Generation and characterization of orthotopic murine models for endometrial cancer

Silvia Cabrera; Marta Llauradó; Josep Castellví; Yolanda Fernandez; Francesc Alameda; Eva Colás; Anna Ruiz; Andreas Doll; Simó Schwartz; Ramon Carreras; Jordi Xercavins; Miguel Abal; Antonio Gil-Moreno; Jaume Reventós

doi:10.1007/s10585-011-9444-2

Generation and characterization of orthotopic murine models for endometrial cancer

Silvia Cabrera^*, Marta Llauradó, Josep Castellví, Yolanda Fernandez, Francesc Alameda, Eva Colás, Anna Ruiz, Andreas Doll, Simó Schwartz, Ramon Carreras, Jordi Xercavins, Miguel Abal, Antonio Gil-Moreno, Jaume Reventós

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We describe the generation of two orthotopic murine models for endometrial cancer (EC).The first model is generated from endometrial Hec-1A cancer cells transfected with luciferase and injected directly into the uterus of female mice. This model allows a follow-up with bioluminescence imaging (BLI) along the experiment and generates abdominal dissemination and lymphatic and hematogenous metastases in high percentages, also detectables with BLI. The dissemination pattern of this model imitates the advanced stages of EC in patients, and its molecular profile corresponds to aggressive type 2 EC (p53 positive, hormone receptors negative, high percentage of Ki67 positive cells). The second model is derived from endometrioid human tissue collected from surgical pieces. By injecting this tissue inside the uterine cavity of a mouse we obtain orthotopic growth with pelvic dissemination and lymph node metastasis. The molecular pattern observed in human type 1 endometrioid EC (p53 negative, low Ki67 index, presence of hormone receptors) is conserved after the murine growth in orthotopic tumor and metastases. This model supposes a singular pre-clinical tool to study therapeutic agents, though it mimics clinical and molecular behavior of endometrioid EC, which is the most common histology in the patient.

Idioma original	Anglès
Pàgines (de-a)	217-227
Nombre de pàgines	11
Revista	Clinical and Experimental Metastasis
Volum	29
Número	3
DOIs	https://doi.org/10.1007/s10585-011-9444-2
Estat de la publicació	Publicada - de març 2012

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Cabrera, S., Llauradó, M., Castellví, J., Fernandez, Y., Alameda, F., Colás, E., Ruiz, A., Doll, A., Schwartz, S., Carreras, R., Xercavins, J., Abal, M., Gil-Moreno, A., & Reventós, J. (2012). Generation and characterization of orthotopic murine models for endometrial cancer. Clinical and Experimental Metastasis, 29(3), 217-227. https://doi.org/10.1007/s10585-011-9444-2

@article{34d3b07384ca438d8dfc56553a82e7b0,

title = "Generation and characterization of orthotopic murine models for endometrial cancer",

abstract = "We describe the generation of two orthotopic murine models for endometrial cancer (EC).The first model is generated from endometrial Hec-1A cancer cells transfected with luciferase and injected directly into the uterus of female mice. This model allows a follow-up with bioluminescence imaging (BLI) along the experiment and generates abdominal dissemination and lymphatic and hematogenous metastases in high percentages, also detectables with BLI. The dissemination pattern of this model imitates the advanced stages of EC in patients, and its molecular profile corresponds to aggressive type 2 EC (p53 positive, hormone receptors negative, high percentage of Ki67 positive cells). The second model is derived from endometrioid human tissue collected from surgical pieces. By injecting this tissue inside the uterine cavity of a mouse we obtain orthotopic growth with pelvic dissemination and lymph node metastasis. The molecular pattern observed in human type 1 endometrioid EC (p53 negative, low Ki67 index, presence of hormone receptors) is conserved after the murine growth in orthotopic tumor and metastases. This model supposes a singular pre-clinical tool to study therapeutic agents, though it mimics clinical and molecular behavior of endometrioid EC, which is the most common histology in the patient.",

