Your search keyword '"Zuo, Zeping"' showing total 11 results

1. Synthesis, optimization and antitumor activity evaluation of sulfonyl benzoyl hydrazide derivatives as novel human LSD1 inhibitors.

Author

Ai, Wei and Zuo, Zeping

Subjects

*LEAD compounds, *TUMOR growth, *CELL cycle, *DRUG development, *SMALL molecules

Abstract

[Display omitted] • Developed a novel structure of LSD1 small molecule inhibitor through rational design. • 10e was optimized through rational design, which showed significant inhibitory activity against LSD1 in vitro. 10e exhibited a significant tumor inhibition rate in vivo. A new set of compounds known as sulfonyl benzoyl hydrazide derivatives were synthesized and tested using cellular assays. Through systematic optimization starting from general structure S-1, compound 10e emerged as highly promising. It exhibited potent inhibitory activity with an IC 50 value of 0.8 nM and possessed moderate clogP. Compounds 10e significantly inhibited solid tumor cells proliferation. Additionally, 10e induced apoptosis and arrested the cell cycle. Furthermore, in vivo studies using an HCT116 xenograft model showed substantial growth inhibition of tumors, accompanied by a favorable safety profile. These findings underscored compound 10e as a novel LSD1 inhibitor with robust efficacy both in vitro and in vivo , establishing it as a promising lead compound for further anticancer drug development. [ABSTRACT FROM AUTHOR]

Published

2024

2. Design and biological evaluation of tetrahydropyridine derivatives as novel human GPR119 agonists.

Author

Zuo, Zeping, Chen, Miaomiao, Shao, Xiaoni, Qian, Xinying, Liu, Xiaocong, Zhou, Xia, Xiang, Jiawei, Deng, Pengchi, Li, Yan, Jie, Hui, Liu, Chunqi, Cen, Xiaobo, Xie, Yongmei, and Zhao, Yinglan

Subjects

*BASAL metabolism, *IN vivo studies, *TYPE 2 diabetes, *LEAD compounds

Abstract

A series of novel tetrahydropyridine derivatives were prepared and evaluated using cell-based measurements. Systematic optimization of general structure G-1 led to the identification of compound 35 (EC 50 = 4.9 nM) and 37 (EC 50 = 8.8 nM) with high GPR119 agonism activity and moderate clog P. Through single and long-term pharmacodynamic experiments, we found that compound 35 showed a hypoglycemic effect and may have an effect on improving basal metabolic rate in DIO mice. Both in vitro and in vivo tests indicated that compound 35 was a potential potent GPR119 agonist in allusion to T2DM treatment. [ABSTRACT FROM AUTHOR]

Published

2020

3. ZY0511, a novel, potent and selective LSD1 inhibitor, exhibits anticancer activity against solid tumors via the DDIT4/mTOR pathway.

Author

Li, Yan, Tao, Lei, Zuo, Zeping, Zhou, Yang, Qian, Xinying, Lin, Yiyun, Jie, Hui, Liu, Chunqi, Li, Zhuoling, Zhang, Huaqin, Zhang, Hu, Cen, Xiaobo, Yang, Shengyong, and Zhao, Yinglan

Subjects

*CANCER cell proliferation, *HELA cells, *HISTONE methylation, *CANCER chemotherapy, *CANCER cells

Abstract

Lysine-specific demethylase1 (LSD1) plays a crucial role in cancer and has become a promising target for cancer therapy. However, the mechanism underlying the role of LSD1 in oncogenesis is poorly understood, and more effective LSD1 inhibitors are needed. Here we report the biological activity of a novel LSD1 inhibitor named ZY0511. ZY0511 specifically inhibited LSD1 activity and the proliferation of various human cancer cells especially the HeLa and HCT116 cells. ZY0511 significantly increased the expression of DDIT4 , a known mTORC1 suppressor, which was a direct downstream target of LSD1 confirmed by ChIP-PCR. ZY0511-induced LSD1 inhibition upregulated the expression of DDIT4 by altering histone H3K4 methylation levels at its promoter, thus suppressing mTORC1 activity. Knockdown of DDIT4 attenuated the anticancer effect of ZY0511. Intraperitoneal administration of ZY0511 significantly prevented the growth of HCT116 and HeLa xenografts in mice and showed no detectable toxicity. Moreover, DDIT4 expression was correlated with the sensitivity of human cancer cells to chemotherapy. Taken together, ZY0511 showed therapeutic potential for solid tumors, the induction of DDIT4 may be used as a predictive biomarker of LSD1 inhibitors. • ZY0511 is a novel LSD1 inhibitor which inhibits cancer cells proliferation. • DDIT4 is a direct downstream target of LSD1 which is a mTORC1 negative regulator. • ZY0511 triggers DDIT4 expression through altering H3K4me1/2 level of its promoter. • DDIT4 is correlated with cancer cells' sensitivity to chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2019

4. ZY0511, a novel, potent and selective LSD1 inhibitor, exhibits anticancer activity against solid tumors via the DDIT4/mTOR pathway.

