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  • Endothelial cells  (2)
  • brightness  (1)
  • dynamic programming  (1)
  • 1
    ISSN: 1572-817X
    Keywords: brightness ; efficiency ; electroluminescence ; organic diode
    Source: Springer Online Journal Archives 1860-2000
    Topics: Electrical Engineering, Measurement and Control Technology , Physics
    Notes: Abstract Remarkable improvement in efficiency and electroluminescence (EL) has been observed in an organic EL device, which consists of a hole-transport layer and a luminescent layer. The hole-transport layer is an N,N′-bis(3-methyphenyl)-N,N′-diphenylbenzidine film. The doped emitting layer consists of 8-(quinolinolate)-aluminum as the host and rubrene as the emission dopant. The doped cell with aluminum cathode demonstrated a luminance in excess of 20,000 cd/m2 and an external quantum efficiency of 2.7%, which is about four times and three times, respectively, greater than those of the undoped cell. The EL emission from the device shows spectral narrowing and a shift to higher energy.
    Type of Medium: Electronic Resource
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  • 2
    Electronic Resource
    Electronic Resource
    Springer
    BIT 31 (1991), S. 220-229 
    ISSN: 1572-9125
    Keywords: E.1 ; I.1.2 ; Split tree ; dynamic programming
    Source: Springer Online Journal Archives 1860-2000
    Topics: Mathematics
    Notes: Abstract Split trees are suitable data structures for storing records with different access frequencies. Under assumption that the access frequencies are all distinct, Huang has proposed anO(n 4 logm) time algorithm to construct an (m+1)-way split tree for a set ofn keys. In this paper, we generalize Huang's algorithm to deal with the case of non-distinct access frequencies. The technique used in the generalized algorithm is a generalization of Hesteret al.'s, where the binary case was considered. The generalized algorithm runs inO(n 5 logm) time.
    Type of Medium: Electronic Resource
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  • 3
    ISSN: 1432-1335
    Keywords: Cancer therapy ; Inflammation ; Endothelial cells
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract GBS toxin is a polysaccharide exotoxin produced by group BStreptococcus. This organism causes sepsis and respiratory distress in human neonates (so-called early onset disease). This disease is marked by a strong inflammatory response only in the lung, with pulmonary sequestration of granulocytes and extensive capillary endothelial damage, and occurs only during the first few days after birth. We have found that a similar inflammatory response can be induced by i.v. infusion of picomole quantities of GBS toxin in the developing vasculature of transplanted tumors in mice and can significantly retard the tumor growth. When optimum treatment with GBS toxin was started shortly after tumor implantation, a majority of tumors in the mice regressed and the mice remained tumor-free for over 5 months. Some tumors regressed in mice receiving short-term treatment with GBS toxin, but recurred after the treatment was stopped. Median survival times were extended by all regimens and all doses of GBS toxin tested. No evidence of toxicity to the vasculature of other tissues was observed. GBS toxin is being tested for cancer therapy in humans.
    Type of Medium: Electronic Resource
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  • 4
    ISSN: 1432-1335
    Keywords: Endothelial cells ; Inflammation ; Cancer therapy
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract A group B streptococcus (GBS) isolated from human neonates diagnosed with sepsis and respiratory distress (“early-onset disease”) produces a polysaccharide exotoxin (GBS toxin) that, when infused in sheep, causes lung pathophysiology similar to that seen in humans. Histological studies have demonstrated that GBS toxin induces a strong inflammatory response in the lung, with pulmonary sequestration of granulocytes and extensive capillary endothelial damage. The susceptibility of humans to GBS toxin is age-dependent and limited to about 4 days after birth. It is rarely evident thereafter. This suggests that the binding of GBS toxin to the target endothelium occurs via specific components in the developing lung endothelial cells of the newborn that are later lost. We report here that GBS toxin can also bind to developing endothelium associated with neoplasia and induce an inflammatory response. GBS toxin was shown by immunohistochemistry to bind to capillary endothelium of human large-cell carcinomas. In nude mice bearing human tumor xenografts, intravenously administered GBS toxin caused tumor necrosis and hemorrhagic lesions, and substantially inhibited the rate of growth of the tumors. In BALB/c mice bearing Madison lung tumors, GBS toxin induced an inflammatory response resulting in marked changes in tumor morphology, including vasodilation, endothelial and tumor cell necrosis, invasion of lymphocytes and macrophages, and capillary thrombosis. In these tumor models, no evidence of toxicity to the vasculature of other tissues was observed. The reported pathophysiology of GBS in human neonates, the lack of disease in non-neonates colonized with GBS, and these results suggest that GBS toxin may have potential as a well tolerated agent in cancer therapy of some human tumors.
    Type of Medium: Electronic Resource
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