Targeting the Hippo Signaling Pathway in Atypical Teratoid Rhabdoid Tumor

Norris, Gregory

26 May 2017

A Thesis submitted to The University of Arizona College of Medicine - Phoenix in partial fulfillment of the requirements for the Degree of Doctor of Medicine. / Atypical teratoid rhabdoid tumor (ATRT) is a highly malignant pediatric central nervous system tumor. The prognosis is often poor, with a 2‐year survival rate estimated at 15%. This dismal prognosis highlights the need to develop new treatment modalities for this devastating pediatric tumor. Recently, a tumor suppressing signaling pathway known as Hippo has emerged as a possible cancer treatment target. The Hippo signaling pathway is involved in organ growth and maintenance, and is dysregulated in many diverse cancers. We used quantitative real‐time PCR to evaluate the mRNA expression profile of Hippo pathway genes. We then used determined the protein expression of various Hippo components using Western blots. The results of this study suggest that Hippo plays a definite role in atypical teratoid rhabdoid tumor.

Cancer

Pediatric

Brain Tumor

Atypical Teratoid Rhabdoid Tumor

Hippo Signaling Pathway

Verteporfin

Propojení buněčné signalizace a metabolismu v nádorových buňkách. / Interplay between cellular signaling and metabolism in cancer cells.

Záhumenská, Romana

January 2017

Hippo signaling pathway represents organ size control mechanism constrained between all metazoans. Individual components of the Hippo signaling pathway were identified as key tumor-suppressors which phosphorylate and inhibit activity of several oncogenic factors and signaling pathways (such as YAP/TAZ, PI3K and mTOR). MST1 kinase is a part of central protein complex of the Hippo signaling pathway and its activation is involved in anti-cancer activity of several drugs. We have demonstrated activation of the MST1 kinase by natural compounds in leukemic cells followed by inhibition of proliferation and induction of apoptosis. Shikonin represents natural naphthoquinonic compound isolated from Lithospermum erythrorhizon which acts as inhibitor of glycolysis and mitochondrial respiratory chain in human cells. Shikonin induces fast activation of the MST1 protein in leukemic cells however mechanism of this activation remains unknown. Therefore, we tried to characterize posttranslational modifications of the MST1 kinase during shikonin treatment of leukemic cells. Firstly, we isolated MST1 kinase from control and shikonin-treated cells using immunoprecipitation. Then we characterized posttranslational modifications of the MST1 protein employing mass spectrometry. Using this approach we found out...

Homeobox A4 Suppresses Vascular Remodeling as a Novel Regulator of YAP/TEAD Transcriptional Activity / ホメオボックスA4はYAP/TEAD転写活性の新規制御因子として、血管リモデリングを抑制する

Kimura, Masahiro

25 May 2020

京都大学 / 0048 / 新制・課程博士 / 博士(医学) / 甲第22641号 / 医博第4624号 / 新制||医||1044(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 山下 潤, 教授 湊谷 謙司, 教授 江藤 浩之 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

Hippo signaling

vascular smooth muscle cells

vascular remodeling

YAP/TEAD pathway

HOX genes

490

Inactivation of the Hippo tumor suppressor pathway promotes melanomagenesis

Vittoria, Marc Anthony

04 February 2022

Melanoma, a malignant neoplasm of melanocytes, is the most lethal form of skin cancer. A majority of melanomas are driven by activating mutations in the kinase BRAF, which drives cellular proliferation through constitutive stimulation of the mitogen-activated protein kinase (MAPK) signaling pathway. Intriguingly, expression of oncogenic BRAF alone in vivo is insufficient to promote melanoma; rather, its expression leads to the development of benign nevi (moles) comprised of growth-arrested melanocytes. The acquisition of additional genetic or epigenetic changes is therefore critical for melanocytes to evade arrest and drive melanomagenesis, however the identity of these changes remains incompletely understood. Here we demonstrate that expression of oncogenic BRAF leads to activation of the Hippo tumor suppressor pathway in vitro, which acts to limit melanocyte proliferation through the inhibition of the pro-growth transcriptional co-activators YAP and TAZ. Melanocyte-specific inactivation of Hippo signaling in vivo, via deletion of the Hippo kinases Lats1/2 alone, or in conjunction with oncogenic Braf expression, potently induces melanoma development in mice. Collectively, our data reveal that the Hippo tumor suppressor pathway represents an important barrier to melanoma development, and implicates YAP and TAZ as new therapeutic targets for the treatment of human melanoma.

