Mécanisme d’action du PBI-1402 impliqué dans l’expansion des progéniteurs érythroïdes humains et murins

Vinet, Sabrina

08 1900

Une des complications importantes d’un traitement intensif de chimio/radio-thérapie est l’aplasie de la moelle osseuse qui peut persister longtemps même après une greffe de cellules souches. Le PBI-1402 est un petit lipide qui a été associé à la diminution de l’apoptose des neutrophiles induite par des agents cytotoxiques. Nos travaux ont démontré que la culture in vitro de progéniteurs hématopoiétiques humains en présence de PBI-1402 induit une augmentation significative du nombre de progéniteurs érythroides (PEryth) (p<0,05). En évaluant la sensibilité des PEryth à l’érythropoietine (Epo), nous avons démontré que le PBI-1402 n’a pas d’effet sensibilisateur et que les cellules répondent de façon similaire aux cellules contrôles. De plus, la combinaison de l’Epo et du « stem cell factor » avec le PBI-1402 permet de prolonger et d’augmenter l’activation d’ERK1/2 (p<0,05), un important signal mitogène. Cet effet est associé à une inhibition de l’activation de la phosphatase MKP-1 dans les cellules exposées au PBI-1402. Nous démontrons aussi la capacité du PBI-1402 à amplifier la prolifération des PEryth et sa capacité à réduire la durée et l’intensité de l’anémie dans un modèle in vivo murin. Des souris ayant reçu une dose létale d’irradiation et subi une transplantation syngénique de moelle osseuse, ont été traitées oralement avec le PBI-1402 pendant 14 jours. Ces souris démontrent une réduction significative de l’anémie post-transplantation versus les souris contrôle (p<0,05). De plus, la moelle osseuse des souris traitées au PBI-1402 présente un nombre de BFU-E et CFU-E plus élevé comparativement au contrôle. Ces résultats démontrent donc le potentiel du PBI-1402 à réduire l’anémie post-transplantation et accélérer la reconstitution érythroïde. / One of the most important complications of intensive radiotherapy or chemotherapy is cytopenia, which can persist for significant amount of time even after stem cell transplantation. PBI-1402, a small lipid, was previously shown to be associated with decreased neutrophil apoptosis caused by cytotoxic agents. Our work has shown that day primary human hematopoietic cell in vitro culture in the presence of PBI-1402 resulted in an increased number of erythroid progenitors (p<0,05). Dose-response experiments evaluating sensitivity to erythropoietin (Epo) of cells exposed to PBI-1402 indicated that PBI-1402 did not have a sensitizing effect and that both treated and control cells respond similarly to Epo. In addition, PBI-1402, used in combination with stem cell factor (SCF) and Epo, enhanced and prolonged ERK1/2 phosphorylation (p<0.05), a signalling pathway important for erythroid progenitor cell proliferation. This effect was associated with a decrease of the phosphatase MKP-1 activation in PBI-1402 exposed cells. This translated into and increased proliferation of erythroid progenitors as well as a reduced duration and level of anemia in an in vivo murine transplantation model. Lethally irradiated mice that received syngeneic stem cell transplantation were treated orally with PBI-1402 for 14 days. These mice demonstrated a significant reduction in post-transplantation anemia in a dose dependent manner compared to control (vehicle)(p<0.05). Moreover, PBI-1402-treated mice harboured significantly higher numbers of BFU-E and CFU-E in bone marrow compared to control (p<0.05). These results demonstrate that PBI-1402 treatment significantly reduced transplantation-induced anemia with concomitant acceleration in erythroid recovery.

Anémie

BFU-E

CFU-E

Epo

ERK1/2

Progéniteurs érythroïdes

Reconstitution érythroïde

PBI-1402,

SCF

MKP-1

Anemia

Erythroid progenitors

Erythroid reconstitution

Estudo fenotípico da região Aorta-Gônada-Mesonefros, de embriões de galinhas Gallus gallus domesticus, com ênfase na aorta dorsal / Phenotypic study of Aorta-Gonads-Mesonephros region of chicken embryos Gallus gallus domesticus emphasizing on the dorsal aorta

