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Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73

One of the reasons to causing blood coagulation in the tissue of xenografted organs was known to incompatibility of the blood coagulation and anti-coagulation regulatory system between TG pigs and primates. Thus, overexpression of human CD73 (hCD73) in the pig endothelial cells is considered as a me...

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Autores principales: Lee, Seung-Chan, Lee, Haesun, Oh, Keon Bong, Hwang, In-Sul, Yang, Hyeon, Park, Mi-Ryung, Ock, Sun-A, Woo, Jae-Seok, Im, Gi-Sun, Hwang, Seongsoo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Korean Society of Developmental Biology 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5532308/
https://www.ncbi.nlm.nih.gov/pubmed/28785737
http://dx.doi.org/10.12717/DR.2017.21.2.157
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author Lee, Seung-Chan
Lee, Haesun
Oh, Keon Bong
Hwang, In-Sul
Yang, Hyeon
Park, Mi-Ryung
Ock, Sun-A
Woo, Jae-Seok
Im, Gi-Sun
Hwang, Seongsoo
author_facet Lee, Seung-Chan
Lee, Haesun
Oh, Keon Bong
Hwang, In-Sul
Yang, Hyeon
Park, Mi-Ryung
Ock, Sun-A
Woo, Jae-Seok
Im, Gi-Sun
Hwang, Seongsoo
author_sort Lee, Seung-Chan
collection PubMed
description One of the reasons to causing blood coagulation in the tissue of xenografted organs was known to incompatibility of the blood coagulation and anti-coagulation regulatory system between TG pigs and primates. Thus, overexpression of human CD73 (hCD73) in the pig endothelial cells is considered as a method to reduce coagulopathy after pig-to-non-human-primate xenotransplantation. This study was performed to produce and breed transgenic pigs expressing hCD73 for the studies immune rejection responses and could provide a successful application of xenotransplantation. The transgenic cells were constructed an hCD73 expression vector under control porcine Icam2 promoter (pIcam2-hCD73) and established donor cell lines expressing hCD73. The numbers of transferred reconstructed embryos were 127 ± 18.9. The pregnancy and delivery rate of surrogates were 8/18 (44%) and 3/18 (16%). The total number of delivered cloned pigs were 10 (2 alive, 7 mummy, and 1 died after birth). Among them, three live hCD73-pigs were successfully delivered by Caesarean section, but one was dead after birth. The two hCD73 TG cloned pigs had normal reproductive ability. They mated with wild type (WT) MGH (Massachusetts General Hospital) female sows and produced totally 16 piglets. Among them, 5 piglets were identified as hCD73 TG pigs. In conclusion, we successfully generated the hCD73 transgenic cloned pigs and produced their litters by natural mating. It can be possible to use a mate for the production of multiple transgenic pigs such as α-1,3-galactosyltransferase knock-out /hCD46 for xenotransplantation.
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spelling pubmed-55323082017-08-07 Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73 Lee, Seung-Chan Lee, Haesun Oh, Keon Bong Hwang, In-Sul Yang, Hyeon Park, Mi-Ryung Ock, Sun-A Woo, Jae-Seok Im, Gi-Sun Hwang, Seongsoo Dev Reprod Original Research Paper One of the reasons to causing blood coagulation in the tissue of xenografted organs was known to incompatibility of the blood coagulation and anti-coagulation regulatory system between TG pigs and primates. Thus, overexpression of human CD73 (hCD73) in the pig endothelial cells is considered as a method to reduce coagulopathy after pig-to-non-human-primate xenotransplantation. This study was performed to produce and breed transgenic pigs expressing hCD73 for the studies immune rejection responses and could provide a successful application of xenotransplantation. The transgenic cells were constructed an hCD73 expression vector under control porcine Icam2 promoter (pIcam2-hCD73) and established donor cell lines expressing hCD73. The numbers of transferred reconstructed embryos were 127 ± 18.9. The pregnancy and delivery rate of surrogates were 8/18 (44%) and 3/18 (16%). The total number of delivered cloned pigs were 10 (2 alive, 7 mummy, and 1 died after birth). Among them, three live hCD73-pigs were successfully delivered by Caesarean section, but one was dead after birth. The two hCD73 TG cloned pigs had normal reproductive ability. They mated with wild type (WT) MGH (Massachusetts General Hospital) female sows and produced totally 16 piglets. Among them, 5 piglets were identified as hCD73 TG pigs. In conclusion, we successfully generated the hCD73 transgenic cloned pigs and produced their litters by natural mating. It can be possible to use a mate for the production of multiple transgenic pigs such as α-1,3-galactosyltransferase knock-out /hCD46 for xenotransplantation. The Korean Society of Developmental Biology 2017-06 2017-06-30 /pmc/articles/PMC5532308/ /pubmed/28785737 http://dx.doi.org/10.12717/DR.2017.21.2.157 Text en ⓒ Copyright an Official Journal of the Korean Society of Developmental Biology. All Rights Reserved http://creativecommons.org/licenses/by-nc/3.0/ This is an Open-Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research Paper
Lee, Seung-Chan
Lee, Haesun
Oh, Keon Bong
Hwang, In-Sul
Yang, Hyeon
Park, Mi-Ryung
Ock, Sun-A
Woo, Jae-Seok
Im, Gi-Sun
Hwang, Seongsoo
Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73
title Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73
title_full Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73
title_fullStr Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73
title_full_unstemmed Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73
title_short Production and Breeding of Transgenic Cloned Pigs Expressing Human CD73
title_sort production and breeding of transgenic cloned pigs expressing human cd73
topic Original Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5532308/
https://www.ncbi.nlm.nih.gov/pubmed/28785737
http://dx.doi.org/10.12717/DR.2017.21.2.157
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