?Mathematical formulae have been encoded as MathML and are displayed in this HTML version using MathJax in order to improve their display. Uncheck the box to turn MathJax off. This feature requires Javascript. Click on a formula to zoom.Abstract
Purpose
Estrogens play important roles in the pathogenesis and progression of breast cancer as well as estrogen-related diseases. Aromatase is a key enzyme in the rate-limiting step of estrogen production, in which its inhibition is one strategy for controlling estrogen levels to improve prognosis of estrogen-related cancers and diseases. Herein, a series of metal (Mn, Cu, and Ni) complexes of 8-hydroxyquinoline (8HQ) and uracil derivatives (4–9) were investigated for their aromatase inhibitory and cytotoxic activities.
Methods
The aromatase inhibition assay was performed according to a Gentest™ kit using CYP19 enzyme, wherein ketoconazole and letrozole were used as reference drugs. The cytotoxicity was tested on normal embryonic lung cells (MRC-5) using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assay.
Results
Only Cu complexes (6 and 9) exhibited aromatase inhibitory effect with IC50 0.30 and 1.7 μM, respectively. Cytotoxicity test against MRC-5 cells showed that Mn and Cu complexes (5 and 6), as well as free ligand 8HQ, exhibited activity with IC50 range 0.74–6.27 μM.
Conclusion
Cu complexes (6 and 9) were found to act as a novel class of aromatase inhibitor. Our findings suggest that these 8HQ–Cu–uracil complexes are promising agents that could be potentially developed as a selective anticancer agent for breast cancer and other estrogen-related diseases.
Introduction
Estrogens are well known as steroidal sex hormones. They not only play roles in the development and maintenance of the female reproductive system,Citation1 but also take part in the regulation of many physiological processes.Citation2–Citation7
Estrogens are synthesized from cholesterol precursorsCitation8 in a multistep process facilitated by different enzymes.Citation8 The last conversion process of C19 steroid (ie, androstenedione or testosterone) into the C18 steroid (ie, estrone or estradiol) by aromatization is considered to be the rate-limiting step of estrogen production.Citation8 This key step is facilitated by the cytochrome P450 complex.Citation9–Citation13 Abnormal estrogen productions have been found to give rise to diseases and complications. Decreased level of estrogens was found to be involved with age-related conditions.Citation2,Citation14 Moreover, estrogens facilitate the growth of certain estrogen-dependent cancers such as breastCitation15,Citation16 and endometrial cancer.Citation17–Citation19
The treatment of breast cancer is multimodal,Citation20 in which endocrine therapy is one of the possible approaches.Citation9 Aromatase inhibition is considered a promising approach to decreasing the amount of estrogen production.Citation1 Recently, aromatase inhibitors have been developed and used as anti-breast cancer agents with preferable treatment outcomes in postmenopausal women.Citation21
Aromatase inhibitors can be classified into two classes based on their chemical structures and mechanism of action.Citation9 Steroidal aromatase inhibitors competitively and covalently bind to aromatase enzyme in an irreversible fashion.Citation22 Non-steroidal aromatase inhibitors contain azoles as the privileged structureCitation1 for coordinating with heme iron (Fe) atom of aromatase enzyme leading to reversible enzyme inhibition.Citation23 Moreover, antifungal agents containing the aza-heterocycle have been shown to afford aromatase inhibitory activity.Citation24–Citation27 Such a finding indicates the significance of a heterocyclic compound bearing the N-atom as a potential aromatase inhibitor.Citation9
On the basis of existing literature, other classes of N-heterocyclic compounds, such as quinoline and pyrimidine, have drawn considerable interest. For example, 8-hydroxyquinoline (8HQ) is a quinoline derivative with potent molecular recognition and coordinating properties to metals.Citation28 It is widely used as a metal chelator as well as for analytical and separation purposes.Citation28 Recently, the anticancer activity of 8HQ-based compounds has been reported.Citation29–Citation33 Moreover, 8HQ and its derivatives exhibit a diverse range of biological activities, such as anti-neurodegenerative,Citation34,Citation35 antimicrobial,Citation36–Citation39 antimalarial,Citation40–Citation42 antioxidant,Citation30,Citation34 anti-inflammatory,Citation43 and anticancer activities.Citation44
Uracil derivatives are widely known for their anticancer properties. For example, 5-fluorouracil is a fluorinated uracil analog with anticancer activity against a wide range of cancers,Citation45,Citation46 such as head and neck,Citation47,Citation48 gastrointestinal,Citation49,Citation50 and breast cancer.Citation51–Citation53 Recently, 5-fluorouracil has been reported to be one of the most prescribed anticancer drugs.Citation54
Transition metal ions play vital roles in many biological processes. They exist in multiple valence and oxidation states,Citation55 which allows them to readily participate in electron transfer reactions and interact with negatively charged molecules.Citation55 Transition metal complexes have been reported and used as anticancer agents.Citation56,Citation57 In this regard, many beneficial effects of metal complexation have been achieved. For example, metal ions can act as chaperones in order to deliver active ligands to target sites in a selective manner. Metal complexation has been shown to improve pharmacokinetic properties such as size, charge, and lipophilicity as well as minimize toxicity.Citation58 It has also been reported that metal complexes can mimic the activity of enzymes such as superoxide dismutase.Citation58–Citation61
In efforts to increase the cancer survival rate, attention has been focused in recent years on multitasking drugs.Citation62 Such multitasking drugs are developed by combining drugs in order to improve their efficiency and minimize toxicity. This strategy aims to achieve synergistic effects exerted by each drug as well as to improve drug delivery properties by controlling the lipophilicity and size of the drug.Citation62
According to these principles of searching for novel aromatase inhibitors, this study employed 8HQ (1) and uracil derivatives including 5-nitrouracil (5Nu [2]) and 5-iodouracil (5Iu [3]) as ligands for the synthesis of mixed-ligand metal complexes 4–9 () that were subsequently tested for their aromatase inhibitory activity and cytotoxicity.
