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首页> 外文期刊>The Journal of laboratory and clinical medicine >The effect of cell-free hemoglobin on intravascular clearance and cellular, plasma, and organ distribution of bacterial endotoxin in rabbits.
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The effect of cell-free hemoglobin on intravascular clearance and cellular, plasma, and organ distribution of bacterial endotoxin in rabbits.

机译:无细胞血红蛋白对兔血管内清除率以及细菌内毒素的细胞,血浆和器官分布的影响。

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摘要

Cell-free hemoglobin (Hb) and bacterial endotoxin (LPS) synergistically produce toxicity. To elucidate possible mechanisms, three groups of rabbits received LPS alone, LPS plus human serum albumin (HSA), or LPS plus Hb (Hb group). The intravascular retention of injected iodine 125-labeled LPS during the 30-minute period analyzed was significantly longer in the Hb group than in the LPS alone or HSA groups (p = 0.0007 and p = 0.03, respectively), especially during the initial 10 minutes. The intravascular half-life of LPS in the LPS control, HSA, and Hb groups was 2.8, 4.0, and 4.9 minutes, respectively; the area under the curve was 1369 +/- 483, 1594 +/- 360, and 1731 +/- 481, respectively (ng/ml x minutes, mean +/- SD); and the total body clearance was 24.7 +/- 9.2, 20.1 +/- 5.4, and 18.9 +/- 6.0 (ml/min, mean +/- SD), respectively. The proportion of LPS associated with blood cells was very small at the initial 1-minute time period, and this decreased even further during the 30-minute period analyzed (p = 0.0001). Over 96% of injected LPS was associated with the cell-free plasma, with 51% to 54% of LPS in the apoprotein fraction at the initial time point and 35% to 37% in the HDL fraction. The proportion of LPS increased significantly in the HDL fraction and decreased significantly in apoproteins during the 30-minute period analyzed (p = 0.0006 and p = 0.002, respectively). However, there were no differences between the three groups. The liver was the main distribution site (74%) of injected LPS among the six organs evaluated. In the Hb group the accumulation of 125I-labeled LPS in the spleen was significantly lower than that in the HSA group (p = 0.05). The synergism of the in vivo toxicity reported for LPS and Hb may be due, in part, to the decreased rate of intravascular clearance of endotoxin.
机译:无细胞血红蛋白(Hb)和细菌内毒素(LPS)协同产生毒性。为了阐明可能的机制,三组兔子单独接受LPS,LPS加人血清白蛋白(HSA)或LPS加Hb(Hb组)。在分析的30分钟内,注射碘125标记的LPS的血管内滞留在Hb组明显长于单独LPS或HSA组(分别为p = 0.0007和p = 0.03),尤其是在最初的10分钟内。 LPS对照组,HSA和Hb组中LPS的血管内半衰期分别为2.8分钟,4.0分钟和4.9分钟。曲线下面积分别为1369 +/- 483、1594 +/- 360和1731 +/- 481(ng / ml x分钟,平均值+/- SD);全身清除率分别为24.7 +/- 9.2、20.1 +/- 5.4和18.9 +/- 6.0(ml / min,平均值+/- SD)。在最初的1分钟时间段内,与血细胞相关的LPS的比例非常小,在所分析的30分钟时间段内,LPS的比例甚至进一步降低(p = 0.0001)。超过96%的注射LPS与无细胞血浆相关,在初始时间点载脂蛋白部分中LPS的比例为51%至54%,HDL部分中的比例为35%至37%。在分析的30分钟内,LPS的比例在HDL分数中显着增加,而在载脂蛋白中则显着下降(分别为p = 0.0006和p = 0.002)。但是,三组之间没有差异。在所评估的六个器官中,肝脏是注射的LPS的主要分布部位(74%)。在Hb组中,脾脏中125I标记的LPS的积累显着低于HSA组(p = 0.05)。对于LPS和Hb报道的体内毒性的协同作用可能部分归因于内毒素在血管内清除率的降低。

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