TOWARDS THE PHYSIOLOGICAL-FUNCTION OF URIC-ACID

被引：677

作者：

BECKER, BF

机构：

[1] Department of Physiology, University of Munich, 8000 Munich 2

来源：

FREE RADICAL BIOLOGY AND MEDICINE | 1993年 / 14卷 / 06期

关键词：

ALLANTOIN; ANGIOTENSIN CONVERTING ENZYME; CORONARY ENDOTHELIUM; CYCLOOXYGENASE; FREE RADICAL; HYPOCHLORITE; NEUTROPHILS; OXALATE; OXIDANT; XANTHINE OXIDASE;

D O I：

10.1016/0891-5849(93)90143-I

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：

Uric acid, or more correctly (at physiological pH values), its monoanion urate, is traditionally considered to be a metabolically inert end-product of purine metabolism in man, without any physiological value. However, this ubiquitous compound has proven to be a selective antioxidant, capable especially of reaction with hydroxyl radicals and hypochlorous acid, itself being converted to innocuous products (allantoin, allantoate, glyoxylate, urea, oxalate). There is now evidence for such processes not only in vitro and in isolated organs, but also in the human lung in vivo. Urate may also serve as an oxidisable cosubstrate for the enzyme cyclooxygenase. As shown for the coronary system, a major site of production of urate is the microvascular endothelium, and there is generally a net release of urate from the human myocardium in vivo. In isolated organ preparations, urate protects against reperfusion damage induced by activated granulocytes, cells known to produce a variety of radicals and oxidants. Intriguingly, urate prevents oxidative inactivation of endothelial enzymes (cyclooxygenase, angiotensin converting enzyme) and preserves the ability of the endothelium to mediate vascular dilatation in the face of oxidative stress, suggesting a particular relationship between the site of urate formation and the need for a biologically potent radical scavenger and antioxidant.

引用

页码：615 / 631

页数：17

共 123 条

[1] AGAMAH ES, 1991, J LAB CLIN MED, V118, P241
[2] URIC-ACID PROVIDES AN ANTIOXIDANT DEFENSE IN HUMANS AGAINST OXIDANT-CAUSED AND RADICAL-CAUSED AGING AND CANCER - A HYPOTHESIS
AMES, BN
CATHCART, R
SCHWIERS, E
HOCHSTEIN, P
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1981, 78 (11): : 6858 - 6862
[3] [Anonymous], 2015, FREE RADICAL BIO MED
[4] REDUCTION OF SPERM WHALE FERRYLMYOGLOBIN BY ENDOGENOUS REDUCING AGENTS - POTENTIAL REDUCIBLE LOCI OF FERRYLMYOGLOBIN
ARDUINI, A
MANCINELLI, G
RADATTI, GL
DAMONTI, W
HOCHSTEIN, P
CADENAS, E
[J]. FREE RADICAL BIOLOGY AND MEDICINE, 1992, 13 (04) : 449 - 454
[5] POSSIBLE MECHANISM OF INHIBITION OF NITRITE-INDUCED OXIDATION OF OXYHEMOGLOBIN BY ERGOTHIONEINE AND URIC-ACID
ARDUINI, A
MANCINELLI, G
RADATTI, GL
HOCHSTEIN, P
CADENAS, E
[J]. ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1992, 294 (02) : 398 - 402
[6] PROSTACYCLIN STIMULATORY ACTIVITY OF REDUCING COFACTORS IN HUMAN-PLASMA FILTRATE - A POTENTIAL ROLE FOR URIC-ACID
ARNOUT, J
KIENAST, J
DECKMYN, H
VERMYLEN, J
[J]. AGENTS AND ACTIONS, 1987, 22 (3-4): : 360 - 361
[7] INACTIVATION OF ALPHA-ANTIPROTEINASE BY HYDROXYL RADICALS - THE EFFECT OF URIC-ACID
ARUOMA, OI
HALLIWELL, B
[J]. FEBS LETTERS, 1989, 244 (01): : 76 - 80
[8] BECKER B F, 1988, Pfluegers Archiv European Journal of Physiology, V411, pR26
[9] ROLE OF URIC-ACID AS AN ENDOGENOUS RADICAL SCAVENGER AND ANTIOXIDANT
BECKER, BF
REINHOLZ, N
LEIPERT, B
RASCHKE, P
PERMANETTER, B
GERLACH, E
[J]. CHEST, 1991, 100 (03) : S176 - S181
[10] URIC-ACID AS RADICAL SCAVENGER AND ANTIOXIDANT IN THE HEART
BECKER, BF
REINHOLZ, N
OZCELIK, T
LEIPERT, B
GERLACH, E
[J]. PFLUGERS ARCHIV-EUROPEAN JOURNAL OF PHYSIOLOGY, 1989, 415 (02): : 127 - 135

← 1 2 3 4 5 6 7 8 9 10 →