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Establishment and Characterization of a Reliable Xenograft Model of Hodgkin Lymphoma Suitable for the Study of Tumor Origin and the Design of New Therapies.
M'kacher, Radhia; Frenzel, Monika; Al Jawhari, Mustafa; Junker, Steffen; Cuceu, Corina; Morat, Luc; Bauchet, Anne-Laure; Stimmer, Lev; Lenain, Aude; Dechamps, Nathalie; Hempel, William M; Pottier, Geraldine; Heidingsfelder, Leonhard; Laplagne, Eric; Borie, Claire; Oudrhiri, Noufissa; Jouni, Dima; Bennaceur-Griscelli, Annelise; Colicchio, Bruno; Dieterlen, Alain; Girinsky, Theodore; Boisgard, Raphael; Bourhis, Jean; Bosq, Jacques; Mehrling, Thomas; Jeandidier, Eric; Carde, Patrice.
Afiliação
  • M'kacher R; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. radhia.mkacher@gmail.com.
  • Frenzel M; Cell Environment, Oncology Section, 75020 Paris, France. radhia.mkacher@gmail.com.
  • Al Jawhari M; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. monika.frenzel@hotmail.com.
  • Junker S; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. mustafa.aljawhari@hotmail.fr.
  • Cuceu C; Institute of Biomedicine, University of Aarhus, DK-8000 Aarhus C, Denmark. sjunker@biomed.au.dk.
  • Morat L; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. cuceu_corina@yahoo.com.
  • Bauchet AL; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. luc.morat@cea.fr.
  • Stimmer L; Platform for Experimental Pathology PathEX/CRC MIRCen/CEA-INSERM, University Paris-Saclay, 92265 Fontenay aux Rroses, France. anne-laure.bauchet@sanofi.com.
  • Lenain A; Platform for Experimental Pathology PathEX/CRC MIRCen/CEA-INSERM, University Paris-Saclay, 92265 Fontenay aux Rroses, France. lev.stimmer@cea.fr.
  • Dechamps N; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. audelenain@yahoo.fr.
  • Hempel WM; Platform for Cell Sorting, CEA, iRCM, 92265 Fontenay aux Roses, France. nathalie.dechamps@cea.fr.
  • Pottier G; Radiobiology and Oncology Laboratory, CEA, iRCM, University Paris-Saclay, 92 265 Fontenay aux Roses, France. williamhempel824@gmail.com.
  • Heidingsfelder L; Laboratoire d'Imagerie Moléculaire Expérimentale Groupe d'Imagerie du Petit Animal CEA/DSV/I2BM/SHFJ/U1023, University Paris-Saclay, 91400 Orsay, France. geraldine.pottier@cea.fr.
  • Laplagne E; MetaSystems GmbH, Robert-Bosch-Str. 6D, 68804 Altlussheim, Germany. lheidingsfelder@metasystems.de.
  • Borie C; Pole Concept, 75016 Paris, France. eric.laplagne@gmail.com.
  • Oudrhiri N; APHP-Hopital Paul Brousse Université Paris Sud/ESteam Paris Inserm UMR 935, 94800 Villejuif, France. claire.borie@aphp.fr.
  • Jouni D; APHP-Hopital Paul Brousse Université Paris Sud/ESteam Paris Inserm UMR 935, 94800 Villejuif, France. noufissa.oudrhiri@aphp.fr.
  • Bennaceur-Griscelli A; APHP-Hopital Paul Brousse Université Paris Sud/ESteam Paris Inserm UMR 935, 94800 Villejuif, France. dimajouni@yahoo.fr.
  • Colicchio B; APHP-Hopital Paul Brousse Université Paris Sud/ESteam Paris Inserm UMR 935, 94800 Villejuif, France. annelise.bennaceur@pbr.aphp.fr.
  • Dieterlen A; IRIMAS, Institut de Recherche en Informatique, Mathématiques, Automatique et Signal, Université de Haute-Alsace, 68093 Mulhouse, France. bruno.colicchio@uha.fr.
  • Girinsky T; IRIMAS, Institut de Recherche en Informatique, Mathématiques, Automatique et Signal, Université de Haute-Alsace, 68093 Mulhouse, France. alain.dieterlen@uha.fr.
  • Boisgard R; Department of Radiation Oncology, Gustave Roussy Cancer Campus, University Paris-Saclay, 94805 Villejuif, France. theogirinsky@me.com.
  • Bourhis J; Laboratoire d'Imagerie Moléculaire Expérimentale Groupe d'Imagerie du Petit Animal CEA/DSV/I2BM/SHFJ/U1023, University Paris-Saclay, 91400 Orsay, France. raphael.boisgard@cea.fr.
  • Bosq J; Department of Radiation Oncology, Gustave Roussy Cancer Campus, University Paris-Saclay, 94805 Villejuif, France. Jean.Bourhis@unil.ch.
  • Mehrling T; Departement of Anapathology, Gustave Roussy Cancer Campus, University Paris-Saclay, 94805 Vilejuif, France. jacques.bosq@gustaveroussy.fr.
  • Jeandidier E; Mundipharma-EDO GmbH, CH-4020 Basel, Switzerland. thomas.mehrling@mundipharma-edo.com.
  • Carde P; Department of Genetic, Groupe Hospitalier de la Région de Mulhouse Sud-Alsace, 68093 Mulhouse, France. jeandidiere@ghrmsa.fr.
Cancers (Basel) ; 10(11)2018 Oct 31.
Article em En | MEDLINE | ID: mdl-30384446
ABSTRACT
To identify the cells responsible for the initiation and maintenance of Hodgkin lymphoma (HL) cells, we have characterized a subpopulation of HL cells grown in vitro and in vivo with the aim of establishing a reliable and robust animal model for HL. To validate our model, we challenged the tumor cells in vivo by injecting the alkylating histone-deacetylase inhibitor, EDO-S101, a salvage regimen for HL patients, into xenografted mice.

