Your search keyword '"Courau, Tristan"' showing total 27 results

1. A myeloid program associated with COVID-19 severity is decreased by therapeutic blockade of IL-6 signaling

Author

Hackney, Jason A, Shivram, Haridha, Vander Heiden, Jason, Overall, Chris, Orozco, Luz, Gao, Xia, Kim, Eugene, West, Nathan, Qamra, Aditi, Chang, Diana, Chakrabarti, Arindam, Choy, David F, Combes, Alexis J, Courau, Tristan, Fragiadakis, Gabriela K, Rao, Arjun Arkal, Ray, Arja, Tsui, Jessica, Hu, Kenneth, Kuhn, Nicholas F, Krummel, Matthew F, Erle, David J, Kangelaris, Kirsten, Sarma, Aartik, Lyon, Zoe, Calfee, Carolyn S, Woodruff, Prescott G, Ghale, Rajani, Mick, Eran, Byrne, Ashley, Zha, Beth Shoshana, Langelier, Charles, Hendrickson, Carolyn M, van der Wijst, Monique GP, Hartoularos, George C, Grant, Tianna, Bueno, Raymund, Lee, David S, Greenland, John R, Sun, Yang, Perez, Richard, Ogorodnikov, Anton, Ward, Alyssa, Ye, Chun Jimmie, Consortium, UCSF COMET, Abe-Jones, Yumiko, Adkisson, Michael, Ansel, K Mark, Asthana, Saurabh, Beagle, Alexander, Bhide, Sharvari, Cai, Cathy, Caldera, Saharai, Calvo, Maria, Carrillo, Sidney A, Chak, Suzanna, Christenson, Stephanie, Collins, Zachary, Darmanis, Spyros, Detweiler, Angela, DeVoe, Catherine, Eckalbar, Walter, Giberson, Jeremy, Gonzalez, Ana, Gordon, Gracie, Serpa, Paula Hayakawa, Jauregui, Alejandra, Jones, Chayse, Ke, Serena, Kushnoor, Divya, Lea, Tasha, Lee, Deanna, Leligdowicz, Aleksandra, Liu, Yale, Mahboob, Salman, Maliskova, Lenka, Matthay, Michael, McCarthy, Elizabeth, Muñoz-Sandoval, Priscila, Neff, Norma, Nguyen, Viet, Nigam, Nishita, Parada, Randy, Phelps, Maira, Pierce, Logan, Prasad, Priya, Rashid, Sadeed, Reeder, Gabriella, Rodriguez, Nicklaus, Samad, Bushra, Schroeder, Andrew, Shaw, Cole, Shen, Alan, Sigman, Austin, Sinha, Pratik, Spitzer, Matthew, Sunshine, Sara, Tang, Kevin, Altamirano, Luz Torres, and Tsitsiklis, Alexandra

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Lung, Coronaviruses, Emerging Infectious Diseases, Infectious Diseases, Acute Respiratory Distress Syndrome, Rare Diseases, Clinical Research, 2.1 Biological and endogenous factors, Good Health and Well Being, UCSF COMET Consortium, Clinical genetics, Immune response, Molecular medicine

Abstract

Altered myeloid inflammation and lymphopenia are hallmarks of severe infections. We identified the upregulated EN-RAGE gene program in airway and blood myeloid cells from patients with acute lung injury from SARS-CoV-2 or other causes across 7 cohorts. This program was associated with greater clinical severity and predicted future mechanical ventilation and death. EN-RAGEhi myeloid cells express features consistent with suppressor cell functionality, including low HLA-DR and high PD-L1. Sustained EN-RAGE program expression in airway and blood myeloid cells correlated with clinical severity and increasing expression of T cell dysfunction markers. IL-6 upregulated many EN-RAGE program genes in monocytes in vitro. IL-6 signaling blockade by tocilizumab in a placebo-controlled clinical trial led to rapid normalization of EN-RAGE and T cell gene expression. This identifies IL-6 as a key driver of myeloid dysregulation associated with worse clinical outcomes in COVID-19 patients and provides insights into shared pathophysiological mechanisms in non-COVID-19 ARDS.

Published

2023

2. Transcriptional space-time mapping identifies concerted immune and stromal cell patterns and gene programs in wound healing and cancer

Author

Hu, Kenneth H, Kuhn, Nicholas F, Courau, Tristan, Tsui, Jessica, Samad, Bushra, Ha, Patrick, Kratz, Johannes R, Combes, Alexis J, and Krummel, Matthew F

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Wound Healing and Care, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Mice, Animals, Humans, Wound Healing, Skin, Neoplasms, Macrophages, Fibroblasts, Stromal Cells, cell-cell crosstalk, fibroblasts, gene programs, immunology, macrophage, skin, systems biology, tumor microenvironment, wound healing, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

Tissue repair responses in metazoans are highly coordinated by different cell types over space and time. However, comprehensive single-cell-based characterization covering this coordination is lacking. Here, we captured transcriptional states of single cells over space and time during skin wound closure, revealing choreographed gene-expression profiles. We identified shared space-time patterns of cellular and gene program enrichment, which we call multicellular "movements" spanning multiple cell types. We validated some of the discovered space-time movements using large-volume imaging of cleared wounds and demonstrated the value of this analysis to predict "sender" and "receiver" gene programs in macrophages and fibroblasts. Finally, we tested the hypothesis that tumors are like "wounds that never heal" and found conserved wound healing movements in mouse melanoma and colorectal tumor models, as well as human tumor samples, revealing fundamental multicellular units of tissue biology for integrative studies.

