wet and dry granulation binder a technical...
TRANSCRIPT
Wet and Dry Granulation BinderA Technical Review
Pharma & Food Solutions
pg 2 pg 3
Granulation Binder - Technical Bulletin | 09-2013Granulation Binder - Technical Bulletin | 09-2013
On the right we provide the results of several studies included in our extensive testing program. These provide representative examples of the effects of METHOCEL™ binders on tablet properties.
Acetaminophen: high-dose, low-solubility drug in the wet-granulationIn a formulation with 50% acetaminophen, METHOCEL™ demonstrated good hardness at concentrations of 3% and 6% of total tablet weight. In some formulations, METHOCEL™ polymers can even provide optimum tablet properties at concentrations of 1% and lower. This ability to provide good hardness at low concentrations makes METHOCEL™ ideal for formulations that contain a high percentage of active drug or other excipients.
Formulating the Medicines That Provide People with Immediate Relief
METHOCELTM Can Help You Get There
When you’re developing immediate release tablet and capsule medicines, we know what you’re looking for: good tablet hardness at low concentration, versatility and compliance with applicable government requirements.
Producing a tablet with a high concentration of the active drug requires a binder that is highly effective at low concentrations. For this, choose METHOCEL™ Premium products from Dow Pharma & Food Solutions, which deliver the necessary tablet hardness without increasing friability and without negatively impacting the release of the drug.
Why Wait When we Can Help you Deliver NowMETHOCEL™ products provide important binding and adhesive properties during the granulation step of the manufacturing process for immediate release tablet and capsule products. They offer several important benefits for every formulator:
• Now that’s the Tablet we’re Looking For: METHOCEL™ polymers produce hard tablets at very low concentrations – as low as 3% when used in formulations for wet granulation processes (low shear, high shear, and fluid bed) and between 6% and 12% for dry granulation (roller compaction) – without increasing friability. With METHOCEL™, minimize tablet size while maximizing the ability to use other excipients to optimize other tablet characteristics, which makes these polymers ideal in formulations with high active drug concentrations.
•Whatever You Need, We Can Help: METHOCEL™ products offer flexibility when manufacturing tablets. Wet and dry granulation processes provide important characteristics to the finished product, including better product flow on tablet presses and capsule-filling equipment, better compressibility and overall improved physical characteristics of tablets, uniform drug content within the dosage form, and fewer industrial hygiene constraints. METHOCEL™ is highly effective in both granulating technologies. These polymers also are compatible with virtually all active ingredients and other excipients, and hydrate quickly in process liquids to minimize mixing and preparation time. At the appropriate concentration, METHOCEL™ can be used to add needed viscosity to the granulating liquid to minimize mixing and preparation time. METHOCEL™ products also can be used in solutions or dry-blended into the powder mass that is to be granulated and then hydrated by spraying water.
• Follow the Rules for Success: METHOCEL™ Premium grades comply with the compendia specifications of the Pharmacopoeia of the U.S., Europe, and Japan (current editions) and the Food Chemicals Codex, third edition.
0 0.1 0.25 0.5 1 1.5 2 2.5 5 10
3500
3000
100200300400500
1000
1500
2000
2500
METHOCELTM E5P LV @ 20°CMETHOCELTM A15P LV @ 20°C
METHOCELTM K3P LV @ 20°C
High ShearLow Shear
20
30
10
14.27
21.41
7.13
MET
HO
CEL
TM
A15
Pre
m L
V
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
K3
Prem
LV
HPC PV
P
Viscosity of aqueous solutions containing METHOCELTM at varying concentration and molecular weightViscosity, mPa•s // Concentration, % Binder
Hardness of compressed tablets containing acetaminophen and granulated with 6% dry binder in low-shear and high-shear granulatorsHardness, strong-cobb units // Binder // Hardness, kiloponds
Hardness of compressed tablets containing acetaminophen and granulated with 6% dry binder in low-shear and high-shear granulatorsHardness, strong-cobb units // Binder // Hardness, kiloponds
High ShearLow Shear
Fluid Bed
20
30
10
14.27
21.41
7.13
PVP
HPC
MET
HO
CEL
TM
K3
Prem
LV
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
A15
Pre
m L
V
pg 4
Granulation Binder - Technical Bulletin | 09-2013
USPSpecifications
0 10 20 30 40 50 60 700
10
20
30
40
50
60
70
80
90
100
PVP - 3% METHOCELTM E5 Prem LV - 3%
HPC-EF - 3%METHOCELTM A15 Prem LV - 3%
USPSpecifications
0 5 10 15 20 25 30 35 400
10
20
30
40
50
60
70
80
90
100
PVP - 3% METHOCELTM E5 Prem LV - 3%
HPC-EF - 3%METHOCELTM A15 Prem LV - 3%
Drug release from compressed tablets containing acetaminophen and granulated with 6% dry binder in solution in a low-shear granulatorDrug released, % // Time, min
Drug release from compressed tablets containing acetaminophen and granulated with 6% binder in solution in afluid-bedgranulatorDrug released, % // Time, min
The desirable hardness characteristics of METHOCEL™ also result in friability performance that is well within acceptable limits at both 3% and 6% binder levels. The drug-release performance represents an average of six test runs. In all cases performance of METHOCEL™ binders was within the USP specifications and comparable to that of PVP binders.