Methodology:

Blood lymphocytes from 50 HL patients and seven HL cell lines were used. Immunohistochemistry, flow cytometry, and cytogenetics analyses were performed. The in vitro and in vivo effects of EDO-S101 were assessed.

Results:

We have successfully determined conditions for in vitro amplification and characterization of the HL L428-c subline, containing a higher proportion of CD30-/CD15- cells than the parental L428 cell line. This subline displayed excellent clonogenic potential and reliable reproducibility upon xenografting into immunodeficient NOD-SCID-gamma (-/-)(NSG) mice. Using cell sorting, we demonstrate that CD30-/CD15- subpopulations can gain the phenotype of the L428-c cell line in vitro. Moreover, the human cells recovered from the seventh week after injection of L428-c cells into NSG mice were small cells characterized by a high frequency of CD30-/CD15- cells. Cytogenetic analysis demonstrated that they were diploid and showed high telomere instability and telomerase activity. Accordingly, chromosomal instability emerged, as shown by the formation of dicentric chromosomes, ring chromosomes, and breakage/fusion/bridge cycles. Similarly, high telomerase activity and telomere instability were detected in circulating lymphocytes from HL patients. The beneficial effect of the histone-deacetylase inhibitor EDO-S101 as an anti-tumor drug validated our animal model.

Conclusion:

Our HL animal model requires only 10³ cells and is characterized by a high survival/toxicity ratio and high reproducibility. Moreover, the cells that engraft in mice are characterized by a high frequency of small CD30-/CD15- cells exhibiting high telomerase activity and telomere dysfunction.
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Texto completo: 1 Base de dados: MEDLINE Idioma: En Revista: Cancers (Basel) Ano de publicação: 2018 Tipo de documento: Article País de afiliação: França
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Idioma: En Revista: Cancers (Basel) Ano de publicação: 2018 Tipo de documento: Article País de afiliação: França