Enhancement of antiproliferative activity by phototautomerization of anthrylphenols

Kralj, Marijeta; Uzelac, Lidija; Wang, Yu-Hsuan; Wan, Peter; Tireli, Martina; Mlinarić-Majerski, Kata; Piantanida, Ivo; Basarić, Nikola

doi:10.1039/c5pp00099h

Pregled bibliografske jedinice broj: 756018

Enhancement of antiproliferative activity by phototautomerization of anthrylphenols

Kralj, Marijeta; Uzelac, Lidija; Wang, Yu-Hsuan; Wan, Peter; Tireli, Martina; Mlinarić-Majerski, Kata; Piantanida, Ivo; Basarić, Nikola

Enhancement of antiproliferative activity by phototautomerization of anthrylphenols // Photochemical & photobiological sciences, 14 (2015), 6; 1082-1092 doi:10.1039/c5pp00099h (međunarodna recenzija, članak, znanstveni)

CROSBI ID: 756018 Za ispravke kontaktirajte CROSBI podršku putem web obrasca

Naslov
Enhancement of antiproliferative activity by phototautomerization of anthrylphenols

Autori
Kralj, Marijeta ; Uzelac, Lidija ; Wang, Yu-Hsuan ; Wan, Peter ; Tireli, Martina ; Mlinarić-Majerski, Kata ; Piantanida, Ivo ; Basarić, Nikola

Izvornik
Photochemical & photobiological sciences (1474-905X) 14 (2015), 6; 1082-1092

Vrsta, podvrsta i kategorija rada
Radovi u časopisima, članak, znanstveni

Ključne riječi
anthracenes ; antiproliferative activity ; excited state proton trasnfer ; quinone methides

Sažetak
Antiproliferative investigation has been conducted on 3 human cancer cell lines HCT 116 (colon), MCF-7 (breast), and H 460 (lung), on a series of 4 anthrylphenols in dark, and upon exposure to light (350 nm). 9-(2-Hydroxyphenyl)anthracene (1) moderately inhibits the proliferation, but the irradiation considerably enhances the effect. The other investigated anthracenes 4-6 exhibit antiproliferative activity in dark, which was not enhanced upon irradiation. The enhancement of the antiproliferative effect on irradiation of 1 was rationalized as being due to the formation of quinone methide (QM 2) by excited state proton transfer. QM 2 acts as an electrophilic species capable of reacting with biological molecules. Although QM 2 reacts with nucleotides, adducts could not be isolated. On the contrary, cysteine adduct 8 has been isolated and characterized, whereas adducts with glycine, serine and tripeptide glutathione have been characterized by MS. Non-covalent binding of 1 to DNA and bovine serum albumin was demonstrated by UV-vis, fluorescence and CD spectroscopy. However, straightforward conclusion about the DNA or ptotein alkylating (damaging) ability of 2 could not be drawn. The results obtained by the irradiations of 1 in the presence of DNA, amino acids and peptides, the cell cycle perturbation analysis, and in vitro translation of GFP suggest that the effect is not only due to the damage of DNA but also the impact on the cellular proteins. Considering that up to date all QM agents were assumed to target dominantly DNA, this is an important finding with impact to the further development of anticancer agents based on QMs.

Izvorni jezik
Engleski

Znanstvena područja
Kemija, Temeljne medicinske znanosti

POVEZANOST RADA

Projekti:
098-0982464-2514 - Uloga različitih mehanizama odgovora stanica na terapiju oštećenjem DNA (Kralj, Marijeta, MZOS ) ( CroRIS)
098-0982914-2918 - Dizajn, sinteza i ispitivanje interakcija malih molekula s DNA, RNA i proteinima (Piantanida, Ivo, MZOS ) ( CroRIS)
02.05/25 - Fotokemija policikličkih molekula: od istraživanja mehanizama reakcije do novih lijekova i medicinskih primjena (Basarić, Nikola, HRZZ ) ( CroRIS)
HRZZ-IP-2013-11-5660 - Mulitidisciplinarni pristup otkriću lijekova s ciljanim djelovanjem na matične stanice tumora – uloga transporta kalija (MultiCaST) (Kralj, Marijeta, HRZZ - 2013-11) ( CroRIS)