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Phosphoregulated orthogonal signal transduction in mammalian cells.

Nature communications (2020-06-20)
Leo Scheller, Marc Schmollack, Adrian Bertschi, Maysam Mansouri, Pratik Saxena, Martin Fussenegger
ABSTRACT

Orthogonal tools for controlling protein function by post-translational modifications open up new possibilities for protein circuit engineering in synthetic biology. Phosphoregulation is a key mechanism of signal processing in all kingdoms of life, but tools to control the involved processes are very limited. Here, we repurpose components of bacterial two-component systems (TCSs) for chemically induced phosphotransfer in mammalian cells. TCSs are the most abundant multi-component signal-processing units in bacteria, but are not found in the animal kingdom. The presented phosphoregulated orthogonal signal transduction (POST) system uses induced nanobody dimerization to regulate the trans-autophosphorylation activity of engineered histidine kinases. Engineered response regulators use the phosphohistidine residue as a substrate to autophosphorylate an aspartate residue, inducing their own homodimerization. We verify this approach by demonstrating control of gene expression with engineered, dimerization-dependent transcription factors and propose a phosphoregulated relay system of protein dimerization as a basic building block for next-generation protein circuits.

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Sigma-Aldrich
Siero fetale bovino, non-USA origin, sterile-filtered, suitable for cell culture
Sigma-Aldrich
Cell Counting Kit -8, per l′analisi della vitalità cellulare, for quantitation of viable cell number in proliferation and cytotoxicity assays
Sigma-Aldrich
Forskolina, For use in molecular biology applications