PLoS ONE (Jan 2014)

Survival of skin graft between transgenic cloned dogs and non-transgenic cloned dogs.

  • Geon A Kim,
  • Hyun Ju Oh,
  • Min Jung Kim,
  • Young Kwang Jo,
  • Jin Choi,
  • Jung Eun Park,
  • Eun Jung Park,
  • Sang Hyun Lim,
  • Byung Il Yoon,
  • Sung Keun Kang,
  • Goo Jang,
  • Byeong Chun Lee

DOI
https://doi.org/10.1371/journal.pone.0108330
Journal volume & issue
Vol. 9, no. 11
p. e108330

Abstract

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Whereas it has been assumed that genetically modified tissues or cells derived from somatic cell nuclear transfer (SCNT) should be accepted by a host of the same species, their immune compatibility has not been extensively explored. To identify acceptance of SCNT-derived cells or tissues, skin grafts were performed between cloned dogs that were identical except for their mitochondrial DNA (mtDNA) haplotypes and foreign gene. We showed here that differences in mtDNA haplotypes and genetic modification did not elicit immune responses in these dogs: 1) skin tissues from genetically-modified cloned dogs were successfully transplanted into genetically-modified cloned dogs with different mtDNA haplotype under three successive grafts over 63 days; and 2) non-transgenic cloned tissues were accepted into transgenic cloned syngeneic recipients with different mtDNA haplotypes and vice versa under two successive grafts over 63 days. In addition, expression of the inserted gene was maintained, being functional without eliciting graft rejection. In conclusion, these results show that transplanting genetically-modified tissues into normal, syngeneic or genetically-modified recipient dogs with different mtDNA haplotypes do not elicit skin graft rejection or affect expression of the inserted gene. Therefore, therapeutically valuable tissue derived from SCNT with genetic modification might be used safely in clinical applications for patients with diseased tissues.