
doi: 10.1038/306611a0
pmid: 6316163
The primary structure of porcine preproenkephalin B has been elucidated by cloning and sequencing cDNA: it contains neoendorphin, dynorphin and leumorphin (containing rimorphin as its amino-terminus). These opioid peptides, each having a leucine-enkephalin structure, act on the kappa-receptor. We have now cloned a human genomic DNA segment containing the preproenkephalin B gene. The structural organization of this gene resembles those of the genes encoding the other opioid peptide precursors, that is, preproenkephalin A and the corticotropin-beta-lipotropin precursor (ACTH-beta-LPH precursor). The primary structure of human preproenkephalin B has been deduced from the gene sequence. The amino acid sequence homology observed between preproenkephalin B and preproenkephalin A, together with the similarity between their gene organizations, suggests that the two genes have been generated from a common ancestor by gene duplication.
Base Sequence, Swine, Animals, Humans, Amino Acid Sequence, DNA Restriction Enzymes, Enkephalins, Cloning, Molecular, Protein Precursors
Base Sequence, Swine, Animals, Humans, Amino Acid Sequence, DNA Restriction Enzymes, Enkephalins, Cloning, Molecular, Protein Precursors
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