USPSpecifications
0 10 20 30 40 50
PVP - 3% METHOCELTM E5 Prem LV - 3%
0
10
20
30
40
50
60
70
80
90
100
HPC-EF - 3%METHOCELTM A15 Prem LV - 3%
Drug release from compressed tablets containing acetaminophen and granulated with 3% dry binder in a high-shear granulatorDrug released, % // Time, min
®TMTrademark of The Dow Chemical Company (“Dow”) or an affiliated company of Dow
pg 6 pg 7
Granulation Binder - Technical Bulletin | 09-2013Granulation Binder - Technical Bulletin | 09-2013
METHOCEL™ at 3% binder level achieved good tablet hardness, though not as consistently high as at 6%. Regardless of the granulation process used, tablets prepared using METHOCEL™ cellulose ethers had friability values below 0.7%. METHOCEL™ A15 Premium LV, E5 Premium LV and K3 Premium LV all demonstrated friability performance that was superior to PVP. The drug-release performance again represents an average of six test runs. In all cases using binders in solution, at least 80% of the active ingredient is released within 15 minutes. For dry binder additions, at least 80% of the active ingredient is released within 30 minutes.
0 105 15 20 25 300
20
40
60
80
100
PVP - 3% METHOCELTM K3 Prem LV - 3%HPC-EF - 3%METHOCELTM E5 Prem LV - 3%
0 40 5010 20 30 600
10
20
30
40
50
60
70
80
90
100
PVP - 6% METHOCELTM K3 Prem LV - 6%HPC-EF - 6%METHOCELTM E5 Prem LV - 6%
Drug release from compressed tablets containing acetaminophen granulated with 3% Dry binder in a high-shear granulator Drug released, % // Time, min
Drug release from compressed tablets containing acetaminophen and granulated with 6% binder in solution in afluid-bedgranulatorDrug released, % // Time, min
Vitamin C (ascorbic acid): high-dose, high-solubility drug in the wet-granulation
In a formulation with 75% ascorbic acid, the hardness values of METHOCEL™ products were equivalent or superior to those achieved with another polymer, polyvinylpyrrolidone (PVP), for all granulating techniques and at both binder levels. Low-shear and high-shear granulations demonstrated comparable hardness values, except for PVP formulations. For PVP, low-shear processing resulted in harder tablets than high-shear processing for dry binder. At 6% binder level in solution, fluid-bed granulations from all products demonstrated excellent tablet hardness, in all cases better than low-shear or high-shear granulations.
