Selenadiazole Derivatives Inhibit Angiogenesis‐Mediated Human Breast Tumor Growth by Suppressing the VEGFR2‐Mediated ERK and AKT Signaling Pathways

Lai, Haoqiang; Fu, Xin; Sang, Chengcheng; Hou, Liyuan; Feng, Pengju; Li, Xiaoling; Chen, Tianfeng

doi:10.1002/asia.201800110

Cited by 20 publications

(10 citation statements)

References 49 publications

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“…Similar to ROS, when the intracellular calcium exceeds a certain threshold, it may in turn inhibit the p44/p42-MAPK pathway leading to crosstalk between other signaling pathways. In addition, studies have shown that MAPK and AKT are the main oxidative stress sensitive signal transduction pathways [25]. Consistent with reported studies, we found that DOX can activate p38MAPK and JNK signals [46].…”

Section: Discussionsupporting

confidence: 91%

“…A549 cells and NCM460 cells were purchased from ATCC (Manassas, VA) and cultured according to manufactory's instruction. After pretreated with NB for 12 h, different doses of chemotherapy agents were added and cocultured for 72 h. Cell viability was determined by MTT assay according to previous publications [25].…”

Section: Cell Culture and Determination Of Cell Viabilitymentioning

confidence: 99%

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Chemosensitization of doxorubicin against lung cancer by nature borneol, involvement of TRPM8-regulated calcium mobilization

Lai¹,

Liu

Lin³

et al. 2020

Preprint

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Background Lung cancer possesses high mortality rate and tolerances to multiple chemotherapeutics. Natural Borneol (NB) is a monoterpenoid compound that found to facilitate the bioavailability of drugs. In this study, we attempted to investigate effects of NB on the chemosensitivity in A549 cells and try to elucidate its therapeutic target. Methods The effects of NB on chemosensitivity in A549 cells was examined by MTT assay. The mechanism studies were evaluated by flow cytometry and western blotting assay. Surface plasmon resonance (SPR) and LC-MS combined analysis (MS-SPRi) was performed to elucidate the candidate target of NB contributes to this synergism. The chemosensitizing capacity of NB in vivo was conducted in nude mice bearing A549 tumors. Results NB pretreatment sensitizes A549 cells to low dosage of DOX, leading to a 15.7% to 41.5% increase in apoptosis, which is corelated with ERK and AKT inactivation but activation of phosphor-p38MAPK, -JNK and p53. Furthermore, this synergism depends on reactive oxygen species (ROS) generation. The MS-SPRi analysis reveals that the transient receptor potential melastatin-8 (TRPM8) is the interaction target of NB in potentiating DOX killing potency. Genetically knock down of TRPM8 significantly suppress the chemosensitizing effects of NB with the involvement of inhibiting ROS generation through restraining calcium mobilization. Moreover, pretreatment of NB synergistically enhanced the anticancer effects of DOX to delay tumor progression in vivo. Conclusions These results suggest that TRPM8 may be a valid therapeutic target in the potential application of NB serves as a chemosensitizer for lung cancer treatment.

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Section: Discussionsupporting

confidence: 91%

Section: Cell Culture and Determination Of Cell Viabilitymentioning

confidence: 99%

Chemosensitization of doxorubicin against lung cancer by nature borneol, involvement of TRPM8-regulated calcium mobilization

Lai¹,

Liu

Lin³

et al. 2020

Preprint

Self Cite

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“…[34] Western Blot Assay AWestern blot assay was used to determine the changes in the expression levels of the proteins after treatment with the iron complexes and TRAIL, according to al iterature procedure. [35]…”

Section: Ros Generationmentioning

confidence: 99%

Iron(II)−Polypyridyl Complexes Inhibit the Growth of Glioblastoma Tumor and Enhance TRAIL‐Induced Cell Apoptosis

Lin

Wang

Lai

et al. 2018

Chemistry An Asian Journal

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A promising cancer-targeting agent for the induction of apoptosis in tumor necrosis factor (TNF) proteins, the TNF-related apoptosis-inducing ligand (TRAIL) ligand, has found limited applications in the treatment of cancer cells, owing to its resistance by cancer cell lines. Therefore, the rational design of anticancer agents that could sensitize cancer cells towards TRAIL is of great significance. Herein, we report that synthetic iron(II)-polypyridyl complexes are capable of inhibiting the proliferation of glioblastoma cancer cells and efficiently enhancing TRAIL-induced cell apoptosis. Mechanistic studies demonstrated that the synthesized complexes induced cancer-cell apoptosis through triggering the activation of p38 and p53 and inhibiting the activation of ERK. Moreover, uPA and MMP-2/MMP-9, among the most important metastatic regulatory proteins, were also found to be significantly alerted after the treatment. Furthermore, we also found that tumor growth in nude mice was significantly inhibited by iron complex Fe2 through the induction of apoptosis without clear systematic toxicity, as indicated by histological analysis. Taken together, this study provides evidence for the further development of metal-based anticancer agents and chemosensitizers of TRAIL for the treatment of human glioblastoma cancer cells.

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“…123 p-Methylbenzaldehyde derived selenadiazole also showed breast cancer tumor growth inhibition in murine model, due to antiangiogenic effect, as reflected by a greater growth inhibition of endothelial cells HUVEC in Matrigel plug assays. 133 2-Indol-3-ylbenzimidazol-6-yl derivative was conjugated to a cyclic peptide containing RGD sequence, able to target αVβ3 integrin. 134 Taking advantage of fluorescent properties of the compound, improved cellular uptake of integrin-overexpressing cancer cells (HepG2) could be confirmed, thus enhancing the effectiveness of radiotherapy in vitro and reproducibility in vivo.…”

Section: 24-selenadiazolesmentioning

confidence: 99%

Development and Therapeutic Potential of Selenazo Compounds

et al. 2019

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Incorporation of selenium (Se) atom into small molecules can substantially enhance their antioxidant, antiinflammatory, antimutagenic, antitumoral or chemopreventive, antiviral, antibacterial, antifungal, antiparasitic, and neuroprotective effects. Specifically, selenazo compounds have received great attention owing to their chemical properties, pharmaceutical applications, and low toxicity. In this Perspective, we compile extensive literature evidence with the description and discussion of the most recent advances in different selenazo and selenadiazo motifs as potential pharmacological candidates. We also provide some perspectives on the challenges and future directions in the advancement of these selenazo compounds, each of which could generate drug candidates for various diseases.

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Selenadiazole Derivatives Inhibit Angiogenesis‐Mediated Human Breast Tumor Growth by Suppressing the VEGFR2‐Mediated ERK and AKT Signaling Pathways

Cited by 20 publications

References 49 publications

Chemosensitization of doxorubicin against lung cancer by nature borneol, involvement of TRPM8-regulated calcium mobilization

Chemosensitization of doxorubicin against lung cancer by nature borneol, involvement of TRPM8-regulated calcium mobilization

Iron(II)−Polypyridyl Complexes Inhibit the Growth of Glioblastoma Tumor and Enhance TRAIL‐Induced Cell Apoptosis

Development and Therapeutic Potential of Selenazo Compounds

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