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 / In-vivo evaluation of immunoregulatory proteins derived from CTLA-4 and PD-L1 for their capacity to inhibit immuno responses in a context of AAV muscle gene therapy

Dupaty, Léa

20 November 2018

La thérapie génique consiste à introduire du matériel génétique dans des cellules dans l’objectif de traiter une pathologie. Le plus souvent, la thérapie génique s’effectue au moyen d’un vecteur viral, transportant le gène jusque dans les cellules cibles. Dans le cas des maladies monogéniques, l’adeno-associated virus (AAV) s’est imposé progressivement comme un vecteur de choix. Son absence de pathogénicité, son large tropisme et sa capacité à transduire des cellules quiescentes sont autant d’avantages comparés à d’autres vecteurs utilisés en thérapie génique. L’utilisation d’AAV est approuvé en Europe pour le traitement d’un déficit rare en lipoprotéine lipase et vient récemment d’être approuvé par les autorités américaines pour le traitement d’un déficit de la vision. Toutefois, les essais de thérapies géniques se heurtent souvent aux réponses immunitaires dirigées contre l’AAV. En effet, les différents composants de ce vecteur viral ont été identifiés comme pouvant déclencher des réponses immunitaires s’opposant à l’efficacité à long terme de la thérapie génique. De plus, la protéine transgénique peut s’avérer immunogène, ce qui conduit au déclenchement de réponses immunitaires, à la destruction des cellules transduites et in fine à l’échec de la thérapie génique. En clinique, des immunosuppresseurs sont utilisés pour palier à ses effets indésirables. Toutefois, de par leurs effets secondaires infectieux et tumorigènes, des stratégies visant plutôt à induire de la tolérance vis-à-vis de la protéine transgénique, associées à un bénéfice pour la santé des patients, se sont développées.L’objectif de ce travail de thèse a été d’implémenter une nouvelle stratégie visant à étudier l’effet immunorégulateur et tolérogène de protéines de fusion dérivées de CTLA-4/Fc et de PD-L1/Fc. Pour cela, nous avons utilisé un modèle murin récapitulant les réponses immunitaires induites par un AAV permettant l’expression d’une protéine modèle fortement immunogène, l’ovalbumine (Ova). Ensuite, des AAV codant pour les protéines au potentiel immunorégulateur ont été synthétisés et injectés aux souris conjointement à l’AAV-Ova. Cette stratégie d’immunorégulation vectorisée (VIR) nous a permis d’évaluer la capacité de chacune des protéines à moduler les réponses immunitaires dirigées contre l’Ova directement in vivo. Au total, ce travail a permis de mettre en évidence i) l’intérêt et les limites de la stratégie VIR, ii) celui du rôle délétère de CTLA-4/Fc au long terme sur les lymphocytes Tregs CD4+FoxP3+, périphériques et centraux, iii) et de démontrer l’intérêt de 2 nouvelles molécules dérivées PD-L1/Fc sur la persistance de l’Ova. / Gene 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.

Thérapie génique

Point de contrôle immunologique

Tolérance immunitaire

CTLA-4

PD-L1

Vecteur adéno-associé

Vectorisation

Gene Therapy

Immune checkpoint

Immune tolerance

CTLA-4

PD-L1

Adeno-associated vector

Vectorization

615.8

616.079

Protinádorová aktivita IL-2 a IL-7 imunokomplexů v kombinaci s αCTLA-4 a αPD-1 monoklonálními protilátkami / Antitumor activity of IL-2 and IL-7 immunocomplexes in combination with αCTLA-4 and αPD-1 mAbs

