Auswahl der wissenschaftlichen Literatur zum Thema „Checkpoint immunitaire“
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Zeitschriftenartikel zum Thema "Checkpoint immunitaire"
Chaudot, F., P. Sève, A. Rousseau, M. Alexandre, P. Fournie, P. Lozac’h, J. Keraen et al. „Inflammation oculaire induite par les inhibiteurs du checkpoint immunitaire“. La Revue de Médecine Interne 43 (Dezember 2022): A488. http://dx.doi.org/10.1016/j.revmed.2022.10.254.
Der volle Inhalt der QuelleKostine, Marie, Aurélien Marabelle, Thierry Schaeverbeke und Maria Kfoury. „Les limites des inhibiteurs de points de contrôle immunitaire et la gestion de leur toxicité“. médecine/sciences 35, Nr. 12 (Dezember 2019): 949–56. http://dx.doi.org/10.1051/medsci/2019191.
Der volle Inhalt der QuellePouchelon, C. A., V. Afanasiev, S. Evrard, M. Tchikviladzé, B. Lapergue, F. Bourdain und A. Wang. „Myasthénie auto-immune induite par le nivolumab, un inhibiteur de checkpoint immunitaire“. Pratique Neurologique - FMC 11, Nr. 1 (Februar 2020): 39–43. http://dx.doi.org/10.1016/j.praneu.2019.10.005.
Der volle Inhalt der QuelleGefard-Gontier, E., R. Markich, S. Prey, C. Dutriaux, E. Gerard, L. Dousset, A. Pham-Ledard et al. „Évolution des métastases osseuses chez les patients traités par inhibiteurs de checkpoint immunitaire“. Revue du Rhumatisme 88 (Dezember 2021): A67. http://dx.doi.org/10.1016/j.rhum.2021.10.104.
Der volle Inhalt der QuelleGuérin, C., M. Laramas, A. Bocquet, L. Bouillet und A. C. Toffart. „Profil de tolérance des inhibiteurs de checkpoint immunitaire selon le type de cancer“. La Revue de Médecine Interne 43 (Dezember 2022): A336. http://dx.doi.org/10.1016/j.revmed.2022.10.030.
Der volle Inhalt der QuelleCottu, A., L. Delaval, A. Forestier, A. Tomelleri, C. Campochiaro, M. Bond, J. Dion et al. „Vascularite des gros vaisseaux associées aux inhibiteurs de checkpoint immunitaire : étude rétrospective multicentrique“. La Revue de Médecine Interne 45 (Juni 2024): A66—A67. http://dx.doi.org/10.1016/j.revmed.2024.04.351.
Der volle Inhalt der QuelleTzoumpa, S., B. Villette, C. Dutriaux, G. Jeudy, V. Tafani, A. Memmi, M. Saint-Jean, C. Nardin, Y. Le Corre und E. Maubec. „Sinusites induites par les inhibiteurs de checkpoint immunitaire : une série française de 12 cas“. Annales de Dermatologie et de Vénéréologie - FMC 2, Nr. 8 (November 2022): A77—A78. http://dx.doi.org/10.1016/j.fander.2022.09.080.
Der volle Inhalt der QuelleDuruisseaux, Michaël, Cécile Lize-Dufranc, Céline Badoual und Frédéric Bibeau. „Biomarqueurs prédictifs de l’efficacité des inhibiteurs de checkpoint immunitaire dans le traitement des cancers“. Annales de Pathologie 37, Nr. 1 (Februar 2017): 46–54. http://dx.doi.org/10.1016/j.annpat.2016.12.016.
Der volle Inhalt der QuelleLenfant, Louis, und Morgan Rouprêt. „Immunothérapie et cancer de la vessie : état des connaissances actuelles et perspectives futures“. Biologie Aujourd'hui 212, Nr. 3-4 (2018): 81–84. http://dx.doi.org/10.1051/jbio/2018028.
Der volle Inhalt der QuelleFrançois, Stéphanie, Daniela Lakomy und Nicole Fabien. „Place du laboratoire d’auto-immunité au cours des traitements par les inhibiteurs de checkpoint immunitaire“. Revue Francophone des Laboratoires 2022, Nr. 542 (Mai 2022): 63–69. http://dx.doi.org/10.1016/s1773-035x(22)00179-4.