Molecular biology

BRAF

Hippo signaling

Melanoma

Mitotic slippage

Whole-genome doubling

YAP

Generation of human alveolar epithelial type I cells from pluripotent stem cells

Burgess, Claire Linnea

10 February 2024

In the distal lung, alveolar epithelial type I cells (AT1s) comprise the vast majority of alveolar surface area and are uniquely flattened to allow the diffusion of oxygen into the capillaries. This structure along with a quiescent, terminally differentiated phenotype has made AT1s particularly challenging to isolate or maintain in cell culture. As a result, there is a lack of established models for the study of human AT1 biology, and in contrast to alveolar epithelial type II cells (AT2s), little is known about the mechanisms regulating their differentiation. Here we engineer a human in vitro AT1 model system through the directed differentiation of induced pluripotent stem cells (iPSC). We first define the global transcriptomes of primary adult human AT1s, suggesting gene-set benchmarks and pathways, such as Hippo-LATS-YAP/TAZ signaling, that are enriched in these cells. Next, we generate iPSC-derived AT2s (iAT2s) and find that activating nuclear YAP signaling is sufficient to promote a broad transcriptomic shift from AT2 to AT1 gene programs. The resulting cells express a molecular, morphologic, and functional phenotype reminiscent of human AT1 cells, including the capacity to form a flat epithelial barrier which produces characteristic extracellular matrix molecules and secreted ligands. Our results indicate a role for Hippo-LATS-YAP signaling in the differentiation of human AT1s and demonstrate the generation of viable AT1-like cells from iAT2s, providing an in vitro model of human alveolar epithelial differentiation and a potential source of human AT1s that until now have been challenging to viably obtain from patients.

Cellular biology

Alveolar epithelial type I cells

Directed differentiation

Hippo signaling

Lung

Pluripotent stem cells

Role of Growth Regulatory Pathways in Eye Development and Differentiation

Wittkorn, Erika L.

05 June 2014

No description available.

Developmental Biology

Biology

Genetics

Differentiation

Hippo signaling pathway

eye development

Drosophila

Rôle des signalisations STAT3 et Hippo dans les gliomes : Identification de nouveaux biomarqueurs pronostiques et cibles thérapeutiques / Role of STAT3 and Hippo signaling pathways in glioma : Identification of new prognostic biomarkers and therapeutic targets

Masliantsev, Konstantin

04 December 2018

Les gliomes malins sont les tumeurs les plus fréquentes du système nerveux central. Les glioblastomes représentant plus de 50% des gliomes, constituent la forme la plus agressive et sont particulièrement résistants à la radiochimiothérapie. Au sein de ces tumeurs réside une sous-population de cellules souches tumorales (CSG) qui pourrait être responsable de leurs initiation, progression et résistance aux traitements. Ces processus sont gouvernés par des voies de signalisation, pour la plupart activées de manière constitutive et dont l’étude est nécessaire afin de mieux comprendre les mécanismes impliqués dans la gliomagenèse. L’objectif de ces travaux de thèse consistait en l’exploration des voies de signalisation STAT3 et Hippo dans les gliomes dans le but d’identifier de nouveaux marqueurs pronostiques et de nouvelles cibles thérapeutiques potentielles. La première partie de ces travaux a montré que la phosphorylation S727 de STAT3 jouait un rôle important dans la radioresistance des CSG et que son inhibition pharmacologique induisait leur radiosensibilisation. Dans un second temps, ces travaux ont montré que deux effecteurs de la signalisation Hippo, YAP1 et TEAD3, sont associés à un mauvais pronostic et qu’ils seraient impliqués dans la prolifération cellulaire et le phénotype des CSG notamment par inhibition de la signature proneurale. Ainsi, ces travaux visent à proposer de nouvelles pistes thérapeutiques, d’une part l’inhibition de la pS727-STAT3 afin de potentialiser les effets de la radiothérapie et d’autre part, les effecteurs de la signalisation Hippo comme biomarqueurs pronostiques et potentielles cibles thérapeutiques. / Malignant gliomas are the most common tumors of central nervous system. Glioblastomas represent more than 50% of all glioma and constitute the most aggressive form of the tumor which is particularly resistant to radiotherapy. The presence of the subpopulation of glioblastoma stem cells (GSC) could be involved in tumor initiation, progression and therapeutic resistance. Hence, these processes are governed by signaling pathways which are mostly constitutively activated and their study is necessary for a better understanding of gliomagenesis. The aim of this PhD thesis was to assess STAT3 and Hippo signaling pathways in glioma to identify new prognostic markers and potential therapeutic targets. The first part on this work showed that pS727 phosphorylation of STAT3 could be involved in radioresistance and its inhibition induced GCS radiosensitization. Additionally, this work showed that YAP1 and TEAD3, two effectors of Hippo signaling, are associated with poor patient survival and could be involved in GSC proliferation and phenotype maintenance by inhibiting proneural gene signature. Thereby, this work aims to offer new therapeutic avenues, on the one hand the inhibition of pS727-STAT3 for radiotherapy potentiation and on the other hand the effectors of Hippo signaling as prognostic biomarkers and potential therapeutic targets.

