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Progress in clinical and biological research最新文献

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Unique structural and biological features of Helicobacter pylori lipopolysaccharides. 幽门螺杆菌脂多糖的独特结构和生物学特性。
A P Moran, G O Aspinall
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引用次数: 0
Reconciling the concepts of endotoxin sensitization and tolerance. 调和内毒素致敏和耐受性的概念。
M A Freudenberg, R Salômao, A Sing, I Mitov, C Galanos
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引用次数: 0
The molecular basis for therapeutic concepts utilizing CD14. 利用CD14治疗概念的分子基础。
F Stelter, M Bernheiden, R Menzel, S Witt, R S Jack, U Grunwald, X Fan, C Schütt

The CD14 molecule is a key receptor on myeloid lineage cells involved in the recognition of lipopolysaccharide (LPS) and Gram-negative bacteria. The application of its soluble form, sCD14, has been shown to protect mice from lethality in LPS-induced shock. Therefore the protein or its derivatives may be considered as a possible therapeutic alternative for the treatment of patients suffering from Gram-negative septic shock. In this study we performed an alanine scan of amino acids 1 to 152 of human CD14. Twenty-three substitution mutants were generated and stably transfected into CHO-cells. In each mutant five amino acids were substituted by alanine. We analyzed (a) whether mutant proteins expressed on the surface of transfectants were recognized by a panel of anti-CD14 monoclonal antibodies (mAb's), (b) the ability of mCD14-mutants to bind LPS and E. coli in a serum- or LBP-dependent manner, and (c) the capacity of soluble mutants to mediate the LPS-induced IL 6 release of U 373 astrocytoma cells. Twenty-one CD14-mutants were expressed on the surface of transfectants and 18 were present as soluble forms in the culture supernatants. We demonstrated that only CD14(39-41,43-44)A completely lacked the ability to bind LPS and E. coli. In addition, a combined mutant CD14(9-13/57,59,61-63)A had very limited capacity to interact with LPS indicating that the LPS-binding site of human CD14 is a conformational epitope. Analysis of LPS-induced activation of CD14-negative U 373 cells revealed that the regions 9-13 and 91-101 are most important for sCD14-mediated signalling.

CD14分子是髓系细胞上参与脂多糖(LPS)和革兰氏阴性细菌识别的关键受体。其可溶性形式sCD14的应用已被证明可以保护lps诱导的休克小鼠免于死亡。因此,该蛋白或其衍生物可被认为是治疗革兰氏阴性脓毒性休克患者的一种可能的治疗选择。在这项研究中,我们对人类CD14的氨基酸1至152进行了丙氨酸扫描。产生23个替代突变体,并稳定地转染到cho细胞中。在每个突变体中,有5个氨基酸被丙氨酸取代。我们分析了(a)转染表面表达的突变蛋白是否被一组抗cd14单克隆抗体(mAb’s)识别,(b) mcd14突变体以血清或lbp依赖的方式结合LPS和大肠杆菌的能力,以及(c)可溶性突变体介导LPS诱导的u373星形细胞瘤细胞IL - 6释放的能力。21个cd14突变体在转染物表面表达,18个以可溶性形式存在于培养上清液中。我们证明只有CD14(39-41,43-44)A完全缺乏结合LPS和大肠杆菌的能力。此外,一个组合突变体CD14(9-13/57,59,61-63) a与LPS的相互作用能力非常有限,这表明人类CD14的LPS结合位点是一个构象表位。对lps诱导的cd14阴性u373细胞的活化分析显示,9-13和91-101区域对scd14介导的信号传导最为重要。
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引用次数: 0
Roles of CD14 in LPS signaling and scavenging: analysis of CD14-transgenic and non-transgenic mice and rats in response to LPS. CD14在LPS信号传导和清除中的作用:CD14转基因和非转基因小鼠和大鼠对LPS的反应分析。
S Yamamoto, Y Tamura, Y Higuchi, N Takai, S Akizuki, M Kataoka, K Matsuura
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引用次数: 0
Endotoxin and sepsis: molecular mechanisms of pathogenesis, host resistance, and therapy. Proceedings of the 4th Conference of the International Endotoxin Society. Nagoya, Japan, October 23-27, 1996. 内毒素与败血症:分子机制、发病机制、宿主耐药性和治疗。第四届国际内毒素学会会议论文集。1996年10月23日至27日,日本名古屋。
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引用次数: 0
Prevention of endotoxin shock through targeting leukocyte adhesion molecules. 靶向白细胞粘附分子预防内毒素休克。
H Higashi, N Mukaida, A Harada, S Watanabe, N Ikeda, Y Suzuki, K Matsushima
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引用次数: 0
Role of hepatocytes in the clearance of lipopolysaccharide and its clinical significance. 肝细胞在脂多糖清除中的作用及其临床意义。
K Tanikawa, Y Mimura, S Sakisaka, K Noguchi
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引用次数: 0
Stimulation of human T lymphocytes by lipopolysaccaride (LPS) in the presence of autologous and heterologous monocytes. 在自体和异源单核细胞存在的情况下,脂多糖(LPS)刺激人T淋巴细胞。
T Mattern, H D Flad, A J Ulmer
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引用次数: 0
The CD11/CD18 integrins: characterization of three novel LPS signaling receptors. CD11/CD18整合素:三种新型LPS信号受体的表征。
R R Ingalls, M A Arnaout, R L Delude, S Flaherty, R Savedra, D T Golenbock
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引用次数: 0
Suppression of TNF and other proinflammatory cytokines by the tetravalent guanylhydrazone CNI-1493. 四价鸟酰腙CNI-1493对TNF等促炎细胞因子的抑制作用。
K J Tracey
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引用次数: 0
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Progress in clinical and biological research
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