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      A synergistic approach of adapalene-loaded nanostructured lipid carriers, and vitamin C co-administration for treating acne

      , , , , , ,
      Drug Development and Industrial Pharmacy
      Informa UK Limited

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          Solid lipid nanoparticles (SLN) for controlled drug delivery – a review of the state of the art

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            Penetration enhancers.

            One long-standing approach for improving transdermal drug delivery uses penetration enhancers (also called sorption promoters or accelerants) which penetrate into skin to reversibly decrease the barrier resistance. Numerous compounds have been evaluated for penetration enhancing activity, including sulphoxides (such as dimethylsulphoxide, DMSO), Azones (e.g. laurocapram), pyrrolidones (for example 2-pyrrolidone, 2P), alcohols and alkanols (ethanol, or decanol), glycols (for example propylene glycol, PG, a common excipient in topically applied dosage forms), surfactants (also common in dosage forms) and terpenes. Many potential sites and modes of action have been identified for skin penetration enhancers; the intercellular lipid matrix in which the accelerants may disrupt the packing motif, the intracellular keratin domains or through increasing drug partitioning into the tissue by acting as a solvent for the permeant within the membrane. Further potential mechanisms of action, for example with the enhancers acting on desmosomal connections between corneocytes or altering metabolic activity within the skin, or exerting an influence on the thermodynamic activity/solubility of the drug in its vehicle are also feasible, and are also considered in this review.
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              Nuclear retinoid receptors and the transcription of retinoid-target genes.

              The pleiotropic effects of retinoids are mediated by nuclear retinoid receptors (RARs and RXRs) which are ligand-activated transcription factors. In response to retinoid binding, RAR/RXR heterodimers undergo major conformational changes and orchestrate the transcription of specific gene networks, through binding to specific DNA response elements and recruiting cofactor complexes that act to modify local chromatin structure and/or engage the basal transcription machinery. Then the degradation of RARs and RXRs by the ubiquitin-proteasome controls the magnitude and the duration of the retinoid response. RARs and RXRs also integrate a variety of signaling pathways through phosphorylation events which cooperate with the ligand for the control of retinoid-target genes transcription. These different modes of regulation reveal unexpected levels of complexity in the dynamics of retinoid-dependent transcription.
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                Author and article information

                Journal
                Drug Development and Industrial Pharmacy
                Drug Development and Industrial Pharmacy
                Informa UK Limited
                0363-9045
                1520-5762
                November 07 2015
                November 17 2015
                June 02 2016
                : 42
                : 6
                : 897-905
                Article
                10.3109/03639045.2015.1104343
                26577703
                91f86aea-4549-4066-922c-0d6fadd52ea1
                © 2016
                History

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