Received for publication February 10, 2006.
Revised February 10, 2006.
Accepted for publication February 13, 2006.
No NO for HO-1 from SNP (Relates to Article by Kim, et al. FastForward 26 January 2006)
Henning Schroder 1*
1 Martin Luther University
* Address correspondence to: E-mail: schroeder{at}pharmazie.uni-halle.de
Abstract
Nitric oxide (NO) and NO donors where among the first
reported inducers of the tissue protective protein heme
oxygenase-1 (HO-1) with a potential for eventual use in
humans. Besides other clinically established NO
releasing drugs, sodium nitroprusside (SNP) has
frequently been employed as an experimental tool to
explore effects of NO on HO-1 and other biological
targets. In this issue of Molecular Pharmacology,
Kim et al. demonstrate that the effects of SNP on
expression of HO-1 are mainly due to free iron released
from SNP in aqueous solution whereas NO plays a
negligible role, if any, as the mediator of response to
SNP. Downstream effects of iron, after being dissociated
from SNP, include increases in intracellular cAMP that
are causally linked to subsequent phosphorylation of
specific MAPK targets and enhanced HO-1 protein levels.
Based on the data by Kim et al., the use of SNP as an
experimental tool to mimic intracellular effects of NO
should be avoided in the future. This work not only
helps revise concepts in NO and HO-1 research but also
may direct future efforts to the role of iron and
reactive oxygen species in the regulation of adenylyl
cyclase.
Key words:
Guanylyl cyclase, Nitric oxide, Adenylyl cyclases, cAMP, cGMP, Protein Kinase A, MAP Kinase, Heme metabolism, Oxidative stress/antioxidants
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