Laurie core ™ (Suglets ®) of high quality medicinal pill core

AAPS 2014 - about ethyl cellulose viscosity changes of the effect of metoprolol sustained-release particles drug release more QbD (design) quality research

Within the manufacturer specification more show the viscosity changes little effect on drug release of slow-release many particles

AAPS 2014 - as a drug carrier laminated sugar pill robustness testing related methods of evaluation

The purpose of this study was designed to evaluate the laboratory and plant scale fluidized bed process produced by the abrasion value compared to the use of oscillation device brittle broken degree determination method to determine the mechanical strength of high quality medicinal pill core Laurie core.

AAPS 2015 - full formula ethyl cellulose membrane coating weight of the coating system and control the pore level effect on drug release

AAPS 2015 - high soluble drugs using ethyl cellulose powder layer of flavor prescription mask product feasibility study

AAPS 2015 poster reprint - this study verifies the love show 7 FP laminated powder as a kind of efficient taste mask technology feasibility.

AAPS 2016 by design of experiment (DOE) optimization of many particles rolling process

This study aims to evaluate the preparation of drug-loading particles more extruding rolling process.By design of experiment (DOE) evaluation formula and the number of process parameters, understand compared with the existing standard sugar pill core products, extrusion rolling process on the particle size and distribution of micro pill, roundness, brittle broken degree and target size affects the yield of micro pill.

AAPS 2017 - more than using particle formula design tool to predict and using process analysis technology and measurement formula ethyl cellulose water medium and coating film thickness of the organic solvent system

AAPS 2020 - different formulation and process of biopharmaceutics classification 1 drugs use Aquacoat ® ECD - 30 membrane coating

AAPS 2020 - Jacques appropriate ® II (Acryl - EZE ® II) coating of omeprazole enteric capsule in vitro and in vivo evaluation after the meal

AAPS 2020 - using exhaust absolute humidity as many particles coating research of control parameters

AAPS 2020 - about through nasogastric tube in esso beauty pull azole late release more granular enteric coating system of in vitro evaluation

AAPS 2021 - using ethyl cellulose dispersed system of propranolol hydrochloride sustained-release drug release stability of many particles

CRS 2008 solvent types of ethyl cellulose membrane release

The aim of this study was to investigate four acceptable solvent combination pellet of EC solution viscosity and the coating effect of drug release.

CRS 2009 - coating system type acetaminophen from ethyl cellulose barrier film coating of the influence of particle release more

2009 CRS posters, coating system type acetaminophen from ethyl cellulose barrier film coating of the influence of particle release more

CRS 2009 - the type and dosage of plasticizer on drug release from ethyl cellulose membrane in the pellet controlled release coating

Plasticizer was studied in maleic acid chlorobenzene the quick release from controlled release coating pellet ethyl cellulose membrane.The type and dosage of plasticizer effect of drug release rate.Choose the type and dosage of plasticizer can be used as an effective method to control drug release.

CRS 2009 molecular weight on drug release from ethyl cellulose barrier membrane more particles

2009 CRS posters, molecular weight on drug release from ethyl cellulose barrier membrane more particles

CRS 2010 - hole agents of ethyl cellulose coating micro pill the effect of drug release

This paper studies the hydrophilic hole agents hydroxypropyl methyl cellulose (HPMC) added to the ethyl cellulose coating and applied to the isopropyl alcohol aqueous solution in the case of (9:1).

CRS 2011 - drug solubility of ethyl cellulose membrane coating micro pill control release

We studied the drug solubility for love show ™ (ETHOCEL ™) medicinal grade ethyl cellulose (EC) coating pellet the effects of drug release.Drug solubility decrease, drug release delay.In addition to the drug solubility, other factors such as drug affinity of membrane control or drugs of ionization degree also can affect the drug release rate.

CRS 2011 - dissolution medium pH value in the micro pill of ethyl cellulose coating effect of drug release

We studied the dissolution medium pH value to love many beautiful ™ (ETHOCEL ™) medicinal grade ethyl cellulose coating pellet the effects of drug release.The results showed that the drug release has nothing to do with the dissolution medium pH.

CRS 2014 - using QbD sample evaluation of ethyl cellulose viscosity changes on the influence of the drug release preparation more grain

The purpose of this study, is within the scope of the producer, product quality standard, evaluation standard level of medicinal product viscosity change for love show the in vitro release of APAP more.

CRS 2016 - why more pill core?

The study explained in the development of many particles sustained-release preparations, choose the larger high quality medicinal pill core as its starting pill core advantage.At the same time

CRS 2016 - full formula ethyl cellulose membrane coating composition and performance of the system stability control

This study aimed to ethyl cellulose organic coating systems - generation ® EC, Obama in intermediate and accelerate 6 months stored under the storage conditions of the composition of the stability and the slow release performance were studied.

CRS 2016 - dose - weight in slow-release more granular system is proportional to the formulation of research

Use of fluidized bed coating machine and ethyl cellulose membrane coating system, the acetaminophen (APAP) laminated prescription pill core after coating.Then different doses of acetaminophen more particles have coating on dose - weight is proportional to the performance of detection, and carries on the comparison to drug release curve.The argument in slow-release more granular system dose - weight is proportional to the idea.This study was to evaluate the different slow release formulation dose - a continuation of the weight is proportional to the strategy

Control micro pill membrane coating sino-soviet Liz ® (Surelease ®) theoretical weight and a comparative study of the actual weight

The purpose of this study is quantitative analysis in the theory of different weight of drug-loading Laurie wire coating sugar pill on ethyl cellulose deposition quantity.Evaluation of Laurie silk ® (Surelease ®) coating micro pill of chlorpheniramine maleate in release curve.

Bitter to Better: Formulation Strategies for Effective Taste Masking

April 2018 Article Tablets and Capsules Magazine, Author Charles Vesey

CRS 2021 _ to the use of the preparation of ethyl cellulose some easy soluble drug propranolol hydrochloride sustained-release pellet formula evaluation

CRS 2021 _ bottom spray fluidized bed process of some using ethyl cellulose membrane layer coating of pharmaceutical product the influence of micro pill

Smell - covering good medicine tastes bitter, no longer smell the formulation strategy covering effectively

In April 2018 Tablets and Capsules Magazine, author Charles Vesey