Crystal structure of the Escherichia coli peptide deformylase

被引:127
作者
Chan, MK [1 ]
Gong, WM [1 ]
Rajagopalan, PTR [1 ]
Hao, B [1 ]
Tsai, CM [1 ]
Pei, DH [1 ]
机构
[1] OHIO STATE UNIV,DEPT CHEM,COLUMBUS,OH 43210
来源
BIOCHEMISTRY | 1997年 / 36卷 / 45期
关键词
D O I
10.1021/bi9711543
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Protein synthesis in bacteria involves the formylation and deformylation of the N-terminal methionine. As eukaryotic organisms differ in their protein biosynthetic mechanisms, peptide deformylase, the bacterial enzyme responsible for deformylation, represents a potential target for antibiotic studies. Here we report the crystallization and 2.9 Angstrom X-ray structure solution of the zinc containing Escherichia coli peptide deformylase. While the primary sequence, tertiary structure, and use of coordinated cysteine suggest that E. call deformylase belongs to a new subfamily of metalloproteases, the environment around the metal appears to have strong geometric similarity to the active sites of the thermolysin family, This suggests a possible similarity in their hydrolytic mechanisms. Another important issue is the origin of the enzyme's specificity for N-formylated over N-acetylated substrates. Based on the structure, the specificity appears to result from hydrogen-bonding interactions which orient the substrate for cleavage, and steric factors which physically limit the size of the N-terminal carbonyl group.
引用
收藏
页码:13904 / 13909
页数:6
相关论文
共 35 条
[1]   ON RELEASE OF FORMYL GROUP FROM NASCENT PROTEIN [J].
ADAMS, JM .
JOURNAL OF MOLECULAR BIOLOGY, 1968, 33 (03) :571-&
[2]   METALLOPROTEINASE SUPER-FAMILIES AND DRUG DESIGN [J].
BLUNDELL, TL .
NATURE STRUCTURAL BIOLOGY, 1994, 1 (02) :73-75
[3]   CRYSTALLOGRAPHIC REFINEMENT BY SIMULATED ANNEALING APPLICATION TO A 2.8-A RESOLUTION STRUCTURE OF ASPARTATE-AMINOTRANSFERASE [J].
BRUNGER, AT .
JOURNAL OF MOLECULAR BIOLOGY, 1988, 203 (03) :803-816
[4]   MECHANISM OF CARBOXYPEPTIDASE-A - HYDRATION OF A KETONIC SUBSTRATE-ANALOG [J].
CHRISTIANSON, DW ;
DAVID, PR ;
LIPSCOMB, WN .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (06) :1512-1515
[5]   VERIFICATION OF PROTEIN STRUCTURES - PATTERNS OF NONBONDED ATOMIC INTERACTIONS [J].
COLOVOS, C ;
YEATES, TO .
PROTEIN SCIENCE, 1993, 2 (09) :1511-1519
[6]   WHOLE-GENOME RANDOM SEQUENCING AND ASSEMBLY OF HAEMOPHILUS-INFLUENZAE RD [J].
FLEISCHMANN, RD ;
ADAMS, MD ;
WHITE, O ;
CLAYTON, RA ;
KIRKNESS, EF ;
KERLAVAGE, AR ;
BULT, CJ ;
TOMB, JF ;
DOUGHERTY, BA ;
MERRICK, JM ;
MCKENNEY, K ;
SUTTON, G ;
FITZHUGH, W ;
FIELDS, C ;
GOCAYNE, JD ;
SCOTT, J ;
SHIRLEY, R ;
LIU, LI ;
GLODEK, A ;
KELLEY, JM ;
WEIDMAN, JF ;
PHILLIPS, CA ;
SPRIGGS, T ;
HEDBLOM, E ;
COTTON, MD ;
UTTERBACK, TR ;
HANNA, MC ;
NGUYEN, DT ;
SAUDEK, DM ;
BRANDON, RC ;
FINE, LD ;
FRITCHMAN, JL ;
FUHRMANN, JL ;
GEOGHAGEN, NSM ;
GNEHM, CL ;
MCDONALD, LA ;
SMALL, KV ;
FRASER, CM ;
SMITH, HO ;
VENTER, JC .
SCIENCE, 1995, 269 (5223) :496-512
[7]   THE MINIMAL GENE COMPLEMENT OF MYCOPLASMA-GENITALIUM [J].
FRASER, CM ;
GOCAYNE, JD ;
WHITE, O ;
ADAMS, MD ;
CLAYTON, RA ;
FLEISCHMANN, RD ;
BULT, CJ ;
KERLAVAGE, AR ;
SUTTON, G ;
KELLEY, JM ;
FRITCHMAN, JL ;
WEIDMAN, JF ;
SMALL, KV ;
SANDUSKY, M ;
FUHRMANN, J ;
NGUYEN, D ;
UTTERBACK, TR ;
SAUDEK, DM ;
PHILLIPS, CA ;
MERRICK, JM ;
TOMB, JF ;
DOUGHERTY, BA ;
BOTT, KF ;
HU, PC ;
LUCIER, TS ;
PETERSON, SN ;
SMITH, HO ;
HUTCHISON, CA ;
VENTER, JC .
SCIENCE, 1995, 270 (5235) :397-403
[8]  
FUREY W, 1995, MACROMOLECULAR CRYST
[9]   THE NMR STRUCTURE OF THE INHIBITED CATALYTIC DOMAIN OF HUMAN STROMELYSIN-1 [J].
GOOLEY, PR ;
OCONNELL, JF ;
MARCY, AI ;
CUCA, GC ;
SALOWE, SP ;
BUSH, BL ;
HERMES, JD ;
ESSER, CK ;
HAGMANN, WK ;
SPRINGER, JP ;
JOHNSON, BA .
NATURE STRUCTURAL BIOLOGY, 1994, 1 (02) :111-118
[10]   IMPORTANCE OF FORMYLABILITY AND ANTICODON STEM SEQUENCE TO GIVE A TRANSFER RNA(MET) AN INITIATOR IDENTITY IN ESCHERICHIA-COLI [J].
GUILLON, JM ;
MECHULAM, Y ;
BLANQUET, S ;
FAYAT, G .
JOURNAL OF BACTERIOLOGY, 1993, 175 (14) :4507-4514
1234