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      AC and DC electrospinning of hydroxypropylmethylcellulose with polyethylene oxides as secondary polymer for improved drug dissolution.

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          Abstract

          Alternating current electrospinning (ACES) capable to reach multiple times higher specific productivities than widely used direct current electrospinning (DCES) was investigated and compared with DCES to prepare drug-loaded formulations based on one of the most widespread polymeric matrix used for commercialized pharmaceutical solid dispersions, hydroxypropylmethylcellulose 2910 (HPMC). In order to improve the insufficient spinnability of HPMC (both with ACES and DCES) polyethylene oxide (PEO) as secondary polymer with intense ACES activity was introduced into the electrospinning solution. Different grades of this polymer used at as low concentrations in the fibers as 0.1% or less enabled the production of high quality HPMC-based fibrous mats without altering its physicochemical properties remarkably. Increasing concentrations of higher molecular weight PEOs led to the thickening of fibers from submicronic diameters to several microns of thickness. ACES fibers loaded with the poorly water-soluble model drug spironolactone were several times thinner than drug-loaded fibers prepared with DCES in spite of the higher feeding rates applied. The amorphous HPMC-based fibers with large surface area enhanced the dissolution of spironolactone significantly, the presence of small amounts of PEO did not affect the dissolution rate. The presented results confirm the diverse applicability of ACES, a novel technique to prepare fibrous drug delivery systems.

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          Author and article information

          Journal
          Int J Pharm
          International journal of pharmaceutics
          Elsevier BV
          1873-3476
          0378-5173
          May 30 2016
          : 505
          : 1-2
          Affiliations
          [1 ] Budapest University of Technology and Economics, Organic Chemistry and Technology Department, H-1111 Budapest, Hungary. Electronic address: baloghattila5@gmail.com.
          [2 ] Budapest University of Technology and Economics, Organic Chemistry and Technology Department, H-1111 Budapest, Hungary.
          [3 ] Chemical and Pharmaceutical Development, Johnson & Johnson Pharmaceutical Research and Development, Janssen Pharmaceutica, B-2340 Beerse, Belgium.
          [4 ] Budapest University of Technology and Economics, Organic Chemistry and Technology Department, H-1111 Budapest, Hungary. Electronic address: zsknagy@oct.bme.hu.
          Article
          S0378-5173(16)30224-1
          10.1016/j.ijpharm.2016.03.024
          26997426
          6f0c8352-d224-4a7a-9cf6-f96088ba1f28
          History

          Electrospinning,Polyethylene oxide,Dissolution enhancement,Hypromellose,Nanofibers

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