Your search keyword '"Malina Xiao"' showing total 14 results

1. SNAI1-dependent upregulation of CD73 increases extracellular adenosine release to mediate immune suppression in TNBC

Author

Meriem Hasmim, Malina Xiao, Kris Van Moer, Akinchan Kumar, Alexandra Oniga, Michel Mittelbronn, Caroline Duhem, Anwar Chammout, Guy Berchem, Jean Paul Thiery, Marianna Volpert, Brett Hollier, Muhammad Zaeem Noman, and Bassam Janji

Subjects

CD73, SNAI1, epithelial-to-mesenchymal transition, adenosine, anti-tumor immune response, immunotherapy, Immunologic diseases. Allergy, RC581-607

Abstract

Triple-negative subtype of breast cancer (TNBC) is hallmarked by frequent disease relapse and shows highest mortality rate. Although PD-1/PD-L1 immune checkpoint blockades have recently shown promising clinical benefits, the overall response rate remains largely insufficient. Hence, alternative therapeutic approaches are warranted. Given the immunosuppressive properties of CD73-mediated adenosine release, CD73 blocking approaches are emerging as attractive strategies in cancer immunotherapy. Understanding the precise mechanism regulating the expression of CD73 is required to develop effective anti-CD73-based therapy. Our previous observations demonstrate that the transcription factors driving epithelial-to-mesenchymal transition (EMT-TF) can regulate the expression of several inhibitory immune checkpoints. Here we analyzed the role of the EMT-TF SNAI1 in the regulation of CD73 in TNBC cells. We found that doxycycline-driven SNAI1 expression in the epithelial -like TNBC cell line MDA-MB-468 results in CD73 upregulation by direct binding to the CD73 proximal promoter. SNAI1-dependent upregulation of CD73 leads to increased production and release of extracellular adenosine by TNBC cells and contributes to the enhancement of TNBC immunosuppressive properties. Our data are validated in TNBC samples by showing a positive correlation between the mRNA expression of CD73 and SNAI1. Overall, our results reveal a new CD73 regulation mechanism in TNBC that participates in TNBC-mediated immunosuppression and paves the way for developing new treatment opportunities for CD73-positive TNBC.

Published

2022

2. Targeting chronic lymphocytic leukemia with N-methylated thrombospondin-1–derived peptides overcomes drug resistance

Author

Elodie Pramil, Linda Herbi Bastian, Thomas Denèfle, Fariba Nemati, Malina Xiao, Eva Lardé, Karim Maloum, Damien Roos-Weil, Elise Chapiro, Magali Le Garff-Tavernier, Frédéric Davi, Didier Decaudin, Marika Sarfati, Florence Nguyen-Khac, Hélène Merle-Béral, Philippe Karoyan, and Santos A. Susin

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: Chronic lymphocytic leukemia (CLL), the most common adulthood leukemia in Western countries, is a very heterogeneous disease characterized by a peripheral accumulation of abnormal CD5+ B lymphocytes in the immune system. Despite new therapeutic developments, there remains an unmet medical need for CLL. Here, we demonstrate that the use of N-methylated thrombospondin-1 (TSP-1)–derived peptides is an efficient way to kill the malignant CLL cells, including those from high-risk individuals with poor clinical prognosis, del11q, del17p, 2p gain, or complex karyotype. PKT16, our hit N-methylated peptide, triggers the elimination of the leukemic cells, sparing the nontumor cells, including the hematopoietic precursors, and reduces the in vivo tumor burden of a CLL-xenograft mice model. A complementary analysis underscores the improved cytotoxic efficiency of PKT16 compared with the previously described TSP-1–derived probes, such as PKHB1. PKT16 elicits an original caspase-independent programmed necrotic mode of cell death, different from necroptosis or ferroptosis, implicating an intracellular Ca2+ deregulation that provokes mitochondrial damage, cell cycle arrest, and the specific death of the malignant CLL cells. The activation of the Gαi proteins and the subsequent drop of cyclic adenosine monophosphate levels and protein kinase A activity regulate this cytotoxic cascade. Remarkably, PKT16 induces the molecular hallmarks of immunogenic cell death, as defined by the calreticulin plasma membrane exposure and the release of adenosine triphosphate and high-mobility group box 1 protein from the dying CLL cells. Thus, PKT16 appears to be able to stimulate an anticancer in vivo immune response. Collectively, our results pave the way toward the development of an efficient strategy against CLL.