Patrícia Alzueta Moreno Martinez

10 October 2012

Conselho Nacional de Desenvolvimento Científico e Tecnológico / Acredita-se que os primeiros progenitores da hematopoese definitiva surjam da diferenciação do endotélio da aorta dorsal, na altura da região da Aorta-Gônada-Mesonefros (AGM). Com o intuito de estudar esta região e o fenótipo das células do endotélio da aorta dorsal nesta posição topográfica, ovos galados de Gallus gallus domesticus L. foram incubados em chocadeira, classificados em estádios de E16 a E25 e processados histotecnologicamente para obtenção de secções seriadas na altura da região AGM. Estas passaram por coloração por Hematoxilina-Eosina, histoquímica para PAS, PAS-diastase e Alcian Blue pH 1.0 e pH 2.5, histoquímica por lectinas fluoresceinadas e imunofluorescência para moléculas de superfície, citoesqueleto e matriz extracelular. Foi observada hipertrofia endotelial no assoalho da aorta nos estádios observados, o qual se apresentava positivo ao PAS, com ocorrência frequente de vacuolizações basais PAS negativas, e o surgimento ocasional de grupamentos celulares intravasculares. Nestes, as células que se destacavam da membrana basal do endotélio expressavam progressivamente mais material PAS positivo, o qual, no entanto, em nenhum momento pareceu se tratar de glicogênio. Em relação às glicosaminoglicanas, notamos a presença predominante de ácido hialurônico por todo o mesênquima da região e em outras estruturas como periferia da notocorda, tubo neural e mesoderma lateral. Ocorreu co-expressão de fibronectina e &#945;-actina de músculo liso em células circunjacentes à aorta, na face ventral do vaso. GFAP e BMP-4 são expressas entre as células do tubo neural e em sua periferia, assim como na notocorda do embrião. As lectinas Abrus precatorius, Lens culinarise Ricinus communis mostraram-se positivas principalmente na região subedotelial do assoalho da aorta nos estádios observados neste trabalho. Bandeiraea simplicifolia exibiu pouca marcação na aorta dorsal e a Arachis hypogeae foi negativa. Outras estruturas da região AGM também expressaram resíduos de açúcares revelados por estas lectinas, tais como: notocorda, tubo neural, mesênquima, intestino primitivo e saco vitelínico. Estes resultados acrescentam elementos morfológicos e bioquímicos ao conhecimento sobre a região AGM de embriões de galinha e sobre o endotélio, possivelmente hemogênico, da aorta dorsal. / Nowadays it is known that firsts definitive hematopoietic progenitors arise from endothelium differentiation of dorsal aorta, at Aorta-Gonad-Mesonephros (AGM) site. In order to study those events and cells phenotype of dorsal aorta endothelium in this topographical site, fertilized eggs of Gallus gallus domesticus L. were incubated, from E16 to E25 and to be processed by histotechonology to obtain serial sections of the AGM site. After this, they were stained with Hematoxilin-Eosin, histochemistry to PAS, diastase PAS and Alcian Blue pH 1.0 and pH 2.5, to obtain a better overview and characterization from cells, also, histochemistry to fluorescein lectins and immunofluorescense to surface molecules, cytoeskeleton andextracellular matrix were performed. Our results showed endothelial hypertrophy of the aorta floor in the stages analyzed, which shown positive for PAS, with frequent appearance of PAS negatives basal vacuolizations and an occasional intravascular cell clusters arise of. It was also observed that cells which were separated from endothelium basal membrane shown progressively were more PAS positive which however in any time seems to be glycogen. Regard of glycosaminoglycans we noted the main presence of hialuronic acid for all the mesenchymes site and in others structures like notochord periphery, neural tube and lateral mesoderm. It was observed fibronectin and smooth muscle &#945;-actin co-expression on aorta surrounding walls, at vessels ventral face. GFAP and BMP-4 are express between the cells of neural tube and surrounding it, as well as at embryo notochord. The lectins Abrus precatorius, Lens culinaris and Ricinus communis showed mostly positive expression on the sub endothelium site of the dorsal aorta floor at the stages analyzed in this work. Bandeiraea simplicifolia showed low expression on dorsal aorta and in Arachis hypogeae it was negative. Other structures of AGMs site also expressed sugar residues revealed by these lectins like: notochord, neural tube, mesenchyme, primitive gut and yolk sac.

Região AGM

Precursores hematopoiéticos

Embrião de galinha

Aorta dorsal

Fenótipo do endotélio

Perfil bioquímico

Hematopoietic progenitors

AGM site

Chicken embryo

Dorsal aorta

Endothelium phenotype

Biochemical profile

MORFOLOGIA

Estudo da proliferação, migração e diferenciação dos precursores neurais do sistema nervoso pós-natal de camundongos (Mus musculus) / Proliferation, migration and differentiation of neural precursor cells NPCs of the post-natal nervous system of mice (Mus musculus) / Estudio de la proliferación, migración y diferenciación de los precursores neurales del sistema nervioso posnatal de ratones (Mus musculus)

Delgado-Garcia, Lina Maria [UNESP]

