Welcome to the new version of CaltechAUTHORS. Login is currently restricted to library staff. If you notice any issues, please email coda@library.caltech.edu
CaltechAUTHORS
Published May 2014 | Supplemental Material + Accepted Version
Journal Article Open

Optimized orthogonal translation of unnatural amino acids enables spontaneous protein double-labelling and FRET

Wang, Kaihang ORCID icon
Sachdeva, Amit
Cox, Daniel J.
Wilf, Nabil M.
Lang, Kathrin
Wallace, Stephen ORCID icon
Mehl, Ryan A.
Chin, Jason W. ORCID icon

Abstract

The ability to introduce different biophysical probes into defined positions in target proteins will provide powerful approaches for interrogating protein structure, function and dynamics. However, methods for site-specifically incorporating multiple distinct unnatural amino acids are hampered by their low efficiency. Here we provide a general solution to this challenge by developing an optimized orthogonal translation system that uses amber and evolved quadruplet-decoding transfer RNAs to encode numerous pairs of distinct unnatural amino acids into a single protein expressed in Escherichia coli with a substantial increase in efficiency over previous methods. We also provide a general strategy for labelling pairs of encoded unnatural amino acids with different probes via rapid and spontaneous reactions under physiological conditions. We demonstrate the utility of our approach by genetically directing the labelling of several pairs of sites in calmodulin with fluorophores and probing protein structure and dynamics by Förster resonance energy transfer.

Additional Information

© 2014 Macmillan Publishers Limited. Received 26 July 2013; Accepted 12 March 2014; Published 20 April 2014. We thank the Medical Research Council (U105181009, UD99999908) and the European Research Council (MC-A024-5PG0A) for financial support. We thank S-P. Chew (MRC-LMB Mass Spectrometry) for obtaining MALDI data. Author Contributions: J.W.C. and K.W. conceived the project. J.W.C., K.W. and A.S. planned and designed experiments and wrote the manuscript, with input from the other authors. R.A.M. provided MjTetPheRS and compound 5 for pilot experiments. All other authors performed experiments or provided reagents. K.W. and A.S. contributed equally to this work. The authors declare no competing financial interests.

Errata

Corrected online 07 January 2014: In the version of this Article originally published, the middle initial of the co-author Nabil M. Wilf was incorrect, and the Acknowledgements section was missing a reference to the European Research Council; the statement should have read: "We thank the Medical Research Council (U105181009, UD99999908) and the European Research Council (MC-A024-PG0A) for financial support. We thank S-P. Chew (MRC-LMB Mass Spectrometry) for obtaining MALDI data." These errors have now been corrected in the online versions of the Article.

Attached Files

Accepted Version - emss-63246.pdf

Supplemental Material - nchem.1919-s1.pdf

Files

nchem.1919-s1.pdf
Files (21.0 MB)
Name Size Download all
md5:fe7b3fbcb80bd2c84f30ad70e77861a9
19.4 MB Preview Download
md5:4d9652159243f8a2f754c41a1991560a
1.6 MB Preview Download

Additional details

Identifiers Related works Funding Dates
Created:
August 20, 2023
Modified:
October 20, 2023