Published

2019

3. Targeting Cytoprotective Autophagy to Enhance Anticancer Therapies

Author

Malina Xiao, Alice Benoit, Meriem Hasmim, Caroline Duhem, Guillaume Vogin, Guy Berchem, Muhammad Zaeem Noman, and Bassam Janji

Subjects

autophagy, cancer resistance, chemotherapy, radiotherapy, targeted therapy, immunotherapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Autophagy is a highly regulated multi-step process that occurs at the basal level in almost all cells. Although the deregulation of the autophagy process has been described in several pathologies, the role of autophagy in cancer as a cytoprotective mechanism is currently well established and supported by experimental and clinical evidence. Our understanding of the molecular mechanism of the autophagy process has largely contributed to defining how we can harness this process to improve the benefit of cancer therapies. While the role of autophagy in tumor resistance to chemotherapy is extensively documented, emerging data point toward autophagy as a mechanism of cancer resistance to radiotherapy, targeted therapy, and immunotherapy. Therefore, manipulating autophagy has emerged as a promising strategy to overcome tumor resistance to various anti-cancer therapies, and autophagy modulators are currently evaluated in combination therapies in several clinical trials. In this review, we will summarize our current knowledge of the impact of genetically and pharmacologically modulating autophagy genes and proteins, involved in the different steps of the autophagy process, on the therapeutic benefit of various cancer therapies. We will also briefly discuss the challenges and limitations to developing potent and selective autophagy inhibitors that could be used in ongoing clinical trials.

Published

2021

4. Improving Cancer Immunotherapy by Targeting the Hypoxic Tumor Microenvironment: New Opportunities and Challenges

Author

Muhammad Zaeem Noman, Meriem Hasmim, Audrey Lequeux, Malina Xiao, Caroline Duhem, Salem Chouaib, Guy Berchem, and Bassam Janji

Subjects

hypoxia, HIF, tumor microenvironment, immune checkpoints, immunotherapy, autophagy, Cytology, QH573-671

Abstract

Initially believed to be a disease of deregulated cellular and genetic expression, cancer is now also considered a disease of the tumor microenvironment. Over the past two decades, significant and rapid progress has been made to understand the complexity of the tumor microenvironment and its contribution to shaping the response to various anti-cancer therapies, including immunotherapy. Nevertheless, it has become clear that the tumor microenvironment is one of the main hallmarks of cancer. Therefore, a major challenge is to identify key druggable factors and pathways in the tumor microenvironment that can be manipulated to improve the efficacy of current cancer therapies. Among the different tumor microenvironmental factors, this review will focus on hypoxia as a key process that evolved in the tumor microenvironment. We will briefly describe our current understanding of the molecular mechanisms by which hypoxia negatively affects tumor immunity and shapes the anti-tumor immune response. We believe that such understanding will provide insight into the therapeutic value of targeting hypoxia and assist in the design of innovative combination approaches to improve the efficacy of current cancer therapies, including immunotherapy.