Der volle Inhalt der QuelleDissertationen zum Thema "Checkpoint immunitaire"
Soussan, Sarah. „B lymphocytes and autoantibodies in immune-related adverse events following immune checkpoint inhibitors in cancer patients“. Electronic Thesis or Diss., Sorbonne université, 2024. https://accesdistant.sorbonne-universite.fr/login?url=https://theses-intra.sorbonne-universite.fr/2024SORUS022.pdf.
Der volle Inhalt der QuelleImmune checkpoints inhibitors (ICI) have revolutionized the treatment of previously incurable malignancies. Unfortunately, the use of ICI also induces a bystander breakdown of peripheral tolerance leading to immune related Adverse Events (irAEs) in 30-90% of treated patients, drastically reducing quality of life and requiring therapy dose reduction or discontinuation. As ICI directly target T cells, they have been considered the main culprit for irAEs. Nevertheless, T cells cannot fully explain adverse events, and the role of B cells and their associated mechanisms have not been characterized. We therefore studied the involvement of peripheral B-cell compartment in irAEs, using both phenotypic and functional approaches, in two cohorts of solid cancer patients treated with anti-PD-1 and/or anti-CTLA-4 monoclonal antibodies. Deep phenotyping of B-cell subsets throughout the treatment and at the onset of irAEs has been performed by multi-parametric spectral flow cytometry. Subsequently, to analyze the functions of B-cell subsets, notably their ability to produce antibodies, we set-up a B-cell culture system allowing in vitro differentiation of B cells into antibody-secreting cells. This gave us the opportunity to analyze the antibody production by circulating B cells and their association with irAEs occurence. The screening of circulating B cells phenotype and function was conducted alongside the evaluation of the serum and plasma reactivity of cancer patients by complementary approaches (ELISA, Western Blot, Immunofluorescence assays). We found that, before treatment, patients that develop ICI-induced irAEs exhibit a significantly lower expression on B cell subsets of the FcγRIIB, CD85j and LAIR-1 inhibitory receptors in melanoma patients and higher expression of the CD95 and CXCR5, respectively activating and lymphoid organs re-circulatory markers in lung cancer patients. In addition, increased in baseline abundance of hyper-activated IgD- memory B cell subset or plasmablasts precursor were observed in patients that will undergo irAEs. Moreover, a part of irAEs patients exhibit baseline or ICI-induce circulating autoantibodies which could be directed against the related tissue of irAEs occurrence. Indeed, patients experiencing cardiac/muscular irAEs demonstrated autoantibodies directed against cardiac tissues and well-defined cardiac/muscle antigens. Finally, IgG derived from cardiac/muscular irAEs patients bound to human cardiomyocytes and perturbed the calcium kinetic and the contractibility of cardiac spheroids. These findings highlight a predisposition of irAEs incidence in patients with baseline highly activated and differentiated circulating B cells associated with autoantibody production. Overall, these results support the potential role of the humoral adaptative immunity in the mechanisms of ICI-induced irAEs
Dal, Cin Julian. „Analyse tissulaire des myopathies inflammatoires idiopathiques et induites par immune-checkpoint-inhibitor : apport des nouvelles approches transcriptomiques“. Electronic Thesis or Diss., Sorbonne université, 2023. https://accesdistant.sorbonne-universite.fr/login?url=https://theses-intra.sorbonne-universite.fr/2023SORUS151.pdf.
Der volle Inhalt der QuelleMyositis are a heterogeneous group of autoimmune pathologies characterized by muscle damage in patients. Myositis are separated into 5 subgroups: dermatomyositis (DM), anti-synthetase syndromes (ASyS), inclusion body myositis (IBM), autoimmune necrotizing myopathies (IMNM) and immune-checkpoint inhibitor (ICI)-induced myositis. The pathophysiological mechanisms, clinical phenotype and prognosis of each subgroup are different. Among myositis, this work focused on IMNM and ICI-induced myositis, which have the poorest prognosis. High-resolution, spatial and single-cell transcriptomic studies have made it possible to study the muscle tissue of patients with these myositis. In ICI-induced myositis, these studies have confirmed the cytotoxicity of CD8 T cells and their central role, mainly of a population of resident memory T cells identified in the muscle, as well as macrophages. We propose a pathogenic model based on the reaction of resident memory T cells to ICI treatments. In IMNM, subgroups of macrophages have been identified composed respectively of pro-inflammatory macrophages, anti-inflammatory macrophages, and macrophages close to fibro-adipogenic progenitors (FAP). We propose that necrosis can stimulate macrophages and induce their recruitment, which would allow the proliferation of FAPs at the origin of exacerbated fibrosis in patients. Understanding mechanisms among others makes it possible to consider new therapeutic targets and improve patient prognosis
Tannous, Désirée. „The combination of Gadolinium-based nanoparticles, radiotherapy and immune checkpoint inhibitors : a novel therapeutic opportunity for cancer treatment“. Thesis, université Paris-Saclay, 2022. http://www.theses.fr/2022UPASL082.
