Selection of Pharmaceutical Antioxidants by Hydrodynamic Voltammetry

Antioxidant compounds are routinely included in pharmaceutical formulations in order to minimize the oxidative degradation of the active pharmaceutical ingredient(s) (API). The effectiveness of the antioxidants being considered is often assessed by creating several formulations with the API(s) and single or multiple antioxidants in order to place each of these formulations on stability under accelerated conditions. This trial and error selection process is costly and time consuming, often taking weeks before the oxidation is observed at a detectable level. Using a flow injection coulometric detector based system, a potential tool has been developed to guide initial antioxidant selection for hindering the oxidative degradation for a given drug substance in its formulation environment. The relative potential for the API to be oxidized can be measured by matching the conditions of the coulometric experiment to the formulation matrix. Using this selection criterion, the choice of antioxidants to study for individual formations can be greatly narrowed, thus leading to a significant savings in development time and cost.     

Surfactant media for constant-current coulometry. Application for the determination of antioxidants in pharmaceuticals

Effect of surfactant presence on electrochemical generation of titrants has been evaluated and discussed for the first time. Cationic (1-dodecylpyridinium and cetylpyridinium bromide), anionic (sodium dodecyl sulfate) and nonionic (Triton X100 and Brij^® 35) surfactants as well as nonionic high molecular weight polymer (PEG 4000) do not react with the electrogenerated bromine, iodine and hexacyanoferrate(III) ions. The electrogenerated chlorine chemically interact with Triton X100 and Brij^® 35. The allowable range of surfactants concentrations providing 100% current yield has been found. Chain-breaking low molecular weight antioxidants (ascorbic acid, rutin, α-tocopherol and retinol) were determined by reaction with the electrogenerated titrants in surfactant media. Nonionic and cationic surfactants can be used for the determination of antioxidants by reaction with the electrogenerated halogens. On contrary, cationic surfactants gives significantly overstated results of antioxidants determination with electrogenerated hexacyanoferrate(III) ions. The use of surfactants in coulometry of α-tocopherol and retinol provides their solubilization and allows to perform titration in water media. Simple, express and reliable coulometric approach for determination of α-tocopherol, rutin and ascorbic acid in pharmaceuticals using surfactant media has been developed. The relative standard deviation of the measurements does not exceed of 5%.     

Photochemical and antioxidant properties of gamma-oryzanol in beta-cyclodextrin-based nanosponges

Gamma-oryzanol (GO), a mixture of ferulic acid esters, has recently attracted a great interest as natural antioxidant extracted from rice-bran oil, usually employed to stabilize food and pharmaceutical raw materials, moreover as sunscreen in cosmetic formulations. Its usefulness, however, is limited by its fast degradation. A recently proposed approach to increase the stability and effectiveness of antioxidants is based on the inclusion in supramolecular structures (nanoparticles, cyclodextrins, liposomes, etc.). In this work we studied the inclusion of GO in β-cyclodextrin-based nanosponges which in the last few years have been chosen for their ability to encapsulate a great variety of substances to decrease their side-effects and to protect them from degradation. The inclusion complex was prepared in 1:1 w/w ratio and characterized by DSC, XRPD and membrane diffusion runs. The photodegradation of GO upon either UVA or UVB irradiation was found to be slowed down by inclusion in nanosponges. The antioxidant effectiveness of the inclusion complex was also assessed and in vitro experiments on porcine ear skin revealed a certain accumulation of GO also when entrapped in the host structure.     

Radiation resistant polypropylene blended with mobilizer,: antioxidants and nucleating agent

Post-irradiation storage of medical disposables prepared from isotactic polypropylene renders them brittle due to degradation. To avoid this, isotactic polypropylene [(is)PP] was blended with a mobilizer, dioctyl pthallate (DOP), three antioxidants (hindered amines and a secondary antioxidant) and benzoic acid to obtain radiation-resistant, thermally-stable and transparent material. Different formulations prepared were subjected to gamma radiation to doses of 25 and 50 kGy. Tests of breakage on bending after ageing in an oven at 70°C up to 12 months have shown that the addition of DOP and the antioxidants imparts improved radiation and thermal stability as compared to (is)PP alone or its blend with DOP. All the formulations irradiated or otherwise demonstrated excellent colour stability even after accelerated ageing at 70°C for prolonged periods.     