02 May 2016

Submitted by LINA MARIA DELGADO GARCIA (linadelgadomvz@gmail.com) on 2016-06-03T17:50:42Z No. of bitstreams: 1 Diss_LinaMDelgadoGarcia_PPG_MV_FMVZ.pdf: 5259973 bytes, checksum: 96b8449017ba967633f1d9ef9da7c741 (MD5) / Approved for entry into archive by Juliano Benedito Ferreira (julianoferreira@reitoria.unesp.br) on 2016-06-06T18:25:40Z (GMT) No. of bitstreams: 1 delgado-garcia_lm_me_bot.pdf: 5259973 bytes, checksum: 96b8449017ba967633f1d9ef9da7c741 (MD5) / Made available in DSpace on 2016-06-06T18:25:40Z (GMT). No. of bitstreams: 1 delgado-garcia_lm_me_bot.pdf: 5259973 bytes, checksum: 96b8449017ba967633f1d9ef9da7c741 (MD5) Previous issue date: 2016-05-02 / No final dos anos 60, os experimentos em proliferação celular anunciaram a neurogênese adulta em mamíferos. Três décadas depois a relação entre neurogênese e células-tronco neurais (NSCs) foi estabelecida. Atualmente, as NSCs são objeto de pesquisas na medicina como modelo de estudo de múltiplos estados anormais e distúrbios orgânicos, além de se propor como uma estratégia em condições com poucas alternativas terapêuticas. Contudo o desenvolvimento destas terapias depende do entendimento dos mecanismos moleculares, celulares e biológicos que controlam a neurogênese e as NSCs. Assim, o objetivo deste trabalho foi o estudo das teorias no funcionamento dos nichos neurogênicos e as NSCs com ênfase na proliferação, migração e diferenciação, além da descrição dos aspectos celulares in vitro dos precursores neurais (NPCs) dos nichos neurogênicos dos mamíferos. Os nichos são regiões do sistema nervoso adulto que apresentam neurogênese pela presença das NSCs e um microambiente celular apropriado. Nos mamíferos existem pelo menos dois nichos, a zona subventricular (SVZ) dos ventrículos laterais e a zona subgranular (SGZ) do hipocampo. Os estudos revisados demostram que existem diferenças e semelhanças no comportamento das NSCs nos nichos neurogênicos adultos, levando a que a proliferação, migração e diferenciação seja menos efetiva quando comparada com o desenvolvimento embrionário. Para finalizar, se descreveu o protocolo para isolamento e cultivo dos NPCs e seus aspectos celulares. Os NPCs proliferaram como populações heterogêneas multipotentes. Após a diferenciação, as células migraram e apresentaram características morfológicas e imunofenotípicas de células neurais imaturas, com o predomínio de células gliais. Em conjunto, os NPCs in vitro mimetizam os aspectos gerais da neurogênese. / In the late 60`s, the experiments on cell proliferation announced adult neurogenesis in mammals. Three decades later, the link between neurogenesis and neural stem cells (NSCs) was recognized. Currently, NSCs are the matter of research in human and veterinary medicine as a model of multiple abnormal states and organic disorders, in addition to be proposed as a strategy for diseases and conditions with few therapeutic alternatives. However, the successful development of these therapies depends on the understanding of molecular, cellular and biological mechanisms that control neurogenesis and NSCs. Therefore, the aim of this work was the study of the theories on neurogenic niches and NSCs with focus in proliferation, migration and differentiation, beyond the description of the cellular aspects of in vitro neural precursors cells (NPCs) of the neurogenic niches of the mammals. The neurogenic niches are regions of the adult nervous system which display complete neurogenesis because of the presence of NSCs and an appropriate cell microenvironment. In mammals, there are at least two neurogenic niches, the subventricular zone (SVZ) of the lateral ventricles and the subgranular zone (SGZ) of the hippocampus. The reviewed studies showed that exists differences and similarities in the behavior of the adult NSCs in the neurogenic niches that lead to less effective proliferation, migration and differentiation; when compared with the embryonic development. Finally, was described the protocol for isolation and cultivation of NPCs and their cellular aspects. NPCs proliferated as heterogeneous multipotent populations. Differentiation analyses showed that cells migrated and showed morphological and immunophenotypical characteristics of immature cells with the predominance of glial cells. Overall, NPCs effectively reproduce the general aspects of neurogenesis.

