Int J App Pharm, Vol 9, Issue 4, 2017, 90-95Original Article


COMPARISON OF THE USP APPARATUS 2 AND 4 FOR TESTING THE IN VITRO RELEASE PERFORMANCE OF IBUPROFEN GENERIC SUSPENSIONS

JOSE RAUL MEDINA*, MARIEL CORTES, ERIK ROMO

Departamento Sistemas Biológicos, Universidad Autónoma Metropolitana-Xochimilco, Mexico City, Mexico
Email: rmlopez@correo.xoc.uam.mx

Received: 13 May 2017, Revised and Accepted: 14 Jun 2017


ABSTRACT

Objective: The aim of this study was the comparison of the in vitro release performance of ibuprofen generic suspensions and reference, based on the hydrodynamic environment generated by the flow-through cell method (USP Apparatus 4). Results were compared with those obtained by the use of the USP Apparatus 2.

Methods: The Advil® suspension (2 g/100 ml) and two generic formulations with the same dose were tested. Dissolution studies were carried out using a USP Apparatus 4 Sotax CE6 with 22.6 mm cells, laminar flow at 16 ml/min, and pH 7.2 phosphate buffer at 37.0±0.5 °C as dissolution medium. Ibuprofen was quantified spectrophotometrically at 222 nm. The in vitro release of the three drug products were studied using the USP Apparatus 2. The dissolution profiles of generic products were compared with the reference by model-independent, model-dependent, and analysis of variance (ANOVA)-based comparisons.

Results: The dissolution profile of the generic product A was similar to the dissolution profile of reference, only with the use of the USP Apparatus 4. The f2 similarity factor was>50 and no significant differences were found with dissolution efficiency data (*P>0.05). Similar results were found with the comparison of t50% and t63.2% values. Similar dissolution profiles between generic product A and reference were also found with ANOVA-based comparisons.

Conclusion: The flow-through cell method was adequate for study the in vitro release of ibuprofen suspensions. It is necessary to evaluate the in vivo performance of the drug products used in order to estimate the predictability of the proposed methodology.

Keywords: Dissolution studies, Flow-through cell apparatus, Generic products, Ibuprofen, Suspension, USP Apparatus 4


INTRODUCTION

Ibuprofen, a poorly water-soluble non-steroidal anti-inflammatory drug (NSAID), is recommended for the treatment of moderate or acute pain. This compound is manufactured as solid oral dosage forms and suspensions. Ibuprofen suspension is widely used as antipyretic in children [1] and it is accessible for the elderly who cannot swallow easily [2]. Some ibuprofen formulations are available as generic drug products. A generic product refers to a bioequivalent product with the same quality and efficacy as the reference [3]. Generic drugs production represents savings for patients and hospitals and these formulations should be evaluated periodically. To determine whether this drug is safely interchangeable, the evaluation of their in vitro performance under conditions that simulate the natural environment of the gastrointestinal tract is very important.

According to the Biopharmaceutics Classification System (BCS), ibuprofen is a Class II drug owing to its low solubility/high permeability characteristics [4]. Class II drugs are compounds with a dissolution-limited absorption and a significant in vitro-in vivo correlation (IVIVC) should be expected using a well-designed in vitro dissolution test. The establishment of a significant IVIVC provides the basis for estimating the in vivo performance of the drug and waives the costly bioequivalence studies [5]. Previously, some researchers have reported the dissolution profiles of ibuprofen suspension using the BCS criteria [2]. Experiments were carried out with the United State Pharmacopeia (USP) paddle apparatus (USP Apparatus 2) with 900 ml of buffer pH 7.2, pH 6.8, pH 4.5, and 0.1 M HCl as dissolution medium. Agitation rates of 25 and 50 rpm were tested. The researchers observed that the higher amount of drug was released at pH 7.2 (more than 100%) during 30 min and that 50 rpm was the adequate condition to discriminate among dissolution profiles. Nevertheless, they only studied the reference product and comparisons, at the same experimental conditions, were carried out with the in vitro release of ibuprofen tablets.

