Response of mouse thymic cells to radiation after transfusion of mesenchymal stem cells

Zhang, Hongmei; Wang, Ling; Guo, Chuangxin; Tong, Zhimin; Liu, Yue; Meng, Xiangkuan; Feng, Hao; Chen, Yubing

doi:10.1097/md.0000000000005295

Cited by 1 publication

(2 citation statements)

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“…Apart from uncontrolled proliferation and apoptosis occurrence, tumour cells as well trigger impaired regulation of cell cycle. Cell circle interphase consists of G1, S and G2 phases, respectively, ensuring DNA synthesis preparation, DNA replication and mitosis preparation . Coptisine (0‐28.11 μmol/L, 24 hours; 0‐75 μmol/L, 48 hours) induced HCT‐116 cell cycle arrest in G1 phase as well as decreased expressions of CDK4, CDK2, cyclin E and cyclin C, which were key genes of G1/S phase …”

Section: Anti‐cancer Propertymentioning

confidence: 99%

“…Cell circle interphase consists of G1, S and G2 phases, respectively, ensuring DNA synthesis preparation, DNA replication and mitosis preparation. 29,30 Coptisine (0-28.11 μmol/L, 24 hours; 0-75 μmol/L, 48 hours) induced HCT-116 cell cycle arrest in G1 phase as well as decreased expressions of CDK4, CDK2, cyclin E and cyclin C, which were key genes of G1/S phase. 31,32 Similar anti-cancer property of coptisine was observed in liver 33,34 In the next study, authors revealed that coptisine and NCI•H1650 cells.…”

Section: Anti -C An Cer Propert Ymentioning

confidence: 99%

See 1 more Smart Citation

Coptisine fromCoptis chinensisexerts diverse beneficial properties: A concise review

Luo

Deng

et al. 2019

J Cellular Molecular Medi

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Coptisine is a natural small‐molecular compound extracted from Coptis chinensis (CC) with a history of using for thousands of years. This work aimed at summarizing coptisine's activity and providing advice for its clinical use. We analysed the online papers in the database of SciFinder, Web of Science, PubMed, Google scholar and CNKI by setting keywords as ‘coptisine’ in combination of ‘each pivotal pathway target’. Based on the existing literatures, we find (a) coptisine exerted potential to be an anti‐cancer, anti‐inflammatory, CAD ameliorating or anti‐bacterial drug through regulating the signalling transduction of pathways such as NF‐κB, MAPK, PI3K/Akt, NLRP3 inflammasome, RANKL/RANK and Beclin 1/Sirt1. However, we also (b) observe that the plasma concentration of coptisine demonstrates obvious non‐liner relationship with dosage, and even the highest dosage used in animal study actually cannot reach the minimum concentration level used in cell experiments owing to the poor absorption and low availability of coptisine. We conclude (a) further investigations can focus on coptisine's effect on caspase‐1‐involved inflammasome assembling and pyroptosis activation, as well as autophagy. (b) Under circumstance of promoting coptisine availability by pursuing nano‐ or microrods strategies or applying salt‐forming process to coptisine, can it be introduced to clinical trial.

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Section: Anti‐cancer Propertymentioning

confidence: 99%