Your search keyword '"Qiao, Hong"' showing total 4 results

1. A new class of hybrid anticancer agents inspired by the synergistic effects of curcumin and genistein: Design, synthesis, and anti-proliferative evaluation.

Author

Chen, Qiao-Hong, Yu, Kevin, Zhang, Xiaojie, Chen, Guanglin, Hoover, Andrew, Leon, Francisco, Wang, Rubing, Subrahmanyam, Nithya, Addo Mekuria, Ermias, and Harinantenaina Rakotondraibe, Liva

Subjects

*ANTINEOPLASTIC agents, *DRUG synergism, *GENISTEIN, *CURCUMIN, *DRUG design, *DRUG synthesis, *THERAPEUTICS

Abstract

Inspired by the synergistic effects of dietary natural products with different scaffolds on the inhibition of cancer cell proliferation, incorporation of central (1 E ,4 E )-1,4-penta-dien-3-one linker (an optimal substitute for the central metabolically unstable diketone linker of curcumin), 1-alkyl-1 H -imidazol-2-yl (a promising bioisostere of terminal aryl group in curcumin), and chromone (the common pharmacophore in genistein and quercetin) into one chemical entity resulted in ten new hybrid molecules, 3-((1 E ,4 E )-5-(1-alkyl-1 H -imidazol-2-yl)-3-oxopenta-1,4-dien-1-yl)-4 H -chromen-4-ones. They were synthesized through a three-step transformation using acid-catalyzed aldol condensation as key step. The WST-1 cell proliferation assay showed that they have greater anti-proliferative potency than curcumin, quercetin, and genistein on both androgen-dependent and androgen-independent human prostate cancer cells. [ABSTRACT FROM AUTHOR]

Published

2015

2. Asymmetric 1,5-diarylpenta-1,4-dien-3-ones: Antiproliferative activity in prostate epithelial cell models and pharmacokinetic studies.

Author

Zhang, Xiaojie, Guo, Shanchun, Chen, Chengsheng, Perez, German Ruiz, Zhang, Changde, Patanapongpibul, Manee, Subrahmanyam, Nithya, Wang, Rubing, Keith, Joshua, Chen, Guanglin, Dong, Yan, Zhang, Qiang, Zhong, Qiu, Zheng, Shilong, Wang, Guangdi, and Chen, Qiao-Hong

Subjects

*PHARMACOKINETICS, *DRUG bioavailability, *EPITHELIAL cells, *DIOLEFINS, *DRUG design, *PROSTATE cancer treatment

Abstract

To further engineer dienones with optimal combinations of potency and bioavailability, thirty-four asymmetric 1,5-diarylpenta-1,4-dien-3-ones ( 25 – 58 ) have been designed and synthesized for the evaluation of their in vitro anti-proliferative activity in three human prostate cancer cell lines and one non-neoplastic prostate epithelial cell line. All these asymmetric dienones are sufficiently more potent than curcumin and their corresponding symmetric counterparts. The optimal dienone 58 , with IC 50 values in the range of 0.03–0.12 μM, is 636-, 219-, and 454-fold more potent than curcumin in three prostate cancer cell models. Dienones 28 and 49 emerged as the most promising asymmetric dienones that warrant further preclinical studies. The two lead compounds demonstrated substantially improved potency in cell models and superior bioavailability in rats, while exhibiting no acute toxicity in the animals at the dose of 10 mg/kg. Dienones 28 and 46 can induce PC-3 cell cycle regulation at the G 0 /G 1 phase. However, dienone 28 induces PC-3 cell death in a different way from 46 even though they share the same scaffold, indicating that terminal heteroaromatic rings are critical to the action of mechanism for each specific dienone. [ABSTRACT FROM AUTHOR]

Published

2017

3. Design, synthesis, and biological evaluation of 1,9-diheteroarylnona-1,3,6,8-tetraen-5-ones as a new class of anti-prostate cancer agents.