A dissolution test for ibuprofen suspensions, using the USP Apparatus 2 at 50 rpm with 900 ml of pH 7.2 phosphate buffer as the dissolution medium, is officially described [6]. Under these conditions, not less than 80% of the drug should be dissolved in 60 min (Q ≥ 80%). This criterion is established to ensure the good quality of the drug products. However, previous studies have shown that despite most drug products meet the pharmacopeial dissolution criteria, some generics differed in their dissolution profiles when comparing with their branded counterparts, which questions the interchangeability between them or even among generic products [7].

The flow-through cell method (USP Apparatus 4) is an alternative apparatus for dissolution studies [8, 9]. Its advantages over the USP Apparatus 2 have been widely demonstrated, especially for the study of the in vitro dissolution performance of poorly water-soluble drugs [10, 11]. The flow-through cell method permits continuous extraction of the drug, simulating absorption into the systemic circulation, generating an intermittent flow of the dissolution medium into the cell where the dosage form is placed [12]. It can be used as an open system, allowing release under sink conditions, which facilitates the dissolution of poorly water-soluble drugs as well as change the dissolution medium within a pH range of physiological relevance [13]. The USP Apparatus 4 has been used to study the in vitro release of ibuprofen from drug products manufactured in immediate-release solid dosage forms [14], and in fixed-dose combination formulations [15].

Despite the advantages of the flow-through cell apparatus over the USP paddle apparatus, little information is available on the in vitro release of ibuprofen suspensions using the USP Apparatus 4. The aim of this study was to characterize the in vitro release performance of ibuprofen from the reference and two generic formulations, using the flow-through cell method. Results obtained were compared with those found with the official USP Apparatus 2.

MATERIALS AND METHODS

Products

Ibuprofen was purchased from Sigma-Aldrich Co. (St. Louis MO, USA). Sodium phosphate monobasic and sodium hydroxide were purchased from J. T. Baker-Mexico. The Advil® suspension (Pfizer SA de CV, Mexico) containing ibuprofen (2 mg/100 ml), was used. The Mexican health authorities (COFEPRIS) have established this brand as reference drug product [16]. Two generic formulations containing the same dose were also used. The assay test was performed on all drug products, according to the procedures described in the USP [6]. The limit of related compound C, pH, and density was also determined.

USP apparatus 2

The dissolution profiles of ibuprofen from generic suspensions were obtained using an automated USP paddle apparatus (Sotax AT-7 Smart, Switzerland), with a piston pump (Sotax CY7-50, Switzerland). A UV/Vis spectrophotometer with 1 mm flow cells (Perkin Elmer Lambda 35, USA) was used. All equipment and data generated were controlled by a specific software designed by Sotax. After 15 min of mechanical agitation and with a syringe, a sample of 1 ml of suspension was added on 900 ml of pH 7.2 phosphate buffer at 37.0±0.5 °C. Rotational speed of 50 rpm was used. Sequential sampling using nitrocellulose filters (Millipore) was performed every 5 min until 60 min, with 12 replicates. The amount of ibuprofen dissolved was determined with a standard calibration curve at 222 nm.

USP apparatus 4

The dissolution profiles of ibuprofen from generic suspensions were obtained using an automated flow-through cell apparatus (Sotax CE6, Switzerland), with 22.6-mm cells (i.d.) and a piston pump (Sotax CY7−50, Switzerland). A UV/Vis spectrophotometer with 1 mm flow cells (Perkin Elmer Lambda 10, USA) was used. In all experiments, laminar flow (with a bed of 6 g of glass beads) was used. Deareated pH 7.2 phosphate buffer at 37.0±0.5 °C was pumped at 16 ml/min. An open system was used, without recycling the dissolution medium. After 15 min of mechanical agitation and with a syringe, a sample of 1 ml of suspension was added into each cell. Sequential sampling using nitrocellulose filters (Millipore) was performed every 5 min until 60 min, with 12 replicates. The amount of ibuprofen dissolved was determined with a standard calibration curve at 222 nm.

