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Query: UMLS:C0019693 (
HIV
)
170,526
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mutations at the glossy1 (gl1) locus of maize (Zea mays L.) quantitatively and qualitatively affect the deposition of cuticular waxes on the surface of seedling leaves. The gl1 locus has been molecularly cloned by transposon tagging with the Mutator transposon system. The epi23 cDNA was isolated by subtractive hybridization as an epidermis-specific mRNA from Senecio odora (Kleinia odora). The deduced amino acid sequence of the GL1 and EPI23 proteins are very similar to each other and to two other plant proteins in which the sequences were deduced from their respective mRNAs. These are the Arabidopsis CER1 protein, which is involved in cuticular wax deposition on siliques, stems, and leaves of that plant, and the protein coded by the rice expressed sequence tag RICS2751A. All four proteins are predicted to be localized in a membrane via a common NH2-terminal domain, which consists of either five or seven membrane-spanning helices. The COOH-terminal portion of each of these proteins, although less conserved, is predicted to be a water-soluble, globular domain. These sequence similarities indicate that these plant orthologs may belong to a superfamily of membrane-bound receptors that have been extensively characterized from animals, including the
HIV
co-receptor fusin (also termed
CXCR4
).
...
PMID:The glossy1 locus of maize and an epidermis-specific cDNA from Kleinia odora define a class of receptor-like proteins required for the normal accumulation of cuticular waxes. 911 70
Since some murine cells expressing human CD4 fail to internalize
HIV
-1, another block was thought to be located at the level of viral entry in addition to CD4. Recently,
CXCR4
was shown to function as a coreceptor for T cell line-tropic
HIV
-1 entry. Here we demonstrated that cells expressing murine
CXCR4
and human CD4 fused with cells expressing the env proteins derived from T cell line-tropic
HIV
-1 and were infected with T cell line-tropic
HIV
-1 strains. In contrast, the same cells were not infected with chimeric clones constructed by substitution of monocyte- or macrophage-tropic strain-derived env region or V3 region into T cell line-tropic
HIV
-1, indicating V3 loop of envelope protein is required for murine CXCR4mediated
HIV
-1 entry. We conclude that murine
CXCR4
is not a species specific barrier to the entry of T cell line-tropic
HIV
-1.
...
PMID:CXCR4/fusin is not a species-specific barrier in murine cells for HIV-1 entry. 915 12
The chemokine receptors
CXCR4
, CCR2B, CCR3, and CCR5 have recently been shown to serve along with CD4 as coreceptors for
HIV
-1. The tropisms of
HIV
-1 strains for subgroups of CD4(+) cells can be explained, at least partly, by the selective use of G protein-coupled receptors (GPCRs). We have identified a novel human gene, STRL33, located on chromosome 3 that encodes a GPCR with sequence similarity to chemokine receptors and to chemokine receptor-like orphan receptors. STRL33 is expressed in lymphoid tissues and activated T cells, and is induced in activated peripheral blood lymphocytes. When transfected into nonhuman NIH 3T3 cells expressing human CD4, the STRL33 cDNA rendered these cells competent to fuse with cells expressing
HIV
-1 envelope glycoproteins (Envs). Of greatest interest, STRL33, in contrast with
CXCR4
or CCR5, was able to function as a cofactor for fusion mediated by Envs from both T cell line-tropic and macrophage-tropic
HIV
-1 strains. STRL33-transfected Jurkat cell lines also supported enhanced productive infection with
HIV
-1 compared with control Jurkat cells. Despite the sequence similarities between STRL33 and chemokine receptors, STRL33-transfected cell lines did not respond to any in a panel of chemokines. Based on the pattern of tissue expression of the STRL33 mRNA, and given the ability of STRL33 to function with Envs of differing tropisms, STRL33 may play a role in the establishment and/or progression of
HIV
-1 infection.
...
PMID:STRL33, A novel chemokine receptor-like protein, functions as a fusion cofactor for both macrophage-tropic and T cell line-tropic HIV-1. 916 30
The chemokine receptor CXCR4 functions as a fusion coreceptor for T cell tropic and dual-tropic
HIV
-1 strains. To identify regions of
CXCR4
that are important for coreceptor function,
CXCR4
-CXCR2 receptor chimeras were tested for the ability to support
HIV
-1 envelope (env) protein-mediated membrane fusion. Receptor chimeras containing the first and second extracellular loops of
CXCR4
supported fusion by T tropic and dual-tropic
HIV
-1 and
HIV
-2 strains and binding of a monoclonal antibody to
CXCR4
, 12G5, that blocks
CXCR4
-dependent infection by some virus strains. The second extracellular loop of
CXCR4
was sufficient to confer coreceptor function to CXCR2 for most virus strains tested but did not support binding of 12G5. Truncation of the
CXCR4
cytoplasmic tail or mutation of a conserved DRY motif in the second intracellular loop did not affect coreceptor function, indicating that phosphorylation of the cytoplasmic tail and the DRY motif are not required for coreceptor function. The results implicate the involvement of multiple
CXCR4
domains in
HIV
-1 coreceptor function, especially the second extracellular loop, though the structural requirements for coreceptor function were somewhat variable for different env proteins. Finally, a hybrid receptor in which the amino terminus of
CXCR4
was replaced by that of CCR5 was active as a coreceptor for M tropic, T tropic, and dual-tropic env proteins. We propose that dual tropism may evolve in CCR5-restricted
HIV
-1 strains through acquisition of the ability to utilize the first and second extracellular loops of
CXCR4
while retaining the ability to interact with the CCR5 amino-terminal domain.