Figure 1 Chemical structures of ligands (1–3) (A) and metal complexes (4–9) (B).
Material and methods
Reagents for cell culture and assay were the following: Dulbecco’s Modified Eagle’s Medium (DMEM) and fetal bovine serum from JR Scientific Inc., Woodland, CA, USA; penicillin–streptomycin and 3(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) from Sigma-Aldrich Co (St Louis, MO, USA); and dimethyl sulfoxide (DMSO) from EMD Millipore, Billerica, MA, USA. CYP19 (a recombinant human aromatase) and O-benzyl fluorescein benzyl ester (DBF) were supplied with the BD Gentest™ kit from BD Biosciences-Discovery Labware, Woburn, MA, USA.
Tested compounds
Mixed-ligand metal complexes (4–9) were synthesized according to a previously described methodCitation30 using 1:1:1 molar ratio of 8HQ:M:5Nu (or 5Iu), where M = Ni, Mn, and Cu. The reaction was carried out in boiling methanol. Products were collected by filtration and washed four to five times with cold methanol. The compounds were confirmed by their infrared spectra, magnetic moment, and melting points.
Infrared spectra were obtained on a Perkin Elmer Spectrum System 2000 Fourier transform infrared spectrometer (Perkin Elmer Inc., Waltham, MA, USA). Magnetic moment was obtained with an MK 1 Magnetic Susceptibility Balance (serial 15257; Sherwood Scientific, Cambridge, UK). Melting points were determined on a Griffin melting point apparatus, UK and were uncorrected.
Cytotoxicity assay
Cytotoxicity was tested using normal embryonic lung cells (MRC-5). The cells were grown in DMEM medium supplemented with 100 U/mL penicillin–streptomycin and 10% fetal bovine serum. Briefly, cell lines suspended in the culture medium were seeded in a 96-well microtiter plate (3599; Corning Incorporated, Corning, NY, USA) at a density of 5×103 to 2×104 cells/well, and incubated at 37°C under a humidified atmosphere (95% air, 5% CO2) for 24 hours. An equal volume of additional medium containing either the serial dilutions of the tested compounds, positive control (doxorubicin), or negative control (DMSO) was added to the desired final concentrations. The plates were further incubated for an additional 48 hours. Cell viability was determined by staining with MTT assay.Citation63–Citation65 The MTT solution (10 μL/100 μL medium) was added to all wells of an assay and plates were incubated as described above for 2–4 hours. Subsequently, DMSO was added to dissolve the resulting formazan by sonication. The plates were read on a microplate reader (Molecular Devices LLC, Sunnyvale, CA, USA) using a test wavelength of 550 nm and a reference wavelength of 650 nm. IC50 value is defined as the drug or the compound concentration that inhibits cell growth by 50% (relative to negative control).
Aromatase inhibition assay
Aromatase inhibitory effect of metal complexes (4–9) and free ligands (1–3) was performed using the method reported by Stresser et al,Citation66 with minor modifications. This method was carried out according to the Gentest kit using CYP19 enzyme and DBF as a fluorometric substrate. DBF was dealkylated by aromatase and then hydrolyzed, providing the fluorescein product.
