Literature DB >> 23094761

Interaction of celecoxib with membranes: the role of membrane biophysics on its therapeutic and toxic effects.

Catarina Pereira-Leite1, Cláudia Nunes, José L F C Lima, Salette Reis, Marlene Lúcio.   

Abstract

The present work provides a biophysical characterization of the interaction of celecoxib, a cyclo-oxigenase-2 selective nonsteroidal anti-inflammatory drug, with membranes using liposomes, constituted by phosphatidylcholines, as membrane model systems. In order to mimic biological conditions, the experiments were performed at physiological pH (7.4); at an acidic pH to mimic the conditions of the inflamed cells (5.0); and at different membrane physical states (gel, ripple, and fluid phase). Important information regarding the celecoxib-membrane interactions was gathered by the complementary biophysical techniques: derivative spectrophotometry was used to determine liposome/water partition coefficient of celecoxib; dynamic light scattering (DLS) measurements were performed to study the influence of celecoxib on lipid main phase transition temperature; fluorescence binding measurements were made to assess the location of celecoxib within the membrane; and small-angle and wide-angle X-ray scattering (SAXS and WAXS) were used to assess the changes in the structure and order of phosphatidylcholine bilayers caused by the presence of celecoxib. The overall results obtained indicate that celecoxib greatly interacts with membranes. Briefly, celecoxib exhibits a high liposome/water partition coefficient that is non-pH-dependent, but the location of celecoxib within the membrane is pH-dependent. In fact, celecoxib is more deeply located inside the membrane at pH 5.0, while it locates closer to the surface at pH 7.4. DLS, SAXS, and WAXS results have shown a high membrane fluidization in the presence of celecoxib, especially at pH 7.4. Overall, the current study can contribute to a biophysical characterization of the celecoxib-membrane interaction. The relevance of the gathered results will be discussed in terms of the reported celecoxib therapeutic and toxic effects.

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Year:  2012        PMID: 23094761     DOI: 10.1021/jp304037v

Source DB:  PubMed          Journal:  J Phys Chem B        ISSN: 1520-5207            Impact factor:   2.991


  7 in total

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Journal:  Sci Rep       Date:  2017-07-24       Impact factor: 4.379

5.  A Molecular Biophysical Approach to Diclofenac Topical Gastrointestinal Damage.

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6.  Rational Development of Liposomal Hydrogels: A Strategy for Topical Vaginal Antiretroviral Drug Delivery in the Context of HIV Prevention.

Authors:  Maria J Faria; Raul Machado; Artur Ribeiro; Hugo Gonçalves; Maria Elisabete C D Real Oliveira; Teresa Viseu; José das Neves; Marlene Lúcio
Journal:  Pharmaceutics       Date:  2019-09-18       Impact factor: 6.321

7.  Antituberculosis Drug Interactions with Membranes: A Biophysical Approach Applied to Bedaquiline.

Authors:  Marina Pinheiro; Heinz Amenitsch; Salette Reis
Journal:  Membranes (Basel)       Date:  2019-10-30
  7 in total

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