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      The production of multi-transgenic pigs: update and perspectives for xenotransplantation.

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          Abstract

          The domestic pig shares many genetic, anatomical and physiological similarities to humans and is thus considered to be a suitable organ donor for xenotransplantation. However, prior to clinical application of porcine xenografts, three major hurdles have to be overcome: (1) various immunological rejection responses, (2) physiological incompatibilities between the porcine organ and the human recipient and (3) the risk of transmitting zoonotic pathogens from pig to humans. With the introduction of genetically engineered pigs expressing high levels of human complement regulatory proteins or lacking expression of α-Gal epitopes, the HAR can be consistently overcome. However, none of the transgenic porcine organs available to date was fully protected against the binding of anti-non-Gal xenoreactive natural antibodies. The present view is that long-term survival of xenografts after transplantation into primates requires additional modifications of the porcine genome and a specifically tailored immunosuppression regimen compliant with current clinical standards. This requires the production and characterization of multi-transgenic pigs to control HAR, AVR and DXR. The recent emergence of new sophisticated molecular tools such as Zinc-Finger nucleases, Transcription-activator like endonucleases, and the CRISPR/Cas9 system has significantly increased efficiency and precision of the production of genetically modified pigs for xenotransplantation. Several candidate genes, incl. hTM, hHO-1, hA20, CTLA4Ig, have been explored in their ability to improve long-term survival of porcine xenografts after transplantation into non-human primates. This review provides an update on the current status in the production of multi-transgenic pigs for xenotransplantation which could bring porcine xenografts closer to clinical application.

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          Author and article information

          Journal
          Transgenic Res.
          Transgenic research
          Springer Nature
          1573-9368
          0962-8819
          Jun 2016
          : 25
          : 3
          Affiliations
          [1 ] Institute of Farm Animal Genetics, Friedrich-Loeffler-Institut, Hoeltystrasse 10, Mariensee, 31535, Neustadt, Germany. heiner.niemann@fli.bund.de.
          [2 ] REBIRTH, Cluster of Excellence, Hannover Medical School, Hannover, Germany. heiner.niemann@fli.bund.de.
          [3 ] Institute of Farm Animal Genetics, Friedrich-Loeffler-Institut, Hoeltystrasse 10, Mariensee, 31535, Neustadt, Germany. bjoern.petersen@fli.bund.de.
          [4 ] REBIRTH, Cluster of Excellence, Hannover Medical School, Hannover, Germany. bjoern.petersen@fli.bund.de.
          Article
          10.1007/s11248-016-9934-8
          10.1007/s11248-016-9934-8
          26820415
          cf8138b4-314c-4207-85bd-7d2ca9a0030e
          History

          Long term survival of porcine xenografts,Somatic cell nuclear transfer,Human organ shortage,Hemeoxygenase-1 gene,DNA nucleases,Anti-coagulant strategy

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