The construction of transgenic and gene knockout/knockin mouse models of human disease

Alfred Doyle; Michael P. McGarry; Nancy A. Lee; James J. Lee

doi:10.1007/s11248-011-9537-3

The construction of transgenic and gene knockout/knockin mouse models of human disease

Alfred Doyle, Michael P. McGarry, Nancy A. Lee, James J. Lee

Biochemistry and Molecular Biology

Research output: Contribution to journal › Review article › peer-review

103 Scopus citations

Abstract

The genetic and physiological similarities between mice and humans have focused considerable attention on rodents as potential models of human health and disease. Together with the wealth of resources, knowledge, and technologies surrounding the mouse as a model system, these similarities have propelled this species to the forefront of biomedical research. The advent of genomic manipulation has quickly led to the creation and use of genetically engineered mice as powerful tools for cutting edge studies of human disease research including the discovery, refinement, and utility of many currently available therapeutic regimes. In particular, the creation of genetically modified mice as models of human disease has remarkably changed our ability to understand the molecular mechanisms and cellular pathways underlying disease states. Moreover, the mouse models resulting from gene transfer technologies have been important components correlating an individual's gene expression profile to the development of disease pathologies. The objective of this review is to provide physician-scientists with an expansive historical and logistical overview of the creation of mouse models of human disease through gene transfer technologies. Our expectation is that this will facilitate on-going disease research studies and may initiate new areas of translational research leading to enhanced patient care.

Original language	English (US)
Pages (from-to)	327-349
Number of pages	23
Journal	Transgenic Research
Volume	21
Issue number	2
DOIs	https://doi.org/10.1007/s11248-011-9537-3
State	Published - Apr 2012

Keywords

Animal model
Biomedical research
Genetic engineering
Murine
Rodent

ASJC Scopus subject areas

Genetics
Animal Science and Zoology
Agronomy and Crop Science
Biotechnology

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10.1007/s11248-011-9537-3

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title = "The construction of transgenic and gene knockout/knockin mouse models of human disease",

abstract = "The genetic and physiological similarities between mice and humans have focused considerable attention on rodents as potential models of human health and disease. Together with the wealth of resources, knowledge, and technologies surrounding the mouse as a model system, these similarities have propelled this species to the forefront of biomedical research. The advent of genomic manipulation has quickly led to the creation and use of genetically engineered mice as powerful tools for cutting edge studies of human disease research including the discovery, refinement, and utility of many currently available therapeutic regimes. In particular, the creation of genetically modified mice as models of human disease has remarkably changed our ability to understand the molecular mechanisms and cellular pathways underlying disease states. Moreover, the mouse models resulting from gene transfer technologies have been important components correlating an individual's gene expression profile to the development of disease pathologies. The objective of this review is to provide physician-scientists with an expansive historical and logistical overview of the creation of mouse models of human disease through gene transfer technologies. Our expectation is that this will facilitate on-going disease research studies and may initiate new areas of translational research leading to enhanced patient care.",

keywords = "Animal model, Biomedical research, Genetic engineering, Murine, Rodent",

author = "Alfred Doyle and McGarry, {Michael P.} and Lee, {Nancy A.} and Lee, {James J.}",

note = "Funding Information: Acknowledgments The authors wish to thank the members of Lee Laboratories as well as colleagues in the research community for insightful discussions and critical comments during the preparation of this review. Moreover, we also wish to acknowledge the tireless efforts of the Mayo Clinic Arizona medical graphic artist Marv Ruona and Joseph Esposito of Research Library Services. In addition, we wish to express our gratitude to the Lee Laboratories administrative staff (Linda Mardel and Charlie Kern), without whom we could not function as an integrated group. This effort was supported by the Mayo Foundation for Medical Education and Research and grants from the National Institutes of Health to JJ Lee (HL065228 and K26-RR019709) and NA Lee (HL058723) as well as a grant from the American Heart Association to JJ Lee (0855703G). Support for A Doyle is provided by a Mayo Clinic Sidney Luckman Family Predoctoral Fellowship.",

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doi = "10.1007/s11248-011-9537-3",

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AU - McGarry, Michael P.

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N1 - Funding Information: Acknowledgments The authors wish to thank the members of Lee Laboratories as well as colleagues in the research community for insightful discussions and critical comments during the preparation of this review. Moreover, we also wish to acknowledge the tireless efforts of the Mayo Clinic Arizona medical graphic artist Marv Ruona and Joseph Esposito of Research Library Services. In addition, we wish to express our gratitude to the Lee Laboratories administrative staff (Linda Mardel and Charlie Kern), without whom we could not function as an integrated group. This effort was supported by the Mayo Foundation for Medical Education and Research and grants from the National Institutes of Health to JJ Lee (HL065228 and K26-RR019709) and NA Lee (HL058723) as well as a grant from the American Heart Association to JJ Lee (0855703G). Support for A Doyle is provided by a Mayo Clinic Sidney Luckman Family Predoctoral Fellowship.

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N2 - The genetic and physiological similarities between mice and humans have focused considerable attention on rodents as potential models of human health and disease. Together with the wealth of resources, knowledge, and technologies surrounding the mouse as a model system, these similarities have propelled this species to the forefront of biomedical research. The advent of genomic manipulation has quickly led to the creation and use of genetically engineered mice as powerful tools for cutting edge studies of human disease research including the discovery, refinement, and utility of many currently available therapeutic regimes. In particular, the creation of genetically modified mice as models of human disease has remarkably changed our ability to understand the molecular mechanisms and cellular pathways underlying disease states. Moreover, the mouse models resulting from gene transfer technologies have been important components correlating an individual's gene expression profile to the development of disease pathologies. The objective of this review is to provide physician-scientists with an expansive historical and logistical overview of the creation of mouse models of human disease through gene transfer technologies. Our expectation is that this will facilitate on-going disease research studies and may initiate new areas of translational research leading to enhanced patient care.

AB - The genetic and physiological similarities between mice and humans have focused considerable attention on rodents as potential models of human health and disease. Together with the wealth of resources, knowledge, and technologies surrounding the mouse as a model system, these similarities have propelled this species to the forefront of biomedical research. The advent of genomic manipulation has quickly led to the creation and use of genetically engineered mice as powerful tools for cutting edge studies of human disease research including the discovery, refinement, and utility of many currently available therapeutic regimes. In particular, the creation of genetically modified mice as models of human disease has remarkably changed our ability to understand the molecular mechanisms and cellular pathways underlying disease states. Moreover, the mouse models resulting from gene transfer technologies have been important components correlating an individual's gene expression profile to the development of disease pathologies. The objective of this review is to provide physician-scientists with an expansive historical and logistical overview of the creation of mouse models of human disease through gene transfer technologies. Our expectation is that this will facilitate on-going disease research studies and may initiate new areas of translational research leading to enhanced patient care.

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The construction of transgenic and gene knockout/knockin mouse models of human disease

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