Hnízdilová, Tereza

January 2019

Biological activity of IL-2 and IL-7 in vivo is significantly increased when complexed with some of the respective anti-cytokine mAb. Different immune cell subsets can be preferentially stimulated depending on the anti-IL-2 mAb used to complex IL-2. IL-2/anti-IL-2 mAb S4B6 immunocomplexes (IL-2/S4B6) induce preferential expansion of CD122high cells whereas IL-2/anti-IL-2 mAb JES6-1 immunocomplexes (IL-2/JES6-1) highly selectively stimulate CD25high cells in mice. Similarly, IL-7/anti-IL-7 mAb M25 immunocomplexes (IL-7/M25) possess higher stimulatory activity for both naïve and memory CD8+ T cells in vivo in comparison to free IL-7. CTLA-4 and PD-1 molecules are inhibitory receptors which negatively regulate proliferation, survival and effector functions of T cells. Blocking antibodies against these molecules represent promising immunotherapeutic tool for treatment of malignant diseases. We examined possible synergism of IL-2/S4B6 and αCTLA-4 plus αPD-1 mAbs in tumor-bearing mice. We found that the expansion of recently activated CD8+ T cells driven by IL-2/S4B6 was further augmented by αCTLA-4 plus αPD-1 mAbs. However, these two immunotherapeutic approaches did not show synergistic antitumor activity in any mouse tumor model tested. Next, we showed that IL-7/M25 possessed higher biological activity...

Immunomodulatory Therapy of Solid Tumors : With a Focus on Monoclonal Antibodies

Sandin, Linda

January 2013

Cancer, historically considered a genetic disease, is currently acknowledged to affect the whole body. Our immune system is one key player that can elicit a response against malignant cells but can also promote tumorigenesis. Tumors avoid immune recognition by creating a suppressive microenvironment and inducing tolerance. T-cells are regarded a major effector cell type in tumor immunotherapy. An important ”switch” needed for T-cell activation involves so-called costimulatory and coinhibitory receptors. In this thesis, experimental tumor models were used to investigate the potential of immunomodulatory antibodies to stimulate immune cells and subsequently eliminate tumors. First, systemic antibody blockade of two negative checkpoint regulators (CTLA-4 and PD-1) present on T-cells was evaluated in combination with local CpG therapy or standard BCG treatment. Indeed, this combinatorial therapy with CpG augmented anti-tumor effects with increased levels of tumor-directed T-cells and reduced tumor-infiltrating Tregs. Secondly, as these immunomodulatory antibodies elicit severe side effects in patients, a local low-dose delivery regimen was explored as an alternative to systemic bolus treatment. Our results demonstrated that an approximately seven times lower dose of aCTLA-4, compared to systemic delivery, could eradicate both primary and distant tumors. CD40-expressing APCs are another potential target in antibody-mediated cancer therapy. CD40-stimulated dendritic cells (DCs) have the capability to activate tumor-directed T-cells to kill tumor cells. We next sought to investigate agonistic CD40 antibody efficacy and in vivo biodistribution when delivered locally compared to the equivalent systemic dose. Anti-tumor effects were dependent on CD8+ T-cells, host CD40 expression and the presence of tumor antigen at the injection site. CD40 antibodies were cleared from the circulation and accumulated in lymphoid organs, where, upon repeated aCD40 dosing, target APC populations increased in numbers and upregulated their surface CD40 expression. Lastly, CD40 agonist antibodies were mixed with nanoparticles to enhance their stimulatory properties. B-cells demonstrated increased proliferative capacity and DCs became more activated when exposed to the cocktail. Further, this combination reduced serum levels of pro-inflammatory cytokines compared to plain antibodies.       The results herein advocate further exploratory studies of the delivery of monoclonal antibodies at the tumor site in order to improve anti-tumor effects and reduce toxicity.

in situ checkpoint blockade

antibody-mediated tumor immunotherapy

CTLA-4

CD40

monoclonal antibodies

experimental animal model

Fc gamma receptor

Increasing T Cell Immunity to Metastatic Osteosarcoma via Modulation of Inhibitory T Cell Receptors

