Anthralin derivatives—inhibition of 5‐lipoxygenase—antipsoriatic efficacy

Tanzer, Helene; Braun, Christine; Seidel, Matthias; Wiegrebe, Wolfgang

doi:10.1002/ardp.2503241104

Cited by 5 publications

(4 citation statements)

References 26 publications

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“…Also not in favor of the "minimum structure" concept was the finding that the topically applied antiproliferatively active 1,8-diacetoxy-anthracene was not converted to a compound with a free C-l hydroxy group 40) . In contrast to the results with the HaCaT keratinocytes we recently found nonphenolic anthrones to be more active as inhibitors of arachidonic acid lipoxygenase from bovine polymorphonuclear leucocytes than anthralin, suggesting a different mode of action 42) .…”

Section: Significance Of Free Hydroxy Group At C-lcontrasting

confidence: 99%

“…8 and 9 also show activity similar to that of anthralin in the inhibition of leucotriene production; the acids 6 and 7, however, were more potent than anthralin. Their IC5o-values for 5-lipoxygenase-inhibition were found to be between 5 and 10 |iM (anthralin: IC 50 « 40 |iM) 42) . Concerning anthralin derivatives bearing acyl chains of different length at C- 10 Mustakallio 43M) has already stated that at this position substituents less bulky than glucose do not hamper antiproliferative activity.…”

Section: Significance Ofligands Replacing One Hydrogen Atom At C-10mentioning

confidence: 99%

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Structure‐function relationship of new anthralin derivatives assayed for growth inhibition and cytotoxicity in human keratinocyte cultures

Bonnekoh

Tanzer

Seidel

et al. 1991

Archiv der Pharmazie

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HaCaT keratinocyte cultures were exposed to twelve hydrophilic anthralin derivatives 1 to 12 with substituents at C-l and C-8 of the anthrone skeleton, of one H at C-10 and of both H's at C-10 by lacton rings ( fig. 1). After 3 uM treatment growth was determined by cellular protein content, ^-thymidineand 14 C-amino-acid-uptake and cytotoxicity by the release of cytoplasmic LDH into the culture medium.-In comparison to acetone control (100%) anthralin suppressed mean protein content, as well as DNA-and protein-synthesis to 33, 28, and 21%, respectively, and the drug revealed an enzyme release of 660%. In relation to the parent drug we found similar cell growth inhibitory effects of compounds 4, 6, 8, 9, 10, and 12. Deriv. 4, 8, and 10 were, however, to some extent less cytotoxic than anthralin, whereas deriv. 6, 9, and 12 were in the same range. An extreme suppression of growth parameters which differed from the anthralin effect by a factor 0.5-0.8 was caused by deriv. 11, showing the same cytotoxicity. Deriv. 1, 2, 3,5, and 7 did not demonstrate any cytotoxicity. Concerning growth parameters, deriv. 2 induced a slight stimulation, deriv. 3 and 7 were completely ineffective, deriv. 1 and 5 induced slightly to moderately inhibited proliferation but both being much less effective than anthralin. These data indicate that the "minimum structure" concept by Krebs and Schaltegger -claiming l-hydroxy-9-anthrone as a precondition for clinical antipsoriatic potency -is not valid at least in cell-biological tests and point toward possible usefulness of some experimental model compounds as alternative antipsoriatics.

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Section: Significance Of Free Hydroxy Group At C-lcontrasting

confidence: 99%

Section: Significance Ofligands Replacing One Hydrogen Atom At C-10mentioning

confidence: 99%

Structure‐function relationship of new anthralin derivatives assayed for growth inhibition and cytotoxicity in human keratinocyte cultures

Bonnekoh

Tanzer

Seidel

et al. 1991

Archiv der Pharmazie

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“…Both metabolites are not effective in 5-LO inhibition. 22 ' 39 Contrary to anthralin, compounds 4p and 7j of our series were not appreciably degraded during the 5-LO assay, and they were not hydrolyzed to anthralin.…”