Viscoelastic characterization of phenolic resin–carbon fiber composite degradation process

Viscoelastic characteristics of cured phenolic resin–carbon fiber composite materials were investigated through glass transition and degradation reaction processes in the high‐temperature region up to 400°C. A typical glass transition of the crosslinked thermoset polymer was followed by irreversible degradation reactions, which were exhibited by the increasing storage modulus and loss modulus peak. A degradation master curve was constructed by using the vertical and horizontal shift factors, both of which complied well with the Arrhenius equation in light of the kinetic expression of degradation rate constants. Using an analogy to the Havriliak–Negami equation in dielectric relaxation phenomena, a viscoelastic modeling methodology was developed to characterize the frequency‐ and temperature‐dependent complex moduli of the degrading thermoset polymer composite systems. The temperature‐dependent relaxation time of the degrading composites was determined in a continuous fashion and showed a minimum relaxation time between the glass transition and degradation reaction regions. The capability of the developed modeling methodology was demonstrated by describing the complex behavior of the viscoelastic complex moduli of reacting phenolic resin composite systems. © 1999 John Wiley & Sons, Inc. J Polym Sci B: Polym Phys 37: 907–918, 1999     

QbD-mediated RP-UPLC method development invoking an FMEA-based risk assessment to estimate nintedanib degradation products and their pathways

QbD is considered an important, fundamental, and integral part of dosage form development. Despite its significance in drug formulations, the knowledge, reference, and guidance for using QbD in analytical science have not been thoroughly documented in the literature. The present study is aimed at bridging the gap between its generated data and the unexplored terrain in formulation science. This study is novel because, for the first time, an exclusive shorter run time UHPLC method for estimating degradation products was developed through the QbD approach, validated, and proved stability indicative. Five degradation impurities were separated and well characterized. Further, the degradation pathway of the anticancer drug nintedanib (NIN) was explored for the first time in the soft gel formulation using tandem quadrupole MS abetted mass identification, and ESI/MS/MS aided structure elucidation was performed. By carefully demonstrating the step-by-step procedure for QbD-based optimization, parameters such as the analytical target profile (ATP) and critical quality attributes (CQAs) were assessed. The risk assessment was performed using failure mode effect analysis (FMEA). Critical method attributes and critical method parameters were identified based on the magnitude of the calculated risk priority number (RPN) value. Designed experiments using 4-factor two-level factorial design monitored three critical quality attributes to arrive at a method operable design space (MODS). The effect of individual method attributes was also analyzed using half-normal and Pareto charts. Control strategies design and RPN values were recalculated based on the DOE output. This RPN value is eventually identified to be significantly smaller and satisfactory within the allowable limit.     

Challenges in polysorbate characterization by mass spectrometry

Polysorbates are used in a variety of applications over a wide range of markets. Simple in concept, these products are complex in actual composition. Mass spectrometry and related techniques have been effectively used to characterize these products, from the major components to the minor residual production byproducts and degradation species. In this paper we review the use of MALDI‐MS, LC/MS, GC/MS, and SFC/MS in the analysis of these materials. The wealth of information provided by MALDI is presented, using Polysorbate 60 as an example. Limitations are described, with the impact of matrix selection and cationization agent demonstrated. Furthermore, unique challenges of MALDI analysis of Polysorbate 80 are shown. Polysorbates have been extensively analyzed, especially by the biopharmaceutical industry, to better understand the impact of various grades of purity and manufacture on the stability of formulations. Using Polysorbate 80 as an example, we illustrate some of the more advanced techniques used to more fully characterize these complex molecules using high‐resolution LC/MS and LC/MS/MS. Finally, the use of other techniques (such as GC/MS and SFC/MS) is briefly reviewed.     

