Fine-tuning of biaryl dihedral angles: structural characterization of five homologous three-atom bridged biphenyls by X-ray crystallography

Edwards, David J.; Pritchard, Robin G.; Wallace, Timothy W.

doi:10.1107/s0108768105006713

Cited by 6 publications

(5 citation statements)

References 46 publications

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“…The difference in potency of 40 and 51 as tubulin polymerisation inhibitors mirrors that of their respective carbocyclic analogues 71 (IC 50 > 50 mM) 48 and 72 (IC 50 1.5 mM), 49 and indicates that at least one oxygen substituent in the C-ring is a prerequisite for tubulinbinding activity. However, the hexamethoxy series comprising 63 and 66-70, which had been prepared from the diol 64 for our crystallographic study, 31 was almost devoid of activity. The cytotoxicity of the dibenzazepine 66 (entry 13) is intriguing, given that its C-ring oxygenation pattern cannot be viewed as optimal, although it is recognised that the link between cytotoxicity and the ability to inhibit tubulin polymerisation is potentially complex.…”

Section: Discussionmentioning

confidence: 92%

“…The preparative routes to the dibenzoxepines 16, 51 and 56 have also been described in a patent application. 32 Compounds 18, 34 20, 34 63 31 and 67-70 31 were prepared using published procedures.…”

Section: Methodsmentioning

confidence: 99%

“…28 The toxicity of colchicine 15 precludes its clinical use as an antimitotic agent, but it is clear that the colchicine binding site of tubulin can accommodate a diverse range of structures and so offers considerable scope for the design of binding agents with minimised pharmacokinetic halflives and cardiostimulatory effects, 29 the latter being a potentially generic problem with tubulin-targeting VDAs. 18d,30 Our interest in the axial chirality of colchicine 15 led us to analyse the variation of the interaryl dihedral angle in a series of heterocyclic variants of the bridged biaryl core, 31 and we observed that the degree of helicity in dibenz [c,e]oxepines closely matches that found in colchicine 15. In pursuing this line we synthesised a series of new dibenz [c,e]oxepines and assessed their ability to inhibit tubulin polymerisation, which led to the identification of 5,7-dihydro-3,9,10,11-tetramethoxydibenz[c,e]oxepin-4-ol 16 as a new lead in the search for effective VDAs.…”

Section: Introductionmentioning

confidence: 94%

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Tubulin-binding dibenz[c,e]oxepines as colchinol analogues for targeting tumour vasculature

et al. 2011

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Various methoxy- and hydroxy-substituted dibenz[c,e]oxepines were prepared via the copper(I)-induced coupling of ether-tethered arylstannanes or the dehydrative cyclisation of 1,1'-biphenyl-2,2'-dimethanols, assembled using the Ullmann cross-coupling of ortho-bromoaryl carbonyl compounds. The dibenzoxepines were screened for their ability to inhibit tubulin polymerisation and the in vitro growth of K562 human chronic myelogenous leukemia cells. The most active was 5,7-dihydro-3,9,10,11-tetramethoxydibenz[c,e]oxepin-4-ol, whose tubulin inhibitory and cytotoxicity (IC(50)) values were 1 μM and 40 nM, respectively.

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Section: Discussionmentioning

confidence: 92%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 94%

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Tubulin-binding dibenz[c,e]oxepines as colchinol analogues for targeting tumour vasculature

et al. 2011

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“…1 A crystallographic analysis of the dibenz [c,e]oxepine nucleus 6 led by virtue of its ability to match, in both degree and sense, the conformational helicity of colchicine 2, which is crucial to the latter's ability to bind to tubulin, 7 and by analogy with Nacetylcolchinol methyl ether (NCME) 3, whose binding to tubulin is strong but rapidly reversible, i.e. compatible with druglike pharmacokinetics.…”

Section: Introductionmentioning

confidence: 99%

Tubulin-binding dibenz[c,e]oxepines: Part 2. Structural variation and biological evaluation as tumour vasculature disrupting agents

Rossington

Hadfield

Shnyder

et al. 2017

Bioorganic & Medicinal Chemistry

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5,7-Dihydro-3,9,10,11-tetramethoxybenz[c,e]oxepin-4-ol 1, prepared from a dibenzyl ether precursor via Pd-catalysed intramolecular direct arylation, possesses broad-spectrum in vitro cytotoxicity towards various tumour cell lines, and induces vascular shutdown, necrosis and growth delay in tumour xenografts in mice at sub-toxic doses. The biological properties of 1 and related compounds can be attributed to their ability to inhibit microtubule assembly at the micromolar level, by binding reversibly to the same site of the tubulin -heterodimer as colchicine 2 and the allocolchinol, N-acetylcolchinol 4.

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“…6,7 The interplay between benzylic central chirality and axis configuration, as illustrated above, is a recurrent theme in atroposelective biaryl synthesis, 1 and our interest in this area led us to investigate the potential of [7,5]-fused lactams based on 6,7dihydrodibenz[c,e]oxazolo [3,2-a]azepin-9-one 2 as conformationally restrained biaryls. Although the ring system in 2 is analogous to the [5,5]-and [6,5]-fused lactams introduced and exploited so productively by Meyers and co-workers, 8 the biaryl lactams described in our preliminary publication 9 were the first of their a School of Chemistry, The University of Manchester, Oxford Road, Manchester, M13 9PL, UK. E-mail: tim.wallace@manchester.ac.uk; Fax: +44 (0) 161 275 4939 b Synthetic Chemistry, GlaxoSmithKline, Medicines Research Centre, Gunnels Wood Road, Stevenage, SG1 2NY, UK type.…”

Section: Introductionmentioning

confidence: 99%

Kinetic and thermodynamic control of axial chirality in biaryl-derived fused oxazolidine lactams exploiting a centre-axis relay of unit efficiency

et al. 2007

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The condensation of a 2-substituted-2-aminoethanol with methyl 2'-formylbiphenyl-2-carboxylate produces only two of the four possible axially chiral 6,7-dihydrodibenz[c,e]oxazolo[3,2-a]azepin-9(4bH)-ones (fused oxazolidine lactams), with kinetically controlled diastereoisomer ratios of up to 96 : 4. Within each lactam product the central chirality of the oxazolidine-fused benzylic position C(4b) is relayed to the biaryl axis with unit efficiency, the mis-matching of these stereogenic elements being prohibited due to strain, as predicted by molecular mechanics calculations. Diastereoisomeric lactam pairs can be equilibrated by heating with acid, and under these thermodynamic conditions reversed diastereoisomer ratios of up to 26 : 74 are observed.

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Fine-tuning of biaryl dihedral angles: structural characterization of five homologous three-atom bridged biphenyls by X-ray crystallography

Cited by 6 publications

References 46 publications

Tubulin-binding dibenz[c,e]oxepines as colchinol analogues for targeting tumour vasculature

Tubulin-binding dibenz[c,e]oxepines as colchinol analogues for targeting tumour vasculature

Tubulin-binding dibenz[c,e]oxepines: Part 2. Structural variation and biological evaluation as tumour vasculature disrupting agents

Kinetic and thermodynamic control of axial chirality in biaryl-derived fused oxazolidine lactams exploiting a centre-axis relay of unit efficiency

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