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Poster / Nov 12, 2017

Optimizing Disintegration in Tablets of Amorphous Solid Dispersions

Authors:

Nuno Neves
João Henriques
Marcio Temtem

Source:

AAPS 2017

Good bioavailability of amorphous solid dispersions (ASDs) not only depends on dissolution rate/extent but also on the capability to inhibit/avoid crystallization, ensuring that supersaturated state is retained to promote absorption. Here, the type and amount of carrier polymer used in ADSs preparation have a strong impact on the rate and extent of precipitation.

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Knowledge Center

Optimizing Disintegration in Tablets of Amorphous Solid Dispersions

Related links

Also in the Knowledge Center

Waste minimization - a case study

Vitro characterization of jet-milled and in-situ-micronized fluticasone-17-propionate

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Browser not supported

Knowledge Center

Optimizing Disintegration in Tablets of Amorphous Solid Dispersions

Related links

Also in the Knowledge Center

Waste minimization - a case study

Vitro characterization of jet-milled and in-situ-micronized fluticasone-17-propionate

Structure of [RhH2(PPh3)2(bipy)]Cl (bipy = 2,2'-bipyridyl) from multinuclear NMR studies

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