For the aromatase inhibition assay, 100 μL of cofactor, containing 78.4 μL of 50 mM phosphate buffer (pH 7.4); 20 μL of 20× nicotinamide adenine dinucleotide phosphate (NADPH)-generating system (26 mM NADP+, 66 mM glucose-6-phosphate, and 66 mM MgCl2); and 1.6 μL of 100 U/mL glucose-6-phosphate dehydrogenase, were pipetted into a 96-well black plate and preincubated in a water bath (37°C) for 10 minutes. The reaction was initiated by addition of 100 μL of enzyme/substrate (E/S) mixture containing 77.3 μL of 50 mM phosphate buffer (pH 7.4); 12.5 μL of 16 pmol/mL CYP19; 0.2 μL of 0.2 mM DBF; and 10 μL of 0.25 mM diluted tested sample (or 10% DMSO as a negative control or ketoconazole 52 μM or letrozole 6.6 nM as a positive control). To exclude background fluorescence of the sample, E/S was added after the reaction was terminated. After incubation at 37°C for 30 minutes, the reaction was stopped by addition of 50 μL of 2.2 N NaOH. To develop adequate signal-to-background ratio, the plate (with lid) was then incubated for 2 hours at 37°C in an air incubator. Fluorescence signal was measured using an excitation wavelength of 490 nm and emission wavelength of 530 nm with cutoff 515 nm. Percentage of inhibition (% inhibition) was calculated by EquationEquation 1(1) . Samples with % inhibition greater than 50 were further diluted and assayed in triplicate. Finally, IC50 values were determined by the plot of concentrations versus % inhibitions.
Results
Metal complexes of 8HQ–uracils (4–9) and free ligands (1–3) were investigated for their aromatase inhibitory activity and cytotoxicity toward normal embryonic lung (MRC-5) cells.
The results () revealed that only Cu complexes (6 and 9) exhibited aromatase inhibitory effect in a dose-dependent manner, with IC50 0.30 and 1.70 μM, respectively. Mn complexes (5 and 8), Ni complexes (4 and 7), and all free ligands (1–3) were shown to be inactive. The plots of concentration versus % inhibition of active complexes (6 and 9) are shown in . Cytotoxicity test of compounds 1–9 () against MRC-5 cells showed that metal complexes (5 and 6) and 8HQ exhibited the activity, with IC50 range 0.74–6.27 μM. The dose–response curves of complexes (5 and 6) are shown in .
Table 1 Aromatase inhibitory (IC50) activity of metal complexes
Table 2 Cytotoxicity (IC50) of metal complexes against MRC-5 cell line
Figure 2 Aromatase inhibitory activity of metal complexes 6 (A) and 9 (B).
Figure 3 Cytotoxicity of metal complexes (5 and 6) against MRC-5 cell line.
Discussion
One of the most commonly occurring types of cancer in women is breast cancer, which is also one of the leading causes of death in women worldwide.Citation67 Estrogens have been found to be one of the leading factors associated with the pathogenesis and progression of estrogen-dependent diseases such as breast cancerCitation1 and endometriosis.Citation8,Citation68 Aromatase is the key enzyme in the rate-limiting step of estrogen production,Citation8 and its inhibition by aromatase inhibitors is one of the approaches to treating and improving prognosis of breast cancerCitation69–Citation71 and estrogen-related diseases.Citation72–Citation74 Recently, aromatase inhibitors have become the drug of choice for estrogen-dependent cancersCitation70,Citation71 and estrogen-related diseases.Citation8,Citation72,Citation73
In this study, a series of 8HQ–uracils metal (Ni, Mn, and Cu) complexes (4–9) were synthesized and investigated for their aromatase inhibitory activity. The results showed that, among all of the tested metal complexes and free ligands, only Cu complexes (6 and 9) were found to be active. Particularly, both Cu complexes were shown to afford more potent aromatase inhibitory activity compared to the positive control, ketoconazole. This can be deduced from the IC50 values of 8HQ–Cu–5Nu (6) and 8HQ–Cu–5Iu (9), which were 8.67- and 1.5-fold less than the ketoconazole, respectively. However, such Cu complexes (6 and 9) displayed weaker aromatase inhibitory activity than letrozole, which is the inhibitor currently used against breast cancer in postmenopausal women. This suggests that Cu ion plays crucial roles in aromatase inhibition. At this point in time, the aromatase inhibition by 8HQ–Cu–uracil (5Nu and 5Iu) complexes has not been previously reported.
It is well recognized that Cu ions are considered one of the risk factors predisposing to the development of cancers facilitated by tumor angiogenesis, growth, and metastasis.Citation75–Citation77 Elevated levels of Cu ions are found in tissues and serum of patients with cancers such as breast, prostate, colon, brain, and lung cancer.Citation78–Citation81 These observations suggest that Cu could serve as one of the selective targets for the treatment of cancers.Citation82
The mechanism of action of non-steroidal aromatase inhibitors can be attributed to their lone-pair electrons as carried by heteroatoms of azole rings that interact with the Fe atom of the porphyrin ring inside the binding site of aromatase, thereby leading to the inactivation of the enzyme.Citation23 Complexation or coordination of metal ions and ligands occurs in a dynamic fashion, as the complexation or coordination of metal ions and ligands can bind in a reversible manner. The dynamic and reversible fashion of binding between metal ions and ligands can be used to explain the experimental results of metal complexes. In this study, metal complexes (4–9) were formed by metal center atoms binding with two different ligands. The possible release mechanism of metal complexes is dependent on electronegativity and metal binding affinity of ligands, as well as pKa at the site of action. Owing to the inherent nature of positively charged metal ions, they mostly occur in the bound state with negatively charged or electron donor molecules.Citation83 Thus, the metal complex may possibly dissociate into one free ligand and one positively charged metal-bound ligand.Citation39,Citation84 Moreover, different sites of metal complex dissociation give rise to different products. The site of metal complex breakage is dependent on the binding affinity between metal ions and each ligand as well as the electronegativity of the ligands.