Published

2019

5. CMTM6 and CMTM7: New leads for PD-L1 regulation in breast cancer cells undergoing EMT

Author

Malina Xiao, Caroline Duhem, Anwar Chammout, Guy Berchem, and Bassam Janji

Subjects

Epithelial-Mesenchymal Transition, MARVEL Domain-Containing Proteins, Humans, Breast Neoplasms, Female, Cell Biology, Chemokines, Molecular Biology, Biochemistry, B7-H1 Antigen, Myelin Proteins

Abstract

Programmed death-ligand 1 (PD-L1) expression has long been used as a biomarker to stratify patients with cancer who will benefit from anti-PD-1/PD-L1 immunotherapy. However, the use of PD-L1 as a biomarker to guide treatment decisions has recently been called into question due to its dynamic and heterogeneous expression within each tumor and among different tumors as well as during tumor cell plasticity. Therefore, understanding the molecular basis of PD-L1 expression would enable delineating its value as a reliable biomarker in the clinic. Here, we provide our perspective on the involvement of CMTM6 and CMTM7 as new lead candidates for the regulation of PD-L1 in breast tumors undergoing an epithelial to mesenchymal transition.

Published

2022

6. Epithelial to Mesenchymal Transition Regulates Surface PD-L1 via CMTM6 and CMTM7 Induction in Breast Cancer

Author

Meriem Hasmim, Brett G. Hollier, Tuan Zea Tan, Guy Berchem, Jean Paul Thiery, Kris Van Moer, Christine Gilles, Malina Xiao, Bassam Janji, Audrey Lequeux, and Muhammad Zaeem Noman

Subjects

0301 basic medicine, Cancer Research, snail1, Cell, Vimentin, lcsh:RC254-282, Article, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, breast cancer, PD-L1, medicine, Gene silencing, Epithelial–mesenchymal transition, skin and connective tissue diseases, Gene knockdown, biology, Chemistry, Mesenchymal stem cell, epithelial to mesenchymal transition, immune checkpoints, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, CMTM family, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research

Abstract

Simple Summary Epithelial to mesenchymal transition (EMT) is a mechanism endowing tumor cells with aggressive properties and escape immune surveillance. Here, we reported that activating EMT process in breast cancer cells upregulates CMTM6, an essential protein required for cell surface expression of PD-L1. In addition to CMTM6, our in silico data on triple negative breast cancer patients showed a positive correlation between EMT markers and two other members of CMTM family (CMTM3 and CMTM7). These results were validated in EMT-inducible MCF-7 model that exhibited a downregulation of cell surface expression of PD-L1 by dual targeting CMTM6 and CMTM7. Considering the prominent role of PD-L1 in tumor immune evasion, our study provides an additional clue on how PD-L1 is regulated in aggressive breast cancer cells and pave the way to assess the therapeutic benefit of EMT inhibitors in combination with anti PD-L1 blockade in highly aggressive breast cancer patients. Abstract CMTM6 is a critical regulator of cell surface expression of PD-L1 in tumor cells, but little is known about the transcriptional regulation of CMTM6. Here we report that the expression of CMTM6 positively correlates with the epithelial to mesenchymal transition (EMT) score in breast cancer cell lines and with the major EMT marker Vimentin in triple-negative breast cancers (TNBC). We showed that CMTM6 is concomitantly overexpressed with PD-L1 in breast mesenchymal compared with the epithelial cells. Driving a mesenchymal phenotype in SNAI1-inducible MCF-7 cells (MCF-7Mes cells) increased both PD-L1 and CMTM6. CMTM6 silencing in MCF-7Mes cells partially reduced cell surface expression of PD-L1, indicating that a proportion of the PD-L1 on the surface of MCF-7Mes cells depends on CMTM6. We also found a positive correlation between CMTM3 and CMTM7 expression with EMT score in breast cancer cells, and with Vimentin in TNBC patients. Dual knockdown of CMTM6 and CMTM7 significantly decreased PD-L1 surface expression in MCF-7Mes cells, indicating that both CMTM6 and CMTM7 regulate the expression of PD-L1. This study highlights the importance of CMTM6 and CMTM7 in EMT-induced PD-L1 and suggests that EMT, CMTM6 or CMTM7 modulators can be combined with anti-PD-L1 in patients with highly aggressive breast cancer.

