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Merck
  • Looking for new pyrimidine acyclic nucleotide analogues designed for phosphorylation by human UMP-CMP kinase.

Looking for new pyrimidine acyclic nucleotide analogues designed for phosphorylation by human UMP-CMP kinase.

Nucleosides, nucleotides & nucleic acids (2007-12-11)
Dimitri Topalis, Hiroki Kumamoto, Julie A C Alexandre, Laurence Dugué, Sylvie Pochet, Sabine Berteina-Raboin, Luigi A Agrofoglio, Dominique Deville-Bonne
摘要

Human UMP-CMP kinase is involved in the phosphorylation of nucleic acid precursors and also in the activation of antiviral analogues including cidofovir, an acyclic phosphonate compound that mimicks dCMP and shows a broad antiviral spectrum. The binding of ligands to the enzyme was here investigated using a fluorescent probe and a competitive titration assay. At the acceptor site, the enzyme was found to accommodate any base, purine and pyrimidine, including thymidine. A method for screening analogues based on their affinity for the UMP binding site was developed. The affinities of uracil vinylphosphonate derivatives modified in the 5 position were found similar to (d)UMP and (d)CMP and improved when compared to cidofovir.

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Sigma-Aldrich
乙烯膦酸, 97%
Sigma-Aldrich
胞苷 5′-二磷酸 钠盐 水合物, from yeast, ≥95%
Sigma-Aldrich
乙烯膦酸, ≥90% (T)
Sigma-Aldrich
2′-脱氧胞苷-5′-二磷酸盐 钠盐, ≥96%