Células-tronco neurais

Desenvolvimento

Medicina regenerativa

Neuroblastos

Neurogênese adulta

Nichos neurogênicos

Progenitores neurais

Adult neurogenesis

Development

Neural progenitors

Neural stem cells

Neuroblasts

Neurogenic niches

Regenerative medicine

Estudo da proliferação, migração e diferenciação dos precursores neurais do sistema nervoso pós-natal de camundongos (Mus musculus)

Delgado-Garcia, Lina Maria

January 2016

Orientador: Rogério Martins Amorim / Resumo: No final dos anos 60, os experimentos em proliferação celular anunciaram a neurogênese adulta em mamíferos. Três décadas depois a relação entre neurogênese e células-tronco neurais (NSCs) foi estabelecida. Atualmente, as NSCs são objeto de pesquisas na medicina como modelo de estudo de múltiplos estados anormais e distúrbios orgânicos, além de se propor como uma estratégia em condições com poucas alternativas terapêuticas. Contudo o desenvolvimento destas terapias depende do entendimento dos mecanismos moleculares, celulares e biológicos que controlam a neurogênese e as NSCs. Assim, o objetivo deste trabalho foi o estudo das teorias no funcionamento dos nichos neurogênicos e as NSCs com ênfase na proliferação, migração e diferenciação, além da descrição dos aspectos celulares in vitro dos precursores neurais (NPCs) dos nichos neurogênicos dos mamíferos. Os nichos são regiões do sistema nervoso adulto que apresentam neurogênese pela presença das NSCs e um microambiente celular apropriado. Nos mamíferos existem pelo menos dois nichos, a zona subventricular (SVZ) dos ventrículos laterais e a zona subgranular (SGZ) do hipocampo. Os estudos revisados demostram que existem diferenças e semelhanças no comportamento das NSCs nos nichos neurogênicos adultos, levando a que a proliferação, migração e diferenciação seja menos efetiva quando comparada com o desenvolvimento embrionário. Para finalizar, se descreveu o protocolo para isolamento e cultivo dos NPCs e seus aspectos celulares. O... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: In the late 60`s, the experiments on cell proliferation announced adult neurogenesis in mammals. Three decades later, the link between neurogenesis and neural stem cells (NSCs) was recognized. Currently, NSCs are the matter of research in human and veterinary medicine as a model of multiple abnormal states and organic disorders, in addition to be proposed as a strategy for diseases and conditions with few therapeutic alternatives. However, the successful development of these therapies depends on the understanding of molecular, cellular and biological mechanisms that control neurogenesis and NSCs. Therefore, the aim of this work was the study of the theories on neurogenic niches and NSCs with focus in proliferation, migration and differentiation, beyond the description of the cellular aspects of in vitro neural precursors cells (NPCs) of the neurogenic niches of the mammals. The neurogenic niches are regions of the adult nervous system which display complete neurogenesis because of the presence of NSCs and an appropriate cell microenvironment. In mammals, there are at least two neurogenic niches, the subventricular zone (SVZ) of the lateral ventricles and the subgranular zone (SGZ) of the hippocampus. The reviewed studies showed that exists differences and similarities in the behavior of the adult NSCs in the neurogenic niches that lead to less effective proliferation, migration and differentiation; when compared with the embryonic development. Finally, was described the proto... (Complete abstract click electronic access below) / Mestre

Células-tronco neurais

Desenvolvimento Desenvolvimento.

Medicina regenerativa.

Neuroblastos

Neurogênese adulta

Nichos neurogênicos

Progenitores neurais

Adult neurogenesis

Development

Neural progenitors

Neural stem cells

Neuroblasts

Neurogenic niches

Regenerative medicine

Estudo fenotípico da região Aorta-Gônada-Mesonefros, de embriões de galinhas Gallus gallus domesticus, com ênfase na aorta dorsal / Phenotypic study of Aorta-Gonads-Mesonephros region of chicken embryos Gallus gallus domesticus emphasizing on the dorsal aorta

