Your search keyword '"CCR5-Rezeptor"' showing total 5 results

1. Natural Cystatin C fragments inhibit GPR15-mediated HIV and SIV infection without interfering with GPR15L signaling

Author

Stefan Pöhlmann, Beatrice H. Hahn, Jan Münch, Konstantin M. J. Sparrer, Christina M. Stürzel, Klaus Seuwen, Rüdiger Gross, Ludger Ständker, Manuel Hayn, Timo Jacob, Andrea Blötz, Frank Kirchhoff, Wolf-Georg Forssmann, Solange Vidal, Mirja Harms, Armando Rodríguez, Sebastian Wiese, Christoph Jung, Nico Preising, and Miriam Kiene

Subjects

Kidney function tests, Chemokine, viruses, T-Lymphocytes, Simian Acquired Immunodeficiency Syndrome, chemokines, HIV Infections, medicine.disease_cause, Receptors, G-Protein-Coupled, Chemokine receptor, DDC 570 / Life sciences, Immunology and Inflammation, G protein-coupled receptors, cystatin C, immunodeficiency viruses, Kathepsine, Receptor, SMALL-MOLECULE INHIBITOR, Multidisciplinary, biology, virus diseases, Biological Sciences, CHEMOKINE RECEPTOR, CORECEPTOR, ENTRY, Receptors, Virus, Simian Immunodeficiency Virus, Chemokines, medicine.symptom, G proteins, Signal Transduction, Proteases, Receptors, Peptide, Inflammation, Virus, PROTEIN-COUPLED RECEPTORS, Viral entry, ddc:570, DIVERSE ROLES, medicine, Animals, Humans, ddc:610, Peptide library, HIV (Viruses), CCR5-Rezeptor, Simian immunodeficiency virus, Virus Internalization, Cystatins, Virology, Cystatin C, HIV-1, biology.protein, GPR15, DDC 610 / Medicine & health

Abstract

GPR15 is a G protein-coupled receptor (GPCR) proposed to play a role in mucosal immunity that also serves as a major entry cofactor for HIV-2 and simian immunodeficiency virus (SIV). To discover novel endogenous GPR15 ligands, we screened a hemofiltrate (HF)-derived peptide library for inhibitors of GPR15-mediated SIV infection. Our approach identified a C-terminal fragment of cystatin C (CysC95-146) that specifically inhibits GPR15-dependent HIV-1, HIV-2, and SIV infection. In contrast, GPR15L, the chemokine ligand of GPR15, failed to inhibit virus infection. We found that cystatin C fragments preventing GPR15-mediated viral entry do not interfere with GPR15L signaling and are generated by proteases activated at sites of inflammation. The antiretroviral activity of CysC95-146 was confirmed in primary CD4+ T cells and is conserved in simian hosts of SIV infection. Thus, we identified a potent endogenous inhibitor of GPR15-mediated HIV and SIV infection that does not interfere with the physiological function of this GPCR., publishedVersion

Published

2020

2. Establishing the interaction between the CC chemokine ligand 5 and the receptors CCR1 and CCR5

Author

Kramp, Birgit K. and Koenen, Robert Ryan

Subjects

Wechselwirkung, CCL5, %22">Ligand , virus diseases, Interaktion, CCR5-Rezeptor, später, stomatognathic diseases, RANTES, stomatognathic system, Biowissenschaften, Biologie, Chemokine, ddc:570, CCR1, Chemokininteraktion

