Grafting Segments from the Extracellular Surface of CCR5 onto a Bacteriorhodopsin Transmembrane Scaffold Confers HIV-1 Coreceptor Activity
Components from the extracellular surface of CCR5 interact with certain macrophage-tropic strains of human immunodeficiency virus type 1 (HIV-1) to mediate viral fusion and entry. To mimic these viral interacting site(s), the amino-terminal and extracellular loop segments of CCR5 were linked in tand...
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Published in | Structure (London) Vol. 10; no. 4; pp. 515 - 525 |
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Main Authors | , , , , , , |
Format | Journal Article |
Language | English |
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United States
Elsevier Inc
01.04.2002
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Abstract | Components from the extracellular surface of CCR5 interact with certain macrophage-tropic strains of human immunodeficiency virus type 1 (HIV-1) to mediate viral fusion and entry. To mimic these viral interacting site(s), the amino-terminal and extracellular loop segments of CCR5 were linked in tandem to form concatenated polypeptides, or grafted onto a seven-transmembrane bacteriorhodopsin scaffold to generate several chimeras. The chimera studies identified specific regions in CCR5 that confer HIV-1 coreceptor function, structural rearrangements in the transmembrane region that may modulate this activity, and a role for the extracellular surface in folding and assembly. Methods developed here may be applicable to the dissection of functional domains from other seven-transmembrane receptors and form a basis for future structural studies. |
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AbstractList | Components from the extracellular surface of CCR5 interact with certain macrophage-tropic strains of human immunodeficiency virus type 1 (HIV-1) to mediate viral fusion and entry. To mimic these viral interacting site(s), the amino-terminal and extracellular loop segments of CCR5 were linked in tandem to form concatenated polypeptides, or grafted onto a seven-transmembrane bacteriorhodopsin scaffold to generate several chimeras. The chimera studies identified specific regions in CCR5 that confer HIV-1 coreceptor function, structural rearrangements in the transmembrane region that may modulate this activity, and a role for the extracellular surface in folding and assembly. Methods developed here may be applicable to the dissection of functional domains from other seven-transmembrane receptors and form a basis for future structural studies. |
Author | Oprian, Daniel D Ngo, Tony Ridge, Kevin D Abdulaev, Najmoutin G Strassmaier, Timothy T Chen, Ruiwu Luecke, Hartmut |
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BackLink | https://www.ncbi.nlm.nih.gov/pubmed/11937056$$D View this record in MEDLINE/PubMed |
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Keywords | chimera G protein-coupled receptor HIV-1 CCR5 bacteriorhodopsin membrane protein folding |
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SubjectTerms | Amino Acid Sequence Animals bacteriorhodopsin Bacteriorhodopsins - chemistry Bacteriorhodopsins - genetics Bacteriorhodopsins - metabolism Cattle CCR5 chimera COS Cells G protein-coupled receptor Genes, Reporter HIV-1 HIV-1 - chemistry HIV-1 - metabolism Humans membrane protein folding Molecular Sequence Data Protein Structure, Secondary Receptors, CCR5 - chemistry Receptors, CCR5 - genetics Receptors, CCR5 - metabolism Receptors, HIV - chemistry Receptors, HIV - metabolism Recombinant Fusion Proteins - chemistry Recombinant Fusion Proteins - genetics Recombinant Fusion Proteins - metabolism Spectrum Analysis |
Title | Grafting Segments from the Extracellular Surface of CCR5 onto a Bacteriorhodopsin Transmembrane Scaffold Confers HIV-1 Coreceptor Activity |
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