Patrícia Alzueta Moreno Martinez

10 October 2012

Conselho Nacional de Desenvolvimento Científico e Tecnológico / Acredita-se que os primeiros progenitores da hematopoese definitiva surjam da diferenciação do endotélio da aorta dorsal, na altura da região da Aorta-Gônada-Mesonefros (AGM). Com o intuito de estudar esta região e o fenótipo das células do endotélio da aorta dorsal nesta posição topográfica, ovos galados de Gallus gallus domesticus L. foram incubados em chocadeira, classificados em estádios de E16 a E25 e processados histotecnologicamente para obtenção de secções seriadas na altura da região AGM. Estas passaram por coloração por Hematoxilina-Eosina, histoquímica para PAS, PAS-diastase e Alcian Blue pH 1.0 e pH 2.5, histoquímica por lectinas fluoresceinadas e imunofluorescência para moléculas de superfície, citoesqueleto e matriz extracelular. Foi observada hipertrofia endotelial no assoalho da aorta nos estádios observados, o qual se apresentava positivo ao PAS, com ocorrência frequente de vacuolizações basais PAS negativas, e o surgimento ocasional de grupamentos celulares intravasculares. Nestes, as células que se destacavam da membrana basal do endotélio expressavam progressivamente mais material PAS positivo, o qual, no entanto, em nenhum momento pareceu se tratar de glicogênio. Em relação às glicosaminoglicanas, notamos a presença predominante de ácido hialurônico por todo o mesênquima da região e em outras estruturas como periferia da notocorda, tubo neural e mesoderma lateral. Ocorreu co-expressão de fibronectina e &#945;-actina de músculo liso em células circunjacentes à aorta, na face ventral do vaso. GFAP e BMP-4 são expressas entre as células do tubo neural e em sua periferia, assim como na notocorda do embrião. As lectinas Abrus precatorius, Lens culinarise Ricinus communis mostraram-se positivas principalmente na região subedotelial do assoalho da aorta nos estádios observados neste trabalho. Bandeiraea simplicifolia exibiu pouca marcação na aorta dorsal e a Arachis hypogeae foi negativa. Outras estruturas da região AGM também expressaram resíduos de açúcares revelados por estas lectinas, tais como: notocorda, tubo neural, mesênquima, intestino primitivo e saco vitelínico. Estes resultados acrescentam elementos morfológicos e bioquímicos ao conhecimento sobre a região AGM de embriões de galinha e sobre o endotélio, possivelmente hemogênico, da aorta dorsal. / Nowadays it is known that firsts definitive hematopoietic progenitors arise from endothelium differentiation of dorsal aorta, at Aorta-Gonad-Mesonephros (AGM) site. In order to study those events and cells phenotype of dorsal aorta endothelium in this topographical site, fertilized eggs of Gallus gallus domesticus L. were incubated, from E16 to E25 and to be processed by histotechonology to obtain serial sections of the AGM site. After this, they were stained with Hematoxilin-Eosin, histochemistry to PAS, diastase PAS and Alcian Blue pH 1.0 and pH 2.5, to obtain a better overview and characterization from cells, also, histochemistry to fluorescein lectins and immunofluorescense to surface molecules, cytoeskeleton andextracellular matrix were performed. Our results showed endothelial hypertrophy of the aorta floor in the stages analyzed, which shown positive for PAS, with frequent appearance of PAS negatives basal vacuolizations and an occasional intravascular cell clusters arise of. It was also observed that cells which were separated from endothelium basal membrane shown progressively were more PAS positive which however in any time seems to be glycogen. Regard of glycosaminoglycans we noted the main presence of hialuronic acid for all the mesenchymes site and in others structures like notochord periphery, neural tube and lateral mesoderm. It was observed fibronectin and smooth muscle &#945;-actin co-expression on aorta surrounding walls, at vessels ventral face. GFAP and BMP-4 are express between the cells of neural tube and surrounding it, as well as at embryo notochord. The lectins Abrus precatorius, Lens culinaris and Ricinus communis showed mostly positive expression on the sub endothelium site of the dorsal aorta floor at the stages analyzed in this work. Bandeiraea simplicifolia showed low expression on dorsal aorta and in Arachis hypogeae it was negative. Other structures of AGMs site also expressed sugar residues revealed by these lectins like: notochord, neural tube, mesenchyme, primitive gut and yolk sac.

Região AGM

Precursores hematopoiéticos

Embrião de galinha

Aorta dorsal

Fenótipo do endotélio

Perfil bioquímico

Hematopoietic progenitors

AGM site

Chicken embryo

Dorsal aorta

Endothelium phenotype

Biochemical profile

MORFOLOGIA

Role chromation remoledačné ATPázy SMARCA5 v krvetvorbě vývoji červených krvinek / Role of Smarca5 (Snf2h) chromation remodeling ATPase in hematopoitic development and erythropoiesis

Kokavec, Juraj

January 2017

The Imitation Switch (ISWI) nuclear ATPase Smarca5 (Snf2h) is one of the most conserved chromatin remodeling factors. It exists in a variety of oligosubunit complexes that move DNA with respect to the histone octamer to generate regularly spaced nucleosomal arrays. Smarca5 interacts with different accessory proteins and represents a molecular motor for DNA replication, repair and transcription. We deleted Smarca5 at the onset of definitive hematopoiesis (Vav1-iCre) and observed that animals die during late fetal development due to anemia. Hematopoietic stem and progenitor cells (HSPCs) accumulated but their maturation towards erythroid and myeloid lineages was inhibited. Proerythroblasts were dysplastic while basophilic erythroblasts were blocked in G2/M and depleted. Smarca5 deficiency led to increased p53 levels, its activation at two residues, one associated with DNA damage (S-18) second with CBP/p300 (K376Ac), and finally activation of the p53 targets. We also deleted Smarca5 in committed erythroid cells (Epor-iCre) and observed that animals were anemic postnatally. Furthermore, 4- OHT-mediated deletion of Smarca5 in the ex vivo cultures confirmed its requirement for erythroid cell proliferation. Thus, Smarca5 plays indispensable roles during early hematopoiesis and erythropoiesis.