January 2015

abstract: Osteosarcoma is the most common bone cancer in children and adolescents. Patients with metastatic osteosarcoma are typically refractory to treatment. Numerous lines of evidence suggest that cytotoxic T-lymphocytes (CTL) limit the development of metastatic osteosarcoma. I have investigated the role of Programmed Death Receptor-1 (PD-1) in limiting the efficacy of immune mediated control of metastatic osteosarcoma. I show that human metastatic, but not primary, osteosarcoma tumors express the ligand for PD-1 (PD-L1) and that tumor infiltrating CTL express PD-1, suggesting this pathway may limit CTL control of metastatic osteosarcoma in patients. PD-L1 is also expressed on the K7M2 osteosarcoma tumor cell line that establishes metastases in mice, and PD-1 is expressed on tumor infiltrating CTL during disease progression. Blockade of PD-1/PD-L1 interactions dramatically improves the function of osteosarcoma-reactive CTL in vitro and in vivo, and results in decreased tumor burden and increased survival in the K7M2 mouse model of metastatic osteosarcoma. My results suggest that blockade of PD-1/PD-L1 interactions in patients with metastatic osteosarcoma should be pursued as a therapeutic strategy. However, PD-1/PD-L1 blockade treated mice still succumb to disease due to selection of PD-L1 mAb resistant tumor cells via up-regulation of other co-inhibitory T cell receptors. Combinational α-CTLA-4 and α-PD-L1 blockade treated mice were able to completely eradicate metastatic osteosarcoma, and generate immunity to disease. These results suggest that blockade of PD-1/PD-L1 interactions in patients with metastatic osteosarcoma, although improves survival, may lead to tumor resistance, requiring combinational immunotherapies to combat and eradicate disease. / Dissertation/Thesis / Doctoral Dissertation Molecular and Cellular Biology 2015

Immunology

Molecular biology

Cellular biology

CTLA-4

Inhibitory Receptors

Metastatic Osteosarcoma

PD-1

PD-L1

T cell exhaustion

The genetic basis of T and B cell contribution to autoimmune diabetes in NOD mice

Motta, Vinícius

January 2006

The nonobese diabetic mouse (NOD) is an excellent animal model to study type 1 diabetes. As with some humans, disease in the NOD mouse is effected by a combination of genetic and environmental factors. At least 20 insulin dependent diabetes (Idd) susceptibility loci have been identified so far, both in humans and in the NOD mouse. In this thesis, the overall aim has been to understand the genetic basis of diabetes in the NOD mouse by assessing immunogically-related phenotypes. As lymphocytes are the main players in the onset and progression to overt diabetes, we searched for physiological abnormalities in T and B cells, which could contribute to the breakdown of tolerance to pancreatic antigens. Ultimately, we postulate that abnormalities in the T or B cell compartments, under the genetic control of a previously defined diabetes susceptibility regions (Idds) could unravel the biological mechanisms underlying diabetes susceptibility and facilitate the identification of etiological polymorphisms involved in the disease. NOD T cells are defective in upregulating CTLA-4 upon in vitro activation. Previous studies have shown that this defect is, at least in part, controlled by gene(s) in the Idd5 region on chromosome 1. In paper I, we provide evidence that defective upregulation of the CTLA-4 in NOD T cells is not controlled by the Idd5.1 and Idd5.2 regions, but rather by genes linked to the telomeric region of chromosome 1 and to the Idd3 locus, for which the prime candidate gene is Il-2. Interestingly, we could restore some of the defective CTLA-4 expression in NOD T cells by the addition of exogenous IL-2 during T cell activation in vitro. In paper II, we show that NOD thymocytes are resistant to superantigen-mediated negative selection and that this trait is under control of the Idd5.2 region. Interestingly, it appears to operate in a T cell non-autonomous manner. In paper III, we describe a competitive advantage of NOD thymocytes to mature when they co-develop with B6 thymocytes in embryo aggregation chimeras. These results imply that defects exist in the positive/negative selection mechanisms in the NOD thymus. Apart from T cells, B cells also play an important role in the initiation of diabetes in NOD mice, probably as antigen presenting cells. In paper IV, we report that the genetic basis of an enlarged marginal zone (MZ) B cell population observed in the NOD mice is linked to the Idd9/Idd11 region. Together, these findings contribute to the dissection of the molecular mechanisms underlying diabetes pathogenesis, and shed light on the contribution of central and peripheral tolerance mechanisms to this process.

