INTERFERON-INDUCED NUCLEAR SIGNALING BY JAK PROTEIN-TYROSINE KINASES

被引：329

作者：

SILVENNOINEN, O

IHLE, JN

SCHLESSINGER, J

LEVY, DE

机构：

[1] NYU, SCH MED, KAPLAN COMPREHENS, CANC CTR, NEW YORK, NY 10016 USA

[2] NYU, SCH MED, DEPT PHARMACOL, NEW YORK, NY 10016 USA

[3] NYU, SCH MED, DEPT PATHOL, NEW YORK, NY 10016 USA

[4] ST JUDE CHILDRENS RES HOSP, DEPT BIOCHEM, MEMPHIS, TN 38105 USA

来源：

NATURE | 1993年 / 366卷 / 6455期

关键词：

D O I：

10.1038/366583a0

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：

INTERFERONS IFN-alpha/beta and IFN-gamma act through independent cell-surface receptors, inducing gene expression through tyrosine phosphorylation of cytoplasmic transcription factors1-5. IFN-alpha stimulates phosphorylation and nuclear localization of the 84/91K and 113K subunits of latent ISGF3 (interferon-stimulated gene factor 3), which combine with the 48K DNA-binding subunit6,7 to bind regulatory elements of IFN-alpha-responsive genes8-10. IFN-gamma activates p91 alone2, inducing IFN-gamma-responsive genes through a distinct DNA element11,12. Genetic complementation studies implicated the tyrosine kinase Tyk2 in IFN-alpha signalling13 and, more recently, the related Jak2 kinase in IFN-gamma signalling14. We now present biochemical evidence for Jak-family kinase involvement in IFN signal transduction. Jak1 was activated in response to IFN-alpha and IFN-gamma; Jak2 responded exclusively to IFN-gamma. Overexpression of either Jak1 or Jak2 stimulated p91 DNA-binding activity and p91-dependent transcription. Overexpression also activated endogenous Jak kinases, suggesting that interactions between Jak kinases are required during interferon signalling.

引用

页码：583 / 585

页数：3

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