Your search keyword '"Cayrol, Romain A."' showing total 10 results

1. CCDC88B interacts with RASAL3 and ARHGEF2 and regulates dendritic cell function in neuroinflammation and colitis.

Author

Olivier, Jean-Frederic, Langlais, David, Jeyakumar, Thiviya, Polyak, Maria J., Galarneau, Luc, Cayrol, Romain, Jiang, Hua, Molloy, Kelly R., Xu, Guoyue, Suzuki, Harumi, LaCava, John, Gros, Philippe, and Fodil, Nassima

Subjects

GUANINE nucleotide exchange factors, CELL physiology, DENDRITIC cells, COLITIS, HUMAN gene mapping

Abstract

CCDC88B is a risk factor for several chronic inflammatory diseases in humans and its inactivation causes a migratory defect in DCs in mice. CCDC88B belongs to a family of cytoskeleton-associated scaffold proteins that feature protein:protein interaction domains. Here, we identified the Rho/Rac Guanine Nucleotide Exchange Factor 2 (ARHGEF2) and the RAS Protein Activator Like 3 (RASAL3) as CCDC88B physical and functional interactors. Mice defective in Arhgef2 or Rasal3 show dampened neuroinflammation, and display altered cellular response and susceptibility to colitis; ARHGEF2 maps to a human Chromosome 1 locus associated with susceptibility to IBD. Arhgef2 and Rasal3 mutant DCs show altered migration and motility in vitro, causing either reduced (Arhgef2) or enhanced (Rasal3) migratory properties. The CCDC88B/RASAL3/ARHGEF2 complex appears to regulate DCs migration by modulating activation of RHOA, with ARHGEF2 and RASAL3 acting in opposite regulatory fashions, providing a molecular mechanism for the involvement of these proteins in DCs immune functions. CCDC88B physically interacts with ARHGEF2 and RASAL3; defective mice show dampened neuroinflammation, altered susceptibility to colitis and altered DCs motility by modulating RHOA, with ARHGEF2 and RASAL3 acting in opposite regulatory fashions. [ABSTRACT FROM AUTHOR]

Published

2024

2. Molecular imaging of a fluorescent antibody against epidermal growth factor receptor detects high-grade glioma.

Author

Zhou, Quan, Vega Leonel, Johana C. M., Santoso, Michelle Rai, Wilson, Christy, van den Berg, Nynke S., Chan, Carmel T., Aryal, Muna, Vogel, Hannes, Cayrol, Romain, Mandella, Michael J., Schonig, Frank, Lu, Guolan, Gambhir, Sanjiv S., Moseley, Michael E., Rosenthal, Eben L., and Grant, Gerald A.

Subjects

FLUORESCENT antibody technique, EPIDERMAL growth factor receptors, GLIOMAS, BIOMARKERS, PROTEIN expression

Abstract

The prognosis for high-grade glioma (HGG) remains dismal and the extent of resection correlates with overall survival and progression free disease. Epidermal growth factor receptor (EGFR) is a biomarker heterogeneously expressed in HGG. We assessed the feasibility of detecting HGG using near-infrared fluorescent antibody targeting EGFR. Mice bearing orthotopic HGG xenografts with modest EGFR expression were imaged in vivo after systemic panitumumab-IRDye800 injection to assess its tumor-specific uptake macroscopically over 14 days, and microscopically ex vivo. EGFR immunohistochemical staining of 59 tumor specimens from 35 HGG patients was scored by pathologists and expression levels were compared to that of mouse xenografts. Intratumoral distribution of panitumumab-IRDye800 correlated with near-infrared fluorescence and EGFR expression. Fluorescence distinguished tumor cells with 90% specificity and 82.5% sensitivity. Target-to-background ratios peaked at 14 h post panitumumab-IRDye800 infusion, reaching 19.5 in vivo and 7.6 ex vivo, respectively. Equivalent or higher EGFR protein expression compared to the mouse xenografts was present in 77.1% HGG patients. Age, combined with IDH-wildtype cerebral tumor, was predictive of greater EGFR protein expression in human tumors. Tumor specific uptake of panitumumab-IRDye800 provided remarkable contrast and a flexible imaging window for fluorescence-guided identification of HGGs despite modest EGFR expression. [ABSTRACT FROM AUTHOR]