Data analysis

The dissolution profiles of the generic drug products A and B vs. reference were compared by model-independent,-dependent and analysis of variance (ANOVA)-based methods [12, 17]. For model-independent comparisons, the f2 similarity factor, mean dissolution time (MDT), and dissolution efficiency (DE) were calculated. Furthermore, the percentage of ibuprofen dissolved at 60 min was also compared. The parameters of generic products A and B vs. reference were compared using a univariate one-way ANOVA followed by a Dunnett’s multiple comparison tests. Differences were considered significant if *P<0.05. For calculation of DE and MDT values, the Excel add-in DDSolver was used [18]. For all statistical comparisons, SigmaPlot software was used (version 11.0).

For model-dependent comparisons, dissolution data were fitted to Weibull, logistic, Gompertz, and probit models. The model with the highest adjusted determination coefficient (R2adjusted) and the minimum Akaike information criterion (AIC) was chosen as the best fit model [17]. Data analysis was performed using the Excel add-in DDSolver. Additionally, dissolution data were fitted to sigmoidal model using SigmaPlot software. With this fit, the t50% and t63.2% values were calculated. The values of the generic products A and B vs. reference were statistically compared and differences were considered significant if *P<0.05.

The ANOVA-based comparisons were carried out with the percentage of ibuprofen dissolved at each time point using a univariate one-way ANOVA followed by a Dunnett’s multiple comparisons test. Differences were considered significant if *P<0.05.

RESULTS AND DISCUSSION

All drug products met the assay test specified in the USP. The percentages of ibuprofen were between 90 and 110% [6]. The limit of related compound C, pH, and density data are shown in table 1.

Table 1: Characterization of ibuprofen suspensions

Code Assay (%), RSD (%) Limit of related compound C (%) pH Density (g/ml)
R 100.8, 0.73 0 4.138 1.2491
A 97.6, 0.21 0 5.366 1.1702
B 99.9, 1.27 0 4.133 1.1729

RSD: relative standard deviation

Dissolution profiles

The dissolution profiles of ibuprofen suspensions are shown in fig. 1. Considering a single-point specification (Q ≥ 80% in 60 min), all drug products met the pharmacopeial dissolution criterion using both dissolution apparatuses. It is important to note that the generic product B released the complete dose of ibuprofen at the first sampling time (5 min) when using the USP Apparatus 2.

Fig. 1: Dissolution profiles of ibuprofen suspensions, R) reference and A) and B) generic products. mean±SD, n = 12

Although all drug products met the pharmacopeial dissolution criterion, differences in dissolution profiles of both generic products vs. reference were found. The f2 similarity factor of the generic products A and B, were 49.48 and 37.98 respectively when using the USP paddle apparatus. In the same order, the f2 values were 63.46 and 40.85, when using the flow-through cell method. With these results, the dissolution profile of the generic product A, was considered similar to the dissolution profile of reference (f2>50), only when using the USP Apparatus 4.

All drug products showed slightly slow in vitro release of ibuprofen when using the flow-through cell apparatus (>35% dissolved in 5 min vs.>50% at the same time with the USP paddle apparatus). Some researchers have suggested that this result can be explained by the hydrodynamic conditions that characterize the USP Apparatus 4, which lacks an agitation mechanism, and by the fact that the dosage form and the drug particles are continuously exposed to uniform laminar flow, similar to the natural environment of the gastro-intestinal tract, causing different dissolution pattern [19]. When using the flow-through cell apparatus, cell size, glass beads, and flow rate are critical factors in determining the dissolution pattern. The flow rate of 16 ml/min is suggested by the European and USP [20]. When the flow rate of the dissolution medium is 16 ml/min, the fluid flow inside the 22.6-mm cells is 4 cm/min [21]. Fotaki et al. [21] reported that the axial velocity of the intestinal fluid is approximately 1.5 cm/min. Therefore, the axial velocity of 4 cm/min generated under the experimental conditions described above is close to reported physiological parameters.