Type 1 Diabetes

NOD mouse

CTLA-4

superantigen

T cells

Idd

marginal zone B cells

embryo aggregation chimera

negative selection

Immunogenetics

Immungenetik

Etude des lymphocytes T régulateurs naturels CD8+CD25+: signature micro-ARN et effets des micro-ARNs sur l'expression de FOXP3, CTLA-4 et GARP / Studying microRNA signature in human Tregs and the effect of microRNAs on Treg associated genes

Jebbawi, Fadi

12 March 2014

Mon travail de thèse a consisté à caractériser une sous-population de lymphocytes T régulateurs naturels de phénotype CD8+CD25+.<p>Nous avons purifié les CD8+CD25+ nTregs et vérifié par cytométrie de flux leur expression en FOXP3 et CTLA-4. Puis nous avons pu montrer que ces cellules possèdent des propriétés suppressives dans un test d’inhibition de la prolifération de lymphocytes T activés allogéniquement. Les lymphocytes CD8+CD25+ nTregs expriment les gènes FOXP3, CTLA-4, GARP et CCL-4 et les cytokines IL-10 et TGF-β. Par contre, les gènes CD28, ICOS, FOXO1 et Helios sont sous-exprimés dans les nTregs CD8+CD25+ par rapport aux lymphocytes T CD8+CD25-. <p>Nous avons établi une signature micro-ARN qui comprend 10 micro-ARNs différentiellement exprimés :7 micro-ARNs sous-exprimés "miR-9, -24, -31, -155, -210, -335 et -449 " et 3 micro-ARNs surexprimés " miR-214, -205 et -509". De plus, nous avons pu explorer la relevance biologique de cette signature micro-ARN en montrant dans un premier temps que les miRs "-31, -24, -210, -335" ciblent spécifiquement la région 3'UTR de FOXP3, de même les miR-9 et miR-155 ciblent la région 3'UTR de CTLA-4, et les miR-24, et -335 ciblent la région 3'UTR de GARP. Ceci a été fait par des expériences de co-transfections suivies d'une mesure de l'activité rapportrice luciférase. De plus, nous avons pu démontrer par des expériences de transduction lentivirale ex vivo, de cellules T primaires, que des micro-ARNs de la signature régulent l’expression de FOXP3, CTLA-4 et GARP dans les Tregs naturels CD8+CD25+ humains. <p>Cette étude montre l'importance des micro-ARNs dans la régulation post-transcriptionnelle des gènes impliqués dans la fonction régulatrice des lymphocytes T régulateurs.<p> / Doctorat en Sciences / info:eu-repo/semantics/nonPublished

Sciences exactes et naturelles

Biologie

T cells

Suppressor cells

RNA

Lymphocytes T

Lymphocytes T suppresseurs

ARN

microRNA

FOXP3

CTLA-4

T régulateurs

GARP

microARN..

T regulatory cells

Identification de causes génétiques du syndrome d’Evans pédiatrique / Identifying genetic causes of pediatric Evans syndrome