Published

2023

3. Cyclone: an accessible pipeline to analyze, evaluate, and optimize multiparametric cytometry data

Author

Patel, Ravi K, Jaszczak, Rebecca G, Im, Kwok, Carey, Nicholas D, Courau, Tristan, Bunis, Daniel G, Samad, Bushra, Avanesyan, Lia, Chew, Nayvin W, Stenske, Sarah, Jespersen, Jillian M, Publicover, Jean, Edwards, Austin W, Naser, Mohammad, Rao, Arjun A, Lupin-Jimenez, Leonard, Krummel, Matthew F, Cooper, Stewart, Baron, Jody L, Combes, Alexis J, and Fragiadakis, Gabriela K

Subjects

Biomedical and Clinical Sciences, Immunology, Immunotherapy, Inflammatory and immune system, Cancer, Good Health and Well Being, Cyclonic Storms, Algorithms, Benchmarking, Cluster Analysis, Technology, cyclone, CyTOF, spectral flow cytometry, spatial expression data, multi-parametric analysis, FlowSOM, clustering optimization, Medical Microbiology, Biochemistry and cell biology, Genetics

Abstract

In the past decade, high-dimensional single-cell technologies have revolutionized basic and translational immunology research and are now a key element of the toolbox used by scientists to study the immune system. However, analysis of the data generated by these approaches often requires clustering algorithms and dimensionality reduction representation, which are computationally intense and difficult to evaluate and optimize. Here, we present Cytometry Clustering Optimization and Evaluation (Cyclone), an analysis pipeline integrating dimensionality reduction, clustering, evaluation, and optimization of clustering resolution, and downstream visualization tools facilitating the analysis of a wide range of cytometry data. We benchmarked and validated Cyclone on mass cytometry (CyTOF), full-spectrum fluorescence-based cytometry, and multiplexed immunofluorescence (IF) in a variety of biological contexts, including infectious diseases and cancer. In each instance, Cyclone not only recapitulates gold standard immune cell identification but also enables the unsupervised identification of lymphocytes and mononuclear phagocyte subsets that are associated with distinct biological features. Altogether, the Cyclone pipeline is a versatile and accessible pipeline for performing, optimizing, and evaluating clustering on a variety of cytometry datasets, which will further power immunology research and provide a scaffold for biological discovery.

Published

2023

4. Spatiotemporal co-dependency between macrophages and exhausted CD8+ T cells in cancer

Author

Kersten, Kelly, Hu, Kenneth H, Combes, Alexis J, Samad, Bushra, Harwin, Tory, Ray, Arja, Rao, Arjun Arkal, Cai, En, Marchuk, Kyle, Artichoker, Jordan, Courau, Tristan, Shi, Quanming, Belk, Julia, Satpathy, Ansuman T, and Krummel, Matthew F

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Immunotherapy, CD8-Positive T-Lymphocytes, Cell Differentiation, Humans, Macrophages, Neoplasms, Tumor Microenvironment, T cell exhaustion, antitumor immunity, immunotherapy, tumor microenvironment, tumor-associated macrophages, anti-tumor immunity, Neurosciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

T cell exhaustion is a major impediment to antitumor immunity. However, it remains elusive how other immune cells in the tumor microenvironment (TME) contribute to this dysfunctional state. Here, we show that the biology of tumor-associated macrophages (TAMs) and exhausted T cells (Tex) in the TME is extensively linked. We demonstrate that in vivo depletion of TAMs reduces exhaustion programs in tumor-infiltrating CD8+ T cells and reinvigorates their effector potential. Reciprocally, transcriptional and epigenetic profiling reveals that Tex express factors that actively recruit monocytes to the TME and shape their differentiation. Using lattice light sheet microscopy, we show that TAM and CD8+ T cells engage in unique, long-lasting, antigen-specific synaptic interactions that fail to activate T cells but prime them for exhaustion, which is then accelerated in hypoxic conditions. Spatially resolved sequencing supports a spatiotemporal self-enforcing positive feedback circuit that is aligned to protect rather than destroy a tumor.

Published

2022

5. Discovering dominant tumor immune archetypes in a pan-cancer census

Author

Combes, Alexis J, Samad, Bushra, Tsui, Jessica, Chew, Nayvin W, Yan, Peter, Reeder, Gabriella C, Kushnoor, Divyashree, Shen, Alan, Davidson, Brittany, Barczak, Andrea J, Adkisson, Michael, Edwards, Austin, Naser, Mohammad, Barry, Kevin C, Courau, Tristan, Hammoudi, Taymour, Argüello, Rafael J, Rao, Arjun Arkal, Olshen, Adam B, Consortium, The Immunoprofiler, Spitzer, Matthew, Fong, Lawrence, Nelson, Amanda, Kumar, Raj, Lee, Justin, Burra, Arun, Hsu, Joy, Hackett, Caroline, Tolentino, Karen, Sjarif, Jasmine, Johnson, Peter, Shao, Evans, Abrau, Darrell, Lupin, Leonard, Shaw, Cole, Collins, Zachary, Lea, Tasha, Corvera, Carlos, Nakakura, Eric, Carnevale, Julia, Alvarado, Michael, Loo, Kimberley, Chen, Lawrence, Chow, Melissa, Grandis, Jennifer, Ryan, Will, El-Sayed, Ivan, Jablons, David, Woodard, Gavitt, Meng, Maxwell W, Porten, Sima P, Okada, Hideho, Tempero, Margaret, Ko, Andrew, Kirkwood, Kim, Vandenberg, Scott, Guevarra, Denise, Oropeza, Erica, Cyr, Chris, Glenn, Pat, Bolen, Jennifer, Morton, Amanda, Eckalbar, Walter, Cai, Cathy, Zhan, Jenny, Davis, Katelyn C, Kelley, Robin K, Chapman, Jocelyn S, Atreya, Chloe E, Patel, Amar, Daud, Adil I, Ha, Patrick, Diaz, Aaron A, Kratz, Johannes R, Collisson, Eric A, Fragiadakis, Gabriela K, Erle, David J, Boissonnas, Alexandre, Asthana, Saurabh, Chan, Vincent, and Krummel, Matthew F

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Genetics, Cancer, Cancer Genomics, Human Genome, Biomarkers, Tumor, Censuses, Cluster Analysis, Cohort Studies, Computational Biology, Flow Cytometry, Gene Expression Regulation, Neoplastic, Humans, Neoplasms, RNA-Seq, San Francisco, Transcriptome, Tumor Microenvironment, Universities, Immunoprofiler Consortium, Pan Cancer analysis, immune profiling, solid tumor microenvironement, system immunology, tumor immunology, unsupervised clustering, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

