2016
DOI: 10.1128/jvi.01068-16
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A Highly Conserved gp120 Inner Domain Residue Modulates Env Conformation and Trimer Stability

Abstract: Previous studies have shown that highly conserved residues in the inner domain of gp120 are required for HIV-1 envelope glycoprotein ( We evaluated the contribution of the hydrophobicity of W69 to conformational changes of Env by replacing it with a series of residues with aliphatic or aromatic side chains of decreasing chain length. We have found that the hydrophobicity of residue 69 is important for Env processing, CD4 binding, and its transition to the CD4-bound conformation. The most deleterious effect was… Show more

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Cited by 19 publications
(18 citation statements)
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“…Mutation of CD4-BS2 residues resulted in decreased CCR5 and 48d binding in the absence of sCD4 (Supplementary Fig. 6b), confirming previous mutagenesis studies that attributed this effect to reduced monomer flexibility caused by altered inter-layer interactions within the inner domain 7,31 . In contrast, in the presence of sCD4, binding to 48d was unaffected by CD4-BS2 mutations, demonstrating that sCD4 was able to induce the full range of conformational changes in the context of the mutated monomer, while binding to CCR5 was only moderately reduced, with the exception of mutant K207E that, as expected, lost the ability to bind CCR5 since this residue is part of the coreceptor-contact surface 32 (Supplementary Fig.…”
Section: Resultssupporting
confidence: 86%
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“…Mutation of CD4-BS2 residues resulted in decreased CCR5 and 48d binding in the absence of sCD4 (Supplementary Fig. 6b), confirming previous mutagenesis studies that attributed this effect to reduced monomer flexibility caused by altered inter-layer interactions within the inner domain 7,31 . In contrast, in the presence of sCD4, binding to 48d was unaffected by CD4-BS2 mutations, demonstrating that sCD4 was able to induce the full range of conformational changes in the context of the mutated monomer, while binding to CCR5 was only moderately reduced, with the exception of mutant K207E that, as expected, lost the ability to bind CCR5 since this residue is part of the coreceptor-contact surface 32 (Supplementary Fig.…”
Section: Resultssupporting
confidence: 86%
“…7). Thus, as suggested 7,31 , the slight reduction of CD4 and CCR5 binding observed in the context of monomeric gp120, as well as the reduced binding of mAb 48d in the absence of sCD4, may be due to reduced molecular flexibility and distant allosteric effects secondary to altered inter-layer adherence within the flexible inner domain of the gp120 glycoprotein.…”
Section: Resultsmentioning
confidence: 76%
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“…Processing was performed and association indices were determined by precipitation of radiolabeled cell lysates and supernatants with mixtures of sera from HIV-1-infected individuals, as previously described (7,26,46,52,53,79). The association index is a measure of the ability of the gp120 molecule to remain associated with the mutant Env trimer complex on the expressing cell, relative to that of the wild-type Env.…”
Section: Methodsmentioning
confidence: 99%
“…Based on their neutralization by sera from HIV-infected individuals, primary isolates are classified using a tiered system; tier-1 Envs are globally sensitive, whereas tier-2 or tier-3 Envs (more commonly encountered in patients) are more resistant (17). Single-site mutations in gp120 or gp41 can render resistant Envs globally sensitive to antibodies (18)(19)(20)(21)(22)(23)(24)(25).…”
mentioning
confidence: 99%