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Glycolytic and Gluconeogenic Growth of Escherichia coli O157:H7 (EDL933) and E. coli K-12 (MG1655) in the Mouse Intestine

机译:小鼠肠中大肠杆菌O157:H7(EDL933)和大肠杆菌K-12(MG1655)的糖酵解和糖原生长

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摘要

Escherichia coli EDL933, an O157:H7 strain, is known to colonize the streptomycin-treated CD-1 mouse intestine by growing in intestinal mucus (E. A. Wadolkowski, J. A. Burris, and A. D. O'Brien, Infect. Immun. 58:2438-2445, 1990), but what nutrients and metabolic pathways are employed during colonization has not been determined. In this study, when the wild-type EDL933 strain was fed to mice along with an EDL933 ΔppsA ΔpckA mutant, which is unable to utilize tricarboxylic acid cycle intermediates and gluconeogenic substrates for growth, both strains colonized the mouse intestine equally well. Therefore, EDL933 utilizes a glycolytic substrate(s) for both initial growth and maintenance when it is the only E. coli strain fed to the mice. However, in the presence of large numbers of MG1655, a K-12 strain, it is shown that EDL933 utilizes a glycolytic substrate(s) for initial growth in the mouse intestine but appears to utilize both glycolytic and gluconeogenic substrates in an attempt to maintain colonization. It is further shown that MG1655 predominantly utilizes glycolytic substrates for growth in the mouse intestine whether growing in the presence or absence of large numbers of EDL933. Data are presented showing that although small numbers of EDL933 grow to large numbers in the intestine in the presence of large numbers of MG1655 when both strains are fed to mice simultaneously, precolonization with MG1655 affords protection against subsequent colonization by EDL933. Moreover, in mice that are precolonized with EDL933, small numbers of MG1655 are able to grow rapidly in the intestine and EDL933 is eliminated. In situ hybridization experiments using E. coli-specific rRNA probes showed that while MG1655 is found only in mucus, EDL933 is found both in mucus and closely associated with intestinal epithelial cells. The data are discussed with respect to competition for nutrients and to the protection that some intestinal commensal E. coli strains might afford against infection by O157:H7 strains.
机译:已知大肠杆菌EDL933(一种O157:H7菌株)通过在肠粘液中生长而在链霉素处理的CD-1小鼠肠道中定殖(EA Wadolkowski,JA Burris和AD O'Brien,Infect。Immun。58:2438-2445 (1990),但是在定植过程中采用了哪些营养和代谢途径尚未确定。在这项研究中,当将野生型EDL933菌株与无法利用三羧酸循环中间体和糖异生底物生长的EDL933ΔppsAΔpckA突变体一起喂给小鼠时,两种菌株均能很好地定居于小鼠肠道。因此,当EDL933是唯一饲喂给小鼠的大肠杆菌菌株时,它利用糖酵解底物进行初始生长和维持。但是,在大量的MG1655(K-12菌株)存在下,表明EDL933利用糖酵解底物在小鼠肠中进行初始生长,但似乎同时利用糖酵解底物和糖异生底物来维持殖民化。进一步表明,无论在存在或不存在大量EDL933的情况下生长,MG1655主要利用糖酵解底物在小鼠肠中生长。呈现的数据显示,当将两种菌株同时饲喂给小鼠时,尽管在大量MG1655的存在下,少量EDL933在肠中生长到大量,但MG1655的预定殖可提供保护,防止随后的EDL933定植。此外,在用EDL933预定殖的小鼠中,少量MG1655能够在肠中快速生长,并且消除了EDL933。使用大肠杆菌特异性rRNA探针的原位杂交实验表明,虽然仅在粘液中发现了MG1655,但在粘液中发现了EDL933,并与肠上皮细胞紧密相关。讨论了有关营养的竞争以及某些肠道共生大肠杆菌菌株可能提供的针对O157:H7菌株感染的保护作用的数据。

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