Cancers display significant heterogeneity with respect to tissue of origin, driver mutations, and other features of the surrounding tissue. It is likely that individual tumors engage common patterns of the immune system-here "archetypes"-creating prototypical non-destructive tumor immune microenvironments (TMEs) and modulating tumor-targeting. To discover the dominant immune system archetypes, the University of California, San Francisco (UCSF) Immunoprofiler Initiative (IPI) processed 364 individual tumors across 12 cancer types using standardized protocols. Computational clustering of flow cytometry and transcriptomic data obtained from cell sub-compartments uncovered dominant patterns of immune composition across cancers. These archetypes were profound insofar as they also differentiated tumors based upon unique immune and tumor gene-expression patterns. They also partitioned well-established classifications of tumor biology. The IPI resource provides a template for understanding cancer immunity as a collection of dominant patterns of immune organization and provides a rational path forward to learn how to modulate these to improve therapy.

Published

2022

6. Global absence and targeting of protective immune states in severe COVID-19

Author

Combes, Alexis J, Courau, Tristan, Kuhn, Nicholas F, Hu, Kenneth H, Ray, Arja, Chen, William S, Chew, Nayvin W, Cleary, Simon J, Kushnoor, Divyashree, Reeder, Gabriella C, Shen, Alan, Tsui, Jessica, Hiam-Galvez, Kamir J, Muñoz-Sandoval, Priscila, Zhu, Wandi S, Lee, David S, Sun, Yang, You, Ran, Magnen, Mélia, Rodriguez, Lauren, Im, KW, Serwas, Nina K, Leligdowicz, Aleksandra, Zamecnik, Colin R, Loudermilk, Rita P, Wilson, Michael R, Ye, Chun J, Fragiadakis, Gabriela K, Looney, Mark R, Chan, Vincent, Ward, Alyssa, Carrillo, Sidney, Matthay, Michael, Erle, David J, Woodruff, Prescott G, Langelier, Charles, Kangelaris, Kirsten, Hendrickson, Carolyn M, Calfee, Carolyn, Rao, Arjun Arkal, and Krummel, Matthew F

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Emerging Infectious Diseases, Coronaviruses, Immunotherapy, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Inflammatory and immune system, Good Health and Well Being, Antibodies, Viral, Antibody Formation, Base Sequence, COVID-19, Female, Humans, Immunoglobulin G, Interferons, Male, Neutrophils, Protein Domains, Receptor, Interferon alpha-beta, Receptors, IgG, SARS-CoV-2, Single-Cell Analysis, Viral Load, UCSF COMET Consortium, General Science & Technology

Abstract

Although infection with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has pleiotropic and systemic effects in some individuals1-3, many others experience milder symptoms. Here, to gain a more comprehensive understanding of the distinction between severe and mild phenotypes in the pathology of coronavirus disease 2019 (COVID-19) and its origins, we performed a whole-blood-preserving single-cell analysis protocol to integrate contributions from all major immune cell types of the blood-including neutrophils, monocytes, platelets, lymphocytes and the contents of the serum. Patients with mild COVID-19 exhibit a coordinated pattern of expression of interferon-stimulated genes (ISGs)3 across every cell population, whereas these ISG-expressing cells are systemically absent in patients with severe disease. Paradoxically, individuals with severe COVID-19 produce very high titres of anti-SARS-CoV-2 antibodies and have a lower viral load compared to individuals with mild disease. Examination of the serum from patients with severe COVID-19 shows that these patients uniquely produce antibodies that functionally block the production of the ISG-expressing cells associated with mild disease, by activating conserved signalling circuits that dampen cellular responses to interferons. Overzealous antibody responses pit the immune system against itself in many patients with COVID-19, and perhaps also in individuals with other viral infections. Our findings reveal potential targets for immunotherapies in patients with severe COVID-19 to re-engage viral defence.

Published

2021

7. A myeloid program associated with COVID-19 severity is decreased by therapeutic blockade of IL-6 signaling

Author

Abe-Jones, Yumiko, Adkisson, Michael, Ansel, K. Mark, Asthana, Saurabh, Beagle, Alexander, Bhide, Sharvari, Cai, Cathy, Caldera, Saharai, Calvo, Maria, Carrillo, Sidney A., Chak, Suzanna, Christenson, Stephanie, Collins, Zachary, Darmanis, Spyros, Detweiler, Angela, DeVoe, Catherine, Eckalbar, Walter, Giberson, Jeremy, Gonzalez, Ana, Gordon, Gracie, Serpa, Paula Hayakawa, Jauregui, Alejandra, Jones, Chayse, Ke, Serena, Kushnoor, Divya, Lea, Tasha, Lee, Deanna, Leligdowicz, Aleksandra, Liu, Yale, Mahboob, Salman, Maliskova, Lenka, Matthay, Michael, McCarthy, Elizabeth, Muñoz-Sandoval, Priscila, Neff, Norma, Nguyen, Viet, Nigam, Nishita, Parada, Randy, Phelps, Maira, Pierce, Logan, Prasad, Priya, Rashid, Sadeed, Reeder, Gabriella, Rodriguez, Nicklaus, Samad, Bushra, Schroeder, Andrew, Shaw, Cole, Shen, Alan, Sigman, Austin, Sinha, Pratik, Spitzer, Matthew, Sunshine, Sara, Tang, Kevin, Altamirano, Luz Torres, Tsitsiklis, Alexandra, Tumurbaatar, Erden, Upadhyay, Vaibhav, Whatley, Alexander, Willmore, Andrew, Wilson, Michael, Winkler, Juliane, Wong, Kristine, Yee, Kimberly, Yu, Michelle, Zhou, Mingyue, Zhu, Wandi S., Hackney, Jason A., Shivram, Haridha, Vander Heiden, Jason, Overall, Chris, Orozco, Luz, Gao, Xia, Kim, Eugene, West, Nathan, Qamra, Aditi, Chang, Diana, Chakrabarti, Arindam, Choy, David F., Combes, Alexis J., Courau, Tristan, Fragiadakis, Gabriela K., Rao, Arjun Arkal, Ray, Arja, Tsui, Jessica, Hu, Kenneth, Kuhn, Nicholas F., Krummel, Matthew F., Erle, David J., Kangelaris, Kirsten, Sarma, Aartik, Lyon, Zoe, Calfee, Carolyn S., Woodruff, Prescott G., Ghale, Rajani, Mick, Eran, Byrne, Ashley, Zha, Beth Shoshana, Langelier, Charles, Hendrickson, Carolyn M., van der Wijst, Monique G.P., Hartoularos, George C., Grant, Tianna, Bueno, Raymund, Lee, David S., Greenland, John R., Sun, Yang, Perez, Richard, Ogorodnikov, Anton, Ward, Alyssa, Ye, Chun Jimmie, Ramalingam, Thiru, McBride, Jacqueline M., Cai, Fang, Teterina, Anastasia, Bao, Min, Tsai, Larry, Rosas, Ivan O., Regev, Aviv, Kapadia, Sharookh B., Bauer, Rebecca N., and Rosenberger, Carrie M.