High ShearLow Shear
10
15
5
7.13
10.70
3.56
MET
HO
CEL
TM
A15
Pre
m L
V
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
K3
Prem
LV
PVP
HPC
High ShearLow Shear
0.6
0.4
0.8
0.2
MET
HO
CEL
TM
A15
Pre
m L
V
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
K3
Prem
LV PV
P
HPC
High ShearLow Shear
Fluid Bed
20
30
10
14.27
21.41
7.13
MET
HO
CEL
TM
K3
Prem
LV
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
A15
Pre
m L
V
PVP
HPC
Friability of compressed tablets containing ascorbic acid and granulated with 6% dry binder in low-shear and high-shear granulatorsFriability, % weight loss // Binder
Hardness of compressed tablets containing ascorbic acid andgranulatedwith6%binderinsolutioninfluid-bed,low-shear, and high-shear granulatorsHardness, strong-cobb units // Binder // Hardness, kiloponds
Hardness of compressed tablets containing ascorbic acid and granulated with 6% dry binder in low-shear and high-shear granulatorsHardness, strong-cobb units // Binder // Hardness, kiloponds
pg 8 pg 9
Granulation Binder - Technical Bulletin | 09-2013Granulation Binder - Technical Bulletin | 09-2013
Methazolamide: low-dose, low-solubility drug in the wet-granulation
In a formulation of 7.1% methazolamide, METHOCEL™ K3 Premium LV produced the best tablet hardness values at a binder level of 3% using a high-shear granulation process. At 6% binder level, hardness values were essentially equivalent for all binder materials, although low-shear granulation processes tended to perform better than high-shear processes.
6%3%
0.3
0.5
0.1
MET
HO
CEL
TM
A15
Pre
m L
V
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
K3
Prem
LV
PVP
HPC
Friability of Compressed Tablets Containing Methazolamide and Granulated with 3% or 6% Binder in a Solution of Fluid-Bed GranulatorTablet friability, % weight loss // Binder
Fluid-bed granulation offered even less differentiation between the three METHOCEL™ products, with performance again equivalent to the PVP binder. The binder level was not a factor for fluid-bed granulation as additional binder did not consistently result in harder tablets. All binders used in this portion of the study produced tablet with low friability—less than 0.6% and well below the 1% industry norm. In terms of drug release from the tablet, all tablets surpassed USP specifications by a significant margin.
0 10 20 30 40 50 60 70 800
20
40
60
80
100
HPC - 6% PVP - 6%METHOCELTM K3 Prem LV - 6%METHOCELTM E6 Prem LV - 6%
METHOCELTM A16 Prem LV - 6%
USPSpecifications
USPSpecifications
0 10 20 30 40 50 60 700
10
20
30
40
50
60
70
80
90
100
METHOCELTM E5 Prem LV - 3% PVP - 3%HPC-EF - 3%METHOCELTM A15 Prem LV - 3%
METHOCELTM K3 Prem LV - 3%
Drug release from compressed tablets containing methazolamide and granulated with 6% dry binder in a high-shear granulatorDrug released, % // Time, min
Drug release from compressed tablets containing methazolamide and granulated with 3% dry binder in a high-shear granulatorDrug released, % // Time, min
pg 10 pg 11
Granulation Binder - Technical Bulletin | 09-2013Granulation Binder - Technical Bulletin | 09-2013
12,5% Binder6,25% Binder
25% Binder
HPC
-EF
PVP
29-3
2
MET
HO
CEL
TM
K3
Prem
LV
MET
HO
CEL
TM
E15
Prem
LV
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
A15
Pre
m L
V
PVP
K90
CA
PP
ING
4
5
2
3
6
1
Friability of compressed tablets containing niacinamideand prepared using roller compaction at 3 tons pressureFriability, % weight loss // Binder
Hardness of compressed tablets containing niacinamideand prepared using roller compaction at 1 ton pressureHardness, strong-cobb units // Binder // Hardness, kiloponds
Hardness of compressed tablets containing niacinamideand prepared using roller compaction at 3 tons pressureHardness, strong-cobb units // Binder // Hardness, kiloponds
HPC-EF PVP 29-32
PVP K90
METHOCELTM E5 Prem LV
METHOCELTM E15 Prem LV
METHOCELTM K3 Prem LVMETHOCELTM A15 Prem LV
0 605550454035302520151050
5
10
15
20
25
PVP
29-3
2
PVP
K90
12,5% Binder6,25% Binder
25% Binder
HPC
-EF
MET
HO
CEL
TM
K3
Prem
LV
MET
HO
CEL
TM
E15
Prem
LV
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
A15
Pre
m L
V
15
10
25
20
5
14.27
7.13PVP
29-3
2
PVP
K90
12,5% Binder6,25% Binder
25% Binder
HPC
-EF
MET
HO
CEL
TM
K3
Prem
LV
MET
HO
CEL
TM
E15
Prem
LV
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
A15
Pre
m L
V
15
10
20
5
14.27
7.13
PVP
29-3
2 PVP
K90
12,5% Binder6,25% Binder
25% Binder
HPC
-EF
118
MET
HO
CEL
TM
K3
Prem
LV
MET
HO
CEL
TM
E15
Prem
LV
142
MET
HO
