AI Article Synopsis

  • Current organ transplantation success relies on calcineurin-inhibitor immunosuppressive regimens, but these often cause severe side effects due to targeting widely expressed molecules.
  • T-cell costimulation, particularly the CD28/CTLA4 pathway and its ligands CD80/CD86, offers a new immunosuppressive target, although earlier CTLA4 fusion proteins showed limited success in primate models.
  • A modified CTLA4-Ig called LEA29Y (belatacept) was developed with two amino acid changes, increasing its potency significantly in vitro and improving renal transplant survival in pre-clinical studies, suggesting that targeted immunotherapy may reduce harmful side effects of standard treatments.

Article Abstract

Current success in organ transplantation is dependent upon the use of calcineurin-inhibitor-based immunosuppressive regimens. Unfortunately, current immunotherapy targets molecules with ubiquitous expression resulting in devastating non-immune side effects. T-cell costimulation has been identified as a new potential immunosuppressive target. The best characterized pathway includes CD28, its homologue CTLA4 and their ligands CD80 and CD86. While an immunoglobulin fusion protein construct of CTLA4 suppressed rejection in rodents, it lacked efficacy in primate transplant models. In an attempt to increase the biologic potency of the parent molecule a novel, modified version of CTLA4-Ig, LEA29Y (belatacept), was constructed. Two amino acid substitutions (L104E and A29Y) gave rise to slower dissociation rates for both CD86 and CD80. The increased avidity resulted in a 10-fold increase in potency in vitro and significant prolongation of renal allograft survival in a pre-clinical primate model. The use of immunoselective biologics may provide effective maintenance immunosuppression while avoiding the collateral toxicities associated with conventional immunsuppressants.

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http://dx.doi.org/10.1111/j.1600-6143.2005.00749.xDOI Listing

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