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1: Role of natural killer cells, macrophages, and accessory molecule interactions in the rejection of pig-to-primate xenografts beyond the hyperacute period. Itescu S, Kwiatkowski P, Artrip JH, Wang SF, Ankersmit J, Minanov OP, Michler RE; Human immunology 1998 May;59(5):275-86. Pubmed Link Pig-to-primate cardiac xenografts surviving
beyond the period of hyperacute rejection succumb after 3-4 days to a
secondary immunologic response characterized by xenograft infiltration
with NK cells and macrophages. Circulating baboon mononuclear cells
contain NK cell precursors which mediate lysis of porcine endothelium by
two distinct mechanisms: antibody-dependent cellular cytotoxicity and
lymphokine activation. IL-2 activated NK lysis of porcine endothelium was
2.4-fold stronger than lysis occurring following engagement of FcRIII by
xenoreactive IgG. IL-2 augmented NK lysis involved interactions between
CD2 and CD49d on baboon NK cells and their respective ligands on porcine
endothelium, since NK lysis was reduced either by using Mabs against CD2,
CD49d, or porcine VCAM, or by treating endothelial cells with PIPLC to
cleave GPI-linked molecules. These results imply that interactions between
accessory molecule receptor-ligand pairs on primate NK cells, macrophages
and porcine endothelium are of critical importance in delayed xenograft
rejection. a PDF of this paper can be provided upon request |