Author

Li, Yan, Tao, Lei, Zuo, Zeping, Zhou, Yang, Qian, Xinying, Lin, Yiyun, Jie, Hui, Liu, Chunqi, Li, Zhuoling, Zhang, Huaqin, Zhang, Hu, Cen, Xiaobo, Yang, Shengyong, and Zhao, Yinglan

Abstract

Lysine-specific demethylase1 (LSD1) plays a crucial role in cancer and has become a promising target for cancer therapy. However, the mechanism underlying the role of LSD1 in oncogenesis is poorly understood, and more effective LSD1 inhibitors are needed. Here we report the biological activity of a novel LSD1 inhibitor named ZY0511. ZY0511 specifically inhibited LSD1 activity and the proliferation of various human cancer cells especially the HeLa and HCT116 cells. ZY0511 significantly increased the expression of DDIT4, a known mTORC1 suppressor, which was a direct downstream target of LSD1 confirmed by ChIP-PCR. ZY0511-induced LSD1 inhibition upregulated the expression of DDIT4 by altering histone H3K4 methylation levels at its promoter, thus suppressing mTORC1 activity. Knockdown of DDIT4 attenuated the anticancer effect of ZY0511. Intraperitoneal administration of ZY0511 significantly prevented the growth of HCT116 and HeLa xenografts in mice and showed no detectable toxicity. Moreover, DDIT4 expression was correlated with the sensitivity of human cancer cells to chemotherapy. Taken together, ZY0511 showed therapeutic potential for solid tumors, the induction of DDIT4 may be used as a predictive biomarker of LSD1 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2019

5. Integrated Solid-Phase Extraction, Ultra-High-Performance Liquid Chromatography–Quadrupole-Orbitrap High-Resolution Mass Spectrometry, and Multidimensional Data-Mining Techniques to Unravel the Metabolic Network of Dehydrocostus Lactone in Rats.

Author

Tian, Yingying, Ma, Beibei, Liu, Chuang, Zhao, Xinyue, Yu, Shangyue, Li, Yilin, Tian, Shiqiu, Pei, Hailuan, Wang, Zijian, Zuo, Zeping, and Wang, Zhibin

Subjects

*SOLID phase extraction, *MASS spectrometry, *LIQUID chromatography-mass spectrometry, *DATA mining, *DAUGHTER ions, *CHINESE medicine, *GLYCINE receptors, *HYDRATION

Abstract

Dehydrocostus lactone (DL) is among the representative ingredients of traditional Chinese medicine (TCM), with excellent anticancer, antibacterial, and anti-inflammatory activities. In this study, an advanced strategy based on ultra-high-performance liquid chromatography–quadrupole-Orbitrap high-resolution mass spectrometry (UHPLC–Q-Orbitrap HRMS) was integrated to comprehensively explore the metabolic fate of DL in rats. First, prior to data collection, all biological samples (plasma, urine, and feces) were concentrated and purified using solid-phase extraction (SPE) pre-treatment technology. Then, during data collection, in the full-scan (FS) data-dependent acquisition mode, FS-ddMS2 was intelligently combined with FS-parent ion list (PIL)-dynamic exclusion (DE) means for targeted monitoring and deeper capture of more low-abundance ions of interest. After data acquisition, data-mining techniques such as high-resolution extracted ion chromatograms (HREICs), multiple mass defect filters (MMDFs), diagnostic product ions (DPIs), and neutral loss fragments (NLFs) were incorporated to extensively screen and profile all the metabolites in multiple dimensions. As a result, a total of 71 metabolites of DL (parent drug included) were positively or tentatively identified. The results suggested that DL in vivo mainly underwent hydration, hydroxylation, dihydrodiolation, sulfonation, methylation, dehydrogenation, dehydration, N-acetylcysteine conjugation, cysteine conjugation, glutathione conjugation, glycine conjugation, taurine conjugation, etc. With these inferences, we successfully mapped the "stepwise radiation" metabolic network of DL in rats, where several drug metabolism clusters (DMCs) were discovered. In conclusion, not only did we provide a refined strategy for inhibiting matrix effects and fully screening major-to-trace metabolites, but also give substantial data reference for mechanism investigation, in vivo distribution visualization, and safety evaluation of DL. [ABSTRACT FROM AUTHOR]

Published

2022

6. Corrigendum to "ZY0511, a novel, potent and selective LSD1 inhibitor, exhibits anticancer activity against solid tumors via the DDIT4/mTOR pathway" [Cancer Lett. 454 (2019) 179-190].