Published

2023

8. KLRG1 and CD103 Expressions Define Distinct Intestinal Tissue-Resident Memory CD8 T Cell Subsets Modulated in Crohns Disease.

Author

Bottois, Hugo, Ngollo, Marjolaine, Hammoudi, Nassim, Courau, Tristan, Bonnereau, Julie, Chardiny, Victor, Grand, Céline, Gergaud, Brice, Allez, Matthieu, and Le Bourhis, Lionel

Subjects

CD103, Crohns disease, IBD – inflammatory bowel diseases, KLRG1, T cells, TRM cells, Antigens, CD, CD8-Positive T-Lymphocytes, Clinical Trials as Topic, Crohn Disease, Gene Expression Profiling, Humans, Immunity, Innate, Immunologic Memory, Inflammation, Integrin alpha Chains, Interleukins, Intestinal Mucosa, Lectins, C-Type, Receptors, Immunologic, T-Lymphocyte Subsets

Abstract

Intestinal tissue-resident memory CD8 T cells (Trm) are non-recirculating effector cells ideally positioned to detect and react to microbial infections in the gut mucosa. There is an emerging understanding of Trm cell differentiation and functions, but their implication in inflammatory bowel diseases, such as Crohns disease (CD), is still unknown. Here, we describe CD8 cells in the human intestine expressing KLRG1 or CD103, two receptors of E-cadherin. While CD103 CD8 T cells are present in high numbers in the mucosa of CD patients and controls, KLRG1 CD8 T cells are increased in inflammatory conditions. Mucosal CD103 CD8 T cells are more responsive to TCR restimulation, but KLRG1 CD8 T cells show increased cytotoxic and proliferative potential. CD103 CD8 T cells originate mostly from KLRG1 negative cells after TCR triggering and TGFβ stimulation. Interestingly, mucosal CD103 CD8 T cells from CD patients display major changes in their transcriptomic landscape compared to controls. They express Th17 related genes including CCL20, IL22, and IL26, which could contribute to the pathogenesis of CD. Overall, these findings suggest that CD103 CD8 T cells in CD induce a tissue-wide alert increasing innate immune responses and recruitment of effector cells such as KLRG1 CD8 T cells.

Published

2020

9. Cocultures of human colorectal tumor spheroids with immune cells reveal the therapeutic potential of MICA/B and NKG2A targeting for cancer treatment.

Author

Courau, Tristan, Bonnereau, Julie, Chicoteau, Justine, Bottois, Hugo, Remark, Romain, Assante Miranda, Laura, Toubert, Antoine, Blery, Mathieu, Aparicio, Thomas, Allez, Matthieu, and Le Bourhis, Lionel

Subjects

Colorectal cancer, Immunotherapy, MICA/B, NKG2A, Spheroids, Antineoplastic Agents, Immunological, Cell Line, Tumor, Cell Proliferation, Cell Survival, Coculture Techniques, Colorectal Neoplasms, HT29 Cells, Histocompatibility Antigens Class I, Humans, Killer Cells, Natural, Molecular Targeted Therapy, NK Cell Lectin-Like Receptor Subfamily C, Spheroids, Cellular, T-Lymphocytes

Abstract

BACKGROUND: Immunotherapies still fail to benefit colorectal cancer (CRC) patients. Relevant functional assays aimed at studying these failures and the efficacy of cancer immunotherapy in human are scarce. 3D tumor cultures, called tumor organoids or spheroids, represent interesting models to study cancer treatments and could help to challenge these issues. METHODS: We analyzed heterotypic cocultures of human colon tumor-derived spheroids with immune cells to assess the infiltration, activation and function of T and NK cells toward human colorectal tumors in vitro. RESULTS: We showed that allogeneic T and NK cells rapidly infiltrated cell line-derived spheroids, inducing immune-mediated tumor cell apoptosis and spheroid destruction. NKG2D, a key activator of cytotoxic responses, was engaged on infiltrating cells. We thus assessed the therapeutic potential of an antibody targeting the specific ligands of NKG2D, MICA and MICB, in this system. Anti-MICA/B enhanced immune-dependent destruction of tumor spheroid by driving an increased NK cells infiltration and activation. Interestingly, tumor cells reacted to immune infiltration by upregulating HLA-E, ligand of the inhibitory receptor NKG2A expressed by CD8 and NK cells. NKG2A was increased after anti-MICA/B treatment and, accordingly, combination of anti-MICA/B and anti-NKG2A was synergistic. These observations were ultimately confirmed in a clinical relevant model of coculture between CRC patients-derived spheroids and autologous tumor-infiltrating lymphocytes. CONCLUSIONS: Altogether, we show that tumor spheroids represent a relevant tool to study tumor-lymphocyte interactions on human tissues and revealed the antitumor potential of immunomodulatory antibodies targeting MICA/B and NKG2A.

Published

2019

10. Activating Immune Recognition in Pancreatic Ductal Adenocarcinoma via Autophagy Inhibition, MEK Blockade, and CD40 Agonism

Author

Jiang, Honglin, Courau, Tristan, Borison, Joseph, Ritchie, Alexa J., Mayer, Aaron T., Krummel, Matthew F., and Collisson, Eric A.

