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メトセル™ プレミアム CR セルロースエーテル(放出制御)


親水性マトリックスシステム製剤の第一選択であり、経口固形製剤からの徐放/放出制御のロバストなメカニズムを提供します。粘度グレードを選択することにより、メトセルTMプレミアムセルロースエーテルはさまざまな薬物の溶解度に対応できるシンプルなソリューションを提供します。錠剤は既存の装置や加工方法により簡単に製造できます。
マトリックス錠剤の処方
アプリケーション | 利点 | 通常使用されるメトセルセルロースエーテル |
---|---|---|
溶解性の低い薬物 | ポリマーが迅速に吸水する事でゲル層を形成; 非イオン性 | E50LV, K100LV, K100LV CR |
溶解性が中程度から高い薬物 | ポリマーが迅速に吸水する事でゲル層を形成; 非イオン性 |
K4M, K15M, K100M, E4M, E10M, K4MCR, K15MCR, K100MCR, E4MCR, E10MCR |
カラコンは、IFFの放出制御に使用されるメトセルTM製品に関するグローバルの独占販売権を所有しています。
METHOCEL™ is a trademark of International Flavors and Fragrances Inc. or its affiliates. © 2021 IFF. All rights reserved
プロダクトアプリケーションデータ

Formulation of an Extended Release Melatonin Dietary Supplement
ドキュメントのダウンロード 電子メールで送信Due to melatonin's short half-life, nutra companies face a challenge designing extended release tablets. Learn how hypromellose may be a solution.
Maintaining Similar Drug Release from Hypromellose Matrices with Identical Dimensions but Different Dose Strengths
ドキュメントのダウンロード 電子メールで送信Method to maintain similar drug release, tablet shape and weight, from a METHOCEL matrix, while adjusting the drug dose.
Technical Bulletin: METHOCEL™ K200M
ドキュメントのダウンロード 電子メールで送信Introducing METHOCEL K200M for extended release formulation
Technical Bulletin:Film Coating of Hydrophilic Matrices
ドキュメントのダウンロード 電子メールで送信Film Coating of Hydrophilic Matrix Tablets : Safety Considerations for Product Design to Minimize Medication Errors
一般的な情報

General Properties of METHOCEL™ Premium Cellulose Ethers
ドキュメントのダウンロード 電子メールで送信This product data sheet describes chemical and physical properties of METHOCEL premium cellulose ethers.
How to Prepare Aqueous Solutions of METHOCEL™
ドキュメントのダウンロード 電子メールで送信Describes preparation of aqueous solutions of METHOCEL.
Quality by Design (QbD) for METHOCEL™ Premium CR Cellulose Ethers
ドキュメントのダウンロード 電子メールで送信Introduction to QbD initiatives for the robust design of product and manufacturing process of hydrophilic matrices.
製品カタログ

Using METHOCEL™ Cellulose Ethers for Controlled Release of Drugs in Hydrophilic Matrix Systems
ドキュメントのダウンロード 電子メールで送信ポスター

