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Differential immune responses to α-gal epitopes on xenografts and allografts: implications for accommodation in xenotransplantation
Masahiro Tanemura, Dengping Yin, Anita S. Chong, Uri Galili
Masahiro Tanemura, Dengping Yin, Anita S. Chong, Uri Galili
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Article

Differential immune responses to α-gal epitopes on xenografts and allografts: implications for accommodation in xenotransplantation

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Abstract

Xenograft recipients produce large amounts of high-affinity anti-Gal IgG in response to Galα1-3Galβ1- 4GlcNAc-R (α-gal) epitopes on the graft. In contrast, ABO-mismatched allograft recipients undergo “accommodation,” a state of very weak immune response to ABO antigens. These differences in anti-carbohydrate immune response were studied in α1,3galactosyltransferase knock-out mice. Pig kidney membranes administered to these mice elicited extensive production of anti-Gal IgG, whereas allogeneic kidney membranes expressing α-gal epitopes elicited only a weak anti-Gal IgM response. Anti-Gal IgG response to xenograft membranes depended on helper T cell activation and was inhibited by anti-CD40L antibody. These T cells were activated by xenopeptides and not by α-gal epitopes. Moreover, allogeneic cell membranes manipulated to express xenoproteins also induced anti-Gal IgG response. Xenoglycoproteins with α-gal epitopes are processed by anti-Gal B cells. Xenopeptides presented by these cells activate a large repertoire of helper T cells required for the differentiation of anti-Gal B cells into cells secreting anti-Gal IgG. Alloglycoproteins with α- gal epitopes have very few immunogenic peptides and fail to activate helper T cells. Similarly, ineffective helper T-cell activation prevents a strong immune response to blood group antigens in ABO-mismatched allograft recipients, thus enabling the development of accommodation.

Authors

Masahiro Tanemura, Dengping Yin, Anita S. Chong, Uri Galili

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Figure 3

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Allogeneic response of α1,3GT KO mice to C3H mice. (a) Stimulation of ly...
Allogeneic response of α1,3GT KO mice to C3H mice. (a) Stimulation of lymphocytes from 5 α1,3GT KO mice in a MLR with irradiated C3H mouse lymphocytes as stimulatory cells (closed columns) or in the absence of stimulatory cells (open columns). (b) Production of alloantibodies in α1,3GT KO mice immunized with C3H kidney membranes; FACS analysis of C3H spleen lymphocytes incubated with sera from nonimmunized α1,3GT KO mice (broken line), or sera from immunized mice (solid line). The left peak in each histogram represents T cells, whereas the right peak represents B cells. Data are from 1 of 5 mice with similar results.

Copyright © 2026 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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