Der volle Inhalt der QuelleScientific discoveries linked to radiotherapy are in continuous progress and almost 60% of cancer diagnosed patients are treated with radiotherapy. However, radiation therapy still faces many limitations due to radioresistance and the side effects inflected on healthy tissues. To overcome these factors, a particular interest has been aroused on the role that nanomedicine could play in the improvement of immune-mediated anti-tumor response. In this context, we decided to assess the ability of the combination of Gadolinium nanoparticles (AGuIX) with ionizing radiation (IR) to stimulate an anti-tumor immunological response and to increase the effectiveness of radiotherapy combined to immune checkpoint blockers.AGuIX are very small nanoparticles composed of a polysiloxane matrix and gadolinium chelates. Thanks to the magnetic properties of gadolinium, these nanoparticles play the role of a contrast agent, in addition to its radiosensitizing properties, thus allowing a better targeting and an enhanced therapeutic index.Our work reveals the ability of the AGuIX+IR combination to induce genomic instability and to stimulate immunomodulatory cell signaling pathways in treated human and murine cancer cells. In parallel, we demonstrate the anti-tumor activity of this combination by assessing tumor growth and overall survival using a preclinical model of immunocompetent mice bearing tumors. Our results strongly demonstrate a synergistic effect of AGuIX + IR combination on tumor growth and overall survival by stimulating the immune system. Finally, we reveal the capacity of AGuIX + IR combination to overcome immune checkpoint blockers resistance.In conclusion, our work shows that the combination of AGuIX+IR stimulates immunomodulatory signaling pathways, induces a strong synergistic anti-tumor response and helps overcoming resistance to immunotherapies
Nougue, Manon. „Rôle immunomodulateur du système lymphatique lors du développement tumoral mammaire“. Electronic Thesis or Diss., Toulouse 3, 2023. http://www.theses.fr/2023TOU30261.
Der volle Inhalt der QuelleThe lymphatic system is a unidirectional vascular network transporting lymph, enabling drainage of interstitial fluids, transport of intestinal lipids, and also immune monitoring and tolerance. Nevertheless, the lymphatic system is involved in many pathologies, and particularly in tumor progression. Indeed, the lymphatic system promotes the metastatic spread, carried by lymphatic vessels to distant organs. More recently, the lymphatic system has been identified as a key regulator of immune responses during tumor development. The immune system is essential for tumor detection and establishment of anti-tumor lymphocyte responses. However, at advanced stages of tumor development, immune escape mechanisms are established in favor of tumor growth. These mechanisms are mediated not only by tumors themselves, but also by various players in the tumor environment. The lymphatic system is one of these players, particularly found in breast tumor environment. Advanced-stage breast adenocarcinomas respond to immunotherapies that target immune checkpoints responsible for immune escape. Indeed, the lymphatic system potentiates tumor response to these immunotherapies, playing a dual role in immunomodulation in the tumor context. Lymphatic vessels are able to recruit T cells to the tumor site to stimulate anti-tumor immune surveillance, but are also able to generate T cell immunosuppressive mechanisms through the expression of immune checkpoints. During my thesis, I therefore studied immunomodulatory mechanisms of the lymphatic system during mammary tumor development. I observed that the lymphatic system controls a switch from immune surveillance to immunosuppression, particularly induced by ligands of TIGIT immune checkpoint. I have shown that activation of tumor lymphatic vessels leads to overexpression of Nectin-2, which inhibits T cells overexpressing TIGIT. This in turn reduces cytotoxic CD8+ T cell responses to promote tumor growth
Miloro, Giorgia. „Déterminer le rôle du récepteur de mort Fas/CD95 dans la co-stimulation des cellules T“. Electronic Thesis or Diss., Université Côte d'Azur, 2020. http://www.theses.fr/2020COAZ6036.
