L'influence de l'hypoxie sur l'expression de podoplanine dans les fibroblastes associés au cancer (CAF) et son rôle dans la progression du cancer du sein / The influence of hypoxia on podoplanin expression in cancer-associated fibroblasts (CAF) and its role in the progression of breast cancer

Tejchman, Anna

06 April 2017

Le tissu tumoral comprend, outre les cellules cancéreuses, une matrice extra-cellulaire modifiée, les cellules endothéliales des vaisseaux sanguins et lymphatiques, immunes et inflammatoires et des fibroblastes actives associés au cancer (CAFs). La podoplanine (PDPN), glycoprotéine transmembranaire de type mucine, y est exprimée dans les cellules cancéreuses et les CAFs. Elleaidea la métastase comme montré dans le carcinome mammaire envahissant les ganglions lymphatiques. Ce travail montre que PDPN module l’interaction chimiokine/récepteur de l’axe CCL21/CCR7 et dépend de l’hypoxie. La progression tumorale est aidée par le stroma ou les CAFs ont des propriétés particulières par rapport aux fibroblastes normaux. Ils promeuvent la croissance tumorale, le recrutement des précurseurs endothéliaux et l’angiogenèse. Dans le carcinome mammaire, 80% des fibroblastes ont un phénotype CAF. Un modèle de CAFs exprimant la PDPN a permis de démontrer l’implication de CCL21/CCR7 dans la reconnaissance entre cellules tumorales et CAFs via la liaison CCL21/PDPN. Les CAFsPDPN+ secrètent des microARNs qui contrôlent des gènes des cellules cancéreuses. MiR-21 est un régulateur oncogène fondamental, par son action sur le suppresseur de tumeur PTEN. Nous avons analysé l’effet de miR-21, ainsi que de miR-210 et miR-29b sur PDPN dans les fibroblastes en hypoxie pour mimer le microenvironnement intratumoral et mis en évidence les différences biologiques comparativement à la normoxie ainsi que l’effet de la podoplanine sur l’angiogenèse par les cellules endothéliales en colocalization avec les CAFs exprimant la podoplanine et sur l’expression des facteurs proangiogéniques. / Tumor is a pathologic tissue including cancer cells, a modified extracellular matrix, endothelial cells, blood and lymphatic vessels, immune and inflammatory cells and activated fibroblasts called cancer-associated fibroblasts (CAFs). Podoplanin (PDPN), mucin-type transmembrane glycoprotein is expressed in tumor cells and CAFs, helps metastasis. Its role in metastaticprocess has been demonstrated for breast cancer cells into lymph nodes. Here we show that PDPN modulates the CCL21/CCR7 chemokine/receptor axis in a hypoxia-dependent manner. Cancer progression depends on the tumour stroma in which CAFs differ from normal fibroblasts. CAFs promote tumour growth, recruitment of endothelial progenitor cells and angiogenesis. In breast cancer up to 80% of fibroblasts display the CAF phenotype. Here a PDPN expressing model of CAFs made it possible to demonstrate the involvement of CCL21/CCR7 axis in the tumor cell-to-CAF recognition through podoplanin binding of CCL21. PDPN positive CAFs secrete microRNAs, which control gene expression at post-transcriptional level and influence cancer cells. MiR-21 is a key regulator of the oncogenic process, through its downstream target proteins among which the tumor suppressor, PTEN. We analyzed the effect of miR-21, but also oncogenic and hypoxia dependent miRs: miR-210 and miR-29b, on PDPN expression in fibroblasts in conditions mimicking the intra tumor microenvironment, i.e. in hypoxia. This points to crucial differences as compared to normoxia. Moreover we uncover the effect of podoplanin on angiogenesis by endothelial cells colocalizing with CAFs expressing podoplanin and on the expression of most prominent proangiogenic factors.