Published

2021

7. Targeting HIF-1 alpha transcriptional activity drives cytotoxic immune effector cells into melanoma and improves combination immunotherapy

Author

Kris Van Moer, Tsolere Arakelian, Meriem Hasmim, Salem Chouaib, Manon Bosseler, Alice Benoit, Audrey Lequeux, Bassam Janji, Muhammad Zaeem Noman, Guy Berchem, Elodie Viry, and Malina Xiao

Subjects

0301 basic medicine, Cancer microenvironment, Cancer Research, medicine.medical_treatment, T cell, Cancer immunotherapy, Biology, Brief Communication, Cancer Vaccines, 03 medical and health sciences, 0302 clinical medicine, Immune system, Blocking antibody, Genetics, medicine, Cytotoxic T cell, Molecular Biology, Melanoma, Tumor microenvironment, Immunotherapy, medicine.disease, Cancer therapeutic resistance, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Vaccines, Subunit, Cancer research, Tumour immunology

Abstract

Hypoxia is a key factor responsible for the failure of therapeutic response in most solid tumors and promotes the acquisition of tumor resistance to various antitumor immune effectors. Reshaping the hypoxic immune suppressive tumor microenvironment to improve cancer immunotherapy is still a relevant challenge. We investigated the impact of inhibiting HIF-1α transcriptional activity on cytotoxic immune cell infiltration into B16-F10 melanoma. We showed that tumors expressing a deleted form of HIF-1α displayed increased levels of NK and CD8+effector T cells in the tumor microenvironment, which was associated with high levels of CCL2 and CCL5 chemokines. We showed that combining acriflavine, reported as a pharmacological agent preventing HIF-1α/HIF-1β dimerization, dramatically improved the benefit of cancer immunotherapy based on TRP-2 peptide vaccination and anti-PD-1 blocking antibody. In melanoma patients, we revealed that tumors exhibiting high CCL5 are less hypoxic, and displayed high NK, CD3+, CD4+and CD8+T cell markers than those having low CCL5. In addition, melanoma patients with high CCL5 in their tumors survive better than those having low CCL5. This study provides the pre-clinical proof of concept for a novel triple combination strategy including blocking HIF-1α transcription activity along vaccination and PD-1 blocking immunotherapy.

Published

2020

8. Inhibition of Vps34 reprograms cold into hot inflamed tumors and improves anti–PD-1/PD-L1 immunotherapy

Author

Muhammad Zaeem Noman, Angelo De Milito, Meriem Hasmim, Martin Andersson, Ravi K. Amaravadi, Malina Xiao, Yasmin Yu, Jenny Viklund, Guy Berchem, Santiago Parpal, Kris Van Moer, Jessica Martinsson, and Bassam Janji

Subjects

0303 health sciences, Tumor microenvironment, Multidisciplinary, biology, business.industry, Melanoma, medicine.medical_treatment, Immunotherapy, medicine.disease, CCL5, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, PD-L1, Cancer research, medicine, biology.protein, CXCL10, Kinase activity, business, CD8, 030304 developmental biology

Abstract

One of the major challenges limiting the efficacy of anti–PD-1/PD-L1 therapy in nonresponding patients is the failure of T cells to penetrate the tumor microenvironment. We showed that genetic or pharmacological inhibition of Vps34 kinase activity using SB02024 or SAR405 (Vps34i) decreased the tumor growth and improved mice survival in multiple tumor models by inducing an infiltration of NK, CD8+, and CD4+ T effector cells in melanoma and CRC tumors. Such infiltration resulted in the establishment of a T cell−inflamed tumor microenvironment, characterized by the up-regulation of pro-inflammatory chemokines and cytokines, CCL5, CXCL10, and IFNγ. Vps34i treatment induced STAT1 and IRF7, involved in the up-regulation of CCL5 and CXCL10. Combining Vps34i improved the therapeutic benefit of anti–PD-L1/PD-1 in melanoma and CRC and prolonged mice survival. Our study revealed that targeting Vps34 turns cold into hot inflamed tumors, thus enhancing the efficacy of anti–PD-L1/PD-1 blockade.