Der volle Inhalt der QuelleFas (CD95/TNFRSF6), a type-I transmembrane receptor of the tumor necrosis factor receptor (TNFR) superfamily, is a well-known cell death activator. However, it has been also implicated in non-cell death processes including cell survival, differentiation, migration. Whereas the molecular cascade that initiates apoptosis upon Fas engagement with its ligand FasL is particularly well described, the informations concerning the molecular mechanisms underlying the Fas mediated non-apoptotic pathways are sparse.As indicated by the induction of autoimmunity and lymphoproliferation in ALPS patients harboringmutations in either the receptor or its ligand, the Fas/FasL system plays a major role in T cell immune homeostasis and thus, in the control of autoimmunity and cancer. On one side, the Fas mediated death has been described critical for (i) the deletion of autoreactive lymphocytes, and thus in the maintenance of peripheral tolerance; (ii) the control of the number of lymphocytes activated by weak antigens during pathogen infections.On the other side, and beyond cell death induction, some Fas non-death pathways have been described in T cells, among which the role of Fas as co-regulatory receptor for the TCR during its activation. Despite the potential importance of this role in immunotherapeutic strategies, only few and controversial studies related to this involvement were done. Indeed, whereas several studies have described Fas as a TCR co-stimulatory receptor, others defined an inhibition of T cell activation by Fas-TCR concomitant stimulation. In this context, the aim of my PhD project consisted into molecularly dissect the Fas-TCR co-signaling.By using both primary T cells and cell lines bearing a specific transgenic TCR, we could define Fas as a costimulatory receptor. By exploiting biochemical approaches as well as flow cytometry and microscopy we could decipher the Fas-TCR crosstalk both at functional and molecular level. First, we show that Fas-TCR costimulation occurs in both naïve and in memory T cells as well as in both CD4+ and CD8+ T cell subpopulations.Molecularly, we could describe that Fas enhances the TCR signaling at membrane proximal level, since the phosphorylation of the first proteins involved in TCR activation is increased. Furthermore, both membrane-bound and soluble FasL are capable to initiate Fas co-stimulatory signal. Lastly, we could exclude the involvement of FADD and Caspase-8, first actors of Fas signaling, in the co-activation, and even more importantly, the involvement of the death domain of Fas cytoplasmic tail, unveiling the implication of another Fas receptor domain. To describe the molecular mechanisms and the context where Fas-TCR co-stimulation occurs might be of an outstanding importance in the comprehension of Fas physiopathology in T cells and for future studies that might involve its potential for immunotherapeutic strategies
Dupaty, Léa. „Evaluation in vivo de protéines immunorégulatrices dérivées de CTLA-4 et de PD-L1 pour leur capacité à inhiber les réponses immunitaires dans le contexte de la thérapie génique musculaire par AAV“. Thesis, Normandie, 2018. http://www.theses.fr/2018NORMR133/document.
Der volle Inhalt der QuelleGene therapy consist into introducing genetic material into cells to treat genetic disorders. Most gene therapies use viral vectors to carry the gene within target cells. In case of monogenic disorders, adeno-associated viruses (AAV) has become a vector of choice because of its lack of pathogenicity, its large tropism and its capacity to transduce quiescent cells. The use of AAV is approved in Europe to treat a rare lysosomal storage disease and has recently been approved by the FDA to treat a genetic cause of blindness. However, most clinical trials face immune responses directed against AAV components which may be highly immunogenic. This deleterious immunogenicity often lead to the trial failure. In addition, transgenic protein can also be immunogenic, aimaing to the destruction of transduced cells and ultimatly to gene therapy failure. In clinic, immunosuppressive drug remain the only option to counteract unwanted immune responses. These drugs possess infectious and tumorigenic side effects, therefore strategies aiming to rather capable to induce tolerance toward the transgenic protein are being developped and needed. The objectif of this work was to implement a new strategy aiming to study the immunoregulatory and tolerogenic effect of fusion proteins derived from CTLA-4 and PD-L1. We used a murin model recapitulating the immunes responses induced by an AAV coding for an immunogenic model protein, ovalbumin (Ova) presented in previous studies by our group and others. Then, we synthesized AAV coding for our newly designed immunoregulatory protein and injected them into mice along with AAV-Ova. This strategy of vectorized immunoregulation (VIR) allowed to evaluate the intrinsic capacity of each individual proteins to modulate immune responses against Ova directly in vivo. Eventually, this work allow to 1) assess the benefits and limits of the VIR strategy, 2) the deletrious long-term effects of CTLA-4/Fc on central and peripheral Tregs in mice, 3) to demonstrate the interest of new molecules specifically derived from PD-L1/Fc over the immune tolerance through the long-term persistance of Ova transgene
Delage, Laure. „Des déficiences génétiques comme modèles naturels pour l'étude de la régulation des checkpoints immunitaires et la caractérisation des réponses auto-immunes“. Electronic Thesis or Diss., Université Paris Cité, 2021. http://www.theses.fr/2021UNIP5190.