Abstract

Chemokines are important mediators and regulators of leukocyte trafficking, therefore, they play a crucial role in the development of inflammatory diseases. CCL5 or RANTES (regulated upon activation, normal T cell expressed and secreted) is a chemokine of relevance to many diseases. Moreover, CCL5-induced monocyte adhesion to inflamed endothelium was shown to be improved in the presence of CXCL4 (Platelet Factor 4). Since this synergy could be attributed to heterodimer formation, the first section of the present study surveys the structural interaction of CCL5 with CXCL4. The interaction was monitored employing the 15N-1H heteronuclear single quantum coherence (HSQC) nuclear magnetic resonance (NMR) technique. For this purpose, 15N-enriched CCL5 was recombinantly expressed in E. coli and subsequently purified. In HSQC spectroscopy, chemical shift changes were mainly observed in the N-terminal residues, which pointed toward a CC-type rather than a CXC-type interaction. Furthermore, small peptide antagonists, inhibiting the CXCL4/CCL5 dimerization, were designed (CKEY2 and the mouse orthologue MKEY). To investigate their pharmacological potential, the influence of MKEY on leukocyte adhesion to activated endothelium was monitored using intravital microscopy. As a control Met-CCT5, a strong antagonist for CCR1 and CCR5, was cloned, expressed and purified employing FPLC and HPLC techniques. Leukocyte recruitment was severely impaired in the presence of MKEY, compared to a control peptide (sMKEY) and in a similar range of Met-CCL5 which encourages the assumption that the synergy is mediated via the receptors CCR1 and/or CCR5. Despite all similarities, CCR1 and CCR5 were shown to mediate distinct functions when bound to CCL5, CCR1 rather mediates arrest and CCR5 appears to be more responsible for transendothelial migration. To establish which domains are important for this functional selectivity, we constructed different CCR5 variants with the distinct extracellular regions of CCR1. These chimeras were stably expressed in L1.2 and HEK293 cells and we investigated their function in response to CCL5, different CCL5 mutants, or together with CXCL4 using chemotaxis and cell arrest assays under laminar flow. First of all, CCL5, CCL5 40s and CCL5-E66A were recombinantly expressed and purified employing FPLC and HPLC techniques. By implementing CCL5 mutants (e.g. CCL5-E66A) with oligomerization defects in laminar flow assays, we were able to show that all receptor variants require oligomerization of CCL5 in order to function properly. In addition, our results reveal that the 40S loop of CCL5 is important for both the CCR1- and CCR5-mediated cell arrest. The 50s loop of CCL5, however, appeared to have a strong preference for CCR5 in inducing cell arrest, since CCR1 responded normal towards CCL5 50s and CCR5 being non-responsive. When the N-terminal domain of CCR5 was exchanged for that of CCR1, the resulting chimera was fully responsive towards CCL5 50s, suggesting that the N-terminal region of CCR1 interacts with the 50s domain of CCR5. The synergistic effect of CXCL4 on CCL5 induced cell arrest was observed in cells exclusively expressing CCR1 when compared to cells expressing CCR5. When the third extracellular loop of CCR1 was engineered into CCR5, the resulting chimeric receptor showed a significant response to the CXCL4/CCL5 heterocomplex, compared to CCL5 alone. These results were confirmed by constructing CCR1-based reverse chimeras for the N-terminal domain and the third extracellular loop. Furthermore we could show the heterodimerization of CCR1 and CCR5 and the synergy of the CXCL4/CCL5 complex is in THP-1 cells mediated via Gαi. In conclusion these results indicate that the extracellular regions of CCR1 and CCR5 have distinct and defined functions in leukocyte recruitment in response to CCL5. In the third section of this thesis the role of the sialyltransferase ST3Gal-IV on CCL5 receptor interaction was investigated, by using neutrophils and monocytes isolated from ST3Gal-IV deficient and from control mice in functional assays in vitro. The results indicate that the addition of sialic acids to the terminal portions of the N- or O-linked sugar chains of the corresponding receptors of CCL5 is of a minor importance for receptor binding and activation, since the cells similarly mobilize calcium upon stimulation with CCL5. Whereas, the adhesion of neutrophils and monocytes from ST3Gal-IV-/- was significant diminished. Taken together the results obtained here rather support the importance of ST3Gal-IV on the generation of functional selectins, which is in line with previous publications.

