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464 results on '"Veillette, André"'

1. CD47 masks pro-phagocytic ligands in cis on tumor cells to suppress antitumor immunity

Author

Tang, Zhenghai, Zhong, Ming-Chao, Qian, Jin, Galindo, Cristian Camilo, Davidson, Dominique, Li, Jiaxin, Zhao, Yunlong, Hui, Enfu, and Veillette, André

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Humans, Antigens, Differentiation, CD47 Antigen, Ligands, Macrophages, Neoplasms, Phagocytosis, Tumor Escape, Animals, Mice, Biochemistry and cell biology
Abstract

Cancer cells often overexpress CD47, which triggers the inhibitory receptor SIRPα expressed on macrophages, to elude phagocytosis and antitumor immunity. Pharmacological blockade of CD47 or SIRPα is showing promise as anticancer therapy, although CD47 blockade has been associated with hematological toxicities that may reflect its broad expression pattern on normal cells. Here we found that, in addition to triggering SIRPα, CD47 suppressed phagocytosis by a SIRPα-independent mechanism. This mechanism prevented phagocytosis initiated by the pro-phagocytic ligand, SLAMF7, on tumor cells, due to a cis interaction between CD47 and SLAMF7. The CD47-SLAMF7 interaction was disrupted by CD47 blockade and by a first-in-class agonist SLAMF7 antibody, but not by SIRPα blockade, thereby promoting antitumor immunity. Hence, CD47 suppresses phagocytosis not only by engaging SIRPα, but also by masking cell-intrinsic pro-phagocytic ligands on tumor cells and knowledge of this mechanism may influence the decision between CD47 blockade or SIRPα blockade for therapeutic purposes.

Published
2023

5. TMEM16F Expressed in Kupffer Cells Regulates Liver Inflammation and Metabolism to Protect Against Listeria Monocytogenes.

Author

Tang, Jianlong, Song, Hua, Li, Shimin, Lam, Sin Man, Ping, Jieming, Yang, Mengyun, Li, Na, Chang, Teding, Yu, Ze, Liu, Weixiang, Lu, Yan, Zhu, Min, Tang, Zhaohui, Liu, Zheng, Guo, Yusong R., Shui, Guanghou, Veillette, André, Zeng, Zhutian, and Wu, Ning

Subjects
LIVER cells, KUPFFER cells, B cells, LISTERIOSIS, LISTERIA monocytogenes, T cells
Abstract

Infection by bacteria leads to tissue damage and inflammation, which need to be tightly controlled by host mechanisms to avoid deleterious consequences. It is previously reported that TMEM16F, a calcium‐activated lipid scramblase expressed in various immune cell types including T cells and neutrophils, is critical for the control of infection by bacterium Listeria monocytogenes (Lm) in vivo. This function correlated with the capacity of TMEM16F to repair the plasma membrane (PM) damage induced in T cells in vitro, by the Lm toxin listeriolysin O (LLO). However, whether the protective effect of TMEM16F on Lm infection in vivo is mediated by an impact in T cells, or in other cell types, is not determined. Herein, the immune cell types and mechanisms implicated in the protective effect of TMEM16F against Lm in vivo are elucidated. Cellular protective effects of TMEM16F correlated with its capacity of lipid scrambling and augment PM fluidity. Using cell type‐specific TMEM16F‐deficient mice, the indication is obtained that TMEM16F expressed in liver Kupffer cells (KCs), but not in T cells or B cells, is key for protection against Listeria in vivo. In the absence of TMEM16F, Listeria induced PM rupture and fragmentation of KCs in vivo. KC death associated with greater liver damage, inflammatory changes, and dysregulated liver metabolism. Overall, the results uncovered that TMEM16F expressed in Kupffer cells is crucial to protect the host against Listeria infection. This influence is associated with the capacity of Kupffer cell‐expressed TMEM16F to prevent excessive inflammation and abnormal liver metabolism. [ABSTRACT FROM AUTHOR]

Published
2024
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7. SLAMF7 is critical for phagocytosis of haematopoietic tumour cells via Mac-1 integrin