Author

Zhang, Xiaojie, Wang, Rubing, Perez, German Ruiz, Chen, Guanglin, Zhang, Qiang, Zheng, Shilong, Wang, Guangdi, and Chen, Qiao-Hong

Subjects

*DRUG design, *DRUG synthesis, *TETRAENES, *CANCER chemotherapy, *PROSTATE cancer treatment, *DRUG efficacy

Abstract

In search of more effective chemotherapeutics for the treatment of castration-resistant prostate cancer and inspired by curcumin analogues, twenty five (1 E ,3 E ,6 E ,8 E )-1,9-diarylnona-1,3,6,8-tetraen-5-ones bearing two identical terminal heteroaromatic rings have been successfully synthesized through Wittig reaction followed by Horner–Wadsworth–Emmons reaction. Twenty-three of them are new compounds. The WST-1 cell proliferation assay was employed to assess their anti-proliferative effects toward both androgen-sensitive and androgen-insensitive human prostate cancer cell lines. Eighteen out of twenty-five synthesized compounds possess significantly improved potency as compared with curcumin. The optimal compound, 78 , is 14- to 23-fold more potent than curcumin in inhibiting prostate cancer cell proliferation. It can be concluded from our data that 1,9-diarylnona-1,3,6,8-tetraen-5-one can serve as a new potential scaffold for the development of anti-prostate cancer agents and that pyridine-4-yls and quinolin-4-yl act as optimal heteroaromatic rings for the enhanced potency of this scaffold. Two of the most potent compounds, 68 and 75 , effectively suppress PC-3 cell proliferation by activating cell apoptosis and by arresting cell cycle in the G 0 /G 1 phase. [ABSTRACT FROM AUTHOR]

Published

2016

4. A new class of flavonol-based anti-prostate cancer agents: Design, synthesis, and evaluation in cell models.

Author

Li, Xiang, Chen, Guanglin, Zhang, Xiaojie, Zhang, Qiang, Zheng, Shilong, Wang, Guangdi, and Chen, Qiao-Hong

Subjects

*FLAVONOLS, *PROSTATE cancer treatment, *DRUG design, *CANCER cell proliferation, *DRUG synthesis, *THERAPEUTICS

Abstract

Flavonoids are a large class of polyphenolic compounds ubiquitously distributed in dietary plants with an array of biological activities. Flavonols are a major sub-class of flavonoids featuring a hydroxyl group at C-3. Certain natural flavonols, such as quercetin and fisetin, have been shown by in vitro cell-based and in vivo animal experiments to be potential anti-prostate cancer agents. However, the Achilles’ heel of flavonols as drug candidates is their moderate potency and poor pharmacokinetic profiles. This study aims to explore the substitution effect of 3-OH in flavonols on the in vitro anti-proliferative potency against both androgen-sensitive and androgen-insensitive human prostate cancer cell lines. Our first lead flavonol (3′,4′-dimethoxyflavonol), eight 3- O -alkyl-3′,4′-dimethoxyflavonols, and six 3- O -aminoalkyl-3′,4′-dimethoxyflavonols have been synthesized through aldol condensation and the Algar–Flynn–Oyamada (AFO) reaction. The WST-1 cell proliferation assay indicates (i) that all synthesized 3- O -alkyl-3′,4′-dimethoxyflavonols and 3- O -aminoalkyl-3′,4′-dimethoxyflavonols are more potent than the parent 3′,4′-dimethoxyflavonol and the natural flavonol quercetin in suppressing prostate cancer cell proliferation; and (ii) that incorporation of a dibutylamino group to the 3-OH group through a three- to five-carbon linker leads to the optimal derivatives with up to 292-fold enhanced potency as compared with the parent flavonol. Flow cytometry analysis showed that the most potent derivative 22 can activate PC-3 cell cycle arrest at the G 2 /M phase and induce PC-3 cell apoptosis. No inhibitory ability of 22 up to 50 μM concentration was observed against PWR-1E normal human epithelial prostate cells, suggesting its in vitro safety profile. The results indicate that chemical modulation at 3-OH is a vital strategy to optimize flavonols as anti-prostate cancer agents. [ABSTRACT FROM AUTHOR]

Published

2016