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  • Other Sources  (3)
  • 1990-1994  (3)
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  • 1
    Publication Date: 2019-07-13
    Description: We recently described a Tn551 insertion in the chromosome of Staphylococcus aureus S6C that resulted in drastically reduced expression of extracellular lipase (M. S. Smeltzer, S. R. Gill, and J. J. Iandolo, J. Bacteriol. 174:4000-4006, 1992). The insertion was localized to a chromosomal site (designated omega 1058) distinct from the lipase structural gene (geh) and the accessory gene regulator (agr), both of which were structurally intact in the lipase-negative (Lip-) mutants. In this report, we describe a phenotypic comparison between strains S6C, a hyperproducer of enterotoxin B; KSI9051, a derivative of S6C carrying the Tn551 insertion at omega 1058; ISP546, an 8325-4 strain that carries a Tn551 insertion in the agr locus; and ISP479C, the parent strain of ISP546 cured of the Tn551 delivery plasmid pI258repA36. Compared with their respective parent strains, ISP546 and KSI9051 produced greatly reduced amounts of lipase, alpha-toxin, delta-toxin, protease, and nuclease. KSI9051 also produced reduced amounts of staphylococcal enterotoxin B. Coagulase production was increased in ISP546 but not in KSI9051. Using a mouse model, we also demonstrated that ISP546 and KSI9051 were far less virulent than ISP479C and S6C. We have designated the genetic element defined by the Tn551 insertion at omega 1058 xpr to denote its role as a regulator of extracellular protein synthesis. We conclude that xpr and agr are similar and possibly interactive regulatory genes that play an important role in pathogenesis of staphylococcal disease.
    Keywords: Life Sciences (General)
    Type: Infection and immunity (ISSN 0019-9567); 61; 3; 919-25
    Format: text
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  • 2
    Publication Date: 2019-07-13
    Description: We report results from an adaptive optics system designed to provide imaging at the diffraction limit of resolution in the near-infrared at the Multiple Mirror Telescope (MMT). For the present experiment, the aperture consisted of five of the six primary mirrors of the MMT, operating as a coherently phased array. The largest components of the atmospherically induced wave-front aberration are the fluctuations in mean phase between the segments. These errors were derived in real time from the Fourier transform of short-exposure stellar images at 2.2 microns and corrected at an image of the telescope pupil with piston motion from a segmented adaptive mirror. At a correction rate of 43 Hz, this level of adaptive control resulted in an integrated image with a clear diffraction-limited component of 0.075 arcsec FWHM. This stabilized component is present directly in the light arriving at the detector and is not the result of postprocessing. We discuss future improvements to our adaptive wave-front control and its application to astronomical observations.
    Keywords: ASTRONOMY
    Type: Astrophysical Journal, Part 2 - Letters (ISSN 0004-637X); 402; 2; p. L81-L84.
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  • 3
    Publication Date: 2019-07-13
    Description: Staphylococcal enterotoxin A (SEA) is significantly better than enterotoxin B (SEB) in activating tumor necrosis factor (TNF) secretion by B6MP102 cells. Both toxins bound to B6MP102 cells; however, SEB competed less effectively with SEA than SEA competed with SEB. This suggested that receptors unique to SEA were present on B6MP102 cells. Signal transduction occurred in response to both toxins. Within 30 s after addition, SEA and SEB significantly increased the F-actin concentration in B6MP102 cells. However, only SEA induced increased TNF mRNA levels. B6MP102 cells incubated with interferon-gamma and SEB secreted TNF. However, enhanced mRNA expression was delayed and the concentration of TNF secreted was less than that of B6MP102 cells stimulated with SEA. Although these data suggest that receptors unique to SEA are present on B6MP102 cells, they also indicate that staphylococcal enterotoxins differentially regulate TNF at the RNA level, perhaps because of differences in binding to the plasma membrane.
    Keywords: Life Sciences (General)
    Type: Journal of leukocyte biology (ISSN 0741-5400); 55; 4; 523-9
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