Published

2021

3. Inactivation of Interferon Regulatory Factor 1 Causes Susceptibility to Colitis-Associated Colorectal Cancer.

Author

Jeyakumar, Thiviya, Fodil, Nassima, Van Der Kraak, Lauren, Meunier, Charles, Cayrol, Romain, McGregor, Kevin, Langlais, David, Greenwood, Celia M. T., Beauchemin, Nicole, and Gros, Philippe

Subjects

INTERFERON regulatory factors, DISEASE susceptibility, COLITIS, COLON cancer, DEXTRAN sulfate

Abstract

The mechanisms linking chronic inflammation of the gut (IBD) and increased colorectal cancer susceptibility are poorly understood. IBD risk is influenced by genetic factors, including the IBD5 locus (human 5q31), that harbors the IRF1 gene. A cause-to-effect relationship between chronic inflammation and colorectal cancer, and a possible role of IRF1 were studied in Irf1-/- mice in a model of colitis-associated colorectal cancer (CA-CRC) induced by azoxymethane and dextran sulfate. Loss of Irf1 causes hyper-susceptibility to CA-CRC, with early onset and increased number of tumors leading to rapid lethality. Transcript profiling (RNA-seq) and immunostaining of colons shows heightened inflammation and enhanced enterocyte proliferation in Irf1−/− mutants, prior to appearance of tumors. Considerable infiltration of leukocytes is seen in Irf1−/− colons at this early stage, and is composed primarily of proinflammatory Gr1+ Cd11b+ myeloid cells and other granulocytes, as well as CD4+ lymphoid cells. Differential susceptibility to CA-CRC of Irf1−/− vs. B6 controls is fully transferable through hematopoietic cells as observed in bone marrow chimera studies. Transcript signatures seen in Irf1−/− mice in response to AOM/DSS are enriched in clinical specimens from patients with IBD and with colorectal cancer. In addition, IRF1 expression in the colon is significantly decreased in late stage colorectal cancer (stages 3, 4) and is associated with poorer prognosis. This suggests that partial or complete loss of IRF1 expression alters the type, number, and function of immune cells in situ during chronic inflammation, possibly via the creation of a tumor-promoting environment. [ABSTRACT FROM AUTHOR]

Published

2019

4. Intestinal infection triggers Parkinson's disease-like symptoms in Pink1−/− mice.

Author

Matheoud, Diana, Cannon, Tyler, Voisin, Aurore, Penttinen, Anna-Maija, Ramet, Lauriane, Fahmy, Ahmed M., Ducrot, Charles, Laplante, Annie, Bourque, Marie-Josée, Zhu, Lei, Cayrol, Romain, Le Campion, Armelle, McBride, Heidi M., Gruenheid, Samantha, Trudeau, Louis-Eric, and Desjardins, Michel

Abstract

Parkinson's disease is a neurodegenerative disorder with motor symptoms linked to the loss of dopaminergic neurons in the substantia nigra compacta. Although the mechanisms that trigger the loss of dopaminergic neurons are unclear, mitochondrial dysfunction and inflammation are thought to have key roles1,2. An early-onset form of Parkinson's disease is associated with mutations in the PINK1 kinase and PRKN ubiquitin ligase genes3. PINK1 and Parkin (encoded by PRKN) are involved in the clearance of damaged mitochondria in cultured cells4, but recent evidence obtained using knockout and knockin mouse models have led to contradictory results regarding the contributions of PINK1 and Parkin to mitophagy in vivo5–8. It has previously been shown that PINK1 and Parkin have a key role in adaptive immunity by repressing presentation of mitochondrial antigens9, which suggests that autoimmune mechanisms participate in the aetiology of Parkinson's disease. Here we show that intestinal infection with Gram-negative bacteria in Pink1−/− mice engages mitochondrial antigen presentation and autoimmune mechanisms that elicit the establishment of cytotoxic mitochondria-specific CD8+ T cells in the periphery and in the brain. Notably, these mice show a sharp decrease in the density of dopaminergic axonal varicosities in the striatum and are affected by motor impairment that is reversed after treatment with l-DOPA. These data support the idea that PINK1 is a repressor of the immune system, and provide a pathophysiological model in which intestinal infection acts as a triggering event in Parkinson's disease, which highlights the relevance of the gut–brain axis in the disease10. In mice lacking PINK1, bacterial infection in the intestine results in mitochondrial antigen presentation and generation of CD8+ T cells, and infected mice develop motor impairments, suggesting that PINK1 suppresses autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2019