Lévy, Eva

11 May 2016

Le syndrome d'Evans est défini par l'existence concomitante ou séquentielle de cytopénies auto-immunes, le plus souvent, anémie hémolytique et thrombopénie immunologique. Chez l'enfant, il peut être secondaire à une infection, une maladie auto-immune systémique ou un déficit immunitaire primitif. Alternativement, chez une grande partie des patients, l'étiologie n'est pas clairement identifiée. Les patients atteints de syndrome d'Evans présentent parfois d'autres atteintes, telles une auto-immunité d'organe, une lymphoprolifération bénigne ou un déficit immunitaire. L'objectif de ce travail était d'identifier des causes génétiques chez des enfants présentant un syndrome d'Evans sans étiologie sous-jacente identifiée. Nous avons centré notre étude sur des formes sévères à début pédiatrique en faisant l'hypothèse qu'une maladie monogénique serait plus fréquente dans ce groupe de patients. Nous avons mis à profit les technologies de séquençage haut débit « nouvelle génération » (NGS) pour réaliser et analyser le séquençage de l'exome de patients et de certains de leurs apparentés afin de mettre en évidence des gènes candidats potentiels. Ce travail a permis l'identification de 4 gènes candidats : LRBA, CTLA-4, STAT3 (mutations gain de fonction) et NFKBIA. L'implication des 3 premiers gènes dans de nouvelles maladies monogéniques où l'auto-immunité est au premier plan a été confirmée par d'autres équipes au cours de ce travail. Pour chacun de ces gènes, nous avons poursuivi 2 objectifs complémentaires : d'une part, tenter de valider l'implication des gènes identifiés dans la maladie des patients. Nous avons pour cela utilisé des approches et techniques variées : biochimie et protéomique afin d'identifier des partenaires protéiques, microscopie confocale pour localiser les protéines et leurs interactions, tests cellulaires in vitro pour mettre en évidence un défaut fonctionnel, marquages en cytométrie en flux pour identifier des modifications dans les sous-populations lymphocytaires. D'autre part, nous avons recherché d'autres mutations de ces gènes chez des patients de phénotype clinique similaire. Nous avons ainsi constitué et exploré 3 cohortes de patients présentant des mutations de LRBA, CTLA-4 ou STAT3. Nous avons rassemblé une cohorte de 18 patients porteurs d'une mutation de LRBA, répartis dans 11 familles. Cela nous a permis de préciser et d'étendre le spectre clinique de cette maladie de découverte récente, avec en particulier des atteintes articulaires sévères s'associant à un diabète précoce, ou des entéropathies. Nous avons identifié 15 nouvelles mutations de transmission autosomique récessive dans le gène LRBA, codant une protéine de fonction inconnue dont l'absence entraine une maladie principalement caractérisée par une poly-auto-immunité. Nous avons identifié 29 partenaires protéiques potentiels de LRBA et précisé la localisation de LRBA dans les différents compartiments cellulaires. Nous avons également établi une cohorte de 12 patients dans 10 familles présentant un déficit en CTLA-4 par haplo-insuffisance. Au delà de la mise en évidence de 9 nouvelles mutations, nous avons décrit une famille où la variation est transmise de façon autosomique récessive. Dans les déficits en LRBA et CTLA-4, nous avons mis en évidence une diminution du pourcentage de lymphocytes T régulateurs parmi les PBMC et une diminution de l'expression de CTLA-4 dans les lymphocytes T activés. Ceci corrobore l'interaction entre ces 2 protéines décrite en parallèle par une autre équipe. Nous avons montré que les spectres cliniques des déficits en LRBA et CTLA-4, fortement chevauchant dans les premières descriptions publiées, pourraient se différencier, malgré l'implication des lymphocytes T régulateurs dans ces 2 maladies. (...) / Evans syndrome is defined by the occurence of autoimmune cytopenias, either at the same time or sequential, mainly autoimmune hemolytic anemia and immune thrombocytopenia. In children, it may be secondary to infections, systemic autoimmune disease, or primary immune deficiency, though in most patients, its etiology isn't obvious. Patients affected with Evans syndrome can also present other features, such as autoimmunity toward a particular organ, benign lymphoproliferation or immunodeficiency. The main goal of this work was to identify genetic causes in children presenting an Evans syndrome without a known underlying etiology. We focused our study on severe, early onset forms of the disease, with the hypothesis that a monogenic disease would be more frequent in this group of patients. Taking advantage of high throughput "Next Generation" sequencing (NGS) techniques, we sequenced and analyzed exome from patients and their relatives in search for adequate candidate genes. We identified 4 candidate genes: LRBA, CTLA-4, STAT3 (gain-of-function mutations), and NFKBA. Implication of the first 3 genes in new monogenic diseases with autoimmunity as a key feature was also confirmed by others during the course of this work. For each gene, we pursued 2 complementary goals: First, we sought to validate the implication of the gene in the patients' disease. To do so, we used various techniques and approaches: biochemistry and proteomics to identify protein partners, confocal microscopy to localize proteins and interactions, in vitro cellular assays to bring to light functional defect, flow cytometry to identify changes in lymphocytes subpopulations. We also looked for other mutations of each gene in patients with a similar clinical presentation. Hence we created and explored 3 cohorts of patients presenting with mutations of LRBA, CTLA-4 or STAT3. We constituted a cohort of 18 patients with LRBA mutations within 11 families. We then were able to precise and extend the clinical spectrum of this recently described disease. In particular, we observed patients with severe chronic arthritis associated with diabetes mellitus or enteropathies. We identified 15 new mutations of autosomal recessive transmission in the LRBA gene, coding a protein of unknown function, which absence is responsible for a disease mainly characterized by autoimmune features. We identified 29 candidate protein partners of LRBA and precized LRBA localisation in cell compartiments. We also established a cohort of 12 patients within 10 families presenting CTLA-4 haploinsufficiency. Beyond describing 9 new mutations, we report a family with autosomal recessive transmission.In LRBA and CTLA-4 deficiencies, we showed a decrease of regulatory T lymphocyte subset proportion among PBMC and a decrease of CTLA-4 expression in activated T cells. These results support the interaction between these 2 proteins, described concurrently by another team. We showed that the clinical spectra of these 2 diseases, although widely overlapping in first published reports, could be different despite a role of regulatory T cells in both. Hence, organ-specific autoimmunity and lymphoproliferation are more frequent in LRBA deficiency whereas granuloma and hypogammaglobulinemia are more present in CTLA-4 deficiency. Theses results suggests a role of genetic modifyers, which remain to identify. Among our cohort of patients with Evans syndrome, we also identified 5 patients within 5 families presenting gain-of-function mutations of STAT3. 3 of those mutations were reported by others during our work and appeared de novo in our patients. Functional validation of the 4th one is in progress. The last mutation follows a recessive transmission and could exemplify a new transmission modality of this disease. (...)

