Stereodivergent Protein Engineering of a Lipase To Access All Possible Stereoisomers of Chiral Esters with Two Stereocenters.


Journal

Journal of the American Chemical Society
ISSN: 1520-5126
Titre abrégé: J Am Chem Soc
Pays: United States
ID NLM: 7503056

Informations de publication

Date de publication:
15 05 2019
Historique:
pubmed: 27 4 2019
medline: 21 8 2020
entrez: 27 4 2019
Statut: ppublish

Résumé

Enzymatic stereodivergent synthesis to access all possible product stereoisomers bearing multiple stereocenters is relatively undeveloped, although enzymes are being increasingly used in both academic and industrial areas. When two stereocenters and thus four stereoisomeric products are involved, obtaining stereodivergent enzyme mutants for individually accessing all four stereoisomers would be ideal. Although significant success has been achieved in directed evolution of enzymes in general, stereodivergent engineering of one enzyme into four highly stereocomplementary variants for obtaining the full complement of stereoisomers bearing multiple stereocenters remains a challenge. Using Candida antarctica lipase B (CALB) as a model, we report the protein engineering of this enzyme into four highly stereocomplementary variants needed for obtaining all four stereoisomers in transesterification reactions between racemic acids and racemic alcohols in organic solvents. By generating and screening less than 25 variants of each isomer, we achieved >90% selectivity for all of the four possible stereoisomers in the model reaction. This difficult feat was accomplished by developing a strategy dubbed "focused rational iterative site-specific mutagenesis" (FRISM) at sites lining the enzyme's binding pocket. The accumulation of single mutations by iterative site-specific mutagenesis using a restricted set of rationally chosen amino acids allows the formation of ultrasmall mutant libraries requiring minimal screening for stereoselectivity. The crystal structure of all stereodivergent CALB variants, flanked by MD simulations, uncovered the source of selectivity.

Identifiants

pubmed: 31023008
doi: 10.1021/jacs.9b02709
doi:

Substances chimiques

Esters 0
Fungal Proteins 0
Lipase EC 3.1.1.3
lipase B, Candida antarctica EC 3.1.1.3

Types de publication

Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

7934-7945

Auteurs

Jian Xu (J)

Department of Chemistry , Zhejiang University , Hangzhou 310027 , PR China.

Yixin Cen (Y)

Department of Chemistry , Zhejiang University , Hangzhou 310027 , PR China.
State Key Laboratory of Bio-organic and Natural Products Chemistry , Shanghai Institute of Organic Chemistry, Chinese Academy of Sciences , Shanghai 200032 , PR China.

Warispreet Singh (W)

School of Chemistry and Chemical Engineering , Queen's University , David Keir Building, Stranmillis Road , Belfast BT9 5AG , Northern Ireland , U.K.

Jiajie Fan (J)

Department of Chemistry , Zhejiang University , Hangzhou 310027 , PR China.

Lian Wu (L)

State Key Laboratory of Bio-organic and Natural Products Chemistry , Shanghai Institute of Organic Chemistry, Chinese Academy of Sciences , Shanghai 200032 , PR China.

Xianfu Lin (X)

Department of Chemistry , Zhejiang University , Hangzhou 310027 , PR China.

Jiahai Zhou (J)

State Key Laboratory of Bio-organic and Natural Products Chemistry , Shanghai Institute of Organic Chemistry, Chinese Academy of Sciences , Shanghai 200032 , PR China.

Meilan Huang (M)

School of Chemistry and Chemical Engineering , Queen's University , David Keir Building, Stranmillis Road , Belfast BT9 5AG , Northern Ireland , U.K.

Manfred T Reetz (MT)

Max-Planck-Institut für Kohlenforschung , Kaiser-Wilhelm-Platz 1 , 45470 Mülheim an der Ruhr , Germany.
Chemistry Department , Philipps-University , Hans-Meerwein-Str. 4 , 35032 Marburg , Germany.

Qi Wu (Q)

Department of Chemistry , Zhejiang University , Hangzhou 310027 , PR China.

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Classifications MeSH