Lifetime prediction of a blue PE100 water pipe

The traditional method to assess the lifetime of plastic pipes is based on hydrostatic pressure testing. A complementary approach has been conducted to monitor the depletion of antioxidants and initiation of thermo-oxidative degradation on a PE100 blue water pipe that had been exposed to hydrostatic pressure in water at low test temperatures (maximum 80 °C).Depletion of antioxidants was monitored using OIT testing and initiation of thermo-oxidative degradation was assessed by iodometric detection of hydroperoxides. An empirical model based on the Arrhenius fit of the data was developed to extrapolate the lifetime of the PE100 pipe material at various service temperatures (10-25 °C). Associated activation energies, E_a, were determined and appeared to be in line with the values obtained from experiments carried out at low test temperatures. The combination of pressure testing and chemical analyses proved to be a very powerful tool to extrapolate the lifetime of plastic pipes.     

Effect of akyl-γ-cyclodextrins on the stability of retinol

Inclusion complexation between retinol (RET) and two synthetic alkyl carbonates of γ-cyclodextrin (alkyl-γ-CD) derivatives, ethyl-γ-cyclodextrin (E-CD) and octyl-γ-cyclodextrin (O-CD), was investigated by means of different techniques. The complexes were characterized by differential scanning calorimetry (DSC). Phase solubility studies, according to the method of Higuchi and Connors [1] were used to evaluate the complexation in aqueous solution at room temperature. In the present study inclusion complexes of retinol with E-CD and with O-CD were prepared to prevent its rapid degradation. In order to investigate the behavior of retinol under UV light, test of irradiation was performed separately on samples prepared dispersing retinol (0.1% w/w) or an equivalent amount of retinol/alkyl-γ-CD respectively in hydroxyethylcellulose (HEC) gel and in an O/W emulsion. The stability over time of retinol was also investigated storing the samples at 40 °C. Moreover retinol permeation through porcine skin has been evaluated employing Franz cells [2]. Retinol solubility was increased in presence of cyclodextrins while DSC analysis suggest that this inclusion agents are able to interact with retinol. Data for skin accumulation in porcine ear skin showed that alkyl-CDs increase of approximatively 1,5-fold retinol skin accumulation. Studies on the stability showed that both the inclusion complexes considered are able to increase retinol stability to light exposure and also to heat.     

Stability studies with a high-performance liquid chromatographic method for the determination of a new anthracycline analogue, 3'-deamino-3'-[2-(S)-methoxy-4-morpholino)doxorubicin (FCE 23762), in the final drug formulation.

A high-performance liquid chromatographic method was studied to optimize the separation of FCE 23762, a new antitumour agent, from both synthetic impurities and degradation products having very similar molecular structures. The main problems faced in the analytical method development using the most common reversed-phase columns available arose from the presence of analytical peaks with poor symmetry, a long analysis time and the separation between FCE 23762 and its R-isomer, which was often unsuitable for the correct determination of the drug substance. The use of a new stationary phase, Zorbax Rx-C8, together with a suitable mobile phase resulted in a good separation between the diastereomers, with satisfactory peak symmetry and run time. The method permitted the study of the stability of the drug substance in formulations for clinical trials.     

Global kinetics of thermal degradation of flame-retarded epoxy resin formulations

A predictive mathematical model to describe mass loss profiles of flame-retardant (FR) containing epoxy resin formulations is proposed. Mass loss is due to thermal degradation of the constituent components and can be described by a generic kinetic scheme with a given set of thermokinetic constants in the form of ordinary differential equations. The scope of this work is to determine the kinetic parameters of the thermal degradation of a known flame-retarded epoxy resin composition by using thermogravimetric analysis and using the acquired data to predict the degradation profiles for other formulations. The mass loss profiles of Visil and intumescent epoxy resin containing formulations were predicted by solving coupled systems of ordinary differential equations and then using Powell minimisation to find the optimal Arrhenius parameters, taking into account the mass ratio of the components in the mixture. The calculated kinetic constants for one formulation (85% resin-15% FR additives) are used to predict the mass loss profiles for other formulations (80% resin-20% FR additives and 90% resin-10% FR additives) with the assumption that the degradation mechanism does not change. The predicted thermal degradation profiles are compared with experimental data acquired using standard laboratory equipment in order to validate the proposed mechanisms. The kinetic parameters obtained adequately describe mass loss history of composite materials studied, even when extremely simplified kinetic schemes have been used.     