Syndrome d'Evans

Anémie hémolytique auto-immune

Purpura thrombopénique immunologique

Auto-immunité

Maladie génétique

Séquençage de l'exome

LRBA

CTLA-4

STAT3 gain de fonction

Lymphocytes T régulateurs

Pédiatrie

Déficit immunitaire

Evans syndrome

Autoimmune hemolytic anemia

Immune thrombocytopenia

Autoimmunity

Genetic disease

Exome sequencing

LRBA

CTLA-4

STAT3 gain-of-function

Regulatory T lymphocytes

Pediatrics

Immune deficiency

571.96

Prognostický a prediktivní význam exprese kontrolních bodů imunitních reakcí u ovariálního karcinomu / The prognostic and predictive role of immune check point inhibitors in ovarian cancer patients

Raková, Jana

January 2018

Epithelial ovarian cancer is the sixth most common tumor disease among women and it is the leading cause of death from all types of gynecologic malignancies. The current standart of care consist of debulking surgery followed by platinum-taxane chemotherapy. Althought some patients benefit from the treatment, most eventually experience platinum-resistance and die from this disease. Immunotherapy based on application of immune checkpoint blockers represents a new treatment strategy in different cancer malignancies. However, emerging clinical data show only limited clinical efficacy of these agents in ovarian cancer patients with objective response rates of 10-15%. Therefore there is a strong need to identify a potential biomarkers, which allows to identify the group of patients, who will benefit the most from this costly treatment. The aim of my diploma thesis was to characterize the prognostic and predictive role of the immune checkpoints within the retrospective and prospective cohort of patients with high-grade serous ovarian cancer (HGSOC). Our study follows, that the expression of PD-L1 molecule and high frequencies of PD-1+ tumor infiltrating lymphocytes (TILs) in tumor microenviroment is significantly correlated with a better prognosis of patients with HGSOC. Moreover, PD-L1 and PD-1...

Immunological Checkpoint Blockade and TLR Stimulation for Improved Cancer Therapy / TLR-stimulering och CTLA-4 samt PD-1 blockad för förbättrad cancerterapi

