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Chiloscyllium plagiosum low-density lipoprotein receptor: Evolutionary conservation of five different functional domains
Authors:Kamal D Mehta  Ruixin Chang  James Norman
Institution:(1) Department of Biochemistry and Molecular Biology, Biomedical Research Building, University of Arkansas for Medical Sciences, College of Medicine, 4301 West Markham, 72205 Little Rock, AR, USA
Abstract:All five functional domains of the low-density lipoprotein (LDL) receptor were assembled in their modern form more than 450 million years ago, as revealed from the cloning and sequencing of an LDL receptor cDNA fromChiloscyllium plagiosum (banded cat shark). The shark LDL receptor has the same overall architecture as the mammalian and amphibian counterparts. Each of the seven cysteine-rich repeats in the ligand binding domain resembles its counterpart in the human LDL receptor more than it does the other repeats in the shark receptor as suggested by the presence of unique ldquosignaturerdquo sequences, indicating that these repeats had already acquired their independent structures by the time of shark development. Furthermore, amino acid sequences of the entire ligand binding domain of shark LDL receptor show 35% identity over a stretch of 294 residues with aLymnaea stagnalis G-protein-linked receptor (LSGLR). The region of homology between these unrelated proteins includes conservation of most of the unique characteristics of the cysteine-rich repeats of LDL receptor at the expected positions in LSGLR. The results presented are consistent with the hypothesis that all seven repeats in the ligand binding domain of LDL receptor may have been lifted directly from an ancestral gene instead of being evolutionary duplications of a single repeat recruited by the primitive LDL receptor from another gene.The nucleotide sequence reported will appear in GenBank under accession number L36118
Keywords:LDL receptor  Interspecies amino acid sequence homology  Ligand binding domain  G-protein-linked receptor  Evolution (Chiloscyllium plagiosum)
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