Caractérisation des progéniteurs cellulaires exprimant les aldéhydes déshydrogénases (ALDH) dans des modèles sains et dystrophiques / Characterization of progenitor cells expressing aldehyde dehydrogenase (ALDH) in healthy and dystrophic models

Etienne, Jessy

21 December 2016

La thérapie cellulaire est une envisagée pour traiter des pathologies cardiaques ou squelettiques basée sur la médecine régénérative. Les progéniteurs cellulaires classiquement utilisés (myoblastes ou cellules mésenchymateuses) n'ont démontré qu'une efficacité limitée. Dans ce contexte, notre laboratoire a identifié une nouvelle catégorie de progéniteurs, sur la base de leur activité enzymatique aldéhyde déshydrogénase (ALDH) mise en évidence par un substrat fluorescent, l'Aldéfluor, et en association avec le marqueur CD34. Les ALDH sont impliquées dans le métabolisme et la détoxification des aldéhydes, et constituent un nouveau marqueur des cellules souches. Ce travail de thèse a permis de mieux caractériser les progéniteurs myogéniques (ALDH+/CD34-) et non myogéniques (ALDH+/CD34+), dans différents contextes physiopathologiques. Leur présence dans différents muscles de primates humains ou non humains, leur persistance au cours du vieillissement naturel ou lors d'atteinte par la dystrophie musculaire de Duchenne (DMD) chez l'Homme et dans des modèles animaux, suggèrent une utilisation possible des cellules ALDH+/CD34- pour des développements thérapeutiques ultérieurs. L'étude phénotypique révèle que des marqueurs transmembranaires sont associés à des sous-populations de cellules ALDH myogéniques ou non myogéniques dont la comparaison permettra de proposer de meilleurs candidats de thérapie cellulaire. En parallèle, les caractérisations histologiques et cytologiques ont identifié des sous-populations exprimant des isoenzymes et les analyses d'expressiongénique réalisées ex vivo et en culture suggèrent que certaines sont impliquées dans l'homéostasie musculaires. / Cell therapy is a regenerative medicine strategy considered for the treatment of cardiac or skeletal muscle diseases. The cellular progenitors used to date (myoblasts or mesenchymal stem cells) provided mitigated success, thus mandating the identification and characterization of new categories of progenitors. Our laboratory has identified new populations of progenitors, based on their Aldehyde Deshydrogenase activity (ALDH) detectable using the fluorescent substrate Aldefluor, associated with the expression of the CD34 marker. ALDH are involved in metabolism and detoxification of aldehydes, they play important roles in cell survival and differentiation and are considered a new marker of stem cells. The present project allowed characterizing extensively the myogenic (ALDH+/CD34-) and non myogenic (ALDH+/CD34+) progenitors, in several physiopathological contexts and animal models. The presence of ALDH+/CD34- cells in distinct muscle groups in Human and non-human Primates, their persistence through natural ageing and despite the ongoing degenerative process observed in Duchenne muscular dystrophy in Human patients and animal models suggest their future use for therapeutic applications. The phenotypic characterization indicated that membrane markers are associated to myogenic or non myogenic sub-populations of ALDH cells. The comparison on their efficacies in vito and in vivo will allow proposing new candidates for cell therapy. In parallele, histological and cytological analysis identified cell populations expressing isoenzymes The analysis of gene expressions suggested that, at least, some of them are involved in muscle homeostasis in situ or in vitro.

