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Oxygen infusions (hemoglobin-vesicles and albumin-hemes) based on nano-molecular sciences

机译:基于纳米分子科学的输氧(血红蛋白囊泡和白蛋白hemes)

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摘要

Since the discovery of a red-colored saline solution of a heme derivative that reversibly binds and releases oxygen (1983), significant efforts have been made to realize an oxygen infusion as a red cell substitute based on the sciences of both molecular assembling phenomena and macromolecular metal complexes. The authors have specified that hemoglobin (Hb)-vesicles (HbV) and recombi-nant human serum albumin-hemes (rHSA-heme) would be the best systems that meet the clinical requirements. (A) Hb is rigorously purified from outdated, donated red cells via pasteurization and ultrafiltration, to completely remove blood type antigen and pathogen. The HbV encapsulates thus purified concentrated Hb solution with a phospholipid bimolecular membrane (diameter, 250 nmφ), and its solution properties can be adjusted comparable with blood. Surface modification of HbV with a water-soluble polymer ensures stable dispersion state and storage over a year at 20℃. In vivo tests have clarified the efficacy for extreme hemodilution and resuscitation from hemorrhagic shock, and safety in terms of biodistribution, metabolism in reticuloendothelial system (RES), clinical chemistry, blood coagulation, etc. The HbV does not induce vasoconstriction thus maintains blood flow and tissue oxygenation. (B) rHSA is now manufactured in Japan as a plasma-expander. The rHSA can incorporate eight heme derivatives (axial base substituted hemes) as oxygen binding sites, and the resulting rHSA-heme is a totally synthetic O{sub}2-carrier. Hb binds endothe-lium-derived relaxation factor, NO, and induces vasoconstriction. The rHSA-heme binds NO as Hb does, however, it does not induce vasoconstriction due to its low pI (4.8) and the resulting low permeability across the vascular wall (1/100 of Hb). A 5%-albumin solution possesses a physiologic oncotic pressure. Therefore, to increase the O{sub}2-transporting capacity, albumin dimer is effective. Albumin dimer can incorporate totally 16 hemes with a regulated oncotic pressure. The rHSA-heme is effective not only as a red cell substitute but also for oxygen therapeutics (e.g. oxygenation for tumor). Significant efforts have been made to produce HbV and rHSA-heme with a facility of Good Manufacturing Practice (GMP) standard, and to start preclinical and finally clinical trials.
机译:自从发现可逆结合并释放氧气的血红素衍生物的红色盐溶液(1983年)以来,基于分子组装现象和大分子科学,人们做出了巨大的努力以实现将氧气注入作为红细胞替代物。金属配合物。作者已经指出,血红蛋白(Hb)-囊泡(HbV)和重组人血清白蛋白-hemes(rHSA-血红素)将是满足临床要求的最佳系统。 (A)通过巴氏灭菌和超滤从过时的捐赠红细胞中严格纯化血红蛋白,以完全去除血型抗原和病原体。 HbV用磷脂双分子膜(直径250nmφ)封装纯化后的浓缩Hb溶液,其溶液特性可与血液媲美。用水溶性聚合物对HbV进行表面改性可确保稳定的分散状态,并在20℃一年以上的储存时间。体内试验明确了从出血性休克进行极度血液稀释和复苏的功效,以及在生物分布,网状内皮系统(RES)的代谢,临床化学,血液凝固等方面的安全性。组织氧合。 (B)rHSA现在作为等离子膨胀机在日本生产。该rHSA可以掺入八个血红素衍生物(轴向取代的血红素)作为氧结合位点,并且所得的rHSA-血红素是完全合成的O {sub} 2-载体。血红蛋白结合内皮来源的舒张因子NO,并诱导血管收缩。 rHSA血红素像Hb一样结合NO,但是,由于其低pI(4.8)以及由此产生的穿过血管壁的低通透性(Hb的1/100),它不会引起血管收缩。 5%的白蛋白溶液具有生理渗透压。因此,为了增加O {sub} 2的运输能力,白蛋白二聚体是有效的。白蛋白二聚体可以在调节的血浆渗透压下整合总共16个血红素。 rHSA-血红素不仅作为红细胞替代物有效,而且对于氧疗法(例如肿瘤的氧合)有效。已经做出了巨大努力,以按照良好生产规范(GMP)标准生产HbV和rHSA血红素,并开始了临床前和最终的临床试验。

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