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脂多糖的临床检测与内毒素血症动物模型

Clinical detection of LPS and animal models of endotoxemia.

作者信息

Redl H, Bahrami S, Schlag G, Traber D L

机构信息

Ludwig Boltzmann Institute for Experimental and Clinical Traumatology, Vienna, Austria.

出版信息

Immunobiology. 1993 Apr;187(3-5):330-45. doi: 10.1016/S0171-2985(11)80348-7.

Abstract

The interest in the study of endotoxemia in the clinical area has increased recently as a result of a) improved and simplified endotoxin determination e.g. chromogenic-kinetic microplate methods (also an improved blood sampling tool is available), b) incidence of sepsis has increased due to improvement in early (e.g. posttraumatic) survival, c) interest in and good evidence for gut translocation as a source of endotoxemia, d) agents have developed, which can antagonize endotoxins. There is evidence that patients with positive endotoxin test in the ICU have a higher incidence of organ failure. To study the pathophysiological consequences of endotoxemia and possible ways of intervention animal models are necessary. The choice of the experimental setting depends on the aim of the study e.g. whether prolonged observation is necessary in survival studies or whether hemodynamic variables have to be measured or whether therapeutic agents only crossreact with primates. Since LPS levels are quite low in clinical studies, an important factor for selection of a relevant animal might be LPS sensitivity, or the use of additional sensitization techniques e.g. galactosamine. Another important aspect in this context is whether LPS is given as bolus or infused up to several days. In this review the dose, time, and route of LPS administration is also discussed. For screening purposes rodents are usually used, or sometimes rabbits due to their higher LPS sensitivity. Another very sensitive animal model is the sheep, which can be chronically instrumented and as a specialty allows lung lymph drainage and thus studies of LPS effects on pulmonary permeability. Pigs are used for hemodynamic studies and often in therapeutical studies if species-specificity of the drug tested is not important, in cases where a large animal is necessary. Finally the non-human primates offer a number of advantages due to human-like physiology, due to the cross-reactivity of human assay systems and accordingly also cross-reactivity of human therapeutic agents. While the chimpanzee also shares the LPS sensitivity of humans, baboons are insensitive like rodents. Thus each model serves to provide some useful purpose and the selection must be made to meet the requirements of the specific questions to be asked, with special emphasis of the chosen endotoxin model on relevance for the human sepsis state.

摘要

近年来,临床领域对内毒素血症研究的兴趣有所增加,原因如下:a) 内毒素测定方法得到改进和简化,例如发色动力学微孔板法(同时也有改进的采血工具);b) 由于早期(如创伤后)生存率的提高,脓毒症的发病率有所上升;c) 肠道细菌易位作为内毒素血症的一个来源受到关注且有充分证据;d) 已研发出可拮抗内毒素的药物。有证据表明,重症监护病房(ICU)内毒素检测呈阳性的患者器官衰竭的发生率更高。为研究内毒素血症的病理生理后果及可能的干预方法,动物模型是必要的。实验设置的选择取决于研究目的,例如在生存研究中是否需要长时间观察,或者是否必须测量血流动力学变量,又或者治疗药物是否仅与灵长类动物有交叉反应。由于临床研究中脂多糖(LPS)水平相当低,选择相关动物的一个重要因素可能是LPS敏感性,或者使用额外的致敏技术,如半乳糖胺。在此背景下的另一个重要方面是LPS是以推注方式给药还是持续输注数天。在本综述中,还讨论了LPS给药的剂量、时间和途径。出于筛选目的,通常使用啮齿动物,有时也使用兔子,因为它们对LPS更敏感。另一个非常敏感的动物模型是绵羊,它可以进行长期仪器植入,其特点是能够进行肺淋巴引流,从而研究LPS对肺通透性的影响。猪用于血流动力学研究,如果所测试药物的种属特异性不重要且需要大型动物时,猪也常用于治疗研究。最后,由于具有类似人类的生理学特性、人类检测系统的交叉反应性以及相应的人类治疗药物的交叉反应性,非人灵长类动物具有许多优势。虽然黑猩猩也具有与人类相似的LPS敏感性,但狒狒像啮齿动物一样不敏感。因此,每个模型都有其有用之处,必须根据要提出的具体问题的要求进行选择,特别强调所选内毒素模型与人类脓毒症状态的相关性。

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