Mangsbo, Sara

January 2009

This thesis concerns the investigation of novel immunotherapies for cancer eradication. CpG therapy was used in order to target antigen-presenting cells (APCs), facilitating antigen presentation and activation of T cells. Blockade of the two major immune checkpoint regulators (CTLA-4 and PD-1) was also studied to ensure proper and sustained T cell activation. The therapies were investigated alone and compared to BCG, the standard immunotherapy in the clinic today for bladder cancer. In addition, CpG as well as BCG was combined with CTLA-4 or PD-1 blockade to examine if the combination could improve therapy. Single and combination strategies were assessed in an experimental bladder cancer model. In addition, one of the therapies (local aCTLA-4 administration) was evaluated in an experimental pancreatic cancer model. To be able to study the effects of CpG in humans, a human whole blood loop system has been used. This allowed us to dissect the potential interplay between CpG and complement. CpG was found to be superior to the conventional therapy, BCG, in our experimental model and T cells were required in order for effective therapy to occur. Used as a monotherapy, CTLA-4 blockade but not PD-1 blockade, prolonged survival of mice. When CTLA-4 or PD-1 blockade was combined with CpG, survival was enhanced and elevated levels of activated T cells were found in treated mice. In addition, Treg levels were decreased in the tumor area compared to tumors in control treated mice. CTLA-4 blockade was also effective when administrated locally, in proximity to the tumor. Compared to systemic CTLA-4 blockade, local administration gave less adverse events and sustained therapeutic success. When CpG was investigated in a human whole blood loop system it was found to tightly interact with complement proteins. This is an interesting finding which warrants further investigation into the role of TLRs in complement biology. Tumor therapy could be affected either negatively or positively by this interaction. The results presented herein are a foundation for incorporating these combination therapies into the clinic, specifically for bladder cancer but in a broader perspective, also for other solid tumors such as pancreatic cancer.

CpG ODNs

TLR-9

CTLA-4

PD-1

PD-L1

B7. H1

immunotherapy

checkpoint blockade

bladder cancer

cancer

complement

TLRs

Compstatin

properdin

C3

experimental animal model

whole blood loop system

combination therapies

Clinical immunology

Klinisk immunologi

Tumour immunology

Tumörimmunologi

Etude des mécanismes cellulaires et moléculaires impliqués dans la fonction suppressive des lymphocytes T régulateurs / Study of molecular and cellular mechanisms involved in regulatory T cell suppressive activity

Denoeud, Julie N.O.