Gliome

Glioblastome

Cellules souches de glioblastomes

Radiorésistance

Stat3

Signalisation Hippo

Yap1

Tead3.

Glioma

Glioblastoma

Glioblastoma stem cells

Radioresistance

Stat3

Hippo signaling

Yap1

Tead3.

612.82

616.994

Role of TRIP6 and Angiomotins in the Regulation of the Hippo Signaling Pathway

Dutta, Shubham

16 March 2018

Mechanical tension is an important regulator of cell proliferation, differentiation, migration and cell death. It is involved in the control of tissue architecture and wound repair and its improper sensing can contribute to cancer. The Hippo tumor suppressor pathway was recently shown to be involved in regulating cell proliferation in response to mechanical tension. The core of the pathway consists of the kinases MST1/2 and LATS1/2, which regulate the target of the pathway, the transcription co-activator YAP/ TAZ (hereafter referred to as YAP). When the Hippo pathway is inactive, YAP remains in the nucleus and promotes cell proliferation and stem cell maintenance. When the Hippo signaling pathway is turned on, MST1/2 phosphorylate and activates LATS1/2. LATS1/2 phosphorylates and inactivates YAP in the cytoplasm which is sequestered and degraded, stopping cell proliferation and promoting differentiation of stem cells. Mechanical forces are transmitted across cells and tissues through the cell-cell junctions and the actin cytoskeleton. However, the factors that connect cell-cell junctions to the Hippo signaling pathway were not clearly known. We identified a LIM domain protein called TRIP6 that functions at the adherens junctions to regulate the Hippo signaling pathway in a tension-dependent manner. TRIP6 responds to mechanical tension at adherens junctions and regulates LATS1/2 activity. Under high mechanical tension, TRIP6 sequesters and inhibits LATS1/2 at adherens junctions to promote YAP activity. Conditions that reduce tension at adherens junctions by inhibition of actin stress fibers or disruption of cell-cell junctions reduce TRIP6-LATS1/2 binding, which activates LATS1/2 to inhibit YAP. Vinculin has been shown to act as part of a mechanosensory complex at adherens junctions. We show that vinculin promotes TRIP6 inhibition of LATS1/2 in response to mechanical tension. Furthermore, we show that TRIP6 competitively inhibits MOB1 (a known LATS1/2 activator) from binding and activating LATS1/2. Together these findings reveal TRIP6 responds to mechanical signals at adherens junctions to regulate the Hippo signaling pathway in mammalian cells.

