STAT3 complements defects in an interferon-resistant cell line: Evidence for an essential role for STAT3 in interferon signaling and biological activities

被引：116

作者：

Yang, CH ^{[1
]}

Murti, A ^{[1
]}

Pfeffer, LM ^{[1
]}

机构：

[1] Univ Tennessee, Ctr Hlth Sci, Dept Pathol, Memphis, TN 38163 USA

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1998年 / 95卷 / 10期

关键词：

D O I：

10.1073/pnas.95.10.5568

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

STAT proteins play critical roles in the signal transduction pathways for various cytokines, The type I interferons (IFN alpha/beta) promote the DNA-binding activity of the transcription factors STAT1, STAT2, and STAT3. Although the requirement for STAT1 and STAT2 in IFN alpha/beta signaling and action is well documented, the biological importance of STAT3 to IFN action has not yet been addressed. We found that STAT3 plays a critical role in signal transduction by IFN alpha/beta. ii human cell line that is resistant to the antiviral and antiproliferative activities of IFN but is still IFN-responsive by virtue of STAT1 and STAT2 activation was found to be defective in STAT3 activation and in induction of NF-kappa B DNA-binding activity, Expression of STAT3 in these resistant cells complemented these signaling defects and also markedly increased cellular sensitivity to the antiviral and antiproliferative effects of IFN, Because STAT3 is involved in the induction of NF-kappa B DNA-binding activity and in the induction of antiviral and antiproliferative activity, our results place STAT3 as an important upstream element in type I IFN signal transduction and in the induction of biological activities. Therefore, our results indicate that STAT1 and STAT2 are not the only STATs required for the expression of the key biological activities of IFN alpha/beta.

引用

页码：5568 / 5572

页数：5

共 39 条

[1] MOLECULAR-CLONING OF APRF, A NOVEL IFN-STIMULATED GENE FACTOR-3 P91-RELATED TRANSCRIPTION FACTOR INVOLVED IN THE GP130-MEDIATED SIGNALING PATHWAY [J].

AKIRA, S ;

NISHIO, Y ;

INOUE, M ;

WANG, XJ ;

WEI, S ;

MATSUSAKA, T ;

YOSHIDA, K ;

SUDO, T ;

NARUTO, M ;

KISHIMOTO, T .

CELL, 1994, 77 (01) :63-71

[2]

BAEUERLE PA, 1994, ANNU REV IMMUNOL, V12, P141, DOI 10.1146/annurev.immunol.12.1.141

[3] STAT3 ACTIVATION BY CYTOKINES UTILIZING GP130 AND RELATED TRANSDUCERS INVOLVES A SECONDARY MODIFICATION REQUIRING AN H7-SENSITIVE KINASE [J].

BOULTON, TG ;

ZHONG, Z ;

WEN, ZL ;

DARNELL, JE ;

STAHL, N ;

YANCOPOULOS, GD .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (15) :6915-6919

[4]

BRANCA AA, 1982, J BIOL CHEM, V257, P13291

[5] PROTEIN-KINASE-B (C-AKT) IN PHOSPHATIDYLINOSITOL-3-OH INASE SIGNAL-TRANSDUCTION [J].

BURGERING, BMT ;

COFFER, PJ .

NATURE, 1995, 376 (6541) :599-602

[6] ACTIVATION OF ACUTE-PHASE RESPONSE FACTOR (APRF)/STAT3 TRANSCRIPTION FACTOR BY GROWTH-HORMONE [J].

CAMPBELL, GS ;

MEYER, DJ ;

RAZ, R ;

LEVY, DE ;

SCHWARTZ, J ;

CARTERSU, C .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (08) :3974-3979

[7] DIRECT BINDING TO AND TYROSINE PHOSPHORYLATION OF THE ALPHA-SUBUNIT OF THE TYPE-I INTERFERON RECEPTOR BY P135(TYK2) TYROSINE KINASE [J].

COLAMONICI, O ;

YAN, H ;

DOMANSKI, P ;

HANDA, R ;

SMALLEY, D ;

MULLERSMAN, J ;

WITTE, M ;

KRISHNAN, K ;

KROLEWSKI, J .

MOLECULAR AND CELLULAR BIOLOGY, 1994, 14 (12) :8133-8142

[8]

COLAMONICI OR, 1994, J BIOL CHEM, V269, P9598

[9] EXPRESSION AND SIGNALING SPECIFICITY OF THE IFNAR CHAIN OF THE TYPE-I INTERFERON RECEPTOR COMPLEX [J].

CONSTANTINESCU, SN ;

CROZE, E ;

MURTI, A ;

WANG, C ;

BASU, L ;

HOLLANDER, D ;

RUSSELLHARDE, D ;

BETTS, M ;

GARCIAMARTINEZ, V ;

MULLERSMAN, JE ;

PFEFFER, LM .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (23) :10487-10491

[10] ROLE OF INTERFERON-ALPHA/BETA RECEPTOR CHAIN-1 IN THE STRUCTURE AND TRANSMEMBRANE SIGNALING OF THE INTERFERON-ALPHA/BETA RECEPTOR COMPLEX [J].