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由大肠杆菌脂多糖诱导的小鼠体内血小板的双相、器官特异性和品系特异性积聚及其在休克中的可能作用。

Biphasic, organ-specific, and strain-specific accumulation of platelets induced in mice by a lipopolysaccharide from Escherichia coli and its possible involvement in shock.

作者信息

Shibazaki M, Nakamura M, Endo Y

机构信息

Department of Pharmacology, School of Dentistry, Tohoku University, Sendai, Japan.

出版信息

Infect Immun. 1996 Dec;64(12):5290-4. doi: 10.1128/iai.64.12.5290-5294.1996.

Abstract

Platelets contain a large amount of 5-hydroxytryptamine (5HT, serotonin). Intravenous injection into BALB/c mice of a Boivin's preparation of lipopolysaccharide (LPS) from Escherichia coli induced rapid 5HT accumulation in the lung (within 5 min) and slow 5HT accumulation in the liver (2 to 5 h later). The rapid response required high doses of LPS (more than 0.1 mg/kg). On the basis of 5HT measurements, 70% or more of the platelets which disappeared from the blood appeared to have accumulated rapidly in the lung, and a large number of platelets were found there by electron microscopy. A shock, which was manifested by crawling, convulsion, or prostration, followed shortly after the rapid accumulation of 5HT in the lung. On the other hand, the slow accumulation of 5HT in the liver could be induced by much lower doses of LPS (1 microg/kg or less), even when given by intraperitoneal injection. This 5HT accumulation appears to be a reflection of platelet accumulation in the liver (Y. Endo and M. Nakamura, Br. J. Pharmacol. 105:613-619, 1992). The combination of a low dose of LPS with D-galactosamine amplified the hepatic accumulation of 5HT, and the mice developed a severe hepatic congestion resulting in death. The rapid response was not induced at all in C3H/HeN mice. These results and comparison with other LPS preparations indicate that some component(s) of LPS from E. coli induces a biphasic, organ-specific and strain-specific accumulation of platelets, and it is proposed that this effect is involved in the development of shock.

摘要

血小板含有大量的5-羟色胺(5HT,血清素)。向BALB/c小鼠静脉注射来自大肠杆菌的博伊文脂多糖(LPS)制剂,可诱导肺中5HT迅速积累(5分钟内),肝脏中5HT缓慢积累(2至5小时后)。快速反应需要高剂量的LPS(超过0.1mg/kg)。根据5HT测量结果,从血液中消失的血小板中70%或更多似乎迅速在肺中积累,并且通过电子显微镜在那里发现了大量血小板。在肺中5HT迅速积累后不久,出现了以爬行、抽搐或虚脱为表现的休克。另一方面,即使通过腹腔注射给予低得多剂量的LPS(1μg/kg或更低),也可诱导肝脏中5HT的缓慢积累。这种5HT积累似乎反映了血小板在肝脏中的积累(远藤洋和中村真,《英国药理学杂志》105:613 - 619,1992)。低剂量LPS与D-半乳糖胺的组合增强了肝脏中5HT的积累,并且小鼠出现严重的肝充血导致死亡。在C3H/HeN小鼠中根本不会诱导快速反应。这些结果以及与其他LPS制剂的比较表明,大肠杆菌LPS的某些成分诱导血小板的双相、器官特异性和品系特异性积累,并且有人提出这种作用与休克的发生有关。

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