Published

2020

9. The emerging impact of autophagy on the antitumor immune response

Author

Muhammad Zaeem Noman, Guy Berchem, Malina Xiao, Meriem Hasmim, Elodie Viry, Bassam Janji, and C. Duhem

Subjects

Immune system, Tumor Escape, law, Autophagy, Regulator, Cancer research, Cytotoxic T cell, Suppressor, Biology, Immune cell infiltration, Homeostasis, law.invention

Abstract

Macroautophagy (hereafter referred to as autophagy) is a cellular degradation process involved in the recycling of damaged organelles and proteins. Occurring at the basal level, autophagy participates in maintaining homeostasis in all cells. Deregulation in this process is observed in several pathologies such as cancer. Autophagy plays a dual role as tumor suppressor or tumor promoter. Such a dual role of autophagy relies on the type, the stage, and the genetic context of the tumor. In well-established tumors, autophagy operates as a mechanism maintaining the survival of tumor cells and inducing their resistance to different anticancer therapies. Emerging new data highlight the involvement of autophagy in modulating tumor cell susceptibility to immune cell-mediated killing by various overlapping mechanisms. Tumoral autophagy is also described as a regulator of immune cell infiltration into the tumor bed. These data inspired substantial attention to develop selective autophagy inhibitors that can be used as new approaches to restore tumor immune surveillance in the context of cancer immunotherapies. This chapter will recapitulate recent findings on how autophagy activation allows tumor escape from cytotoxic immune cells and regulation of intra-tumoral infiltration by immune components. We are now facing a major challenge to develop drugs selectively inhibiting the autophagic process that can be used in combination with current cancer immunotherapeutic approaches.

Published

2020

10. Contributors

Author

Pascale Adami, Olivier Adotévi, Lionel Apetoh, Alvaro Baeza Garcia, Bruce Baguley, Guy Berchem, Benjamin Bonavida, Gilles Boschetti, Giulio Cavalli, Simone Cenci, Sandy Chen, Salem Chouaib, I.A. Ciechomska, S. Cyranowski, Malgorzata Czystowska, Régis Delage-Mourroux, Sushil Dhakal, Caroline Duhem, Agnete S.T. Engelsen, Mathias Faure, Leïla Fonderflick, Michaël Guittaut, Meriem Hasmim, Elise Jacquin, Bassam Janji, B. Kaminska, James B. Lorens, Maria Lie Lotsberg, Stephane Nancey, Muhammad Zaeem Noman, Aurore Rozières, Jerome Thiery, Christophe Viret, Elodie Viry, Theresa L. Whiteside, Valerie R. Wiersma, and Malina Xiao

Published

2020

11. Driving Cytotoxic Natural Killer Cells into Melanoma: If CCL5 Plays the Music, Autophagy Calls the Shots

Author

Markus Ollert, Malina Xiao, Martyna Szpakowska, Bassam Janji, Ludovic Ménard, Andy Chevigné, Muhammad Zaeem Noman, Manon Bosseler, and Guy Berchem

Subjects

Cytotoxicity, Immunologic, 0301 basic medicine, Cancer Research, Cell type, Autophagy-Related Proteins, Antineoplastic Agents, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, Autophagy, medicine, Animals, Humans, Cytotoxic T cell, Molecular Targeted Therapy, Chemokine CCL5, Melanoma, Tumor microenvironment, Adipogenesis, business.industry, Chloroquine, medicine.disease, Immunity, Innate, Gene Expression Regulation, Neoplastic, Killer Cells, Natural, 030104 developmental biology, Tumor progression, Cancer cell, Cancer research, Signal transduction, business, Biomarkers, Hydroxychloroquine, Signal Transduction