Author

Chen, Jun, Zhong, Ming-Chao, Guo, Huaijian, Davidson, Dominique, Mishel, Sabrin, Lu, Yan, Rhee, Inmoo, Pérez-Quintero, Luis-Alberto, Zhang, Shaohua, Cruz-Munoz, Mario-Ernesto, Wu, Ning, Vinh, Donald C, Sinha, Meenal, Calderon, Virginie, Lowell, Clifford A, Danska, Jayne S, and Veillette, André

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Cancer, Actins, Animals, Antigens, Differentiation, CD47 Antigen, Female, Hematologic Neoplasms, Humans, Macrophage-1 Antigen, Macrophages, Male, Mice, Mice, Knockout, Phagocytosis, Receptors, Immunologic, Signaling Lymphocytic Activation Molecule Family, General Science & Technology
Abstract

Cancer cells elude anti-tumour immunity through multiple mechanisms, including upregulated expression of ligands for inhibitory immune checkpoint receptors. Phagocytosis by macrophages plays a critical role in cancer control. Therapeutic blockade of signal regulatory protein (SIRP)-α, an inhibitory receptor on macrophages, or of its ligand CD47 expressed on tumour cells, improves tumour cell elimination in vitro and in vivo, suggesting that blockade of the SIRPα-CD47 checkpoint could be useful in treating human cancer. However, the pro-phagocytic receptor(s) responsible for tumour cell phagocytosis is(are) largely unknown. Here we find that macrophages are much more efficient at phagocytosis of haematopoietic tumour cells, compared with non-haematopoietic tumour cells, in response to SIRPα-CD47 blockade. Using a mouse lacking the signalling lymphocytic activation molecule (SLAM) family of homotypic haematopoietic cell-specific receptors, we determined that phagocytosis of haematopoietic tumour cells during SIRPα-CD47 blockade was strictly dependent on SLAM family receptors in vitro and in vivo. In both mouse and human cells, this function required a single SLAM family member, SLAMF7 (also known as CRACC, CS1, CD319), expressed on macrophages and tumour cell targets. In contrast to most SLAM receptor functions, SLAMF7-mediated phagocytosis was independent of signalling lymphocyte activation molecule-associated protein (SAP) adaptors. Instead, it depended on the ability of SLAMF7 to interact with integrin Mac-1 (refs 18, 19, 20) and utilize signals involving immunoreceptor tyrosine-based activation motifs. These findings elucidate the mechanism by which macrophages engulf and destroy haematopoietic tumour cells. They also reveal a novel SAP adaptor-independent function for a SLAM receptor. Lastly, they suggest that patients with tumours expressing SLAMF7 are more likely to respond to SIRPα-CD47 blockade therapy.

Published
2017

12. Two novel mutations in ZAP70 gene that result in human immunodeficiency

Author

Llamas-Guillén, Beatriz Adriana, Pastor, Nina, López-Herrera, Gabriela, González-Serrano, Maria Edith, Valenzuela-Vázquez, Lucero, Bravo-Adame, Maria Elena, Villanueva-Cabello, Tania Maria, Gaytán, Paul, Yañez, Jorge, Martinez-Duncker, Ivan, Ruiz-Fernández, Miguel, Veillette, André, Espinosa-Padilla, Sara Elva, and Cruz-Munoz, Mario Ernesto

Published
2017
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14. Data from Alternative Splicing of the Inhibitory Immune Checkpoint Receptor SLAMF6 Generates a Dominant Positive Form, Boosting T-cell Effector Functions

Author

Hajaj, Emma, primary, Zisman, Elad, primary, Tzaban, Shay, primary, Merims, Sharon, primary, Cohen, Jonathan, primary, Klein, Shiri, primary, Frankenburg, Shoshana, primary, Sade-Feldman, Moshe, primary, Tabach, Yuval, primary, Yizhak, Keren, primary, Navon, Ami, primary, Stepensky, Polina, primary, Hacohen, Nir, primary, Peretz, Tamar, primary, Veillette, André, primary, Karni, Rotem, primary, Eisenberg, Galit, primary, and Lotem, Michal, primary

Published
2023
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15. Supplementary Figures S1-5 from Alternative Splicing of the Inhibitory Immune Checkpoint Receptor SLAMF6 Generates a Dominant Positive Form, Boosting T-cell Effector Functions