Published

2022

11. Correction: Activated dendritic cells modulate proliferation and differentiation of human myoblasts

Author

Ladislau, Leandro, Portilho, Débora M., Courau, Tristan, Solares-Pérez, Alhondra, Negroni, Elisa, Lainé, Jeanne, Klatzmann, David, Bonomo, Adriana, Allenbach, Yves, Benveniste, Olivier, Riederer, Ingo, Savino, Wilson, Mouly, Vincent, Butler-Browne, Gillian, and Benjamim, Claudia F.

Published

2022

12. Role of Chemokine Receptor CCR4 and Regulatory T Cells in Wound Healing of Diabetic Mice

Author

Barros, Janaína F., Waclawiak, Ingrid, Pecli, Cyntia, Borges, Paula A., Georgii, Janaína L., Ramos-Junior, Erivan S., Canetti, Claudio, Courau, Tristan, Klatzmann, David, Kunkel, Steven L., Penido, Carmen, Canto, Fábio B., and Benjamim, Claudia F.

Published

2019

13. Cyclone: an accessible pipeline to analyze, evaluate, and optimize multiparametric cytometry data.

Author

Patel, Ravi K., Jaszczak, Rebecca G., Im, Kwok, Carey, Nicholas D., Courau, Tristan, Bunis, Daniel G., Samad, Bushra, Avanesyan, Lia, Chew, Nayvin W., Stenske, Sarah, Jespersen, Jillian M., Publicover, Jean, Edwards, Austin W., Naser, Mohammad, Rao, Arjun A., Lupin-Jimenez, Leonard, Krummel, Matthew F., Cooper, Stewart, Baron, Jody L., and Combes, Alexis J.

Subjects

CYTOMETRY, CYCLONES, DIMENSIONAL reduction algorithms, TRANSMISSIBLE tumors, MACROPHAGES

Abstract

In the past decade, high-dimensional single-cell technologies have revolutionized basic and translational immunology research and are now a key element of the toolbox used by scientists to study the immune system. However, analysis of the data generated by these approaches often requires clustering algorithms and dimensionality reduction representation, which are computationally intense and difficult to evaluate and optimize. Here, we present Cytometry Clustering Optimization and Evaluation (Cyclone), an analysis pipeline integrating dimensionality reduction, clustering, evaluation, and optimization of clustering resolution, and downstream visualization tools facilitating the analysis of a wide range of cytometry data. We benchmarked and validated Cyclone on mass cytometry (CyTOF), full-spectrum fluorescence-based cytometry, and multiplexed immunofluorescence (IF) in a variety of biological contexts, including infectious diseases and cancer. In each instance, Cyclone not only recapitulates gold standard immune cell identification but also enables the unsupervised identification of lymphocytes and mononuclear phagocyte subsets that are associated with distinct biological features. Altogether, the Cyclone pipeline is a versatile and accessible pipeline for performing, optimizing, and evaluating clustering on a variety of cytometry datasets, which will further power immunology research and provide a scaffold for biological discovery [ABSTRACT FROM AUTHOR]

Published

2023

14. Activated dendritic cells modulate proliferation and differentiation of human myoblasts

Author

Ladislau, Leandro, Portilho, Débora M., Courau, Tristan, Solares-Pérez, Alhondra, Negroni, Elisa, Lainé, Jeanne, Klatzmann, David, Bonomo, Adriana, Allenbach, Yves, Benveniste, Olivier, Riederer, Ingo, Savino, Wilson, Mouly, Vincent, Butler-Browne, Gillian, and Benjamim, Claudia F.

Published

2018

15. Autologous T cell responses to primary human colorectal cancer spheroids are enhanced by ectonucleotidase inhibition.

Author

Bonnereau, Julie, Courau, Tristan, Asesio, Nicolas, Salfati, Delphine, Bouhidel, Fatiha, Corte, Hélène, Hamoudi, Sarah, Hammoudi, Nassim, Lavolé, Julie, Vivier-Chicoteau, Justine, Chardiny, Victor, Maggiori, Leon, Blery, Mathieu, Remark, Romain, Bonnafous, Cécile, Cattan, Pierre, Toubert, Antoine, Bhat, Purnima, Allez, Matthieu, and Aparicio, Thomas

Subjects

T cells, GRANZYMES, RECTAL cancer, T cell receptors, COLORECTAL cancer, MONONUCLEAR leukocytes, REGULATORY T cells, CYTOTOXIC T cells

Published

2023

16. Regulatory T-cell development and function are impaired in mice lacking membrane expression of full length intercellular adhesion molecule-1

Author

Gottrand, Gaëlle, Courau, Tristan, Thomas-Vaslin, Véronique, Prevel, Nicolas, Vazquez, Thomas, Ruocco, Maria Grazia, Lambrecht, Benedicte, Bellier, Bertrand, Colombo, Bruno M., and Klatzmann, David

Published

2015

17. Publisher Correction: Global absence and targeting of protective immune states in severe COVID-19

Author

Combes, Alexis J., Courau, Tristan, Kuhn, Nicholas F., Hu, Kenneth H., Ray, Arja, Chen, William S., and Chew, Nayvin W.

Subjects

Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Author(s): Alexis J. Combes [sup.1] [sup.2] [sup.3] , Tristan Courau [sup.1] [sup.2] [sup.3] , Nicholas F. Kuhn [sup.1] [sup.2] , Kenneth H. Hu [sup.1] [sup.2] , Arja Ray [sup.1] [sup.2] [...]

