Your search keyword '"Clynes, Raphael"' showing total 6 results

1. Receptor for advanced glycation end products: fundamental roles in the inflammatory response: winding the way to the pathogenesis of endothelial dysfunction and atherosclerosis.

Author

Ramasamy R, Yan SF, Herold K, Clynes R, and Schmidt AM

Subjects

Animals, Atherosclerosis etiology, Diabetes Mellitus, Type 1 etiology, Diabetes Mellitus, Type 1 physiopathology, Encephalomyelitis, Autoimmune, Experimental physiopathology, Humans, Receptor for Advanced Glycation End Products, Signal Transduction, Atherosclerosis physiopathology, Endothelium, Vascular physiopathology, Inflammation physiopathology, Receptors, Immunologic physiology

Abstract

The multiligand receptor for advanced glycation end products (RAGE) of the immunoglobulin superfamily is expressed on multiple cell types implicated in the immune-inflammatory response and in atherosclerosis. Multiple studies have elucidated that ligand-RAGE interaction on cells, such as monocytes, macrophages, and endothelial cells, mediates cellular migration and upregulation of proinflammatory and prothrombotic molecules. In addition, recent studies reveal definitive rules for RAGE in effective T lymphocyte priming in vivo. RAGE ligand AGEs may be formed in diverse settings; although AGEs are especially generated in hyperglycemia, their production in settings characterized by oxidative stress and inflammation suggests that these species, in part via RAGE, may contribute to the pathogenesis of atherosclerosis. In murine models of atherosclerosis, vascular inflammation is a key factor and one which is augmented, in parallel with even further increases in RAGE ligands, in diabetic macrovessels. The findings that antagonism and genetic disruption of RAGE in atherosclerosis-susceptible mice strikingly reduces vascular inflammation and atherosclerotic lesion area and complexity link RAGE intimately to these processes and suggest that RAGE is a logical target for therapeutic intervention in aberrant inflammatory mechanisms and in atherosclerosis.

Published

2008

2. Receptor for AGE (RAGE): weaving tangled webs within the inflammatory response.

Author

Clynes R, Moser B, Yan SF, Ramasamy R, Herold K, and Schmidt AM

Subjects

Animals, Humans, Ligands, Receptor for Advanced Glycation End Products, Stress, Physiological metabolism, Wound Healing, Inflammation metabolism, Receptors, Immunologic metabolism

Abstract

The family of RAGE ligands, including Advanced Glycation Endproducts (AGEs), S100/calgranulins, High Mobility Group Box-1 (HMGB1) and amyloid beta peptide (Abeta) and beta-sheet fibrils are highly enriched in immune and inflammatory foci. In parallel, upregulation of Receptor for AGE (RAGE) is noted in diverse forms of inflammation and autoimmunity, based on experiments examining human tissues as well as animal models. Indeed, prior to the demonstration that S100/calgranulins were signal transduction ligands of RAGE, these molecules were considered "biomarkers" of disease and disease activity in disorders such as colitis and arthritis. Premiere roles for RAGE in advancing cellular migration implicate this receptor in targeting immune cells to vulnerable foci. Once engaged, ligand-RAGE interaction in inflammatory and vascular cells amplifies upregulation of inflammatory cytokines, adhesion molecules and matrix metalloproteinases (MMPs). Discerning the primal versus chronic injury-provoking roles for this ligand-receptor interaction is a challenge in delineating the functions of the ligand/RAGE axis. As RAGE is expressed by many of the key cell types linked integrally to the immune response, we propose that the sites and time course of ligand-RAGE stimulation determine the phenotype produced by this axis. Ultimately, drawing the fine line between antagonism versus stimulation of the receptor in health and disease will depend on the full characterization of RAGE in repair versus injury.

Published

2007

3. Receptor for advanced glycation end products (RAGE) in a dash to the rescue: inflammatory signals gone awry in the primal response to stress.

Author

Herold K, Moser B, Chen Y, Zeng S, Yan SF, Ramasamy R, Emond J, Clynes R, and Schmidt AM

Subjects

Animals, Humans, Models, Immunological, Receptor for Advanced Glycation End Products, Signal Transduction, Inflammation metabolism, Inflammation pathology, Receptors, Immunologic metabolism, Stress, Physiological metabolism

Abstract

The multiligand receptor for advanced glycation end products (RAGE) of the Ig superfamily transduces the biological impact of discrete families of ligands, including advanced glycation end products, certain members of the S100/calgranulin family, high mobility group box-1, Mac-1 (alpha(M)beta(2), CD11b/CD18), and amyloid-beta peptide and beta-sheet fibrils. Although structurally dissimilar, at least at the monomeric level, recent evidence suggests that oligomeric forms of these RAGE ligands may be especially apt to activate the receptor and up-regulate a program of inflammatory and tissue injury-provoking genes. The challenge in probing the biology of RAGE and its impact in acute responses to stress and the potential development of chronic disease is to draw the line between mechanisms that evoke repair versus those that sustain inflammation and tissue damage. In this review, we suggest the concept that the ligands of RAGE comprise a primal program in the acute response to stress. When up-regulated in environments laden with oxidative stress, inflammation, innate aging, or high glucose, as examples, the function of these ligand families may be transformed from ones linked to rapid repair to those that drive chronic disease. Identification of the threshold beyond which ligands of RAGE mediate repair versus injury is a central component in delineating optimal strategies to target RAGE in the clinic.

Published

2007

4. The Receptor for Advanced Glycation End Products (RAGE) Affects T Cell Differentiation in OVA Induced Asthma.

Author

Akirav, Eitan M., Henegariu, Octavian, Preston-Hurlburt, Paula, Schmidt, Ann Marie, Clynes, Raphael, and Herold, Kevan C.

