Lipid-based oral delivery systems for skin deposition of a potential chemopreventive DIM derivative: characterization and evaluation. Academic Article

abstract

• The objective of this study was to explore the oral route as a viable potential for the skin deposition of a novel diindolylmethane derivative (DIM-D) for chemoprevention activity. Various lipid-based oral delivery systems were optimized and compared for enhancing DIM-D's oral bioavailability and skin deposition. Preformulation studies were performed to evaluate the log P and solubility of DIM-D. Microsomal metabolism, P-glycoprotein efflux, and caco-2 monolayer permeability of DIM-D were determined. Comparative evaluation of the oral absorption and skin deposition of DIM-D-loaded various lipid-based formulations was performed in rats. DIM-D showed pH-dependent solubility and a high log P value. It was not a strong substrate of microsomal degradation and P-glycoprotein. SMEDDs comprised of medium chain triglycerides, monoglycerides, and kolliphor-HS15 (36.700.42nm). SNEDDs comprised of long chain triglycerides, cremophor RH40, labrasol, and TPGS (84.0014.14nm). Nanostructured lipid carriers (NLC) consisted of compritol, miglyol, and surfactants (116.502.12nm). The blank formulations all showed >70% cell viability in caco-2 cells. Differential Scanning Calorimetry confirmed the amorphization of DIM-D within the lipid matrices while Atomic Force Microscopy showed particle size distribution similar to the dynamic light scattering data. DIM-D also showed reduced permeation across caco-2 monolayer that was enhanced (p<0.05) by SNEDDs in comparison to SMEDDs and NLC. Fabsolute for DIM-D SNEDDs, SMEDDs, and NLC was 0.14, 0.04, and 0.007, respectively. SNEDDs caused 53.90, 11.32, and 15.08-fold more skin deposition of DIM-D than the free drug, SMEDDs, and NLC, respectively, at 2h following oral administration and shows a viable potential for use in skin cancer chemoprevention. Graphical Abstract .

authors

• Safe, Stephen

published proceedings

• Drug Deliv Transl Res

author list (cited authors)

• Boakye, C., Patel, K., Patel, A. R., Faria, H., Zucolotto, V., Safe, S., & Singh, M.

citation count

• 5

complete list of authors

• Boakye, Cedar HA||Patel, Ketan||Patel, Apurva R||Faria, Henrique AM||Zucolotto, Valtencir||Safe, Stephen||Singh, Mandip

publication date

• October 2016

publisher

• Springer Nature  Publisher

published in

• Drug Delivery and Translational Research  Journal

keywords

• Administration, Oral
• Animals
• Atp Binding Cassette Transporter, Subfamily B, Member 1
• Biological Availability
• Caco-2 Cells
• Cell Survival
• Chemistry, Pharmaceutical
• Diindolylmethane (dim)
• Drug Delivery Systems
• Drug Stability
• Emulsions
• First Pass Metabolism
• Humans
• Indoles
• Lipid-based Drug Delivery Systems
• Lipids
• Male
• Microsomes
• Oral Delivery
• P-glycoprotein Efflux Pump
• Particle Size
• Rats
• Skin
• Skin Delivery
• Solubility

PubMed Central ID

• 27405772

Digital Object Identifier (DOI)

• 10.1007/s13346-016-0302-2

start page

• 526

end page

• 539

volume

• 6

issue

• 5

URL

• http%3A%2F%2Fdx.doi.org%2F10.1007%2Fs13346-016-0302-2