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工程化红细胞成为红细胞传感器:初探。

Engineering erythrocytes to be erythrosensors: first steps.

机构信息

Dalton Cardiovascular Research Center, Department of Medical Pharmacology and Physiology, University of Missouri, USA.

出版信息

Blood Cells Mol Dis. 2011 Aug 15;47(2):100-6. doi: 10.1016/j.bcmd.2011.05.001.

Abstract

Molecules can be loaded into mammalian erythrocytes through a reversible lysis pore that forms in the membrane when placed in hypotonic media, the result being resealed red cell ghosts. Many studies on the sidedness of transport processes have utilized this approach. In addition, red cell ghosts encapsulated with enzymes have been used in patients to treat specific enzyme deficiencies, particularly when the substrate can cross the red cell membrane. Our long-term goal is to put fluorescent sensors inside erythrocytes, return the loaded red cell ghosts to the animal or patient, and then monitor the fluorescence non-invasively to follow changes in plasma analyte concentration. In this paper, we present a novel dialysis method for making the red cell ghosts. In addition, we present a theoretical analysis showing that it is not necessary that every loaded red cell ghost has the same dye concentration. Finally we discuss the constraints on the optimal affinity for the sensor/analyte interaction.

摘要

分子可以通过可逆的溶血孔装载到哺乳动物的红细胞中,当将其置于低渗介质中时,膜中会形成这种孔,其结果是重新密封的红细胞血影。许多关于运输过程的偏侧性的研究都利用了这种方法。此外,用酶包裹的红细胞血影已被用于治疗特定的酶缺乏症的患者,特别是当底物可以穿过红细胞膜时。我们的长期目标是将荧光传感器置于红细胞内,将负载的红细胞血影返回给动物或患者,然后非侵入性地监测荧光,以跟踪血浆分析物浓度的变化。在本文中,我们提出了一种用于制造红细胞血影的新的透析方法。此外,我们还提出了一种理论分析,表明并非每个负载的红细胞血影都具有相同的染料浓度。最后,我们讨论了对传感器/分析物相互作用的最佳亲和力的限制。

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