Carcinome mammaire

Fibroblastes associés au cancer (CAFs)

Hypoxie

Microenvironnement

Podoplanine (PDPN)

Mammary carcinoma

Cancer associated fibroblasts (CAFs)

Hypoxia

Microenvironment

Podoplanin (PDPN)

572.68

Studium epitelově mezenchymových interakcí v nádorech vycházejících z dlaždicových epitelů / Study of Epithelial Mesenchymal Interactions in Squamous Epithelium Derived Tumors

Kodet, Ondřej

January 2014

This thesis is focused on the epithelial mesenchymal interactions in tumors derived from squamous epithelium including tumors arising from minor cell population (melanocytes). This study is also reflecting aspects of epithelial glycobiology resp. the study of endogenous lectins, the galectins, in head and neck squamous carcinomas. Galectins represent, in the current concepts of cell and tumor biology molecules with a remarkable potential. Galectins participate, besides in regulation of pre- and postnatal homeostasis in normal tissues, also in many pathological processes such as autoimmune reactions or malignancies. In this thesis, we demonstrated the presence of galectin-1 and -2 and their glycoligands in interphasic and mitotic nuclei, which may contribute to regulation of the cell cycle. Furthermore, we demonstrated galectin-9 as a sensitive marker of transformation normal to the dysplastic squamous epithelium in head and neck. The epithelial mesenchymal interactions represent mechanisms, which are responsible for dynamic maintenance of the homeostasis of the organism during prenatal development, postnatal growth and during cyclic renewal of certain tissues. These interactions also participate in wound healing. On the other hand they play a crucial role in the process of tumor transformation,...

Studium epitelově mezenchymových interakcí v nádorech vycházejících z dlaždicových epitelů / Study of Epithelial Mesenchymal Interactions in Squamous Epithelium Derived Tumors

Kodet, Ondřej

January 2014

This thesis is focused on the epithelial mesenchymal interactions in tumors derived from squamous epithelium including tumors arising from minor cell population (melanocytes). This study is also reflecting aspects of epithelial glycobiology resp. the study of endogenous lectins, the galectins, in head and neck squamous carcinomas. Galectins represent, in the current concepts of cell and tumor biology molecules with a remarkable potential. Galectins participate, besides in regulation of pre- and postnatal homeostasis in normal tissues, also in many pathological processes such as autoimmune reactions or malignancies. In this thesis, we demonstrated the presence of galectin-1 and -2 and their glycoligands in interphasic and mitotic nuclei, which may contribute to regulation of the cell cycle. Furthermore, we demonstrated galectin-9 as a sensitive marker of transformation normal to the dysplastic squamous epithelium in head and neck. The epithelial mesenchymal interactions represent mechanisms, which are responsible for dynamic maintenance of the homeostasis of the organism during prenatal development, postnatal growth and during cyclic renewal of certain tissues. These interactions also participate in wound healing. On the other hand they play a crucial role in the process of tumor transformation,...

Role fibroblastů při hojení ran a rakovině / Role of fibroblasts in wound healing and cancer

Mateu Sanz, Rosana

January 2021

Fibroblasts are stromal cells ubiquitously present in the human body. They often appear in a quiescent state and can become activated in response to tissue remodeling signals. Activated fibroblasts acquire biosynthetic, pro-inflammatory and contractile properties, key functions for wound healing. In addition, the presence of permanently activated fibroblasts is one of the hallmarks of cancer. The purpose of this work is to investigate the differences between newborn and adult fibroblasts and keratinocytes in their implication in scarless wound healing, the origin of cancer associated fibroblasts (CAF)s and the influence of fibroblasts in melanoma invasion. Evidence suggests that wounds heal almost without scar in newborns. To understand the mechanisms that contribute to scarless wound healing we focused on the differences between newborn and adult fibroblasts and keratinocytes, which are cells present in human skin and participating in wound healing process. A comparison of the expression profile between newborn and adult fibroblasts showed differentially regulated genes related to the acute phase of the inflammatory response and ECM organization, traits involved in wound healing. We also found that newborn fibroblast showed higher differentiation potential, exhibited markers of pluripotency and...

