Literature DB >> 2600087

Different combinations of cysteine-rich repeats mediate binding of low density lipoprotein receptor to two different proteins.

D W Russell1, M S Brown, J L Goldstein.   

Abstract

Seven imperfect repeats of a 40-amino acid cysteine-rich sequence constitute the ligand binding domain of the low density lipoprotein (LDL) receptor. To assess the contribution of each repeat, three site-directed mutations were made individually in each repeat: 1) deletion of the repeat, 2) substitution of a conserved isoleucine with aspartic acid, and 3) substitution of a conserved aspartic acid with tyrosine. cDNAs containing these mutations were transfected into simian COS cells and assayed for their ability to bind LDL, which contains a 500-kDa protein ligand (apoB-100), and beta-migrating very low density lipoprotein (beta-VLDL), which contains multiple copies of a 33-kDa ligand (apoE). The results showed that binding of the two ligands required different combinations of repeats. LDL binding required repeats 3-7; deletion of any one of these repeats markedly reduced LDL binding. In contrast, beta-migrating very low density lipoprotein binding was insensitive to the loss of any single repeat with the important exception of repeat 5, whose loss reduced binding by 60%. The same effects were obtained when each of the repeats was altered by either of the two substitution mutations. The current findings suggest that a multiplicity of cysteine-rich repeats may allow a single protein to bind several different protein ligands by employing different combinations of repeats.

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Year:  1989        PMID: 2600087

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  97 in total

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Journal:  J Biol Chem       Date:  2018-03-20       Impact factor: 5.157

7.  The binding ability analysis of the normal VLDL receptor and its mutant.

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10.  The LDL receptor and LRP are receptors for beta VLDL on pigeon monocyte-derived macrophages.

Authors:  N L Jones; M Gupta; J C Lewis
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