Mohamad Haitham Ayad scite author profile

Mohamad Haitham Ayad

3Publications

17Citation Statements Received

11Citation Statements Given

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Affiliations

Johnson & Johnson (Israel), Addex Therapeutics (Switzerland), Johnson & Johnson (United States)

Publications

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Amorphous solid dispersion successfully improved oral exposure of ADX71943 in support of toxicology studies

Ayad

Bonnet

Quinton³

et al. 2012

Drug Development and Industrial Pharmacy

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ADX71943 is a potent and selective GABA(b) receptor positive allosteric modulator (PAM) which exhibits poor aqueous solubility at all physiologically relevant pHs. The aim of this study was to identify an adequate formulation to improve the solubility of ADX71943 to achieve a sufficiently high plasma exposure after oral administration to support the toxicology program. Considering the overall physicochemical properties and the low solubility of ADX71943 in a variety of solvents, solid dispersion, and particle size reduction have been successfully chosen as potential strategies to improve its oral bioavailability. Both technologies have proven useful in improving the in vitro dissolution profile and as a result of the solubility enhancement, higher bioavailability was obtained in vivo. As the solid dispersion gave better bioavailability (30-fold compared with the neat active pharmaceutical ingredient (API)), this formulation was selected for the toxicology study. Changing the crystalline form of ADX71943 into amorphous state by preparing a solid dispersion has greatly improved its oral bioavailability and has allowed achieving the required plasma concentration needed in toxicology studies.

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Rational formulation strategy from drug discovery profiling to human proof of concept

Ayad

2014

Drug Delivery

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The objective of this paper is to introduce some strategic guidance to a rational formulation strategy of new molecules as oral dosage forms, based on a sound scientific understanding of factors determining the oral bioavailability. The critical implication of permeability and solubility is discussed along with the efficient dose of the drug. The concept of dose-solubility number is introduced as a tool for chemists to assess the develop-ability of different molecules very early during discovery stage. Based on this understanding, a rational formulation strategy for preclinical and early clinical phases is provided. The technical considerations and limitations of different formulation technologies are discussed and illustrated via concrete examples. This approach has the advantage of streamlining the formulation process in order to avoid delaying the development of new drugs due to formulation related issues.

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Sample Size for Tablet Compression and Capsule Filling Events During Process Validation

Charoo¹,

Durivage

Rahman

et al. 2017

Journal of Pharmaceutical Sciences

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