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Hui Zeng

Researcher at Chinese Academy of Sciences

Publications -  5
Citations -  69

Hui Zeng is an academic researcher from Chinese Academy of Sciences. The author has contributed to research in topics: Cancer & Liver cancer. The author has an hindex of 3, co-authored 5 publications receiving 34 citations.

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125I suppressed the Warburg effect viaregulating miR-338/PFKL axis in hepatocellular carcinoma

TL;DR: In this article, the effect of 125I irradiation on glycolysis was detected and miR-338 directly interacted with PFKL and suppressed its expression, which was a new potential strategy for HCC clinical treatment.
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MicroRNA-339 inhibits human hepatocellular carcinoma proliferation and invasion via targeting ZNF689.

TL;DR: It is revealed that miR-339 inhibits HCC growth through targeting oncoprotein ZNF689 and restoration of miR -339 might be feasible therapeutic strategy for HCC treatment.
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lncRNA PCAT6 facilitates cell proliferation and invasion via regulating the miR-326/hnRNPA2B1 axis in liver cancer.

TL;DR: Wang et al. as mentioned in this paper showed that the expression of PCAT6 and heterogeneous nuclear ribonucleoprotein A2B1 was upregulated in liver cancer tissues compared with non-cancerous tissues and were associated with poor overall survival time, whereas microRNA (miR)-326 expression was downregulated.
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Evaluation of efficacy of transcatheter arterial chemoembolization combined with computed tomography-guided radiofrequency ablation for hepatocellular carcinoma using magnetic resonance diffusion weighted imaging and computed tomography perfusion imaging: A prospective study.

TL;DR: It is indicated that MR-DWI and CT-PI can effectively evaluate the efficacy of TACE combined with CT-RFA and postoperative recurrence of HCC and show lower AFP concentration than those of SD’s PD.
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Atorvastatin potentiates the chemosensitivity of human liver cancer cells to cisplatin via downregulating YAP1

TL;DR: The results of the present study suggested the underlying mechanisms of atorvastatin chemosensitivity in inducing liver cancer cell apoptosis via downregulating YAP1 and implicated the potential application of atOrvastsatin-potentiated chemos sensitivity in liver cancer therapy.