Safety and efficacy of sodium caprate in promoting oral drug absorption: from in vitro to the clinic
A major challenge in oral drug delivery is the development of novel dosage forms to promote absorption of poorly permeable drugs across the intestinal epithelium. To date, no absorption promoter has been approved in a formulation specifically designed for oral delivery of Class III molecules. Promot...
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Veröffentlicht in: | Advanced drug delivery reviews 2009-12, Vol.61 (15), p.1427-1449 |
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Sprache: | eng |
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Zusammenfassung: | A major challenge in oral drug delivery is the development of novel dosage forms to promote absorption of poorly permeable drugs across the intestinal epithelium. To date, no absorption promoter has been approved in a formulation specifically designed for oral delivery of Class III molecules. Promoters that are designated safe for human consumption have been licensed for use in a recently approved buccal insulin spray delivery system and also for many years as part of an ampicillin rectal suppository. Unlike buccal and rectal delivery, oral formulations containing absorption promoters have the additional technical hurdle whereby the promoter and payload must be co-released in high concentrations at the small intestinal epithelium in order to generate significant but rapidly reversible increases in permeability. An advanced promoter in the clinic is the medium chain fatty acid (MCFA), sodium caprate (C
10), a compound already approved as a food additive. We discuss how it has evolved to a matrix tablet format suitable for administration to humans under the headings of mechanism of action at the cellular and tissue level as well as
in vitro and
in vivo efficacy and safety studies. In specific clinical examples, we review how C
10-based formulations are being tested for oral delivery of bisphosphonates using
Gastro
Intestinal
Permeation
Enhancement
Technology, GIPET® (Merrion Pharmaceuticals, Ireland) and in a related solid dose format for antisense oligonucleotides (ISIS Pharmaceuticals, USA). |
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ISSN: | 0169-409X 1872-8294 |
DOI: | 10.1016/j.addr.2009.09.006 |