4.7 Article

Synthetic design of farnesyl-electrostatic peptides for development of a protein kinase A membrane translocation switch

Journal

SCIENTIFIC REPORTS
Volume 11, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41598-021-95840-8

Keywords

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Funding

  1. National Institute of Health [R01 GM123130]
  2. DARPA [HR0011-16-C-0139]

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The study successfully designed a molecular switch that can rapidly translocate to different cellular locations based on the activity of PKA. By arranging peptide sequences and testing different valence numbers, an efficient peptide switch was identified that exhibited dynamic translocation dependent on PKA activity.
Molecular switches that respond to a biochemical stimulus in cells have proven utility as a foundation for developing molecular sensors and actuators that could be used to address important biological questions. Developing a molecular switch unfortunately remains difficult as it requires elaborate coordination of sensing and actuation mechanisms built into a single molecule. Here, we rationally designed a molecular switch that changes its subcellular localization in response to an intended stimulus such as an activator of protein kinase A (PKA). By arranging the sequence for Kemptide in tandem, we designed a farnesylated peptide whose localization can dramatically change upon phosphorylation by PKA. After testing a different valence number of Kemptide as well as modulating the linker sequence connecting them, we identified an efficient peptide switch that exhibited dynamic translocation between plasma membranes and internal endomembranes in a PKA activity dependent manner. Due to the modular design and small size, our PKA switch can have versatile utility in future studies as a platform for visualizing and perturbing signal transduction pathways, as well as for performing synthetic operations in cells.

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