Synthesis of functional human hemoglobin in transgenic mice

Richard R. Behringer; Thomas M. Ryan; Michael P. Reilly; Toshio Asakura; Richard D. Palmiter; Ralph L. Brinster; Tim M. Townes

doi:10.1126/science.2772649

Synthesis of functional human hemoglobin in transgenic mice

Richard R. Behringer, Thomas M. Ryan, Michael P. Reilly, Toshio Asakura, Richard D. Palmiter, Ralph L. Brinster, Tim M. Townes

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96 Scopus citations

Abstract

Human α- and β-globin genes were separately fused downstream of two erythroid-specific deoxyribonuclease (DNase) I super-hypersensitive sites that are normally located 50 kilobases upstream of the human β-globin gene. These two constructs were coinjected into fertilized mouse eggs, and expression was analyzed in transgenic animals that developed. Mice that had intact copies of the transgenes expressed high levels of correctly initiated human α- and β-globin messenger RNA specifically in erythroid tissue. An authentic human hemoglobin was formed in adult erythrocytes that when purified had an oxygen equilibrium curve identical to the curve of native human hemoglobin A (Hb A). Thus, functional human hemoglobin can be synthesized in transgenic mice. This provides a foundation for production of mouse models of human hemoglobinopathies such as sickle cell disease.

Original language	English (US)
Pages (from-to)	971-973
Number of pages	3
Journal	Science
Volume	245
Issue number	4921
DOIs	https://doi.org/10.1126/science.2772649
State	Published - 1989
Externally published	Yes

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@article{13a9c52f0c0e48658d39d7a630eb25ae,

title = "Synthesis of functional human hemoglobin in transgenic mice",

abstract = "Human α- and β-globin genes were separately fused downstream of two erythroid-specific deoxyribonuclease (DNase) I super-hypersensitive sites that are normally located 50 kilobases upstream of the human β-globin gene. These two constructs were coinjected into fertilized mouse eggs, and expression was analyzed in transgenic animals that developed. Mice that had intact copies of the transgenes expressed high levels of correctly initiated human α- and β-globin messenger RNA specifically in erythroid tissue. An authentic human hemoglobin was formed in adult erythrocytes that when purified had an oxygen equilibrium curve identical to the curve of native human hemoglobin A (Hb A). Thus, functional human hemoglobin can be synthesized in transgenic mice. This provides a foundation for production of mouse models of human hemoglobinopathies such as sickle cell disease.",

author = "Behringer, {Richard R.} and Ryan, {Thomas M.} and Reilly, {Michael P.} and Toshio Asakura and Palmiter, {Richard D.} and Brinster, {Ralph L.} and Townes, {Tim M.}",

year = "1989",

doi = "10.1126/science.2772649",

language = "English (US)",

volume = "245",

pages = "971--973",

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T1 - Synthesis of functional human hemoglobin in transgenic mice

AU - Behringer, Richard R.

AU - Ryan, Thomas M.

AU - Reilly, Michael P.

AU - Asakura, Toshio

AU - Palmiter, Richard D.

AU - Brinster, Ralph L.

AU - Townes, Tim M.

PY - 1989

Y1 - 1989

N2 - Human α- and β-globin genes were separately fused downstream of two erythroid-specific deoxyribonuclease (DNase) I super-hypersensitive sites that are normally located 50 kilobases upstream of the human β-globin gene. These two constructs were coinjected into fertilized mouse eggs, and expression was analyzed in transgenic animals that developed. Mice that had intact copies of the transgenes expressed high levels of correctly initiated human α- and β-globin messenger RNA specifically in erythroid tissue. An authentic human hemoglobin was formed in adult erythrocytes that when purified had an oxygen equilibrium curve identical to the curve of native human hemoglobin A (Hb A). Thus, functional human hemoglobin can be synthesized in transgenic mice. This provides a foundation for production of mouse models of human hemoglobinopathies such as sickle cell disease.

AB - Human α- and β-globin genes were separately fused downstream of two erythroid-specific deoxyribonuclease (DNase) I super-hypersensitive sites that are normally located 50 kilobases upstream of the human β-globin gene. These two constructs were coinjected into fertilized mouse eggs, and expression was analyzed in transgenic animals that developed. Mice that had intact copies of the transgenes expressed high levels of correctly initiated human α- and β-globin messenger RNA specifically in erythroid tissue. An authentic human hemoglobin was formed in adult erythrocytes that when purified had an oxygen equilibrium curve identical to the curve of native human hemoglobin A (Hb A). Thus, functional human hemoglobin can be synthesized in transgenic mice. This provides a foundation for production of mouse models of human hemoglobinopathies such as sickle cell disease.

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Synthesis of functional human hemoglobin in transgenic mice

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