Big Chemical Encyclopedia

Chemical substances, components, reactions, process design ...

Articles Figures Tables About

Pharmaceutical dosage forms compression

As a therapeutic agent, ch oline is adininistered orally in the form of symps or elixers containing the chloride, citrates or bitartrate, or in the form of compressed tablets or capsules of the dihydrogen citrate. Choline is also given in small doses as a nutritional supplement in combination with a variety of other materials. In dry pharmaceutical-dosage forms, the dihydrogen citrate is usually preferred because of its lower tendency to absorb atmospheric moisture. Both salts have been used parenteraHy. [Pg.102]

Shangraw RF. Compressed tablets by direct compression. In Leiberman HA, Lachman L, Schwatz JB, eds. Pharmaceutical Dosage Forms Tablets. New York Marcel Dekker, Inc., 1990 195-246. [Pg.124]

The critical unit operations that should be monitored and/or optimized are the reaction and fermentation steps for the purpose of increasing API yield and reducing the residual impurity profile. Other critical unit operations that are especially important to the end user (pharmaceutical dosage form operations) include precipitation or crystallization, milling, sizing, and purification operations, which may affect the physical properties (particle size and shape, bulk powder flow, blend uniformity, and compressibility) of the API. [Pg.409]

Microcrystalline Cellulose. Microcrystalline cellulose is a purified, partially depolymerized cellulose that occurs as a white, odorless, tasteless, crystalline powder composed of porous particles. It is widely used in pharmaceutical dosage forms, primarily as a filler-binder in oral tablets and capsules with both wet granulation and direct compression processes. Microcrystalline cellulose was marketed first in 1964 by the FMC Corporation under name Avicel PH in four different particle size grades, each with different properties.37 Addition of Avicel into a spray-dried lactose-based formulation overcame compressibility problems. At the same time, the lactose enhanced the flowability of the Avicel products available at that time. The direct compression tableting process became a reality, rather than a concept, partially because of the availability of Avicel. As of 2007, Avicel PH is commercially available in 10 types with different particle size, density, and moisture grades that have different properties and applications (Table 7.6).38 Other brands of microcrystalline cellulose are also available on the pharmaceutical market, including Pharmacel 101 and 102 from DMV International and Emcocel 50 M and 90 M from JRS Pharma. [Pg.175]

FIGURE 2 Mixing and filling lines for pharmaceutical dosage forms. Using this hydropneumatic system, instead of the mechanical system in Figure 1, the liquid moves by the pressure generated in a compressed air tank. [Pg.323]

Bandelin, F.J. Compressed tablets by wet granulation. In Pharmaceutical Dosage Forms Tablets, Lieberman, H.A., Lachman, L., Schwartz, J.B. Eds. Marcel Dekker, Inc. New York, 1989 I, 160-164. [Pg.2236]

Compressed Tablets. This popular type of dosage form offers convenience, stabiUty, accuracy and precision, and good bioavadabihty of active ingredients. After the best formulation has been estabflshed, compressed tablets can be manufactured at high rates of speed on advanced equipment. Tablets can be made to achieve rapid dmg release or to produce delayed, repeat, or prolonged therapeutic action (Controlled release technology, pharmaceutical). ... [Pg.229]

One approach to the study of solubility is to evaluate the time dependence of the solubilization process, such as is conducted in the dissolution testing of dosage forms [70], In this work, the amount of drug substance that becomes dissolved per unit time under standard conditions is followed. Within the accepted model for pharmaceutical dissolution, the rate-limiting step is the transport of solute away from the interfacial layer at the dissolving solid into the bulk solution. To measure the intrinsic dissolution rate of a drug, the compound is normally compressed into a special die to a condition of zero porosity. The system is immersed into the solvent reservoir, and the concentration monitored as a function of time. Use of this procedure yields a dissolution rate parameter that is intrinsic to the compound under study and that is considered an important parameter in the preformulation process. A critical evaluation of the intrinsic dissolution methodology and interpretation is available [71]. [Pg.26]

Lubrication is an important unit operation in manufacturing solid oral dosage forms, particularly when using a direct compression platform. Pharmaceutical lubricants can have a significant impact on product performance (e.g., disintegration and dissolution) as well as manufacturability. Lubrication is one of the most critical aspects of a tablet formulation. A lubricant is intended to reduce the friction between the tablet surface and die wall during and after compaction to enable easy ejection of the tablet. In low-dose dmg product development, three issues are associated with lubricating a direct compression formulation ... [Pg.168]

See other pages where Pharmaceutical dosage forms compression is mentioned: [Pg.549]    [Pg.237]    [Pg.202]    [Pg.1088]    [Pg.1161]    [Pg.1186]    [Pg.165]    [Pg.1653]    [Pg.2235]    [Pg.3682]    [Pg.310]    [Pg.179]    [Pg.552]    [Pg.591]    [Pg.128]    [Pg.61]    [Pg.128]    [Pg.2275]    [Pg.320]    [Pg.1]    [Pg.596]    [Pg.373]    [Pg.479]    [Pg.4]    [Pg.27]    [Pg.450]    [Pg.199]    [Pg.268]    [Pg.371]    [Pg.241]    [Pg.6]    [Pg.12]    [Pg.127]    [Pg.140]    [Pg.151]    [Pg.176]    [Pg.104]    [Pg.89]    [Pg.111]   
See also in sourсe #XX -- [ Pg.3905 ]



SEARCH



Pharmaceutical dosage forms

© 2024 chempedia.info