Aldéhydes déshydrogénases (ALDH)

Dystrophie musculaire de Duchenne (DMD)

Progéniteurs myogéniques

Thérapie cellulaire

Cell therapy

Aldehyde Deshydrogenase

Duchenne muscular dystrophy

Myogenic progenitors

572.8

Identification and characterization of the progenitor niche of the Merkel cell lineage : from homeostasis to cancer

Doucet, Yanne

04 December 2015

La peau est organisée en niche de cellules souches/progénitrices qui contribuent au maintien des lignées épidermiques pendant l’homéostasie permettant ainsi de conserver l’intégrité du tissue. Les différentes cascades de signalisation qui régulent cet équilibre sont essentielles et la perturbation de ces voix peuvent amener à une différentiation anormale des kératinocytes, pouvant engendrer des cancers de la peau. Le but de cette thèse était d’identifier et de caractériser la population de progéniteurs responsables de la maintenance d’une niche épidermique spécialisée dans la mechanotransduction du toucher léger appelée les cellules de Merkel. Mon étude a porté sur le rôle des progéniteurs épithéliaux localisés dans le dôme du toucher (DT) de l’épiderme dans des conditions d’homéostasie ainsi que sur le développement du carcinome des cellules de Merkel. Basé sur l’analyse de données de microarray, j’ai identifié une nouvelle population de progéniteurs qui expriment de manière spécifique Kératine 17 (K17). Des expériences de traçage de lignées cellulaires démontrent que ces cellules donnent naissance aux cellules de Merkel (CM) ainsi qu’aux cellules squameuses. De plus, l’ablation génétique sélective des progéniteurs des CMs dans le DT a montré que cette niche est isolée et indépendante du reste de l’épiderme. Ces résultats établissent les CMs comme la quatrième lignée cellulaire de la peau. Cette découverte a permis l’établissement de nouveaux outils pour l’étude de conditions pathologiques associées à la lignée des cellules de Merkel, telles que les carcinomes des cellules de Merkel et le déclin du toucher léger avec l’âge. / The skin is organized in highly regionalized stem or progenitor cell niches that are in charge of maintaining all epidermal lineages during homeostasis. Disruption of molecular pathways that tightly regulate this balance leads to abnormal specification and differentiation of keratinocytes, eventually causing skin cancer. The goal of this thesis was to identify and characterize the progenitor population responsible for the maintenance of an epidermal niche specialized for mechanosensory signaling: the Merkel cell lineage. This work focused on the role of the epithelial progenitors located in the touch dome (TD) of hairy skin under homeostatic conditions and in a Merkel cell carcinoma (MCC) context. Based on previous microarray data, I first identified a distinct population of the interfollicular epidermis uniquely expressing Keratin 17 (K17). By lineage tracing analysis, I demonstrated that these cells give rise to the Merkel cell (MC) and squamous lineage. More importantly, selective genetic ablation of K17+ TD keratinocytes (TDKC) showed that the TD is a self-autonomous niche defining it as the 4th lineage of the skin. Interestingly, TDKCs may be involved in maintaining innervation of the Merkel cell-neurite complex. These critical results have established a new plateform for the field to allow studies of pathological skin conditions such as Merkel cell carcinoma and the loss of tactile acuity with age.

Dome du toucher

Cellules de Merkel

Progeniteurs epidermiques

Peau

Cellules souches

Carcinome des cellules de Merkel

Touch dome

Merkel cells

Epidermal progenitors

Skin

Stem cell niche

Merkel cell carcinoma

Role des Péricytes Pulmonaires dans l’Hypertension Artérielle Pulmonaire : à la recherche de nouvelles cibles thérapeutiques / Role of pericytes pulmonary in Pulmonary arterial hypertension : in search of new therapeutic targets

