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介孔硅/聚谷氨酸肽树枝状聚合物的双重靶向合成及其在溶栓中的应用。

Synthesis of mesoporous silica/polyglutamic acid peptide dendrimer with dual targeting and its application in dissolving thrombus.

机构信息

State Key Laboratory of Applied Organic Chemistry, Key Laboratory of Nonferrous Metal Chemistry and Resources Utilization of Gansu Province, Department of Chemistry and Chemical Engineering, Lanzhou University, Lanzhou, China.

Longnan Teacher's College, Longnan, China.

出版信息

J Biomed Mater Res A. 2019 Aug;107(8):1824-1831. doi: 10.1002/jbm.a.36703. Epub 2019 May 1.

Abstract

With the frequent occurrence of thrombus diseases, thrombus has become a factor endangering human health. Nattokinase (NK) is a new generation of thrombolytic drug with efficient thrombolytic effect and no major side effects. However, it is easily inactivated in external environment due to its sensitivity, which is still a challenge for its generalized application. Herein, a mesoporous silica/polyglutamic acid peptide dendrimer (M-MSNs-G -RGD) nanoparticle was prepared to protect and transport NK. First, magnetic mesoporous silica nanoparticles (M-MSNs) were prepared as the core of the whole nanoparticle, then polyglutamic acid peptide dendrimer (G ) was bonded to form M-MSNs-G . At last, arginine-glycine-aspartic peptide (RGD) was grafted onto the M-MSNs-G to obtain M-MSNs-G -RGD. The physical and chemical characteristics and biological toxicity of M-MSNs-G -RGD were studied. Thrombus-targeting nanocomposites M-MSNs-G -RGD/NK were prepared by loading the thrombolytic drug NK via electrostatic interaction. In vitro and in vivo targeted thrombolytic experiments showed that the nanoparticles exhibited significant thrombolysis ability. These results suggested the potential application of M-MSNs-G -RGD/NK in dual targeted thrombolysis.

摘要

随着血栓疾病的频繁发生,血栓已成为危害人类健康的因素之一。纳豆激酶(NK)是一种新型的溶栓药物,具有高效的溶栓作用,且无明显的副作用。然而,由于其敏感性,它在外部环境中很容易失活,这仍然是其广泛应用的一个挑战。本文制备了一种介孔硅/聚谷氨酸肽树枝状大分子(M-MSNs-G-RGD)纳米粒子,用于保护和输送 NK。首先,制备磁性介孔硅纳米粒子(M-MSNs)作为整个纳米粒子的核心,然后将聚谷氨酸肽树枝状大分子(G)键合形成 M-MSNs-G。最后,将精氨酸-甘氨酸-天冬氨酸肽(RGD)接枝到 M-MSNs-G 上,得到 M-MSNs-G-RGD。研究了 M-MSNs-G-RGD 的物理化学特性和生物毒性。通过静电相互作用将溶栓药物 NK 装载到血栓靶向纳米复合材料 M-MSNs-G-RGD/NK 中。体外和体内靶向溶栓实验表明,纳米粒子具有显著的溶栓能力。这些结果表明,M-MSNs-G-RGD/NK 在双重靶向溶栓中具有潜在的应用前景。

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