Your search keyword '"Chemokine receptor CCR5"' showing total 10 results

1. Structure activity relationship studies of natural product chemokine receptor CCR5 antagonist anibamine toward the development of novel anti prostate cancer agents

Author

Zhang, Feng, Arnatt, Christopher K., Haney, Kendra M., Fang, Harrison C., Bajacan, John E., Richardson, Amanda C., Ware, Joy L., and Zhang, Yan

Subjects

*STRUCTURE-activity relationship in pharmacology, *CHEMOKINE receptors, *NATURAL products, *DRUG development, *ANTINEOPLASTIC agents, *PROSTATE cancer, *MOLECULAR structure

Abstract

Abstract: Recent studies have indicated that the CCR5 chemokine receptor may be a potential target for treating prostate cancer. Thus, development of CCR5 antagonists may provide novel prostate cancer therapy. Anibamine, a novel pyridine quaternary alkaloid isolated from Aniba sp., was found to effectively compete with 125I-gp120 in binding to the chemokine receptor CCR5, with an IC50 = 1 μM. Anibamine is the first natural product reported as a CCR5 antagonist, and thus provides a novel structural skeleton unique from other lead compounds that have generally been identified from high-throughput screening efforts. In order to refine the lead compound''s structure and improve the therapeutic index of anibamine derivatives as potential anti prostate cancer agents, the approach of “deconstruction–reconstruction–elaboration” was applied in the structure–activity relationship studies of this work. Here, we report the design, syntheses and anti prostate cancer activities of anibamine and 17 analogues. The results from the in vitro and in vivo studies described here show that this class of compounds has potential to provide novel leads as anti prostate cancer agents. [Copyright &y& Elsevier]

Published

2012

2. Anibamine, a natural product CCR5 antagonist, as a novel lead for the development of anti-prostate cancer agents

Author

Zhang, Xueping, Haney, Kendra M., Richardson, Amanda C., Wilson, Eden, Gewirtz, David A., Ware, Joy L., Zehner, Zendra E., and Zhang, Yan

Subjects

*NATURAL products, *CHEMICAL inhibitors, *ANTINEOPLASTIC agents, *DRUG development, *PROSTATE cancer treatment, *CHEMOKINES, *CELL receptors, *CELL proliferation

Abstract

Abstract: Accumulating evidence indicates that the chemokine receptor CCR5 and the chemokine CCL5 may be involved in the proliferation and metastasis of prostate cancer. Consequently, chemokine receptor CCR5 antagonists could potentially act as anti-prostate cancer agents. As the first natural product CCR5 antagonist, anibamine provides a novel chemical structural skeleton compared with other known antagonists identified through high-throughput screening. Our studies demonstrate that anibamine produces significant inhibition of prostate cancer cell proliferation at micromolar to submicromolar concentrations as well as suppressing adhesion and invasion of the highly metastatic M12 prostate cancer cell line. Preliminary in vivo studies indicate that anibamine also inhibits prostate tumor growth in mice. These findings indicate that anibamine may prove to be a novel lead compound for the development of prostate cancer therapeutic agents. [Copyright &y& Elsevier]

Published

2010

3. Beta-chemokine receptor CCR5 in human spermatozoa and its relationship with seminal parameters.

Author

Barbonetti, A., Vassallo, M. R. C., Pelliccione, F., D'Angeli, A., Santucci, R., Muciaccia, B., Stefanini, M., Francavilla, F., and Francavilla, S.

Subjects

*CHEMOKINES, *SPERMATOZOA, *CELL receptors, *GENE expression, *CELL membranes

Abstract

BACKGROUND: Chemokine receptor CCR5, the main HIV-1 coreceptor, is present in the human spermatozoa. This study aimed to investigate (i) whether the percentage of CCR5-positive spermatozoa varies under conditions associated with changes in the membrane architecture, such as capacitation and fixation/permeabilization procedures; (ii) whether there is any relationship between individual variability in sperm CCR5 expression and semen parameters. [ABSTRACT FROM PUBLISHER]

Published

2009

4. Is the European spatial distribution of the HIV-1-resistant CCR5-Δ32 allele formed by a breakdown of the pathocenosis due to the historical Roman expansion?