CEL
TM
E5 P
rem
LV
MET
HO
CEL
TM
A15
Pre
m L
V29
0
40
50
20
30
70
60
10
Time to 90% drug release from compressed tablets containing niacinamide and prepared using roller compaction at 3 tons pressure Time to 90% drug release, minutes // Binder
Rate of drug release from compressed tablets containing niacinamide with 12.5% binder and preparedusing roller compaction at 3 tons pressureDrug released, % // Time, min
Niacinamide: high-dose, high-solubility drug in the roller-compaction
A study looked at three formulations with niacinamide (88.5%, 82.5% and 70.75%) plus METHOCEL™. The level of pressure applied to the compactor rolls was important to the quality of the finished tablets. In general, low roller pressures resulted in tablets with higher hardness. At the lowest binder level (6.25%), hardness values of tablets produced at 1- and 3-ton pressures were marginal, and friability was excessive. At the highest binder level (25%), hardness was generally improved and friability (with the exception of PVP) was good. At most binder levels and roller pressures, hardness and friability values for the METHOCEL™ products were better than PVP.Tablet drug-release times were primarily a function of binder concentration and molecular weight rather than roller pressure.
For the METHOCEL™ products, the time required to release 90% of the drug at the lowest binder level ranged from 6–8 minutes for the lower molecular weight products (E5 Premium LV and K3 Premium LV) to 5–12 minutes for the higher molecular weight products (E15 Premium LV and A15 Premium LV).
The time required to release 90% of the drug at the intermediate binder concentration increased to 16–18 minutes for E5 Premium LV and K3 Premium LV to 19–40 minutes for E15 Premium LV and A15 Premium LV.
The highest binder concentration required 44 and 59 minutes for K3 Premium LV and E5 Premium LV, respectively, and 290 and 142 minutes for A15 Premium LV and E15 Premium LV, respectively, for 90% drug release.
Times to 90% release for PVP were generally lower than the METHOCEL™ products at the lowest concentration, but the release times were not as sensitive to increases in binder concentration. However, the physical properties of these tablets were poor; i.e, the tablets exhibited capping.
Times to 90% release for the Nisso HPC-EF were between the low and high molecular weight METHOCEL™ products.
®TMTrademark of The Dow Chemical Company (“Dow”) or an affiliated company of Dow • Form No. 198-02294 - 10/13 EST
Dow requests that customers considering use of Dow products in medical applications notify Dow so that appropriate assessments may be conducted. Dow has a Corporate Medical Application Policy in place that guides the use of Dow products in potential new pharmaceutical and medical device uses. Dow reviews all new applications/uses according to this Medical Application Policy to determine if the use is appropriate for Dow materials. Dow does not endorse or claim suitability of its products for specific medical applications. It is the responsibility of the medical device or pharmaceutical manufacturer to determine that the Dow product is safe, lawful, and technically suitable for the intended use. DOW MAKES NO WARRANTIES, EXPRESS OR IMPLIED, CONCERNING THE SUITABILITY OF ANY DOW PRODUCT FOR USE IN MEDICAL APPLICATIONS.
NOTICE: No freedom from infringement of any patent owned by Dow or others is to be inferred. Because use conditions and applicable laws may differ from one location to another and may change with time, Customer is responsible for determining whether products and the information in this document are appropriate for Customer’s use and for ensuring that Customer’s workplace and disposal practices are in compliance with applicable laws and other government enactments. The product shown in this literature may not be available for sale and/or available in all geographies where Dow is represented. The claims made may not have been approved for use in all countries. Dow assumes no obligation or liability for the information in this document. References to “Dow” or the “Company” mean the Dow legal entity selling the products to Customer unless otherwise expressly noted. NO WARRANTIES ARE GIVEN; ALL IMPLIED WARRANTIES OF MERCHANTABILITY OR FITNESS FOR A PARTICULAR PURPOSE ARE EXPRESSLY EXCLUDED.
North America +1 800 447 4369Europe, Middle East, Africa +31 11 567 2626Pacific +60379655392Latin America +55 11 5184 8722
www.dowpharmaandfood.com