Author

Hajaj, Emma, primary, Zisman, Elad, primary, Tzaban, Shay, primary, Merims, Sharon, primary, Cohen, Jonathan, primary, Klein, Shiri, primary, Frankenburg, Shoshana, primary, Sade-Feldman, Moshe, primary, Tabach, Yuval, primary, Yizhak, Keren, primary, Navon, Ami, primary, Stepensky, Polina, primary, Hacohen, Nir, primary, Peretz, Tamar, primary, Veillette, André, primary, Karni, Rotem, primary, Eisenberg, Galit, primary, and Lotem, Michal, primary

Published
2023
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16. Cis interactions between CD2 and its ligands on T cells are required for T cell activation

Author

Li, Bin, primary, Lu, Yan, additional, Zhong, Ming-Chao, additional, Qian, Jin, additional, Li, Rui, additional, Davidson, Dominique, additional, Tang, Zhenghai, additional, Zhu, Kaiwen, additional, Argenty, Jérémy, additional, de Peredo, Anne Gonzalez, additional, Malissen, Bernard, additional, Roncagalli, Romain, additional, and Veillette, André, additional

Published
2022
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20. When killers become thieves: Trogocytosed PD-1 inhibits NK cells in cancer

Author

Hasim, Mohamed S., primary, Marotel, Marie, additional, Hodgins, Jonathan J., additional, Vulpis, Elisabetta, additional, Makinson, Olivia J., additional, Asif, Sara, additional, Shih, Han-Yun, additional, Scheer, Amit K., additional, MacMillan, Olivia, additional, Alonso, Felipe G., additional, Burke, Kelly P., additional, Cook, David P., additional, Li, Rui, additional, Petrucci, Maria Teresa, additional, Santoni, Angela, additional, Fallon, Padraic G., additional, Sharpe, Arlene H., additional, Sciumè, Giuseppe, additional, Veillette, André, additional, Zingoni, Alessandra, additional, Gray, Douglas A., additional, McCurdy, Arleigh, additional, and Ardolino, Michele, additional

Published
2022
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31. CD47 masks pro-phagocytic ligands in cison tumor cells to suppress antitumor immunity

Author

Tang, Zhenghai, Zhong, Ming-Chao, Qian, Jin, Galindo, Cristian Camilo, Davidson, Dominique, Li, Jiaxin, Zhao, Yunlong, Hui, Enfu, and Veillette, André

Abstract

Cancer cells often overexpress CD47, which triggers the inhibitory receptor SIRPα expressed on macrophages, to elude phagocytosis and antitumor immunity. Pharmacological blockade of CD47 or SIRPα is showing promise as anticancer therapy, although CD47 blockade has been associated with hematological toxicities that may reflect its broad expression pattern on normal cells. Here we found that, in addition to triggering SIRPα, CD47 suppressed phagocytosis by a SIRPα-independent mechanism. This mechanism prevented phagocytosis initiated by the pro-phagocytic ligand, SLAMF7, on tumor cells, due to a cisinteraction between CD47 and SLAMF7. The CD47–SLAMF7 interaction was disrupted by CD47 blockade and by a first-in-class agonist SLAMF7 antibody, but not by SIRPα blockade, thereby promoting antitumor immunity. Hence, CD47 suppresses phagocytosis not only by engaging SIRPα, but also by masking cell-intrinsic pro-phagocytic ligands on tumor cells and knowledge of this mechanism may influence the decision between CD47 blockade or SIRPα blockade for therapeutic purposes.

Published
2023
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33. Alternative Splicing of the Inhibitory Immune Checkpoint Receptor SLAMF6 Generates a Dominant Positive Form, Boosting T-cell Effector Functions

Author

Hajaj, Emma, primary, Zisman, Elad, additional, Tzaban, Shay, additional, Merims, Sharon, additional, Cohen, Jonathan, additional, Klein, Shiri, additional, Frankenburg, Shoshana, additional, Sade-Feldman, Moshe, additional, Tabach, Yuval, additional, Yizhak, Keren, additional, Navon, Ami, additional, Stepensky, Polina, additional, Hacohen, Nir, additional, Peretz, Tamar, additional, Veillette, André, additional, Karni, Rotem, additional, Eisenberg, Galit, additional, and Lotem, Michal, additional

