Nitric oxide (NO), produced in different cell types through the conversion of L-arginine into L-citrulline by the enzyme NO synthase, has been proposed to exert its action in several physiological and pathological events. The great propensity for nitrosothiol formation and breakdown represents a mechanism which modulates the action of macromolecules containing NO-reactive Cys residues at their active centre and/or allosteric sites. Based on the human haemoglobin (Hb) structure and accounting for the known acid-base catalysed Cys beta 93-nitrosylation and Cys beta 93NO-denitrosylation processes, the putative amino acid sequence (Lys/Arg/His/Asp/Glu)Cys(Asp/Glu) (sites -1, 0, and + 1, respectively) has been proposed as the minimum consensus motif for Cys-NO reactivity. Although not found in human Hb, the presence of a polar amino acid residue (Gly/Ser/Thr/Cys/Tyr/Asn/Gln) at the -2 position has been observed in some NO-reactive protein sequences (e.g., NMDA receptors). However, the most important component of the tri- or tetra-peptide consensus motif has been recognised as the Cys(Asp/Glu) pair [Stamler et at, Neuron (1997) 18, 691-696]. Here, we analyse the three-dimensional structure of several proteins containing NO-reactive Cys residues, and show that their nitrosylation and denitrosylation processes may depend on the Cys-Sy atomic structural microenvironment rather than on the tri- or tetra-peptide sequence consensus motif.

Ascenzi, P., Colasanti, M., Persichini, T., Muolo, M., Polticelli, F., Venturini, G., et al. (2000). Re-evaluation of amino acid sequence and structural consensus rules for cysteine-nitric oxide reactivity RID A-4573-2009. BIOLOGICAL CHEMISTRY, 381(7), 623-627 [10.1515/BC.2000.081 WC Biochemistry & Molecular Biology].

Re-evaluation of amino acid sequence and structural consensus rules for cysteine-nitric oxide reactivity RID A-4573-2009

POLTICELLI, Fabio;
2000-01-01

Abstract

Nitric oxide (NO), produced in different cell types through the conversion of L-arginine into L-citrulline by the enzyme NO synthase, has been proposed to exert its action in several physiological and pathological events. The great propensity for nitrosothiol formation and breakdown represents a mechanism which modulates the action of macromolecules containing NO-reactive Cys residues at their active centre and/or allosteric sites. Based on the human haemoglobin (Hb) structure and accounting for the known acid-base catalysed Cys beta 93-nitrosylation and Cys beta 93NO-denitrosylation processes, the putative amino acid sequence (Lys/Arg/His/Asp/Glu)Cys(Asp/Glu) (sites -1, 0, and + 1, respectively) has been proposed as the minimum consensus motif for Cys-NO reactivity. Although not found in human Hb, the presence of a polar amino acid residue (Gly/Ser/Thr/Cys/Tyr/Asn/Gln) at the -2 position has been observed in some NO-reactive protein sequences (e.g., NMDA receptors). However, the most important component of the tri- or tetra-peptide consensus motif has been recognised as the Cys(Asp/Glu) pair [Stamler et at, Neuron (1997) 18, 691-696]. Here, we analyse the three-dimensional structure of several proteins containing NO-reactive Cys residues, and show that their nitrosylation and denitrosylation processes may depend on the Cys-Sy atomic structural microenvironment rather than on the tri- or tetra-peptide sequence consensus motif.
2000
Ascenzi, P., Colasanti, M., Persichini, T., Muolo, M., Polticelli, F., Venturini, G., et al. (2000). Re-evaluation of amino acid sequence and structural consensus rules for cysteine-nitric oxide reactivity RID A-4573-2009. BIOLOGICAL CHEMISTRY, 381(7), 623-627 [10.1515/BC.2000.081 WC Biochemistry & Molecular Biology].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11590/137963
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