5. Single-cell analysis reveals T cell infiltration in old neurogenic niches.

Author

Dulken, Ben W., Buckley, Matthew T., Navarro Negredo, Paloma, Saligrama, Naresha, Cayrol, Romain, Leeman, Dena S., George, Benson M., Boutet, Stéphane C., Hebestreit, Katja, Pluvinage, John V., Wyss-Coray, Tony, Weissman, Irving L., Vogel, Hannes, Davis, Mark M., and Brunet, Anne

Abstract

The mammalian brain contains neurogenic niches that comprise neural stem cells and other cell types. Neurogenic niches become less functional with age, but how they change during ageing remains unclear. Here we perform single-cell RNA sequencing of young and old neurogenic niches in mice. The analysis of 14,685 single-cell transcriptomes reveals a decrease in activated neural stem cells, changes in endothelial cells and microglia, and an infiltration of T cells in old neurogenic niches. T cells in old brains are clonally expanded and are generally distinct from those in old blood, which suggests that they may experience specific antigens. T cells in old brains also express interferon-γ, and the subset of neural stem cells that has a high interferon response shows decreased proliferation in vivo. We find that T cells can inhibit the proliferation of neural stem cells in co-cultures and in vivo, in part by secreting interferon-γ. Our study reveals an interaction between T cells and neural stem cells in old brains, opening potential avenues through which to counteract age-related decline in brain function. Single-cell transcriptomic analysis of neurogenic niches in young and old mice reveals that T cells infiltrate the neurogenic niches of old mice and inhibit the proliferation of neural stem cells, in part through expression of interferon-γ. [ABSTRACT FROM AUTHOR]

Published

2019

6. CCDC88B is required for pathogenesis of inflammatory bowel disease.

Author

Fodil, Nassima, Moradin, Neda, Leung, Vicki, Olivier, Jean-Frederic, Radovanovic, Irena, Jeyakumar, Thiviya, Flores Molina, Manuel, McFarquhar, Ashley, Cayrol, Romain, Bozec, Dominique, Shoukry, Naglaa H., Michiaki Kubo, Dimitrieva, Julia, Louis, Edouard, Theatre, Emilie, Dahan, Stephanie, Yukihide Momozawa, Georges, Michel, Yeretssian, Garabet, and Gros, Philippe

Abstract

Inflammatory bowel disease (IBD) involves interaction between host genetic factors and environmental triggers. CCDC88B maps within one IBD risk locus on human chromosome 11q13. Here we show that CCDC88B protein increases in the colon during intestinal injury, concomitant with an influx of CCDC88B+lymphoid and myeloid cells. Loss of Ccdc88b protects against DSS-induced colitis, with fewer pathological lesions and reduced intestinal inflammation in Ccdc88b-deficient mice. In a T cell transfer model of colitis, Ccdc88b mutant CD4+ T cells do not induce colitis in immunocompromised hosts. Expression of human CCDC88B RNA and protein is higher in IBD patient colons than in control colon tissue. In human CD14+ myeloid cells, CCDC88B is regulated by cis-acting variants. In a cohort of patients with Crohn’s disease, CCDC88B expression correlates positively with disease risk. These findings suggest that CCDC88B has a critical function in colon inflammation and the pathogenesis of IBD. [ABSTRACT FROM AUTHOR]

Published

2017

7. Isolation of Human Brain Endothelial Cells and Characterization of Lipid Raft-Associated Proteins by Mass Spectroscopy.