Published
2021
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35. Circulating Precursor CCR7loPD-1hi CXCR5+ CD4+ T Cells Indicate Tfh Cell Activity and Promote Antibody Responses upon Antigen Reexposure

Author

He, Jing, Tsai, Louis M., Leong, Yew Ann, Hu, Xin, Ma, Cindy S., Chevalier, Nina, Sun, Xiaolin, Vandenberg, Kirsten, Rockman, Steve, Ding, Yan, Zhu, Lei, Wei, Wei, Wang, Changqi, Karnowski, Alexander, Belz, Gabrielle T., Ghali, Joanna R., Cook, Matthew C., Riminton, Sean D., Veillette, André, Schwartzberg, Pamela L., Mackay, Fabienne, Brink, Robert, Tangye, Stuart G., Vinuesa, Carola G., Mackay, Charles R., Li, Zhanguo, and Yu, Di

Published
2013
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41. CD155 on Tumor Cells Drives Resistance to Immunotherapy by Inducing the Degradation of the Activating Receptor CD226 in CD8+ T Cells

Author

Braun, Matthias, primary, Aguilera, Amelia Roman, additional, Sundarrajan, Ashmitha, additional, Corvino, Dillon, additional, Stannard, Kimberley, additional, Krumeich, Sophie, additional, Das, Indrajit, additional, Lima, Luize G., additional, Meza Guzman, Lizeth G., additional, Li, Kunlun, additional, Li, Rui, additional, Salim, Nazhifah, additional, Jorge, Maria Villancanas, additional, Ham, Sunyoung, additional, Kelly, Gabrielle, additional, Vari, Frank, additional, Lepletier, Ailin, additional, Raghavendra, Ashwini, additional, Pearson, Sally, additional, Madore, Jason, additional, Jacquelin, Sebastien, additional, Effern, Maike, additional, Quine, Brodie, additional, Koufariotis, Lambros T., additional, Casey, Mika, additional, Nakamura, Kyohei, additional, Seo, Eun Y., additional, Hölzel, Michael, additional, Geyer, Matthias, additional, Kristiansen, Glen, additional, Taheri, Touraj, additional, Ahern, Elizabeth, additional, Hughes, Brett G.M., additional, Wilmott, James S., additional, Long, Georgina V., additional, Scolyer, Richard A., additional, Batstone, Martin D., additional, Landsberg, Jennifer, additional, Dietrich, Dimo, additional, Pop, Oltin T., additional, Flatz, Lukas, additional, Dougall, William C., additional, Veillette, André, additional, Nicholson, Sandra E., additional, Möller, Andreas, additional, Johnston, Robert J., additional, Martinet, Ludovic, additional, Smyth, Mark J., additional, and Bald, Tobias, additional

Published
2020
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42. Alternative splicing of SLAMF6 in human T cells creates a co-stimulatory isoform that counteracts the inhibitory effect of the full-length receptor

Author

Hajaj, Emma, primary, Zisman, Elad, additional, Tzaban, Shay, additional, Merims, Sharon, additional, Cohen, Jonathan, additional, Klein, Shiri, additional, Frankenburg, Shoshana, additional, Sade-Feldman, Moshe, additional, Tabach, Yuval, additional, Yizhak, Keren, additional, Navon, Ami, additional, Stepensky, Polina, additional, Hacohen, Nir, additional, Peretz, Tamar, additional, Veillette, André, additional, Karni, Rotem, additional, Eisenberg, Galit, additional, and Lotem, Michal, additional

Published
2020
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43. Critical Role of Lipid Scramblase TMEM16F in Phosphatidylserine Exposure and Repair of Plasma Membrane after Pore Formation

Author

Wu, Ning, primary, Cernysiov, Vitalij, additional, Davidson, Dominique, additional, Song, Hua, additional, Tang, Jianlong, additional, Luo, Shanshan, additional, Lu, Yan, additional, Qian, Jin, additional, Gyurova, Ivayla E., additional, Waggoner, Stephen N., additional, Trinh, Vincent Quoc-Huy, additional, Cayrol, Romain, additional, Sugiura, Ayumu, additional, McBride, Heidi M., additional, Daudelin, Jean-François, additional, Labrecque, Nathalie, additional, and Veillette, André, additional

Published
2020
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