Gene expression profiling of human lymph node-positive gastric adenocarcinomas

Foerster, Susann

12 January 2011

In dieser Arbeit wurden Genexpressionsprofile diffuser und intestinaler Magenadenokarzinome mittels Microarray-Technik erstellt. Der intestinale Typ konnte als stark proliferierender Tumor mit signifikanter Überexpression von zellzyklusrelevanten Genen definiert werden, während der diffuse Typ als stark stromaabhängig mit signifikanter Überexpression von Genen der extrazellulären Matrix hervortrat. Thrombospondin 4 (THBS4) wurde dabei als das am stärksten differentiell exprimierte Gen identifiziert, wobei seine mRNA in diffusen Tumoren eminent überexprimiert wird. Immunhistochemische Studien bestätigten diese starke Überexpression auf Proteinebene und zeigten, dass THBS4 eine übermäßig angereicherte extrazelluläre Komponente des Tumorstromas ist. Kolokalisierungsstudien zeigten zudem, dass THBS4-positive Zellen auch positiv für Vimentin und Smooth muscle actin (alpha) sind. Diese Ergebnisse belegen, dass THBS4 von Tumor-assoziierten Fibroblasten (TAF) exprimiert wird. Dies konnte durch zusätzliche in vitro Experimente bestätigt werden, die aufzeigten, dass TAF von diffusen Tumoren eine stärkere THBS4-mRNA Expression aufweisen als normale Fibroblasten des Magens. Abschließend konnten in vitro Kokultur-Studien aufdecken, dass die THBS4-Expression in Fibroblasten durch Tumorzellen diffuser Magentumore transkriptionell stimuliert wird. Metastasenbefall regionaler Lymphknoten (N+) ist bei den meisten Magenadenokarzinomdiagnosen bereits vorhanden. Dieser ist der stärkste derzeit verfügbare Parameter zur Abschätzung der Prognose, reicht aber für eine eindeutige Vorhersage nicht aus. Um ergänzende molekulare Prognoseindikatoren zu identifizieren, wurden aus den Microarray-Daten Gene, deren Expression mit dem klinischen Verlauf von N+ Patienten korreliert, extrahiert. Einige dieser Gene, z.B. RAN binding protein 17 und ras-related associated with diabetes, konnten mittels quantitativer real-time PCR als Marker für verkürztes progressionsfreies Überleben validiert werden. / In this work, gene expression profiles of diffuse and intestinal-type gastric adenocarcinomas were established using the microarray technique. The intestinal type was identified to be a highly proliferative entity with significant overexpression of cell cycle-relevant genes, whereas the diffuse type was proven to be strongly stroma-dependent with significant overexpression of extracellular matrix genes. Thrombospondin 4 (THBS4) was identified as the gene most differentially expressed between the two types with vast mRNA overexpression in diffuse-type tumors. Immunohistochemical studies proved overexpression on protein level and elucidated that THBS4 is a heavily accumulated extracellular constituent of the tumor stroma. Colocalization studies uncovered that THBS4-positive cells are also positive for vimentin and alpha-smooth muscle actin. These data signify that THBS4 is expressed by subpopulations of cancer-associated fibroblasts (CAFs). This was further evidenced by in vitro experiments demonstrating that THBS4 mRNA expression is increased in CAFs of diffuse-type tumors compared to normal gastric fibroblasts. Finally, in vitro coculture studies revealed that transcriptional THBS4 expression in fibroblasts is stimulated by diffuse-type gastric tumor cells. Metastatic involvement of regional lymph nodes (N+) usually accompanies diagnosis of gastric adenocarcinoma and is currently considered the most important parameter for assessment of prognosis. However, estimation of prognosis based on this parameter alone is not sufficiently reliable. In order to identify additional molecular prognosis markers, genes whose expression correlates with clinical outcome of N+ patients were extracted from the microarray data. Via quantitative real-time PCR, several genes, e.g. RAN binding protein 17 and ras-related associated with diabetes, were successfully validated to allow an expression-based stratification of patients with respect to disease-free survival.

Prognose

Genexpressionsprofilierung

Magenadenokarzinom

Tumorstroma

extrazelluläre Matrix

Tumor-assoziierte Fibroblasten

N-Stadium

klinischer Verlauf

prognosis

gene expression profiling

gastric adenocarcinoma

tumor stroma

extracellular matrix

cancer-associated fibroblasts

N-stage

clinical outcome

570 Biowissenschaften, Biologie

32 Biologie

XH 2600

ddc:570

Rôle du récepteur des androgènes dans les communications cellulaires au sein du cancer de la prostate / Role of androgen receptor in cellular communications in prostate cancer

