Delivery of bioactive peptides and proteins across oral (Buccal) mucosa

Senel, Sevda and Kremer, Mary and Nagy, Katalin and Squier, Christopher (2001) Delivery of bioactive peptides and proteins across oral (Buccal) mucosa. CURRENT PHARMACEUTICAL BIOTECHNOLOGY, 2 (2). pp. 175-186. ISSN 1389-2010

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Official URL: https://doi.org/10.2174/1389201013378734

Abstract

The identification of an increasing array of highly potent, endogenous peptide and protein factors termed cytokines, that can be efficiently synthesized using recombinant DNA technology, offers exciting new approaches for drug therapy. However, the physico-chemical and biological properties of these agents impose limitations in formulation and development of optimum drug delivery systems as well as on the routes of delivery. Oral mucosa, including the lining of the cheek (buccal mucosa), floor of mouth and underside of tongue (sublingual mucosa) and gingival mucosa, has received much attention in the last decade because it offers excellent accessibility, is not easily traumatized and avoids degradation of proteins and peptides that occurs as a result of oral administration, gastrointestinal absorption and first-pass hepatic metabolism. Peptide absorption occurs across oral mucosa by passive diffusion and it is unlikely that there is a carrier-mediated transport mechanism. The principal pathway is probably via the intercellular route where the major permeability barrier is represented by organized array of neutral lipids in the superficial layers of the epithelium. The relative role of aqueous as opposed to the lipid pathway in drug transport is still under investigation; penetration is not necessarily enhanced by simply increasing lipophilicity, for other effects, such as charge and molecular size, also play an important role in absorption of peptide and protein drugs. Depending on the pharmacodynamics of the peptides, various oral mucosal delivery systems can be designed. Delivery of peptide/protein drugs by conventional means such as solutions has some limitations. The possibility of excluding a major part of drug from absorption by involuntary swallowing and the continuous dilution due to salivary flow limits a controlled release. However these limitations can be overcome by adhesive dosage forms such as gels, films, tablets, and patches. They can localize the formulation and improve the contact with the mucosal surface to improve absorption of peptides and proteins. Addition of absorption promoters/permeabilizers in bioadhesive dosage forms will be essential for a successful peptide/protein delivery system.

Item Type:	Article
Uncontrolled Keywords:	Animalia; PROTEINS; PEPTIDES; Humans; Drug Delivery Systems; Cell Membrane Permeability; Animals; tongue; tablet; swallowing; salivation; recombinant DNA technology; protein degradation; physical chemistry; pharmacodynamics; permeability barrier; oral drug administration; nonhuman; mouth mucosa; mouth; molecular size; LIPOPHILICITY; INJURY; human; gingiva; GEL; gastrointestinal absorption; first pass effect; FILM; epithelium; Electricity; Drug therapy; drug penetration; drug formulation; drug development; DRUG DESIGN; drug delivery system; dilution; DIFFUSION; controlled study; controlled release formulation; cheek mucosa; biosynthesis; ARTICLE; aqueous solution; animal model; animal experiment; active transport; ABSORPTION; recombinant alpha interferon; protirelin; protein derivative; peptide derivative; OXYTOCIN; Octreotide; lisinopril; lipid; INTERFERON; INSULIN; granulocyte colony stimulating factor; gonadorelin; glucagon like peptide 1; enalapril; drug vehicle; cytokine; CAPTOPRIL; CALCITONIN; buserelin
Subjects:	R Medicine / orvostudomány > RK Dentistry / fogászat
SWORD Depositor:	MTMT SWORD
Depositing User:	MTMT SWORD
Date Deposited:	09 Oct 2017 12:37
Last Modified:	09 Oct 2017 12:37
URI:	http://real.mtak.hu/id/eprint/65189

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