Przejdź do zawartości
Merck
HomeSolid Formulation StrategiesDry Granulation in Solid Oral Formulation: Advantages of Spray-Dried Mannitol in Roll Compaction

Dry Granulation in Solid Oral Formulation:
Advantages of Spray-Dried Mannitol in Roll Compaction

Spray-dried Mannitol

The Application of Fillers and Binders in Solid Dosage Formulation

Pharmaceutical excipients are frequently used as fillers and fillers/binders in the formulation of solid dosage forms. Fillers add volume and confer mechanical properties that offer greater flowability and compressibility which facilitate manufacturing and increase final formulation robustness and content uniformity. These aspects are particularly relevant in the formulation of highly potent, low dose active pharmaceutical ingredients (APIs) where content uniformity can be challenging.

Advantages of Mannitol for Solid Dosage Formulation

In recent years, mannitol has gained popularity as an excipient in solid dosage formulation due to its beneficial physicochemical properties. Because it is chemically inert, has good compactibility, and low hygroscopicity1, it can be used in formulations to produce robust tablets and as a diluent in rapidly dispersing oral dosage forms.2 It also has a good taste and mouth feel enabling its use for chewable, sublingual and orodispersible tablet formulations.

A variety of pre-processed and unprocessed grades of mannitol are commercially available for use as an excipient in pharmaceutical formulations. For production of dosage forms for oral administration by direct compression processes, directly compressible grades are available.

In cases where a direct compression process is not suitable due to possible separation or de-mixing of components of varying particle sizes, dry granulation can be included before tableting. This step can increase the bulk density of powders and improve flow properties. Moreover, it helps to improve content uniformity of the final formulation which is essential when processing highly potent APIs. Mannitol can serve as a filler/binder for dry granulation by roller compaction, which can be used for moisture or heat sensitive APIs as no solvents, liquid binders or elevated temperatures are applied in the process.3

The following studies, funded by our organization and performed by researchers from Heinrich-Heine University, Duesseldorf, Germany, explored tableting behavior and comparative compressibility of various pre-processed and unprocessed mannitol grades in dry granulation. The roller compaction behavior of different mannitol grades was investigated in placebo formulations or in combination with enalapril maleate as a model low-dose API. Results of these studies reveal differences in performance and can help guide selection of the best mannitol grade for dry granulation processes.

Tableting Behavior of Spray-Dried Mannitols

This study compared the suitability of spray-dried mannitol grades for roller compaction and the suitability of the resulting granules for tableting processes.4

Five spray-dried and commercially available mannitol grades (designated “A” through “E”) with similar particle size distributions were selected to explore their suitability for roller compaction and subsequent tableting processes.

Powders were granulated using an instrumented roller compactor (Mini-Pactor® 250/50, Gerteis Maschinen + Processengineering AG) with the compaction force set to 2 kN/cm and 10 kN/cm, respectively; the gap between the rolls (1.5 mm) and the roll speed (5 rpm) were kept constant during the process. For unprocessed grades, the roll speed was set to 3 rpm with a gap of 2.0 mm. Ribbons were granulated with a star-granulator using a 1.25 mm sieve. The granules were mixed with 1% magnesium stearate and compressed on a rotary tablet press (Pressima, IMA S.p.A.) equipped with planar 10 mm punches at compression forces of 3, 6, 9, 12 and 15 kN into tablets with a total tablet weight of 500 mg.

Tablets formulated using mannitol A and B (Parteck® M 100 and Parteck® M 200 excipients, respectively) achieved the highest tensile strength after direct compression due to the large specific surface area of the raw material (Figure 1). In contrast, mannitol E lacked a sufficient surface area for bonding during tableting and this led to tablets with decreased mechanical resistance (Figure 1, Figure 3). BET results show that in general, when compared to the raw material, the specific surface area of the granules was increased after roller compaction. This effect became more apparent at high compaction forces and could be detected for every investigated mannitol grade. The increase of granule surface area can be attributed to extensive fragmentation of the brittle mannitol which is more pronounced when higher compaction forces are applied.5

BET surface area (n = 3) of roller compacted granules in comparison to the powder material, measured using nitrogen absorption surface analysis.

Figure 1.BET surface area (n = 3) of roller compacted granules in comparison to the powder material, measured using nitrogen absorption surface analysis.

With increasing compaction forces used in the roller compaction process, a loss of compressibility was observed for all excipients (Figure 2). This effect can be associated with particle size enlargement and the work-hardening phenomenon following roller compaction.6 As shown in Figure 3, however, both mannitol A and B required less compression force to achieve the desired friability of <1%.

Tensile strength of tablets made of granules roller compacted at A) 2 kN/cm and B) 10 kN/cm (n = 10), calculated according to Fell and Newton.

Figure 2.Tensile strength of tablets made of granules roller compacted at A) 2 kN/cm and B) 10 kN/cm (n = 10), calculated according to Fell and Newton.6

Friability of tablets made of granules roller compacted at A) 2 kN/cm and B) 10 kN/cm (n = 3), measured according to Ph. Eur.