The structure of the nematic-isotropic interface in polymer systems

The structure of the nematic-isotropic interfacial layer is studied theoretically for systems formed by rod-like and persistent macromolecules. It is shown that the width of interfacial layer is normally of the order of the straight part of a molecule. This allows us to use the approach which describes intermolecular interactions phenomenologically (i.e. it allows us to consider all interactions), at the same time this approach describes molecular flexibility microscopically (i.e. it allows us to study the effects of flexibility correctly). It was found, that non-monotonic gradient profiles in the surface layer of the order parameter or of the concentration of molecules as a function of the coordinate perpendicular to the interface are possible. For example, a thin layer with abnormal ordering of molecules along the surface may exist near the interface for some systems.     

New rheological developments for reactive processing of poly(ε-caprolactone)

This short review aims to show how an integrated activity on reactive processing have been developed these last years in our laboratory. We can say that the originality of this approach is based on combining developments in chemistry, in line instrumentation, and rheology aspects. Our rheological works can be divided into four important contributions: rheo-physics, rheo-chemistry, rheo-mixing and rheo-processing. These different parts are illustrated from the ε-caprolactone polymerisation in bulk and dispersed media. Rheo-physics studies allowed us to calculate the molecular weight distribution and chain structures of in situ polymerised poly(ε-caprolactone) samples. From rheo-chemistry works, we are now able to predict the variation of the complex shear modulus versus the extent of the polymerisation. The developments of new rheological tools such as rheo-mixer enable us to investigate complex mixing situations encountered in reactive polymer blends and formulations. Lastly, a rheo-processing approach based on the in-line measurement of the viscosity in a slit rheometer at the die exit of the extruder allows us to envisage its application to the experimental control of the reactive processing in extruder. To cite this article: P. Cassagnau et al., C. R. Chimie 9 (2006).     

Application of linked scans in pyrolysis mass spectrometry of polymers

Linked scans have been used in the pyrolysis mass spectrometry of polymers containing arylene and/or heteroarylene together with vinylene units. This technique based on metastable ions allows the study of characteristic sequences in complex mixtures of degradation ions up to high mass regions. Essential information is obtained concerning the mechanism of polymerization via the Wittig reaction, the pyrolytic and electron impact induced degradation processes and the ion structures which characterize the polymers.     

Degradation studies of quetiapine fumarate by liquid chromatography–diode array detection and tandem mass spectrometry methods

Quetiapine fumarate (QUE) is an antipsychotic agent with a chemical structure that is susceptible to degradation; therefore, it is important to study its stability using appropriate analytical tools. Knowledge of the stability profile of a drug is important because chemical degradation of its active component often results in a loss of potency, affecting its efficacy and safety. This current work reports degradation studies of QUE as drug substance, under different stress conditions such as oxidation, hydrolysis, heat, humidity and photolysis, by a stability‐indicating LC method. The chemical stability was evaluated using a simple HPLC/diode array detection method, with a core‐shell C₁₈ column under isocratic conditions, which allows the separation of all primary degradation products (DPs) in a short run time. QUE was mainly degraded under oxidative and hydrolytic conditions, with the formation of three and two DPs, respectively, which were identified by electrospray ionization–tandem mass spectrometry. The method was properly validated in terms of linearity, accuracy, precision, selectivity, robustness and quantitation limit. Commercial tablets containing 25 mg of QUE were quantified, with results obtained within the United States Pharmacopeia limits. The proposed method is suitable to assess the stability and perform routine analysis of QUE in pharmaceutical samples.     

Study of electrochemical stability of conducting polymers by bidimensional spectroelectrochemistry: p- and n-doping of poly(4,4′-bis(butylthio)-2,2′-bithiophene) films

UV-vis bidimensional spectroelectrochemistry has been applied to the study of the electrochemical stability of conducting polymer films during p- and n-doping processes. Specifically, poly(4,4′-bis(butylthio)-2,2′-bithiophene) has been chosen as example to prove the usefulness and suitability of this multi-response technique to characterize polymer stability during p- and n-doping. It was found that oxidative doping and corresponding de-doping alone did not result in noticeable polymer film degradation. However, in experiments involving both p- and n-doping of this conducting polymer, soluble species arising from the polymer film were detected in solution for the first time, indicating a lower electrochemical stability of the film under these experimental conditions. Moreover, bidimensional spectroelectrochemistry has enabled us not only to detect the soluble degradation products, but also the potential range in which the degradation takes place.     

