Intestinal permeability determinants of norfloxacin in Ussing chamber model

Cassiana Mendes; Gabriela C Meirelles; Marcos A S Silva; Gilles Ponchel

doi:10.1016/j.ejps.2018.05.030

Intestinal permeability determinants of norfloxacin in Ussing chamber model

Eur J Pharm Sci. 2018 Aug 30:121:236-242. doi: 10.1016/j.ejps.2018.05.030. Epub 2018 May 31.

Authors

Cassiana Mendes¹, Gabriela C Meirelles², Marcos A S Silva³, Gilles Ponchel²

Affiliations

¹ CNRS UMR 8612, Université de Paris Sud XI, Faculté de Pharmacie, 5 rue J.B. Clément, 92296 Châtenay-Malabry, France; Post graduation Program in Pharmaceutical Sciences, Quality Control Laboratory, Universidade Federal de Santa Catarina, J/K 207, 88040-900 Florianópolis, SC, Brazil. Electronic address: cassi_ana@yahoo.com.br.
² CNRS UMR 8612, Université de Paris Sud XI, Faculté de Pharmacie, 5 rue J.B. Clément, 92296 Châtenay-Malabry, France.
³ Post graduation Program in Pharmaceutical Sciences, Quality Control Laboratory, Universidade Federal de Santa Catarina, J/K 207, 88040-900 Florianópolis, SC, Brazil.

PMID: 29860116
DOI: 10.1016/j.ejps.2018.05.030

Abstract

Recently, many efforts are taken to identify the intestinal uptake and efflux transporters since they are responsible for the absorption of many drugs as their interactions. Norfloxacin (NFX) is a fluoroquinolone that presents low solubility and low permeability, and as a consequence, low bioavailability. In this context, the aim of this study is evaluate for the first time the intestinal permeability mechanisms of NFX by Ussing chamber model. The low permeation of NFX at low temperature, where the efflux pumps are not active, reveals that NFX permeation is transporter-dependent. The permeation study at different level of intestine demonstrated that NFX passage is in the decrescent order: ileum > jejunum > duodenum > colon, probably attributed to transporters that are expressed differently along the intestinal tract. NFX intestinal flow was evaluated in the presence of many inhibitors and substrates to identify the uptake and efflux transporters implicate in NFX permeability mechanism. It could be observed that BCRP and MRPs are involved in the NFX efflux and PEPT1, PMAT and OCT in the NFX uptake transport. Furthermore, this work revealed that NFX has itself an affinity for OCTN and OATP, demonstrating that NFX could inhibit these transporters and influence the absorption of other drugs. The updated description of NFX intestinal permeability factors could contribute to the development of rational pharmaceutical formulations that could circumvent the efflux problems and consequently improve NFX biopharmaceutical properties and avoid drug-drug interactions.

Keywords: Budesonide (PubChem CID: 5281004); Cyclosporine (PubChem CID: 5284373); Efflux; Intestinal permeability; Levofloxacin (PubChem CID: 149096); Lisinopril (PubChem CID: 5362119); MK-571 (PubChem CID: 5281888); Norfloxacin; Norfloxacin (PubChem CID: 4539); Novobiocin (PubChem CID: 54675769); Quinidine (PubChem CID: 441074); Rhodamine 123 (PubChem CID: 65217); Transporter; Uptake; Ussing chamber; Verapamil (PubChem CID: 2520).

MeSH terms

Animals
Anti-Bacterial Agents / metabolism*
Biological Transport
Intestinal Absorption*
Intestinal Mucosa / metabolism*
Male
Membrane Transport Proteins / metabolism*
Norfloxacin / metabolism*
Rats, Wistar

Substances

Anti-Bacterial Agents
Membrane Transport Proteins
Norfloxacin