Literature DB >> 32786217

Macropinocytosis as a Key Determinant of Peptidomimetic Uptake in Cancer Cells.

Daniel Y Yoo1, Stephanie A Barros1, Gordon C Brown1, Christian Rabot1, Dafna Bar-Sagi2, Paramjit S Arora1.   

Abstract

Peptides and peptidomimetics represent the middle space between small molecules and large proteins-they retain the relatively small size and synthetic accessibility of small molecules while providing high binding specificity for biomolecular partners typically observed with proteins. During the course of our efforts to target intracellular protein-protein interactions in cancer, we observed that the cellular uptake of peptides is critically determined by the cell line-specifically, we noted that peptides show better uptake in cancer cells with enhanced macropinocytic indices. Here, we describe the results of our analysis of cellular penetration by different classes of conformationally stabilized peptides. We tested the uptake of linear peptides, peptide macrocycles, stabilized helices, β-hairpin peptides, and cross-linked helix dimers in 11 different cell lines. Efficient uptake of these conformationally defined constructs directly correlated with the macropinocytic activity of each cell line: high uptake of compounds was observed in cells with mutations in certain signaling pathways. Significantly, the study shows that constrained peptides follow the same uptake mechanism as proteins in macropinocytic cells, but unlike proteins, peptide mimics can be readily designed to resist denaturation and proteolytic degradation. Our findings expand the current understanding of cellular uptake in cancer cells by designed peptidomimetics and suggest that cancer cells with certain mutations are suitable mediums for the study of biological pathways with peptide leads.

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Year:  2020        PMID: 32786217      PMCID: PMC7755425          DOI: 10.1021/jacs.0c02109

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


  77 in total

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10.  Plasma membrane V-ATPase controls oncogenic RAS-induced macropinocytosis.

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  10 in total

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3.  Landscaping macrocyclic peptides: stapling hDM2-binding peptides for helicity, protein affinity, proteolytic stability and cell uptake.

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5.  A Sos proteomimetic as a pan-Ras inhibitor.

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6.  Unprotected peptide macrocyclization and stapling via a fluorine-thiol displacement reaction.

Authors:  Md Shafiqul Islam; Samuel L Junod; Si Zhang; Zakey Yusuf Buuh; Yifu Guan; Mi Zhao; Kishan H Kaneria; Parmila Kafley; Carson Cohen; Robert Maloney; Zhigang Lyu; Vincent A Voelz; Weidong Yang; Rongsheng E Wang
Journal:  Nat Commun       Date:  2022-01-17       Impact factor: 14.919

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9.  Tuning Electrostatic and Hydrophobic Surfaces of Aromatic Rings to Enhance Membrane Association and Cell Uptake of Peptides.

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Review 10.  Alternative approaches to target Myc for cancer treatment.

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  10 in total

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