keywords = "Animal model, Bioluminescence, Endometrial cancer, Murine model, Orthotopic model",

author = "Silvia Cabrera and Marta Llaurad{\'o} and Josep Castellv{\'i} and Yolanda Fernandez and Francesc Alameda and Eva Col{\'a}s and Anna Ruiz and Andreas Doll and Sim{\'o} Schwartz and Ramon Carreras and Jordi Xercavins and Miguel Abal and Antonio Gil-Moreno and Jaume Revent{\'o}s",

note = "Funding Information: Fig. 3 Immunohistochemical characterization of the orthotopic mouse models. a Images of the Hec-1A cell line derived model showed positivity to p53, Ki67 with high expression and negativity to progesterone and estrogen receptors as type 2, non-endometrioid EC. b Immunohistochemical images of the tissue derived model, showed Acknowledgments The authors would like to thank Lisa Piccione for correction of the manuscript. This work has been supported by the Spanish Ministry of Science and Innovation (SAF 2005-06771; SAF 2008-03996; SAF 2010-10635-E; SAF2011-26548), the Spanish Ministry of Health (RTICC RD06/0020/0058, RD06/0020/1034; CP08/00142; PI08/0797), the Catalan Institute of Health (DURSI 2005SGR00553) and the Department of Universities and Research, Catalan Government (2009SGR00487, 2005SGR00553), the ACCIO glandular structure with negativity to p53 and positivity to progesterone and estrogen receptors as endometrioid, low grade EC. ER estrogen receptors, PR progesterone receptors, Bcat β-catenin, PAN para-aortic lymph node program (RDITSCON07-1-0001), the Foundation La Marato de TV3 (grant 050431), the IV Grant Fundaci{\'o} Santiago Dexeus Font for Clinical Investigation Projects 2009, the National Programme of Biotechnology (FIT-010000-2007-26), and the European Commission Program Fondo Europeo de Desarrollo Regional (FEDER). M.LL. is recipient of a predoctoral fellowship from the Spanish Ministry of Innovation and Science (FI07/00423).",

year = "2012",

month = mar,

doi = "10.1007/s10585-011-9444-2",

language = "English",

volume = "29",

pages = "217--227",

journal = "Clinical and Experimental Metastasis",

issn = "0262-0898",

publisher = "Springer Science and Business Media B.V.",

number = "3",

}

Cabrera, S, Llauradó, M, Castellví, J, Fernandez, Y, Alameda, F, Colás, E, Ruiz, A, Doll, A, Schwartz, S, Carreras, R, Xercavins, J, Abal, M, Gil-Moreno, A & Reventós, J 2012, 'Generation and characterization of orthotopic murine models for endometrial cancer', Clinical and Experimental Metastasis, vol. 29, núm. 3, pàg. 217-227. https://doi.org/10.1007/s10585-011-9444-2

TY - JOUR

T1 - Generation and characterization of orthotopic murine models for endometrial cancer