Author

Faure, Eric and Royer-Carenzi, Manuela

Subjects

*HIV infections, *CHEMOKINES, *ANTI-infective agents, *PATHOGENIC microorganisms, *VIRUS diseases, *GENETIC mutation, *FOSSIL DNA

Abstract

Abstract: We studied the possible effects of the expansion of ancient Mediterranean civilizations during the five centuries before and after Christ on the European distribution of the mutant allele for the chemokine receptor gene CCR5 which has a 32-bp deletion (CCR5-Δ32). There is a strong evidence for the unitary origin of the CCR5-Δ32 mutation, this it is found principally in Europe and Western Asia, with generally a north–south downhill cline frequency. Homozygous carriers of this mutation show a resistance to HIV-1 infection and a slower progression towards AIDS. However, HIV has clearly emerged too recently to have been the selective force on CCR5. Our analyses showed strong negative correlations in Europe between the allele frequency and two historical parameters, i.e. the first colonization dates by the great ancient Mediterranean civilizations, and the distances from the Northern frontiers of the Roman Empire in its greatest expansion. Moreover, other studies have shown that the deletion frequencies in both German Bronze Age and Swedish Neolithic populations were similar to those found in the corresponding modern populations, and this deletion has been found in ancient DNA of around 7000 years ago, suggesting that in the past, the deletion frequency could have been relatively high in European populations. In addition, in West Nile virus pathogenesis, CCR5 plays an antimicrobial role showing that host genetic factors are highly pathogen-specific. Our results added to all these previous data suggest that the actual European allele frequency distribution might not be due to genes spreading, but to a negative selection resulting in the spread of pathogens principally during Roman expansion. Indeed, as gene flows from colonizers to European native populations were extremely low, the mutational changes might be associated with vulnerability to imported infections. To date, the nature of the parasites remains unknown; however, zoonoses could be incriminated. [Copyright &y& Elsevier]

Published

2008

5. Analysis of second messenger pathways stimulated by different chemokines acting at the chemokine receptor CCR5

Author

Leach, K., Charlton, S.J., and Strange, P.G.

Subjects

*CHEMOKINES, *FORSKOLIN, *T cells, *PERTUSSIS toxin

Abstract

Abstract: The chemokine receptor, CCR5, responds to several chemokines leading to changes in activity in several signalling pathways. Here, we investigated the ability of different chemokines to provide differential activation of pathways. The effects of five CC chemokines acting at CCR5 were investigated for their ability to inhibit forskolin-stimulated 3′–5′-cyclic adenosine monophosphate (cAMP) accumulation and to stimulate Ca2+ mobilisation in Chinese hamster ovary (CHO) cells expressing CCR5. Macrophage inflammatory protein 1α (D26A) (MIP-1α (D26A), CCL3 (D26A)), regulated on activation, normal T-cell expressed and secreted (RANTES, CCL5), MIP-1β (CCL4) and monocyte chemoattractant protein 2 (MCP-2, CCL8) were able to inhibit forskolin-stimulated cAMP accumulation, whilst MCP-4 (CCL13) could not elicit a response. CCL3 (D26A), CCL4, CCL5, CCL8 and CCL13 were able to stimulate Ca2+ mobilisation through CCR5, although CCL3 (D26A) and CCL5 exhibited biphasic concentration–response curves. The Ca2+ responses induced by CCL4, CCL5, CCL8 and CCL13 were abolished by pertussis toxin, whereas the response to CCL3 (D26A) was only partially inhibited by pertussis toxin, indicating Gi/o-independent signalling induced by this chemokine. Although the rank order of potency of chemokines was similar between the two assays, certain chemokines displayed different pharmacological profiles in cAMP inhibition and Ca2+ mobilisation assays. For instance, whilst CCL13 could not inhibit forskolin-stimulated cAMP accumulation, this chemokine was able to induce Ca2+ mobilisation via CCR5. It is concluded that different chemokines acting at CCR5 can induce different pharmacological responses, which may account for the broad spectrum of chemokines that can act at CCR5. [Copyright &y& Elsevier]

Published

2007

6. Diverse signalling by different chemokines through the chemokine receptor CCR5

Author

Mueller, Anja, Mahmoud, Nasir G., and Strange, Philip G.

