Specific ablation of Stat3β distorts the pattern of stat3-responsive gene expression and impairs recovery from endotoxic shock

Joo Yeon Yoo; David L. Huso; Daniel Nathans; Stephen Desiderio

doi:10.1016/S0092-8674(02)00636-0

Specific ablation of Stat3β distorts the pattern of stat3-responsive gene expression and impairs recovery from endotoxic shock

Joo Yeon Yoo, David L. Huso, Daniel Nathans, Stephen Desiderio

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

110 Scopus citations

Abstract

Alternative splicing of the gene for Stat3, a transcription factor activated by the IL-6 family of cytokines, produces two isoforms: Stat3α and a dominant-negative variant, Stat3β. Stat3β-deficient mice were generated by gene targeting. Despite intact expression and phosphorylation of Stat3α, overall Stat3 activity was impaired in Stat3β^-/- cells. Global comparison of transcription in Stat3β^+/+ and Stat3β^-/- cells revealed stable differences. Stat3β-deficient mice exhibit diminished recovery from endotoxic shock and hyperresponsiveness of a subset of endotoxin-inducible genes in liver. The hepatic response to endotoxin in wild-type mice is accompanied by a transient increase in the ratio of Stat3β to Stat3α. These findings indicate a critical role for Stat3β in the control of systemic inflammation.

Original language	English (US)
Pages (from-to)	331-344
Number of pages	14
Journal	Cell
Volume	108
Issue number	3
DOIs	https://doi.org/10.1016/S0092-8674(02)00636-0
State	Published - 2002
Externally published	Yes

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/S0092-8674(02)00636-0

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title = "Specific ablation of Stat3β distorts the pattern of stat3-responsive gene expression and impairs recovery from endotoxic shock",

abstract = "Alternative splicing of the gene for Stat3, a transcription factor activated by the IL-6 family of cytokines, produces two isoforms: Stat3α and a dominant-negative variant, Stat3β. Stat3β-deficient mice were generated by gene targeting. Despite intact expression and phosphorylation of Stat3α, overall Stat3 activity was impaired in Stat3β-/- cells. Global comparison of transcription in Stat3β+/+ and Stat3β-/- cells revealed stable differences. Stat3β-deficient mice exhibit diminished recovery from endotoxic shock and hyperresponsiveness of a subset of endotoxin-inducible genes in liver. The hepatic response to endotoxin in wild-type mice is accompanied by a transient increase in the ratio of Stat3β to Stat3α. These findings indicate a critical role for Stat3β in the control of systemic inflammation.",

author = "Yoo, {Joo Yeon} and Huso, {David L.} and Daniel Nathans and Stephen Desiderio",

note = "Funding Information: We thank Mitra Cowan of the Johns Hopkins Transgenic Core Facility, the Howard Hughes Medical Institute Biopolymers Laboratory at Johns Hopkins, Dr. Leonidas Koniaris for helpful discussions, and Karl Clodfelter and Dominic Dordai for technical assistance. Microarray hybridization and scanning were performed by the Center for Cancer Research-Howard Hughes Medical Institute Biopolymers Laboratory at Massachusetts Institute of Technology. This work was supported by the Howard Hughes Medical Institute.",

year = "2002",

doi = "10.1016/S0092-8674(02)00636-0",

language = "English (US)",

volume = "108",

pages = "331--344",

journal = "Cell",

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publisher = "Elsevier B.V.",

number = "3",

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T1 - Specific ablation of Stat3β distorts the pattern of stat3-responsive gene expression and impairs recovery from endotoxic shock

AU - Yoo, Joo Yeon

AU - Huso, David L.

AU - Nathans, Daniel

AU - Desiderio, Stephen

N1 - Funding Information: We thank Mitra Cowan of the Johns Hopkins Transgenic Core Facility, the Howard Hughes Medical Institute Biopolymers Laboratory at Johns Hopkins, Dr. Leonidas Koniaris for helpful discussions, and Karl Clodfelter and Dominic Dordai for technical assistance. Microarray hybridization and scanning were performed by the Center for Cancer Research-Howard Hughes Medical Institute Biopolymers Laboratory at Massachusetts Institute of Technology. This work was supported by the Howard Hughes Medical Institute.

PY - 2002

Y1 - 2002

N2 - Alternative splicing of the gene for Stat3, a transcription factor activated by the IL-6 family of cytokines, produces two isoforms: Stat3α and a dominant-negative variant, Stat3β. Stat3β-deficient mice were generated by gene targeting. Despite intact expression and phosphorylation of Stat3α, overall Stat3 activity was impaired in Stat3β-/- cells. Global comparison of transcription in Stat3β+/+ and Stat3β-/- cells revealed stable differences. Stat3β-deficient mice exhibit diminished recovery from endotoxic shock and hyperresponsiveness of a subset of endotoxin-inducible genes in liver. The hepatic response to endotoxin in wild-type mice is accompanied by a transient increase in the ratio of Stat3β to Stat3α. These findings indicate a critical role for Stat3β in the control of systemic inflammation.

AB - Alternative splicing of the gene for Stat3, a transcription factor activated by the IL-6 family of cytokines, produces two isoforms: Stat3α and a dominant-negative variant, Stat3β. Stat3β-deficient mice were generated by gene targeting. Despite intact expression and phosphorylation of Stat3α, overall Stat3 activity was impaired in Stat3β-/- cells. Global comparison of transcription in Stat3β+/+ and Stat3β-/- cells revealed stable differences. Stat3β-deficient mice exhibit diminished recovery from endotoxic shock and hyperresponsiveness of a subset of endotoxin-inducible genes in liver. The hepatic response to endotoxin in wild-type mice is accompanied by a transient increase in the ratio of Stat3β to Stat3α. These findings indicate a critical role for Stat3β in the control of systemic inflammation.

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SN - 0092-8674

VL - 108

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EP - 344

JO - Cell

JF - Cell

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Specific ablation of Stat3β distorts the pattern of stat3-responsive gene expression and impairs recovery from endotoxic shock

Abstract

ASJC Scopus subject areas

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