Der volle Inhalt der QuelleRecessive NBEAL2 mutations have been reported in patients with Gray Platelet Syndrome (GPS). This syndrome is characterized by a macro-thrombocytopenia, with platelets lacking alpha-granules, leading to bleeding disorders, often associated with splenomegaly. Thus, NBEAL2 plays a crucial role in the trafficking of alpha-granules in platelets. Moreover, our lab has also described NBEAL2 deficiencies in patients presenting clinical features of the autoimmune lymphoproliferative syndrome, suggesting a role of NBEAL2 in immune homeostasis and tolerance. A broader international cohort of GPS patients has been described, revealing immune system abnormalities (autoimmune diseases, autoantibodies, lymphopenia). If the role of NBEAL2 in the traffic of granules is often investigated, the exact mechanism leading to the development of autoimmune manifestations in GPS patients remains unknown. NBEAL2 belongs to a protein family involved in vesicular trafficking, all of which possess a conserved BEACH domain. Within this BEACH-domain containing proteins family, one of the closest members to NBEAL2 is LRBA. LRBA is involved in the recycling of CTLA-4, an inhibitory immune checkpoint. CTLA-4 plays a crucial role in the regulation of immune responses and tolerance. Recessive mutations of LRBA lead to similar clinical features as partial CTLA-4 deficiency: autoimmunity, lymphocytic infiltrations, and progressive B lymphopenia. Physiologically, LRBA prevents the lysosomal degradation of CTLA-4 and allows its recycling to the membrane. By analogy with LRBA, we investigated the importance of NBEAL2 in immune checkpoints intracellular trafficking and we brought new insights on its role in lymphocytes. Thus, NBEAL2 is a scaffold protein, binding LRBA, and involved in CTLA-4 trafficking as well as in vesicular trafficking in general. This work brings new knowledge to the regulation of CTLA-4 in activated T lymphocytes, a list of new partners for NBEAL2 protein and a new model of vesicular trafficking in which NBEAL2 is involved. Finally, a better understanding of the mechanisms leading to autoimmunity in patients with gray platelets syndrome could lead to better diagnosis and treatment management
Bendavid-Anquetil, Céline. „Rôle des anticorps monoclonaux au cours des myopathies auto-immunes : de l’étude des auto-anticorps spécifiques des myopathies nécrosantes auto-immunes à la description physiopathologique des myosites induites par l’immunothérapie anti-tumorale“. Electronic Thesis or Diss., Sorbonne université, 2021. http://www.theses.fr/2021SORUS257.
Der volle Inhalt der QuelleMyositis is a rare autoimmune disease that may occur spontaneously, idiopathic inflammatory myopathies, or be induced by treatments such as immune checkpoint inhibitors (ICI). Among myositis, this work focused on the study of two entities: immune-mediated necrotizing myopathy (IMNM), and ICI-induced myositis. Inflammatory myopathies are separated into homogeneous subgroups in terms of clinical, biological, and histological phenotype thanks to the identification of myositis-specific autoantibodies. Each of these entities is associated with antibodies that play a role in the occurrence of the disease by different mechanisms. In IMNM, anti-SRP (signal recognition particle) autoantibodies appear to play a direct pathogenic role via activation of the classical complement pathway. Thirteen anti-SRP autoantibodies from patient samples were produced, including five autoantibodies specifically recognizing SRP by two different techniques. These human anti-SRP autoantibodies will be used to develop models of IMNM and to understand their mechanisms of action as well as to define their antigenic targets. Regarding ICI-induced myositis, therapeutic monoclonal antibodies directed against inhibitory co-stimulatory molecules induce a break of immune tolerance within the muscle tissue. The description of a series of patients from pharmacovigilance database allowed us to characterize a specific clinical phenotype associated with a poor prognosis, particularly in the case of associated myocarditis. The study of the systemic immune response and of the muscle transcriptomic profile has highlighted a central role of cytotoxic T lymphocytes and macrophages in the pathophysiology of the disease.Eventually, the description of pathophysiological mechanisms is mandatory to identify new therapeutic targets and then improve myositis treatment strategy
Anna, François. „Développement d'une immunothérapie anti-tumorale basée sur un récepteur antigénique chimérique (CAR) ciblant le point de contrôle immunitaire HLA-G : implications pour les tumeurs et leur microenvironnement“. Thesis, Université de Paris (2019-....), 2019. https://wo.app.u-paris.fr/cgi-bin/WebObjects/TheseWeb.woa/wa/show?t=4021&f=26655.
