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@article{837295, author = {Marini Palomeque, María Victoria and Christofis, Petros and Nováková, Olga and Kašpárková, Jana and Farrell, Nicholas and Brabec, Viktor}, article_location = {UK}, article_number = {18}, keywords = {platinum complexes; DNA; antitumor}, language = {eng}, issn = {0305-1048}, journal = {Nucleic Acids Research}, title = {Conformation, protein recognition and repair of DNA interstrand and intrastrand cross-links of antitumor trans-[PtCl2(NH3)(thiazole)]}, volume = {33}, year = {2005} }
TY - JOUR ID - 837295 AU - Marini Palomeque, María Victoria - Christofis, Petros - Nováková, Olga - Kašpárková, Jana - Farrell, Nicholas - Brabec, Viktor PY - 2005 TI - Conformation, protein recognition and repair of DNA interstrand and intrastrand cross-links of antitumor trans-[PtCl2(NH3)(thiazole)] JF - Nucleic Acids Research VL - 33 IS - 18 SP - 5819–5828 EP - 5819–5828 PB - Oxford University Press SN - 03051048 KW - platinum complexes KW - DNA KW - antitumor N2 - Replacement of one ammine in clinically ineffective trans-[PtCl2(NH3)2] (transplatin) by a planar N-heterocycle, thiazole, results in significantly enhanced cytotoxicity. Unlike "classical" cisplatin {cis-[PtCl2(NH3)2]} or transplatin, modification of DNA by this prototypical cytotoxic transplatinum complex trans-[PtCl2(NH3)(thiazole)] (trans-PtTz) leads to monofunctional and bifunctional intra or interstrand adducts in roughly equal proportions. DNA fragments containing site-specific bifunctional DNA adducts of trans-PtTz were prepared. The structural distortions induced in DNA by these adducts and their consequences for high-mobility group protein recognition, DNA polymerization and nucleotide excision repair were assessed in cell-free media by biochemical methods. Whereas monofunctional adducts of trans-PtTz behave similar to the major intrastrand adduct of cisplatin [J. Kasparkova, O. Novakova, N. Farrell and V. Brabec (2003) Biochemistry, 42, 792-800], bifunctional cross-links behave distinctly differently. The results suggest that the multiple DNA lesions available to trans-planaramine complexes may all contribute substantially to their cytotoxicity so that the overall drug cytotoxicity could be the sum of the contributions of each of these adducts. However, acquisition of drug resistance could be a relatively rare event, since it would have to entail resistance to or tolerance of multiple, structurally dissimilar DNA lesions. ER -
MARINI PALOMEQUE, María Victoria, Petros CHRISTOFIS, Olga NOVÁKOVÁ, Jana KAŠPÁRKOVÁ, Nicholas FARRELL a Viktor BRABEC. Conformation, protein recognition and repair of DNA interstrand and intrastrand cross-links of antitumor trans-[PtCl2(NH3)(thiazole)]. \textit{Nucleic Acids Research}. UK: Oxford University Press, 2005, roč.~33, č.~18, s.~5819–5828. ISSN~0305-1048.
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