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细菌对四环素的耐药性:机制、传播及临床意义。

Bacterial resistance to tetracycline: mechanisms, transfer, and clinical significance.

作者信息

Speer B S, Shoemaker N B, Salyers A A

机构信息

Keck Laboratories, California Institute of Technology, Pasadena 91125.

出版信息

Clin Microbiol Rev. 1992 Oct;5(4):387-99. doi: 10.1128/CMR.5.4.387.

Abstract

Tetracycline has been a widely used antibiotic because of its low toxicity and broad spectrum of activity. However, its clinical usefulness has been declining because of the appearance of an increasing number of tetracycline-resistant isolates of clinically important bacteria. Two types of resistance mechanisms predominate: tetracycline efflux and ribosomal protection. A third mechanism of resistance, tetracycline modification, has been identified, but its clinical relevance is still unclear. For some tetracycline resistance genes, expression is regulated. In efflux genes found in gram-negative enteric bacteria, regulation is via a repressor that interacts with tetracycline. Gram-positive efflux genes appear to be regulated by an attenuation mechanism. Recently it was reported that at least one of the ribosome protection genes is regulated by attenuation. Tetracycline resistance genes are often found on transmissible elements. Efflux resistance genes are generally found on plasmids, whereas genes involved in ribosome protection have been found on both plasmids and self-transmissible chromosomal elements (conjugative transposons). One class of conjugative transposon, originally found in streptococci, can transfer itself from streptococci to a variety of recipients, including other gram-positive bacteria, gram-negative bacteria, and mycoplasmas. Another class of conjugative transposons has been found in the Bacteroides group. An unusual feature of the Bacteroides elements is that their transfer is enhanced by preexposure to tetracycline. Thus, tetracycline has the double effect of selecting for recipients that acquire a resistance gene and stimulating transfer of the gene.

摘要

四环素因其低毒性和广谱活性而一直是广泛使用的抗生素。然而,由于临床上重要细菌中越来越多的四环素耐药菌株出现,其临床效用一直在下降。两种耐药机制占主导地位:四环素外排和核糖体保护。已经鉴定出第三种耐药机制,即四环素修饰,但其临床相关性仍不清楚。对于一些四环素耐药基因,其表达是受调控的。在革兰氏阴性肠道细菌中发现的外排基因,其调控是通过与四环素相互作用的阻遏物进行的。革兰氏阳性外排基因似乎是通过衰减机制进行调控的。最近有报道称,至少一种核糖体保护基因是通过衰减进行调控的。四环素耐药基因经常存在于可传递元件上。外排耐药基因通常存在于质粒上,而参与核糖体保护的基因在质粒和自我传递的染色体元件(接合转座子)上均有发现。一类最初在链球菌中发现的接合转座子,可以从链球菌转移到多种受体,包括其他革兰氏阳性菌、革兰氏阴性菌和支原体。另一类接合转座子已在拟杆菌属中发现。拟杆菌属元件的一个不寻常特征是,预先接触四环素会增强它们的转移。因此,四环素具有双重作用,既选择获得耐药基因的受体,又刺激该基因的转移。

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