NITRIC OXIDE-BASED POSSIBILITIES FOR PHARMACOTHERAPY

被引：41

作者：

PORSTI, I ^{[1
]}

PAAKKARI, I ^{[1
]}

机构：

[1] UNIV HELSINKI, DEPT PHARMACOL & TOXICOL, SF-00170 HELSINKI, FINLAND

来源：

ANNALS OF MEDICINE | 1995年 / 27卷 / 03期

关键词：

NITRATES; NITRIC OXIDE; NITRIC OXIDE DONORS; PHARMACOTHERAPY;

D O I：

10.3109/07853899509002594

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

The goal of nitric oxide (NO) based pharmacotherapy is to reach proper homeostasis of NO metabolism in the target tissue where endogenous production of NO is either too weak or excessively increased. In addition to the classic NO-based therapy of cardiovascular conditions with nitrates, a variety of new therapeutic possibilities have emerged including sexual disorders, gastrointestinal system, immunology, tumour growth regulation and respiratory disorders. NO levels of target tissues can be affected directly by NO donors, or indirectly by increasing the level of L-arginine, a substrate of nitric oxide synthase (NOS). While increased production of NO by induceable NOS (iNOS) by, for example, cytokines does not at present seem therapeutically meaningful, increased NO production by constitutive NOS (cNOS) may be involved in the beneficial effects of ACE inhibitors or oestrogens. NO production may be pharmacologically decreased by inhibition of expression of iNOS by glucocorticoids while both cNOS and iNOS derived NO production is inhibition by administration of false substrates, for example L-NAME. Additionally, the respiratory system and related vessels can be reached directly and more selectively by inhalation of pure NO gas. Possible problems in administering NO and perhaps some NO-donors include the toxic nature of the compound itself whereby vital enzyme systems may be inhibited and tissue damaging radicals formed. Future prospects of NO-based pharmacotherapy may feature selective ligands to different NOS isoforms and tissue selective donors that release NO in a controlled fashion.

引用

页码：407 / 420

页数：14

共 232 条

[1] INHIBITION OF CRYPTOCOCCUS-NEOFORMANS REPLICATION BY NITROGEN-OXIDES SUPPORTS THE ROLE OF THESE MOLECULES AS EFFECTORS OF MACROPHAGE-MEDIATED CYTOSTASIS
ALSPAUGH, JA
GRANGER, DL
[J]. INFECTION AND IMMUNITY, 1991, 59 (07) : 2291 - 2296
[2] NITRIC-OXIDE SYNTHESIZED FROM L-ARGININE REGULATES VASCULAR TONE IN THE CORONARY CIRCULATION OF THE RABBIT
AMEZCUA, JL
PALMER, RMJ
DESOUZA, BM
MONCADA, S
[J]. BRITISH JOURNAL OF PHARMACOLOGY, 1989, 97 (04) : 1119 - 1124
[3] NITRIC-OXIDE - MEDIATOR, MURDERER, AND MEDICINE
ANGGARD, E
[J]. LANCET, 1994, 343 (8907) : 1199 - 1206
[4] BENEFICIAL-EFFECTS OF 2 FORMS OF NO ADMINISTRATION IN FELINE SPLANCHNIC ARTERY-OCCLUSION SHOCK
AOKI, N
JOHNSON, G
LEFER, AM
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1990, 258 (02): : G275 - G281
[5] HYPOXIC PULMONARY VASOCONSTRICTION IS ENHANCED BY INHIBITION OF THE SYNTHESIS OF AN ENDOTHELIUM DERIVED RELAXING FACTOR
ARCHER, SL
TOLINS, JP
RAIJ, L
WEIR, EK
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1989, 164 (03) : 1198 - 1205
[6] QUINAPRIL TREATMENT AND ARTERIAL SMOOTH-MUSCLE RESPONSES IN SPONTANEOUSLY HYPERTENSIVE RATS
ARVOLA, P
RUSKOAHO, H
WUORELA, H
PEKKI, A
VAPAATALO, H
PORSTI, I
[J]. BRITISH JOURNAL OF PHARMACOLOGY, 1993, 108 (04) : 980 - 990
[7] NITRIC-OXIDE IN THE KIDNEY - SYNTHESIS, LOCALIZATION, AND FUNCTION
BACHMANN, S
MUNDEL, P
[J]. AMERICAN JOURNAL OF KIDNEY DISEASES, 1994, 24 (01) : 112 - 129
[8] ABNORMAL CONTRACTILE FUNCTION DUE TO INDUCTION OF NITRIC-OXIDE SYNTHESIS IN RAT CARDIAC MYOCYTES FOLLOWS EXPOSURE TO ACTIVATED MACROPHAGE-CONDITIONED MEDIUM
BALLIGAND, JL
UNGUREANU, D
KELLY, RA
KOBZIK, L
PIMENTAL, D
MICHEL, T
SMITH, TW
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1993, 91 (05) : 2314 - 2319
[9] NITRIC-OXIDE GENERATION FROM NITROPRUSSIDE BY VASCULAR TISSUE - EVIDENCE THAT REDUCTION OF THE NITROPRUSSIDE ANION AND CYANIDE LOSS ARE REQUIRED
BATES, JN
BAKER, MT
GUERRA, R
HARRISON, DG
[J]. BIOCHEMICAL PHARMACOLOGY, 1991, 42 : S157 - S165
[10] ROLE OF ENDOTHELIUM-DERIVED RELAXING FACTOR IN RENAL AUTOREGULATION IN CONSCIOUS DOGS
BAUMANN, JE
PERSSON, PB
EHMKE, H
NAFZ, B
KIRCHHEIM, HR
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1992, 263 (02): : F208 - F213

← 1 2 3 4 5 6 7 8 9 10 →