Section: Discussionmentioning

confidence: 69%

Antipsoriatic anthrones with modulated redox properties. 1. Novel 10-substituted 1,8-dihydroxy-9(10H)-anthracenones as inhibitors of 5-lipoxygenase

Müller

Gürster²,

Piwek³

et al. 1993

J. Med. Chem.

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112

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The syntheses, the biological evaluation, and the structure-activity relationships of a novel series of l,8-dihydroxy-9(10H)-anthracenones bearing acyl-, alkyl-, or alkylidene-linked aromatic substituents in the 10-position are described. The phenylacyl and phenylalkylidene analogs were far more potent inhibitors of 5-lipoxygenase (5-LO) from bovine polymorphonuclear leukocytes (IC50 values in the 10 -7 M range) than the antipsoriatic drug anthralin, whereas phenylalkyl analogs were only weak inhibitors. Among the active compounds were both potent generators of hydroxyl radicals, as determined by deoxyribose degradation, and strong reducers of the stable free radical 2,2-diphenyl-l-picrylhydrazyl (DPPH). However, several derivatives of this series maintained 5-LO inhibitory activity but did not generate hydroxyl radicals and were not reactive with DPPH. In particular, phenylacyl analogs were also 6 times more efficient in inhibition of lipid peroxidation in model membranes than anthralin. Structure-activity relationships have shown that the presence of free phenolic groups in the attached aromatic ring is beneficial but not required for 5-LO inhibitory potency. The inhibitory potency in the 10-phenylacyl series increased with the length of the acyl chain with three methylene units being the optimum, suggesting a specific enzyme interaction which would not be expected for nonspecific redox inhibitors.Psoriasis is a widespread, chronic inflammatory and scaling skin disease, mainly characterized by increased cell proliferation of the epidermis.

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“…In light of these findings some biological studies on anthralin derivatives have to be reconsidered, since in each of these studies − the putative anthracenone 2a was prepared from 3 according to the method of Attree and Perkin . Confirmation of the position of the methoxy groups is therefore necessary before conclusions are drawn from the results of experiments which are performed to determine the structural features necessary for antipsoriatic activity.…”

Section: Resultsmentioning

confidence: 99%

Syntheses of Anthracenones. 2. Preparation of 1,8-Dimethoxy- (Dimethylanthralin) and 4,5-Dihydroxy-9(10H)-anthracenone (Isoanthralin): A Revision

et al. 1996

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The reduction of 1,8-dimethoxyanthracenedione with zinc dust and aqueous ammonia gives a mixture of 1,8-dimethoxyanthracene and 4,5-dimethoxy-9(10H)-anthracenone, rather than the isomeric 1,8-dimethoxy-9(10H)-anthracenone (dimethylanthralin). This isomer was obtained exclusively using SnCl(2) in HCl and acetic acid as reducing agent at room temperature. The structure was confirmed to exist as the tautomeric 1,8-dimethoxy-9-hydroxyanthracene. Furthermore, the reduction of 1,8-diacetoxyanthracenedione with SnCl(2) in HCl and acetic acid leads to 1,8-dihydroxy-9(10H)-anthracenone (anthralin) rather than 4,5-dihydroxy-9(10H)-anthracenone (isoanthralin), which was prepared by ether cleavage of 4,5-dimethoxy-9(10H)-anthracenone. In light of these findings some biological studies on antipsoriatic anthracenones have to be reconsidered.

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Anthralin derivatives—inhibition of 5‐lipoxygenase—antipsoriatic efficacy

Cited by 5 publications

References 26 publications

Structure‐function relationship of new anthralin derivatives assayed for growth inhibition and cytotoxicity in human keratinocyte cultures

Structure‐function relationship of new anthralin derivatives assayed for growth inhibition and cytotoxicity in human keratinocyte cultures

Antipsoriatic anthrones with modulated redox properties. 1. Novel 10-substituted 1,8-dihydroxy-9(10H)-anthracenones as inhibitors of 5-lipoxygenase

Syntheses of Anthracenones. 2. Preparation of 1,8-Dimethoxy- (Dimethylanthralin) and 4,5-Dihydroxy-9(10H)-anthracenone (Isoanthralin): A Revision

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