Role of the Liver in Alloimmune Response following Inoculation of Donor Spleen Cells

Author:

He Li1,Dono Keizo1,Gotoh Mitsukazu2,Okumura Masaki1,Takeda Yutaka1,Shimizu Junzo1,Nagano Hiroaki1,Nakamori Shoji1,Umeshita Koji1,Sakon Masato1,Monden Morito1

Affiliation:

1. Department of Surgery II, Osaka University Medical School, Osaka 565-0871, Japan

2. Department of Surgery I, Fukushima Municipal Medical University, 1 Hikarigaoka, Fukushima 960-1295, Japan

Abstract

The liver is thought to be an immunologically privileged organ in the response to inoculated antigens. We previously demonstrated that it is possible to localize inoculated antigens to the liver alone or only to extrahepatic tissue using orthotopic syngeneic liver transplantation (OSLT). In this study, we analyzed more detailed mechanisms of the anti-alloimmune response in the liver. DA rat spleen cells were systemically injected into WS rats (donor spleen cell inoculation, DSI). In the sensitized liver-grafted (SLG) group, after DSI, liver grafts were retrieved from sensitized WS rats, then transplanted into naive WS rats. In the sensitized liver-removed (SLR) group, after DSI, WS rats were totally hepatectomized and given livers transplanted from naive WS rats. All the rats were challenged with heterotopic heart grafts 10 days after DSI. Mean heart graft survival in the control, DSI, SLG, and SLR groups were 11.6 ± 1.6, 10.7 ±2.4, 4.4 ± 1.0, and 24.6 ± 6.3 days, respectively. Accelerated rejection in the SLG group as well as graft prolongation in the SLR group disappeared when OSLT was performed 2 days after DSI or later. Irradiation of DA splenocytes before inoculation did not alter graft survival in SLG. However, pretreatment with gadolinium chloride prior to DSI attenuated the antidonor response in the SLG group. In conclusion, a vigorous antidonor response occurred in the liver after systemic inoculation of spleen cells. It peaked 1 day after DSI and disappeared rapidly. Kupffer cells seemed to play an important role in this phenomenon.

Publisher

SAGE Publications

Subject

Transplantation,Cell Biology,Biomedical Engineering

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