8HQ is the investigated ligand with a potent metal chelating ability.Citation33,Citation85–Citation87 It contains lone-pair electron donors as carried by the ring’s nitrogen (N) as well as oxygen (O) atom of the OH group, which can be donated upon metal complexation. Therefore, the metal ion may possibly retain its binding with 8HQ. On the other hand, the high electronegativity property of uracil ligands (5Iu or 5Nu) can result in the release of 8HQ–metal charged complex and free uracil ligand.Citation39,Citation61 Our results suggest that Cu is required for aromatase inhibition. A plausible explanation may be attributed to the redox-reactive nature of Cu ion that gives rise to its high affinity to bind electrons and organic molecules.Citation83 Therefore, Cu ions in the released complexes (possibly 8HQ–Cu) could bind to organic compartments of aromatase enzyme, which may consequently cause conformational change of the enzyme leading to perturbation of the catalytic activity. Alternatively, the released 8HQ–Cu charged complex could interact with the target site and subsequently release 8HQ free ligand, which is a potent Fe chelator.Citation84,Citation88 Consequently, 8HQ could possibly chelate Fe contained within the aromatase enzyme, thereby leading to the inactivation of the aromatase enzyme. However, our results indicate that the free ligand 8HQ was an inactive aromatase inhibitor with 18% inhibitory effect at 12.5 μM. It is therefore reasonable to consider that the inhibitory activity requires the compound to have high absorption to the target site of action. This is clearly observed for highly lipophilic 8HQ–Cu–5Nu (5Iu) complexes (6 and 9) as compared to the free ligand 8HQ. A closer look at the structure of 8HQ–metal–uracil complexes revealed that the electronegativity of coordinating atoms of uracil ligands influenced the dissociation of the complexes. Particularly, two O atoms were used in 5Nu complexation, while two carbon (C) atoms with double bond were used in the case of 5Iu. The electronegativity of the O atom is much higher than that of the C atom. Therefore, the electron withdrawing effect of 5Nu is much stronger than that of 5Iu, leading to a higher ability of 5Nu to dissociate from the molecule of metal complex. This phenomenon could be used in explaining why the 8HQ–Cu–5Nu complex (6) exhibited more potent aromatase inhibitory effect than that of the 8HQ–Cu–5Iu complex (9). The Cu complex 6 displayed a higher IC50 value (0.74 μM) in cytotoxicity, compared to its aromatase inhibition with IC50 of 0.30 μM. Other metal (Ni and Mn) complexes (4, 5, 7 and 8), as inactive aromatase inhibitors, exerted their weak inhibitory effects at 12.5 μM in the percentage of 8%, 33%, 13%, and 27%, respectively. This may be due to the property of metal-centered atoms affecting the compounds’ interactions with the target site of action.
Selectivity is another important issue to consider in the development of anticancer drugs.Citation54 It was found that drugs with poor selectivity can cause undesirable toxicities.Citation89 Since, cancers require Cu ions for their growth and metastasis.Citation75–Citation77 For medicinal use, Cu ion could be a selective target in cancer therapy.Citation82 In addition, 8HQCitation90 and uracil derivativesCitation45 are anticancer agents.Citation88,Citation91 Particularly, 8HQ has been shown to provide substantial cytotoxic activity against the human breast cancer MCF-7 cell line.Citation35
Conclusion
Aromatase inhibitors represent one of the most promising types of agent for the treatment of estrogen-dependent cancers and diseases. A series of mixed-ligand 8HQ–uracil derivative metal complexes were synthesized and investigated for their aromatase inhibitory and cytotoxic activities. Notably, among all of the tested metal complexes, Cu complexes (6 and 9) were found to act as a novel class of aromatase inhibitor, with higher activity than the reference drug (ketoconazole) but less than the letrozole. Our findings suggest that these 8HQ–Cu–uracil complexes are promising agents that could be potentially developed as a selective anticancer agent for breast cancer and other estrogen-related diseases.
Acknowledgments
This project was supported by the research grant of Srinakharinwirot University (BE 2555) and by the Office of the Higher Education Commission, Mahidol University under the National Research Universities Initiative. We gratefully acknowledge the Chulabhorn Research Institute for performing aromatase inhibition and cytotoxic assays.
Disclosure
The authors report no conflicts of interest in this work.
