UNIGE document Scientific Article
previous document  unige:20175  next document
add to browser collection
Title

HLA-E/human beta2-microglobulin transgenic pigs: protection against xenogeneic human anti-pig natural killer cell cytotoxicity

Authors
Weiss, Elisabeth H.
Lilienfeld, Benjamin G.
Muller, Sigrid
Muller, Elfriede
Herbach, Nadja
Kessler, Barbara
Wanke, Rudiger
Schwinzer, Reinhard
show hidden authors show all authors [1 - 11]
Published in Transplantation. 2009, vol. 87, no. 1, p. 35-43
Abstract BACKGROUND: Natural killer (NK) cells participate in pig-to-primate xenograft rejection both by antibody-dependent and -independent mechanisms. A majority of human NK cells express the inhibitory receptor CD94/NKG2A, which binds specifically to human leukocyte antigen (HLA)-E, a trimeric complex consisting of the HLA-E heavy chain, beta2-microglobulin (beta2m), and a peptide derived from the leader sequence of some major histocompatibility complex class I molecules. METHODS: To use this mechanism for protection of pig tissues against human NK cell-mediated cytotoxicity, we generated transgenic pigs by pronuclear microinjection of genomic fragments of HLA-E with an HLA-B7 signal sequence and of human beta2-microglobulin (hubeta2m) into zygotes. RESULTS: Three transgenic founder pigs were generated. Northern blot analysis of RNA from peripheral blood mononuclear cells revealed the presence of the expected transcript sizes for both transgenes in two of the three founders. The founder with the highest expression and his offspring were characterized in detail. Fluorescence-activated cell sorting (FACS) and Western blot analyses demonstrated consistent expression of HLA-E and hubeta2m in peripheral blood mononuclear cells. Immunohistochemistry revealed the presence of HLA-E and hubeta2m on endothelial cells of many organs, including heart and kidney. In vitro studies showed that lymphoblasts and endothelial cells derived from HLA-E/hubeta2m transgenic pigs are effectively protected against human NK cell-mediated cytotoxicity, depending on the level of CD94/NKG2A expression on the NK cells. Further, HLA-E/hubeta2m expression on porcine endothelial cells inhibited the secretion of interferon (IFN)-gamma by co-cultured human NK cells. CONCLUSIONS: This novel approach against cell-mediated xenogeneic responses has important implications for the generation of multitransgenic pigs as organ donors for clinical xenotransplantation.
Keywords AnimalsAnimals, Genetically ModifiedCell Movement/immunologyCells, CulturedCytotoxicity, Immunologic/*immunologyEndothelial Cells/immunology/metabolismHLA Antigens/*immunologyHistocompatibility Antigens Class I/*immunologyHumansKiller Cells, Natural/cytology/*immunologyOrgan SpecificitySwine/*immunologyTransplantation, Heterologous/*immunologyBeta 2-Microglobulin/genetics/*immunology/metabolism
Identifiers
PMID: 19136889
Full text
Article - document accessible for UNIGE members only Limited access to UNIGE
Structures
Research group Groupe Seebach Jorg Dieter (transplantation et immunologie) (856)
Citation
(ISO format)
WEISS, Elisabeth H. et al. HLA-E/human beta2-microglobulin transgenic pigs: protection against xenogeneic human anti-pig natural killer cell cytotoxicity. In: Transplantation, 2009, vol. 87, n° 1, p. 35-43. https://archive-ouverte.unige.ch/unige:20175

217 hits

1 download

Update

Deposited on : 2012-04-23

Export document
Format :
Citation style :