Stability of 25 mg/mL Azacitidine Suspensions Kept in Fridge after Freezing

Balouzet, Clara; Chanat, Cédric; Jobard, Marion; Brandely-Piat, Marie-Laure; Chast, François

doi:10.1515/pthp-2016-0023

Cited by 5 publications

(7 citation statements)

References 6 publications

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“…It is known that rapid and reversible hydrolysis of the azacitidine occurs in an aqueous medium, which leads to N-formyl RibosylGuanylUrea (RGU-CHO) formation, which is irreversibly hydrolyzed into RibosylGuanylUrea (RGU). It is a two-stage degradation [ 7 , 8 , 9 , 10 , 11 , 23 ]. These hydrolysis products do not produce toxicological or therapeutic effects, but they lead only to decreasing azacitidine potency [ 9 , 10 , 24 ].…”

Section: Resultsmentioning

confidence: 99%

“…However, already at time zero, chromatograms showed, besides the azacitidine peak with an average retention time (RT) of 4.3 min, the presence of four other peaks, including two peaks attributed to RGU-CHO and RGU with an average RT of 2.9 min and 2.0 min, respectively [ 7 , 8 , 9 , 10 , 11 , 23 ], and other two peaks with an average RT of 2.5 min and 3.6 min, which were more clearly detected in chromatograms obtained from Vidaza ® (50 µg/mL) subjected to heat stress (see the violet line, Figure 1 ).…”

Section: Resultsmentioning

confidence: 99%

“…Instead, when refrigerated sterile water for injection (2–8 °C) is used, the suspension remains stable for another 22 h if stored at 2–8 °C [ 5 ]. Indeed, the azacitidine is very unstable in an aqueous solution [ 6 , 7 , 8 , 9 ] and it is rapidly hydrolyzed to several degradation products (DPs) in a temperature-dependent process [ 10 , 11 ].…”

Section: Introductionmentioning

confidence: 99%

“…However, published results are not that recent, heterogeneous in terms of quality and relevance, and many of them do not take practical needs into account and the results need to be confirmed using the formulation currently administered in clinical practice (i.e., a 25 mg/mL aqueous azacitidine suspension) [ 18 , 19 ]. Moreover, most of the studies considered only chemical stability and did not evaluate a potential variation over time of the physical and microbiological parameters of reconstituted Vidaza ® [ 7 , 10 , 11 , 12 , 20 , 21 ].…”

Section: Introductionmentioning

confidence: 99%

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Development and Validation of a New Storage Procedure to Extend the In-Use Stability of Azacitidine in Pharmaceutical Formulations

Iudicello

Genovese

Strusi³

et al. 2021

Pharmaceuticals

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Stability studies performed by the pharmaceutical industry are principally designed to fulfill licensing requirements. Thus, post-dilution or post-reconstitution stability data are frequently limited to 24 h only for bacteriological reasons, regardless of the true physicochemical stability which could, in many cases, be longer. In practice, the pharmacy-based centralized preparation may require preparation in advance for administration, for example, on weekends, holidays, or in general when pharmacies may be closed. We report an innovative strategy for storing resuspended solutions of azacitidine, a well-known chemotherapic agent, for which the manufacturer lists maximum stability of 22 h. By placing the syringe with the azacitidine reconstituted suspension between two refrigerant gel packs and storing it at 4 °C, we found that the concentration of azacitidine remained above 98% of the initial concentration for 48 h, and no change in color nor the physicochemical properties of the suspension were observed throughout the study period. The physicochemical and microbiological properties were evaluated by HPLC–UV and UHPLC-HRMS analysis, FTIR spectroscopy, pH determination, visual and subvisual examination, and sterility assay. The HPLC-UV method used for evaluating the chemical stability of azacitidine was validated according to ICH. Precise control of storage temperature was obtained by a digital data logger. Our study indicates that by changing the storage procedure of azacitidine reconstituted suspension, the usage window of the drug can be significantly extended to a time frame that better copes with its use in the clinical environment.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Development and Validation of a New Storage Procedure to Extend the In-Use Stability of Azacitidine in Pharmaceutical Formulations

Iudicello

Genovese

Strusi³

et al. 2021

Pharmaceuticals

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“…This failure can be either a primary failure (lack of any response to azacitidine), a secondary failure (disease progressed after a first response, serum drug level is low) or a toxicity failure (azacitidine treatment was terminated due to severe side effects) [15,16]. A part of these failures can be attributed to the chemical and pharmacological properties of this drug, as azacitidine is sensitive to water, undergoing rapid and reversible hydrolysis, producing N-formylribosylguanylurea, followed by its irreversible hydrolysis to ribosylguanylurea (Figure 1) [17,18], which explains its short half-life after administration. Additionally, because of its hydrophilic nature, poor cell internalization has been observed, which is a common problem for most hydrophilic drugs.…”

Section: Introductionmentioning

confidence: 99%

Azacitidine Omega-3 Self-Assemblies: Synthesis, Characterization, and Potent Applications for Myelodysplastic Syndromes

et al. 2021

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5-Azacitidine, a cytidine analogue used as a hypomethylating agent, is one of the main drugs for the treatment of myelodysplastic syndromes (MDSs) and acute myeloid leukemia (AML) in the elderly. However, after administration, it exhibits several limitations, including restricted diffusion and cellular internalization due to its hydrophilicity, and a rapid enzymatic degradation by adenosine deaminase. The aim of this study was to improve the drug cell diffusion and protect it from metabolic degradation via the synthesis of amphiphilic prodrugs and their potential self-assembly. Azacitidine was conjugated to two different omega-3 fatty acids, eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA). The carboxylic acid group of the omega-3 fatty acids was effectively conjugated to the amine group of the azacitidine base, yielding two amphiphilic prodrugs. Nanoprecipitation of the obtained prodrugs was performed and self-assemblies were successfully obtained for both prodrugs, with a mean diameter of 190 nm, a polydispersity index below 0.2 and a positive zeta potential. The formation of self-assemblies was confirmed using pyrene as a fluorescent dye, and the critical aggregation concentrations were determined: 400 µM for AzaEPA and 688 µM for AzaDHA. Additionally, the stability of the obtained self-assemblies was studied and after 5 days their final stable arrangement was reached. Additionally, cryo-TEM revealed that the self-assemblies attain a multilamellar vesicle supramolecular structure. Moreover, the obtained self-assemblies presented promising cytotoxicity on a leukemia human cell line, having a low IC50 value, comparable to that of free azacitidine.

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