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Cross-Linked Hemoglobin-Albumin Cluster as an Artificial O_2

机译:交联血红蛋白 - 白蛋白簇作为人造O_2

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The decrease in blood donor population by the low birthrate and aging causes serious problem to bring a lack of blood transfusion. Under such social situation, the great current interest in synthesizing red blood cell (RBC) substitutes continues to grow. Hemoglobin (Hb)-based O_2 carriers of several kinds have been extensively developed, such as intramolecularly cross-linked Hb, polymerized Hb, and poly(ethylene- glycol)-conjugated Hb. However, none satisfies all requirements for use as an RBC substitute. A common side effect is mild hypertension resulting from NO scavenging by Hb diffused into extra vascular space. Recently, we have prepared core-shell structured hemoglobin-albumin cluster (Hb-HSA_3) by conjugation of Hb with human serum albumin (HSA) as a new type of artificial O_2 carrier. In this paper, we report for the first time the synthesis and O_2 binding property of more stable and robust protein cluster having intramolecularly cross-linked Hb as a core, ββHb-HSA_3 (Fig. 1). The ββHb-HSA_3 was synthesized by covalent wrapping ββHb with HSA. Initially, ββHb was prepared by cross-linking of two thiol groups in cysteine-93(β_1 and β_2) using 1,11-bis-(maleimido)triethylene glycol. Then, the obtained ββHb was wrapped covalently with HSA by linkage of Hb surface lysines to HSA cysteine-34 via succinimidyl-4-(N-maleimido-methyl)cyclohexane-1-carboxylate. Excess HSA was removed by gel filtration chromatography. HPLC and Native-PAGE measurements of the resultant product revealed that major component of the cluster was ββHb-HSA_3 heterotetramer. The isoelectric point (pI=5.1) was very close to the values of HSA and Hb-HSA_3. The UV-vis. absorption spectral pattern of ββHb-HSA_3 in response to N_2, O_2, CO were fundamentally identical to those of Hb and Hb-HSA_3. The O_2 affinity (P_(50)=6 Torr) was slightly higher than that of Hb-HSA_3. Consequently, ββHb-HSA_3 is expected to be useful as a unique artificial O_2 carrier having a long-term circulation in the bloodstream without subunit dissociation of the core Hb.
机译:由少子献血者人口减少老化造成严重的问题,使缺乏输血。在这样的社会形势,在合成红细胞(RBC)的替代品的大电流的关注持续升温。血红蛋白(Hb)为基础的几种O_2载体已被广泛地开发出来,如分子内交联的血红蛋白,血红蛋白聚合,和聚(乙烯乙二醇)缀合的血红蛋白。然而,没有满足用作替代RBC所有要求。常见的副作用是通过从血红蛋白清除NO产生轻度高血压扩散到血管外空间中。最近,我们制备核 - 壳结构血红蛋白白蛋白簇(HB-HSA_3)通过与人血清白蛋白(HSA)的Hb结合作为一种新型人工O_2载体。在本文中,我们报道首次合成和O_2结合更稳定和稳健的蛋白质性质簇具有分子内交联的血红蛋白作为核心,ββHb-HSA_3(图1)。所述ββHb-HSA_3通过用HSA共价包裹ββHb合成。最初,ββHb物通过交联二个巯基的半胱氨酸-93使用1,11-双 - (马来酰亚胺)(β_1和β_2)三乙二醇制备。然后,将所得ββHb通过经由琥珀酰亚胺基-4-(N-马来酰亚胺基甲基)血红蛋白表面赖氨酸的联动HSA半胱氨酸-34共价HSA包裹环己烷-1-羧酸叔丁酯。过量HSA通过凝胶过滤色谱法除去。所得到的产物的HPLC和Native-PAGE测量显示的集群的该主要部分是ββHb-HSA_3异四聚体。等电点(pI = 5.1)是非常接近的HSA和Hb-HSA_3的值。紫外可见。响应于N_2,O_2,COββHb-HSA_3的吸收光谱图分别为从根本上的那些相同的Hb和Hb-HSA_3的。的O_2亲和力(P_(50)= 6托)比HB-HSA_3的略高。因此,ββHb-HSA_3预计将作为具有在血流长期循环没有芯血红蛋白亚基解离的唯一人工O_2载体是有用的。

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