Der volle Inhalt der QuelleOver the last decade, anti-tumor immunotherapies have been a breakthrough in the oncology field following the clinical successes obtained with immune checkpoint inhibitors (ICPs) or chimeric antigenic receptors (CAR) based therapies. However, they are less effective against solid tumors, especially because of the lack of tumor specific antigen and of a tumor microenvironment capable of inhibiting the immune response favoring the tumor expansion. The HLA-G molecule is an immunosuppressive protein originally exclusively demonstrated to be involved in maternal-fetal tolerance but whose function has been hijacked by tumors to inhibit and escape from immune responses. HLA-G is now identified as an exquisite tumor associated antigen and its inhibition is crucial to restore the anti-tumor immune responses. Yet, no immunotherapy directed against HLA-G has been developed to date.The lack of effective treatment against or targeting HLA-G is related to the inefficiency to induce antibodies against this complex protein since HLA-G could be expressed through several isoforms that are immunosuppressives. In the first part of this study, thanks to an original immunization method based on the use of lentiviral vectors, we demonstrate the possibility to generate antibodies which are capable to recognize the HLA-G interaction domain with its receptors and are expected to inhibit the ICP function of HLA-G. The second part describes a CAR-T cell immunotherapy targeting HLA-G for its TAA properties. We first focused on the regulation and on the expression of the CAR chain at the transcriptional level. This approach was meant to limit the side effects caused by CAR therapies such as continuous activation of the CAR-T cells or elimination of healthy cells expressing the targeted antigen. We then generated two new 3rd generation CARs demonstrated to specifically recognize major HLA-G isoforms expressed by tumor cells and to eradicate HLA-G expressing tumor cells in vitro and in vivo. Several optimizations were carried out on the CAR chain structure to increase CAR-T cells cytotoxic function and to control their persistence through the insertion of the iC9 suicide gene. Given the results presented here, we provide the first vitro and vivo proofs of concept that a CAR therapy directly targeting HLA-G, and more generally an ICP is strikingly efficient.Finally, we discussed the potential for both anti-HLA-G blocking monoclonal antibodies and CAR-T cells immunotherapies against solid tumors and its implication against the tumor microenvironment and possible combinations with other immunotherapies
Wierz, Marina. „Characterization of the Tumor Microenvironment in Chronic Lymphocytic Leukemia by Mass Cytometry : Implications for Immunotherapy Dual PD1/LAG3 Immune Checkpoint Blockade Limits Tumor Development in a Murine Model of Chronic Lymphocytic Leukemia High-dimensional Mass Cytometry Analysis Revealed Microenvironment Complexity in Chronic Lymphocytic Leukemia“. Thesis, université Paris-Saclay, 2020. http://www.theses.fr/2020UPASL020.
Der volle Inhalt der QuelleChronic lymphocytic leukemia (CLL), the most frequent leukemia in adults, is characterized by the accumulation of mature B lymphocytes in peripheral blood and lymphoid tissues. The progression of CLL is highly dependent on complex interactions within the tumor microenvironment (TME) and despite recent advances in CLL treatment targeting the TME, CLL remains an incurable disease. Therefore, we wanted to deeply characterize the immune landscape in the TME in murine and human CLL to identify novel potential targets for an immunotherapeutic approach. For this purpose, we performed a comprehensive and extensive characterization by high-dimensional mass cytometry to establish an extensive cartography of immune cell subsets. We demonstrated that relevant changes in the immune cell composition, especially the expansion of specific lymphoid and myeloid immune cell subsets, are associated with strong immune suppression thereby contributing to an escape phenotype in CLL. These CLL-associated changes can be restored in preclinical models by a dual PD1/LAG3 immune checkpoint blockade. Moreover, we demonstrated a high T cell heterogeneity between patients that can be stratified according to their T cell profile, and the correlation of specific T cell subsets with time to initial treatment, highlighting their potential prognostic value. In conclusion, with this first CyTOF study in CLL, we expanded the current knowledge of the phenotypic complexity of the TME. We demonstrated that dual targeting of immune checkpoints efficiently controlled CLL development in preclinical models and therefore could have potential benefits in CLL to restore a functional anti-tumor immunity