Constitutive cell surface association between CD4 and CCR5

Wu, Lijun; Stantchev, Tzanko S.; Feng, Yanru; Ugolini, Sophie; Chen, Hong; Shen, Zhimin; Riley, James L.; Broder, Christopher C.; Sattentau, Quentin J.; Dimitrov, Dimiter S.

doi:10.1073/pnas.96.13.7496

Cited by 169 publications

(153 citation statements)

References 43 publications

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“…Such interactions are likely to favor the association rate of gp120 with CCR5, recently proposed as being strictly dependent upon a close vicinity of CD4 and CCR5 in living cells (20). Furthermore, the observation that CD4 poorly co-immunoprecipitated with CXCR4 (19,21,22) supports the attractive hypothesis that preferential interactions between CCR5 and CD4 may be relevant to the predominance of R5-tropic HIV isolates in the course of viral infection. Nevertheless, this possibility remains debated, as it was recently inferred using coprecipitation, high-resolution deconvolution microscopy and resonance energy transfer techniques, that CD4 and CCR5 do not exist in a stable complex at the cell membrane (23,24).…”

Section: Entry Of Human Immunodeficiency Virus (Hiv)supporting

confidence: 50%

CD4 and CCR5 Constitutively Interact at the Plasma Membrane of Living Cells

Gaibelet

Planchenault

Mazères

et al. 2006

Journal of Biological Chemistry

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Human immunodeficiency virus entry into target cells requires sequential interactions of the viral glycoprotein envelope gp120 with CD4 and chemokine receptors CCR5 or CXCR4. CD4 interaction with the chemokine receptor is suggested to play a critical role in this process but to what extent such a mechanism takes place at the surface of target cells remains elusive. To address this issue, we used a confocal microspectrofluorimetric approach to monitor fluorescence resonance energy transfer at the cell plasma membrane between enhanced blue and green fluorescent proteins fused to CD4 and CCR5 receptors. We developed an efficient fluorescence resonance energy transfer analysis from experiments carried out on individual cells, revealing that receptors constitutively interact at the plasma membrane. Binding of R5-tropic HIV gp120 stabilizes these associations thus highlighting that ternary complexes between CD4, gp120, and CCR5 occur before the fusion process starts. Furthermore, the ability of CD4 truncated mutants and CCR5 ligands to prevent association of CD4 with CCR5 reveals that this interaction notably engages extracellular parts of receptors. Finally, we provide evidence that this interaction takes place outside raft domains of the plasma membrane. Entry of human immunodeficiency virus (HIV)4 into target cells relies on sequential interactions between gp120, the surface subunit of the viral glycoprotein envelope (Env), with cell surface CD4 and the G-protein-coupled chemokine receptors CXCR4 or CCR5 that act as co-receptors (1). Following binding to the co-receptor, conformational changes in Env are thought to expose its transmembrane subunit gp41, which inserts into the host cell plasma membrane and to initiate fusion and the infection processes (2).Triggering of an efficient fusion between viral and host cell membranes is thought to be a cooperative process that requires multiple engagements between Env and its receptors (3-5). Virus entry thus depends on membrane density of CD4 and chemokine receptors, which is expected to be influenced by their sequestration into delimited membrane domains. In support of this view, high-resolution electron microscopy-based approaches have demonstrated that CCR5, CXCR4, and CD4 form homogeneous microclusters on cell surface microvilli in primary macrophages and T cells (6). The requirement of cholesterol for chemokine receptor functions and HIV entry (7-9) led to the hypothesis that cholesterol-and sphingolipid-enriched raft membrane domains represent privileged sites in which receptors localize. Nonetheless, the observations that coreceptors barely associate with rafts (8, 10, 11) and that CD4 mutants localizing to non-raft domains are fully competent for HIV entry (8, 12) challenged this view.Clustering within domains is also likely to favor interaction between receptors, which is consistent with the proposed existence and functioning of CCR5 and CXCR4 as oligomers (13-16), a current view that also prevails for other classes of G-protein-coupled receptors (17, 18). In ear...

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Section: Entry Of Human Immunodeficiency Virus (Hiv)supporting

confidence: 50%

CD4 and CCR5 Constitutively Interact at the Plasma Membrane of Living Cells

Gaibelet

Planchenault

Mazères

et al. 2006

Journal of Biological Chemistry

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“…Apparently, receptors involved in sensing chemotactic gradients are preferentially localized to the leading edge in a polarized cell. CCR5 also colocalizes with CD4 at the cell surface [9]. Viewed altogether, these data suggest that the localization of CCRs to the leading edge may allow for interaction with TCRs, thereby modulating TCR mediated signaling cascades.…”