Schreyer, Edwige

12 October 2018

La castration représente le traitement de référence du cancer de la prostate à un stade avancé. Cependant, la plupart des patients rechute du fait notamment de l’émergence de variants tronqués constitutivement actifs du récepteur des androgènes (RA). Le microenvironnement tumoral, en particulier les fibroblastes associés au cancer (CAFs), favorisent largement la progression tumorale. Ils sont très hétérogènes et dérivent de plusieurs types cellulaires dont les cellules souches mésenchymateuses (MSCs). Afin de mettre à jour l’impact des variants du RA sur le microenvironnement tumoral, mon projet de thèse a porté sur l’étude des effets de ces variants du RA sur la différenciation des MSCs en CAFs. Les résultats obtenus m’ont permis de démontrer un impact positif du variant RA Q641X sur l’expression du facteur de différenciation VEGF par les cellules tumorales, ainsi que sur l’expression des marqueurs de différenciation en CAFs FSP-1, CXCL12, PDGFR-β, ainsi que VEGF, au niveau des MSCs. Ces données suggèrent que le variant RA Q641X est capable d’induire la différenciation des MSCs en CAFs, soulignant ainsi l’importance de développer de nouvelles stratégies thérapeutiques ciblant ces variants du RA. / Androgen ablation therapy remains the most common treatment for patients with advanced prostate cancer. However, most patients will relapse due to the emergence of truncated constitutively active androgen receptor (AR) variants. The tumor microenvironment is another necessary feature driving prostate cancer progression. Cancer associated fibroblasts (CAFs) are the major specialized stromal cells that favor tumor progression. These cells are very heterogeneous and derive from several other cell types as mesenchymal stem cells (MSCs). In order to highlight the impact of AR variants on surrounding tumor stroma, the aim of my project was to investigate the effects of these AR variants on MSCs differentiation into CAFs. I noticed that the expression of VEGF, a CAF differentiation factor, was upregulated in tumor cells expressing AR Q641X variant. Similarly, the expression of CAF differentiation markers FSP-1, CXCL12, PDGFR-β, and VEGF was enhanced in MSCs in presence of AR Q641X variant. These data highlight an unknown property of AR Q641X variant in prostate tumor cells that is its ability to induce MSCs differentiation into CAFs, underlining the urgent need to develop novel strategies targeting these AR variants.

Cancer de la prostate

Microenvironnement tumoral

Fibroblastes associés au cancer

Cellules souches mésenchymateuses

Prostate cancer

Tumor microenvironment

Cancer associated fibroblasts

Mesenchymal stem cells

572.8

616.99

Rôle de la cytokine Leukemia Inhibitory Factor (LIF) dans l'activation et le maintien des fibroblastes pro-invasifs lors de la carcinogénèse / Role of Leukemia inhibitory Factor in the activation and maintenance of pro-invasive fibroblasts in cancer

