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在高水平β-内酰胺抗性从缓症链球菌转移至肺炎链球菌的过程中获得五种高分子量青霉素结合蛋白变体。

Acquisition of five high-Mr penicillin-binding protein variants during transfer of high-level beta-lactam resistance from Streptococcus mitis to Streptococcus pneumoniae.

作者信息

Hakenbeck R, König A, Kern I, van der Linden M, Keck W, Billot-Klein D, Legrand R, Schoot B, Gutmann L

机构信息

Max-Planck Institut für Molekulare Genetik, Berlin, Germany.

出版信息

J Bacteriol. 1998 Apr;180(7):1831-40. doi: 10.1128/JB.180.7.1831-1840.1998.

Abstract

Penicillin-resistant isolates of Streptococcus pneumoniae generally contain mosaic genes encoding the low-affinity penicillin-binding proteins (PBPs) PBP2x, PBP2b, and PBP1a. We now present evidence that PBP2a and PBP1b also appear to be low-affinity variants and are encoded by distinct alleles in beta-lactam-resistant transformants of S. pneumoniae obtained with chromosomal donor DNA from a Streptococcus mitis isolate. Different lineages of beta-lactam-resistant pneumococcal transformants were analyzed, and transformants with low-affinity variants of all high-molecular-mass PBPs, PBP2x, -2a, -2b, -1a, and -1b, were isolated. The MICs of benzyl-penicillin, oxacillin, and cefotaxime for these transformants were up to 40, 100, and 50 microg/ml, respectively, close to the MICs for the S. mitis donor strain. Recruitment of low-affinity PBPs was accompanied by a decrease in cross-linked muropeptides as revealed by high-performance liquid chromatography of muramidase-digested cell walls, but no qualitative changes in muropeptide chemistry were detected. The growth rates of all transformants were identical to that of the parental S. pneumoniae strain. The results stress the potential for the acquisition by S. pneumoniae of high-level beta-lactam resistance by interspecies gene transfer.

摘要

肺炎链球菌的青霉素耐药菌株通常含有编码低亲和力青霉素结合蛋白(PBPs)PBP2x、PBP2b和PBP1a的嵌合基因。我们现在提供证据表明,PBP2a和PBP1b似乎也是低亲和力变体,并且由从缓症链球菌分离株获得的染色体供体DNA在肺炎链球菌的β-内酰胺耐药转化体中由不同的等位基因编码。分析了β-内酰胺耐药肺炎球菌转化体的不同谱系,并分离出具有所有高分子量PBPs(PBP2x、-2a、-2b、-1a和-1b)低亲和力变体的转化体。这些转化体对苄青霉素、苯唑西林和头孢噻肟的最低抑菌浓度(MIC)分别高达40、100和50μg/ml,接近缓症链球菌供体菌株的MIC。如通过对溶菌酶消化的细胞壁进行高效液相色谱分析所揭示的,低亲和力PBPs的募集伴随着交联的胞壁肽减少,但未检测到胞壁肽化学性质的定性变化。所有转化体的生长速率与亲本肺炎链球菌菌株相同。结果强调了肺炎链球菌通过种间基因转移获得高水平β-内酰胺耐药性的可能性。

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