Author

Cayrol, Romain, Haqqani, Arsalan S., Ifergan, Igal, Dodelet-Devillers, Aurore, and Prat, Alexandre

Published

2011

8. Functions of lipid raft membrane microdomains at the blood–brain barrier.

Author

Dodelet-Devillers, Aurore, Cayrol, Romain, van Horssen, Jack, Haqqani, Arsalan S., de Vries, Helga E., Engelhardt, Britta, Greenwood, John, and Prat, Alexandre

Subjects

*BILAYER lipid membranes, *NERVOUS system blood-vessels, *CENTRAL nervous system, *TIGHT junctions, *CELL adhesion

Abstract

The blood–brain barrier (BBB) is a highly specialized structural and functional component of the central nervous system that separates the circulating blood from the brain and spinal cord parenchyma. Brain endothelial cells (BECs) that primarily constitute the BBB are tightly interconnected by multiprotein complexes, the adherens junctions and the tight junctions, thereby creating a highly restrictive cellular barrier. Lipid-enriched membrane microdomain compartmentalization is an inherent property of BECs and allows for the apicobasal polarity of brain endothelium, temporal and spatial coordination of cell signaling events, and actin remodeling. In this manuscript, we review the role of membrane microdomains, in particular lipid rafts, in the BBB under physiological conditions and during leukocyte transmigration/diapedesis. Furthermore, we propose a classification of endothelial membrane microdomains based on their function, or at least on the function ascribed to the molecules included in such heterogeneous rafts: (1) rafts associated with interendothelial junctions and adhesion of BECs to basal lamina ( scaffolding rafts); (2) rafts involved in immune cell adhesion and migration across brain endothelium ( adhesion rafts); (3) rafts associated with transendothelial transport of nutrients and ions ( transporter rafts). [ABSTRACT FROM AUTHOR]

Published

2009

9. Activated leukocyte cell adhesion molecule promotes leukocyte trafficking into the central nervous system.

Author

Cayrol, Romain, Wosik, Karolina, Berard, Jennifer L, Dodelet-Devillers, Aurore, Ifergan, Igal, Kebir, Hania, Haqqani, Arsalan S, Kreymborg, Katharina, Krug, Sebastian, Moumdjian, Robert, Bouthillier, Alain, Becher, Burkhard, Arbour, Nathalie, David, Samuel, Stanimirovic, Danica, and Prat, Alexandre

Abstract

Adhesion molecules of the immunoglobulin superfamily are crucial effectors of leukocyte trafficking into the central nervous system. Using a lipid raft-based proteomic approach, we identified ALCAM as an adhesion molecule involved in leukocyte migration across the blood-brain barrier (BBB). ALCAM expressed on BBB endothelium localized together with CD6 on leukocytes and with BBB endothelium transmigratory cups. ALCAM expression on BBB cells was upregulated in active multiple sclerosis and experimental autoimmune encephalomyelitis lesions. Moreover, ALCAM blockade restricted the transmigration of CD4+ lymphocytes and monocytes across BBB endothelium in vitro and in vivo and reduced the severity and delayed the time of onset of experimental autoimmune encephalomyelitis. Our findings indicate an important function for ALCAM in the recruitment of leukocytes into the brain and identify ALCAM as a potential target for the therapeutic dampening of neuroinflammation. [ABSTRACT FROM AUTHOR]

Published

2008

10. Human TH17 lymphocytes promote blood-brain barrier disruption and central nervous system inflammation.

Author

Kebir, Hania, Kreymborg, Katharina, Ifergan, Igal, Dodelet-Devillers, Aurore, Cayrol, Romain, Bernard, Monique, Giuliani, Fabrizio, Arbour, Nathalie, Becher, Burkhard, and Prat, Alexandre

Subjects

LYMPHOCYTES, MULTIPLE sclerosis, NERVOUS system blood-vessels, BRAIN blood-vessels, CENTRAL nervous system, DISEASES

Abstract

TH17 lymphocytes appear to be essential in the pathogenesis of numerous inflammatory diseases. We demonstrate here the expression of IL-17 and IL-22 receptors on blood-brain barrier endothelial cells (BBB-ECs) in multiple sclerosis lesions, and show that IL-17 and IL-22 disrupt BBB tight junctions in vitro and in vivo. Furthermore, TH17 lymphocytes transmigrate efficiently across BBB-ECs, highly express granzyme B, kill human neurons and promote central nervous system inflammation through CD4+ lymphocyte recruitment. [ABSTRACT FROM AUTHOR]

Published

2007