References
- Brueggemeier RW Hackett JC Diaz-Cruz ES Aromatase inhibitors in the treatment of breast cancer Endocr Rev 2005 26 3 331 345 15814851
- Martín-Millán M Castañeda S Estrogens, osteoarthritis and inflammation Joint Bone Spine 2013 80 4 368 373 23352515
- Straub RH The complex role of estrogens in inflammation Endocr Rev 2007 28 5 521 574 17640948
- Cutolo M Wilder RL Different roles for androgens and estrogens in the susceptibility to autoimmune rheumatic diseases Rheum Dis Clin North Am 2000 26 4 825 839 11084946
- Pettersson K Gustafsson JA Role of estrogen receptor beta in estrogen action Annu Rev Physiol 2001 63 1 165 192 11181953
- Michet CJJr McKenna CH Elveback LR Kaslow RA Kurland LT Epidemiology of systemic lupus erythematosus and other connective tissue diseases in Rochester, Minnesota, 1950 through 1979 Mayo Clin Proc 1985 60 2 105 113 3974288
- Couse JF Korach KS Estrogen receptor null mice: what have we learned and where will they lead us? Endocr Rev 1999 20 3 358 417 10368776
- Attar E Bulun SE Aromatase and other steroidogenic genes in endometriosis: translational aspects Hum Reprod Update 2006 12 1 49 56 16123052
- Recanatini M Cavalli A Valenti P Nonsteroidal aromatase inhibitors: recent advances Med Res Rev 2002 22 3 282 304 11933021
- Simpson ER Mahendroo MS Means GD Aromatase cytochrome P450, the enzyme responsible for estrogen biosynthesis Endocr Rev 1994 15 3 342 355 8076586
- Schweikert HU Milewich L Wilson JD Aromatization of androstenedione by cultured human fibroblasts J Clin Endocrinol Metab 1976 43 4 785 795 977721
- Perel E Wilkins D Killinger DW The conversion of androstenedione to estrone, estradiol, and testosterone in breast tissue J Steroid Biochem 1980 13 1 89 94 7382486
- Miller WR Hawkins RA Forrest AP Significance of aromatase activity in human breast cancer Cancer Res 1982 42 Suppl 8 3365s 3368s 7083201
- Richelson LS Wahner HW Melton LJ Riggs BL Relative contributions of aging and estrogen deficiency to postmenopausal bone loss N Engl J Med 1984 311 20 1273 1275 6493283
- Osborne CK Steroid hormone receptors in breast cancer management Breast Cancer Res Treat 1998 51 3 227 238 10068081
- Simpson E Rubin G Clyne C The role of local estrogen biosynthesis in males and females Trends Endocrinol Metab 2000 11 5 184 188 10856920
- Yang S Fang Z Suzuki T Regulation of aromatase P450 expression in endometriotic and endometrial stromal cells by CCAAT/enhancer binding proteins (C/EBPs): decreased C/EBPbeta in endometriosis is associated with overexpression of aromatase J Clin Endocrinol Metab 2002 87 5 2336 2345 11994385
- Yamaki J Yamamoto T Okada H Aromatization of androstenedione by normal and neoplastic endometrium of the uterus J Steroid Biochem 1985 22 1 63 66 3974228
- Watanabe K Sasano H Harada N Aromatase in human endometrial carcinoma and hyperplasia. Immunohistochemical, in situ hybridization, and biochemical studies Am J Pathol 1995 146 2 491 500 7856758
- Löfgren L Wallberg B Wilking N Tamoxifen and megestrol acetate for postmenopausal breast cancer: diverging effects on liver proteins, androgens, and glucocorticoids Med Oncol 2004 21 4 309 318 15579914
- Sainsbury R The development of endocrine therapy for women with breast cancer Cancer Treat Rev 2013 39 5 507 517 23102614
- Brueggemeier RW Li PK Chen HH Moh PP Katlic NE Biochemical and pharmacological development of steroidal inhibitors of aromatase J Steroid Biochem Mol Biol 1990 37 3 379 385 2257241
- Graves PE Salhanick HA Stereoselective inhibition of aromatase by enantiomers of aminoglutethimide Endocrinology 1979 105 1 52 57 446416
- Vanden Bossche H Willemsens G Roels I R 76713 and enantiomers: selective, nonsteroidal inhibitors of the cytochrome P450-dependent oestrogen synthesis Biochem Pharmacol 1990 40 8 1707 1718 2242008
- Mason JI Murry BA Olcott M Sheets JJ Imidazole antimycotics: inhibitors of steroid aromatase Biochem Pharmacol 1985 34 7 1087 1092 3921030
- Steele RE Mellor LB Sawyer WK Wasvary JM Browne LJ In vitro and in vivo studies demonstrating potent and selective estrogen inhibition with the nonsteroidal aromatase inhibitor CGS 16949A Steroids 1987 50 1–3 147 161 2973160
