Synthesis and Evaluation of Quindoline Derivatives as G-Quadruplex Inducing and Stabilizing Ligands and Potential Inhibitors of Telomerase

Zhou, Jin; Lu, Yu; Ou, Tian Miao; Zhou, Jun; Huang, Zifang; Zhu, Xiao Feng; Du, Cui Juan; Bu, Xian Zhang; Ma, Lin; Gu, Lian Quan; Li, Yue Ming; Chan, Albert S. C.

doi:10.1021/jm050041b

Cited by 162 publications

(126 citation statements)

References 34 publications

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“…[15] This N-methylated quinacridine was selected because it does not interact with copper, as a result of the electronic poorness of its intracyclic nitrogen atoms and the lack of an ortho-chelating system (see the Supporting Information). As seen in Figure 1 B and C, the presence of either 360A or MMQ 16 led to an increase of the 295 (positive) and 265 nm (negative) signals, as previously reported for strong quadruplex binders. [7,13,16] These observations imply that in the presence of either ligand, the antiparallel structure is stabilized (Scheme 1 A, right).…”

supporting

confidence: 85%

“…The situation is dramatically different in the presence of MMQ 16 As demonstrated by the example of MMQ 16 (Figure 1 E), a tight-binding quadruplex ligand impeded the Cu-mediated unfolding of the 22AG quadruplex. However, 360A, which is known to have a higher affinity for the quadruplex than MMQ 16 (DT 1/2 = 21 versus 16 8C, respectively; see the Supporting Information), [4a, 15, 17] did not inhibit Cu II -mediated denaturation (Figure 1 D).…”

Section: Methodsmentioning

confidence: 96%

“…However, 360A, which is known to have a higher affinity for the quadruplex than MMQ 16 (DT 1/2 = 21 versus 16 8C, respectively; see the Supporting Information), [4a, 15, 17] did not inhibit Cu II -mediated denaturation (Figure 1 D). This observation can only be explained by a copper-related modification of the 360A quadruplex affinity, an alteration that must originate from a specific and reversible Cu II interaction with 360A.…”

Section: Methodsmentioning

confidence: 99%

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A Metal‐Mediated Conformational Switch Controls G‐Quadruplex Binding Affinity

et al. 2008

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supporting

confidence: 85%

Section: Methodsmentioning

confidence: 96%

Section: Methodsmentioning

confidence: 99%

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A Metal‐Mediated Conformational Switch Controls G‐Quadruplex Binding Affinity

et al. 2008

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“…[159,160] It is interesting that 11-subsitituted quindolines (Figure 11 d) designed and synthesized by our research group show stronger telomerase inhibitory activity than the disubstituted quindolines, with tel IC 50 values of 0.44-12.3 mm. [55,161] This can be attributed to the nitrogen atom in the pyridine ring of quindoline. Electron-donating groups such as substituted amino groups at the 11-position can enhance the basicity of the nitrogen atom in the pyridine ring, which is protonated at physiological pH, resulting in an increase in the electrostatic interaction between the quindoline derivatives and the negative electrostatic center of the G-quadruplex.…”

Section: Quindoline Analoguesmentioning

confidence: 99%

G‐Quadruplexes: Targets in Anticancer Drug Design

et al. 2008

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G-quadruplexes are special secondary structures adopted in some guanine-rich DNA sequences. As guanine-rich sequences are present in important regions of the eukaryotic genome, such as telomeres and the regulatory regions of many genes, such structures may play important roles in the regulation of biological events in the body. G-quadruplexes have become valid targets for new anticancer drugs in the past few decades. Many leading compounds that target these structures have been reported, and a few of them have entered preclinical or clinical trials. Nonetheless, the selectivity of this kind of antitumor compound has yet to be improved in order to suppress the side effects caused by nonselective binding. As drug design targets, the topology and structural characteristics of quadruplexes, their possible biological roles, and the modes and sites of small-ligand binding to these structures should be understood clearly. Herein we provide a summary of published research that has set out to address the above problem to provide useful information on the design of small ligands that target G-quadruplexes. This review also covers research methodologies that have been developed to study the binding of ligands to G-quadruplexes.

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“…Our previous studies showed that SYUIQ-5, a Cryptolepine derivative, could induce and stabilize G-quadruplexes (32). Long-term exposure of cells to low concentrations of SYUIQ-5 caused senescence and telomere shortening (33).…”

Section: Introductionmentioning

confidence: 99%

G-quadruplex ligand SYUIQ-5 induces autophagy by telomere damage and TRF2 delocalization in cancer cells

Zhou

Deng

Zhang

et al. 2009

Molecular Cancer Therapeutics

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Agents stabilizing G-quadruplexes have the potential to destroy the functional structure of telomere and could therefore act as antitumor agents. We previously reported that SYUIQ-5 could stabilize G-quadruplex, induce senescence, and inhibit c-myc gene promoter activity. In this study, we showed that SYUIQ-5 inhibited proliferation of CNE2 and HeLa cancer cells, triggered a rapid and potent telomere DNA damage response characterized by the formation of telomeric foci γ-H2AX, and obviously induced autophagy with the features of increased LC3-II and a punctuated pattern of YFP-LC3 fluorescence. These phenomena may primarily depend on the delocalization of TRF2 from telomere, which was further degraded by proteasomes. Furthermore, overexpression of TRF2 inhibited SYUIQ-5-induced γ-H2AX expression. Also, ATM was activated following SYUIQ-5 treatment. The pretreatment with ATM inhibitor ku55933 and ATM siRNA effectively reduced the production of γ-H2AX and LC3-II. ATM knockdown partially antagonized the anticancer effects of SYUIQ-5. Moreover, inhibition of autophagy by short hairpin RNA against the autophagy-related gene ATG5 attenuated the cytotoxicity of SYUIQ-5. These results indicated that SYUIQ-5 triggered potent telomere damage through TRF2 delocalization from telomeres, and eventually induced autophagic cell death in cancer cells. Our findings exhibit a novel mechanism that is responsible for the antitumor effects of SYUIQ-5. [Mol Cancer Ther 2009;8 (12):3203-13]

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Synthesis and Evaluation of Quindoline Derivatives as G-Quadruplex Inducing and Stabilizing Ligands and Potential Inhibitors of Telomerase

Cited by 162 publications

References 34 publications

A Metal‐Mediated Conformational Switch Controls G‐Quadruplex Binding Affinity

A Metal‐Mediated Conformational Switch Controls G‐Quadruplex Binding Affinity

G‐Quadruplexes: Targets in Anticancer Drug Design

G-quadruplex ligand SYUIQ-5 induces autophagy by telomere damage and TRF2 delocalization in cancer cells

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