Figure 3.Friability of tablets made of granules roller compacted at A) 2 kN/cm and B) 10 kN/cm (n = 3), measured according to Ph. Eur.

This study demonstrated that while roller compacting spray-dried mannitol grades resulted in robust tablets, final formulation performance was strongly dependent on the type of mannitol. Parteck® M 100 and Parteck® M 200 mannitols (A and B) were shown to produce granules with the largest surface area and tablets with highest tensile strength and lowest friabilities.

Comparison of Pre-Processed and Unprocessed Mannitols

The purpose of this study was to compare the roller compaction and tableting behavior of commercially available pre-processed (spray-dried and granulated) mannitol grades and unprocessed crystalline mannitol in its β- and δ-modification.7

The mannitol grades evaluated included two preprocessed granulated grades, designated “A” and “B”, and two spray-dried grades, designated “C” (Parteck® M 200 excipient) and “D”. Crystalline mannitol in the β- (“E”) and δ-form (“F”) were selected as unprocessed material. All powders were granulated, and tablets produced and characterized as described in the first case study. Compression forces of 3–18 kN were applied to produce the tablets.

While roller compaction of mannitol A and B led to tablets with sufficient tensile strength applying compression forces ≥ 9 kN, granules made of spray-dried raw materials (C and D) were characterized by a superior compressibility and higher tensile strengths even at lower compression forces (Figure 4).

Compressibility of granules made using unprocessed and pre-processed mannitol grades roller compacted with A) 2 kN/cm and B) 10 kN/cm (n = 10).

Figure 4.Compressibility of granules made using unprocessed and pre-processed mannitol grades roller compacted with A) 2 kN/cm and B) 10 kN/cm (n = 10).

As in the first case study, a loss in compressibility was observed for every mannitol grade (pre-processed and unprocessed β- and δ-mannitol) with increasing compaction force used in the roller compaction process (Figure 4). This can be attributed to particle size enlargement and the work-hardening phenomenon.6

In accordance with the results of the first case study, the specific surface areas of the granules increased after roller compaction (Figure 5). This effect became more apparent at high compaction forces and can be attributed to the strong fragmentation behavior of mannitol.8 Tablets of Parteck® M 200 excipient (“C”) showed a considerably larger interparticular contact area due to the large BET surface area of both powder and granules (Figure 5) which resulted in higher tensile strength (Figure 4).

BET surface area (n = 3) of granules in comparison to the powder material.

Figure 5.BET surface area (n = 3) of granules in comparison to the powder material.

This study demonstrated that while roller compaction of granulated starting materials and crystalline δ-mannitol resulted in granules and tablets with desirable properties, the spray-dried grade with the largest surface area (mannitol C = Parteck® M 200 excipient) showed good compactibility during the dry granulation process and exhibited superior compressibility during the tableting process when compressed into the final dosage form.

Roller Compaction Behavior and Tabletability of Mannitol-Based Enalapril Formulations

The case studies described above demonstrated that unprocessed, crystalline δ-mannitol, spray-dried and granulated grades are suitable for roller compaction. The following study was undertaken to evaluate roller compaction behavior of different mannitol grades in combination with enalapril maleate as model low-dose API as well as the tableting performance of the resulting granules.9

Enalapril maleate and different mannitol grades were blended for 20 minutes in a shaker-mixer at 50 rpm. The powder mixtures were granulated using an instrumented roller compactor (Mini-Pactor® 250/25, Gerteis Maschinen + Processengineering AG) with a compaction force of 8 kN/cm. The gap between the rolls (2 mm) and the roll speed (3 rpm) were kept constant during the process. Ribbons were granulated with a star-granulator using a 1.25 mm-sieve. The granules were mixed for 2 minutes with 1% magnesium stearate. Tablets with a total drug load of 2.5 mg enalapril maleate and a total tablet weight of 200 mg were produced on an instrumented rotary tablet press (Pressima, IMA S.p.A.) equipped with planar 8 mm punches, using compression pressures of 3–18 kN.

All formulations could be roller compacted to granules and compressed into tablets. Roller compaction of enalapril maleate and spray-dried mannitol yielded granules with low amounts of fines and good flow properties (formulation A and B, with A using Parteck® M 200 excipient; Table 1). In contrast, granules of pre-granulated raw material and unprocessed δ-mannitol were characterized by higher amounts of small particles (formulation C and D; Figure 6), which is an explanation for the fair flowability in comparison to the good flowability of granules based on spray-dried mannitol grades.

Table 1.Amount of fines and ffc values of the granules (mean +/- s, n = 3). Particle size distribution was determined via digital image analysis; fines were considered to be particles ≤90 μm. Flowability of the granules was determined as the flowability function (ff) using an automated ring shear tester.
Particle size distribution of the produced granules (n = 3), determined via digital image analysis.

Figure 6.Particle size distribution of the produced granules (n = 3), determined via digital image analysis.

Formulation A tablets based on Parteck® M 200 mannitol showed the highest tensile strengths (Figure 7).

