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通过抗生物素蛋白-生物素系统完全保护反义寡核苷酸免受血清核酸酶降解。

Complete protection of antisense oligonucleotides against serum nuclease degradation by an avidin-biotin system.

作者信息

Boado R J, Pardridge W M

机构信息

Department of Medicine, UCLA School of Medicine 90024.

出版信息

Bioconjug Chem. 1992 Nov-Dec;3(6):519-23. doi: 10.1021/bc00018a010.

DOI:10.1021/bc00018a010
PMID:1334437
Abstract

It has been recently demonstrated that a complex of avidin, a cationic protein, and a monobiotinylated antisense oligonucleotide for the GLUT1 glucose transporter mRNA is taken up by cells in vitro and by organs in vivo via absorptive-mediated endocytosis. In the present study, a GLUT1 biotinylated oligonucleotide-avidin construct showing complete protection against serum 3'-exonuclease-mediated degradation is described. 21-mer antisense oligonucleotides complementary to nucleotides 162-182 and 161-181 of the bovine GLUT1 glucose transporter mRNA were synthesized with a 6-aminodeoxyuridine at positions 3 and 20, respectively, biotinylated with NHS- or NHS-XX-biotin to yield near 5'- or near 3'-biotinylated oligonucleotide (bio-DNA), and 5'- and 3'-end radiolabeled. Serum induced a rapid degradation of unprotected (no avidin) [5'-32P]-5'-bio-DNA (> 95% at 30 min). Avidin partially protected this construct (approximately 31% of intact 21-mer oligo remained at 1 h). Similar results were obtained with the [3'-32P]-5'-bio-DNA; however, no degradation products of varying size were observed, confirming that the degradation is mediated primarily by a 3'-exonuclease. Incubation of the [5'-32P]-3'-bio-DNA with serum showed a rapid conversion to the 20- and 19-mer forms (t1/2 approximately 13 min). Conversely, avidin totally protected this construct against the serum 3'-exonuclease. In conclusion, avidin fully protects antisense oligonucleotides biotinylated at the near 3'-terminus against serum 3'-exonuclease degradation, and this property may be useful for avidin-mediated drug delivery of oligonucleotides to tissues in vivo or to cultured cells in vitro.

摘要

最近有研究表明,抗生物素蛋白(一种阳离子蛋白)与针对葡萄糖转运蛋白1(GLUT1)mRNA的单生物素化反义寡核苷酸形成的复合物,在体外可被细胞摄取,在体内可被器官通过吸附介导的内吞作用摄取。在本研究中,描述了一种对血清3'-核酸外切酶介导的降解具有完全保护作用的GLUT1生物素化寡核苷酸-抗生物素蛋白构建体。合成了与牛GLUT1葡萄糖转运蛋白mRNA的核苷酸162 - 182和161 - 181互补的21聚体反义寡核苷酸,分别在第3位和第20位含有6-氨基脱氧尿苷,用NHS-生物素或NHS-XX-生物素进行生物素化,得到接近5'-或接近3'-生物素化的寡核苷酸(生物素化DNA),并对5'-和3'-末端进行放射性标记。血清可导致未受保护(无抗生物素蛋白)的[5'-32P]-5'-生物素化DNA快速降解(30分钟时>95%)。抗生物素蛋白对该构建体有部分保护作用(1小时时约31%的完整21聚体寡核苷酸保留)。[3'-32P]-5'-生物素化DNA也得到了类似结果;然而,未观察到大小不同的降解产物,证实降解主要由3'-核酸外切酶介导。[5'-32P]-3'-生物素化DNA与血清孵育显示快速转化为20聚体和19聚体形式(半衰期约13分钟)。相反,抗生物素蛋白完全保护该构建体免受血清3'-核酸外切酶的作用。总之,抗生物素蛋白可完全保护接近3'-末端生物素化的反义寡核苷酸免受血清3'-核酸外切酶降解,这一特性可能有助于抗生物素蛋白介导的寡核苷酸在体内向组织或体外培养细胞的药物递送。

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