首页> 外文期刊>Pharmaceutical research >Recombinant human serum albumin dimer has high blood circulation activity and low vascular permeability in comparison with native human serum albumin.
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Recombinant human serum albumin dimer has high blood circulation activity and low vascular permeability in comparison with native human serum albumin.

机译:与天然人血清白蛋白相比,重组人血清白蛋白二聚体具有高血液循环活性和低血管通透性。

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PURPOSE: Human serum albumin (HSA) is used clinically as an important plasma expander. Albumin infusion is not recommended for critically ill patients with hypovolemia, burns, or hypoalbuminemia because of the increased leakage of albumin into the extravascular spaces, thereby worsening edema. In the present study, we attempted to overcome this problem by producing a recombinant HSA (rHSA) dimer with decreased vascular permeability and an increased half-life. METHODS: Two molecules of rHSA were genetically fused to produce a recombinant albumin dimer molecule. The pharmacokinetics and biodistribution of the recombinant proteins were evaluated in normal rats and carrageenin-induced paw edema mouse model. RESULTS: The conformational properties of this rHSA dimer were similar to those for the native HSA (the HSA monomer), as evidenced by the Western blot and spectroscopic studies. The biological half-life and area under the plasma concentration-time curve of the rHSA dimer were approximately 1.5 times greater than those of the monomer. Dimerization has also caused a significant decrease in the total body clearance and distribution volume at the steady state of the native HSA. rHSA dimer accumulated to a lesser extent in the liver, skin, muscle, and fat, as compared with the native HSA. Up to 96 h, the vascular permeability of the rHSA dimer was less than that of the native HSA in paw edema mouse models. A prolonged plasma half-life of the rHSA dimer was also observed in the edema model rats. CONCLUSIONS: rHSA dimer has a high retention rate in circulating blood and a lower vascular permeability than that of the native HSA.
机译:目的:人血清白蛋白(HSA)在临床上被用作重要的血浆扩张剂。对于血容量不足,烧伤或低白蛋白血症的重症患者,不建议输注白蛋白,因为白蛋白渗入血管外腔的机会增加,从而使水肿恶化。在本研究中,我们试图通过生产具有降低的血管通透性和延长的半衰期的重组HSA(rHSA)二聚体来克服这一问题。方法:将两个rHSA分子遗传融合以产生重组白蛋白二聚体分子。在正常大鼠和角叉菜胶诱导的爪水肿小鼠模型中评估了重组蛋白的药代动力学和生物分布。结果:该rHSA二聚体的构象性质与天然HSA(HSA单体)的构象性质相似,这已通过蛋白质印迹和光谱研究证明。 rHSA二聚体的血浆浓度-时间曲线下的生物半衰期和面积约为单体的1.5倍。二聚化还导致天然HSA稳态时的总体清除率和分布体积显着下降。与天然HSA相比,rHSA二聚体在肝脏,皮肤,肌肉和脂肪中的积累程度较低。长达96小时,在爪水肿小鼠模型中,rHSA二聚体的血管通透性低于天然HSA。在水肿模型大鼠中还观察到rHSA二聚体的血浆半衰期延长。结论:rHSA二聚体与天然HSA相比,在血液中的保留率高,血管通透性低。

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