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止血针:通过儿茶酚胺氧化途径控制止血时间。

Hemostatic Needles: Controlling Hemostasis Time by a Catecholamine Oxidative Pathway.

机构信息

Department of Intelligent Precision Healthcare Convergence, SKKU Institute for Convergence, Sungkyunkwan University (SKKU), 2066 Seobu-ro, Suwon 16419, Republic of Korea.

R&D Center, InnoTherapy Inc., Seonyu-ro 13-gil, Yeongdeungpo-gu, Seoul 07327, Republic of Korea.

出版信息

ACS Appl Mater Interfaces. 2021 Mar 10;13(9):10741-10747. doi: 10.1021/acsami.0c22223. Epub 2021 Feb 23.

Abstract

Most infectious human viruses are generally found in the bloodstream after being released by infected organs. Thus, hemorrhage in patients, whose blood contains infectious viruses might be a significant risk for secondary infections. In this work, a self-sealing hemostatic needle that causes no bleeding even after its removal is reported. The materials used for the self-sealing needles are inspired by mussel adhesive polysaccharide, chitosan-catechol, which shows a rapid phase transition from a solid phase (i.e., a thin film) to an adhesive gel upon coming into contact with blood. We found that the self-sealing time for the complete hemostasis depends on the oxidation pathway of the conjugated catechol. For high-temperature oxidation (i.e., 60 °C), Michael addition is a dominant oxidative coupling reaction, which weakens the chitosan-catechol attachment force on the needle surface. Thus, the film is easily transferred to the hemorrhaging sites, with the result that there is no bleeding even after a short injection time (<5 s). In contrast, during low-temperature oxidation (4 °C), Schiff base formation is dominant, which strengthens the film attachment force on the needle surface, resulting in continued bleeding owing to a dearth of tissue transfer after the injection.

摘要

大多数感染人类的病毒通常在受感染器官释放后存在于血液中。因此,血液中含有传染性病毒的出血患者可能存在继发感染的重大风险。在这项工作中,报道了一种即使在移除后也不会引起出血的自密封止血针。自密封针的材料灵感来自贻贝类黏多糖、儿茶素-壳聚糖,它在与血液接触时会迅速从固相(即薄膜)转变为黏附性凝胶。我们发现,完全止血的自密封时间取决于共轭儿茶酚的氧化途径。对于高温氧化(即 60°C),迈克尔加成是主要的氧化偶联反应,它会削弱儿茶素-壳聚糖在针表面的附着力。因此,薄膜很容易转移到出血部位,结果是即使注射时间很短(<5 秒)也不会出血。相比之下,在低温氧化(4°C)时,席夫碱形成占主导地位,这增强了薄膜在针表面的附着力,导致注射后由于组织转移不足而持续出血。

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