Polarographic Measurements of Spontaneous and Mitochondria‐Promoted Oxidation of 5,6‐and 5,7‐Dihydroxytryptamine

Klemm, H. P.; Baumgarten, H. G.; Schlossberger, H.

doi:10.1111/j.1471-4159.1980.tb09016.x

Cited by 30 publications

(12 citation statements)

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“…Neither the MH ion of 5,6-DHT nor the ions related to its oligomerization products are detectable. These results show the high reactivity of 5,6-DHT in the presence of peroxidase H 2 O 2 and may be explained as due to the reaction pattern proposed by Klemm et al 25 5,6-DHT easily autooxidizes (see Scheme 2), generating an electrophilic o-quinone and other oxidation products which undergo extensive covalent binding with protein nucleophiles both in vitro 26 and in vivo. 27 The data obtained here may be explained by the formation, catalytically induced by H 2 O 2 , of such oxidation products and their fast reaction with peroxidase.…”

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confidence: 71%

“…Formation of simple oligomers up to octamers was observed and, even after 360 minutes, the reaction environment remained reddish-brown in color, with the production of only small amounts of precipitate. This comparison shows that only in the reaction of peroxidase H 2 O 2 are reactive species, like those indicated by Klemm et al, 25 produced. Instead, the reaction of 5,7-DHT peroxidase H 2 O 2 leads to the formation of oligomers.…”

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confidence: 77%

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Influence of peroxidase on the oligomerization of 5,6- and 5,7-dihydroxytryptamine investigated by matrix-assisted laser desorption/ionization mass spectrometry

Bertazzo

Favretto²,

Costa

et al. 1998

Rapid Commun. Mass Spectrom.

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The influence of peroxidase in the melanogenesis of 5,6-and 5,7-dihydroxytryptamines (DHT) was investigated by matrix-assisted laser desorption/ionization mass spectrometry. Incubation was carried out with peroxidase, in the presence or absence of hydrogen peroxide. Samples were withdrawn at various times, ultrafiltered to remove the enzyme and immediately lyophilized. Reaction of the two isomers with peroxidase alone revealed processes similar to those observed in the case of reaction with tyrosinase, leading to low molecular mass oligomers. Reaction with peroxidase and hydrogen peroxide showed very different reactivity of the two isomers. 5,6-DHT immediately led to the formation of a black precipitate, probably due to the reaction of its oxidation products with the enzyme. In contrast, 5,7-DHT formed oligomers, up to nonamers, originating from the molecule itself and from its oxidation products. Both isomers showed the same chemical reactivity with respect to hydrogen peroxide alone, with the formation of up to nonamer species from both original molecules and their oxidation products. # 1998 John Wiley & Sons, Ltd. Received 16 March 1998; Revised 17 April 1998; Accepted 20 April 1998 5,6-and 5,7-dihydroxytryptamine (5,6-DHT and 5,7-DHT) are formed in the brain from 5-hydroxytryptamine (5-HT, serotonin) either by autooxidation or enzymatically, and are known for their destructive action in vivo of both central and peripheral noradrenergic neurons.1-3 Both drugs are employed in in vivo studies, in which their neurotoxic action is of practical concern. The final process that results in neurotoxicity is similar for both drugs, i.e. covalent binding of reactive intermediates to nucleophiles in proteins. 4 In the presence of oxygen they form coloured quinones, pink with 5,7-DHT and black with 5,6-DHT, 5 which may either undergo polymerization (establishing melanin-like structures) or react with sulfydryl groups in peptides and proteins. 6 This reaction is accelerated when tyrosinase is added to the reaction medium, with the formation of insoluble black melanin-like pigments.In previous studies, 7,8 despite the usual assumption that neuromelanin originates from catecholamines, in an attempt to demonstrate that tryptamines are involved in melanogenesis we undertook an in vitro investigation of the enzymatic reaction of 5,6-DHT and 5,7-DHT with mushroom tyrosinase. Structural information on the reaction intermediates was obtained after withdrawing samples at different reaction times, and after ultrafiltration and lyophilization. The resulting samples were analysed by means of matrixassisted laser desorption/ionization (MALDI) mass spectrometry, which clearly identified several oligomer species in the reaction mixture. Using the MALDI approach it was found that, after 30 min, the reaction of 5,6-DHT with tyrosinase leads to a series of oligomers with molecular masses of 382, 572, 762, 952, 1142382, 572, 762, 952, , 1332382, 572, 762, 952, and 1522 to the oligomerization products of the precursor from dimer (382 Da)...

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confidence: 71%

mentioning

confidence: 77%

Influence of peroxidase on the oligomerization of 5,6- and 5,7-dihydroxytryptamine investigated by matrix-assisted laser desorption/ionization mass spectrometry

Bertazzo

Favretto²,

Costa

et al. 1998

Rapid Commun. Mass Spectrom.