18 June 2010

La réponse immune représente une réponse complexe à laquelle correspond une succession d’événements orchestrés finement. Parmi les mécanismes qui régulent la réponse immune, les lymphocytes T régulateurs (Tregs) assurent le maintien de la tolérance en périphérie et le contrôle des réponses immunes adaptatives. Ils représentent une population hétérogène et leurs mécanismes de suppression sont toujours l’objet d’intenses recherches. Suivant le contexte de suppression et leur nature, les lymphocytes Tregs réalisent une inhibition de l’activation des lymphocytes Th, soit directement, soit via la modulation de la fonction des cellules dendritiques (DC). <p>Dans un modèle d’immunisation par des cellules dendritiques chargées de KLH, les lymphocytes Tregs naturels contrôlent sélectivement l’initiation des réponses de type Th1/CTL spécifiques de l’antigène. Le but de ce travail était de définir quels sont les acteurs potentiels du contrôle de cette réponse. A l’aide de l’anticorps PC61 dirigé contre le récepteur CD25 et éliminant les lymphocytes Tregs naturels, nous avons montré que le ligand de costimulation CD70 joue un rôle clé dans leur régulation de la réponse Th1/CTL (Article 1). Ainsi, dans des conditions normales, la cytokine IL-12 induit principalement l’initiation de la réponse Th1 in vivo, tandis qu’en l’absence de lymphocytes Tregs naturels, la voie CD70/CD27 est une voie alternative d’induction de l’IFN-γ. Cette voie d’activation pourrait être opérationnelle dans certains contextes infectieux lorsque les lymphocytes Tregs sont déstabilisés voire éliminés, par exemple lors d’infections par Toxoplasma gondii ou par les virus HTLV1, SIV ou HIV. Nous avons montré que les lymphocytes Tregs naturels diminuent l’expression du ligand CD70 sur les DC, de manière dépendante de son récepteur CD27. <p>Ensuite, nous nous sommes intéressés à une deuxième population de lymphocytes T régulateurs, les lymphocytes Tregs ICOShigh induits in vivo par le traitement avec l’anticorps anti-CTLA-4. Dans le cadre d’une colite induite par l’agent alkylant TNBS et mettant en jeu une réponse Th1, cette population de lymphocytes Tregs amplifiée par le traitement à l’anticorps anti-CTLA-4 régule la réponse immune via la cytokine anti-inflammatoire IL-10 et l’enzyme immunosuppressive IDO (Article 2). Ainsi, les résultats obtenus nous ont permis de répondre à notre objectif et de définir certains mécanismes de suppression des lymphocytes Tregs naturels et des lymphocytes Tregs induits. <p>Dans la dernière partie de ce travail, nous avons cherché à comparer les populations de lymphocytes Tregs naturels et ICOShigh présentes dans l’intestin d’une souris naïve. Une analyse transcriptomique a révélé que ces deux populations s’opposent sur les plans phénotypique et fonctionnel. Nous proposons un modèle dans lequel les deux populations de lymphocytes Tregs agiraient en synergie pour maintenir l’homéostasie intestinale. Les lymphocytes Tregs ICOShigh différenciés au niveau local et continuellement activés contrôleraient la réponse inflammatoire associée à la présence de la flore commensale. Les lymphocytes Tregs naturels, en quiescence dans les ganglions mésentériques, n’interviendraient qu’en cas d’infection par des pathogènes.<p>L’étude des lymphocytes T régulateurs soulève un certain nombre de concepts clés de l’immunité :la spécificité des réponses, la distinction des microorganismes commensaux et pathogènes… Mieux connaître les lymphocytes Tregs dans un modèle murin permettra de mieux comprendre les réponses inflammatoires intestinales chroniques observées chez l'homme et d’envisager, à terme, de nouveaux traitements.<p>/<p>An immune response is complex and implies numerous sequential events. It is regulated by different mechanisms, among which regulatory T cells maintain peripheral tolerance and control adaptive immune responses. Regulatory T cells are very heterogeneous and suppress immune responses through different mechanisms, still under investigation. They can inhibit T cell activation directly or through the modulation of dendritic cell function, depending on their nature and the tissular context.<p>In a dendritic cell-mediated immunization model, naturally occurring regulatory T cells selectively control the priming of antigen-specific Th1/CTL responses. Our goal was to define the potential actors of this control, targeted by natural regulatory T cells. Using the PC61 antibody which targets and depletes these cells, we showed that the costimulation ligand CD70 plays a key role in their control of Th1/CTL responses (first article). We showed that mainly IL-12 provokes Th1 development in normal conditions, wheras CD70 plays a major role in priming Th1 responses in the absence of natural Tregs. This pathway can be operational if regulatory T cells are destabilized or even depleted, for example during infection with Toxoplasma gondii or with HTLV1, SIV or HIV. We showed that natural Tregs downregulate CD70 expression on the surface of DCs.<p>Next, we focused on another regulatory T cell population, induced in vivo by the anti-CTLA-4 mAb treatment. In a model of pro-Th1 colitis, induced by the alkylating agent TNBS, these ICOShigh regulatory T cells exert an IL-10 and IDO-dependant control over the immune response (second article). Thus, we succeeded in determining some control mechanisms of the immune response targeted by two populations of regulatory T cells.<p>Finally, we compared two regulatory T cell populations: naturally occurring regulatory T cells and ICOShigh regulatory T cells from the intestines of naïve mice. A transcriptional analysis revealed two populations phenotypically and functionally distinct. We proposed a model in which these populations act synergistically and both maintain intestinal homeostasis. ICOShigh regulatory T cells might control commensal gut flora-specific inflammatory responses and quiescent natural regulatory T cells from mesenteric lymph nodes might control potential pathogen infections.<p>As a conclusion, this study raises some immunological issues: specificity of immune responses, distinction between commensal and pathogenic microorganisms… A better knowledge of these regulatory populations will lead to a better understanding of human intestinal responses and in the medium term will lead to new therapeutic approaches and tools.<p> / Doctorat en Sciences / info:eu-repo/semantics/nonPublished

Biologie

Sciences exactes et naturelles

T cells

Molecular immunology

Dendritic cells

Lymphocytes T

Immunologie moléculaire

Cellules dendritiques

réponse Th1

lymphocytes T régulateurs

anti-CTLA-4

ICOS

TNBS colitis

IL-10

colite TNBS

IL-10/ regulatory T cells

Th1 responses

indoleamin-2

3-dioxygenase

CD70

indoléamine-2

3-dioxygénase