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人工肺中固定在纤维膜上的碳酸酐酶与二氧化碳交换的动力学。

Kinetics of CO2 exchange with carbonic anhydrase immobilized on fiber membranes in artificial lungs.

作者信息

Arazawa D T, Kimmel J D, Federspiel W J

机构信息

McGowan Institute for Regenerative Medicine, University of Pittsburgh, 3025 East Carson Street, Pittsburgh, PA, 15203, USA.

出版信息

J Mater Sci Mater Med. 2015 Jun;26(6):193. doi: 10.1007/s10856-015-5525-0. Epub 2015 Jun 2.

Abstract

Artificial lung devices comprised of hollow fiber membranes (HFMs) coated with the enzyme carbonic anhydrase (CA), accelerate removal of carbon dioxide (CO2) from blood for the treatment of acute respiratory failure. While previous work demonstrated CA coatings increase HFM CO2 removal by 115 % in phosphate buffered saline (PBS), testing in blood revealed a 36 % increase compared to unmodified HFMs. In this work, we sought to characterize the CO2 mass transport processes within these biocatalytic devices which impede CA coating efficacy and develop approaches towards improving bioactive HFM efficiency. Aminated HFMs were sequentially reacted with glutaraldehyde (GA), chitosan, GA and afterwards incubated with a CA solution, covalently linking CA to the surface. Bioactive CA-HFMs were potted in model gas exchange devices (0.0119 m(2)) and tested for esterase activity and CO2 removal under various flow rates with PBS, whole blood, and solutions containing individual blood components (plasma albumin, red blood cells or free carbonic anhydrase). Results demonstrated that increasing the immobilized enzyme activity did not significantly impact CO2 removal rate, as the diffusional resistance from the liquid boundary layer is the primary impediment to CO2 transport by both unmodified and bioactive HFMs under clinically relevant conditions. Furthermore, endogenous CA within red blood cells competes with HFM immobilized CA to increase CO2 removal. Based on our findings, we propose a bicarbonate/CO2 disequilibrium hypothesis to describe performance of CA-modified devices in both buffer and blood. Improvement in CO2 removal rates using CA-modified devices in blood may be realized by maximizing bicarbonate/CO2 disequilibrium at the fiber surface via strategies such as blood acidification and active mixing within the device.

摘要

由涂有碳酸酐酶(CA)的中空纤维膜(HFM)组成的人工肺装置,可加速从血液中去除二氧化碳(CO₂),用于治疗急性呼吸衰竭。虽然之前的工作表明,在磷酸盐缓冲盐水(PBS)中,CA涂层可使HFM对CO₂的去除率提高115%,但在血液中的测试显示,与未改性的HFM相比,去除率提高了36%。在这项工作中,我们试图表征这些生物催化装置内的CO₂传质过程,这些过程会阻碍CA涂层的功效,并开发提高生物活性HFM效率的方法。将胺化的HFM依次与戊二醛(GA)、壳聚糖、GA反应,然后与CA溶液孵育,将CA共价连接到表面。将生物活性CA-HFM封装在模型气体交换装置(0.0119 m²)中,并在不同流速下用PBS、全血和含有单个血液成分(血浆白蛋白、红细胞或游离碳酸酐酶)的溶液测试其酯酶活性和CO₂去除率。结果表明,增加固定化酶活性并不会显著影响CO₂去除率,因为在临床相关条件下,来自液体边界层的扩散阻力是未改性和生物活性HFM传输CO₂的主要障碍。此外,红细胞内的内源性CA与HFM固定的CA竞争,以增加CO₂的去除。基于我们的发现,我们提出了一个碳酸氢盐/CO₂不平衡假说,以描述CA改性装置在缓冲液和血液中的性能。通过血液酸化和装置内的主动混合等策略,在纤维表面最大化碳酸氢盐/CO₂不平衡,可能会提高CA改性装置在血液中去除CO₂的速率。

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