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“…Two intracellular catalytic mechanisms have been proposed to explain the evolvement of the strong neurotoxicity potential of 5,7-DHT in vivo following its accumulation in monoaminergic neurons by transporters: 1) mitochondria-(i.e., cytochrome c-) mediated speeding of the autoxidation process of 5,7-DHT (transfer of electrons from 5,7-DHT to the cytochrome-c segment of the respiratory chain (Klemm et al, 1980), and 2) interaction of the hydroperoxide intermediate(s) of autoxidized 5,7-DHT (and its MAO-metabolites) with GSH-peroxidase and formation of trihydroxyindoles which autoxidize (via semiquinone radical intermediates) to give the 4,7-p-quinone of 5-OH-tryptamine (Sinhababu and Borchardt 1985; Tabatabaei and Dryhurst 1998).…”

Section: Hg Baumgarten and L Lachenmayer 590mentioning

confidence: 99%

“…Indole dimers then undergo autoxidation and intermolecular coupling to eventually yield insoluble melanoid polymeric products (Tabatabaie and Dryhurst, 1998). We have shown that rat brain mitochondria accelerate the autoxidation process of 5,6-DHT (Klemm et al, 1980). Under these conditions, oxidation of 5,6-DHT to the corresponding o-quinone is likely to occur.…”

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confidence: 95%

“…In SH-deficient milieu, intramolecular cyclization involving the side chain yields aminochrome I which rearranges to form the more stable 5,6-dihydroxyindole. 5,6-Dihydroxyindole (a natural intermediate in enzyme catalyzed melanogenesis) undergoes autoxidation to form the corresponding p-quinoneimine or to yield 5,6-o-indolequinone via semiquinone radical intermediates, a process during which H 2 O 2 is generated (Klemm et al, 1980;Blank et al, 1998). The semi-quinone radical intermediates serve as driving forces in the autoxidation process via generation of O 2 -.…”

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Serotonin neurotoxins — past and present

Baumgarten

Lachenmayer

2004

neurotox res

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Autoxidation pathways and redox reactions of dihydroxytryptamines (5,6- and 5,7-DHT) and of 6-hydroxydopamine (6-OH-DA) are illustrated, and their potential role in aminergic neurotoxicity is discussed. It is proposed that certain aspects of the cytotoxicity of 6-OH-DA and of the DHTs, namely redox cycling of their quinone- and quinoneimine-intermediates as a source of free radicals, may also apply to quinoidal reactive intermediates and to glutathionyl- or cysteinyl conjugates ("thioether adducts") of o-dihydroxylated (catechol-like) metabolites of certain substituted amphetamines (of methylenedioxymethamphetamine (MDMA) and of methylenedioxyamphetamine (MDA)). Despite similarities in their primary interaction with the plasmalemmal (serotonergic transporter/dopamine transporter, SERT/DAT) and vesicular monoamine transporters (VMAT2), MDMA and fenfluramine (N-ethyl-meta-trifluoromethamphetamine, Fen) differ substantially in many aspects of their metabolism, pharmacokinetics, pharmacology, and neurotoxicology profile; the consequences of these differences for neuronal response patterns and long-term survival prospects are not yet fully understood. However, sustained hyperthermia appears to be a critical factor in these differences. Methodological requirements for adequate detection and description of pre- and postsynaptic forms of drug-induced neurotoxicity are exemplified using recently published accounts. The inclusion of microglial markers into research strategies has widened contemporary pathogenetic concepts on methamphetamine (MA)-induced neurotoxicity as an example of inflammatory neurodegeneration, thus complementing the traditional ROS and RNS-dependent stress models. Amphetamine-type neurotoxicity studies may assist in elaborating of preventive strategies for human neurodegenerative disorders.

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Early development of an identified serotonergic neuron inHelisoma trivolvis embryos: Serotonin expression, de-expression, and uptake

1998

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Polarographic Measurements of Spontaneous and Mitochondria‐Promoted Oxidation of 5,6‐and 5,7‐Dihydroxytryptamine

Cited by 30 publications

References 15 publications

Influence of peroxidase on the oligomerization of 5,6- and 5,7-dihydroxytryptamine investigated by matrix-assisted laser desorption/ionization mass spectrometry

Influence of peroxidase on the oligomerization of 5,6- and 5,7-dihydroxytryptamine investigated by matrix-assisted laser desorption/ionization mass spectrometry

Serotonin neurotoxins — past and present

Early development of an identified serotonergic neuron inHelisoma trivolvis embryos: Serotonin expression, de-expression, and uptake

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