AAPS 2005 - Investigation of a Directly Compressible Hypromellose Matrix Formulation for a Low Dose, Practically Insoluble Drug
ドキュメントのダウンロード 電子メールで送信Formulation of an ER direct compression Indapamide (1.5 mg) matrix tablet using METHOCEL
AAPS 2005 - Particle Swelling and Coalescence to Gel Layer Formation
ドキュメントのダウンロード 電子メールで送信Swelling and coalescence behavior of HPMC and Starch 1500, in order to monitor the contribution to gel layer formation in matrices.
AAPS 2006 - Evaluation of Verapamil HCl ER Matrix Formulations
ドキュメントのダウンロード 電子メールで送信Investigating the use of dissolution testing apparatus III and biorelevant dissolution media to understand in vivo release of drug from hydrophilic matrices.
AAPS 2006 - Influence of Hydro-Alcoholic Media on Hypromellose Matrix Systems
ドキュメントのダウンロード 電子メールで送信Effect of hydro-alcoholic dissolution media on the swelling and drug release properties of METHOCEL matrices.
AAPS 2006 - Modulation of Drug Release from Hypromellose (HPMC) Matrices: Suppression of the Initial Burst Effect
ドキュメントのダウンロード 電子メールで送信Method to minimize a burst of drug release typically observed in the early phases of release of highly soluble actives from METHOCEL matrices.
AAPS 2007 - Bi-Phasic Drug Release from Drug Layered, ER Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Process to achieve an immediate and extended release profile from an HPMC matrix system.
AAPS 2007 - Influence of Anionic Polymers on Hydrochlorothiazide ER Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Blending anionic polymers with HPMC to extend release; effects of varying polymer blend ratio and excipient choice - drug release profile and textural properties.
AAPS 2007 - Investigation of the Effects of Hydro-Alcoholic Media on Rheological and Textural Properties of Various Grades of Hypromellose
ドキュメントのダウンロード 電子メールで送信Effect of hydro-alcoholic dissolution media on the textural properties of METHOCEL matrices, and rheological properties of METHOCEL solutions.
AAPS 2008 - Influence of Hydrodynamic Conditions on Verapamil Hydrochloride Release from Hydrophilic Matrices Using Ionic and Non-Ionic Polymers
ドキュメントのダウンロード 電子メールで送信Combination of HPMC with ionic polymers in ER matrices, with a soluble API, provides robust formulations which are insensitive to hydrodynamic conditions.
AAPS 2010 - Application of QbD Principles to the Formulation of ER Propranolol Hydrochloride Hydrophilic Matrix Tablets
ドキュメントのダウンロード 電子メールで送信Effects of variation in hypromellose physico-chemical properties on powder flow, tablet physical properties and in vitro drug release profiles, from an ER hydrophilic matrix tablet using QbD principles.
AAPS 2010 - Effect of Filler Type on Low Dose Acetaminophen Hydrophilic Matrix Formulations
ドキュメントのダウンロード 電子メールで送信Effect of four commonly used fillers in formulation and processing of HPMC matrices utilizing a high shear wet granulation process.
AAPS 2011 - Barrier Membrane Coating of Hydrophilic Matrices of Sparingly Soluble Drug, Acetaminophen: A Strategy to Reduce Possible Food Effect
ドキュメントのダウンロード 電子メールで送信Application of a barrier membrane (BM) coating consisting of Surelease and a pore-former, Opadry.
AAPS 2011 - Influence of Sodium Carboxymethylcellulose on Drug Release from Polyethylene Oxide and Hypromellose ER Matrices
ドキュメントのダウンロード 電子メールで送信Influence of ionic polymer NaCMC, on the release of model drug from ER formulations containing non-ionic polymers, PEO or HPMC, as matrix formers.
AAPS 2012 - Barrier Membrane Coated Hydrophilic Matrices: Robustness of Metoprolol Tartrate Release under Biorelevant Test Conditions – Impact of Media Composition
ドキュメントのダウンロード 電子メールで送信Joint poster - Ernst Moritz Arndt University & Colorcon
AAPS 2012 - Critical Material Attributes Consideration for ER Propranolol HCl Hydrophilic Matrix Tablets
ドキュメントのダウンロード 電子メールで送信Hypromellose CMA had no significant effect on the physical properties of ER matrix tablets, but may impact drug release profiles when level of METHOCEL is low (15% w/w).
AAPS 2013 - Investigation of Drug Release Performance of Hydrophilic Extended Release Formulations in Bio-Relevant Media
ドキュメントのダウンロード 電子メールで送信Drug Release Performance of Hydrophilic ER Formulations in Bio-Relevant Media
AAPS 2014 - Study of Dose-proportionality in Hydrophilic Matrix Tablets using Propranolol HCl as a Model Drug
ドキュメントのダウンロード 電子メールで送信Study of the surface area to volume ratio (SA/V) of uncoated matrices analyzed to explore feasibility of getting similar release profiles at proportional weights of tablets.
AAPS 2015 - Eliminating Burst Release of Highly Soluble Drug from Hydrophilic Matrix Tablets Using Venlafaxine as a Model Drug
ドキュメントのダウンロード 電子メールで送信Combination of ionic low viscosity polymer with high viscosity Hypromellose reduced drug release within first 2 hours of dissolution.
CRS 2003 - The Influence of Film Coatings on Performance of Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Study on the influence of three film coating systems on the performance of hypromellose sustained release matrices, stored under different conditions up to 12 months.
CRS 2005 - Relevance of USP Methodology in the Development of a Verapamil Hydrochloride (240mg) ER Formulation