Published

2021

18. Regulatory T Cells Orchestrate Similar Immune Evasion of Fetuses and Tumors in Mice.

Author

Nehar-Belaid, Djamel, Courau, Tristan, Dérian, Nicolas, Ruocco, Maria Grazia, Klatzmann, David, and Florez, Laura

Subjects

*T cells, *PREGNANCY, *EMBRYOS, *TUMORS, *FETUS, *LABORATORY mice

Abstract

Embryos and tumors are both masses of dividing cells expressing foreign Ags, but they are not rejected by the immune system. We hypothesized that similar tolerogenic mechanisms prevent their rejection. Global comparison of fetal and tumor microenvironments through transcriptomics in mice revealed strikingly similar and dramatic decreases in expression of numerous immune-related pathways, including Ag presentation and T cell signaling. Unsupervised analyses highlighted the parallel kinetics and similarities of immune signature downregulation, from the very first days after tumor or embryo implantation. Besides upregulated signatures related to cell proliferation, the only significant signatures shared by the two conditions across all biological processes and all time points studied were downmodulated immune response signatures. Regulatory T cell depletion completely reverses this immune downmodulation to an immune upregulation that leads tofetal or tumor immune rejection. We propose that evolutionarily selected mechanisms that protect mammalian fetuses from immune attack are hijacked to license tumor development. [ABSTRACT FROM AUTHOR]

Published

2016

19. Tumor-associated macrophage heterogeneity is driven by tissue territories in breast cancer.

Author

Laviron, Marie, Petit, Maxime, Weber-Delacroix, Eléonore, Combes, Alexis J., Arkal, Arjun Rao, Barthélémy, Sandrine, Courau, Tristan, Hume, David A., Combadière, Christophe, Krummel, Matthew F., and Boissonnas, Alexandre

Abstract

Tissue-resident macrophages adapt to local signals within tissues to acquire specific functions. Neoplasia transforms the tissue, raising the question as to how the environmental perturbations contribute to tumor-associated macrophage (TAM) identity and functions. Combining single-cell RNA sequencing (scRNA-seq) with spatial localization of distinct TAM subsets by imaging, we discover that TAM transcriptomic programs follow two main differentiation paths according to their localization in the stroma or in the neoplastic epithelium of the mammary duct. Furthermore, this diversity is exclusively detected in a spontaneous tumor model and tracks the different tissue territories as well as the type of tumor lesion. These TAM subsets harbor distinct capacity to activate CD8+ T cells and phagocyte tumor cells, supporting that specific tumor regions, rather than defined activation states, are the major drivers of TAM plasticity and heterogeneity. The distinctions created here provide a framework to design cancer treatment targeting specific TAM niches. [Display omitted] • TAMs differentiate according to their localization in situ • TAM heterogeneity is associated with resident TAM diversity prior to tumor development • Orthotopic tumor models negate TAM diversity • Similar heterogeneity is found in human breast TAMs The origin of tumor-associated macrophage (TAM) heterogeneity is unclear. Laviron et al. show that TAM diversity is driven by the various tissue territories existing prior to tumor apparition and by the state of tumor malignancy. This provides a definition of TAM heterogeneity according to their spatial distribution in situ. [ABSTRACT FROM AUTHOR]

Published

2022

20. Self-Specific Memory Regulatory T Cells Protect Embryos at Implantation in Mice.

Author

Ting Chen, Darrasse-Jèze, Guillaume, Bergot, Anne-Sophie, Courau, Tristan, Churlaud, Guillaume, Valdivia, Karina, Strominger, Jack L., Ruocco, Maria Grazia, Chaouat, Gérard, and Klatzmann, David

Subjects

*EMBRYO implantation, *T cells, *PREGNANCY, *INTERLEUKIN-2, *PROTEIN-tyrosine kinases, *LABORATORY mice, *PHYSIOLOGY

Abstract

Regulatory T cells (Tregs) play crucial roles in both fetal and tumor development. We recently showed that immunosurveillance by pre-existing CD44highCD62Llow activated/memory Tregs (amTregs) specific for self-Ags protects emergent tumor cells in mice. This Treg response of a memory type is more rapid than and dominates the antitumor response of tumor-specific effector T cells. In this study, we report striking similarities between the early Treg responses to embryo and tumor implantation. Tregs are rapidly recruited to uterus-draining lymph nodes and activated in the first days after embryo implantation in both syngeneic and allogeneic matings; express the markers of the amTreg subset; and are at least in part self-Ag specific, as seen in tumor emergence. Unlike in the tumor emergence setting, however, for which preimmunization against tumor Ags is sufficient for complete tumor eradication even in the presence of Tregs, Treg depletion is additionally required for high frequencies of fetus loss after preimmunization against paternal tissue Ags. Thus, amTregs play a major role in protecting embryos in both naive and preimmune settings. This role and the ensuing therapeutic potential are further highlighted by showing that Treg stimulation, directly by low-dose IL-2 or indirectly by Fms-related tyrosine kinase 3 ligand, led to normal pregnancy rates in a spontaneous abortion-prone model. [ABSTRACT FROM AUTHOR]

Published

2013

21. Critical role of CD206+ macrophages in promoting a cDC1-NK-CD8 T cell anti-tumor immune axis.

Author

Ray A, Hu KH, Kersten K, Courau T, Kuhn NF, Zaleta-Linares I, Samad B, Combes AJ, and Krummel MF

Abstract

Tumor-associated macrophages (TAMs) are frequently categorized as being 'M1' or 'M2' polarized, even as substantial data challenges this binary modeling of macrophage cell state. One molecule consistently referenced as a delineator of a putative immunosuppressive 'M2' state is the surface protein CD206. We thus made a novel conditional CD206 ( Mrc1 ) knock-in mouse to specifically visualize and/or deplete CD206+ 'M2-like' TAMs and assess their correspondence with pro-tumoral immunity. Early, but not late depletion of CD206+ macrophages and monocytes (here, 'Mono/Macs') led to an indirect loss of a key anti-tumor network of NK cells, conventional type I dendritic cells (cDC1) and CD8 T cells. Among myeloid cells, we found that the CD206+ TAMs are the primary producers of CXCL9, and able to differentially attract activated CD8 T cells. In contrast, a population of stress-responsive TAMs ("Hypoxic" or Spp1 +) and immature monocytes, which lack CD206 expression and become prominent following early depletion, expressed markedly diminished levels of CXCL9. Those NK and CD8 T cells which enter CD206-depleted tumors express vastly reduced levels of the corresponding receptor Cxcr3 , the cDC1-attracting chemokine Xcl1 and cDC1 growth factor Flt3l transcripts. Consistent with the loss of this critical network, early CD206+ TAM depletion decreased tumor control by antigen specific CD8 T cells in mice. Likewise, in humans, the CD206 Replete , but not the CD206 Depleted Mono/Mac gene signature correlated robustly with CD8 T cell, NK cell and stimulatory cDC1 gene signatures and transcriptomic signatures skewed towards CD206 Replete Mono/Macs associated with better survival. Together, these findings negate the unqualified classification of CD206+ 'M2-like' macrophages as immunosuppressive by illuminating contexts for their role in organizing a critical tumor-reactive archetype of immunity., Competing Interests: Declaration of Interests: The authors declare no competing interests

