Double Drug Delivery Using Capped Mesoporous Silica Microparticles for the Effective Treatment of Inflammatory Bowel Disease

6533b820fe1ef96bd127a5ca

RESEARCH PRODUCT

Double Drug Delivery Using Capped Mesoporous Silica Microparticles for the Effective Treatment of Inflammatory Bowel Disease

Félix Sancenón Virginia Merino Virginia Merino Marta González-álvarez Pablo Gaviña Pablo Gaviña Daniel Ferri Daniel Ferri Isabel González-álvarez Ramón Martínez-máñez Ana M. Costero Ana M. Costero ÉDgar Pérez-esteve Adrián H. Teruel

subject

Male Hydrocortisone TECNOLOGIA DE ALIMENTOS Reducing agent Pharmaceutical Science 02 engineering and technology Mesoporous silica microparticles 030226 pharmacology & pharmacy Inflammatory bowel disease Sodium dithionite 03 medical and health sciences chemistry.chemical_compound Hydrolysis Drug Delivery Systems 0302 clinical medicine QUIMICA ORGANICA In vivo Drug Discovery QUIMICA ANALITICA medicine Rhodamine B Animals Gated materials Rats Wistar Mesalamine Olsalazine Rhodamines Colon targeted release QUIMICA INORGANICA Mesoporous silica Colitis Inflammatory Bowel Diseases Silicon Dioxide 021001 nanoscience & nanotechnology Smart drug delivery materials Rats chemistry Drug delivery Molecular Medicine 0210 nano-technology medicine.drug Nuclear chemistry

description

[EN] Silica mesoporous microparticles loaded with both rhodamine B fluorophore (S1) or hydrocortisone (S2), and capped with an olsalazine derivative, are prepared and fully characterized. Suspensions of Si and S2 in water at an acidic and a neutral pH show negligible dye/drug release, yet a notable delivery took place when the reducing agent sodium dithionite is added because of hydrolysis of an azo bond in the capping ensemble. Additionally, olsalazine fragmentation induced 5-aminosalicylic acid (5-ASA) release. In vitro digestion models show that S1 and S2 solids are suitable systems to specifically release a pharmaceutical agent in the colon. In vivo pharmacokinetic studies in rats show a preferential rhodamine B release from Si in the colon. Moreover, a model of ulcerative colitis is induced in rats by oral administration of 2,4,6-trinitrobenzenesulfonic acid (TNBS) solutions, which was also used to prove the efficacy of S2 for colitis treatment. The specific delivery of hydrocortisone and 5-ASA from S2 material to the colon tissue in injured rats markedly lowers the colon/body weight ratio and the clinical activity score. Histological studies showed a remarkable reduction in inflammation, as well as an intensive regeneration of the affected tissues.

year	journal	country	edition	language
2019-01-01

10.13039/501100003359 https://dx.doi.org/10.1021/acs.molpharmaceut.9b00041