Compressibility of the produced granules (n = 10). Tensile strength was calculated according to Fell and Newton.

Figure 7.Compressibility of the produced granules (n = 10). Tensile strength was calculated according to Fell and Newton.6

As shown in Table 2, all tablets assessed for content uniformity met the Ph. Eur. requirements (2.9.40).

Table 2.Acceptance values according to Ph. Eur. 2.9.40 (n = 10) for formulations A, B and D.

Enalapril maleate formulations based on the different mannitol grades were successfully produced via roller compaction and had the desired flow properties, an acceptable amount of fines and met pharmacopoeial requirements for content uniformity. Tablets containing granules based on Parteck® M 200 spray-dried mannitol (formulation A), however, showed the highest tensile strengths, very low amount of fines and best content uniformity compared to other grades.

Optimizing a Solid Dose Formulation with Mannitol

While a number of commercially available mannitol options are suitable for dry granulation, these case studies highlight important differences among various grades. Performance is strongly dependent on the type of mannitol used; in all cases, spray-dried mannitols produced granules with improved compressibility in comparison to granulated or crystalline mannitol grades, resulting in tablets with higher tensile strength and lower friabilities.

When comparing different commercially available spray-dried mannitol grades, a high initial surface area of the mannitol was a critical success factor. Parteck® M excipients showed the highest surface areas before and after granulation. These excipients offered distinct advantages in terms of compressibility and tensile strength of the resulting tablets both in placebo and verum formulations.

These case studies confirm that all investigated mannitol grades were suitable for roller compaction and highlighted important differences among the materials. In all cases, spray-dried mannitol with a high surface area produced granules and tablets with superior properties as evidenced by the advantages of compressibility and tensile strength both in placebo and API formulations.

As such, roller compaction can be successfully used to improve tableting performance of the selected formulation in terms of flow properties and content uniformity of the final dosage form. It is important to note however, that the selected excipient grade is critical for formulation performance. This is why excipient particle properties should be considered early in the formulation development process to ensure a robust final product as well as a smooth transition to commercial scale. If the optimum grade of mannitol is used from the beginning of the process, performance of the final formulation will be superior in comparison to processes using other, less suitable grades.

Learn more about formulation development and guidelines for these manufacturing processes and suitable excipients in our Formulation Handbook.


Products
Loading

References

1.
Ohrem HL, Schornick E, Kalivoda A, Ognibene R. 2014. Why is mannitol becoming more and more popular as a pharmaceutical excipient in solid dosage forms?. Pharmaceutical Development and Technology. 19(3):257-262. https://doi.org/10.3109/10837450.2013.775154
2.
Rowe, et al. Handbook of Pharmaceutical Excipients, 7th Edition. London: Pharmaceutical Press, 2012.
3.
Smith TJ, Sackett G, et al. Development, scale-up, and optimization of process parameters: roller compaction. In: Qiu Y, Chen Y, Zhang G, Liu L, Porter W, editors. Developing Solid Oral Dosage Forms: Pharmaceutical Theory and Practice. 1 ed. Oxford: Elsevier Ltd.; 2009. p. 715–24..
4.
Summarized from poster “Roll compaction of mannitol: Tableting behavior of various spray-dried mannitols before and after dry granulation” presented at 2012 AAPS Annual Meeting; data collected in cooperation with Heinrich-Heine University, Duesseldorf, Germany. Authors: CM. Wagner, G. Moddelmog, H. Ohrem, J. Breitkreutz.
5.
Herting M, Kleinebudde P. 2008. Studies on the reduction of tensile strength of tablets after roll compaction/dry granulation. European Journal of Pharmaceutics and Biopharmaceutics. 70(1):372-379. https://doi.org/10.1016/j.ejpb.2008.04.003
6.
Fell J, Newton J. 1970. Determination of Tablet Strength by the Diametral-Compression Test. Journal of Pharmaceutical Sciences. 59(5):688-691. https://doi.org/10.1002/jps.2600590523
7.
Summarized from poster “Roll compaction of mannitol: Comparative compactibility study of various pre-processed and unprocessed mannitol grades” presented at 2013 AAPS Annual Meeting; data collected in cooperation with Heinrich-Heine University, Duesseldorf, Germany. Authors: CM. Wagner, M. Pein, G. Moddelmog, J. Breitkreutz.
8.
Nordström J, Klevan I, Alderborn G. 2012. A protocol for the classification of powder compression characteristics. European Journal of Pharmaceutics and Biopharmaceutics. 80(1):209-216. https://doi.org/10.1016/j.ejpb.2011.09.006
9.
Summarized from poster “Applicability of roll compaction for mannitol based enalapril formulations” presented at 2014 PBP World Meeting on Pharmaceutics; data prepared by Heinrich-Heine University, Duesseldorf, Germany. Authors: CM. Wagner, M. Pein, J. Breitkreutz.
Zaloguj się, aby kontynuować

Zaloguj się lub utwórz konto, aby kontynuować.

Nie masz konta użytkownika?