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Blockade of the OX40 ligand prolongs corneal allograft survival

โœ Scribed by Takaaki Hattori; Yoshihiko Usui; Yoko Okunuki; Yasushi Sonoda; Masahiko Usui; Eiko Takada; Junichiro Mizuguchi; Hideo Yagita; Ko Okumura; Hisaya Akiba; Masaru Takeuchi


Book ID
102165455
Publisher
John Wiley and Sons
Year
2007
Tongue
English
Weight
205 KB
Volume
37
Category
Article
ISSN
0014-2980

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โœฆ Synopsis


Abstract

Although corneal transplantation is one of the most common tissue transplantations and is known to have a high graft acceptance rate, occasional corneal graft rejection remains a cause of blindness. OX40, a member of the TNF receptor superfamily, is expressed on activated T cells, and transmits a costimulatory signal by binding to OX40 ligand (OX40L) expressed on several cells with antigenโ€presenting functions. Using a blocking monoclonal antibody (mAb) against murine OX40L, we investigated the role of OX40 in a murine model of corneal transplantation. C3H/He mouse corneas were transplanted to BALB/c mice orthotopically. Administration of antiโ€OX40L mAb significantly reduced allograft rejection, and increased graft survival rate to 40% at 8โ€„weeks after transplantation, while all corneas were rejected within 5โ€„weeks in control IgGโ€treated mice. Similar reduced rejection was observed when wildโ€type donor corneas were transplanted to OX40Lโ€deficient recipients. In vitro study revealed that the antiโ€OX40L mAb treatment reduced proliferative response and IFNโ€ฮณ production of draining lymph node cells in response to stimulation with donor alloantigen. These results demonstrate that OX40L blockade is effective for prolongation of corneal allograft survival by inhibiting recipient T cell activation.


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