Therapeutic Implication of 'Iturin A' for Targeting MD-2/TLR4 Complex to Overcome Angiogenesis and Invasion

Overview

Journal Cell Signal

Date 2017 Mar 29

PMID 28347875

Citations 14

Authors

Goutam Dey

Rashmi Bharti

Probir Kumar Ojha

Ipsita Pal

Y Rajesh

Indranil Banerjee

Payel Banik

Sheetal Parida

Aditya Parekh

Ramkrishna Sen

Mahitosh Mandal

Affiliations

Soon will be listed here.

Abstract

Tumor angiogenesis and invasion are deregulated biological processes that drive multistage transformation of tumors from a benign to a life-threatening malignant state activating multiple signaling pathways including MD-2/TLR4/NF-κB. Development of potential inhibitors of this signaling is emerging area for discovery of novel cancer therapeutics. In the current investigation, we identified Iturin A (A lipopeptide molecule from Bacillus megaterium) as a potent inhibitor of angiogenesis and cancer invasion by various in vitro and in vivo methods. Iturin A was found to suppress VEGF, a powerful inducer of angiogenesis and key player in tumor invasion, as confirmed by ELISA, western blot and real time PCR. Iturin A inhibited endothelial tube arrangement, blood capillary formation, endothelial sprouting and vascular growth inside the matrigel. In addition, Iturin A inhibited MMP-2/9 expression in MDA-MB-231 and HUVEC cells. Cancer invasion, migration and colony forming ability were significantly hampered by Iturin A. Expressions of MD-2/TLR4 and its downstream MyD88, IKK-α and NF-κB were also reduced in treated MDA-MB-231 and HUVEC cells. Western blot and immunofluorescence study showed that nuclear accumulation of NF-κB was hampered by Iturin A. MD-2 siRNA or plasmid further confirmed the efficacy of Iturin A by suppressing MD-2/TLR4 signaling pathway. The in silico docking study showed that the Iturin A interacted well with the MD-2 in MD-2/TLR4 receptor complex. Conclusively, inhibition of MD-2/TLR4 complex with Iturin A offered strategic advancement in cancer therapy.

Citing Articles

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Zhao H, Yan L, Guo L, Sun H, Huang Q, Shao D AMB Express. 2021; 11(1):67.

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