Subjects

T cell differentiation, OVALBUMINS, ASTHMA, IMMUNE response, LABORATORY mice, CYTOKINES, COMPARATIVE studies

Abstract

The receptor for glycation end products (RAGE) has been previously implicated in shaping the adaptive immune response. RAGE is expressed in T cells after activation and constitutively in T cells from patients with diabetes. The effects of RAGE on adaptive immune responses are not clear: Previous reports show that RAGE blockade affects Th1 responses. To clarify the role of RAGE in adaptive immune responses and the mechanisms of its effects, we examined whether RAGE plays a role in T cell activation in a Th2 response involving ovalbumin (OVA)-induced asthma in mice. WT and RAGE deficient wild-type and OT-II mice, expressing a T cell receptor specific for OVA, were immunized intranasally with OVA. Lung cellular infiltration and T cell responses were analyzed by immunostaining, FACS, and multiplex bead analyses for cytokines. RAGE deficient mice showed reduced cellular infiltration in the bronchial alveolar lavage fluid and impaired T cell activation in the mediastinal lymph nodes when compared with WT mice. In addition, RAGE deficiency resulted in reduced OT-II T cell infiltration of the lung and impaired IFNγ and IL-5 production when compared with WT mice and reduced infiltration when transferred into WT hosts. When cultured under conditions favoring the differentiation of T cells subsets, RAGE deficient T cells showed reduced production of IFNγ but increased production of IL-17. Our data show a stimulatory role for RAGE in T activation in OVA-induced asthma. This role is largely mediated by the effects of RAGE on T cell proliferation and differentiation. These findings suggest that RAGE may play a regulatory role in T cell responses following immune activation. [ABSTRACT FROM AUTHOR]

Published

2014

5. ILT3.Fc inhibits the production of exosomes containing inflammatory microRNA in supernatants of alloactivated T cells.

Author

Xu, Zheng, Ho, Sophey, Chang, Chih-Chao, Liu, Zhuoru, Li, Muyang, Vasilescu, Elena R., Clynes, Raphael A., Vlad, George, and Suciu-Foca, Nicole

Subjects

*MICRORNA, *T cells, *EXOSOMES, *CELL culture, *INFLAMMATION, *IMMUNOREGULATION

Abstract

Immune activation needs to be tightly regulated to control immune-mediated tissue damage. Inhibitory pathways serve to terminate an immune response and resolve inflammation. Persistent exposure to antigens can drive development of adaptive regulatory cells. Similarly exposure of activated T cells to the recombinant ILT3-Fc molecule during priming triggers the differentiation of CD8 T suppressor cells and the induction of CD4 T helper anergy. Ts express high levels of immunoregulatory signature genes together with low levels of microRNA which control their function. Analysis of microRNA contained by exosomes from cultures in which T cells were alloactivated in the presence or absence of ILT3.Fc, demonstrated that this agent inhibits the release of inflammatory microRNA. The source of such inflammatory microRNA was found to reside in alloactivated CD4 T cells, since exosomes from MLC primed CD4 T cells were shown to diminish the suppressive activity of ILT3-Fc-induced CD8+ Ts at high effector to suppressor T cell ratios. This indicates that inflammatory exosomes can swing the balance between effector and regulatory T cells in favor of immunity. These data suggest that isolation and characterization of micro-RNA containing exosomes in patients' circulation may be of use for treatment, prevention and monitoring of immune activation. [ABSTRACT FROM AUTHOR]

Published

2014

6. 1011-LBP: ILT3Fc inhibits the inflammatory effect of exosomes from primary MLC.

Author

Xu, Zheng, Chang, Chih-Chao, Ho, Sophey, Liu, Zhuoru, Vlad, George, Cortesini, Raffaello, Clynes, Raphael A., and Suciu-Foca, Nicole

Subjects

*INFLAMMATION, *EXOSOMES, *CELL communication, *MICRORNA, *SYNAPSES, *GENE expression

Abstract

Aim: Exosomes may contribute to cell-cell communication at the level of immunological synapses or at a distance, by delivering mRNA and miRNA modifying the recipient cell protein production and gene expression. The present study aims to determine whether the effect of ILT3Fc on allostimulated CD8 T cells is accompanied by changes in the miRNA content of exosomes generated during allostimulation. Methods: Exosomes were isolated from culture supernatants of MLC in which CD3 T cells had been stimulated with allogeneic APC in the presence or absence of ILT3Fc. The identity and relative quantity of the exosomal miRNA content was determined by RT-PCR. The inhibitory or inflammatory properties of these exosomes were evaluated by 24h pretreatment of sorted CD8 Ts from MLC containing ILT3Fc. The CD8 T cells were then tested for the effect on the proliferation of naive, syngeneic T cells primed in response to the same stimulating APC. Results: CD8 Ts primed in the presence of ILT3Fc inhibit syngeneic CD4 T cell responses by >80%. When CD8 Ts are pretreated with inflammatory exosomes, and are used in MLC at lower than 1:1 ratios to respoding Th cells, they lose inhibitory activity. These exosomes contain miRNA-21, -30b, -146a, -155, -395, and Let7a, known to be increased in T cells during activation. In contrast, exosomes obtained from T cells primed in the presence of ILT3Fc, do not abolish CD8 Ts inhibitory potential, suggesting that ILT3Fc blocks the release into the medium or alters the RNA content of inflammatory exosomes. Conclusions: Micro RNA contained by exosomes released from alloactivated T cells enhance T helper activity even in the presence of T suppressor cells. This suggests the potential use of exosomal inflammatory miRNA as a monitor of cellular immune responses against the graft. Furthermore, such exosomes may be of use in eliciting immune T cell responses against tumors or microbial agents. [Copyright &y& Elsevier]

Published

2014