Literature DB >> 7256086

Multiple antibiotic resistance in South African strains of Streptococcus pneumoniae: mechanism of resistance to beta-lactam antibiotics.

S Zighelboim, A Tomasz.   

Abstract

Multiply antibiotic-resistant strains of Streptococcus pneumoniae appeared in South Africa in 1977. In these organisms resistance to chloramphenicol is caused by an inducible, drug-inactivating enzyme; however, the basis for resistance to other antibiotics is unknown. Pneumococci with increased resistance to beta-lactam antibiotics do not produce beta-lactamases, a finding indicating the presence of intrinsic resistance to these drugs. One approach to the understanding of the mechanism of this resistance was to study the pattern of penicillin-binding proteins (PBPs) in the South African pneumococci. With the use of highly radioactive penicillin to label PBPs in vivo, it was found that the South African pneumococci have a PBP pattern that differs from that of the sensitive laboratory strain R6 in several respects. Differences include (1) a lack of PBPs la and lb; (2) the presence of a new, faster moving protein (lower molecular weight), named PBP lc; (3) an apparent decrease in the affinity of PBP 2a for [3H]penicillin; and (4) a lack of PBP 2b. Taking advantage of the fact that penicillin resistance is a property acquired in a stepwise process, a series of isogenic and progressively more resistant transformants was constructed. DNA from the resistant South African strain 8249 of S. pneumoniae was used as the donor in a series of transformations for which the recipients were either strain R6 or transformants of organisms with lower levels of resistance. In vivo labeling of the PBPs of these transformants revealed a gradual shift from a pattern similar to that of the sensitive strain (in the transformants of lower resistance) to a pattern resembling that of the highly resistant donor strain (in the transformants of higher resistance) as the level of penicillin resistance increased.

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Year:  1981        PMID: 7256086     DOI: 10.1093/clinids/3.2.267

Source DB:  PubMed          Journal:  Rev Infect Dis        ISSN: 0162-0886


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Authors:  Z Markiewicz; A Tomasz
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Review 4.  World-wide development of antibiotic resistance in pneumococci.

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5.  Dynamic capsule restructuring by the main pneumococcal autolysin LytA in response to the epithelium.

Authors:  Colin C Kietzman; Geli Gao; Beth Mann; Lance Myers; Elaine I Tuomanen
Journal:  Nat Commun       Date:  2016-02-29       Impact factor: 14.919

  5 in total

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