Published

2024

22. Cyclone: an accessible pipeline to analyze, evaluate and optimize multiparametric cytometry data.

Author

Patel RK, Jaszczak RG, Kwok I, Carey ND, Courau T, Bunis D, Samad B, Avanesyan L, Chew NW, Stenske S, Jespersen JM, Publicover J, Edwards A, Naser M, Rao AA, Lupin-Jimenez L, Krummel MF, Cooper S, Baron J, Combes AJ, and Fragiadakis GK

Abstract

In the past decade, high-dimensional single cell technologies have revolutionized basic and translational immunology research and are now a key element of the toolbox used by scientists to study the immune system. However, analysis of the data generated by these approaches often requires clustering algorithms and dimensionality reduction representation which are computationally intense and difficult to evaluate and optimize. Here we present Cyclone, an analysis pipeline integrating dimensionality reduction, clustering, evaluation and optimization of clustering resolution, and downstream visualization tools facilitating the analysis of a wide range of cytometry data. We benchmarked and validated Cyclone on mass cytometry (CyTOF), full spectrum fluorescence-based cytometry, and multiplexed immunofluorescence (IF) in a variety of biological contexts, including infectious diseases and cancer. In each instance, Cyclone not only recapitulates gold standard immune cell identification, but also enables the unsupervised identification of lymphocytes and mononuclear phagocytes subsets that are associated with distinct biological features. Altogether, the Cyclone pipeline is a versatile and accessible pipeline for performing, optimizing, and evaluating clustering on variety of cytometry datasets which will further power immunology research and provide a scaffold for biological discovery.

Published

2023

23. Spatiotemporal co-dependency between macrophages and exhausted CD8 + T cells in cancer.

Author

Kersten K, Hu KH, Combes AJ, Samad B, Harwin T, Ray A, Rao AA, Cai E, Marchuk K, Artichoker J, Courau T, Shi Q, Belk J, Satpathy AT, and Krummel MF

Subjects

Cell Differentiation, Humans, Macrophages, Tumor Microenvironment, CD8-Positive T-Lymphocytes, Neoplasms genetics

Abstract

T cell exhaustion is a major impediment to antitumor immunity. However, it remains elusive how other immune cells in the tumor microenvironment (TME) contribute to this dysfunctional state. Here, we show that the biology of tumor-associated macrophages (TAMs) and exhausted T cells (T ex ) in the TME is extensively linked. We demonstrate that in vivo depletion of TAMs reduces exhaustion programs in tumor-infiltrating CD8 + T cells and reinvigorates their effector potential. Reciprocally, transcriptional and epigenetic profiling reveals that T ex express factors that actively recruit monocytes to the TME and shape their differentiation. Using lattice light sheet microscopy, we show that TAM and CD8 + T cells engage in unique, long-lasting, antigen-specific synaptic interactions that fail to activate T cells but prime them for exhaustion, which is then accelerated in hypoxic conditions. Spatially resolved sequencing supports a spatiotemporal self-enforcing positive feedback circuit that is aligned to protect rather than destroy a tumor., Competing Interests: Declaration of interests A.T.S. is a scientific founder of Immunai and founder of Cartography Biosciences and receives research funding from Merck Research Laboratories and Allogene Therapeutics. M.F.K. is a founder and shareholder in Pionyr Immunotherapeutics and in Foundery Innovations, which prosecute and develop novel immunotherapeutics, respectively. The other authors declare no competing interests., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

24. Global Absence and Targeting of Protective Immune States in Severe COVID-19.

Author

Combes AJ, Courau T, Kuhn NF, Hu KH, Ray A, Chen WS, Cleary SJ, Chew NW, Kushnoor D, Reeder GC, Shen A, Tsui J, Hiam-Galvez KJ, Muñoz-Sandoval P, Zhu WS, Lee DS, Sun Y, You R, Magnen M, Rodriguez L, Leligdowicz A, Zamecnik CR, Loudermilk RP, Wilson MR, Ye CJ, Fragiadakis GK, Looney MR, Chan V, Ward A, Carrillo S, Matthay M, Erle DJ, Woodruff PG, Langelier C, Kangelaris K, Hendrickson CM, Calfee C, Rao AA, and Krummel MF

Abstract

While SARS-CoV-2 infection has pleiotropic and systemic effects in some patients, many others experience milder symptoms. We sought a holistic understanding of the severe/mild distinction in COVID-19 pathology, and its origins. We performed a whole-blood preserving single-cell analysis protocol to integrate contributions from all major cell types including neutrophils, monocytes, platelets, lymphocytes and the contents of serum. Patients with mild COVID-19 disease display a coordinated pattern of interferon-stimulated gene (ISG) expression across every cell population and these cells are systemically absent in patients with severe disease. Severe COVID-19 patients also paradoxically produce very high anti-SARS-CoV-2 antibody titers and have lower viral load as compared to mild disease. Examination of the serum from severe patients demonstrates that they uniquely produce antibodies with multiple patterns of specificity against interferon-stimulated cells and that those antibodies functionally block the production of the mild disease-associated ISG-expressing cells. Overzealous and auto-directed antibody responses pit the immune system against itself in many COVID-19 patients and this defines targets for immunotherapies to allow immune systems to provide viral defense., One Sentence Summary: In severe COVID-19 patients, the immune system fails to generate cells that define mild disease; antibodies in their serum actively prevents the successful production of those cells.