Published

2013

3. HIV gene therapy using zinc finger nucleases (ZFNs) and transcription activator-like effector nucleases (TALENs)

Author

Schmidt, Kerstin and Schmidt, Kerstin

Abstract

HIV ist nach wie vor unheilbar. Eine vielversprechende Alternative ist HIV Gentherapie mittels Designernukleasen, wie Zinkfingernukleasen (ZFN) und Transcription activator-like effector Nukleasen (TALEN), die das CCR5 Gen zerstören. Eine Möglichkeit, um die Anwendung für Patienten mit CXCR4 -tropen Virus zu erweitern, wäre das Einbringen eines membranverankerten Fusioninhibitors (maC46) in das zerstörte CCR5 Gen. Die Zerstörung des CCR5 Gens konnte in verschiedenen Zelllinien für ZFN und TALEN gezeigt werden. Die Integration von maC46 in den CCR5 Lokus wurde durch einen adenoviralen Vektor in T Zellen gezeigt. Genmodifizierte Zellen zeigten eine reduzierte CCR5 Expression und eine reduzierte Viruslast nach Infektion mit einem CCR5-tropen Virus. Da nur eine sehr geringe Menge an Zellen genmodifiziert war, konnte keine Selektion von maC46 genmodifizierten Zellen nachgewiesen werden. Außerdem wurde das Risiko einer möglichen Stammzelltherapie mit den CCR5 ZFN untersucht. In dem hier beschriebenen „worst case“ Genotoxizitätsmodel wurden die humanen CCR5 ZFN durch lentiviralen Gentransfer stabil in murinen Stammzellen exprimiert. Die erste Kohorte, mit einer geringeren Vektor Dosis, war unauffällig. Die zweite Kohorte, behandelt mit einer höheren Vektor Dosis, entwickelte das Myelodysplastische Syndrom. Die lentiviralen Integrationsstellen waren für beide Kohorten unauffällig. Das hier beschriebene Krankheitsbild könnte durch unkontrollierte ZFN Aktivität im murinen Genom und daraus folgender genomischer Instabilität entstanden sein. Schlussfolgernd wurde die maximal mögliche Dosis an ZFN in Stammzellen erreicht, die weitaus höher ist, als die in der Klinik bei transientem Gentransfer verwendete Menge. Folglich sind ZFN eine sichere Möglichkeit für HIV Gentherapie., Although a broad panel of antiviral drugs has become available for the therapy of HIV infection, treatment is not curative. HIV gene therapy using designer nucleases, such as zinc finger nucleases (ZFNs) and Transcription activator-like effector nucleases (TALENs) that disrupt the CCR5 gene are a promising tool. To broaden the application for patients harboring CXCR4 tropic viruses, a targeted knock in of an antiviral gene into the disrupted CCR5 gene, would contribute to an overall antiviral effect. The antiviral gene used here was the membrane anchored C46 (maC46). CCR5 knock out was achieved in different cell lines using ZFNs and TALENs and targeted integration of the maC46 peptide could be established in a T cell line for ZFNs upon adenoviral delivery. ZFN modified cells showed a reduced CCR5 receptor expression and a reduced viral load upon CCR5 tropic HIV-1 challenge. Since only low gene marking was achieved no selection of maC46 expressing cells could be shown. In the second part of this work the risk of a potential hematopoietic stem cell (HSC) therapy with the CCR5 ZFNs was investigated. In the here described “worst case” genotoxicity mouse model the CCR5 ZFNs were constitutively expressed in murine HSC upon lentiviral delivery. Two cohorts, treated with the human CCR5 ZFN were analyzed. The low dose cohort stayed healthy, whereas the high dose cohort developed signs of myelodysplastic syndrome. Lentiviral integration sites were similar in both cohorts and not responsible for disease development in the high dose cohort. Off target activity of the ZFNs probably led to genome instability and the onset of the disease. In conclusion, the maximal tolerated dose was established for the CCR5 ZFNs. This dosage is higher than what would be expected in a clinical setting for HSC cell therapy, where ZFN will only be expressed transiently, making ZFNs a possible therapy for HIV infected patients., by Kerstin Schmidt, Abweichender Titel laut Übersetzung der Verfasserin/des Verfassers, Innsbruck, Med. Univ., Diss., 2014

Published

2014

4. Genetische Assoziationsstudien der immunologisch relevanten Gene CCR5, CX3CR1 und RANTES zur klinischen Risikostratifizierung von Patienten mit chronischer Hepatitis C

Author

Werth, Alexa and Rossaint, Rolf

Subjects

RANTES, haplotype, Risikostratifizierung, Medizin, RFLP, ddc:610, risk stratification, CCR5-Rezeptor, Hepatitis C, Haplotyp, Polymerase-Kettenreaktion

