Solution Structure of an Intramolecular (3 + 1) Human Telomeric G-Quadruplex Bound to a Telomestatin Derivative

Chung, Wan Jun; Heddi, Brahim; Tera, Masayuki; Iida, Keisuke; Nagasawa, Kazuo; Phan, Anh Tuân

doi:10.1021/ja405843r

Cited by 163 publications

(179 citation statements)

References 69 publications

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“…G4 structure stabilization was recorded for sanguinarine in a considerably stronger extent than berberine. The ∆T m of F21T varied considerably in presence of these three alkaloids, although molecular modeling methods suggest almost the similar mode of interactions and comparable binding energies in the hybrid 3+1 topology [64]. Non-electrostatic interactions in the binding of small molecules to G4 are preferable for telomerase inhibition under physiological conditions [60].…”

Section: Discussionmentioning

confidence: 99%

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Selectivity of major isoquinoline alkaloids from Chelidonium majus towards telomeric G-quadruplex: A study using a transition-FRET (t-FRET) assay

Noureini

Esmaeili

Abachi

et al. 2017

Biochimica et Biophysica Acta (BBA) - General Subjects

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BackgroundNatural bioproducts are invaluable resources in drug discovery. Isoquinoline alkaloids of Chelidonium majus constitute a structurally diverse family of natural products that are of great interest, one of them being their selectivity for human telomeric G-quadruplex structure and telomerase inhibition. MethodsThe study focuses on the mechanism of telomerase inhibition by stabilization of telomeric Gquadruplex structures by berberine, chelerythrine, chelidonine, sanguinarine and papaverine. Telomerase activity and mRNA levels of hTERT were estimated using quantitative telomere repeat amplification protocol and qPCR, in MCF-7 cells treated with different groups of alkaloids. The selectivity of the main isoquinoline alkaloids of Chelidonium majus towards telomeric Gquadruplex forming sequences were explored using a sensitive modified thermal FRET-melting measurement in the presence of the complementary oligonucleotide CT22. We assessed and monitored G-quadruplex topologies using circular dichroism (CD) methods, and compared spectra to previously well-characterized motifs, either alone or in the presence of the alkaloids, Molecular modeling was performed to rationalize ligand binding to the G-quadruplex structure. ResultsThe results highlight strong inhibitory effects of chelerythrine, sanguinarine and berberine on telomerase activity, most likely through substrate sequestration. These isoquinoline alkaloids interacted strongly with telomeric sequence G-quadruplex. In comparison, chelidonine and papaverine had no significant interaction with the telomeric quadruplex, while they strongly inhibited telomerase at transcription level of hTERT. Altogether, all of the studied alkaloids showed various levels and mechanisms of telomerase inhibition. ConclusionsWe report on a comparative study of anti-telomerase activity of the isoquinoline alkaloids of Chelidonium majus. Chelerythrine was most effective in inhibiting telomerase activity by substrate sequesteration through G-quadruplex stabilization. General SignificanceUnderstanding structural and molecular mechanisms of anti-cancer agents can help in developing new and more potent drugs with fewer side effects. Isoquinolines are the most biologically active agents from Chelidonium majus, which have shown to be telomeric G-quadruplex stabilizers and potent telomerase inhibitors.

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Section: Discussionmentioning

confidence: 99%

“…The hybrid 3+1 topology of intramolecular telomeric quadruplex (PDB id 2MB3) was used as the starting point to study G4-ligand interactions [64]. The docking and molecular dynamics protocol was adapted from Ohnmacht et al [39].…”

Section: Molecular Dynamics (Md) Simulationsmentioning

confidence: 99%

Selectivity of major isoquinoline alkaloids from Chelidonium majus towards telomeric G-quadruplex: A study using a transition-FRET (t-FRET) assay

Noureini

Esmaeili

Abachi

et al. 2017

Biochimica et Biophysica Acta (BBA) - General Subjects

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“…More recently a series of macrocyclic molecules (telomestatin analogues) have been developed, with improved features over telomestatin parental structure (Granzhan et al 2010). Macrocyclic hexaoxazole L2H2-6 M (2) OTD is such a derivative of telomestatin which interact with G-quadruplex by p-stacking and electrostatic interactions (Chung et al 2013) telomestatin is currently under clinical trials (Kim and McAlpine 2013). Daunomycin (Fig.…”

Section: Compounds Targeting Telomeric Dna G-quadruplex Ligandsmentioning

confidence: 99%

Human telomerase inhibitors from microbial source

Kiran

Palaniswamy

Angayarkanni

2015

World J Microbiol Biotechnol

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Telomerase enzyme inhibitors have gained attention of scientific field due to the specificity of action of telomerase based therapies. Some telomerase have good combinatorial action with certain DNA damaging drugs. Natural compounds isolated from microbes provide a new scope of screening and large scale production of telomerase inhibitors. This review emphasizes the biochemistry and mode of action of different types of telomerase inhibitors isolated from microbial sources. Also elaborates on classification of telomerase inhibitors based on their mode of action in cancer cells.

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“…Finally, by combining the structural aspects of T4 and Telomestatin, Nagasawa et al made T9, which had a better potency in stabilizing the G-quadruplex than the one of T4 [67]. Resolving the structure of a complex formed between T9 and human telomeric G-quadruplex DNA, Nagasawa et al concluded that the analogue interacted with the G-quadruplex via p-stacking and electrostatic interactions [68].…”

Section: Telomestatinmentioning

confidence: 99%

Predicting the unpredictable: Recent structure–activity studies on peptide-based macrocycles

Wahyudi

McAlpine

2015

Bioorganic Chemistry

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Solution Structure of an Intramolecular (3 + 1) Human Telomeric G-Quadruplex Bound to a Telomestatin Derivative

Cited by 163 publications

References 69 publications

Selectivity of major isoquinoline alkaloids from Chelidonium majus towards telomeric G-quadruplex: A study using a transition-FRET (t-FRET) assay

Selectivity of major isoquinoline alkaloids from Chelidonium majus towards telomeric G-quadruplex: A study using a transition-FRET (t-FRET) assay

Human telomerase inhibitors from microbial source

Predicting the unpredictable: Recent structure–activity studies on peptide-based macrocycles

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