Published

2020

25. KLRG1 and CD103 Expressions Define Distinct Intestinal Tissue-Resident Memory CD8 T Cell Subsets Modulated in Crohn's Disease.

Author

Bottois H, Ngollo M, Hammoudi N, Courau T, Bonnereau J, Chardiny V, Grand C, Gergaud B, Allez M, and Le Bourhis L

Subjects

CD8-Positive T-Lymphocytes classification, Clinical Trials as Topic, Crohn Disease physiopathology, Gene Expression Profiling, Humans, Immunity, Innate, Inflammation, Interleukins immunology, T-Lymphocyte Subsets immunology, Antigens, CD metabolism, CD8-Positive T-Lymphocytes immunology, Crohn Disease immunology, Immunologic Memory, Integrin alpha Chains metabolism, Intestinal Mucosa immunology, Lectins, C-Type metabolism, Receptors, Immunologic metabolism

Abstract

Intestinal tissue-resident memory CD8 T cells (Trm) are non-recirculating effector cells ideally positioned to detect and react to microbial infections in the gut mucosa. There is an emerging understanding of Trm cell differentiation and functions, but their implication in inflammatory bowel diseases, such as Crohn's disease (CD), is still unknown. Here, we describe CD8 cells in the human intestine expressing KLRG1 or CD103, two receptors of E-cadherin. While CD103 CD8 T cells are present in high numbers in the mucosa of CD patients and controls, KLRG1 CD8 T cells are increased in inflammatory conditions. Mucosal CD103 CD8 T cells are more responsive to TCR restimulation, but KLRG1 CD8 T cells show increased cytotoxic and proliferative potential. CD103 CD8 T cells originate mostly from KLRG1 negative cells after TCR triggering and TGFβ stimulation. Interestingly, mucosal CD103 CD8 T cells from CD patients display major changes in their transcriptomic landscape compared to controls. They express Th17 related genes including CCL20, IL22, and IL26, which could contribute to the pathogenesis of CD. Overall, these findings suggest that CD103 CD8 T cells in CD induce a tissue-wide alert increasing innate immune responses and recruitment of effector cells such as KLRG1 CD8 T cells., (Copyright © 2020 Bottois, Ngollo, Hammoudi, Courau, Bonnereau, Chardiny, Grand, Gergaud, Allez and Le Bourhis.)

Published

2020

26. TGF- β and VEGF cooperatively control the immunotolerant tumor environment and the efficacy of cancer immunotherapies.

Author

Courau T, Nehar-Belaid D, Florez L, Levacher B, Vazquez T, Brimaud F, Bellier B, and Klatzmann D

Subjects

Animals, Cell Line, Tumor, Female, Immune Tolerance, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Neoplasms therapy, T-Lymphocytes, Regulatory cytology, Transforming Growth Factor beta genetics, Vascular Endothelial Growth Factor A genetics, Gene Silencing, Immunotherapy, Neoplasms immunology, Transforming Growth Factor beta metabolism, Vascular Endothelial Growth Factor A metabolism

Abstract

Tregs imprint an early immunotolerant tumor environment that prevents effective antitumor immune responses. Using transcriptomics of tumor tissues, we identified early upregulation of VEGF and TGF-β pathways compatible with tolerance imprinting. Silencing of VEGF or TGF-β in tumor cells induced early and pleiotropic modulation of immune-related transcriptome signatures in tumor tissues. These were surprisingly similar for both silenced tumors and related to common downstream effects on Tregs. Silencing of VEGF or TGF-β resulted in dramatically delayed tumor growth, associated with decreased Tregs and myeloid-derived suppressor cells and increased effector T cell activation in tumor infiltrates. Strikingly, co-silencing of TGF-β and VEGF led to a substantial spontaneous tumor eradication rate and the combination of their respective inhibitory drugs was synergistic. VEGF and/or TGF-β silencing also restored tumor sensitivity to tumor-specific cell therapies and markedly improved the efficacy of anti-PD-1/anti-CTLA-4 treatment. Thus, TGF-β and VEGF cooperatively control the tolerant environment of tumors and are targets for improved cancer immunotherapies.

Published

2016

27. Self-specific memory regulatory T cells protect embryos at implantation in mice.

Author

Chen T, Darrasse-Jèze G, Bergot AS, Courau T, Churlaud G, Valdivia K, Strominger JL, Ruocco MG, Chaouat G, and Klatzmann D

Subjects

Adoptive Transfer, Animals, Female, Flow Cytometry, Humans, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Neoplasms, Experimental immunology, Pregnancy, Reverse Transcriptase Polymerase Chain Reaction, Embryo Implantation immunology, Embryo, Mammalian immunology, Immune Tolerance immunology, Immunologic Memory immunology, T-Lymphocytes, Regulatory immunology

Abstract

Regulatory T cells (Tregs) play crucial roles in both fetal and tumor development. We recently showed that immunosurveillance by pre-existing CD44(high)CD62L(low) activated/memory Tregs (amTregs) specific for self-Ags protects emergent tumor cells in mice. This Treg response of a memory type is more rapid than and dominates the antitumor response of tumor-specific effector T cells. In this study, we report striking similarities between the early Treg responses to embryo and tumor implantation. Tregs are rapidly recruited to uterus-draining lymph nodes and activated in the first days after embryo implantation in both syngeneic and allogeneic matings; express the markers of the amTreg subset; and are at least in part self-Ag specific, as seen in tumor emergence. Unlike in the tumor emergence setting, however, for which preimmunization against tumor Ags is sufficient for complete tumor eradication even in the presence of Tregs, Treg depletion is additionally required for high frequencies of fetus loss after preimmunization against paternal tissue Ags. Thus, amTregs play a major role in protecting embryos in both naive and preimmune settings. This role and the ensuing therapeutic potential are further highlighted by showing that Treg stimulation, directly by low-dose IL-2 or indirectly by Fms-related tyrosine kinase 3 ligand, led to normal pregnancy rates in a spontaneous abortion-prone model.

Published

2013