Literature DB >> 18691113

An update on the xenograft and mouse models suitable for investigating new therapeutic compounds for the treatment of B-cell malignancies.

Paolo Macor1, Erika Secco, Sonia Zorzet, Claudio Tripodo, Claudio Celeghini, Francesco Tedesco.   

Abstract

B-cell malignancies account for over the 90% of all lymphoid neoplasms. The clonal proliferations of B-cells show a high degree of variation in terms of clinical and presenting features, histopathology, immunophenotype, and genetics. Primary tumor samples are useful for examining the characteristics of a patient's own tumor, although both primary leukemic cells and cell lines provide an initial step for screening novel compounds for their activity in some hematological malignancies, they should be followed by models in intact animals. In this review, we try to summarize the animal models generated to study B-cell malignancies, in particular, B-cell lymphoma, B-cell CLL and MM that represent the major part of B-cell malignancies. Animals that spontaneously develop cancer are flawed to predict human disease. The development of human tumor xenograft models represented a big step towards more clinically relevant models. The major problems of these models are the requirement of immuno-compromised animals and the inability of these models to recapitulate the complex relationship between the tumor and the microenvironment. A number of strategies have been also applied to develop genetically engineered models of malignancies, in which the tumor arises "naturally" in the host. The disadvantages of these models include the differences between rodent and human stroma and that they can not be used to characterise anti-tumor activity of many immunotherapeutic drugs. These models can be used to study the molecular processes critical for the development, proliferation and survival of hematological malignancies and to characterise potential therapeutic targets.

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Year:  2008        PMID: 18691113     DOI: 10.2174/138161208785294591

Source DB:  PubMed          Journal:  Curr Pharm Des        ISSN: 1381-6128            Impact factor:   3.116


  8 in total

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2.  Validation of a mouse xenograft model system for gene expression analysis of human acute lymphoblastic leukaemia.

Authors:  Amy L Samuels; Violet K Peeva; Rachael A Papa; Marin J Firth; Richard W Francis; Alex H Beesley; Richard B Lock; Ursula R Kees
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Review 3.  Mouse models as a translational platform for the development of new therapeutic agents in multiple myeloma.

Authors:  P Tassone; P Neri; R Burger; M T Di Martino; E Leone; N Amodio; M Caraglia; P Tagliaferri
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4.  Specific tumor-stroma interactions of EBV-positive Burkitt's lymphoma cells in the chick chorioallantoic membrane.

Authors:  Jürgen Becker; Ana Covelo-Fernandez; Frederike von Bonin; Dieter Kube; Jörg Wilting
Journal:  Vasc Cell       Date:  2012-03-09

5.  The CD37-targeted antibody-drug conjugate IMGN529 is highly active against human CLL and in a novel CD37 transgenic murine leukemia model.

Authors:  K A Beckwith; F W Frissora; M R Stefanovski; W H Towns; C Cheney; X Mo; J Deckert; C M Croce; J M Flynn; L A Andritsos; J A Jones; K J Maddocks; G Lozanski; J C Byrd; N Muthusamy
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6.  In vivo imaging enables high resolution preclinical trials on patients' leukemia cells growing in mice.

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Journal:  PLoS One       Date:  2012-12-31       Impact factor: 3.752

7.  The chick chorioallantoic membrane as an in vivo xenograft model for Burkitt lymphoma.

Authors:  Marcel Klingenberg; Jürgen Becker; Sonja Eberth; Dieter Kube; Jörg Wilting
Journal:  BMC Cancer       Date:  2014-05-18       Impact factor: 4.430

8.  A pre-clinical model of resistance to induction therapy in pediatric acute lymphoblastic leukemia.

Authors:  A L Samuels; A H Beesley; B D Yadav; R A Papa; R Sutton; D Anderson; G M Marshall; C H Cole; U R Kees; R B Lock
Journal:  Blood Cancer J       Date:  2014-08-01       Impact factor: 11.037

  8 in total

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