ドキュメントのダウンロード 電子メールで送信Impact of the type of dissolution testing method on drug release.
CRS 2006 - Effect of Film Coating and Storage Conditions on the Performance of Metformin HCl 500 mg ER Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Influence of three film coating systems on the performance of Metformin HCl (500mg) extended release (ER) Hypromellose matrices.
CRS 2006 - Influence of Formulation Variables on Drug Release Kinetics from Hypromellose ER Matrices
ドキュメントのダウンロード 電子メールで送信Mathematical modeling to summarize the influence of several formulation variables on drug release from METHOCEL matrices.
CRS 2006 - Investigation of a Venlafaxine HCl ER Formulation using Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Minimizing burst of drug release of highly soluble actives from METHOCEL matrices; granulation of the drug, and coating on top of the matrix, with Surelease
CRS 2008 - Use of Roller Compaction in the Preparation of Verapamil Hydrochloride ER Matrix Tablets Containing Hydrophilic Polymers
ドキュメントのダウンロード 電子メールで送信Evaluation of roller compaction on the flow and compressibility of blends of HPMC, polyvinyl acetate phthalate(PVAP) and carbomer - ER verapamil HCl matrix formulation.
CRS 2009 - Investigation of Moisture-Activated Granulation of Hydrophilic Polymer Blends in Verapamil HCl ER Matrices
ドキュメントのダウンロード 電子メールで送信Effects of processing on the properties of the polymer blend, tablets and drug release.
CRS 2009 - Investigation of the Effect of Tablet Geometry and Film Coating on Drug Release from Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Different tablet shapes to evaluate the effect of geometry on the release of model drugs, with varying aqueous solubility and dose, from hydrophilic matrices at constant tablet surface area/volume ratios.
CRS 2010 - Effect of Processing Conditions on Hypromellose Matrix Formulations of Acetaminophen Prepared by a High Shear Wet Granulation Process
ドキュメントのダウンロード 電子メールで送信Processing guidelines for developing a hypromellose matrix formulation using a wet granulation process; with extra-granular addition of HPMC and Starch 1500 resulting in increased tablet hardness.
CRS 2010 - Utility of Ultra-High Viscosity Hypromellose in ER Matrix Formulations
ドキュメントのダウンロード 電子メールで送信Showing that the use of ultra-high viscosity BENECEL K200M in an ER matrix system did not show any advantage in drug release retardation compared to METHOCEL K100M.
CRS 2011 - Application of QbD Principles to the Formulation of ER Theophylline Hydrophilic Matrix Tablets
ドキュメントのダウンロード 電子メールで送信Ranges of viscosity, % HP and particle size of METHOCEL™ K15M Premium CR had no significant effect on physical properties of power blends, tablet physical properties and drug release profiles.
CRS 2011 - Use of Starch 1500® to Minimize Variability on Drug Release from Hypromellose Matrices
ドキュメントのダウンロード 電子メールで送信Starch 1500 in formulation design, supporting QbD study and minimizing formulation variability
CRS 2012 - Barrier Membrane Coating of Hydrophilic Matrices of a Very Soluble Drug, Metoprolol Tartrate at High Dose: A Strategy to Eliminate the Initial Burst Release
ドキュメントのダウンロード 電子メールで送信Application of barrier membrane (BM) coating, using Surelease with a pore-former, Opadry; elimination of the burst effect, followed by near zero order release.
CRS 2013 - Barrier Membrane Coating of Hydrophilic Matrices: A Simplified Strategy to Attain Zero Order Drug Release
ドキュメントのダウンロード 電子メールで送信Alternative formulation strategy for dosage forms where zero order release of drug is desired
CRS 2013 - Consideration of Critical Material Attributes in Hypromellose-Based Hydrophilic Matrices Comprising Drugs of Various Solubility
ドキュメントのダウンロード 電子メールで送信Case studies using theophylline (water solubility 8.3 mg/ml) or HCTZ (water solubility ~0.7 mg/ml) with METHOCEL K4M and Starch 1500 as the matrix former
CRS 2017 - Approaches to Reduce the Weight of Extended Release Tablets: Metformin HCl
ドキュメントのダウンロード 電子メールで送信CRS 2017 - Study of Dose-Weight Proportionality of IR/SR Fixed Dose Combination
ドキュメントのダウンロード 電子メールで送信CRS 2018 - Application of Barrier Membrane Coating to Reduce the Weight of Metformin HCI Extended Release Tablets
ドキュメントのダウンロード 電子メールで送信CRS 2020 - Effect of Different Fillers on Low Dose Extended Release Hydrophilic Matrix Tablets
ドキュメントのダウンロード 電子メールで送信CRS 2020 Poster Reprint
ホワイトペーパー/記事

Applications of Complementary Polymers in HPMC Hydrophilic Extended Release Matrices
ドキュメントのダウンロード 電子メールで送信Drug Delivery Technology - July/Aug 2009
Excipient Update: Influence of fillers, compression force, film coating, and storage conditions on performance of hypromellose matrices
ドキュメントのダウンロード 電子メールで送信Drug Delivery Technology - Jan/Feb 2004
Influence of Excipients on Drug Release from Hydroxypropyl Methylcellulose Matrices
ドキュメントのダウンロード 電子メールで送信JOURNAL OF PHARMACEUTICAL SCIENCES, VOL. 93, NO. 11, Nov 2004
Investigation of the Influence of Tablet Shape, Geometry & Film Coating on Drug Release From Hypromellose Extended-Release Matrices
ドキュメントのダウンロード 電子メールで送信Drug Delivery Technology article published March 2010.