Abstract

Autophagy is a quality control process executed at the basal level in almost all cell types. However, in cancer cells, autophagy is activated by several stimuli, including hypoxia. Depending on tumor type, stage, and genetic context, autophagy is a double-edged sword. Autophagy promotes regression in newly established tumors; however, it supports tumor progression in well-established tumors by maintaining cancer cell survival under stress conditions. These data, in addition to the emerging role of autophagy in impairing antitumor immunity, have attracted significant interest in developing autophagy inhibitors as a new approach to cancer treatment. The enthusiasm for developing selective drugs inhibiting autophagy has been seriously challenged by the discovery that most autophagy-related proteins display nonautophagic functions. Autophagy inhibitors chloroquine and hydroxychloroquine are currently being investigated in several clinical trials in combination with standard anticancer therapies. Here, we provide a brief overview on the nonautophagic function of autophagy-related proteins and summarize the major mechanisms whereby autophagy modulation could positively or negatively impact cancer therapies. We also focus on the emerging role of targeting autophagy in the improvement of NK-mediated antitumor immunity through the regulation of CCL5 and its receptors' expression in melanoma, and we provide some clues revealing how autophagy modulators could be exploited to improve cancer immunotherapies.

Published

2018

12. Targeting chronic lymphocytic leukemia with N-methylated thrombospondin-1–derived peptides overcomes drug resistance

Author

Frederic Davi, Malina Xiao, Thomas Denèfle, Philippe Karoyan, Eva Lardé, Florence Nguyen-Khac, Santos A. Susin, Elise Chapiro, H. Merle-Beral, Damien Roos-Weil, Fariba Nemati, Karim Maloum, Didier Decaudin, Elodie Pramil, Magali Le Garff-Tavernier, Marika Sarfati, Linda Herbi Bastian, Centre de Recherche des Cordeliers (CRC (UMR_S_1138 / U1138)), École pratique des hautes études (EPHE), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Université Paris Diderot - Paris 7 (UPD7)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), Sorbonne Université (SU), Université Sorbonne Paris Cité (USPC), Université Paris Descartes - Paris 5 (UPD5), Université Paris Diderot - Paris 7 (UPD7), Laboratoire des biomolécules (LBM UMR 7203), Centre National de la Recherche Scientifique (CNRS)-Sorbonne Université (SU)-Département de Chimie - ENS Paris, École normale supérieure - Paris (ENS Paris), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-École normale supérieure - Paris (ENS Paris), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Chimie Moléculaire de Paris Centre (FR 2769), Institut de Chimie du CNRS (INC)-École normale supérieure - Paris (ENS Paris), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Ecole Nationale Supérieure de Chimie de Paris - Chimie ParisTech-PSL (ENSCP), Université Paris sciences et lettres (PSL)-Ecole Superieure de Physique et de Chimie Industrielles de la Ville de Paris (ESPCI Paris), Université Paris sciences et lettres (PSL)-Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Ecole Nationale Supérieure de Chimie de Paris - Chimie ParisTech-PSL (ENSCP), Université Paris sciences et lettres (PSL)-Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut Curie [Paris], Service d'Hématologie Biologique [CHU Pitié-Salpêtrière], CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Service d'Hématologie clinique [CHU Pitié-Salpêtrière], Centre Hospitalier de l'Université de Montréal (CHUM), Université de Montréal (UdeM), École pratique des hautes études (EPHE)-Université Paris Diderot - Paris 7 (UPD7)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), Chimie Moléculaire de Paris Centre (FR 2769), École normale supérieure - Paris (ENS Paris)-Université Pierre et Marie Curie - Paris 6 (UPMC)-Ecole Nationale Supérieure de Chimie de Paris- Chimie ParisTech-PSL (ENSCP)-ESPCI ParisTech-Centre National de la Recherche Scientifique (CNRS)-École normale supérieure - Paris (ENS Paris)-Université Pierre et Marie Curie - Paris 6 (UPMC)-Ecole Nationale Supérieure de Chimie de Paris- Chimie ParisTech-PSL (ENSCP)-ESPCI ParisTech-Centre National de la Recherche Scientifique (CNRS)-Département de Chimie - ENS Paris, École normale supérieure - Paris (ENS Paris)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Institut Curie, Assistance publique - Hôpitaux de Paris (AP-HP) (APHP)-CHU Pitié-Salpêtrière [APHP], and Service d'Hématologie Clinique [CHU Pitié-Salpêtrière]

