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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

Process for the preparation of purified crystalline iohexol by crystallization using ethanol

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Browser not supported

Knowledge Center

Optimizing Disintegration in Tablets of Amorphous Solid Dispersions

Related links

Also in the Knowledge Center

Process for the preparation of purified crystalline iohexol by crystallization using ethanol

Process for the preparation of crystalline and solvent-free iohexol

Isolation and x-ray crystal structure analysis of a hydrazine-containing rhodium catalyst, [(MeOH)2H]+[RhCl4(PPh3)(NHMeNHMe)]-

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