T cell-activated macrophages are capable of both recognition and rejection of pancreatic islet xenografts

被引:85
作者
Yi, SN
Hawthorne, WJ
Lehnert, AM
Ha, H
Wong, JKW
van Rooijen, N
Davey, K
Patel, AT
Walters, SN
Chandra, A
O'Connell, PJ [1 ]
机构
[1] Univ Sydney, Westmead Hosp, Natl Pancreas Transplant Unit, Westmead, NSW 2145, Australia
[2] Free Univ Amsterdam, Dept Cell Biol, Amsterdam, Netherlands
关键词
D O I
10.4049/jimmunol.170.5.2750
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Macrophages have been proposed as the major effector cell in T cell-mediated xenograft rejection. To determine their role in this response, NOD-SCID mice were transplanted with fetal pig pancreas (FPP) before reconstitution with CD4(+) T cells from BALB/c mice. Twelve days after CD4(+) T cell reconstitution, purified macrophages (depleted of T cells) were isolated from CD4(+) T cell-reconstituted FPP recipient mice and adoptively transferred to their nonreconstituted counterparts. After adoptive macrophage transfer, FPP recipient mice transferred with macrophages from CD4(+) T cell-reconstituted mice demonstrated xenograft destruction along with massive macrophage infiltration at day 4 and complete graft destruction at day 8 postmacrophage transfer. By contrast, FPP recipients that received macrophages from nonreconstituted mice showed intact FPP xenografts with few infiltrating macrophages at both days 4 and 8 after macrophage transfer. The graft-infiltrating macrophages showed increased expression of their activation markers. Depletion of endogenous macrophages or any remaining CD4(+) T cells did not delay graft rejection in the macrophage-transferred FPP recipients, whereas depletion of transferred macrophages with clodronate liposomes prevented graft rejection. Our results show that macrophages primed by FPP and activated by CD4(+) T cells were attracted from the peripheral circulation and were capable of specific targeting and destruction of FPP xenografts. This suggests that in xenograft rejection, there are macrophage-specific recognition and targeting signals that are independent of those received by T cells.
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页码:2750 / 2758
页数:9
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