Hippo signaling pathway

TRIP6

vinculin

LATS

MOB

YAP

stretch

mechanosensing

mechanical tension

adheres junction

cell junction

Biology

Cell and Developmental Biology

Élucidation des rôles de YAP1 et TAZ dans l'ovaire chez la souris

Godin, Philippe

12 1900

L’ovaire est un organe indispensable à la fonction reproductive, car il permet la production, la maturation et la libération de la cellule germinale femelle, l’ovocyte. Malgré son rôle central dans la régulation de la reproduction chez la femme, plusieurs de ses processus physiologiques et de ses conditions pathologiques sont encore imparfaitement décrits. La caractérisation du rôle de nouveaux régulateurs pourrait permettre l’élucidation de plusieurs questionnements actuels en physiologie ovarienne. Initialement étudiée dans l’organogenèse et l’oncogenèse pour son implication dans la prolifération, la migration, la différenciation et l’apoptose cellulaire, la voie de signalisation Hippo pourrait s’avérer être un facteur déterminant dans la physiologie ovarienne. En effet, elle a été récemment rapportée comme participant à la régulation de l’activation folliculaire, de la prolifération des cellules de la granulosa et de l’ovulation. La voie Hippo consiste en une cascade de kinases menant ultimement à la phosphorylation des deux co-régulateurs transcriptionnels YAP1 (yes-associated protein 1) et TAZ (transcriptional coactivator with a PDZ-binding motif). L’objectif général de ce projet de thèse était de caractériser les rôles de Yap1/Taz dans la physiologie ovarienne en utilisant des modèles murins transgéniques d’inactivation conditionnelle de ces gènes dans les cellules de la granulosa. La première portion du projet a conduit à la caractérisation d’un phénotype inattendu de défaut des oviductes. Les souris femelles adultes étaient sous-fertiles et leur fonction ovarienne était intacte. En fait, la sous-fertilité était causée par le piégeage des embryons dans des dilatations de la paroi de l’oviducte, empêchant ainsi leur transport adéquat vers l’utérus. Nous sommes parvenus à démontrer que la perte d’expression de YAP1/TAZ dans les couches musculeuses de l’oviducte conduisait à un amincissement progressif de sa paroi et était ultimement responsable de l’échec du transport embryonnaire. Dans la seconde portion du projet, nous avons utilisé la culture primaire de cellules de la granulosa afin de décrire l’implication de la voie Hippo dans l’ovulation. Nous avons identifié la protéine kinase A comme modulateur clé de l’activation de la voie Hippo par l’hormone lutéinisante (LH). En utilisant un système adénoviral de délétion de Yap1/Taz, nous avons mis en évidence l’importance de leur expression pour l’induction de plusieurs gènes cibles de la LH. Ensuite, au moyen d’une expérience d’immunoprécipitation de la chromatine, nous avons démontré l’implication de YAP1 dans la régulation de la transcription de l’amphiréguline, un effecteur central de la cascade de signalisation de la LH. Dans son ensemble, ce projet a permis de mettre la lumière sur de nouveaux rôles de la voie de signalisation Hippo dans la régulation des cellules musculaires lisses de l’oviducte et des cellules de la granulosa durant l’ovulation chez la souris. Elles ouvrent la voie à une investigation plus précise de l’implication de la voie Hippo dans ces deux organes clés du système reproducteur femelle. / The ovary is a central organ of the female reproductive tract involved in oocyte production, maturation and release. Still, many physiological and pathological ovarian processes remain to be described more comprehensively. The precise characterization of the roles of new ovarian regulators would contribute to a better understanding of its physiology. The Hippo signaling pathway was initially studied for its roles in cellular proliferation, apoptosis, migration and differentiation during organ and tumor development. Recently, it has been shown to be involved during normal physiological processes of multiple organs, including the ovary. Hippo was shown to be involved in the activation of primordial follicles, in the proliferation of granulosa cells and during ovulation. Hippo consists of a central kinase cascade leading to the phosphorylation of YAP1 (yes-associated protein 1) and TAZ (transcriptional coactivator with a PDZ-binding motif), the two transcriptional coactivators of the pathway. The objective of this thesis was to characterize the precise roles of Yap1/Taz in ovarian physiology using transgenic mouse models of their genetic deletion in granulosa cells. The first part of this thesis project led to the characterization of an unexpected oviductal phenotype. Adult females were subfertile and their ovarian function was unaffected. The subfertility was rather caused by the entrapment of embryos in oviductal dilations, preventing their normal transport to the uterus. We demonstrated that loss of YAP1/TAZ expression in oviductal smooth muscle cells led to a gradual thinning of the oviductal wall and was responsible for the embryo transport impediment. In the second part of this project, we cultured primary mouse granulosa cells to characterize the roles of the Hippo signaling pathway during ovulation. We showed that protein kinase A is a key effector of Hippo activation following the luteinizing hormone (LH) surge. We then demonstrated that Yap1/Taz expression is required for the induction of several LH target genes. Using a chromatin immunoprecipitation experiment, we were able to show that YAP1 drives the expression of amphiregulin, a key paracrine transmitter of the LH signal, during the early events of ovulation. Together, these results identified new roles of the Hippo signaling pathway in the regulation of oviductal smooth muscle cells and of granulosa cells during ovulation. This thesis project opens the door to new avenues of investigation of Hippo involvement in the regulation of the female reproductive system.

Reproduction

Voie de signalisation Hippo

YAP1

TAZ

Souris transgéniques

Oviducte

Cellules musculaires lisses

Ovaire

Ovulation

Cellules de la granulosa

Hippo signaling pathway

Transgenic mice

Oviduct

Ovary

Smooth muscle cells

Granulosa cells

Physiology / Physiologie (UMI : 0719)