ROLES OF PROTEIN-TYROSINE PHOSPHATASES IN STAT1-ALPHA-MEDIATED CELL SIGNALING

被引：87

作者：

HAQUE, SJ

FLATI, V

DEB, A

WILLIAMS, BRG

机构：

[1] Dept. of Cancer Biology, Research Inst., Cleveland Clinic Foundation, Cleveland, OH 44195

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1995年 / 270卷 / 43期

关键词：

D O I：

10.1074/jbc.270.43.25709

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Different Stat proteins are activated through phosphorylation of unique tyrosine residues in response to different cytokines and growth factors. Interferon-gamma activates Stat1 molecules that form homodimers and bind cognate DNA elements. Here we show that treatment of permeabilized cells with 200-500 mu M peroxo-derivatives of vanadium, molybdenum, and tungsten results in the accumulation of constitutively phosphorylated Stat1 alpha molecules, In contrast, treatment of permeabilized cells with orthovanadate, vanadyl sulfate, molybdate, and tungstate at the same range of concentrations does not result in the accumulation of activated Stat1 alpha molecules in the absence of ligand. However, these compounds inhibit the inactivation of interferon-gamma-induced DNA-binding activity of Stat1 alpha. A 4-6-h exposure of the permeabilized cells to orthovanadate, molybdate, and tungstate, but not vanadyl sulfate, results in a ligand-independent activation of Stat1 alpha, which is blocked by the inhibition or depletion of NADPH oxidase activity in the cells, indicating that NADPH oxidase-catalyzed superoxide formation is required for the bioconversion of these metal oxides to the corresponding peroxo-compounds. Interestingly, Ligand-independent Stat1 alpha activation by peroxo-derivatives of these transition metals does not require Jak1, Jak2, or Tyk2 kinase activity, suggesting that other kinases can phosphorylate Stat1 alpha on tyrosine 701.

引用

页码：25709 / 25714

页数：6

共 57 条

[31] SPECIFIC RECRUITMENT OF SH-PTP1 TO THE ERYTHROPOIETIN RECEPTOR CAUSES INACTIVATION OF JAK2 AND TERMINATION OF PROLIFERATIVE SIGNALS
KLINGMULLER, U
LORENZ, U
CANTLEY, LC
NEEL, BG
LODISH, HF
[J]. CELL, 1995, 80 (05) : 729 - 738
[32] RAPID ACTIVATION OF THE INTERFERON-GAMMA SIGNAL-TRANSDUCTION PATHWAY BY INHIBITORS OF TYROSINE PHOSPHATASES
LAMB, P
HASLAM, J
KESSLER, L
SEIDEL, HM
STEIN, RB
ROSEN, J
[J]. JOURNAL OF INTERFERON RESEARCH, 1994, 14 (06): : 365 - 373
[33] ALPHA-INTERFERON AND GAMMA INTERFERON STIMULATE TRANSCRIPTION OF A SINGLE GENE THROUGH DIFFERENT SIGNAL TRANSDUCTION PATHWAYS
LEW, DJ
DECKER, T
DARNELL, JE
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (12) : 5404 - 5411
[34] A NEW FUNCTION FOR A PHOSPHOTYROSINE PHOSPHATASE - LINKING GRB2-SOS TO A RECEPTOR TYROSINE KINASE
LI, W
NISHIMURA, R
KASHISHIAN, A
BATZER, AG
KIM, WJH
COOPER, JA
SCHLESSINGER, J
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1994, 14 (01) : 509 - 517
[35] SPECIFICITY OF RECEPTOR TYROSINE KINASE SIGNALING - TRANSIENT VERSUS SUSTAINED EXTRACELLULAR SIGNAL-REGULATED KINASE ACTIVATION
MARSHALL, CJ
[J]. CELL, 1995, 80 (02) : 179 - 185
[36] MATSUYAMA T, 1993, CELL, V75, P83, DOI 10.1016/S0092-8674(05)80086-8
[37] ZIP CODES DIRECT INTRACELLULAR PROTEIN-TYROSINE PHOSPHATASES TO THE CORRECT CELLULAR ADDRESS
MAURO, LJ
DIXON, JE
[J]. TRENDS IN BIOCHEMICAL SCIENCES, 1994, 19 (04) : 151 - 155
[38] MILARSKI KL, 1994, J BIOL CHEM, V269, P21239
[39] THE PROTEIN-TYROSINE KINASE JAK1 COMPLEMENTS DEFECTS IN INTERFERON-ALPHA/BETA AND INTERFERON-GAMMA SIGNAL-TRANSDUCTION
MULLER, M
BRISCOE, J
LAXTON, C
GUSCHIN, D
ZIEMIECKI, A
SILVENNOINEN, O
HARPUR, AG
BARBIERI, G
WITTHUHN, BA
SCHINDLER, C
PELLEGRINI, S
WILKS, AF
IHLE, JN
STARK, GR
KERR, IM
[J]. NATURE, 1993, 366 (6451) : 129 - 135
[40] COMPLEMENTATION OF A MUTANT-CELL LINE - CENTRAL ROLE OF THE 91-KDA POLYPEPTIDE OF ISGF3 IN THE INTERFERON-ALPHA AND INTERFERON-GAMMA SIGNAL-TRANSDUCTION PATHWAYS
MULLER, M
LAXTON, C
BRISCOE, J
SCHINDLER, C
IMPROTA, T
DARNELL, JE
STARK, GR
KERR, IM
[J]. EMBO JOURNAL, 1993, 12 (11) : 4221 - 4228

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