Subjects

Models, Molecular, Necroptosis, Chronic lymphocytic leukemia, [SDV]Life Sciences [q-bio], Antineoplastic Agents, Apoptosis, medicine.disease_cause, Thrombospondin 1, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, hemic and lymphatic diseases, Cell Line, Tumor, medicine, Cyclic AMP, Cytotoxic T cell, Animals, Humans, 030304 developmental biology, 0303 health sciences, Lymphoid Neoplasia, Cell Death, Chemistry, Molecular Mimicry, [SDV.MHEP.HEM]Life Sciences [q-bio]/Human health and pathology/Hematology, Hematology, Cell Cycle Checkpoints, medicine.disease, Cyclic AMP-Dependent Protein Kinases, Leukemia, Lymphocytic, Chronic, B-Cell, Xenograft Model Antitumor Assays, 3. Good health, Mitochondria, Molecular mimicry, Leukemia, Disease Models, Animal, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Caspases, Cancer research, Immunogenic cell death, Female, CD5, Peptides, Signal Transduction

Abstract

International audience; Chronic lymphocytic leukemia (CLL), the most common adulthood leukemia in Western countries, is a very heterogeneous disease characterized by a peripheral accumulation of abnormal CD5+ B lymphocytes in the immune system. Despite new therapeutic developments, there remains an unmet medical need for CLL. Here, we demonstrate that the use of N-methylated thrombospondin-1 (TSP-1)-derived peptides is an efficient way to kill the malignant CLL cells, including those from high-risk individuals with poor clinical prognosis, del11q, del17p, 2p gain, or complex karyotype. PKT16, our hit N-methylated peptide, triggers the elimination of the leukemic cells, sparing the nontumor cells, including the hematopoietic precursors, and reduces the in vivo tumor burden of a CLL-xenograft mice model. A complementary analysis underscores the improved cytotoxic efficiency of PKT16 compared with the previously described TSP-1-derived probes, such as PKHB1. PKT16 elicits an original caspase-independent programmed necrotic mode of cell death, different from necroptosis or ferroptosis, implicating an intracellular Ca2+ deregulation that provokes mitochondrial damage, cell cycle arrest, and the specific death of the malignant CLL cells. The activation of the Gαi proteins and the subsequent drop of cyclic adenosine monophosphate levels and protein kinase A activity regulate this cytotoxic cascade. Remarkably, PKT16 induces the molecular hallmarks of immunogenic cell death, as defined by the calreticulin plasma membrane exposure and the release of adenosine triphosphate and high-mobility group box 1 protein from the dying CLL cells. Thus, PKT16 appears to be able to stimulate an anticancer in vivo immune response. Collectively, our results pave the way toward the development of an efficient strategy against CLL.

Published

2019

13. Impact of hypoxic tumor microenvironment and tumor cell plasticity on the expression of immune checkpoints

Author

Irene Bocci, Malina Xiao, Kris Van Moer, Delphine Sauvage, Meriem Hasmim, Bassam Janji, Guy Berchem, Muhammad Zaeem Noman, Manon Bosseler, Audrey Lequeux, and Elodie Viry

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, Cell Plasticity, Tumor cells, CD47 Antigen, Bioinformatics, B7-H1 Antigen, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antineoplastic Agents, Immunological, Cancer immunotherapy, Neoplasms, Tumor Microenvironment, Medicine, Animals, Humans, In patient, Epithelial–mesenchymal transition, Hypoxic tumor, business.industry, Hypoxia (medical), Immune checkpoint, Cell Hypoxia, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, medicine.symptom, business

