Genes and spectrum: The theoretical limits

被引：8

作者：

Amyes, SGB ^{[1
]}

机构：

[1] Univ Edinburgh, Sch Med, Dept Med Microbiol, Edinburgh EH8 9AG, Midlothian, Scotland

来源：

CLINICAL INFECTIOUS DISEASES | 1998年 / 27卷

关键词：

D O I：

10.1086/514918

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Antibiotic resistance can result either from mutations within a chromosomal gene or from mobile genes imported from outside. In the last 15 years, some of these mobile genes have shown a propensity to adapt to successive antibiotic challenges, the most versatile being the class A beta-lactamases. The TEM and SHV beta-lactamase nuclei, usually after one initial critical mutation, allow a series of successive mutations that increase the spectrum to hydrolyze most cephalosporins. The class C beta-lactamases also show some versatility; while it migrates from the chromosome, subtle changes can occur in the gene to broaden the spectrum. Trimethoprim resistance has shown less adaptability in gram-negative bacteria, but in gram-positive organisms the plasmid has captured the chromosomal dihydrofolate reductase of Staphylococcus epidermidis, and a minimal number of changes have occurred that decrease the binding of trimethroprim. Other resistance mechanisms appear less adaptable, relying rather on the importation of new genes to cope with new challenges.

引用

页码：S21 / S28

页数：8

共 63 条

[1] PREVALENCE OF TRIMETHOPRIM-RESISTANT DIHYDROFOLATE-REDUCTASE GENES IDENTIFIED WITH OLIGONUCLEOTIDE PROBES IN PLASMIDS FROM ISOLATES OF COMMENSAL FECAL FLORA
ADRIAN, PV
KLUGMAN, KP
AMYES, SGB
[J]. JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY, 1995, 35 (04) : 497 - 508
[2] PREVALENCE AND GENETIC LOCATION OF NONTRANSFERABLE TRIMETHOPRIM-RESISTANT DIHYDROFOLATE-REDUCTASE GENES IN SOUTH-AFRICAN COMMENSAL FECAL ISOLATES
ADRIAN, PV
THOMSON, CJ
KLUGMAN, KP
AMYES, SGB
[J]. EPIDEMIOLOGY AND INFECTION, 1995, 115 (02) : 255 - 267
[3] AMYES SG, 1997, MOL GENETICS DRUG RE, P1
[4] R-FACTOR TRIMETHOPRIM RESISTANCE MECHANISM - INSUSCEPTIBLE TARGET SITE
AMYES, SGB
SMITH, JT
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1974, 58 (02) : 412 - 418
[5] NOVEL DIHYDROFOLATE REDUCTASES ISOLATED FROM EPIDEMIC STRAINS OF TRIMETHOPRIM SULFAMETHOXAZOLE-RESISTANT SHIGELLA-SONNEI
BARG, NL
HUTSON, FS
WHEELER, LA
THOMSON, CJ
AMYES, SGB
WHARTON, M
SCHAFFNER, W
[J]. JOURNAL OF INFECTIOUS DISEASES, 1990, 162 (02) : 466 - 473
[6] SEQUENCE IDENTITY WITH TYPE-VIII AND ASSOCIATION WITH IS176 OF TYPE-IIIC DIHYDROFOLATE-REDUCTASE FROM SHIGELLA-SONNEI
BARG, NL
REGISTER, S
THOMSON, C
AMYES, S
[J]. ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1995, 39 (01) : 112 - 116
[7] Characterization of the plasmidic beta-lactamase CMY-2, which is responsible for cephamycin resistance
Bauernfeind, A
Stemplinger, I
Jungwirth, R
Giamarellou, H
[J]. ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1996, 40 (01) : 221 - 224
[8] SPREAD OF KLEBSIELLA-PNEUMONIAE PRODUCING SHV-5 BETA-LACTAMASE AMONG HOSPITALIZED-PATIENTS
BAUERNFEIND, A
ROSENTHAL, E
EBERLEIN, E
HOLLEY, M
SCHWEIGHART, S
[J]. INFECTION, 1993, 21 (01) : 18 - 22
[9] Sequences of p-lactamase genes encoding CTX-M-1 (MEN-1) and CTX-M-2 and relationship of their amino acid sequences with those of other beta-lactamases
Bauernfeind, A
Stemplinger, I
Jungwirth, R
Ernst, S
Casellas, JM
[J]. ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1996, 40 (02) : 509 - 513
[10] BERG DE, 1989, GENE TRANSFER ENV, P99

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