Selective Hypoxia‐Cytotoxin 7‐Fluoro‐2‐Aminophenazine 5,10‐Dioxide: Toward “Candidate‐to‐Drug” Stage in the Drug‐Development Pipeline

Dávila, Belén; Sánchez, Carina; Fernández, Marcelo; Cerecetto, Hugo; Lecot, Nicole; Cabral, Pablo; Glisoni, Romina Julieta; González, Mercedes

doi:10.1002/slct.201902601

Cited by 5 publications

(14 citation statements)

References 48 publications

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“…After 5 days of inoculation, tumor diameters were measured daily with a sterile vernier caliper. The two tumor diameters, width and length, were measured and the tumor volume (V) was calculated using the following equation: V = (width 2 × length)/2 [ 15 , 54 , 55 , 56 , 57 ].…”

Section: Methodsmentioning

confidence: 99%

“…If the metabolization is by reduction of the N- oxide to amines, via two electrons, it leads to an agent that could interact with biomolecules like DNA, RNA polymerases and topoisomerases or both and the amine-protonation promotes an exclusively confined in the diseased tissue due to the acidic pH of the tumor cell microenvironment in the hypoxic conditions [ 13 , 14 ]. Derivatives of phenazine dioxides, such as the compound 2-amino-7-fluorophenazine 5,10-dioxide (FNZ), have low aqueous solubility (208 µg/mL) that prevents their selective action at the tumor level, their oral administration, parenteral and transdermal [ 11 , 15 , 16 ]. Thus, its clinical use would be restricted, due to the low biodistribution of the body aqueous milieu.…”

Section: Introductionmentioning

confidence: 99%

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Development and Evaluation of 2-Amino-7-Fluorophenazine 5,10-Dioxide Polymeric Micelles as Antitumoral Agents for 4T1 Breast Cancer

et al. 2021

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2-Amino-7-fluorophenazine 5,10-dioxide (FNZ) is a bioreducible prodrug, poorly soluble in water, with potential anticancer activity on hypoxic-tumors. This poor solubility limits its potential applications in clinic. Amphiphilic pristine polymeric micelles (PMs) based on triblock copolymers Pluronic® and Tetronic®, glycosylated derivatives and their mixtures with preformed-liposomes (LPS), were analyzed as strategies to improve the bioavailability of FNZ. FNZ encapsulations were performed and the obtaining nanostructures were characterized using UV-visible spectroscopy (UV-VIS), Transmission Electron Microscopy (TEM), Fourier transform infrared analysis and Dynamic Light Scattering (DLS). The most promising nanoformulations were analyzed for their potential toxicity and pharmacologically, at 20 mg/kg FNZ-doses, in a stage-IV murine metastatic-breast tumor model. The results revealed that the solubility of the encapsulated-FNZ increased up to seven times and the analysis (UV-VIS, DLS and TEM) confirmed the interaction between vehicles and FNZ. In all the cases appropriate encapsulation efficiencies (up to 70%), monodisperse nanometric particle sizes (PDI = 0.180–0.335), adequate Z-potentials (−1.59 to −26.4 mV), stabilities and spherical morphologies were obtained. The in vitro profile of FNZ controlled releases corresponded mainly to a kinetic Higuchi model. The in vitro/in vivo biological studies revealed non-toxicity and relevant tumor-weight diminution (up to 61%).

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Development and Evaluation of 2-Amino-7-Fluorophenazine 5,10-Dioxide Polymeric Micelles as Antitumoral Agents for 4T1 Breast Cancer

et al. 2021

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“…The two diameters of the tumor, width ( W ) and length ( L ), were perpendicular to each other and cover the largest portion of the tumor in each direction. Tumor volume ( T V ) was calculated using Equation (3) [ 66,67 ]

T_{normalV} = false(W^{2} \times L false) / 2

Ex vivo fluorescence imaging analysis of the accumulation of CUR‐loaded PMs was carried out by the i.v. injection of PMs in the tail vein of female BALB/c mice with induced 4T1 tumor (mean weight of 26.0 ± 1.9 g).…”

Section: Methodsmentioning

confidence: 99%

“…Biodistribution of Curcumin-Loaded Pristine and Glucosylated Polymeric Micelles: 4T1 breast tumors were developed in female BALB/c mice at the Reagent Unit for Experiment Biomodels (URBE, Facultad de Medicina, Universidad de la República, Montevideo, Uruguay) as previously described. [58,66,67] The average weight of BALB/c (5 to 7 weeks old) was between 23.6 and 25.2 g, housed in wire mesh cages at 20 ± 2°C with 12 h artificial light-dark cycles. Animals were fed ad libitum to standard pellet diet and water and were used after a minimum of 3 days acclimation to the housing conditions.…”

Section: Half-maximal Inhibitory Concentration Of Free Cur and Cur-lomentioning

confidence: 99%

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Glucosylated Polymeric Micelles Actively Target a Breast Cancer Model

Lecot

Glisoni

Oddone

et al. 2020

Advanced Therapeutics

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This work investigates the potential of glycosylation to actively target nanodrug delivery systems to adult solid tumors overexpressing glucose transporters. The highly hydrophobic fluorescent compound curcumin (CUR) is nanoencapsulated within polymeric micelles of pristine and glucosylated poly(ethylene oxide)‐poly(propylene oxide) block copolymers, and their interaction with breast cancer (BC) cells is investigated in vitro and in vivo. The aqueous solubility of CUR is increased more than 50 000‐fold and spherical nanoparticles display size in the 40 to 500 nm range, as determined by transmission electron microscopy and by dynamic light scattering, respectively. Uptake studies conducted in the BC cell line 4T1 in vitro demonstrate that glucosylation enhances nanoparticle internalization. Finally, the ability of unmodified and glucosylated polymeric micelles to accumulate in female BALB/c mice bearing 4T1‐induced tumors is compared by ex vivo bioimaging with auspicious results.

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The Phenazine Scaffold Used as Cytotoxic Pharmacophore Applied in Bactericidal, Antiparasitic and Antitumor Agents

Miksa

2022

Helvetica Chimica Acta

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Phenazine derivatives are important bactericidal antibiotics and antiparasitic compounds which can be used in synergistic combinations with anticancer drugs in chemotherapy treatments. The development of synthetic phenazines with anticancer activity improves the effectiveness of chemotherapy. Chemical variations introduced at the phenazine core which is known as a chromophore with fluorescent properties provide advanced theranostic agents useful in optical bioimaging techniques and photodynamic anticancer therapy. This review summarizes the field of structural modifications of phenazine derivatives which have been tested against different parasitic and bacterial infections. The report highlights advances in design and biological evaluations of phenazines as anticancer drugs for the development of new chemotherapeutic as well as bio‐imaging reagents.

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Selective Hypoxia‐Cytotoxin 7‐Fluoro‐2‐Aminophenazine 5,10‐Dioxide: Toward “Candidate‐to‐Drug” Stage in the Drug‐Development Pipeline

Cited by 5 publications

References 48 publications

Development and Evaluation of 2-Amino-7-Fluorophenazine 5,10-Dioxide Polymeric Micelles as Antitumoral Agents for 4T1 Breast Cancer

Development and Evaluation of 2-Amino-7-Fluorophenazine 5,10-Dioxide Polymeric Micelles as Antitumoral Agents for 4T1 Breast Cancer

Glucosylated Polymeric Micelles Actively Target a Breast Cancer Model

The Phenazine Scaffold Used as Cytotoxic Pharmacophore Applied in Bactericidal, Antiparasitic and Antitumor Agents

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