Model-independent comparisons

The mean values±standard error of the mean (SEM) of ibuprofen dissolved at 60 min, and model-independent parameters MDT and DE, are shown in table 2. In all comparisons, significant differences were observed between the dissolution profiles of the generic products A and B vs. reference (*P<0.05), excepting the DE value of the generic product A, with the USP Apparatus 4 (*P>0.05).

Table 2: Model-independent parameters of ibuprofen suspensions

USP Code % Diss. at 60 min MDT (min) DE (%)
2 R 101.97±2.30 6.81±0.17 90.35±1.88
A 91.33±1.23* 4.14±0.16* 85.01±1.08*
B 108.58±0.84* 3.36±0.10* 102.49±0.75*
4 R 103.77±1.55 5.28±0.21 94.67±1.63
A 111.08±2.75* 6.86±0.22* 98.33±2.31
B 88.90±1.96* 6.12±0.25* 79.79±1.61*

R: reference, A and B: generic products, MDT: mean dissolution time, DE: dissolution efficiency. mean±SEM, n = 12, *P<0.05

The model-independent parameters MDT and DE are commonly used parameters to compare dissolution profiles. The MDT represents the average time at which 63.2% of the dose is dissolved, and DE relates the area under the curve of the dissolution profile to the total area of the rectangle formed, by the theoretical dissolution of 100% of the dose and the time interval of the test. The MDT and DE have been also proposed as satisfactory parameters for in vitro-in vivo correlation (IVIVC) levels B and C [22]. Level B is defined as the relationship between the MDT and mean residence time (average time that a molecule stays in the body), and both parameters are calculated by statistical moments analysis. Level C is defined as the association between a dissolution time point (t50%, t85%, etc.) and one pharmacokinetic parameter, such as area under the curve, Cmax, or Tmax. The DE value is used by some researchers as an appropriate parameter to expresses the global drug dissolution performance, useful for comparison of dissolution profiles [23] or to relate it to some in vivo parameter.

Model-dependent comparisons

The R2 adjusted and AIC mean values for ibuprofen suspensions are shown in table 3.

Table 3: Criteria used for the selection of the best fit model

USP Apparatus 2 USP Apparatus 4
Code Weibull logistic Gompertz probit Weibull logistic Gompertz probit
R2adjusted
R 0.9888 0.9773 0.9722 0.9813 0.9968 0.9951 0.9939 0.9965
A 0.9968 0.9973 0.9974 0.9970 0.9969 0.9991 0.9976 0.9996
B 0.9460 0.9453 0.9452 0.9450 0.9901 0.9817 0.9774 0.9850
AIC
R 33.33 47.04 50.16 43.21 28.71 33.85 37.22 29.26
A 0.06 -2.12 -2.38 -0.61 33.26 19.16 30.92 7.74
B -5.56 -5.49 -5.46 -5.29 27.12 33.20 37.18 29.13

R: reference, A and B: generic products, AIC: Akaike information criterion. Mean, n = 12

The dissolution data of the reference and generic product B, were well fitted to the Weibull function when using USP Apparatus 2 and 4. Both products reached the highest values of R2adjusted and the lowest values of AIC. The dissolution data for the generic product A were well fitted to the Gompertz function and probit equation, when using the USP Apparatus 2 and 4, respectively. None of the ibuprofen data was well fitted by the logistic model.

The Weibull function (Eq. 1) is widely used for the study of in vitro drug release mechanisms [24]. An advantage of this model is that parameter calculation is independent of whether or not sink conditions prevail [25]. As the generic product B and reference were well adjusted to this function, β parameter was used to compare the dissolution profiles. Mean data were compared by a Student’s t-test and significant differences were found (*P<0.05). The dissolution profiles of generic product B were considered dissimilar respect to the dissolution profile of reference, in both dissolution apparatuses.

