Literature DB >> 1712490

Molecular cloning and primary structure of Kell blood group protein.

S Lee1, E D Zambas, W L Marsh, C M Redman.   

Abstract

The Kell blood group is a major antigenic system in human erythrocytes. Kell antigens reside on a 93-kDa membrane glycoprotein that is surface-exposed and associated with the underlying cytoskeleton. We isolated tryptic peptides and, based on the amino acid sequence of one of the peptides and by using the PCR, prepared a specific oligonucleotide to screen a lambda gt10 human bone-marrow cDNA library. Four clones were isolated, one containing cDNA with an open reading frame for an 83-kDa protein. All known Kell amino acid sequences were present in the deduced sequence; moreover, rabbit antibody to a 30-amino acid peptide, prepared from this sequence, reacted on an immunoblot with authentic Kell protein. The Kell cDNA sequence predicts a 732-amino acid protein. Hydropathy analysis indicates a single membrane-spanning region, suggesting that Kell protein is oriented with 47 of its N-terminal amino acids in the cell cytoplasm, and a 665-amino acid segment, which contains six possible N-glycosylation sites, is located extracellularly. Computer-based search showed that Kell has structural and sequence homology to a family of zinc metalloglycoproteins with neutral endopeptidase activity.

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Year:  1991        PMID: 1712490      PMCID: PMC52081          DOI: 10.1073/pnas.88.14.6353

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  30 in total

1.  Kell blood group antigens are part of a 93,000-dalton red cell membrane protein.

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4.  Characterization of the blood group Kell (K1) antigen with a human monoclonal antibody.

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6.  The function and structure of the metal coordination sites within the glucocorticoid receptor DNA binding domain.

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8.  Genetic evidence that zinc is an essential co-factor in the DNA binding domain of GAL4 protein.

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Authors:  M A Shipp; J Vijayaraghavan; E V Schmidt; E L Masteller; L D'Adamio; L B Hersh; E L Reinherz
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  26 in total

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Authors:  K R Purohit; J L Weber; L J Ward; B J Keats
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2.  Another example of a KEL1 variant red cell phenotype due to a threonine to serine change at position 193 of Kell glycoprotein.

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4.  Mutagenesis of Glu403 to Cys in rabbit neutral endopeptidase-24.11 (neprilysin) creates a disulphide-linked homodimer: analogy with endothelin-converting enzyme.

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5.  Withdrawn

Authors: 
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7.  Regional chromosomal assignment of the Kell blood group locus (KEL) to chromosome 7q33-q35 by fluorescence in situ hybridization: evidence for the polypeptide nature of antigenic variation.

Authors:  M T Murphy; N Morrison; J S Miles; R H Fraser; N K Spurr; E Boyd
Journal:  Hum Genet       Date:  1993-07       Impact factor: 4.132

8.  Computer modeling and nanosecond simulation of the enzyme-substrate complex of the common lymphoblastic leukemia antigen (neprilysin) indicates shared residues at the primary specificity pocket (S1') with matrix metalloproteases.

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10.  Biosynthesis, processing, trafficking, and enzymatic activity of mouse neprilysin 2.

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