Communication Between Immune and Non-Immune Cells in Intestinal Health and Disease

Cruz, Michelle

26 May 2023

No description available.

Cellular Biology

Immunology

Pathology

immunology

T cells

mucosal immunology

epithelial cells

intestinal epithelial cell

spheroids

organoids

coculture

Effect of Interferon α on HLA-DR Expression by Human Buccal Epithelial Cells

Smith, J. Kelly, Chi, David S., Krishnaswamy, Guha, Srikanth, Sujata, Reynolds, Scott, Berk, Steven L.

27 August 1996

We have studied the effect of interferon α (IFN-α) on MHC class II expression by human buccal epithelial cells (BEC), and mRNA expression by BEC and mucosal-associated mononuclear cells (MAMC). In 6 experiments, freshly collected BEC were suspended at a concentration of 1.0 x 105/ml in RPMI 1640 and incubated in the presence of 0-10000 IU/ml of human lymphoblastoid IFN-α (HuIFN-α). Zero and six hour samples were analyzed by single color flow cytometry using FITC-labeled murine IgG1 monoclonal antibody to HLA-DR. Preparations were also analyzed for expression of cytokine transcripts (IL-2 IL-4, IL-5, IL-6, IL-8, IFN-γ, GM-CSF) by reverse transcriptase polymerase chain reaction (RT-PCR). Increasing concentrations of IFN-α resulted in proportionate increases in the percentage of HLA-DR + BEC (r = 0.7897, p = 0.0627) and in the percentage of HLA-DR + staining at higher intensities (101 to 102 log fluorescence intensity) (LFI) (r = 0.40l0, p = 0.0424). The percentage of HLA-DR + BEC rose from a mean of 1.5% with no IFN-α to 7% with 10000 IU/ml IFN-α (p < 0.05). The percentage of HLA-DR + BEC staining at 101 to 102 LFI rose from a mean of 8.3% with no added IFN-α to 19.2% with 10000 IU/ml IFN-α (p <0.05). Unstimulated BEC constitutively expressed IL-8 and GM-CSF. IFN-α stimulated preparations also expressed IFN-γ, possibly due to the presence of MAMC, which comprised 2-9% of the total cell population. These data indicated that HuIFN-α upregulates MHC class II expression by human BEC, possibly by enhancing IFN-γ production by MAMC present in the culture preparations.

cytokine mRNA transcripts

human buccal epithelial cells

human lymphoblastoid interferon

MHC class II antigens

mucosal-associated mononuclear cells

The Role of Prolactin in CCL28 Regulation

Hyde, Jennie

06 March 2007

Infants are born with naive immune systems, making them susceptible to a variety of infections. In order to protect the newborn infant it is important that mothers be able to pass protective IgA antibodies to their infants through breast milk. B cells that produce IgA enter the mammary tissue during lactation and secrete IgA into the milk. During pregnancy, the mammary tissue expresses high levels of chemokines, molecules that allow lymphocytes to selectively home to specific tissues. The chemokine CCL28 has been shown to be upregulated during both pregnancy and lactation, and is vital for the ability of IgA-producing B cells to home to the mammary tissue during lactation. The aim of this study was to determine whether CCL28 expression is regulated by prolactin signaling.

CCL28

IgA-producing B cells

mucosal immunity

prolactin

Infants

mammary tissue

chemokines

pregnancy

lactation

IgA

breast milk

Microbiology

Three Dimensional Characterization of Vocal Fold Fluid Structure Interactions

Nielson, Joseph R.

