Some inhibitors of purine nucleoside phosphorylase
Author(s) -
L.H. Pogosian,
Л. С. Нерсесова,
M G Gazariants,
Z S Mkrtchian,
J.I. Akopian
Publication year - 2011
Publication title -
biomeditsinskaya khimiya
Language(s) - English
Resource type - Journals
eISSN - 2310-6972
pISSN - 2310-6905
DOI - 10.18097/pbmc20115705526
Subject(s) - purine nucleoside phosphorylase , phosphorolysis , purine , nucleoside , guanine , biochemistry , chemistry , purine analogue , purine metabolism , nucleotide , enzyme , nucleic acid , transplantation , nucleotide salvage , nucleoside analogue , biology , medicine , gene
Purine nucleoside phosphorylase (PNP) catalyzes reversible phosphorolysis of purine deoxy- and ribonucleosides with formation (d)Rib-1-P and corresponding bases. PNP plays a leading role in the cell metabolism of nucleosides and nucleotides, as well as in maintaining the immune status of an organism. The major aim of the majority of studies on the PNP is the detection of highly effective inhibitors of this enzyme, derivatives of purine nucleosides used in medicine as immunosuppressors, which are essential for creating selective T-cell immunodeficiency in a human body for organ and tissue transplantation.The present work is devoted to the study of the effects of some synthetic derivatives of purine nucleosides on activity of highly purified PNP from rabbit spleen and also from human healthy and tumor tissues of lung and kidneys. Purine nucleoside analogues modified at various positions of both the heterocyclic base and carbohydrate residues have been investigated. Several compounds, including 8-mercapto-acyclovir, 8-bromo-9-(3,4-hydroxy-butyl)guanine, which demonstrated potent PNP inhibition, could be offered for subsequent study as immunosuppressors during organ and tissue transplantation.
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