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Computational insights into the interaction mechanism of transcription cofactor vestigial-like protein 4 binding to TEA domain transcription factor 4 by molecular dynamics simulation and molecular mechanics generalized Born/surface area) calculation.

J Biomol Struct Dyn. 2019; 
Gao J, Zhang Y, Chen H, Chen Q, Feng D, Zhang L, Li C.
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Peptide Synthesis … To validate the results from MD simulations, several Biotinylated VGLL4 peptides (ie, VGLL4218–252, VGLL4223–250, VGLL4deletion-b1, VGLL4mutant-a2, and VGLL4deletion-a3) were syn- thesized by GenScript (Piscataway, NJ, USA) … Get A Quote

摘要

Hippo pathway has been implicated in the suppression of tissue overgrowth and tumor formation by restricting the oncogenic activity of Yes-associated protein (YAP). Transcription cofactor vestigial-like protein 4 (VGLL4), a natural YAP antagonist that competes with YAP for TEA domain transcription factor 4 (TEAD4) binding is a potential tumor suppressor in human gastric cancer. Comparing with the full length of VGLL4, the Tondu 2 domain of VGLL4 alone is fully functional in inhibiting YAP-induced TEAD4 reporter activity. Revealing the details of binding interaction between VGLL4 and TEAD4 would accelerate the discovery of improved drugs against YAP-driven human cancers. We investigated systematically the intera... More

关键词

Hippo pathway; MM/GBSA calculation; TEAD4; VGLL4; molecular dynamics simulation