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@article{792859, author = {Kašpárková, Jana and Novaková, Olga and Marini Palomeque, María Victoria and Najajreh, Yousef and Gibson, Dan and Perez, JoseandManuel and Brabec, Viktor}, article_location = {Bethesda, USA}, article_number = {48}, keywords = {cisplatin; platinum complexes; DNA; antitumor}, language = {eng}, issn = {0021-9258}, journal = {Journal of Biological Chemistry}, title = {Activation of trans geometry in bifunctional mononuclear platinum complexes by a piperidine ligand. Mechanistic studies on antitumor action}, volume = {278}, year = {2003} }
TY - JOUR ID - 792859 AU - Kašpárková, Jana - Novaková, Olga - Marini Palomeque, María Victoria - Najajreh, Yousef - Gibson, Dan - Perez, Jose-Manuel - Brabec, Viktor PY - 2003 TI - Activation of trans geometry in bifunctional mononuclear platinum complexes by a piperidine ligand. Mechanistic studies on antitumor action JF - Journal of Biological Chemistry VL - 278 IS - 48 SP - 47516-47525 EP - 47516-47525 PB - Amer. Soc. Biochem. Mol. Biol. SN - 00219258 KW - cisplatin KW - platinum complexes KW - DNA KW - antitumor N2 - A paradigm for the structure-pharmacological activity relationship of bifunctional platinum antitumor drugs is that the trans isomer of antitumor cisplatin (transplatin) is clinically ineffective. To this end, however, several new complexes of the trans structure have been identified that exhibit cytotoxicity in tumor cells that is even better than that of the analogous cis isomers. We reported recently (Kasparkova, J., Marini, V., Najajreh, Y., Gibson, D., and Brabec, V. (2003) Biochemistry 42, 6321-6332) that the replacement of one ammine ligand by the heterocyclic ligand, such as piperidine, piperazine, or 4-picoline in the molecule of transplatin resulted in a radical enhancement of its cytotoxicity. We examined oligodeoxyribonucleotide duplexes bearing a site-specific cross-link of the transplatin analogue containing the piperidine ligand by biochemical methods. The results indicate that in contrast to transplatin, trans-(PtCl2(NH3)(piperidine)) forms stable 1,3-intrastrand cross-links in double-helical DNA that distort DNA and are not readily removed from DNA by nucleotide excision repair system. Hence, the intrastrand cross-links of trans-(PtCl2(NH3)(piperidine)) could persist for a sufficiently long time, potentiating its toxicity toward tumor cells. trans-(PtCl2(NH3)(piperidine)) also forms in DNA minor interstrand cross-links that are similar to those of transplatin so that these adducts appear less likely candidates for genotoxic lesion responsible for antitumor effects of trans-(PtCl2(NH3)(piperidine)). Hence, the role of structurally unique intrastrand cross-links in the anti-tumor effects of transplatin analogues in which one ammine group is replaced by a heterocyclic ligand may predominate. ER -
KAŠPÁRKOVÁ, Jana, Olga NOVAKOVÁ, María Victoria MARINI PALOMEQUE, Yousef NAJAJREH, Dan GIBSON, Jose-Manuel PEREZ and Viktor BRABEC. Activation of trans geometry in bifunctional mononuclear platinum complexes by a piperidine ligand. Mechanistic studies on antitumor action. \textit{Journal of Biological Chemistry}. Bethesda, USA: Amer. Soc. Biochem. Mol. Biol., 2003, vol.~278, No~48, p.~47516-47525. ISSN~0021-9258.
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