Albrengues, Jean

03 December 2014

Le stroma inflammatoire joue un rôle primordial lors de la carcinogénèse. Dans ce contexte, nous montrons que la cytokine LIF est à l'origine d'une population de fibroblastes capable de remodeler la matrice extracellulaire de manière à la rendre permissive à l'invasion collective des cellules tumorales. En effet, nous montrons que la production de LIF par les cellules tumorales et fibroblastiques, après une stimulation au TGFβ, va réguler les capacités contractiles et pro-invasives de ces dernières via la régulation du cytosquelette d'acto-myosine et de manière indépendante de l'expression de α-SMA. En effet, l'inhibition pharmacologique des kinases JAKs permet de bloquer l'environnement fibrotique des tumeurs et d'ainsi bloquer l'invasion des cellules tumorales in vitro et in vivo. Nous montrons ensuite que LIF est à l'origine d'un switch épigénétique responsable de l'activation constitutive de la voie de signalisation JAK1/STAT3. Ce processus, régulé par la forme acétylée de STAT3, et son interaction avec l'ADN methyltransférase DNMT3b permet l'hypermethylation du promoter de la phosphatase SHP1 et donc la phosphorylation constitutive de JAK1. Une fois mis en place, ce nouveau profil de méthylation est maintenu par DNMT1. La surexpression de LIF dans les carcinomes humains corréle avec un environnement fibrotique, la présence de nodules invasifs et un mauvais pronostic clinique. De même, il existe une forte corrélation négative entre l'acétylation de STAT3 et l'expression de SHP1 dans le stroma tumoral. Nos résultats montrent qu'inhiber l'activité des DNMT et des kinases JAK permet de reprogrammer les capacités pro-invasive des fibroblastes associés aux carcinomes. / Signaling crosstalk between tumor cells and fibroblasts confers proinvasive properties to the tumor microenvironment. We identify LIF as a tumor promoter that mediates proinvasive activation of stromal fibroblasts independent of alpha-smooth muscle actin expression. We demonstrate that a pulse of transforming growth factor β (TGF-β) establishes stable proinvasive fibroblast activation by inducing LIF production in both fibroblasts and tumor cells. In fibroblasts, LIF mediates TGF-β-dependent actomyosin contractility and extracellular matrix remodeling, which results in collective carcinoma cell invasion. Indeed, pharmacological inhibition of JAK activity by counteracts fibroblast-dependent carcinoma cell invasion in vitro and in vivo. We next unveil that LIF initiates an epigenetic switch leading to the constitutive activation of JAK1/STAT3 signaling, which results in sustained pro-invasive activity of fibroblasts. The process is mediated by p300-histone acetyltransferase acetylation of STAT3, and DNA methyltransferase DNMT3b, which induce the hypermethylation of SHP1 phosphatase promoter and results in constitutive phosphorylation of JAK1. Sustained JAK1/STAT3 signaling is maintained by DNMT1. Accordingly, carcinomas display strong LIF upregulation, which correlates with dense collagen fiber organization, cancer cell collective invasion, and poor clinical outcome. Moreover, we show that STAT3 acetylation and phosphorylation are inversely correlated with SHP1 expression in tumors stroma. Combined inhibition of DNMT activities and JAK signaling results in long-term reversion of CAF-associated pro-invasive activity and restoration of the wild-type fibroblast phenotype.

Micro-environnement tumoral

Fibroblastes associés aux carcinomes

Invasion tumorale

Fibrose

Leukemia Inhibitory Factor

JAK/STAT

Épigénétique

Tumor microenvironment

Cancer associated fibroblasts

Tumor invasion

Fibrosis

Leukemia Inhibitory Factor

JAK/STAT signaling

Epigenetics

Empéripolèse des cellules de lymphomes humains Ramos par les fibroblastes

Oualha, Nadia

12 1900

No description available.

Microenvironnement tumoral

Stroma tumoral

Fibroblastes associés au cancer

VCAM-1

VLA-4

vimentine

Migration transcellulaire

Ramos

Cellules de lymphome

Tumor microenvironment

Tumor stroma

Cancer-associated-fibroblasts

Vimentin

Lymphoma cells

Transcellular migration

Dipeptidyl peptidáza-IV a Fibroblastový aktivační protein v gliomagenezi. / Dipeptidyl peptidase-IV and Fibroblast activation protein in gliomagenesis.

Trylčová, Jana

January 2018

"Dipeptidyl peptidase-IV Activity and/or Structure Homologues"(DASH) represent a newly defined group of multifunctional molecules, typically bearing dipeptidyl peptidase-IV- like hydrolytic activity. Dipeptidyl peptidase-IV (DPP-IV) cleaves out X-Pro dipeptides from the N-terminus of peptides. Other molecules carrying similar enzyme activity, such as Fibroblast activation protein (FAP), DPP-II, DPP8 and DPP9 or even DPP-IV structure-like but hydrolytically inactive molecules (DPP6 and DPP10) also belong to this group. Recent knowledge suggest a substantial role of DASH in cancer pathogenesis. The aim of this study is a preparation of a biological model and its use for understanding the mechanisms of interaction(s) between transformed glial cells and stroma in the processes of origin and development of tumors derived from neuroectoderm. Stable transfected human glioblastoma cell lines with inducible gene expression of DPP-IV, Fibroblast activation protein and their enzymatically inactive mutated forms, were prepared within the project. Prepared cell lines are used as a tool for studying not only the "autocrine" importance of DPP-IV and FAP for the expressing cells in in-vitro, but also for their potential "paracrine" effect(s) within the tumor microenvironment after homotopic implantation into the...