Bordenave, Jennifer

20 September 2019

Les péricytes sont fortement suspectés de jouer un rôle déterminant dans la physiopathologie de l’hypertension artérielle pulmonaire (HTAP), non seulement en raison de leur position et distribution, de leur rôle dans l'homéostasie vasculaire, de leur plasticité et spécificité tissulaire, mais aussi vu leur nette augmentation en nombre autour des artérioles pulmonaires remodelées. Cependant, les mécanismes impliqués dans leur accumulation autour des vaisseaux remodelés ainsi que leur importance dans la mise en place et la progression de l’HTAP restent encore incompris. De plus, nous ne savons pas si les péricytes présentent ou non des anomalies phénotypiques dans l’HTAP.C’est pourquoi ces travaux de doctorat ont visé à : 1) Identifier les possibles anomalies intrinsèques des péricytes provenant de patients HTAP ; 2) Préciser rôle de la voie de signalisation CXCL12/CXCR4/CXCR7 dans l’augmentation de la couverture péricytaire et tester des inhibiteurs de cette voie dans des modèles précliniques d’hypertension pulmonaire (HP) ; 3) Etudier l’impact du pouvoir mésenchymateux des péricytes dans le remodelage vasculaire pulmonaire associé à l’HTAP.Nos données ont permis d’une part de démontrer que les péricytes provenant de patients HTAP possédent des défauts intrinsèques dans les mécanismes de prolifération, de migration et de différenciation cellulaire et que la voie du CXCL12 contribue fortement à l’augmentation anormale de la couverture péricytaire autour des vaisseaux remodelés de patients HTAP. D’autre part, via leur capacité à se différencier en cellules contractiles, nous avons pu démontrer que les péricytes contribuaient directement au remodelage vasculaire pulmonaire.En conclusion, notre étude montre ainsi l’importance du rôle des péricytes pulmonaires dans la progression de l’hypertension artérielle pulmonaire humaine et expérimentale. / Pericytes (PCs) are strongly suspected to play a determining role in the pathophysiology of pulmonary arterial hypertension (PAH), because of their position and distribution, role in vascular homeostasis, versatility and tissue-specificity, but also because they accumulate around remodeled pulmonary arterioles in PAH. However, the underlying mechanisms and their dynamic role in PAH are still unknown. Furthermore, we do not know whether pulmonary PCs are phenotypically and functionally altered in PAH. To answer these questions, our objective were: 1) To examine the phenotypic and functional characteristics of human pulmonary PCs derived from control and PAH patients; 2) To precise the role of the intrinsic abnormalities in the altered phenotype of pulmonary PCs in PAH; 3) To study the dynamic role(s) of pulmonary PCs in preclinical PAH models, especially through modulation of the CXCL12/CXCR4/CXCR7 signaling pathway. Taken together, our findings identify for the first time phenotypic and functional abnormalities of pulmonary PCs in PAH with pathogenetic significance since they increased directly their proliferation, migration and capacity to differentiate in smooth muscle-like cells.

Hypertension pulmonaire

Péricyte

Remodelage vasculaire pulmonaire

Sdf-1

Progéniteurs mésenchymateux

Lignage cellulaire

Pulmonary hypertension

Pericyte

Pulmonary vascular remodeling

Sdf-1

Mesenchymal progenitors

Lineage tracing

The Role of Fibro-Adipogenic Progenitors in Radiation-Induced Muscle Pathology

Collao, Nicolás

21 December 2023

Globally, cancer is one of the leading causes of mortality, with an estimated 18.1 million cancer cases, 10 million deaths, and 1.9 million new cases diagnosed in 2020 (Sung et al., 2021). However, during the past several decades, cancer survival has improved such that 82% of children and >2/3 of adults diagnosed with cancer will survive beyond five years (World Health Organization (WHO) - Childhood Cancer, 2021). Skeletal muscle atrophy and fibrosis are long-term adverse effects experienced by 80% of cancer survivors for which there is no available therapy (Paulino, 2004). These long-term consequences are related to the toxicity from the cancer treatment, leading to alterations in skeletal muscle function which can lead to comorbidities and increased mortality among cancer survivors (Paulino, 2004; Williams et al., 2016). Thus, novel approaches to address the long-term effects of cancer therapy on skeletal muscle are critically needed. Exercise training is a potential non-pharmacological strategy that improves common cancer- and treatment-related side effects (Mustian et al., 2012). Specifically, exercise programs that combine resistance and endurance training (RET) have been shown to improve muscle strength and cardiovascular fitness in cancer survivors (Tong et al., 2020). The mechanisms responsible for these effects remain unknown. The remarkable plasticity of skeletal muscle relies primarily on muscle stem (satellite) cells (MuSCs) (Lepper et al., 2011) that are regulated, in part, by muscle-resident stromal cells (Bentzinger et al., 2013). These different stromal cell types, including: vascular endothelial cells (ECs), immune cells, and mesenchymal progenitors, also known as fibro-adipogenic progenitors (FAPs), create the muscle stem cell niche (Yin et al., 2013). FAPs possess a dual role as they are involved in skeletal muscle maintenance and regeneration by secreting pro-myogenic trophic factors (Biferali et al., 2019; Joe et al., 2010; Uezumi et al., 2010; Wosczyna et al., 2019), but also contribute to fibrotic and fatty tissue accumulation in chronic degenerative conditions (Uezumi et al., 2010). The divergent features of FAPs highly depend on signals they receive from their microenvironment (Giuliani et al., 2021); however, FAP's contribution to cancer treatment-induced muscle pathology in cancer survivors remains unknown. The overall objective of this thesis is to begin to develop an understanding of the role of FAPs in cancer treatment-induced muscle pathology and to determine if RET represents an effective therapy to prevent the long-term muscle defects of juvenile cancer plus therapy.

Mesenchymal Progenitors

Skeletal muscle

Cancer

Chemoradiation therapy

single-cell RNA sequencing

Exercise training

Resistant and endurance exercise

Stem cell

Atrophy

Muscle Cachexia

Extracellular matrix

Myofibroblast