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XB-ART-10867
Exp Eye Res 2000 Jun 01;706:731-6. doi: 10.1006/exer.2000.0839.
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Xenopus IRBP, a phylogenetically remote protein, is uveitogenic in Lewis rats.

Gelderman MP , Gonzalez-Fernandez F , Baer CA , Wiggert B , Chan CC , Vistica BP , Gery I .


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Mammalian interphotoreceptor retinoid-binding proteins (IRBPs) are highly uveitogenic in Lewis rats. Xenopus laevis IRBP resembles mammalian IRBP in its four-fold structure, and has approximately 70% amino acid sequence identity with the bovine protein. This study investigated the uveitogenicity of recombinant Xenopus IRBP and two of its derived peptides in Lewis rats. Rats immunized with Xenopus IRBP developed uveoretinitis as well as pineal inflammation. The Xenopus molecule was, however, less immunopathogenic than the bovine IRBP. Of the two Xenopus IRBP peptides tested, 1180-1191 was remarkably uveitogenic, whereas sequence 521-540 exhibited low activity. It is assumed, therefore, that as with bovine IRBP, peptide 1180-1191 is the major uveitogenic sequence in Xenopus IRBP. The role individual residues of these peptides play in the immunopathogenic process is discussed. Our data thus demonstrate that despite its being phylogenetically remote, Xenopus IRBP is uveitogenic in Lewis rats

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Species referenced: Xenopus laevis
Genes referenced: grb10 rbp3