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首页> 外文期刊>Biomaterials >Effect of trastuzumab-modified antisense oligonucleotide-loaded human serum albumin nanoparticles prepared by heat denaturation.
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Effect of trastuzumab-modified antisense oligonucleotide-loaded human serum albumin nanoparticles prepared by heat denaturation.

机译:热变性制备的曲妥珠单抗修饰的反义寡核苷酸负载的人血清白蛋白纳米粒子的作用。

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摘要

Nanoparticles represent a promising tool for targeted drug delivery to tumour cells and are able to protect drugs against degradation. In our present study we developed targeted nanoparticles loaded with antisense oligonucleotides (ASOs) against Plk1 (polo-like kinase 1) prepared by heat denaturation instead of using glutaraldehyde. Glutaraldehyde can lead to an inactivation of ASOs through chemical crosslinking and is a toxic entity. We examined the ideal preparation conditions and characterised the resulting particles in terms of physico-chemical properties, ASO recovery after enzymatic degradation and stability. Stable monodisperse nanoparticles with an ASO recovery of more than 80% could be prepared at a temperature of 105 degrees C for 10 min. Furthermore we performed quantitative real-time PCR and Western blot to detect an ASO-mediated effect on Plk1 in BT-474 cells. We observed a significant reduction of Plk1 mRNA and protein expression. Thus, this is the first report of ASO-loaded HSA nanoparticles prepared by heat denaturation, where an impact on gene expression could be observed. The data provide the basis for the further development of carrier systems for ASOs to reduce off-target effects evoked by systemically administered ASOs and to achieve a better penetration into primary and metastatic target cells.
机译:纳米颗粒代表了靶向药物递送至肿瘤细胞的有前途的工具,并且能够保护药物免于降解。在我们目前的研究中,我们开发了靶向纳米粒子,该纳米粒子负载了通过热变性而不是使用戊二醛制备的针对Plk1(polo样激酶1)的反义寡核苷酸(ASO)。戊二醛可以通过化学交联导致ASO失活,并且是一种有毒的物质。我们检查了理想的制备条件,并根据理化性质,酶降解后的ASO回收率和稳定性对了所得颗粒进行了表征。 ASO回收率超过80%的稳定的单分散纳米颗粒可以在105摄氏度的温度下制备10分钟。此外,我们进行了定量实时PCR和Western印迹,以检测ASO介导的BT-474细胞中Plk1的作用。我们观察到Plk1 mRNA和蛋白质表达的显着降低。因此,这是通过热变性制备的载有ASO的HSA纳米颗粒的第一份报告,其中可以观察到对基因表达的影响。数据为进一步开发ASO载体系统提供了基础,以减少全身给药的ASO引起的脱靶效应,并更好地渗透到原代和转移靶细胞中。

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