Eq. [1]

Where α is the scale parameter and β is the shape parameter [18].

Because all drug products showed adequate R2adjusted values, the Weibull parameters of the three formulations were calculated, and parameters and Td values are shown in table 4.

Table 4: Model-dependent parameters (Weibull function) and Td values

USP Code α β Fmax Td (±SEM)
2 R 8.16 1.08 102.19 6.81±0.22
A 12.09 1.69 90.83 4.11±0.15
B 0.47 0.08* 114.01
4 R 61.55 2.15 105.11 6.79±0.15
A 43.18 1.84 111.09 7.70±0.20
B 49.82 1.87* 89.58 7.27±0.25

α: scale parameter, β: shape parameter. Mean, n = 12, *P<0.05, † no real value was found

As in vitro release of ibuprofen from the generic product, B was fast, using the USP paddle apparatus (the complete dose was dissolved at 5 min), no real value for the Td parameter was found. The Td parameter is equivalent to the model-independent parameter MDT [26].

The Weibull shape parameter β characterizes the dissolution profile as exponential (β = 1); as sigmoid S-shaped, with upward curvature followed by a turning point (β>1); or as parabolic, with a steeper initial slope that is consistent with the exponential (β<1) [26]. The in vitro release of ibuprofen from the three drug products showed β values>1, meaning sigmoidal profiles excepting the generic product B under the hydrodynamic environment of USP Apparatus 2. By the obtained results, the in vitro release of ibuprofen from suspensions seems not to be the same in the USP Apparatus 2 and 4. To confirm this result, the MDT and Td values were separately plotted by dissolution apparatus. Results are shown in fig. 2.


Fig. 2: Linear regression between Td vs. MDT values of ibuprofen from the generic products A and B and reference (R) Mean, n = 12

Only linear regression of data obtained with the USP Apparatus 4 was significant (*P<0.05). This results confirm that the in vitro release of ibuprofen suspensions, under the hydrodynamic environment generated by the USP Apparatus 4, is better than that generated by the USP paddle apparatus, independently of the used formulation. These results agree with previous reports of in vitro studies of ibuprofen in fixed-dose combination formulations [15].

Because an inconsistent fitting was found when using the mathematical models described above, and with almost all drug products the β values were>1, the sigmoidal model (Eq. 2) was used to fit the dissolution data.

Eq. [2]

Where a, b and x0 are constants [18].

The data adjusted to the sigmoidal model allowed to obtain R2 values higher than 0.99, excepting the R2 value of the generic product B (>0.98). With a, b, and x0 parameters, the t50% and t63.2% values were calculated. Data of sigmoidal model parameters and tx% values are shown in table 5.

Table 5: Model-dependent parameters (Sigmoidal equation) and tx% values

USP Code R2 a b x0 t50% (min) t63.2% (min)
2 R 0.9954 101.94 4.54 4.62 4.45 6.88
A 0.9974 90.83 1.49 3.35 3.65* 4.58*
B 0.9843 109.62 35.23 -98.07
4 R 0.9973 105.14 1.92 5.74 5.59 6.58
A 0.9973 111.04 2.51 6.41 5.92 7.14
B 0.9937 89.61 2.56 5.99 6.56* 8.21*

Mean, n = 12, *P<0.05, † no real values were found

As the in vitro release of ibuprofen from the generic product B was fast, when using the USP Apparatus 2, no real value for the t50% and t63.2% parameters were calculated. Dissolution profiles were compared with the tx% values and significant differences were found (*P<0.05) between the generic product A vs. reference (USP Apparatus 2, Student’s t-test), and between the generic product B vs. reference (USP Apparatus 4, univariate one-way ANOVA).

