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Oxygen therapeutics--current concepts.

机译:氧气疗法-当前概念。

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摘要

PURPOSE: In an effort to develop agents that enhance the oxygen-delivery capability of blood without the risks associated with allogeneic blood transfusions, several products are undergoing development and clinical trials. These oxygen transport agents can be divided into two main groups, perfluorocarbon (PFC) emulsions and modified hemoglobin solutions. SOURCE: Articles from the literature on the development and clinical trials of oxygen therapeutic agents were reviewed. PRINCIPAL FINDING: PFCs are synthetic fluorinated hydrocarbons that increase dissolved oxygen in the fluid phase of the blood without binding the oxygen molecule. They enhance oxygen delivery significantly and may be used to augment the technique of intraoperative autologous donation. Two PFC products have been tested in Phase III clinical trials. Hemoglobin-based oxygen carriers (HBOCs) are either cross-linked or microencapsulated hemoglobin molecules. Modification of the human hemoglobin molecule with intra- and inter-molecular cross-linking eliminates renal toxicity and improves the oxygen dissociation characteristics of the molecule. These modifications are necessary because stroma-free hemoglobin (Hb) does not release oxygen in the physiologic range and dissociates into dimers which can be rapidly filtered by the kidney, leading to renal toxicity. In addition to human Hb, bovine hemoglobin is another source of raw material for HBOC products. Recombinant human Hb has also been produced, using an E. coli expression system, for HBOC manufacturing. Four cross-linked hemoglobin products have been tested in Phase III clinical trials. CONCLUSION: While no product has yet been approved for clinical use, preliminary studies with oxygen therapeutics show promising results, with effective oxygen carrying capacity and acceptable side effect profiles. In the future, the formation of a hybrid product which combines the best features from several of the products currently undergoing development may yield the ideal oxygen therapeutic agent.
机译:目的:为了开发能增强血液的氧气输送能力而又没有同种异体输血相关风险的药物,一些产品正在开发和临床试验中。这些氧气传输剂可分为两大类,全氟化碳(PFC)乳液和改良的血红蛋白溶液。资料来源:综述了有关氧治疗剂的开发和临床试验的文献。主要发现:PFC是合成的氟化烃,可增加血液流体相中的溶解氧而不与氧分子结合。它们显着增强了氧气的输送,可用于增强术中自体捐赠的技术。两种PFC产品已在III期临床试验中进行了测试。基于血红蛋白的氧载体(HBOC)是交联的或微囊化的血红蛋白分子。用分子内和分子间交联修饰人血红蛋白分子消除了肾脏毒性并改善了该分子的氧解离特性。这些修饰是必需的,因为无基质的血红蛋白(Hb)不会在生理范围内释放氧气并分解成二聚体,二聚体可以被肾脏迅速过滤,从而导致肾脏毒性。除人血红蛋白外,牛血红蛋白也是HBOC产品的另一种原料来源。还使用大肠杆菌表达系统生产了重组人Hb,用于HBOC生产。四种交联的血红蛋白产品已在III期临床试验中进行了测试。结论:虽然尚未批准将任何产品用于临床,但氧疗的初步研究显示出令人鼓舞的结果,有效的氧携带能力和可接受的副作用。将来,结合目前正在开发的几种产品的最佳功能的混合产品的形成可能会产生理想的氧气治疗剂。

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