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首页> 外文期刊>International journal of medical microbiology: IJMM >The host response to endotoxin, antilipopolysaccharide strategies, and the management of severe sepsis
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The host response to endotoxin, antilipopolysaccharide strategies, and the management of severe sepsis

机译:宿主对内毒素的反应,抗脂多糖策略以及严重脓毒症的治疗

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摘要

Endotoxin, more accurately referred to as lipopolysaccharide (LPS), is recognized as the most potent microbial mediator implicated in the pathogenesis of sepsis and septic shock. Despite its discovery over one century ago, the fundamental role of endotoxin in most patients with septic shock remains enigmatic and its value as a target for therapeutic intervention continues to be a contentious clinical issue. LPS is viewed by the host as an alarm molecule indicating microbial invasion by gram-negative bacterial pathogens. The release of large quantities of LPS into the bloodstream is clearly deleterious to the host, and this event can precipitate the induction of a potentially lethal array of inflammatory mediators and procoagulant factors. The host response to highly purified LPS can create diffuse endothelial injury, tissue hypo-perfusion, disseminated intravascular coagulation, and refractory shock. Numerous attempts to block endotoxin activity in clinical trials with septic patients have met with inconsistent and largely negative results. The tremendous knowledge gained within the past decade into the precise molecular basis for LPS-mediated cellular activation and tissue injury has generated a new generation of therapies that specifically disrupt LPS signaling. This information should provide the necessary insights to specifically target anti-LPS interventions in the ongoing effort to improve the management of sepsis. (c) 2007 Elsevier GmbH. All rights reserved.
机译:内毒素,更准确地称为脂多糖(LPS),被认为是与脓毒症和败血性休克的发病机理有关的最有效的微生物介体。尽管在一个多世纪以前就发现了内毒素,但它在大多数脓毒性休克患者中的基本作用仍然是个谜,它作为治疗干预目标的价值仍然是一个有争议的临床问题。宿主将LPS视为一个警报分子,表明微生物被革兰氏阴性细菌病原体入侵。大量LPS向血液中的释放显然对宿主有害,并且此事件可能促使诱发一系列潜在的致死性炎症介质和促凝血因子。宿主对高度纯化的LPS的反应可引起弥漫性内皮损伤,组织灌注不足,弥散性血管内凝血和难治性休克。在败血病患者的临床试验中,许多阻止内毒素活性的尝试均出现了不一致且很大程度上为阴性的结果。在过去十年中,获得了有关LPS介导的细胞活化和组织损伤的精确分子基础的丰富知识,产生了新一代的治疗方法,可特异性破坏LPS信号传导。该信息应提供必要的见识,以在不断努力改善败血症的治疗中专门针对抗LPS干预措施。 (c)2007 Elsevier GmbH。版权所有。

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