Enzymatic assembly of carbon–carbon bonds via iron-catalysed sp^sup 3^ C–H functionalization

Enzymatic assembly of carbon–carbon bonds via iron-catalysed sp^sup 3^ C–H functionalization

Although abundant in organic molecules, carbon-hydrogen (C-H) bonds are typically considered unreactive and unavailable for chemical manipulation. Recent advances in C-H functionalization technology have begun to transform this logic, while emphasizing the importance of and challenges associated wit...

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Bibliographic Details
Published in:Nature (London) Vol. 565; no. 7737; pp. 67 - 72
Main Authors: Zhang, Ruijie K, Chen, Kai, Huang, Xiongyi, Wohlschlager, Lena, Renata, Hans, Arnold, Frances H
Format: Journal Article
Language:English
Published: London Nature Publishing Group 03-01-2019
Subjects:
Alkylation
Carbon
Catalysis
Catalysts
Chemical bonds
Chemistry
Coding
Cytochrome
Cytochrome P450
Cytochromes P450
Directed evolution
E coli
Enzymes
Evolution
Genetic code
Genetic engineering
Genetic transformation
Haem
Hydrogen
Insertion
Iron
Ligands
Mutagenesis
Mutation
Natural products
Noble metals
Organic chemistry
Proteins
Selectivity
Serine
Substrates
Transition metals
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Summary:Although abundant in organic molecules, carbon-hydrogen (C-H) bonds are typically considered unreactive and unavailable for chemical manipulation. Recent advances in C-H functionalization technology have begun to transform this logic, while emphasizing the importance of and challenges associated with selective alkylation at a sp3 carbon. Here we describe iron-based catalysts for the enantio-, regio- and chemoselective intermolecular alkylation of sp3 C-H bonds through carbene C-H insertion. The catalysts, derived from a cytochrome P450 enzyme in which the native cysteine axial ligand has been substituted for serine (cytochrome P411), are fully genetically encoded and produced in bacteria, where they can be tuned by directed evolution for activity and selectivity. That these proteins activate iron, the most abundant transition metal, to perform this chemistry provides a desirable alternative to noble-metal catalysts, which have dominated the field of C-H functionalization. The laboratory-evolved enzymes functionalize diverse substrates containing benzylic, allylic or а-amino C-H bonds with high turnover and excellent selectivity. Furthermore, they have enabled the development of concise routes to several natural products. The use of the native iron-haem cofactor of these enzymes to mediate sp3 C-H alkylation suggests that diverse haem proteins could serve as potential catalysts for this abiological transformation, and will facilitate the development of new enzymatic C-H functionalization reactions for applications in chemistry and synthetic biology.
ISSN:0028-0836
1476-4687
DOI:10.1038/s41586-018-0808-5