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      Ex Vivo Adenoviral Vector Gene Delivery Results in Decreased Vector-associated Inflammation Pre- and Post–lung Transplantation in the Pig

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          Abstract

          Acellular normothermic ex vivo lung perfusion (EVLP) is a novel method of donor lung preservation for transplantation. As cellular metabolism is preserved during perfusion, it represents a potential platform for effective gene transduction in donor lungs. We hypothesized that vector-associated inflammation would be reduced during ex vivo delivery due to isolation from the host immune system response. We compared ex vivo with in vivo intratracheal delivery of an E1-, E3-deleted adenoviral vector encoding either green fluorescent protein (GFP) or interleukin-10 (IL-10) to porcine lungs. Twelve hours after delivery, the lung was transplanted and the post-transplant function assessed. We identified significant transgene expression by 12 hours in both in vivo and ex vivo delivered groups. Lung function remained excellent in all ex vivo groups after viral vector delivery; however, as expected, lung function decreased in the in vivo delivered adenovirus vector encoding GFP (AdGFP) group with corresponding increases in IL-1β levels. Transplanted lung function was excellent in the ex vivo transduced lungs and inferior lung function was seen in the in vivo group after transplantation. In summary, ex vivo delivery of adenoviral gene therapy to the donor lung is superior to in vivo delivery in that it leads to less vector-associated inflammation and provides superior post-transplant lung function.

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          Author and article information

          Journal
          Mol Ther
          Mol. Ther
          Molecular Therapy
          Nature Publishing Group
          1525-0016
          1525-0024
          June 2012
          27 March 2012
          : 20
          : 6
          : 1204-1211
          Affiliations
          [1 ] Latner Thoracic Surgery Research Laboratories, Toronto General Research Institute, University of Toronto , Toronto, Ontario, Canada
          [2 ] Department of Physiology and Experimental Medicine, Hospital for Sick Children , Toronto, Ontario, Canada
          Author notes
          [* ]Toronto Lung Transplant Program, Toronto General Hospital, 200 Elizabeth Street, 9N946 Toronto, Ontario, Canada M5G 2C4. E-mail: shaf.keshavjee@ 123456uhn.on.ca
          Article
          PMC3369301 PMC3369301 3369301 mt201257
          10.1038/mt.2012.57
          3369301
          22453765
          9e454978-611e-4b95-bd8d-dcaf8416120b
          Copyright © 2012 The American Society of Gene & Cell Therapy
          History
          : 18 September 2011
          : 23 February 2012
          Categories
          Original Article

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