Subjects

*CHEMOKINES, *MEMBRANE proteins, *HIV, *BLOOD plasma

Abstract

Abstract: We have investigated the signalling properties of the chemokine receptor, CCR5, using several assays for agonism: stimulation of changes in intracellular Ca2+ or CCR5 internalisation in CHO cells expressing CCR5 or stimulation of [35S]GTPγS binding in membranes of CHO cells expressing CCR5. Four isoforms of the chemokine CCL3 with different amino termini (CCL3, CCL3(2–70), CCL3(5–70), CCL3L1) were tested in these assays in order to probe structure/activity relationships. Each isoform exhibited agonism. The pattern of agonism (potency, maximal effect) was different in the three assays, although the rank order was the same with CCL3L1 being the most potent and efficacious. The data show that the amino terminus of the chemokine is important for signalling. A proline at position 2 (CCL3L1) provides for high potency and efficacy but the isoform with a serine at position 2 (CCL3(2–70)) is as efficacious in some assays showing that the proline is not the only determinant of high efficacy. We also increased the sensitivity of CCR5 signalling by treating cells with sodium butyrate, thus increasing the receptor/G protein ratio. This allowed the detection of a change in intracellular Ca2+ after treatment with CCL7 and Met-RANTES showing that these ligands possess measurable but low efficacy. This study therefore shows that sodium butyrate treatment increases the sensitivity of signalling assays and enables the detection of efficacy in ligands previously considered as antagonists. The use of different assay systems, therefore, provides different estimates of efficacy for some ligands at this receptor. [Copyright &y& Elsevier]

Published

2006

7. Genomic organization, expression profile, and characterization of the new protein PRA1 domain family, member 2 (PRAF2)

Author

Fo, Crystal S., Coleman, Craig S., Wallick, Christopher J., Vine, Alex L., and Bachmann, André S.

Subjects

*HUMAN genetics, *HISTOLOGY, *HUMAN chromosomes, *CELL nuclei, *SMALL intestine, *LYMPHOID tissue

Abstract

Abstract: PRA1 domain family, member 2 (PRAF2) is a new 19 kDa protein with four putative transmembrane (TM) domains. PRAF2 (formerly designated JM4) belongs to a new protein family, which plays a role in the regulation of intracellular protein transport. Recently, PRAF2 was found to interact with the chemokine receptor CCR5 [Schweneker, M., Bachmann, A.S., Moelling, K., 2005. JM4 is a four-transmembrane protein binding to the CCR5 receptor. FEBS Lett. 579, 1751–1758]. In order to further study the function and regulation of PRAF2, we determined its genomic structure and its protein expression pattern in normal and cancerous human tissues. PRAF2 encodes a 178-residue protein, whose sequence is related to PRAF1 (PRA1/prenylin) and PRAF3 (JWA/GTRAP3–18). The human PRAF2 gene contains three exons separated by two introns and is located on human chromosome Xp11.23. The recombinant PRAF2 protein was readily expressed in Schneider 2 (S2) insect cells, and the native protein was detected in human tissues with strong expression in the brain, small intestine, lung, spleen, and pancreas. The protein was undetectable in tissue of the testes. Strong PRAF2 protein expression was also found in human tumor tissues of the breast, colon, lung, and ovary, with a weaker staining pattern in normal tissues of the same patient. Our studies show for the first time that the CCR5-interacting PRAF2 protein is expressed in several human tissues with a possible function in ER/Golgi transport and vesicular traffic. [Copyright &y& Elsevier]

Published

2006

8. Interactions of Opioid and Chemokine Receptors: Oligomerization of mu, kappa, and delta with CCR5 on Immune Cells

Author

Suzuki, Shunji, Chuang, Linda F., Yau, Peter, Doi, Roy H., and Chuang, Ronald Y.