05 July 2012

Voice quality is strongly linked to quality of life; those who suffer from voice disorders are adversely affected in their social, family, and professional relationships. An effort has been made to more fully understand the physics behind how the voice is created, specifically the fluid structure interactions that occur during vocal fold vibration. Many techniques have been developed and implemented to study both the motion of the vocal folds and the airflow that creates the motion. Until recently these techniques have sought to understand a highly three-dimensional phenomenon with 1D or 2D perspectives.This research focuses on the development and implementation of an experimental technique to obtain three-dimensional characterizations of vocal fold motion and fluid flow. Experiments were performed on excised human vocal fold models at the University Hospital Erlangen Medical School in Erlangen, Germany. A novel technique for tracking the motion of the vocal folds using multiple camera viewpoints and limited user interaction was developed. Four high-speed cameras (2000 fps) recorded an excised vocal fold model vibrating at 250 Hz. Based on the images from these four cameras a fully 3D reconstruction of the superior surface of the vocal folds was achieved. The 3D reconstruction of 70 consecutive time steps was assembled to characterize the motion of the vocal folds over eight cycles. The 3D reconstruction accurately modeled the observed behavior of vocal fold vibration with a clearly visible mucosal wave. The average reprojection error for this technique was on par with other contemporary techniques (~20 micrometers). A whole field, time resolved, three-dimensional reconstruction of the vocal fold fluid flow was obtained using synthetic aperture particle image velocimetry. Simultaneous 3D flow fields, subglottal pressure waves, and superior surface motion were presented for 2 consecutive cycles of oscillation. The vocal fold fluid flow and motion measurements correlated with behavior observed in previous three-dimensional studies. A higher resolution view of one full cycle of oscillation was compiled from 16 time resolved data sets via pressure data. The result was a full three-dimensional characterization of the evolution and disintegration of the glottal jet.

Joseph Nielson

SAPIV

synthetic aperture

superior surface

vocal folds

three-dimensional

particle image velocimetry

glottal jet

mucosal wave

Mechanical Engineering

Design and Synthesis of Ceragenins–Cationic Steroid Antimicrobial Compounds, Structural Improvement and Synthesis of Cyclopentenone Prostaglandins and Modification and Synthesis of Derivatives of Ribityllumazines: Potential Antigens for Activation of MAIT Cells

Li, Yubo

01 April 2019

Antimicrobial peptides (AMPs) are ubiquitous and display broad-spectrum antimicrobial activity that can control bacterial colonization of surfaces. Ceragenins are small-molecule mimics of AMPs and have several advantages over AMPs, including cost of manufacture and stability. A ceragenin, CSA-120, modified with an acrylamide group was directly incorporated into fluoropolymer coatings as a means of inhibiting bacterial biofilm formation. The ceragenin-containing coatings displayed improved performance. By conjugating a copper chelating group to the ceragenin, chelation of 64Cu by the conjugate was effective and provided a stable complex that allowed in vivo imaging. This conjugate may provide a means of identifying infection sites in patients presenting general signs of infection without localized symptoms. A combination nanoparticle comprised of a maghemite core for enhanced T2 MRI contrast diagnostics, a colloidal silver shell acting as an antimicrobial and therapeutic vehicle, and a ceragenin (CSA- 124) surfactant providing microbial adhesion was synthesized and characterized by multiple methods. Silver nanoparticles conjugated with ceragenin, CSA-124, as a potential Gram-positiveselective antimicrobial were synthesized and termed as CSA-SNPs. Herein, CSA-SNPs are characterized using multiple methods and the antimicrobial properties are determined through minimum inhibitory concentration/minimum bactericidal concentration (MIC/MBC) and time-kill study. Prostanoids are a natural subclass of eicosanoids generated mainly from metabolic oxidation of arachidonic acid. Cyclopentenone prostaglandins (cyPGs) contain a highly reactive α,β-unsaturated carbonyl group in their cyclopentenone ring and possess three main potentially therapeutic properties: anti-inflammatory, antiproliferative and antiviral. We designed and synthesized EC and its derivatives in reducing secretion of pro-inflammatory cytokines IL-6 and IL-12. Mucosal-Associated Invariant T (MAIT) Cells are unique innate-like T cells and play a key role in host defense against bacterial and fungal infection as well as in human autoimmune diseases. The MAIT cells are activated through T-cell receptor αβ chain (TCR-αβ) binding with the MR1-ligand, which is vitamin B metabolites presented on MR1. Rribityllumazines, one of important MR1-ligand was synthesized in my study.

