4.7 Article

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

Journal

MOLECULAR PHARMACEUTICS
Volume 16, Issue 6, Pages 2418-2429

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.molpharmaceut.9b00041

Keywords

mesoporous silica microparticles; gated materials; smart drug delivery materials; colon targeted release; inflammatory bowel disease

Funding

  1. Generalitat Valenciana [PROMETE02018/024]
  2. Spanish Government (MINECO/FEDER) [AGL2015-70235-C2-2-R, MAT2015-64139-C4-1-R]
  3. Spanish MEC
  4. Electron Microscopy Service at the UPV

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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.

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