Effects of cytotoxic cis- and trans-diammine monochlorido platinum(II) complexes on selenium-dependent redox enzymes and DNA

Lemmerhirt, H.; Behnisch, S.; Bodtke, A.; Lillig, Ch.H.; Pazderová, L.; Kašpárková, Jana; Brabec, Viktor; Bednarski, P.J.

doi:https://dx.doi.org/10.1016/j.jinorgbio.2017.10.011

Počet záznamů: 1

Effects of cytotoxic cis- and trans-diammine monochlorido platinum(II) complexes on selenium-dependent redox enzymes and DNA

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SYSNO ASEP	0486052
Druh ASEP	J - Článek v odborném periodiku
Zařazení RIV	J - Článek v odborném periodiku
Poddruh J	Článek ve WOS
Název	Effects of cytotoxic cis- and trans-diammine monochlorido platinum(II) complexes on selenium-dependent redox enzymes and DNA
Tvůrce(i)	Lemmerhirt, H. (DE) Behnisch, S. (DE) Bodtke, A. (DE) Lillig, Ch.H. (DE) Pazderová, L. (CZ) Kašpárková, Jana (BFU-R)_{RID, ORCID} Brabec, Viktor (BFU-R)_{RID, ORCID} Bednarski, P.J. (DE)
Celkový počet autorů	8
Zdroj.dok.	Journal of Inorganic Biochemistry. - : Elsevier - ISSN 0162-0134 Roč. 178, JAN2018 (2018), s. 94-105
Poč.str.	12 s.
Forma vydání	Tištěná - P
Jazyk dok.	eng - angličtina
Země vyd.	US - Spojené státy americké
Klíč. slova	glutathione-peroxidase ; thioredoxin reductase
Vědní obor RIV	CE - Biochemie
Obor OECD	Biochemistry and molecular biology
CEP	GA17-09436S GA ČR - Grantová agentura ČR
Institucionální podpora	BFU-R - RVO:68081707
UT WOS	000419999600010
DOI	10.1016/j.jinorgbio.2017.10.011
Anotace	Here we present the preparation of 14 pairs of cis-and trans-diammine monochlorido platinum(II) complexes, coordinated to heterocycles (i.e., imidazole, 2-methylimidazole and pyrazole) and linked to various acylhydrazones, which were designed as potential inhibitors of the selenium-dependent enzymes glutathione peroxidase 1 (GPx-1) and thioredoxin reductase 1 (TrxR-1). However, no inhibition of bovine GPx-1 and only weak inhibition of murine TrxR-1 was observed in in vitro assays. Nonetheless, the cis configured diammine monochlorido Pt(II) complexes exhibited cytotoxic and apoptotic properties on various human cancer cell lines, whereas the trans configured complexes generally showed weaker potency with a few exceptions. On the other hand, the trans complexes were generally more likely to lack cross-resistance to cisplatin than the cis analogues. Platinum was found bound to the nuclear DNA of cancer cells treated with representative Pt complexes, suggesting that DNA might be a possible target. Thus, detailed in vitro binding experiments with DNA were conducted. Interactions of the compounds with calf thymus DNA were investigated, including Pt binding kinetics, circular dichroism (CD) spectral changes, changes in DNA melting temperatures, unwinding of supercoiled plasmids and ethidium bromide displacement in DNA. The CD results indicate that the most active cis configured pyrazole-derived complex causes unique structural changes in the DNA compared to the other complexes as well as to those caused by cisplatin, suggesting a denaturation of the DNA structure. This may be important for the antiproliferative activity of this compound in the cancer cells.
Pracoviště	Biofyzikální ústav
Kontakt	Jana Poláková, polakova@ibp.cz, Tel.: 541 517 244
Rok sběru	2018

Počet záznamů: 1