Spectrophotometric assay of retinol via charge-transfer complexes

Simple and sensitive spectrophotometric methods for the assay of retinol have been presented. The first method was based on the reaction of retinol with iodine to give a molecular charge-transfer complex, the retinol acting as n-donor and iodine as -electron acceptor. The second method depends on the formation of a highly coloured stable radical anion between retinol and 7,7,8,8-tetracyanoquinodimethane (TCNQ as a -electron acceptor. The molecular ratios of the reactants in the complexes have been established and the experimental conditions leading to maximum charge-transfer bands were also studied. Beer's law is obeyed over the retinol concentration range 2.5–26 µg/ml. The proposed procedures have been applied successfully to the analysis of drug formulation. The average recovery and average standard deviation was 99.99 ±1.13% with retinol-iodine and 100.001 ± 1.31% with retinol-TCNQ. A kinetic study was performed by heating retinol at 50°C for different periods of time, the result obtained by plotting log c against time indicates that thermal decomposition of retinol is of first order. The results obtained by both methods were in good agreement with those obtained by the official method. The developed procedures were found to be simple, accurate and precise and can be used for the determination of retinol in presence of its degradation products.     

Predicting the lifetime of fluorosilicone o-rings

Long-term (up to 1000 days) accelerated oven-aging studies on a commercial fluorosilicone o-ring seal are used to predict the sealing lifetime at room temperature (23 °C). The study follows force decay (relaxation) on squeezed o-ring material using isothermal compression stress relaxation (CSR) techniques. The relaxation is normally a complex mix of reversible physical effects and non-reversible chemical effects but we utilize an over-strain approach to quickly achieve physical equilibrium. This allows us to concentrate the measurements on the chemical relaxation effects of primary interest to lifetime assessment. The long-term studies allow us to access a fairly broad temperature range (80-138 °C) which results in improved modeling of the temperature dependence of the accelerated data. Non-Arrhenius behavior is observed with evidence of a significant lowering of the activation energy at the lowest accelerated aging temperature (80 °C). This observation is consistent with numerous recent accelerated aging studies that probed temperature ranges large enough to observe similar non-Arrhenius behavior. The extrapolated predictions imply that significant loss of sealing force requires on the order of 50-100 years at 23 °C. Field aging results out to ∼25 years at 23 °C are shown to be in reasonable accord with the significant change in Arrhenius slope observed from the accelerated aging study.     

Comparison of Generic Hydrochlorothiazide Formulations by Means of TG and DSC Coupled to a Photovisual System

The compatibilities and stabilities of some binary mixtures and generic hydrochlorothiazide formulations were studied by using TG, DSC and a DSC-photovisual system. The kinetic parameters were determined via the Arrhenius equations. Tablet B presented higher compatibility and thermal stability than those of tablets A and C. The photovisual system demonstrated that the decomposition of tablet A occurs before the melting point, due to the Maillard reaction between the hydrochlorothiazide and lactose present in the formulation. The behaviour and rate constants of binary mixtures suggest that lactose can be substituted for microcrystalline cellulose, MC(101), in tablet A. The DSC and TG data revealed different characteristics of compatibility and stability in generic formulations from different manufacturers. This revised version was published online in July 2006 with corrections to the Cover Date.     

Kinetics studies of the degradation of sirolimus in solid state and in liquid medium

The use of sirolimus and its analogs has been evaluated for the treatment of different cancer types. The stability studies of sirolimus enabled to determine the kinetics of its chemical reactions in solid state and in the liquid medium. During intrinsic stability tests in a liquid medium, sirolimus showed a lack of stability when exposed to heat, neutral and basic hydrolysis. Analysis by high-performance liquid chromatography detected: two degradation products after exposure to heat; one degradation product for both basic and neutral hydrolyses; and all degradation products exhibited UV spectra similar to the drug’s spectrum. Kinetics studies in a liquid medium revealed low drug stability in methanolic solution; this instability may be exacerbated in the presence of water or high pH. The application of solid-state kinetic models showed that the drug degrades in accordance with the diffusion dimensional model, with greater stability and an expiration date equal to 6 years, demonstrating that sirolimus has satisfactory stability in the solid state. Through this understanding, it is possible to develop more stable pharmaceutical formulations using sirolimus.