AU - Cabrera, Silvia

AU - Llauradó, Marta

AU - Castellví, Josep

AU - Fernandez, Yolanda

AU - Alameda, Francesc

AU - Colás, Eva

AU - Ruiz, Anna

AU - Doll, Andreas

AU - Schwartz, Simó

AU - Carreras, Ramon

AU - Xercavins, Jordi

AU - Abal, Miguel

AU - Gil-Moreno, Antonio

AU - Reventós, Jaume

N1 - Funding Information: Fig. 3 Immunohistochemical characterization of the orthotopic mouse models. a Images of the Hec-1A cell line derived model showed positivity to p53, Ki67 with high expression and negativity to progesterone and estrogen receptors as type 2, non-endometrioid EC. b Immunohistochemical images of the tissue derived model, showed Acknowledgments The authors would like to thank Lisa Piccione for correction of the manuscript. This work has been supported by the Spanish Ministry of Science and Innovation (SAF 2005-06771; SAF 2008-03996; SAF 2010-10635-E; SAF2011-26548), the Spanish Ministry of Health (RTICC RD06/0020/0058, RD06/0020/1034; CP08/00142; PI08/0797), the Catalan Institute of Health (DURSI 2005SGR00553) and the Department of Universities and Research, Catalan Government (2009SGR00487, 2005SGR00553), the ACCIO glandular structure with negativity to p53 and positivity to progesterone and estrogen receptors as endometrioid, low grade EC. ER estrogen receptors, PR progesterone receptors, Bcat β-catenin, PAN para-aortic lymph node program (RDITSCON07-1-0001), the Foundation La Marato de TV3 (grant 050431), the IV Grant Fundació Santiago Dexeus Font for Clinical Investigation Projects 2009, the National Programme of Biotechnology (FIT-010000-2007-26), and the European Commission Program Fondo Europeo de Desarrollo Regional (FEDER). M.LL. is recipient of a predoctoral fellowship from the Spanish Ministry of Innovation and Science (FI07/00423).

PY - 2012/3

Y1 - 2012/3

N2 - We describe the generation of two orthotopic murine models for endometrial cancer (EC).The first model is generated from endometrial Hec-1A cancer cells transfected with luciferase and injected directly into the uterus of female mice. This model allows a follow-up with bioluminescence imaging (BLI) along the experiment and generates abdominal dissemination and lymphatic and hematogenous metastases in high percentages, also detectables with BLI. The dissemination pattern of this model imitates the advanced stages of EC in patients, and its molecular profile corresponds to aggressive type 2 EC (p53 positive, hormone receptors negative, high percentage of Ki67 positive cells). The second model is derived from endometrioid human tissue collected from surgical pieces. By injecting this tissue inside the uterine cavity of a mouse we obtain orthotopic growth with pelvic dissemination and lymph node metastasis. The molecular pattern observed in human type 1 endometrioid EC (p53 negative, low Ki67 index, presence of hormone receptors) is conserved after the murine growth in orthotopic tumor and metastases. This model supposes a singular pre-clinical tool to study therapeutic agents, though it mimics clinical and molecular behavior of endometrioid EC, which is the most common histology in the patient.

AB - We describe the generation of two orthotopic murine models for endometrial cancer (EC).The first model is generated from endometrial Hec-1A cancer cells transfected with luciferase and injected directly into the uterus of female mice. This model allows a follow-up with bioluminescence imaging (BLI) along the experiment and generates abdominal dissemination and lymphatic and hematogenous metastases in high percentages, also detectables with BLI. The dissemination pattern of this model imitates the advanced stages of EC in patients, and its molecular profile corresponds to aggressive type 2 EC (p53 positive, hormone receptors negative, high percentage of Ki67 positive cells). The second model is derived from endometrioid human tissue collected from surgical pieces. By injecting this tissue inside the uterine cavity of a mouse we obtain orthotopic growth with pelvic dissemination and lymph node metastasis. The molecular pattern observed in human type 1 endometrioid EC (p53 negative, low Ki67 index, presence of hormone receptors) is conserved after the murine growth in orthotopic tumor and metastases. This model supposes a singular pre-clinical tool to study therapeutic agents, though it mimics clinical and molecular behavior of endometrioid EC, which is the most common histology in the patient.

KW - Animal model

KW - Bioluminescence

KW - Endometrial cancer

KW - Murine model

KW - Orthotopic model

UR - https://www.scopus.com/pages/publications/84857261580

U2 - 10.1007/s10585-011-9444-2

DO - 10.1007/s10585-011-9444-2

M3 - Article

C2 - 22198674

AN - SCOPUS:84857261580

SN - 0262-0898

VL - 29

SP - 217

EP - 227

JO - Clinical and Experimental Metastasis

JF - Clinical and Experimental Metastasis

IS - 3

ER -

Generation and characterization of orthotopic murine models for endometrial cancer

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