AI Article Synopsis

  • The text discusses the engineering of a new protein called uniRapR, which can change shape in response to a small molecule, allowing for precise regulation.
  • Researchers demonstrated its ability to switch configurations through computer simulations, lab experiments, and live organism studies.
  • UniRapR was used to control Src kinase activity, resulting in observable effects on cell behavior in both HeLa cells and zebrafish, showcasing its potential for studying cellular signaling pathways.

Article Abstract

Design of a regulatable multistate protein is a challenge for protein engineering. Here we design a protein with a unique topology, called uniRapR, whose conformation is controlled by the binding of a small molecule. We confirm switching and control ability of uniRapR in silico, in vitro, and in vivo. As a proof of concept, uniRapR is used as an artificial regulatory domain to control activity of kinases. By activating Src kinase using uniRapR in single cells and whole organism, we observe two unique phenotypes consistent with its role in metastasis. Activation of Src kinase leads to rapid induction of protrusion with polarized spreading in HeLa cells, and morphological changes with loss of cell-cell contacts in the epidermal tissue of zebrafish. The rational creation of uniRapR exemplifies the strength of computational protein design, and offers a powerful means for targeted activation of many pathways to study signaling in living organisms.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3637791PMC
http://dx.doi.org/10.1073/pnas.1218319110DOI Listing

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