Author

Li, Yan, Tao, Lei, Zuo, Zeping, Zhou, Yang, Qian, Xinying, Lin, Yiyun, Jie, Hui, Liu, Chunqi, Li, Zhuoling, Zhang, Huaqin, Zhang, Hu, Cen, Xiaobo, Yang, Shengyong, and Zhao, Yinglan

Subjects

*HELA cells, *MTOR protein, *GENE expression, *THERAPEUTICS, *CANCER cells

Published

2019

7. Network pharmacology and experimental verification to explore the anti-migraine mechanism of Yufeng Ningxin Tablet.

Author

Yu, Shangyue, Fan, Chunlan, Li, Yilin, Pei, Hailuan, Tian, Yingying, Zuo, Zeping, Wang, Zijian, Liu, Chuang, Zhao, Xinyue, and Wang, Zhibin

Subjects

*IN vitro studies, *MEDICINAL plants, *HERBAL medicine, *IN vivo studies, *MIGRAINE, *ANIMAL experimentation, *CELLULAR signal transduction, *GENE expression, *PHARMACEUTICAL chemistry, *PLANT extracts, *CHINESE medicine

Abstract

Yufeng Ningxin Tablet (YNT) is a traditional Chinese medicine formula, that has been used clinically to treat migraine for many years. It is composed of one herb Pueraria lobata var. lobata (Willd.) Ohwi (Relevant Chinese name: Gegen). Previously, it has been recorded by traditional Chinese doctor that Gegen could be used as medicine to treat migraine. However, the underlying mechanism of action remains to be investigated. It was to explore the effect and mechanism of YNT on migraine based on network pharmacology and experimental verification. First, with the network pharmacology, the effective chemical components and target genes of YNT were filtrated, the YNT-compound-migraine-targets network was constructed. The protein-protein interaction network (PPI) and literature reports were combined to identify potential targets of YNT in the treatment of migraine. Then, the representative compounds of YNT were characterized by LC-MS/MS and the major effect components were identified. Finally, the prediction results of network pharmacology were verified by animal and cell experiments. 7 bioactive components of YNT could act on 97 migraine potential targets. The 5 bioactive components could be characterized comprehensively of YNT. The key therapeutic targets and pathways were collected including 5-HT, CGRP, inflammation and nociceptive factors, and NF-κB signaling pathway. Animal experiments showed that YNT could increase the expression level of 5-HT and reduce the expression of CGRP, NF-κB, c-fos and IL-1β. YNT could inhibit LPS-induced neuroinflammation by NF-κB in BV2 cells in vitro. Western blotting analysis results showed YNT inhibited the NF-κB and phospho–NF–κB levels. It is the first time to verify the consistency between the metabolic components of YNT by LC-MS/MS and the active components predicted by network pharmacology. Meanwhile, the potential mechanism of YNT in the treatment of migraine was studied by combining network pharmacology and in vitro and in vivo experiments. • Investigating the anti-migraine mechanism of YNT by network pharmacology and experiment firstly. • Key anti-migraine targets including 5-HT, CGRP, NF-κB, IL-1β, and c-fos. • Two prototypical components and four metabolic components predicted by network pharmacology were validated. • Puerarin and Daidzein from YNT can treat migraine. [ABSTRACT FROM AUTHOR]

Published

2023

8. Corrigendum to "Design, synthesis and biological evaluation of novel procaine derivatives for intravenous anesthesia" [Bioorg. Med. Chem. Lett. 60 (2022) 128587].

