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Literature DB >> 21827806

Cellular uptake of transportan 10 and its analogs in live cells: Selectivity and structure-activity relationship studies.

Jingjing Song¹, Ming Kai, Wei Zhang, Jindao Zhang, Liwei Liu, Bangzhi Zhang, Xin Liu, Rui Wang.

Abstract

Transportan 10 (TP10) is an amphipathic cell-penetrating peptide with high translocation ability. In order to obtain more details of structure-activity relationship of TP10, we evaluated the effects of structure and charge on its translocation ability. Our results demonstrated that disrupting the helical structure or Arg substitution could remarkably decrease the cellular uptake of TP10. However, increasing the number of positive charge was an effective strategy to enhance translocation ability of TP10. Furthermore, the molecular dynamics simulation supported the results derived from experiments, suggesting that higher membrane disturbance leads to higher cellular uptake of peptides. In addition, our study also demonstrated TP10 and its analogs preferentially entered cancer cells rather than normal cells. The uptake selectivity toward cancer cells makes TP10 and its analogs as potent CPPs for drug delivery.

Entities: Chemical Disease

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Year: 2011 PMID： 21827806 DOI： 10.1016/j.peptides.2011.07.018

Source DB: PubMed Journal: Peptides ISSN： 0196-9781 Impact factor: 3.750

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Cited

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