Protection of xenografts by a combination of immunoisolation and a single dose of anti-CD4 antibody
Details
Publication Year 2001-03-01,Volume 10,Issue #2,Page 183-193
Journal Title
CELL TRANSPLANTATION
Publication Type
Journal Article
Abstract
Immunoisolation is the separation of transplanted cells from cells of the immune system using a semipermeable membrane. Using one such immunoisolation capsule-the TheraCyte (R) device-we have assessed the survival of encapsulated xenogeneic tissue in vivo as well as the contribution of CD3(+\e) T cells to encapsulated xenograft rejection. The foreign body reaction to the TheraCyte (R) capsule in vivo was assessed by transplanting empty capsules into normal mice. These capsules elicit a foreign body response by the host animal. Encapsulated CHO, NIT-1, and PK-15 cells were placed in culture and in immunodeficient mice to investigate their growth characteristics in the TheraCyte (R) device. These cell lines survive both in culture and in immunodeficient SCID mice. Xenogeneic PK cells were also transplanted into normal C57BL/6 mice. These cells do not survive in normal mice despite the absence of direct contact between infiltrating and encapsulated cells. In addition, the survival of encapsulated cells in mice treated with a single dose of anti-CD4 antibody was examined. This was assessed using two systems: 1) histological analysis of capsule sections: 2) a quantitative luciferase reporter system using PK cells transfected to express luciferase. In both cases, anti-CD4 antibody contributed to prolonged encapsulated xenogeneic cell survival. Encapsulated xenogeneic cells survive in immunodeficient mice but not normal mice. Treatment of normal mice with anti-CD3 antibody results in prolonged survival of xenogeneic cells that can be measured using a luciferase reporter system. These results highlight the contribution of CD4(+\e) T cells to encapsulated xenograft rejection.
Publisher
COGNIZANT COMMUNICATION CORP
Keywords
CELL-IMPERMEABLE MEMBRANES; HUMAN FACTOR-IX; MONOCLONAL-ANTIBODY; DIFFUSION-CHAMBERS; ISLET XENOGRAFTS; T-CELLS; MICE; DESTRUCTION; NEOVASCULARIZATION; TRANSPLANTATION
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Creation Date: 2001-03-01 12:00:00
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