...
PMID:Evolution of HIV-1 coreceptor usage through interactions with distinct CCR5 and CXCR4 domains. 917 34
The human cytomegalovirus encodes a beta-chemokine receptor (US28) that is distantly related to the human chemokine receptors CCR5 and
CXCR4
, which also serve as cofactors for the entry into cells of human immunodeficiency virus-type 1 (HIV-1). Like CCR5, US28 allowed infection of CD4-positive human cell lines by primary isolates of
HIV
-1 and
HIV
-2, as well as fusion of these cell lines with cells expressing the viral envelope proteins. In addition, US28 mediated infection by cell line-adapted
HIV
-1 for which
CXCR4
was an entry cofactor.
...
PMID:Identification of a chemokine receptor encoded by human cytomegalovirus as a cofactor for HIV-1 entry. 920 39
Ligation of CCR5 by the CC chemokines RANTES, MIP-1alpha or MIP-1beta, and of
CXCR4
by the CXC chemokine SDF-1alpha, profoundly inhibits the replication of
HIV
strains that use these coreceptors for entry into CD4(+) T lymphocytes. The mechanism of entry inhibition is not known. We found a rapid and extensive downregulation of
CXCR4
by SDF-1alpha and of CCR5 by RANTES or the antagonist RANTES(9-68). Confocal laser scanning microscopy showed that CCR5 and
CXCR4
, after binding to their ligands, are internalized into vesicles that qualify as early endosomes as indicated by colocalization with transferrin receptors. Internalization was not affected by treatment with Bordetella pertussis toxin, showing that it is independent of signaling via Gi-proteins. Removal of SDF-1alpha led to rapid, but incomplete surface reexpression of
CXCR4
, a process that was not inhibited by cycloheximide, suggesting that the coreceptor is recycling from the internalization pool. Deletion of the COOH-terminal, cytoplasmic domain of
CXCR4
did not affect
HIV
entry, but prevented SDF-1alpha-induced receptor downregulation and decreased the potency of SDF-1alpha as inhibitor of
HIV
replication. Our results indicate that the ability of the coreceptor to internalize is not required for
HIV
entry, but contributes to the
HIV
suppressive effect of CXC and CC chemokines.
...
PMID:HIV coreceptor downregulation as antiviral principle: SDF-1alpha-dependent internalization of the chemokine receptor CXCR4 contributes to inhibition of HIV replication. 920 8
Several members of the chemokine-receptor family serve, in conjunction with CD4, as receptors for the entry of human immunodeficiency virus type I (
HIV
-1) into cells. The principal receptor for entry of macrophage-tropic (M-tropic)
HIV
-1 strains is CCR5, whereas that for T-cell-line-tropic (T-tropic) strains is
CXCR4
. Unlike
HIV
-1, infection with either M-tropic or T-tropic strains of simian immunodeficiency virus (SIV) can be mediated by CCR5, but not
CXCR4
. SIV strains will also infect CD4+ cells that lack CCR5, which suggests that these strains use as yet unidentified receptors. Here we use an expression-cloning strategy to identify SIV receptors and have isolated genes encoding two members of the seven-transmembrane G-protein-coupled receptor family that are used not only by SIVs, but also by strains of
HIV
-2 and M-tropic
HIV
-1. Both receptors are closely related to the chemokine-receptor family and are expressed in lymphoid tissues. One of the receptors is also expressed in colon and may therefore be important in viral transmission. Usage of these new receptors following experimental infection of non-human primates with SIV strains may provide important insight into viral transmission and the mechanisms of SIV- and
HIV
-induced acquired immune-deficiency syndrome.
...
