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Design of small molecules targeting I-BAR proteins.

Curr. Pharm. Des.. 2015; 
CaoMeng,ChangWeiwei,ZhengMing,XieLi,ZhangYu,CaiJin,ChenJunqing,ZhanXi,JiMin,Gu
Products/Services Used Details Operation
Proteins, Expression, Isolation and Analysis … Protein concen- trations were determined by either Protein Assay or SDS/PAGE followed by Coomassie Blue staining using (BSA) as a reference The synthetic peptides MIM-S3 and MIM-S3-FITC were commer- cially prepared by GenScript Get A Quote

摘要

Missing in metastasis (MIM, also MTSS1) is a member of the inverse Bin-Amphiphysin-Rvs (I-BAR) family that senses and stabilizes negative membrane protrusions. Abnormal expression of MIM has been frequently associated with a subset of human cancers and may play different roles in different stages of tumor progression. Overexpression of MIM-I-BAR in 293A cells potentiated the cell growth and increased the toxic response to paclitaxel. To modulate the function of MIM within cells, we designed several short peptide derivatives to target I-BAR dimerization. One of these derivatives had a cyclic configuration with a potency to disrupt the dimerization of MIM or ABBA proteins in vitro, and to be readily interna... More

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