Section: A Role For Chemokines In the Recruitment And Polarization Ofmentioning

confidence: 70%

“…GPCR-mediated transactivation of the epidermal growth factor [107] and the platelet-derived growth factor receptors [108] have been reported. Given that CCL5-CCR5 activation of Jurkat T cells correlates with the expression of CD3 [19], that CCR5 expression is associated with constitutive CD4 [9] expression and CCR5 localizes to lipid rafts upon ligand binding [4,6], activated CCR5 may function to recruit signaling intermediates of the TCR to potentiate (co)stimulation of T cells. CCL5 at micromolar doses can induce two distinct calcium fluxes in T cells: one dependent on G-proteins and the other on tyrosine kinases [15].…”

Section: Ccr Cross-talk With the Tcr Signaling Complexmentioning

confidence: 99%

Chemokines: attractive mediators of the immune response

Wong

Fish

2003

Seminars in Immunology

227

186

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“…Numerous experimental variables may contribute to complementation efficiency, including the surface densities of each of the participating proteins, the binding affinities between gp120 and each receptor, the efficiencies of subunit interactions, etc. The findings of constitutive interactions between CD4 and coreceptors may have significance in this regard (14,31), as may the recent proposal that cooperative interactions involving multiple CCR5 molecules are required for the HIV-1 infection pathway (32). Also of note is that certain complementation effects were not uniformly noted; for example, LAV-BS complemented SF162 wild type for fusion with CXCR4-expressing targets cells (Fig.…”

Section: Discussionmentioning

confidence: 92%

Cooperative subunit interactions within the oligomeric envelope glycoprotein of HIV-1: Functional complementation of specific defects in gp120 and gp41

Salzwedel

Berger

2000

Proc. Natl. Acad. Sci. U.S.A.

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The envelope glycoprotein (Env) of HIV-1 is displayed on the surface of the virion or infected cell as an oligomer of multiple gp120͞gp41 complexes. We sought to unravel the relationships between this oligomeric structure and the requirements for sequential interactions with CD4 and coreceptor (CCR5 or CXCR4). We used a quantitative cell fusion assay to examine the effects of coexpressing pairs of Envs, each nonfunctional because of a specific defect in one of the essential properties. We observed efficient fusion activity upon coexpression of two Env variants, one containing a gp41 subunit with a mutated fusion peptide and the other containing a gp120 subunit with a mutated CD4 binding site or a mismatched coreceptor specificity. We also observed fusion upon coexpression of two Env variants with distinct gp120 defects, i.e., a CD4 binding site mutation and the incorrect coreceptor specificity determinants. Coimmunoprecipitation experiments verified the efficient formation of mixed oligomers, suggesting that the observed fusion reflected subunit complementation within the oligomeric complex. These results support a model in which cooperative subunit interactions within the Env oligomer result in concerted conformational changes upon receptor binding, resulting in activation for fusion. The implications of these findings for Env function and virus neutralization are discussed.T he envelope glycoprotein (Env) of HIV-1 mediates virus entry into target cells by catalyzing a complex series of receptor-binding events and associated conformational changes that result ultimately in fusion between the membranes of the virion and target cell. The biochemical outline of the fusion reaction has been established (reviewed in refs. 1-4). The external gp120 subunit must bind to two distinct receptors on the target cell: CD4 (the ''primary receptor'') and a specific chemokine receptor (the coreceptor, usually CCR5 or CXCR4). These receptor interactions trigger the transmembrane gp41 subunit to promote fusion via a process that is presumed to involve insertion of its N-terminal fusion peptide into the membrane of the target cell. A specific sequence of receptor interactions is required to activate the fusion reaction, as revealed by binding analyses with soluble gp120 (5-7), fusion and infectivity experiments with soluble CD4 (8, 9), high-resolution x-ray crystallographic structural determinations (10), and sitedirected mutagenesis studies (11). In the favored model, CD4 binding exposes, creates, or stabilizes the coreceptor binding determinants on gp120; interaction with coreceptor triggers additional conformational changes, leading to gp41 activation and consequent fusion.Env is first synthesized as a high molecular weight precursor designated gp160. The protein forms a homo-oligomer in the endoplasmic reticulum and is transported to the Golgi apparatus where processing by a host cell protease(s) occurs; the functional Env on the surface of both the infected cell and the virion is a homo-oligomer of multiple gp120͞gp41 noncova...

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Constitutive cell surface association between CD4 and CCR5

Cited by 169 publications

References 43 publications

CD4 and CCR5 Constitutively Interact at the Plasma Membrane of Living Cells

CD4 and CCR5 Constitutively Interact at the Plasma Membrane of Living Cells

Chemokines: attractive mediators of the immune response

Cooperative subunit interactions within the oligomeric envelope glycoprotein of HIV-1: Functional complementation of specific defects in gp120 and gp41

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