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The Antigen Receptor (NCCRP-1) on Catfish and Zebrafish Nonspecific Cytotoxic Cells Belongs to a New Gene Family Characterized by an F-Box-Associated Domain

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Abstract

The catfish nonspecific cytotoxic cell receptor protein (NCCRP-1) provides an important function in target cell recognition and activation of cytotoxicity. This report identifies and characterizes a zebrafish orthologue of the catfish NCCRP-1. The zebrafish NCCRP-1 cDNA contains an open reading frame that encodes a predicted protein of 237 amino acids with a MW of 27 kDa and a pI of 5.5. Sequence similarities comparisons show that the NCCRP-1 receptors from these two phylogenetically distant species share a high degree of identity. These results suggested that NCCRP-1 performs a crucial function in innate immunity in teleosts. Further, a zebrafish 17-mer peptide corresponding to the catfish NCCRP-1 antigen-binding domain inhibited (catfish) cytotoxicity toward conventional tumor target cells (HL-60). These data appeared to indicate that the zebrafish NCCRP-1 protein may function as an antigen recognition molecule and, as such, may participate in innate immunity in teleosts. A homology search of the zebrafish NCCRP-1 protein revealed that it shares a significant level of identity with another group of proteins belonging to an F-box subfamily. These proteins share an F-box domain in the N terminus (not present in NCCRP-1) and an extremely conserved C-terminal region that has been termed the F-box-associated domain (FBA). The FBA is currently of unknown function. A new gene family is proposed in this work, based on similarities in the FBA sequences with the catfish and zebrafish NCCRP-1 peptides. This new gene family includes several F-box domain-containing proteins and a predicted C. elegans protein.

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Received: 20 June 2001 / Accepted: 31 August 2001

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Jaso-Friedmann, L., Peterson, D., Gonzalez, D. et al. The Antigen Receptor (NCCRP-1) on Catfish and Zebrafish Nonspecific Cytotoxic Cells Belongs to a New Gene Family Characterized by an F-Box-Associated Domain. J Mol Evol 54, 386–395 (2002). https://doi.org/10.1007/s00239-001-0027-8

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  • DOI: https://doi.org/10.1007/s00239-001-0027-8

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