Abstract

Hepatitis C represents an inflammtion of the liver, which is influenced by a variety of epidemological and viral factors, as well as genetical traits of the host. This study examined the influence and impact of genetical variations of chemokine receptors such as CCR 5 and CX3CR1 and the chemokine RANTES on chronic hepatitis C. The polymorphisms of the CC-chemokinereceptors delta32 (CCR5 delta32), the combined SNPs CX3CR1 V249I and T280M, as well as analysis of the haplotype of the RANTES gene were evaluated and correlated with chemical and histological parameters to reveal a potential influence on an antiviral therapy for chronic hepatitis C. A total of 330 patients suffering from chronic hepatitis C of two independent groups from the university hospital Aachen and Berlin and a control group, consisiting of 152 age- and gender-matched hepatitis C virus negative individuals with a similar risk of exposition, were included in this study. The results of this study revealed that:(1) None of the tested SNPs was associated with an increased susceptibility towards an infection with hepatitis C. Analysis of the haplotypes of the RANTES gene also showed no difference between the study and control groups. (2) Analysis of the CCR5 delta32-deletion polymorphisms showed no significant difference between HCV-RNA viral load, liver enzyme profile or fibrosis score in regard to presence or absence of the polymorphe CCR5 delta32-alleles. A higher level of inflammation was found in the liver biopsies of the patient group of the University Hospital Aachen and a reduced response to the medical therapy of the patients of the Berlin group in the presence of the CCR5 delta32-mutation. However, these findings could not be confirmed by studying the other patient group of Aachen or Berlin, respectively, neither when analyzing the two combined groups of patients.(3) The CX3CR1 249I-allel was found to be associated with a higher HCV-RNA viral load and a higher degree of fibrosis of the liver biopsies. This finding was confirmed in the combined analysis of the SNPs CX3CR1 V249I and T280M.(4) Analysis of the RANTES gene identified four frequent haplotypes. RANTES-haplotypes, which carry the RANTES Int 1.1 C and the 3' 222 C- allel were found in a significantly higher number among patients with a negative response to therapy. This finding was also confirmed for patients with the HCV-genotype 1+4. These results suggest that the RANTES-haplotypes might contribute to the complex interaction between the hepatitis C virus and the polygenic determined immune response of the patient receiving antiviral therapy. The results of this study underline the importance and influence of chemokines and their receptors on the progress of hepatitis C and will help to develop new therapeutic strategies against this devastating illness. However, further investigation including a larger number of individuals, as well as different study populations is necessary to confirm the findings of this study.

Published

2008

5. Über die Rolle der Chemokinrezeptoren bei der Migration von T-Helferzellen an den Ort des chirurgischen Traumas bzw. der lokalen Entzündung

Author

Adam, S. (Stephanie), Schwering, H. (Hans), and Universitäts- und Landesbibliothek Münster

Subjects

TH1-Helferzellen, chirurgisches Trauma, Immunregulation, Migration, Chemokinrezeptoren, CXCR3-Rezeptor, CCR5-Rezeptor, Medicine and health, ddc:610

Abstract

Lymphozyten-Subpopulationen wurden anhand ihrer CD-Oberflächenmarker und Chemokinrezeptoren untersucht. Die Untersuchungen wurden nach elektiven chirurgischen Eingriffen vergleichend im Vollblut und im peritonealen Drainagesekret vorgenommen. Die dargelegten Ergebnisse bestätigen eine lokale Zellrekrutierung von T-Helferzellen (CD3+/CD4+-Lymphozyten) am Ort des chirurgischen Trauma. Zur Rolle der Chemokinrezeptoren bei der Migration von T-Helferzellen konnte gezeigt werden, dass der Chemokinrezeptor CXCR3 von Bedeutung ist. Da dieser unter den T-Helferzellen im wesentlichen auf den TH1-Zellen exprimiert wird, kann man ihm eine Beteiligung am Abwanderungsprozess von TH1-Zellen aus dem peripheren Blut zum Ort des chirurgischen Traumas zuschreiben. Im Gegensatz dazu zeigt die Arbeit, dass der CCR5 Rezeptor bei den immunregulativen Mechanismen nach einer Operation keine Rolle zu spielen scheint.

Published

2004