Antimicrobial peptides

Ceragenin

Cationic Steroid Antimicrobial

Nanoparticle

Cyclopentenone prostaglandins

Mucosal-Associated Invariant T

Rribityllumazines

Biochemistry

Physical Sciences and Mathematics

IGA MEDIATED DEFENSES AGAINST HIV-1

Wright, Alison Laing

08 February 2008

No description available.

Health Sciences, Immunology

IgA

Immunoglobulin

HIV

Human immunodeficiency virus

Intracellular Neutralization

Viral Excretion

Mucosal

Immunology

Epithelial

polymeric immunoglobulin receptor

pIgR

MECHANISTIC UNDERSTANDING OF THE REGULATION OF LUNG RESIDENT MEMORY T CELLS INDUCED BY TB VACCINATION STRATEGIES

Haddadi, Siamak

January 2018

In the recent years, it has been well established that primary respiratory viral infection-induced lung resident memory CD8 T cells (TRM) characterized by the expression of integrins CD49a and CD103, as well as the early-activation marker CD69, constitute the first line of defense against reinfection. On the other hand, viral vector-based respiratory mucosal (RM) vaccination, as well as parenteral vaccination followed by airway luminal manipulation induce lasting and protective lung T cell immunity towards pulmonary tuberculosis (TB). However, it remains poorly understood whether and how these TB vaccination strategies induce TRM in the lung. As such, within this thesis we will investigate generation of lung CD8 TRM upon different TB vaccination strategies and the underlying mechanisms regulating establishment of such cells. Here using distinct models of replication-deficient adenoviral vector-based TB vaccination, we find that RM vaccination leads to generation of lung CD8 TRM identified by the expression of CD69, CD103, and very late activation Ag 1 (VLA-1). These TRM-associated molecules are acquired by CD8 T cells in distinct tissues. In this regard, VLA-1 is acquired during T cell priming in draining mediastinal lymph nodes (dMLNs) and the others acquired after T cells entered the lung. Once in the lung, Ag-specific CD8 TRM continue to express VLA-1 at high levels through the effector/expansion, contraction, and memory phases of T cell responses. We also reveal that VLA-1 is not required for homing of these cells to the lung, but it negatively regulates them in the contraction phase. Furthermore, VLA-1 has a negligible role in the maintenance of such cells in the lung. Separately, we have observed that while parenteral intramuscular vaccination alone does not induce lung CD8 TRM, subsequent RM inoculation of an Ag-dependent, but not a non-specific inflammatory agonist induces lung CD8 TRM. Such generation of lung CD8 TRM needs CD4 T cell help. These findings not only fill the current knowledge gap, but also hold important implications in developing effective vaccination strategies towards mucosal intracellular infectious diseases such as acquired immunodeficiency syndrome (AIDS), TB and herpes virus infection. / Thesis / Doctor of Philosophy (PhD)

Platelet Function in Dogs with Chronic Liver Disease

Wilkinson, Ashley R.