PMID:Expression cloning of new receptors used by simian and human immunodeficiency viruses. 923 Apr 27
The chemokines are a homologous serum protein family characterized by their ability to induce activation of integrin adhesion molecules and leukocyte migration. Chemokines interact with their receptors, which are composed of a single-chain, seven-helix, membrane-spanning protein coupled to G proteins. Two CC chemokine receptors, CCR3 and CCR5, as well as the
CXCR4
chemokine receptor, have been shown necessary for infection by several
HIV
-1 virus isolates. We studied the effect of the chemokine monocyte chemoattractant protein 1 (MCP-1) and of a panel of MCP-1 receptor (CCR2)-specific monoclonal antibodies (mAb) on the suppression of
HIV
-1 replication in peripheral blood mononuclear cells. We have compelling evidence that MCP-1 has potent
HIV
-1 suppressive activity when
HIV
-1-infected peripheral blood lymphocytes are used as target cells. Furthermore, mAb specific for the MCP-1R CCR2 which recognize the third extracellular CCR2 domain inhibit all MCP-1 activity and also block MCP-1 suppressive activity. Finally, a set of mAb specific for the CCR2 amino-terminal domain, one of which mimics MCP-1 activity, has a potent suppressive effect on
HIV
-1 replication in M- and T-tropic
HIV
-1 viral isolates. We conjecture a role for CCR2 as a coreceptor for
HIV
-1 infection and map the
HIV
-1 binding site to the amino-terminal part of this receptor. This concurs with results showing that the CCR5 amino terminus is relevant in
HIV
-1 infection, although chimeric fusion of various extracellular domains shows that other domains are also implicated. We discuss the importance of CCR2 structure relative to its coreceptor role and the role of anti-CCR2 receptor antibodies in the prevention of
HIV
-1 infection.
...
PMID:The amino-terminal domain of the CCR2 chemokine receptor acts as coreceptor for HIV-1 infection. 923 95
The critical role of chemokine receptors (CCR5 and
CXCR4
) in human immunodeficiency virus-type 1 (HIV-1) infection and pathogenesis prompted a search for polymorphisms in other chemokine receptor genes that mediate
HIV
-1 disease progression. A mutation (CCR2-64I) within the first transmembrane region of the CCR2 chemokine and
HIV
-1 receptor gene is described that occurred at an allele frequency of 10 to 15 percent among Caucasians and African Americans. Genetic association analysis of five acquired immunodeficiency syndrome (AIDS) cohorts (3003 patients) revealed that although CCR2-64I exerts no influence on the incidence of
HIV
-1 infection,
HIV
-1-infected individuals carrying the CCR2-64I allele progressed to AIDS 2 to 4 years later than individuals homozygous for the common allele. Because CCR2-64I occurs invariably on a CCR5-+-bearing chromosomal haplotype, the independent effects of CCR5-Delta32 (which also delays AIDS onset) and CCR2-64I were determined. An estimated 38 to 45 percent of AIDS patients whose disease progresses rapidly (less than 3 years until onset of AIDS symptoms after HIV-1 exposure) can be attributed to their CCR2-+/+ or CCR5-+/+ genotype, whereas the survival of 28 to 29 percent of long-term survivors, who avoid AIDS for 16 years or more, can be explained by a mutant genotype for CCR2 or CCR5.
...
PMID:Contrasting genetic influence of CCR2 and CCR5 variants on HIV-1 infection and disease progression. Hemophilia Growth and Development Study (HGDS), Multicenter AIDS Cohort Study (MACS), Multicenter Hemophilia Cohort Study (MHCS), San Francisco City Cohort (SFCC), ALIVE Study. 925 28
The chemokine receptors
CXCR4
, CCR2b, CCR3, and CCR5 are cell entry coreceptors for
HIV
-1. Using an
HIV
-1 envelope (Env)-dependent cell-cell fusion model of entry, we show that CCR3 can interact with Envs from certain macrophage (M)-tropic strains (which also use CCR5), T cell line (TCL)-tropic laboratory-adapted strains (which also use
CXCR4
), and a dual-tropic primary isolate (which also uses CCR2b, CCR5, and
CXCR4
). Paradoxically, CCR1 is the closest homologue to CCR3 (63% amino acid identity), but lacked
HIV
-1 coreceptor activity. These results confirm and extend previous reports. Replacing the N-terminal segment of CCR3 with that of CCR1 abolished activity of the resulting chimera for M-tropic and TCL-tropic Envs, but not for the dual-tropic Env. Replacing extracellular loop 2 of CCR3 with that of CCR1 abolished activity for TCL-tropic Envs, but not for M- and dual-tropic Envs. A chimera containing all four extracellular regions of CCR3 on a backbone of CCR1 lacked any activity. Env-CCR3 interactions were strongly inhibited by the major CCR3 ligand eotaxin, but weakly or not at all by other CCR3 ligands. With primary macrophages, eotaxin induced transient calcium flux and partially inhibited fusion with cells expressing M-tropic Envs. We conclude that specificity determinants for different Envs are located in shared and distinct extracellular regions of CCR3, the transmembrane/cytoplasmic domains make major contributions to coreceptor function, and CCR3 may be used by certain
HIV
-1 strains as a cell fusion factor on macrophages.
...
PMID:Determinants of HIV-1 coreceptor function on CC chemokine receptor 3. Importance of both extracellular and transmembrane/cytoplasmic regions. 925 50
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