Production of α1,3-Galactosyltransferase-Deficient Pigs

Carol J. Phelps(Kraft Heinz (United States)), Chihiro Koike, Todd Vaught(Kraft Heinz (United States)), Jeremy Boone(Kraft Heinz (United States)), Kevin D. Wells(Kraft Heinz (United States)), Shu-Hung Chen(Kraft Heinz (United States)), Suyapa Ball(Kraft Heinz (United States)), Susan Specht, Irina A. Polejaeva(Kraft Heinz (United States)), Jeff A. Monahan(Kraft Heinz (United States)), Pete M. Jobst(Kraft Heinz (United States)), Sugandha B. Sharma, Ashley E. Lamborn(Kraft Heinz (United States)), Amy S. Garst(Kraft Heinz (United States)), Marilyn Moore(Roslin Institute), Anthony J. Demetris, William A. Rudert(Children's Hospital of Pittsburgh), Rita Bottino(Children's Hospital of Pittsburgh), Suzanne Bertera(Children's Hospital of Pittsburgh), Massimo Trucco(Children's Hospital of Pittsburgh), Thomas E. Starzl, Yifan Dai(Kraft Heinz (United States)), David Ayares(Kraft Heinz (United States))
Science
January 16, 2003
Cited by 1,106

Abstract

The enzyme alpha1,3-galactosyltransferase (alpha1,3GT or GGTA1) synthesizes alpha1,3-galactose (alpha1,3Gal) epitopes (Galalpha1,3Galbeta1,4GlcNAc-R), which are the major xenoantigens causing hyperacute rejection in pig-to-human xenotransplantation. Complete removal of alpha1,3Gal from pig organs is the critical step toward the success of xenotransplantation. We reported earlier the targeted disruption of one allele of the alpha1,3GT gene in cloned pigs. A selection procedure based on a bacterial toxin was used to select for cells in which the second allele of the gene was knocked out. Sequencing analysis demonstrated that knockout of the second allele of the alpha1,3GT gene was caused by a T-to-G single point mutation at the second base of exon 9, which resulted in inactivation of the alpha1,3GT protein. Four healthy alpha1,3GT double-knockout female piglets were produced by three consecutive rounds of cloning. The piglets carrying a point mutation in the alpha1,3GT gene hold significant value, as they would allow production of alpha1,3Gal-deficient pigs free of antibiotic-resistance genes and thus have the potential to make a safer product for human use.


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