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Theoretical study of fast repair of DNA damage by cistanoside C and analogs: Mechanism and docking |
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| Authors: | O Sperandio BT Fan K Zakrzewska ZJ Jia RL Zheng A Panaye |
| Institution: | 1. Institut de Topologie de Dynamique des Systèmes, CNRS ESA7986 , Université Paris7-Denis-Diderot , 1, rue Guy de la Brosse, Paris , 75005 , France;2. Laboratoire de Biochimie Théorique , Institut de Biologie Physico-Chimique , 13, rue Pierre et Marie Curie, Paris , 75005 , France;3. State Key Laboratory of Applied Organic Chemistry , Lanzhou University , Lanzhou , 730000 , People's Republic of China;4. Department of Biology , Lanzhou University , Lanzhou , 730000 , People's Republic of China |
| Abstract: | Experiments show that the natural substances phenylpropanoid glycosides (PPGs) extracted from pelicularis spicata are capable of repairing DNA damaged by oxygen radicals. Based on kinetic measurements and experiments on tumor cells, a theoretical study of the interaction between PPG molecules and isolated DNA bases, as well as a DNA fragment has been performed. An interaction mechanism reported early has been refined. The docking calculations performed using junction minimization of nucleic acids (JUMNA) software showed that the PPG molecules can be docked into the minor groove of DNA and form complexes with the geometry suitable for an electron transfer between guanine radical and the ligand. Such complexes can be formed without major distortions of DNA structure and are further stabilized by the interaction with the rhamnosyl side-groups. |
| Keywords: | Phenylpropanoid Glycosides Cistanoside C And Analogs Repair Of Dna Damage Mechanism Docking |