Activities of 7-Nitroindazole and 1-(2-(Trifluoromethylphenyl)-imidazole Independent of Neuronal Nitric-Oxide Synthase Inhibition

Matsumura, Nobuko; Kikuchi-Utsumi, Kazue; Nakaki, Toshio

doi:10.1124/jpet.107.135160

Cited by 18 publications

(15 citation statements)

References 39 publications

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“…In a study conducted by our group, pretreatment with 7-nitroindazole (7-NI), an nNOS inhibitor, also prevented both GSH depletion and nitrotyrosine formation induced by MPTP. Although we recently found 7-NI to be non-specific to nNOS (131), a previous report demonstrated attenuation of MPTP neurotoxicity in nNOS-deficient mice (132). These results suggest a major role of ONOO − derived from nNOS in MPTP-induced GSH depletion.…”

Section: Parkinson's Model and Eaac1mentioning

confidence: 74%

Regulation of Neuronal Glutathione Synthesis

2008

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Abstract. The brain is among the major organs generating large amounts of reactive oxygen species and is especially susceptible to oxidative stress. Glutathione (GSH) plays critical roles as an antioxidant, enzyme cofactor, cysteine storage form, the major redox buffer, and a neuromodulator in the central nervous system. GSH deficiency has been implicated in neurodegenerative diseases. GSH is a tripeptide comprised of glutamate, cysteine, and glycine. Cysteine is the rate-limiting substrate for GSH synthesis within neurons. Most neuronal cysteine uptake is mediated by sodium-dependent excitatory amino acid transporter (EAAT) systems, known as excitatory amino acid carrier 1 (EAAC1). Previous studies demonstrated EAAT is vulnerable to oxidative stress, leading to impaired function. A recent study found EAAC1-deficient mice to have decreased brain GSH levels and increased susceptibility to oxidative stress. The function of EAAC1 is also regulated by glutamate transporter associated protein 3-18. This review focuses on the mechanisms underlying GSH synthesis, especially those related to neuronal cysteine transport via EAAC1, as well as on the importance of GSH functions against oxidative stress.

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Section: Parkinson's Model and Eaac1mentioning

confidence: 74%

Regulation of Neuronal Glutathione Synthesis

2008

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“…However, the margin for inhibition between nNOS and eNOS is at best 4-fold. It has been speculated that 7-NI may act through an unknown mechanism other than nNOS inhibition [Matsumura et al, 2008].…”

Section: Discussionmentioning

confidence: 99%

Neuronal Nitric Oxide Synthase Inhibition Prevents Cerebral Palsy following Hypoxia-Ischemia in Fetal Rabbits: Comparison between JI-8 and 7-Nitroindazole

Derrick

Ji³

et al. 2011

Dev Neurosci

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moderately and 13 severely affected kits and 5 stillbirths, compared with 8 normal, 3 moderately affected and 5 severely affected kits and 10 stillbirths in the 7-NI group. In terms of neurobehavioral outcome, 7-NI was not different from saline treatment, while JI-8 was superior to saline and 7-NI in its protective effect (p ! 0.05). In the surviving kits, JI-8 significantly improved the locomotion score over both saline and 7-NI scores. JI-8 was also significantly superior to saline in preserving smell, muscle tone and righting reflex function, but 7-NI did not show significant improvement. Furthermore, a 100-fold increase in the dose (15.75 mol/kg) of 7-NI significantly decreased systolic blood pressure in the dam, while JI-8 did not. The new class of inhibitors such as JI-8 shows promise in the prevention of cerebral palsy and is superior to the previously more commonly used nNOS inhibitor.

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“…S-Methyl- l -thiocitrulline (Furfine et al ., 1994) is also used, albeit less frequently, to selectively inhibit nNOS in vitro and in vivo , yet studies show that the compound is <10-fold selective for isolated nNOS over eNOS (Furfine et al ., 1994; Boer et al ., 2000; both using human NOS isozymes). The use of other compounds with moderate or good selectivity for isolated nNOS, such as S , S ′-1,4-phenylene-bis(1,2-ethanediyl)bis-isothiourea (100-fold selectivity over eNOS; tested using isolated human NOS by Boer et al ., 2000), 1[2-(trifluoromethyl)phenyl]-1 H -imidazole (TRIM; 38-fold selectivity over eNOS determined with homogenates of mouse cerebellum and bovine aortic endothelial cells; Handy et al ., 1995) and AR-R17477 (28-fold over eNOS using human isozymes, Brzozowski et al ., 2011; 100-fold for rat nNOS over human eNOS in partially purified preparations, Reif et al ., 2000), is also hampered by problems such as a lack of specificity (isothioureas, see Babu and Griffith, 1998a; TRIM, Matsumura et al ., 2008) and/or a lack of availability (AR-R17477).…”

Section: Discussionmentioning

confidence: 99%

On the selectivity of neuronal NOS inhibitors

Pigott

Bartus

Garthwaite

2013

British J Pharmacology

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Background and PurposeIsoform-selective inhibitors of NOS enzymes are desirable as research tools and for potential therapeutic purposes. Vinyl-l-N-5-(1-imino-3-butenyl)-l-ornithine (l-VNIO) and Nω-propyl-l-arginine (NPA) purportedly have good selectivity for neuronal over endothelial NOS under cell-free conditions, as does N-[(3-aminomethyl)benzyl]acetamidine (1400W), which is primarily an inducible NOS inhibitor. Although used in numerous investigations in vitro and in vivo, there have been surprisingly few tests of the potency and selectivity of these compounds in cells. This study addresses this deficiency and evaluates the activity of new and potentially better pyrrolidine-based compounds.Experimental ApproachThe inhibitors were evaluated by measuring their effect on NMDA-evoked cGMP accumulation in rodent hippocampal slices, a response dependent on neuronal NOS, and ACh-evoked cGMP synthesis in aortic rings of the same animals, an endothelial NOS-dependent phenomenon.Key Resultsl-VNIO, NPA and 1400W inhibited responses in both tissues but all showed less than fivefold higher potency in the hippocampus than in the aorta, implying useless selectivity for neuronal over endothelial NOS at the tissue level. In addition, the inhibitors had a 25-fold lower potency in the hippocampus than reported previously, the IC50 values being approximately 1 μM for l-VNIO and NPA, and 150 μM for 1400W. Pyrrolidine-based inhibitors were similarly weak and nonselective.Conclusion and ImplicationsThe results suggest that l-VNIO, NPA and 1400W, as well as the newer pyrrolidine-type inhibitors, cannot be used as neuronal NOS inhibitors in cells without stringent verification. The identification of inhibitors with useable selectivity in cells and tissues remains an important goal.

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Activities of 7-Nitroindazole and 1-(2-(Trifluoromethylphenyl)-imidazole Independent of Neuronal Nitric-Oxide Synthase Inhibition

Cited by 18 publications

References 39 publications

Regulation of Neuronal Glutathione Synthesis

Regulation of Neuronal Glutathione Synthesis

Neuronal Nitric Oxide Synthase Inhibition Prevents Cerebral Palsy following Hypoxia-Ischemia in Fetal Rabbits: Comparison between JI-8 and 7-Nitroindazole

On the selectivity of neuronal NOS inhibitors

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