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首页> 外文期刊>Medicinal chemistry >Hemoglobin enhances the biological activity of synthetic and natural bacterial (endotoxic) virulence factors: a general principle.
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Hemoglobin enhances the biological activity of synthetic and natural bacterial (endotoxic) virulence factors: a general principle.

机译:血红蛋白增强合成和天然细菌(内毒素)毒力因子的生物活性:一般原理。

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Although hemoglobin (Hb) is mainly present in the cytoplasm of erythrocytes (red blood cells), lower concentrations of pure, cell-free Hb are released permanently into the circulation due to an inherent intravascular hemolytic disruption of erythrocytes. Previously it was shown that the interaction of Hb with bacterial endotoxins (lipopolysaccharides, LPS) results in a significant increase of the biological activity of LPS. There is clear evidence that the enhancement of the biological activity of LPS by Hb is connected with a disaggregation of LPS. From these findings one questions whether the property to enhance the biological activity of endotoxin, in most cases proven by the ability to increase the cytokine (tumor-necrosis-factor-alpha, interleukins) production in human mononuclear cells, is restricted to bacterial endotoxin or is a more general principle in nature. To elucidate this question, we investigated the interaction of various synthetic and natural virulence (pathogenicity) factors with hemoglobin of human or sheep origin. In addition to enterobacterial R-type LPS a synthetic bacterial lipopeptide and synthetic phospholipid-like structures mimicking the lipid A portion of LPS were analysed. Furthermore, we also tested endotoxically inactive LPS and lipid A compounds such as those from Chlamydia trachomatis. We found that the observations made for endotoxically active form of LPS can be generalized for the other synthetic and natural virulence factors: In every case, the cytokine-production induced by them is increased by the addition of Hb. This biological property of Hb is connected with its physical property to convert the aggregate structures of the virulence factors into one with cubic symmetry, accompanied with a considerable reduction of the size and number of the original aggregates.
机译:尽管血红蛋白(Hb)主要存在于红细胞(红细胞)的细胞质中,但由于内在的红细胞血管内溶血性破坏,较低浓度的纯净,无细胞的Hb会永久释放到循环系统中。先前已证明Hb与细菌内毒素(脂多糖,LPS)的相互作用导致LPS的生物学活性显着增加。有明确的证据表明,Hb增强LPS的生物学活性与LPS的分解有关。从这些发现中,有人质疑增强内毒素生物学活性的特性是否在大多数情况下被细菌内毒素所限制,该能力在增加人类单核细胞中细胞因子(肿瘤坏死因子-α,白介素)产生的能力上得到了证明。本质上是更普遍的原则。为了阐明这个问题,我们研究了各种合成和自然毒力(致病性)因子与人或绵羊血红蛋白的相互作用。除了肠细菌R型LPS,还分析了合成细菌脂肽和模仿LPS脂质A部分的合成磷脂样结构。此外,我们还测试了内毒素灭活的LPS和脂质A化合物,例如来自沙眼衣原体的化合物。我们发现,针对内毒素活性形式的LPS的观察结果可以推广到其他合成和自然毒力因子:在每种情况下,通过添加Hb可以增加由它们诱导的细胞因子产生。血红蛋白的这种生物学特性与其物理特性有关,可将毒力因子的聚集体结构转化为立方对称结构,同时大大减少了原始聚集体的大小和数量。

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