NITRIC-OXIDE ENHANCES PROSTAGLANDIN-H SYNTHASE-1 ACTIVITY BY A HEME-INDEPENDENT MECHANISM - EVIDENCE IMPLICATING NITROSOTHIOLS

被引：68

作者：

HAJJAR, DP

LANDER, HM

PEARCE, SFA

UPMACIS, RK

POMERANTZ, KB

机构：

[1] Department of Biochemistry, Cornell University Medical College, New York, New York 10021

来源：

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY | 1995年 / 117卷 / 12期

关键词：

NITRIC OXIDE; CYCLOOXYGENASE; PROSTAGLANDIN H SYNTHASE-1; EICOSANOIDS; HEME; NITROSOTHIOLS;

D O I：

10.1021/ja00117a004

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

A mechanism by which nitric oxide (NO) enhances prostaglandin-H synthase-1 (PCHS-1) activity is described. Under aerobic conditions, NO stimulates the conversion of arachidonic acid to prostaglandin E(2) (PGE(2)) and PGD(2) in a dose- (5-100 mu M) and time- (over 5 min) dependent manner. PGHS-1 possesses several potential targets for NO interaction; heme and Tyr 385 (both of which are necessary for catalytic function) and three reduced cysteines (Cys 313, 512, and 540), all of which are located in the catalytic domain. Our data demonstrate that NO activated PGHS-1 independently of heme. The Soret band absorbance of PGHS-1 was unaffected by NO in air but was increased by carbon monoxide (GO). Heme-NO conjugates added to apo-PGHS-1 inhibited PGHS-1 activity relative to the addition of heme alone. PGHS-1 activity was also inhibited by H2O2. NO also activated PGHS-1 independently of Tyr 385, since tetranitromethane treatment of PGHS-1 did not block the enhancement of PGHS-1 by NO. However, NO promoted formation of nitrosothiols in a dose-dependent manner which plateaued at 3 mol nitrosothiol/mol PGHS-1. The kinetics of nitrosothiol formation directly correlated with measurements of PGHS-1 activity. The formation of nitrosothiols occurred concomitantly with a significant change in the secondary structure of PGHS-1. Our data suggest that enhancement of PGHS-1 activity by NO occurs by S-nitrosation of cysteine residues located in the catalytic domain, with subsequent alterations in secondary structure.

引用

页码：3340 / 3346

页数：7

共 45 条

[31] NITRIC-OXIDE ACTIVATES CYCLOOXYGENASE ENZYMES
SALVEMINI, D
MISKO, TP
MASFERRER, JL
SEIBERT, K
CURRIE, MG
NEEDLEMAN, P
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (15) : 7240 - 7244
[32] SAMUELSSON B, 1978, ADV PROSTAGLANDIN TH, P1
[33] NITRIC-OXIDE MODULATES PROSTACYCLIN BIOSYNTHESIS IN THE LUNG OF ENDOTOXIN-TREATED RATS
SAUTEBIN, L
DIROSA, M
[J]. EUROPEAN JOURNAL OF PHARMACOLOGY, 1994, 262 (1-2) : 193 - 196
[34] A SCHEME FOR THE COLORIMETRIC DETERMINATION OF MICROGRAM AMOUNTS OF THIOLS
SAVILLE, B
[J]. ANALYST, 1958, 83 (993) : 670 - 672
[35] THE NITRIC-OXIDE SYNTHASE FAMILY OF PROTEINS
SESSA, WC
[J]. JOURNAL OF VASCULAR RESEARCH, 1994, 31 (03) : 131 - 143
[36] SHIMOKAWA T, 1990, J BIOL CHEM, V265, P20073
[37] S-NITROSYLATION OF PROTEINS WITH NITRIC-OXIDE - SYNTHESIS AND CHARACTERIZATION OF BIOLOGICALLY-ACTIVE COMPOUNDS
STAMLER, JS
SIMON, DI
OSBORNE, JA
MULLINS, ME
JARAKI, O
MICHEL, T
SINGEL, DJ
LOSCALZO, J
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (01) : 444 - 448
[38] S-NITROSYLATION OF TISSUE-TYPE PLASMINOGEN-ACTIVATOR CONFERS VASODILATORY AND ANTIPLATELET PROPERTIES ON THE ENZYME
STAMLER, JS
SIMON, DI
JARAKI, O
OSBORNE, JA
FRANCIS, S
MULLINS, M
SINGEL, D
LOSCALZO, J
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (17) : 8087 - 8091
[39] BIOCHEMISTRY OF NITRIC-OXIDE AND ITS REDOX-ACTIVATED FORMS
STAMLER, JS
SINGEL, DJ
LOSCALZO, J
[J]. SCIENCE, 1992, 258 (5090) : 1898 - 1902
[40] REDOX SIGNALING - NITROSYLATION AND RELATED TARGET INTERACTIONS OF NITRIC-OXIDE
STAMLER, JS
[J]. CELL, 1994, 78 (06) : 931 - 936

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