IMPORTANCE OF THE HIS-298 RESIDUE IN THE CATALYTIC MECHANISM OF THE STREPTOMYCES R61 EXTRACELLULAR DD-PEPTIDASE

被引：21

作者：

HADONOU, AM ^{[1
]}

JAMIN, M ^{[1
]}

ADAM, M ^{[1
]}

JORIS, B ^{[1
]}

DUSART, J ^{[1
]}

GHUYSEN, JM ^{[1
]}

FRERE, JM ^{[1
]}

机构：

[1] STATE UNIV LIEGE,INST CHIM,CTR INGN PROT,B6,B-4000 SART,BELGIUM

来源：

BIOCHEMICAL JOURNAL | 1992年 / 282卷

关键词：

D O I：

10.1042/bj2820495

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：

Among the active-site-serine penicillin-recognizing proteins, the Streptomyces R61 extracellular DD-peptidase is the only one to have a His-Thr-Gly sequence [instead of Lys-Thr(Ser)-Gly] in 'box' VII. The His residue was replaced by Gln or Lys. Both mutations induced a marked decrease in the rates of both tripeptide substrate hydrolysis and acylation by benzylpenicillin and cephalosporin C. The rate of hydrolysis of the thioester hippuryl thioglycollate was less affected. The most striking result was the disproportionate loss of transpeptidation properties by both mutants, indicating an important role of His-298 in this reaction. We believe that this result represents the first modification of a DD-peptidase leading to a specific decrease of the transpeptidation-to-hydrolysis ratio.

引用

页码：495 / 500

页数：6

共 26 条

[1] CHROMOGENIC DEPSIPEPTIDE SUBSTRATES FOR BETA-LACTAMASES AND PENICILLIN-SENSITIVE DD-PEPTIDASES
ADAM, M
DAMBLON, C
PLAITIN, B
CHRISTIAENS, L
FRERE, JM
[J]. BIOCHEMICAL JOURNAL, 1990, 270 (02) : 525 - 529
[2] THE MUTATION LYS234HIS YIELDS A CLASS-A BETA-LACTAMASE WITH A NOVEL PH-DEPENDENCE
BRANNIGAN, J
MATAGNE, A
JACOB, F
DAMBLON, C
JORIS, B
KLEIN, D
SPRATT, BG
FRERE, JM
[J]. BIOCHEMICAL JOURNAL, 1991, 278 : 673 - 678
[3] AUTOMATED-ANALYSIS OF ENZYME INACTIVATION PHENOMENA - APPLICATION TO BETA-LACTAMASES AND DD-PEPTIDASES
DEMEESTER, F
JORIS, B
RECKINGER, G
BELLEFROIDBOURGUIGNON, C
FRERE, JM
WALEY, SG
[J]. BIOCHEMICAL PHARMACOLOGY, 1987, 36 (14) : 2393 - 2403
[4] THE CRYSTAL-STRUCTURE OF THE BETA-LACTAMASE OF STREPTOMYCES-ALBUS G AT 0.3 NM RESOLUTION
DIDEBERG, O
CHARLIER, P
WERY, JP
DEHOTTAY, P
DUSART, J
ERPICUM, T
FRERE, JM
GHUYSEN, JM
[J]. BIOCHEMICAL JOURNAL, 1987, 245 (03) : 911 - 913
[5] PRIMARY STRUCTURE OF THE STREPTOMYCES R61 EXTRACELLULAR DD-PEPTIDASE .1. CLONING INTO STREPTOMYCES-LIVIDANS AND NUCLEOTIDE-SEQUENCE OF THE GENE
DUEZ, C
PIRONFRAIPONT, C
JORIS, B
DUSART, J
URDEA, MS
MARTIAL, JA
FRERE, JM
GHUYSEN, JM
[J]. EUROPEAN JOURNAL OF BIOCHEMISTRY, 1987, 162 (03): : 509 - 518
[6] ENZYME-PRODUCTION BY GENETICALLY ENGINEERED STREPTOMYCES STRAINS - INFLUENCE OF CULTURE CONDITIONS
ERPICUM, T
GRANIER, B
DELCOUR, M
LENZINI, VM
NGUYENDISTECHE, M
DUSART, J
FRERE, JM
[J]. BIOTECHNOLOGY AND BIOENGINEERING, 1990, 35 (07) : 719 - 726
[7] LARGE-SCALE PREPARATION OF PURIFIED EXOCELLULAR DD-CARBOXYPEPTIDASE-TRANSPEPTIDASE OF STREPTOMYCES STRAIN-R61
FOSSATI, P
SAINTGHISLAIN, M
SICARD, PJ
FRERE, JM
DUSART, J
KLEIN, D
GHUYSEN, JM
[J]. BIOTECHNOLOGY AND BIOENGINEERING, 1978, 20 (04) : 577 - 587
[8] Frere J M, 1976, Methods Enzymol, V45, P610
[9] DIRECTION OF PEPTIDE TRIMER SYNTHESIS FROM DONOR-ACCEPTOR SUBSTRATE NALPHA-(ACETYL)-NEPSILON-(GLYCYL)-L-LYSYL-D-ALANYL-D-ALANINE BY EXOCELLULAR DD-CARBOXYPEPTIDASE-TRANSPEPTIDASE OF STREPTOMYCES-R61
FRERE, JM
GHUYSEN, JM
ZEIGER, AR
PERKINS, HR
[J]. FEBS LETTERS, 1976, 63 (01) : 112 - 116
[10] FRERE JM, 1985, CRC CR REV MICROBIOL, V11, P299

← 1 2 3 →