Genetic induction of tumorigenesis in Swine

S. J. Adam; L. A. Rund; K. N. Kuzmuk; J. F. Zachary; L. B. Schook; C. M. Counter

doi:10.1038/sj.onc.1209892

Genetic induction of tumorigenesis in Swine

S. J. Adam, L. A. Rund, K. N. Kuzmuk, J. F. Zachary, L. B. Schook, C. M. Counter

Animal Sciences

Research output: Contribution to journal › Article › peer-review

Abstract

The transition from basic to clinical cancer research for a number of experimental therapeutics is hampered by the lack of a genetically malleable, large animal model. To this end, we genetically engineered primary porcine cells to be tumorigenic by expression of proteins known to perturb pathways commonly corrupted in human cancer. Akin to human cells, these porcine cells were quite resistant to transformation, requiring multiple genetic changes. Moreover, the transformed porcine cells produced tumors when returned to the isogenic host animal. The ability to now rapidly and reproducibly genetically induce tumors of sizes similar to those treated clinically in a large mammal similar to humans in many respects will provide a robust cancer model for preclinical studies dependant on generating large tumors.

Original language	English (US)
Pages (from-to)	1038-1045
Number of pages	8
Journal	Oncogene
Volume	26
Issue number	7
DOIs	https://doi.org/10.1038/sj.onc.1209892
State	Published - Feb 15 2007

Keywords

Cancer
Model
Porcine

ASJC Scopus subject areas

Molecular Biology
Cancer Research
Genetics

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10.1038/sj.onc.1209892

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title = "Genetic induction of tumorigenesis in Swine",

abstract = "The transition from basic to clinical cancer research for a number of experimental therapeutics is hampered by the lack of a genetically malleable, large animal model. To this end, we genetically engineered primary porcine cells to be tumorigenic by expression of proteins known to perturb pathways commonly corrupted in human cancer. Akin to human cells, these porcine cells were quite resistant to transformation, requiring multiple genetic changes. Moreover, the transformed porcine cells produced tumors when returned to the isogenic host animal. The ability to now rapidly and reproducibly genetically induce tumors of sizes similar to those treated clinically in a large mammal similar to humans in many respects will provide a robust cancer model for preclinical studies dependant on generating large tumors.",

keywords = "Cancer, Model, Porcine",

author = "Adam, {S. J.} and Rund, {L. A.} and Kuzmuk, {K. N.} and Zachary, {J. F.} and Schook, {L. B.} and Counter, {C. M.}",

note = "Funding Information: We thank C Linardic, D Kendall, G Ivaldi, J Beever, N Hamad, I York, J Sedivy and M Dewhirst for advice or assistance and AR Means for support. We also thank the Histopathology Laboratory, College of Veterinary Medicine, University of Illinois. This work was supported by grants from the Elsa U Pardee Foundation, Duke Comprehensive Cancer Center, NIH (CA94184) and USDA (2002-35205-12712). CMC is Leukemia and Lymphoma Scholar, LAR is supported by a Cargill Research Fellowship. SJA is supported by a DoD Predoctoral Training Fellowship (BC050468).",

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AU - Adam, S. J.

AU - Rund, L. A.

AU - Kuzmuk, K. N.

AU - Zachary, J. F.

AU - Schook, L. B.

AU - Counter, C. M.

N1 - Funding Information: We thank C Linardic, D Kendall, G Ivaldi, J Beever, N Hamad, I York, J Sedivy and M Dewhirst for advice or assistance and AR Means for support. We also thank the Histopathology Laboratory, College of Veterinary Medicine, University of Illinois. This work was supported by grants from the Elsa U Pardee Foundation, Duke Comprehensive Cancer Center, NIH (CA94184) and USDA (2002-35205-12712). CMC is Leukemia and Lymphoma Scholar, LAR is supported by a Cargill Research Fellowship. SJA is supported by a DoD Predoctoral Training Fellowship (BC050468).

PY - 2007/2/15

Y1 - 2007/2/15

N2 - The transition from basic to clinical cancer research for a number of experimental therapeutics is hampered by the lack of a genetically malleable, large animal model. To this end, we genetically engineered primary porcine cells to be tumorigenic by expression of proteins known to perturb pathways commonly corrupted in human cancer. Akin to human cells, these porcine cells were quite resistant to transformation, requiring multiple genetic changes. Moreover, the transformed porcine cells produced tumors when returned to the isogenic host animal. The ability to now rapidly and reproducibly genetically induce tumors of sizes similar to those treated clinically in a large mammal similar to humans in many respects will provide a robust cancer model for preclinical studies dependant on generating large tumors.

AB - The transition from basic to clinical cancer research for a number of experimental therapeutics is hampered by the lack of a genetically malleable, large animal model. To this end, we genetically engineered primary porcine cells to be tumorigenic by expression of proteins known to perturb pathways commonly corrupted in human cancer. Akin to human cells, these porcine cells were quite resistant to transformation, requiring multiple genetic changes. Moreover, the transformed porcine cells produced tumors when returned to the isogenic host animal. The ability to now rapidly and reproducibly genetically induce tumors of sizes similar to those treated clinically in a large mammal similar to humans in many respects will provide a robust cancer model for preclinical studies dependant on generating large tumors.

KW - Cancer

KW - Model

KW - Porcine

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Genetic induction of tumorigenesis in Swine

Abstract

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