloride-mediated coupling of an appropriate m(7)GMP analogue with a given P-1,P-2-di(1-imidazolyl) derivative. The analogues were evaluated as tools for studying cap-dependent processes in a number of biochemical assays, including determination of affinity to eukaryotic initiation factor eIF4E, susceptibility to enzymatic hydrolysis, and translational efficiency in vitro. The results indicate that modification in the phosphate chain can increase binding to cap-interacting proteins and provides higher resistance to degradation. Furthermore, modified derivatives of m(7)GTP were found to be potent inhibitors of cap-dependent translation in cell free systems. (C) 2015 Elsevier Ltd. All rights reserved.

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