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In vivo tumor growth inhibition and biodistribution studies of locked nucleic acid (LNA) antisense oligonucleotides

机译:锁核酸(LNA)反义寡核苷酸的体内肿瘤生长抑制和生物分布研究

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摘要

Locked nucleic acids (LNA) are novel high-affinity DNA analogs that can be used as genotype-specific drugs. The LNA oligonucleotides (LNA PO ODNs) are very stable in vitro and in vivo without the need for a phosphorothiolated backbone. In this study we tested the biological fate and the efficacy in tumor growth inhibition of antisense oligonucleotides directed against the gene of the large subunit of RNA polymerase II (POLR2A) that are completely synthesized as LNA containing diester backbones. These full LNA oligonucleotides strongly reduce POLR2A protein levels. Full LNA PO ODNs appeared to be very stable compounds when injected into the circulation of mice. Full LNA PO ODNs were continuously administered for 14 days to tumor-bearing nude mice. Tumor growth was inhibited sequence specifically at dosages from 1 mg/kg/day. LNA PO ODNs appeared to be non-toxic at dosages <5 mg/kg/day. Biodistribution studies showed the kidneys to have the highest uptake of LNA PO ODNs and urinary secretion as the major route of clearance. This report shows that LNA PO ODNs are potent genotype-specific drugs that can inhibit tumor growth in vivo.
机译:锁核酸(LNA)是新型的高亲和力DNA类似物,可用作基因型特异性药物。 LNA寡核苷酸(LNA PO ODN)在体外和体内非常稳定,不需要硫代磷酸化的骨架。在这项研究中,我们测试了针对RNA聚合酶II(POLR2A)大亚基基因的反义寡核苷酸的生物学命运和抑制肿瘤生长的功效,这些反义寡核苷酸已完全合成为包含LNA的二酯骨架。这些完整的LNA寡核苷酸可大大降低POLR2A蛋白水平。完整的LNA PO ODN似乎是非常稳定的化合物,当注入小鼠循环系统中时。将完整的LNA PO ODN连续14天施用于荷瘤裸鼠。从1 mg / kg /天的剂量开始,肿瘤的生长受到抑制,具体表现在序列上。 LNA PO ODNs在<5 mg / kg /天的剂量下似乎无毒。生物分布研究表明,肾脏对LNA PO ODNs的吸收最高,而尿液分泌是主要的清除途径。该报告表明,LNA PO ODN是有效的基因型特异性药物,可以抑制体内肿瘤的生长。

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