Subjects

*OPIOID receptors, *CHEMOKINES, *CELL membranes

Abstract

Activation of opioid receptors by morphine was previously shown to specifically induce the expression of chemokine receptor CCR5, promoting simian AIDS virus entry and replication in immune cells. The present study was undertaken to determine whether these two structurally and functionally distinct G-protein-coupled receptors are in close proximity and form an oligomeric complex in the cell membrane so that the activation of one triggers the activity of the other. Both human CEM ×174 and monkey lymphocytes were used in this study and gave similar results. Immunoprecipitation experiments showed that CCR5, but not CD4 nor Na+/H+ exchanger, coprecipitates with all three subtypes (mu, delta, and kappa) of opioid receptors. A single protein band immunoreactive with antibodies against both the CCR5 and the opioid receptors was identified after electrophoresis on nondenaturing polyacrylamide gels. Chemical crosslinking experiments using glutaraldehyde or BS3 indicate that these receptors are closely situated on the cell membrane with an intermolecular distance less than 11.4A˚. Functional studies revealed that a combination treatment of cells with morphine, an agonist for mu, and MIP-1β, a ligand for CCR5, suppresses the inhibitory effect of MIP-1β and increases the stimulatory effect of morphine on CCR5 expression. These results suggest that oligomerization of chemokine receptor CCR5 and opioid receptors on the cell membrane of human or monkey lymphocytes may modulate receptor functions. [Copyright &y& Elsevier]

Published

2002

9. Chemokine receptor CCR5: polymorphism at protein level

Author

Suzuki, Shunji, Miyagi, Tomoko, Chuang, Linda F., Yau, Peter M., Doi, Roy H., and Chuang, Ronald Y.

Subjects

*CHEMOKINES, *MORPHINE, *ISOHORMONES

Abstract

Polymorphisms in chemokine receptor CCR5 genes have been implicated in HIV disease progression, resistance, or non-progressive infection. Multiple CCR5 transcripts and mRNA diversity have also been identified. This study presents evidence to show that two distinct forms of CCR5 protein, 62 and 42 kDa, are present in human lymphocytic cells and monkey peripheral blood mononuclear cells. The ratio of these two forms of CCR5 changes with cell growth. The 62 kDa CCR5 predominates if the electrophoresis sample buffer does not contain reducing agent. However, the 62 and the 42 kDa CCR5 are not interconvertible. Morphine sulfate induces the formation and expression of both forms of CCR5 whereas RANTES, MIP-1α or MIP-1β inhibits them. Localization studies indicate that the 62 kDa CCR5 resides mainly on the cell membrane and the 42 kDa CCR5 is present solely in the cytoplasm of the cells. [Copyright &y& Elsevier]

Published

2002

10. More about the Viking hypothesis of origin of the Δ32 mutation in the CCR5 gene conferring resistance to HIV-1 infection

Author

Lucotte, Gérard and Dieterlen, Florent

Subjects

*HIV infections, *GENES, *CHEMOKINES, *INFLAMMATORY mediators, *CELL receptors, *GENETIC mutation

Abstract

The chemokine receptor CCR5 constitutes the major coreceptor for the HIV-1, because a mutant allele of the CCR5 gene named Δ32 was shown to provide to homozygotes a strong resistance against infection. In the present study the frequency of the Δ32 allele was collected in 36 European populations and in Cyprus, and the highest allele frequencies were found in Nordic countries. We constructed an allele map of Δ32 frequencies in Europe; the map is in accordance to the Vikings hypothesis of the origin of the mutation and his dissemination during the eighth to the tenth centuries. [Copyright &y& Elsevier]

Published

2003