10 June 2019

Background: Dogs with acquired chronic liver disease often have hemostatic derangements. It is currently unknown whether dogs with acquired chronic liver disease have decreased platelet function and alterations in von Willebrand factor (vWF) that may contribute to hemostatic abnormalities. Hypothesis: Dogs with chronic liver disease have prolonged platelet closure time (CT), assessed with the PFA-100®, and buccal mucosal bleeding time (BMBT), and increased vWF concentration compared to healthy dogs. Animals: Eighteen dogs with chronic acquired liver disease undergoing ultrasound-guided needle biopsy of the liver or laparoscopic liver biopsy and eighteen healthy age-matched control dogs. Methods: Prospective study. BMBT, CT using the PFA-100®, and vWF antigen were measured in dogs with chronic liver enzyme elevation undergoing ultrasound-guided needle biopsy of the liver or laparoscopic liver biopsy. After undergoing ultrasound-guided needle biopsy, dogs were monitored for hemorrhage with serial packed cell volume measurements and focused assessment with sonography. An unpaired t-test was used for normally distributed data and the Mann-Whitney test was used when non-Gaussian distribution was present. The level of significance was set at P <0.05. Results: The CT was not different between the two groups (P = 0.27). The BMBT was significantly longer in the liver disease group compared to the control group (P = 0.019). There was no difference in the mean vWF antigen of the two groups (P = 0.077). Conclusions and clinical relevance: These results demonstrate mild impairment of primary hemostasis in dogs with chronic liver disease based on prolongation of BMBT. / Master of Science / Background: Dogs with chronic liver disease often have abnormal blood clotting activity. It is currently unknown whether dogs with chronic liver disease have decreased platelet function and alterations in von Willebrand factor (vWF) that may contribute to blood clotting abnormalities. Platelet function can be assessed using the PFA-100®, which measures platelet closure time (CT), and buccal mucosal bleeding time (BMBT). The PFA-100 simulates blood in circulation to assess platelet function. BMBT is a crude but readily available test to assess platelet function in practices without sophisticated methods of assessing platelet function. Hypothesis: Dogs with chronic liver disease have prolonged CT and BMBT, which both suggest platelet dysfunction. Additionally, dogs with chronic liver disease have increased vWF concentration compared to healthy dogs. Animals: Eighteen dogs with chronic acquired liver disease undergoing ultrasound-guided needle biopsy of the liver or laparoscopic liver biopsy and eighteen healthy age-matched control dogs. Methods: Prospective study. BMBT, CT, and vWF antigen were measured in dogs with chronic liver disease undergoing ultrasound-guided needle biopsy of the liver or laparoscopic liver biopsy. After undergoing ultrasound-guided needle biopsy, dogs were monitored for hemorrhage. Results: The CT was not different between the two groups but the BMBT was significantly longer in the liver disease group compared to healthy dogs. There was no difference in the mean vWF antigen between the two groups. Conclusions and clinical relevance: These results demonstrate mild impairment of blood clotting activity in dogs with chronic liver disease based on prolongation of BMBT compared to healthy dogs. Prolongation of BMBT compared to healthy dogs is suggestive of endothelial dysfunction and/or platelet dysfunction in dogs with chronic liver disease.

Platelet function

liver disease

chronic hepatitis

PFA-100

closure time

buccal mucosal bleeding time

von Willebrand factor

liver biopsy

Étude des facteurs influençant la susceptibilité à l'infection au VIH chez des femmes africaines

