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Published July 10, 2018 | Published + Supplemental Material
Journal Article Open

Catalytic iron-carbene intermediate revealed in a cytochrome c carbene transferase

Lewis, Russell D. ORCID icon
Garcia-Borràs, Marc ORCID icon
Chalkley, Matthew J. ORCID icon
Buller, Andrew R. ORCID icon
Houk, K. N. ORCID icon
Kan, S. B. Jennifer ORCID icon
Arnold, Frances H. ORCID icon

Abstract

Recently, heme proteins have been discovered and engineered by directed evolution to catalyze chemical transformations that are biochemically unprecedented. Many of these nonnatural enzyme-catalyzed reactions are assumed to proceed through a catalytic iron porphyrin carbene (IPC) intermediate, although this intermediate has never been observed in a protein. Using crystallographic, spectroscopic, and computational methods, we have captured and studied a catalytic IPC intermediate in the active site of an enzyme derived from thermostable Rhodothermus marinus (Rma) cytochrome c. High-resolution crystal structures and computational methods reveal how directed evolution created an active site for carbene transfer in an electron transfer protein and how the laboratory-evolved enzyme achieves perfect carbene transfer stereoselectivity by holding the catalytic IPC in a single orientation. We also discovered that the IPC in Rma cytochrome c has a singlet ground electronic state and that the protein environment uses geometrical constraints and noncovalent interactions to influence different IPC electronic states. This information helps us to understand the impressive reactivity and selectivity of carbene transfer enzymes and offers insights that will guide and inspire future engineering efforts.

Additional Information

© 2018 National Academy of Sciences. Published under the PNAS license. Contributed by Frances H. Arnold, May 31, 2018 (sent for review April 26, 2018; reviewed by Kara L. Bren and Ryan G. Hadt). We thank J. M. Bollinger Jr., K. Chen, X. Huang, C. Krebs, C. J. Pollock, and R. K. Zhang for helpful discussions and A. Tang for experimental assistance. This work was supported by National Science Foundation Division of Chemistry Grant CHE-1361104 (to K.N.H.); the Rothenberg Innovation Initiative (RI2) Program (S.B.J.K. and F.H.A.); the Jacobs Institute for Molecular Engineering for Medicine at Caltech (S.B.J.K. and F.H.A.); National Science Foundation Division of Molecular and Cellular Biosciences Grant MCB-1513007 (to F.H.A.); and Office of Chemical, Bioengineering, Environmental and Transport Systems SusChEM Initiative Grant CBET-1403077 (to F.H.A.). R.D.L. is supported by NIH National Research Service Award Training Grant 5 T32 GM07616. M.G.-B. thanks the Ramón Areces Foundation for a postdoctoral fellowship. M.J.C. thanks the Center for Environmental Microbial Interactions at Caltech for a fellowship. Crystallography experiments were supported by J. Kaiser and the Caltech Molecular Observatory. EPR experiments were performed with the assistance of P. Oyala and supported by National Science Foundation Grant NSF-1531940 (to the Caltech EPR Facility). Computational resources were provided by the University of California, Los Angeles Institute for Digital Research and Education and the Extreme Science and Engineering Discovery Environment, which is supported by National Science Foundation Grant OCI-1053575. R.D.L. and M.G.-B. contributed equally to this work. Author contributions: R.D.L., M.G.-B., K.N.H., S.B.J.K., and F.H.A. designed research; R.D.L., M.G.-B., M.J.C., and S.B.J.K. performed research; R.D.L., M.G.-B., M.J.C., A.R.B., K.N.H., S.B.J.K., and F.H.A. analyzed data; and R.D.L., M.G.-B., K.N.H., S.B.J.K., and F.H.A. wrote the paper. Reviewers: K.L.B., University of Rochester; and R.G.H., Argonne National Laboratory. The authors declare no conflict of interest. Data deposition: The atomic coordinates and structure factors have been deposited in the Protein Data Bank, www.wwpdb.org (PDB ID codes 6CUK and 6CUN). This article contains supporting information online at www.pnas.org/lookup/suppl/doi:10.1073/pnas.1807027115/-/DCSupplemental.

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