The tx% and sampling time values are commonly used to characterize the drug release rate. The tx% value corresponds to the time necessary to release a determined percentage of drug (e. g., t10%, t50%, t90%) and the sampling time corresponds to the amount of drug dissolved in that time (e. g., t10 min, t50 min, t90 min). Pharmacopeias use this parameter as an acceptable limit for the dissolution test (e. g., t45 min ≥ 80%) [27].

ANOVA-based comparisons

ANOVA-based comparisons were used to compare the dissolution profiles of the ibuprofen suspensions. The advantage of this approach is that it is not restricted to any of the requirements of model-independent comparisons. Additionally, it does not depend on data fitting to a specific equation. Comparisons between the generic products A and B vs. reference, when using both dissolution apparatuses, were carried out at each sampling time. Results are shown in table 6.

Table 6: Dunnett’s multiple comparison tests for the percentage of ibuprofen dissolved at each time point of the generic product A and B vs. reference

Comparison Time (min) USP Apparatus 2 USP Apparatus 4
Difference *P Difference *P
A vs. R 5 14.31 <0.05 2.89 >0.05
10 12.28 <0.05 3.92 >0.05
15 1.57 >0.05 0.11 >0.05
20 8.80 <0.05 3.37 >0.05
25 5.60 <0.05 4.96 >0.05
30 10.64 <0.05 5.67 >0.05
35 10.73 <0.05 6.06 >0.05
40 10.73 <0.05 6.36 >0.05
45 10.72 <0.05 6.61 >0.05
50 10.75 <0.05 6.83 >0.05
55 10.72 <0.05 7.06 <0.05
60 10.63 <0.05 7.30 <0.05
B vs. R 5 50.79 <0.05 6.69 <0.05
10 28.14 <0.05 21.66 <0.05
15 14.09 <0.05 16.82 <0.05
20 7.16 <0.05 16.74 <0.05
25 10.59 <0.05 16.39 <0.05
30 5.81 <0.05 16.00 <0.05
35 5.85 <0.05 15.74 <0.05
40 6.04 <0.05 15.54 <0.05
45 6.20 <0.05 15.36 <0.05
50 6.27 <0.05 15.20 <0.05
55 6.39 <0.05 15.03 <0.05
60 6.61 <0.05 14.87 <0.05

Significant differences were found (*P<0.05) at most time points excepting, the generic product A vs. reference until 50 min. when using the flow-through cell apparatus. The statistical analysis emphasized the great sensitivity and discriminative capacity of the flow-through cell apparatus in the evaluation of the in vitro release of ibuprofen suspensions in comparison to the official USP paddle apparatus.

After the application of the three methods to compare the dissolution profiles of two generic products of ibuprofen suspensions against the reference it can be observed that with the use of the USP Apparatus 2, the dissolution profiles of the generic products A and B were dissimilar, however, with the flow-through cell apparatus only the generic product B had dissimilar dissolution profile. The relationship of these differences with the in vivo performance has not been demonstrated yet. Because little information is available on ibuprofen suspensions under the hydrodynamic environment generated by the USP Apparatus 2 and 4, additional research is necessary. Some authors have suggested the optimization of the flow-through cell to obtain reliable and discriminative results reflecting the formulation variables prior to bioequivalence testing [12]; as well as the in vivo bioequivalence studies for generic and brand drugs are required to be conducted to ascertain more precise therapeutic and clinical equivalence [28]. Finally, it is important to emphasize that this is the first in vitro release study of ibuprofen generic suspensions comparing the flow-through cell method and the official USP paddle apparatus. The clinical impact of the results here obtained should be evaluated using appropriate clinical protocols.

CONCLUSION

Characterization of the in vitro release of ibuprofen suspensions using the flow-through cell apparatus revealed similarities in the dissolution rate of the generic formulation A and the reference product. Given the physicochemical characteristics of ibuprofen and the environment in which the formulations were tested, the differences found with the generic formulation B could be of clinical relevance.

CONFLICT OF INTERESTS

All authors have none to declare

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