- Bhatnagar AS Häusler A Schieweck K Lang M Bowman R Highly selective inhibition of estrogen biosynthesis by CGS 20267, a new non-steroidal aromatase inhibitor J Steroid Biochem Mol Biol 1990 37 6 1021 1027 2149502
- Albrecht M Fiege M Osetska O 8-Hydroxyquinolines in metallosupramolecular chemistry Coord Chem Rev 2008 252 8–9 812 824
- Lescoat G Léonce S Pierré A Gouffier L Gaboriau F Antiproliferative and iron chelating efficiency of the new bis-8-hydroxyquinoline benzylamine chelator S1 in hepatocyte cultures Chem Biol Interact 2012 195 2 165 172 22197641
- Prachayasittikul S Worachartcheewan A Pingaew R Metal complexes of uracil derivatives with cytotoxicity and superoxide scavenging activity Lett Drug Des Discov 2012 9 3 282 287
- Ding WQ Lind SE Metal ionophores – an emerging class of anticancer drugs IUBMB Life 2009 61 11 1013 1018 19859983
- Daniel KG Chen D Orlu S Cui QC Miller FR Dou QP Clioquinol and pyrrolidine dithiocarbamate complex with copper to form proteasome inhibitors and apoptosis inducers in human breast cancer cells Breast Cancer Res 2005 7 6 R897 R908 16280039
- Prachayasittikul V Prachayasittikul S Ruchirawat S Prachayasittikul V 8-Hydroxyquinolines: a review of their metal chelating properties and medicinal applications Drug Des Devel Ther 2013 7 1157 1178
- Zheng H Gal S Weiner LM Novel multifunctional neuroprotective iron chelator-monoamine oxidase inhibitor drugs for neurodegenerative diseases: in vitro studies on antioxidant activity, prevention of lipid peroxide formation and monoamine oxidase inhibition J Neurochem 2005 95 1 68 78 16181413
- Zheng H Weiner LM Bar-Am O Design, synthesis, and evaluation of novel bifunctional iron-chelators as potential agents for neuroprotection in Alzheimer’s, Parkinson’s, and other neurodegenerative diseases Bioorg Med Chem 2005 13 3 773 783 15653345
- Pavlov A Takuchev N Georgieva N Drug design by regression analyses of newly synthesized derivatives of 8-quinolinol Biotechnology & Biotechnological Equipment 2012 26 1 164 169
- Jeon JH Lee CH Lee HS Antimicrobial activities of 2-methyl-8-hydroxyquinoline and its derivatives against human intestinal bacteria Journal of the Korean Society for Applied Biological Chemistry 2009 52 2 202 205
- Ahmed SM Ismail DA Synthesis and biological activity of 8-hydroxyquinoline and 2-hydroxypyridine quaternary ammonium salts J Surfactants Deterg 2008 11 3 231 235
- Srisung S Suksrichavalit T Prachayasittikul S Ruchirawat S Prachayasittikul V Antimicrobial activity of 8-hydroxyquinoline and transition metal complexes International Journal of Pharmacology 2013 9 2 170 175
- Strobl JS Seibert CW Li Y Inhibition of Toxoplasma gondii and Plasmodium falciparum infections in vitro by NSC3852, a redox active antiproliferative and tumor cell differentiation agent J Parasitol 2009 95 1 215 223 18837587
- Scheibel LW Adler A Antimalarial activity of selected aromatic chelators. III. 8-Hydroxyquinolines (oxines) substituted in positions 5 and 7, and oxines annelated in position 5,6 by an aromatic ring Mol Pharmacol 1982 22 1 140 144 6811856
- Madrid PB Sherrill J Liou AP Weisman JL Derisi JL Guy RK Synthesis of ring-substituted 4-aminoquinolines and evaluation of their antimalarial activities Bioorg Med Chem Lett 2005 15 4 1015 1018 15686903
- Kim YH Woo KJ Lim JH 8-Hydroxyquinoline inhibits iNOS expression and nitric oxide production by down-regulating LPS-induced activity of NF-kappaB and C/EBPbeta in Raw 264.7 cells Biochem Biophys Res Commun 2005 329 2 591 597 15737626
- Yamato M Hashigaki K Yasumoto Y Synthesis and antitumor activity of tropolone derivatives. 6. Structure-activity relationships of antitumor-active tropolone and 8-hydroxyquinoline derivatives J Med Chem 1987 30 10 1897 1900 3116257
- Álvarez P Marchal JA Boulaiz H 5-Fluorouracil derivatives: a patent review Expert Opin Ther Pat 2012 22 2 107 123 22329541
- Marchal JA Boulaiz H Rodríguez-Serrano F 5-fluorouracil derivatives induce differentiation mediated by tubulin and HLA class I modulation Med Chem 2007 3 3 233 239 17504194
- Adelstein DJ Li Y Adams GL An intergroup phase III comparison of standard radiation therapy and two schedules of concurrent chemoradiotherapy in patients with unresectable squamous cell head and neck cancer J Clin Oncol 2003 21 1 92 98 12506176