Lajoie, Julie

12 1900

Chez la femme, la majorité des cas d’infection au VIH sont acquis lors de relations hétérosexuelles. Cependant, très peu d’informations sont disponibles concernant l’immunité locale naturelle du tractus génital féminin, les facteurs influençant la susceptibilité à l’infection au VIH dans ce compartiment, ainsi que la réponse immunitaire de la muqueuse enclenchée après l’infection. Le but de notre projet est donc d’étudier certains facteurs pouvant être impliqués dans la susceptibilité à l’infection au VIH, afin de mieux comprendre l’immunité du tractus génital féminin. Nous avons, dans un premier temps, analysé le rôle du polymorphisme des gènes HLA-G et HLA-E sur la susceptibilité au VIH dans une population de femmes zimbabwéennes. La présence de l’allèle HLA-G*0105N, en combinaison avec le génotype HLA-EG/HLA-EG, était associée avec une diminution du risque d’infection. Puis, dans une étude cas-contrôle de travailleuses du sexe (TS) du Bénin, nous avons mesuré l’expression de HLA-G soluble au niveau du plasma. Nous avons observé une différence significative dans l’expression de HLA-G soluble, celle-ci étant plus faible dans le groupe des TS VIH positives comparé aux groupes de TS VIH négatives et de femmes VIH négatives de la population générale. Nous avons aussi analysé l’expression de cytokines et chimiokines dans le sérum et le tractus génital des participantes de l’étude du Bénin. Nous avons constaté que chez les TS VIH positives il y avait une expression plus élevée des chimiokines MPC-3, IP-10 et MIG dans le tractus génital et le sérum comparativement aux deux autres groupes. Les patrons d’expression des cytokines variaient selon les compartiments : le niveau de TNF-α et IFN-γ était plus élevé dans le tractus génital des TS VIH positives, alors que le niveau d’IL-2, d’IL-10 et de TNF-α était plus faible dans le sang des TS VIH positives, comparativement aux deux autres groupes. Ainsi, au niveau du tractus génital des femmes VIH positives, il semble y avoir une activation chronique du système immunitaire dans le but de favoriser la dissémination/perpétuation du virus. Les patrons d’expression différents entre le milieu systémique et génital nous montrent que l’immunité présente dans un compartiment n’est pas nécessairement le reflet de l’autre. Nous avons aussi observé une augmentation significative des niveaux d’IL-4, de MIP-1α, de MIP-1β et de MCP-1 dans le sérum des TS VIH négatives. Ces personnes, hautement exposées mais non infectées, semblent démontrer une plus grande capacité à enclencher une réponse immunitaire précoce pour empêcher la dissémination du virus. Notre étude a donc permis d’acquérir de nouvelles connaissances sur l’immunité du tractus génital féminin en relation avec l’infection au VIH. / Initial exposure to HIV during heterosexual transmission occurs in the female genital tract. However, little is known about the local immunity, the factors influencing the susceptibility to HIV infection and the immune response in the female genital tract against HIV infection. The aim of this study is to analyse some factors that could be implicated in the susceptibility to HIV infection and to analyse, in part, the immunity present in the female genital tract. We investigated the role of HLA-G and HLA-E in the susceptibility to HIV infection in a cohort of Zimbabwean women. We found that the presence of HLA-G*0105N allele in combination with the genotype HLA-EG/HLA-EG was associated with a decrease in the risk of HIV infection. We also measured the expression of soluble HLA-G in a study of commercial sex workers (CSW) in Benin. Levels of soluble HLA-G were lower in the HIV-1-infected CSWs compared to those observed in both the HIV-1-uninfected CSWs and the HIV-1-uninfected women from the general population at low risk of infection. We also analysed the chemokine and cytokine expression patterns in the serum and female genital tract of the three groups of women. HIV-1-infected CSWs had significantly higher blood and genital levels of the chemokines IP-10, MCP-3 and MIG compared with those in both the HIV-1-uninfected CSW and non-CSW groups. HIV-1-infected CSWs had significantly higher genital mucosal levels of the cytokines TNF-α and IFN-γ compared with those in both the HIV-uninfected CSW and non-CSW groups. In contrast, the serum levels of the cytokines IL-2, IL-10 and TNF-α were lower in HIV-1-infected CSWs compared with those in the other groups. This suggests the presence of a constant immune cells recruitment and immune activation in the female genital tract in order to favour perpetuation and dissemination of the virus. Our results also demonstrate the important difference between the systemic and the mucosal immunity. We also observed a significant increase in the levels of IL-4, MIP-1α, MIP-1β and MCP-1 in the serum of the HIV-1-uninfected CSWs. It seems that these highly-exposed and yet uninfected women can have a better capacity to mount an early immune response against HIV. This study gives us new insights of the mucosal immunology of HIV infection.

