Complexation of norfloxacin with DNA in the presence of caffeine

“…It has been reported previously that CAF and other MTX form stacking aggregates with aromatic dyes: acridine orange [82][83][84], ethidium bromide [20,81,85], 4 ,6-diamidino-2-phenylindole (DAPI) [81], methylene blue [86], anticancer drugs: doxorubicin, mitoxantrone, and daunomycin [17,24,81,87], antibacterial agent norfloxacin [88], vitamin B 2 derivative flavinmononucleotide [87], neurotoxins [36,89], and aromatic mutagens [22,35]. Some of these reports reveal in vivo effects of observed heterocomplexation, indicating that molecular complex formation between aromatic compounds can be relevant in biological systems [22,35,36,89].…”

“…It was demonstrated that CAF and other MTX can inhibit DNA binding or even induce deintercalation of aromatic ligands from DNA [20,21,84,88]. It is still discussed whether this effect results barely from the decrease in ligand availability due to its interception by MTX or can be also contributed to the reduction of binding sites on DNA available for ligands caused by MTX intercalation.…”

Heterocyclic Aromatic Amines Heterocomplexation with Biologically Active Aromatic Compounds and Its Possible Role in Chemoprevention

“…It has been reported previously that CAF and other MTX form stacking aggregates with aromatic dyes: acridine orange [82][83][84], ethidium bromide [20,81,85], 4 ,6-diamidino-2-phenylindole (DAPI) [81], methylene blue [86], anticancer drugs: doxorubicin, mitoxantrone, and daunomycin [17,24,81,87], antibacterial agent norfloxacin [88], vitamin B 2 derivative flavinmononucleotide [87], neurotoxins [36,89], and aromatic mutagens [22,35]. Some of these reports reveal in vivo effects of observed heterocomplexation, indicating that molecular complex formation between aromatic compounds can be relevant in biological systems [22,35,36,89].…”

“…It was demonstrated that CAF and other MTX can inhibit DNA binding or even induce deintercalation of aromatic ligands from DNA [20,21,84,88]. It is still discussed whether this effect results barely from the decrease in ligand availability due to its interception by MTX or can be also contributed to the reduction of binding sites on DNA available for ligands caused by MTX intercalation.…”

Heterocyclic Aromatic Amines Heterocomplexation with Biologically Active Aromatic Compounds and Its Possible Role in Chemoprevention

“…A method has been suggested to analyse the 'interceptor' and 'protector' mechanisms simultaneously in recent reports on the CAF-Antibiotic [44,64] and Vitamin-Antibiotic [50] systems. In the present work that analysis is generalised for the group of aromatic molecules, which exert their biological effect via complexation with DNA.…”

Quantitation of the molecular mechanisms of biological synergism in a mixture of DNA-acting aromatic drugs

“…Hetero-association in Drug-xanthine systems has been extensively studied by NMR, UV-vis, Fluorescence spectroscopies, titration microcalorimetry, partitioning in waterorganic mixture, molecular modelling and other techniques for the following aromatic drugs: daunomycin (DAU) [127,[133][134][135][136], doxorubicin (DOX) [33,42,127,[137][138][139], actinomycin D (AMD) and its derivatives [133,[140][141][142][143], benzene and its derivatives [122,144], novantrone/mitoxantrone (NOV) [42, 127, 135-137, 145, 146], nogalamycin (NOG) [138], norfloxacin (NOR) [135,136,147], camptothecins [139,148,149], quinoxaline [84], chloroquine [84], DAPI [150], phenothiazines [121,151,152], riboflavin [135,[153][154][155], porphyrins [156,157], acridine mutagens [53,54,124,125,[133][134]…”

Hetero-association of aromatic molecules in aqueous solution