- Adelstein DJ Saxton JP Lavertu P Maximizing local control and organ preservation in stage IV squamous cell head and neck cancer with hyperfractionated radiation and concurrent chemotherapy J Clin Oncol 2002 20 5 1405 1410 11870186
- Moertel CG Childs DSJr Reitemeier RJ Colby MYJr Holbrook MA Combined 5-fluorouracil and supervoltage radiation therapy of locally unresectable gastrointestinal cancer Lancet 1969 294 7626 865 867 4186452
- Seitz JF Milan C Giovannini M Fondation Française de Cancérologie Digestive Groupe Digestif de la Fédération Nationale des Centres de Lutte Contre le Cancer Concurrent concentrated radio-chemotherapy of epidermoid cancer of the esophagus. Long-term results of a phase II national multicenter trial in 122 non-operable patients (FFCD 8803) Gastroenterol Clin Biol 2000 24 2 201 210 French 12687962
- Saniger E Campos JM Entrena A Medium benzene-fused oxacycles with the 5-fluorouracil moiety: synthesis, antiproliferative activities and apoptosis induction in breast cancer cells Tetrahedron 2003 59 29 5457 5467
- Espinosa A Marchal JA Aránega A Gallo MA Aiello S Campos J Antitumoural properties of benzannelated seven-membered 5-fluorouracil derivatives and related open analogues. Molecular markers for apoptosis and cell cycle dysregulation Farmaco 2005 60 2 91 97 15752467
- Saniger E Campos JM Entrena A Neighbouring-group participation as the key step in the reactivity of acyclic and cyclic salicyl-derived O,O-acetals with 5-fluorouracil. Antiproliferative activity, cell cycle dysregulation and apoptotic induction of new O,N-acetals against breast cancer cells Tetrahedron 2003 59 40 8017 8026
- Mazzaferro S Bouchemal K Ponchel G Oral delivery of anticancer drugs II: the prodrug strategy Drug Discov Today 2013 18 1–2 93 98 22960308
- Rafique S Idrees M Nasim A Akbar H Athar A Transition metal complexes as potential therapeutic agents Biotechnology and Molecular Biology Reviews 2010 5 2 38 45
- Jackson A Davis J Pither RJ Rodger A Hannon MJ Estrogen-derived steroidal metal complexes: agents for cellular delivery of metal centers to estrogen receptor-positive cells Inorg Chem 2001 40 16 3964 3973 11466055
- Brow JM Pleatman CR Bierbach U Cytotoxic acridinylthiourea and its platinum conjugate produce enzyme-mediated DNA strand breaks Bioorg Med Chem Lett 2002 12 20 2953 2955 12270182
- Hambley TW Developing new metal-based therapeutics: challenges and opportunities Dalton Trans 2007 43 4929 4937 17992277
- Suksrichavalit T Prachayasittikul S Nantasenamat C Isarankura-Na-Ayudhya C Prachayasittikul V Copper complexes of pyridine derivatives with superoxide scavenging and antimicrobial activities Eur J Med Chem 2009 44 8 3259 3265 19375194
- Suksrichavalit T Prachayasittikul S Piacham T Isarankura-Na-Ayudhya C Nantasenamat C Prachayasittikul V Copper complexes of nicotinic-aromatic carboxylic acids as superoxide dismutase mimetics Molecules 2008 13 12 3040 3056 19078847
- Pingaew R Worachartcheewan A Prachayasittikul V Prachayasittikul S Ruchirawat S Prachayasittikul V Transition metal complexes of 8 aminoquinoline-5-substituted uracils with antioxidative and cytotoxic a ctivities Lett Drug Des Discov 2013 10 9 859 864
- Castonguay A Doucet C Juhas M Maysinger D New ruthenium(II)-letrozole complexes as anticancer therapeutics J Med Chem 2012 55 20 8799 8806 22991922
- Mosmann T Rapid colorimetric assay for cellular growth and survival: application to proliferation and cytotoxicity assays J Immunol Methods 1983 65 1–2 55 63 6606682
- Carmichael J DeGraff WG Gazdar AF Minna JD Mitchell JB Evaluation of a tetrazolium-based semiautomated colorimetric assay: assessment of chemosensitivity testing Cancer Res 1987 47 4 936 942 3802100
- Tominaga H Ishiyama M Ohseto F A water-soluble tetrazolium salt useful for colorimetric cell viability assay Analytical Communications 1999 36 2 47 50
- Stresser DM Turner SD McNamara J A High-throughput screen to identify inhibitors of aromatase (CYP19) Anal Biochem 2000 284 2 427 430 10964434
- Jemal A Siegel R Ward E Cancer statistics, 2008 CA Cancer J Clin 2008 58 2 71 96 18287387