Author

Yin, Jiaqi, Zhao, Yi, He, Qian, Hai, Ao, Peng, Yanlai, Zuo, Zeping, Gao, Lu, Song, Zhenlei, and Ke, Bowen

Subjects

*BIOSYNTHESIS, *INTRAVENOUS anesthesia, *PROCAINE

Published

2022

9. Design, synthesis and biological evaluation of novel procaine derivatives for intravenous anesthesia.

Author

Yin, Jiaqi, Zhao, Yi, He, Qian, Hai, Ao, Peng, Yanlai, Zuo, Zeping, Song, Zhenlei, and Ke, Bowen

Subjects

*BIOSYNTHESIS, *INTRAVENOUS anesthesia, *PROCAINE, *METHYL aspartate receptors

Abstract

[Display omitted] A series of novel procaine derivatives for intravenous anesthesia were prepared and evaluated by physicochemical properties and pharmacodynamic experiments in vivo and in vitro. Systematic optimization of procaine led to the identification of 6f , 6g , 6h , 6o , 6p and 6q with higher TI value and moderate log D. Compared with procaine (TI = 1.65), most procaine derivatives demonstrated better security, among which compound 6h (TI = 2.68) was the most notable one and showed fewer adverse events in animals. The result of hNR2B-HEK293 assay indicated that compound 6h suppressed the NMDA receptor 2B subtype channel activity and it showed more than 80% inhibitory effect at the concentration of 500 μM. [ABSTRACT FROM AUTHOR]

Published

2022

10. Discovery of novel inhibitors of human phosphoglycerate dehydrogenase by activity-directed combinatorial chemical synthesis strategy.

Author

Zhou, Xia, Tan, Yuping, Gou, Kun, Tao, Lei, Luo, Yuan, Zhou, Yue, Zuo, Zeping, Sun, Qingxiang, Luo, Youfu, and Zhao, Yinglan

Subjects

*COMBINATORIAL chemistry, *CHEMICAL synthesis, *HIGH throughput screening (Drug development), *DNA synthesis, *BREAST cancer

Abstract

[Display omitted] • We identified novel potent PHGDH inhibitors using high throughput screening. • We used activity-directed combinatorial chemical synthesis to optimize compounds. • b36 inhibited serine synthesis and induced cell cycle arrest in S-phase in vitro. Serine, the source of the one-carbon units essential for de novo purine and deoxythymidine synthesis plays a crucial role in the growth of cancer cells. Phosphoglycerate dehydrogenase (PHGDH) which catalyzes the first, rate-limiting step in de novo serine biosynthesis has become a promising target for the cancer treatment. Here we identified H-G6 as a potential PHGDH inhibitor from the screening of an in-house small molecule library based on the enzymatic assay. We adopted activity-directed combinatorial chemical synthesis strategy to optimize this hit compound. Compound b36 was found to be the noncompetitive and the most promising one with IC 50 values of 5.96 ± 0.61 μM against PHGDH. Compound b36 inhibited the proliferation of human breast cancer and ovarian cancer cells, reduced intracellular serine synthesis, damaged DNA synthesis, and induced cell cycle arrest. Collectively, our results suggest that b36 is a novel PHGDH inhibitor, which could be a promising modulator to reprogram the serine synthesis pathway and might be a potential anticancer lead worth further exploration. [ABSTRACT FROM AUTHOR]

Published

2021

11. Uric Acid Produces an Inflammatory Response through Activation of NF-κB in the Hypothalamus: Implications for the Pathogenesis of Metabolic Disorders.

Author

Lu, Wenjie, Shao, Xiaoni, Li, Yan, Hu, Jing, Zuo, Zeping, Zhao, Yinglan, Xu, Youzhi, Gao, Fabao, Shao, Xue, Cen, Xiaobo, and Zhou, Liangxue

Subjects

*URIC acid, *METABOLIC syndrome, *DIABETES, *HYPOTHALAMUS, *INFLAMMATION, *PROGNOSIS, *THERAPEUTICS

Abstract

Epidemiological studies have shown that an elevated uric acid (UA) level predicts the development of metabolic syndrome and diabetes; however, there is no direct evidence of this, and the underlying mechanism remains unclear. Here, we showed that a high-UA diet triggered the expression of pro-inflammatory cytokines, activated the NF-κB pathway, and increased gliosis in the hypothalamus. Intracerebroventricular injection of UA induced hypothalamic inflammation and reactive gliosis, whereas these effects were markedly ameliorated by the inhibition of NF-κB. Moreover, magnetic resonance imaging confirmed that hyperuricemia in rodents and humans was associated with gliosis in the mediobasal hypothalamus. Importantly, the rats administered UA exhibited dyslipidemia and glucose intolerance, which were probably mediated by hypothalamic inflammation and hypothalamic neuroendocrine alterations. These results suggest that UA can cause hypothalamic inflammation via NF-κB signaling. Our findings provide a potential therapeutic strategy for UA-induced metabolic disorders. [ABSTRACT FROM AUTHOR]

Published

2015