Literature DB >> 21454587

Glycine dimerization motif in the N-terminal transmembrane domain of the high density lipoprotein receptor SR-BI required for normal receptor oligomerization and lipid transport.

Leonid Gaidukov1, Andrew R Nager, Shangzhe Xu, Marsha Penman, Monty Krieger.   

Abstract

Scavenger receptor class B, type I (SR-BI), a CD36 superfamily member, is an oligomeric high density lipoprotein (HDL) receptor that mediates negatively cooperative HDL binding and selective lipid uptake. We identified in the N-terminal transmembrane (N-TM) domain of SR-BI a conserved glycine dimerization motif, G(15)X(2)G(18)X(3)AX(2)G(25), of which the submotif G(18)X(3)AX(2)G(25) significantly contributes to homodimerization and lipid uptake activity. SR-BI variants were generated by mutations (single or multiple GlyLeu substitutions) or by replacing the N-TM domain with those from other CD36 superfamily members containing (croquemort) or lacking (lysosomal integral membrane protein (LIMP) II) this glycine motif (chimeras). None of the SR-BI variants exhibited altered surface expression (based on antibody binding) or HDL binding. However, the G15L/G18L/G25L triple mutant exhibited reductions in cell surface homo-oligomerization (>10-fold) and the rate of selective lipid uptake (∼ 2-fold). Gly(18) and Gly(25) were necessary for normal lipid uptake activity of SR-BI and the SR-BI/croquemort chimera. The lipid uptake activity of the glycine motif-deficient SR-BI/LIMP II chimera was low but could be increased by introducing glycines at positions 18 and 25. The rate of lipid uptake mediated by SR-BI/LIMP II chimeras was proportional to the extent of receptor oligomerization. Thus, the glycine dimerization motif G(18)X(3)AX(2)G(25) in the N-TM domain of SR-BI contributes substantially to the homo-oligomerization and lipid transport activity of SR-BI but does not influence the negative cooperativity of HDL binding. Oligomerization-independent binding cooperativity suggests that classic allostery is not involved and that the negative cooperativity is probably the consequence of a "lattice effect" (interligand steric interference accompanying binding to adjacent receptors).

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Year:  2011        PMID: 21454587      PMCID: PMC3099662          DOI: 10.1074/jbc.M111.229872

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


  85 in total

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Journal:  Arteriosclerosis       Date:  1990 Nov-Dec

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Journal:  J Biol Chem       Date:  1991-09-05       Impact factor: 5.157

4.  Structures and high and low affinity ligand binding properties of murine type I and type II macrophage scavenger receptors.

Authors:  J Ashkenas; M Penman; E Vasile; S Acton; M Freeman; M Krieger
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5.  Glycophorin A dimerization is driven by specific interactions between transmembrane alpha-helices.

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8.  Ligand size as a determinant for catabolism by the low density lipoprotein (LDL) receptor pathway. A lattice model for LDL binding.

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Journal:  J Biol Chem       Date:  1991-10-15       Impact factor: 5.157

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Journal:  J Biol Chem       Date:  1987-02-25       Impact factor: 5.157
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  35 in total

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Journal:  Metabolism       Date:  2014-03-21       Impact factor: 8.694

3.  Extracellular disulfide bonds support scavenger receptor class B type I-mediated cholesterol transport.

Authors:  Gabriella A Papale; Paul J Hanson; Daisy Sahoo
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4.  Benzo-fused lactams from a diversity-oriented synthesis (DOS) library as inhibitors of scavenger receptor BI (SR-BI)-mediated lipid uptake.

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Journal:  Bioorg Med Chem Lett       Date:  2015-04-01       Impact factor: 2.823

Review 5.  SR-B1: A Unique Multifunctional Receptor for Cholesterol Influx and Efflux.

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7.  Exoplasmic cysteine Cys384 of the HDL receptor SR-BI is critical for its sensitivity to a small-molecule inhibitor and normal lipid transport activity.

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Review 8.  Transmembrane helix dimerization: beyond the search for sequence motifs.

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Review 9.  Scavenger receptor B type 1: expression, molecular regulation, and cholesterol transport function.

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