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The Biological Effect of an Antisense Oligonucleotide Depends on Its Route of Endocytosis and Trafficking

机译:反义寡核苷酸的生物学效应取决于其内吞和贩运的途径

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We demonstrate that the biological effect of an oligonucleotide is influenced by its route of cellular uptake. Utilizing a splice-switching antisense oligonucleotide (SSO) and a sensitive reporter assay involving correction of RNA splicing, we examined induction of luciferase in cells treated either with various concentrations of an unconjugated ("free") SSO or an SSO conjugated to a bivalent RGD ligand that promotes binding to the alpha v beta 3 integrin (RGD-SSO). Under conditions of equal accumulation in cells, the RGD- SSO consistently had a greater effect on luciferase induction than the unconjugated SSO. We determined that the RGD- SSO and the unconjugated SSO were internalized by distinct endocytotic pathways, suggesting that the route of internalization affects the magnitude of the biological response.
机译:我们证明寡核苷酸的生物学效应受其细胞摄取途径的影响。利用剪接转换反义寡核苷酸(SSO)和涉及RNA剪接校正的敏感报告基因检测,我们研究了用各种浓度的未结合(“游离”)SSO或与二价RGD结合的SSO处理的细胞中荧光素酶的诱导促进与αv beta 3整联蛋白(RGD-SSO)结合的配体。在细胞中积累相等的条件下,RGD-SSO始终比未结合的SSO对萤光素酶诱导的影响更大。我们确定RGD-SSO和未结合的SSO被不同的内吞途径内化,表明内化途径影响生物学反应的强度。

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