VIH

HIV

HLA-G

HLA-G

Immunologie

Mucosal immunology

Sang

Africa

Afrique

Cytokines

Cytokines

Chemokines

Chimiokines

Étude du microenvironnement immunitaire des tumeurs du poumon avec réarrangement ALK et rôle des lymphocytes résidents mémoires dans les tumeurs muqueuses (poumon, ORL) / Analyse of the tumor microenvironment of ALK rearranged adenocarcinoma and key role of the resident memory T cells in mucosal tumor

Pinot Roussel, Hélène

17 November 2016

Les cancers du poumon se placent au quatrième rang des cancers tous sexes confondus et constituent la première cause de mortalité par cancer pour l’homme et la troisième chez la femme. Le pronostic est sombre avec une survie relative globale estimée à 43% à 1 an et 14% à 5 ans. Les adénocarcinomes, les carcinomes épidermoïdes et les carcinomes à grandes cellules selon la classification OMS 2015 correspondent à 85% de ces cancers. Les adénocarcinomes pulmonaires ont été scindés en de multiples entités grâce aux progrès des techniques de biologie moléculaire ayant permis d’identifier différentes mutations (EGFR, RAS..) ou réarrangement chromosomique (EML4-ALK), à l’origine de ces tumeurs. Différentes thérapies ciblées ont pu ainsi être développées afin de contrecarrer ces anomalies tels que le crizotinib en cas de réarrangement EML4-Alk ou l’erlotinib en cas de mutation de l’EGFR. Chacun de ces sous-types tumoraux a une présentation clinique et une évolution qui lui est propre. Nous nous sommes particulièrement intéressés au réarrangement ALK, car la génération de néoépitopes dérivés de ce réarrangement pourrait induire une réponse immunitaire. Par ailleurs, il avait été montré dans des lymphomes qu’une translocation NPM-ALK induisait l’expression de PD-L1 via Stat 3. Or la liaison de PD-L1 à PD-1 exprimé par les lymphocytes T (LT) délivre un signal inhibiteur à ces cellules. Ce mécanisme d’échappement constitue une cible thérapeutique via des anticorps qui bloquent cette interaction. Le premier objectif de ce travail a consisté à caractériser la réponse immunitaire effectrice (LT-CD8) et les mécanismes régulant cette réponse (expression de PD-L1, de PD1, infiltration par des LT régulateurs, perte du CMH de classe 1) dans les adénocarcinomes du poumon avec un réarrangement ALK. Cette étude a été réalisée avec une nouvelle méthode de quantification des cellules immunes reposant sur une analyse multiparamétrique in situ fluorescente avec une analyse spectrale permettant de s’affranchir des problèmes de compensation de fluorescence. J’ai montré que les tumeurs du poumon avec un réarrangement ALK exprimaient plus fréquemment PD-L1 que les tumeurs non mutées ou présentant une mutation de l’EGFR. Si le nombre médian de lymphocytes T-CD8+, exprimant ou non PD1 ne différait pas entre les différents groupes, nous avons montré que les tumeurs ALK réarrangé présentaient, avec une fréquence plus grande, une expression de PD-L1 associée à un infiltrat LT-CD8+ total ou intratumoral ou CD8+PD1+ total ou intra-tumoral supérieurs à la médiane. Cette corrélation n’était pas retrouvée, ni dans les ADC EGFR muté ni dans les ADC non ALK, non EGFR, non KRAS. L’expression de PD-L1 associée à l’infiltration par les LT-CD8 exprimant PD-1 sont considérées comme des biomarqueurs de réponse à l’immunothérapie par des anti-PD-1/PDL-1. Cette caractérisation du microenvironnement des tumeurs du poumon avec un réarrangement ALK pourrait permettre de mieux comprendre le profil de réponse des patients à cette immunothérapie. La paroi alvéolaire du poumon est une surface muqueuse séparant l’organisme du monde extérieur. Or il est connu que la réponse immunitaire muqueuse n’est pas similaire à la réponse observée dans le sang aussi bien en termes de phénotype des cellules présentes dans ces deux compartiments que par le mode de génération et d’induction de ces cellules. Dans un premier travail de l’équipe nous avons montré que seule une vaccination par voie nasale (voie