Abstract

Compared to traditional therapies, such as surgery, radio-chemotherapy, or targeted approaches, immunotherapies based on immune checkpoint blockers (ICBs) have revolutionized the treatment of cancer. Although ICBs have yielded long-lasting results and have improved patient survival, this success has been seriously challenged by clinical observations showing that only a small fraction of patients benefit from this revolutionary therapy and no benefit has been found in patients with highly aggressive tumors. Efforts are currently ongoing to identify factors that predict the response to ICB. Among the different predictive markers established so far, the expression levels of immune checkpoint genes have proven to be important biomarkers for informing treatment choices. Therefore, understanding the mechanisms involved in the regulation of immune checkpoints is a key element that will facilitate novel combination approaches and optimize patient outcome. In this review, we discuss the impact of hypoxia and tumor cell plasticity on immune checkpoint gene expression and provide insight into the therapeutic value of the EMT signature and the rationale for novel combination approaches to improve ICB therapy and maximize the benefits for patients with cancer.

Published

2018

14. CXCL10 Is an Agonist of the CC Family Chemokine Scavenger Receptor ACKR2/D6

Author

Andy Chevigné, Giulia D’uonnolo, Martyna Szpakowska, Muhammad Zaeem Noman, Tomasz Uchański, Malina Xiao, Markus Ollert, Yong Jun Kwon, Guy Berchem, Max Marc Roger Meyrath, Bassam Janji, and Nathan Reynders

Subjects

ACKR3, 0301 basic medicine, Agonist, ACKR2, Cancer Research, Chemokine, medicine.drug_class, IP-10, DPP4, CXCR3, lcsh:RC254-282, Scavenger, 03 medical and health sciences, Chemokine receptor, 0302 clinical medicine, medicine, CXCL10, Scavenger receptor, scavenger, CD26, biology, Chemistry, Brief Report, NanoBRET, hemic and immune systems, CXCL12, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, CXCL2, Ligand (biochemistry), NanoBiT, Cell biology, IP‐10, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, D6

Abstract

Simple Summary The atypical chemokine receptor ACKR2 plays an important role in the tumour microenvironment. It has long been considered as a scavenger of inflammatory chemokines exclusively from the CC family. In this study, we identified the CXC chemokine CXCL10 as a new strong agonist ligand for ACKR2. CXCL10 is known to drive the infiltration of immune cells into the tumour bed and was previously reported to bind to CXCR3 only. We demonstrated that ACKR2 acts as a scavenger reducing the availability of CXCL10 for CXCR3. Our study sheds new light on the complexity of the chemokine network and the potential role of CXCL10 regulation by ACKR2 in tumour immunology. Abstract Atypical chemokine receptors (ACKRs) are important regulators of chemokine functions. Among them, the atypical chemokine receptor ACKR2 (also known as D6) has long been considered as a scavenger of inflammatory chemokines exclusively from the CC family. In this study, by using highly sensitive β-arrestin recruitment assays based on NanoBiT and NanoBRET technologies, we identified the inflammatory CXC chemokine CXCL10 as a new strong agonist ligand for ACKR2. CXCL10 is known to play an important role in the infiltration of immune cells into the tumour bed and was previously reported to bind to CXCR3 only. We demonstrated that ACKR2 is able to internalize and reduce the availability of CXCL10 in the extracellular space. Moreover, we found that, in contrast to CC chemokines, CXCL10 activity towards ACKR2 was drastically reduced by the dipeptidyl peptidase 4 (DPP4 or CD26) N-terminal processing, pointing to a different receptor binding pocket occupancy by CC and CXC chemokines. Overall, our study sheds new light on the complexity of the chemokine network and the potential role of CXCL10 regulation by ACKR2 in many physiological and pathological processes, including tumour immunology. Our data also testify that systematic reassessment of chemokine-receptor pairing is critically needed as important interactions may remain unexplored.

Published

2021