Three-dimensional structures of enzymes useful for β-lactam antibiotic production

被引：17

作者：

Barends, TRM ^{[1
]}

Yoshida, H ^{[1
]}

Dijkstra, BW ^{[1
]}

机构：

[1] Univ Groningen, Biophys Chem Lab, NL-9747 AG Groningen, Netherlands

来源：

CURRENT OPINION IN BIOTECHNOLOGY | 2004年 / 15卷 / 04期

关键词：

D O I：

10.1016/j.copbio.2004.06.009

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

Significant advances have been made in the structure-based engineering of enzymes useful for beta-lactam antibiotic production. Structure-based engineering of penicillin G acylase and cephalosporin acylase has resulted in improved enzymes for use in enzymatic production processes. The structures of many other enzymes that could be used in the production of beta-lactam antibiotics, such as enzymes from the beta-lactam biosynthetic pathway and beta-lactam antibiotic-converting enzymes, have been determined. The interest in these structures suggests that the future may see an even more extensive use of rationally engineered biocatalysts in antibiotic production than today.

引用

页码：356 / 363

页数：8

共 27 条

[1] Role of αArg145 and βArg263 in the active site of penicillin acylase of Escherichia coli [J].

Alkema, WBL ;

Prins, AK ;

de Vries, E ;

Janssen, DB .

BIOCHEMICAL JOURNAL, 2002, 365 :303-309

[2] The role of hydrophobic active-site residues in substrate specificity and acyl transfer activity of penicillin acylase [J].

Alkema, WBL ;

Dijkhuis, AJ ;

de Vries, E ;

Janssen, DB .

EUROPEAN JOURNAL OF BIOCHEMISTRY, 2002, 269 (08) :2093-2100

[3] Characterization of the β-lactam binding site of penicillin acylase of Escherichia coli by structural and site-directed mutagenesis studies [J].

Alkema, WBL ;

Hensgens, CMH ;

Kroezinga, EH ;

de Vries, E ;

Floris, R ;

van der Laan, JM ;

Dijkstra, BW ;

Janssen, DB .

PROTEIN ENGINEERING, 2000, 13 (12) :857-863

[4] Towards new β-lactam antibiotics [J].

Andersson, I ;

van Scheltinga, ACT ;

Valegård, K .

CELLULAR AND MOLECULAR LIFE SCIENCES, 2001, 58 (12-13) :1897-1906

[5] Biotechnological applications of penicillin acylases:: state-of-the-art [J].

Arroyo, M ;

de la Mata, I ;

Acebal, C ;

Castillón, MP .

APPLIED MICROBIOLOGY AND BIOTECHNOLOGY, 2003, 60 (05) :507-514

[6] The sequence and crystal structure of the α-amino acid ester hydrolase from Xanthomonas citri define a new family of β-lactam antibiotic acylases [J].

Barends, TRM ;

Polderman-Tijmes, JJ ;

Jekel, PA ;

Hensgens, CMH ;

de Vries, EJ ;

Janssen, DB ;

Dijkstra, BW .

JOURNAL OF BIOLOGICAL CHEMISTRY, 2003, 278 (25) :23076-23084

[7] The reaction cycle of isopenicillin N synthase observed by X-ray diffraction [J].

Burzlaff, NI ;

Rutledge, PJ ;

Clifton, IJ ;

Hensgens, CMH ;

Pickford, M ;

Adlington, RM ;

Roach, PL ;

Baldwin, JE .

NATURE, 1999, 401 (6754) :721-724

[8] Ligand-induced conformational change in penicillin acylase [J].

Done, SH ;

Brannigan, JA ;

Moody, PCE ;

Hubbard, RE .

JOURNAL OF MOLECULAR BIOLOGY, 1998, 284 (02) :463-475

[9] PENICILLIN ACYLASE HAS A SINGLE-AMINO-ACID CATALYTIC CENTER [J].

DUGGLEBY, HJ ;

TOLLEY, SP ;

HILL, CP ;

DODSON, EJ ;

DODSON, G ;

MOODY, PCE .

NATURE, 1995, 373 (6511) :264-268

[10] Structure-based prediction of modifications in glutarylamidase to allow single-step enzymatic production of 7-aminocephalosporanic acid from cephalosporin C [J].

Fritz-Wolf, K ;

Koller, KP ;

Lange, G ;

Liesum, A ;

Sauber, K ;

Schreuder, H ;

Aretz, W ;

Kabsch, W .

PROTEIN SCIENCE, 2002, 11 (01) :92-103

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