muqueuse) permettait le recrutement dans une tumeur de la sphère ORL ou du poumon, de LT anti-tumoraux et la régression de tumeurs muqueuses ORL et pulmonaires, contrairement à une vaccination par voie systémique (intramusculaire). Cette efficacité de la vaccination muqueuse était associée à l’induction de lymphocytes T résidents mémoires (Trm) dans les sites muqueux (poumon, ORL) caractérisés par l’expression des intégrines CD103 et CD49a. (...) / Lung cancer is the most common cause of cancer-related mortality worlwide and a therapeutic challenge. Approximately 5% to 6% of non-small cell lung carcinoma (NSCLC) have chromosomal rearrangements of the anaplastic lymphoma kinase (ALK) gene, which mainly involve the echinoderm microtubule–associated protein-like 4 (EML4) gene as a partner. Even if the ALK tyrosine kinase inhibitor (TKI), crizotinib, has been successfully developed in these patients, resistance invariably occurs leading to tumor relapse. The ALK rearranged protein is immunogenic, was shown to induce PD-L1 and highlight the potential of immunotherapy in this cancer. The first issue of our work was to set up an immunofluorescence multiplex platform to comprehensively analyse the tumor microenvironment of a retrospective cohort of 29 ALK positive ADC, compared to 27 EGFR mutated ADC and 25 wild type ADC. Mean number of total CD8+T cells expressing or not PD-1 and the ratio of CD8/regulatory T cells weren’t significantly different between the various subgroups. The percentage of tumor cells expressing PD-L1 were higher in the ALK positive ADC, than in the EGFR positive ADC or WT lung cancer. We found a significant correlation in ALK positive ADC between the number of total or intratumoral (intraT) CD8+ or PD-1+CD8+T and the expression of PD-L1 by tumor cells suggesting a possible role of adaptive immunity in the regulation of PD-L1 on these tumor cells. Furthermore, the percentage of patients displaying two criteria of clinical response (% PD-L1 on tumor cells and infiltration by intraT PD-1+CD8+ or CD8+T cells) was higher in the ALK positive ADC. According to our results, a subgroup of ALK rearranged lung ADC patients may represent good candidates to be treated by anti-PD-1/PD-L1 antibodies. The alveolar wall is a mucosal site in contact with the environment. Resident memory T cells (Trm) found most prominently at mucosal sites represent a new subset of long lived memory T cells that remain in tissue and do not recirculate. Due to their role in local immunity, strategies to elicit Trm after vaccination have been developed. We and others clearly showed that mucosal immunization were more efficient than the conventional systemic route (intramuscular, subcutaneous) to elicit Trm at the mucosal tumor site. Indeed, the mucosal route of immunization imprints T cells with a mucosal homing program defined by a profile of integrin and chemokine receptors promoting their homing to the site of initial activation. A correlation was observed between the ability to elicit these cells at the tumor site and the control of tumor growth. The second issue of this work was to characterize in a mouse model Trm after mucosal cancer vaccine administration and in human lung cancer. We first developed various original strategies (mucosal immunization, use of mucosal vector, modulation of TGF, parabiosis experiments) to elicit or inhibit Trm in a preclinical model of head and neck cancer. All these experiments converged to demonstrate that the induction of Trm are required for the control of tumor growth. In order to extrapolate this role of Trm in humans, we found that the number of Trm correlated with a better overall survival in lung cancer in multivariate analysis. The induction of Trm may represent a new surrogate biomarker for the efficacy of cancer vaccine.

Cancer du poumon

ALK

PD-L1

Biomarqueurs

Tumeur muqueuse

Vaccin

Trm

Lung cancer

ALK

PD-L1

Biomarker

Mucosal tumor

Vaccin

Trm

616.99424