- Bulun SE Noble LS Takayama K Endocrine disorders associated with inappropriately high aromatase expression J Steroid Biochem Mol Biol 1997 61 3–6 133 139 9365182
- Dowsett M Cuzick J Ingle J Meta-analysis of breast cancer outcomes in adjuvant trials of aromatase inhibitors versus tamoxifen J Clin Oncol 2010 28 3 509 518 19949017
- Mouridsen H Gershanovich M Sun Y Superior efficacy of letrozole versus tamoxifen as first-line therapy for postmenopausal women with advanced breast cancer: results of a phase III study of the international letrozole breast cancer group J Clin Oncol 2001 19 10 2596 2606 11352951
- Paridaens RJ Dirix LY Beex LV Phase III study comparing exemestane with tamoxifen as first-line hormonal treatment of metastatic breast cancer in postmenopausal women: the European Organisation for Research and Treatment of Cancer Breast Cancer Cooperative Group J Clin Oncol 2008 26 30 4883 4890 18794551
- Shippen ER West WJJr Successful treatment of severe endometriosis in two premenopausal women with an aromatase inhibitor Fertil Steril 2004 81 5 1395 1398 15136110
- Takayama K Zeitoun K Gunby RT Sasano H Carr BR Bulun SE Treatment of severe postmenopausal endometriosis with an aromatase inhibitor Fertil Steril 1998 69 4 709 713 9548162
- Amsterdam LL Gentry W Jobanputra S Wolf M Rubin SD Bulun SE Anastrazole and oral contraceptives: a novel treatment for endometriosis Fertil Steril 2005 84 2 300 304 16084868
- Brewer GJ Copper control as an antiangiogenic anticancer therapy: lessons from treating Wilson’s disease Exp Biol Med (Maywood) 2001 226 7 665 673 11444102
- Theophanides T Anastassopoulou J Copper and carcinogenesis Crit Rev Oncol Hematol 2002 42 1 57 64 11923068
- Daniel KG Harbach RH Guida WC Dou QP Copper storage diseases: Menkes, Wilsons, and cancer Front Biosci 2004 9 2652 2662 15358588
- Nayak SB Bhat VR Upadhyay D Udupa SL Copper and ceruloplasmin status in serum of prostate and colon cancer patients Indian J Physiol Pharmacol 2003 47 1 108 110 12708132
- Huang YL Sheu JY Lin TH Association between oxidative stress and changes of trace elements in patients with breast cancer Clin Biochem 1999 32 2 131 136 10211630
- Rizk SL Sky-Peck HH Comparison between concentrations of trace elements in normal and neoplastic human breast tissue Cancer Res 1984 44 11 5390 5394 6488192
- Turecký L Kalina P Uhlíková E Námerová S Križko J Serum ceruloplasmin and copper levels in patients with primary brain tumors Klin Wochenschr 1984 62 4 187 189 6323815
- Chen D Cui QC Yang H Clioquinol, a therapeutic agent for Alzheimer’s disease, has proteasome-inhibitory, androgen receptor-suppressing, apoptosis-inducing, and antitumor activities in human prostate cancer cells and xenografts Cancer Res 2007 67 4 1636 1644 17308104
- Bleackley MR Macgillivray RTA Transition metal homeostasis: from yeast to human disease Biometals 2011 24 5 785 809 21479832
- Anjaneyulu Y Rao RP Swamy RY Eknath A Rao KN In vitro antimicrobial-activity studies on the mixed ligand complexes of Hg(II) with 8-hydroxyquinoline and salicylic acids Proceedings of the Indian Academy of Sciences – Chemical Sciences 1982 91 2 157 163
- Pollak Y Mechlovich D Amit T Effects of novel neuroprotective and neurorestorative multifunctional drugs on iron chelation and glucose metabolism J Neural Transm 2013 120 1 37 48 22446839
- Crouch PJ Barnham KJ Therapeutic redistribution of metal ions to treat Alzheimer’s disease Acc Chem Res 2012 45 9 1604 1611 22747493
- Cherny RA Atwood CS Xilinas ME Treatment with a copper-zinc chelator markedly and rapidly inhibits beta-amyloid accumulation in Alzheimer’s disease transgenic mice Neuron 2001 30 3 665 676 11430801
- Bush AI Tanzi RE Therapeutics for Alzheimer’s disease based on the metal hypothesis Neurotherapeutics 2008 5 3 421 432 18625454
- Malet-Martino M Martino R Clinical studies of three oral prodrugs of 5-fluorouracil (Capecitabine, UFT, S-1): a review Oncologist 2002 7 4 288 323 12185293
- Ding WQ Liu B Vaught JL Yamauchi H Lind SE Anticancer activity of the antibiotic clioquinol Cancer Res 2005 65 8 3389 3395 15833873
- Shaw AY Chang CY Hsu MY Synthesis and structure-activity relationship study of 8-hydroxyquinoline-derived Mannich bases as anticancer agents Eur J Med Chem 2010 45 7 2860 2867 20359788