Literature DB >> 26298529

Screening of multi-targeted natural compounds for receptor tyrosine kinases inhibitors and biological evaluation on cancer cell lines, in silico and in vitro.

Pushpendra Singh1, Felix Bast.   

Abstract

Receptors for growth factors encompass within the superfamily of receptor tyrosine kinases and are known to regulate numerous biological processes including cellular growth, proliferation, metabolism, survival, cell differentiation and apoptosis. These receptors have recently caught the attention of the researchers as an attractive target to combat cancer owing to the evidence suggesting their over-expression in cancer cells. Therefore, we studied receptor-based molecular docking of IR (PDB; 3ETA), IGF1R (PDB; 1K3A), EGFR (PDB; 1M17), VEGFIR (PDB; 3HNG), and VEGFIIR (PDB; 2OH4) against natural compounds. Further, in vitro investigation of the biological effect of lead molecules in an array of cancer cell lines was done. All selected natural compounds were docked with the X-ray crystal structure of selected protein by employing GLIDE (Grid-based Ligand Docking with Energetics) Maestro 9.6. InterBioScreen natural compounds docked with each selected protein molecules by using GLIDE high throughput virtual screening. On the basis of Gscore, we select 20 compounds along with 68 anticancer compounds for GLIDE extra precision molecular docking. It was discovered in this study that compound epigallocatechin gallate (EGCG) yielded magnificent Gscore with IGF1R (PDB; 1K3A) and VEGFIIR (PDB; 2OH4), and protein-ligand interactions are chart out. Effect of EGCG on biological activity such as mRNA expression of selected protein, cell proliferation, oxidative stress, and cell migration was reported after the 48 h treatments in cancer cell lines. The RT-PCR densitometric bands analysis showed that compound EGCG reduced the mRNA expression of IGF1R, VEGFIIR, and mTOR at 80 μM concentration. Moreover, EGCG significantly reduced cell proliferation and ROS generation after 48 h treatments. Our result also indicated a reduction in the potential for cell migration that might show in vivo anti-metastasis activity of EGCG.

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Year:  2015        PMID: 26298529     DOI: 10.1007/s12032-015-0678-8

Source DB:  PubMed          Journal:  Med Oncol        ISSN: 1357-0560            Impact factor:   3.064


  47 in total

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3.  Extra precision glide: docking and scoring incorporating a model of hydrophobic enclosure for protein-ligand complexes.

Authors:  Richard A Friesner; Robert B Murphy; Matthew P Repasky; Leah L Frye; Jeremy R Greenwood; Thomas A Halgren; Paul C Sanschagrin; Daniel T Mainz
Journal:  J Med Chem       Date:  2006-10-19       Impact factor: 7.446

4.  Challenges in the design of multitarget drugs against multifactorial pathologies: a new life for medicinal chemistry?

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9.  The synthetic flavonoid WYC02-9 inhibits cervical cancer cell migration/invasion and angiogenesis via MAPK14 signaling.

Authors:  Yun-Ju Chen; Yu-Jen Cheng; Amos C Hung; Yang-Chang Wu; Ming-Feng Hou; Yu-Chang Tyan; Shyng-Shiou F Yuan
Journal:  Gynecol Oncol       Date:  2013-10-18       Impact factor: 5.482

10.  EGCG, a major green tea catechin suppresses breast tumor angiogenesis and growth via inhibiting the activation of HIF-1α and NFκB, and VEGF expression.

Authors:  Jian-Wei Gu; Kristina L Makey; Kevan B Tucker; Edmund Chinchar; Xiaowen Mao; Ivy Pei; Emily Y Thomas; Lucio Miele
Journal:  Vasc Cell       Date:  2013-05-02
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  5 in total

Review 1.  Flavonoids: structure-function and mechanisms of action and opportunities for drug development.

Authors:  Stephen Safe; Arul Jayaraman; Robert S Chapkin; Marcell Howard; Kumaravel Mohankumar; Rupesh Shrestha
Journal:  Toxicol Res       Date:  2021-01-20

Review 2.  In Vitro and In Silico Studies of the Molecular Interactions of Epigallocatechin-3-O-gallate (EGCG) with Proteins That Explain the Health Benefits of Green Tea.

Authors:  Koichi Saeki; Sumio Hayakawa; Shogo Nakano; Sohei Ito; Yumiko Oishi; Yasuo Suzuki; Mamoru Isemura
Journal:  Molecules       Date:  2018-05-28       Impact factor: 4.411

3.  Computational Identification of Potential Multitarget Inhibitors of Nipah Virus by Molecular Docking and Molecular Dynamics.

Authors:  Vinay Randhawa; Shivalika Pathania; Manoj Kumar
Journal:  Microorganisms       Date:  2022-06-09

4.  Role of IGF-1R in ameliorating apoptosis of GNE deficient cells.

Authors:  Reema Singh; Priyanka Chaudhary; Ranjana Arya
Journal:  Sci Rep       Date:  2018-05-09       Impact factor: 4.379

Review 5.  Computational Molecular Docking and X-ray Crystallographic Studies of Catechins in New Drug Design Strategies.

Authors:  Shogo Nakano; Shin-Ichi Megro; Tadashi Hase; Takuji Suzuki; Mamoru Isemura; Yoriyuki Nakamura; Sohei Ito
Journal:  Molecules       Date:  2018-08-13       Impact factor: 4.411

  5 in total

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