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补骨脂素衍生的寡核苷膦酸甲酯与兔珠蛋白信使核糖核酸的光化学交联

Photochemical cross-linking of psoralen-derivatized oligonucleoside methylphosphonates to rabbit globin messenger RNA.

作者信息

Kean J M, Murakami A, Blake K R, Cushman C D, Miller P S

机构信息

Division of Biophysics, School of Hygiene and Public Health, Johns Hopkins University, Baltimore, Maryland 21205.

出版信息

Biochemistry. 1988 Dec 27;27(26):9113-21. doi: 10.1021/bi00426a008.

DOI:10.1021/bi00426a008
PMID:2468360
Abstract

Antisense oligodeoxyribonucleoside methylphosphonates targeted against various regions of mRNA or precursor mRNA are selective inhibitors of mRNA expression both in cell-free systems and in cells in culture. The efficiency with which methylphosphonate oligomers interact with mRNA, and thus inhibit translation, can be considerably increased by introducing photoactivatable psoralen derivatives capable of cross-linking with the mRNA. Oligonucleoside methylphosphonates complementary to coding regions of rabbit alpha- or beta-globin mRNA were derivatized with 4'-(aminoalkyl)-4,5',8-trimethylpsoralens by attaching the psoralen group to the 5' end of the oligomer via a nuclease-resistant phosphoramidate linkage. The distance between the psoralen group and the 5' end of the oligomer can be adjusted by changing the number of methylene groups in the aminoalkyl linker arm. The psoralen-derivatized oligomers specifically cross-link to their complementary sequences on the targeted mRNA. For example, an oligomer complementary to nucleotides 56-67 of alpha-globin mRNA specifically cross-linked to alpha-globin mRNA upon irradiation of a solution of the oligomer and rabbit globin mRNA at 4 degrees C. Oligomers derivatized with 4'-[[N-(2-amino-ethyl)amino]methyl]-4,5',8-trimethylpsoralen gave the highest extent of cross-linking to mRNA. The extent of cross-linking was also determined by the chain length of the oligomer and the structure of the oligomer binding site. Oligomers complementary to regions of mRNA that are sensitive to hydrolysis by single-strand-specific nucleases cross-linked to an approximately 10-30-fold greater extent than oligomers complementary to regions that are insensitive to nuclease hydrolysis.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

针对mRNA或前体mRNA不同区域的反义寡脱氧核糖核苷甲基膦酸酯,在无细胞系统和培养细胞中都是mRNA表达的选择性抑制剂。通过引入能够与mRNA交联的光活化补骨脂素衍生物,可以显著提高甲基膦酸酯寡聚物与mRNA相互作用并抑制翻译的效率。与兔α-或β-珠蛋白mRNA编码区互补的寡核苷甲基膦酸酯,通过耐核酸酶的氨基磷酸酯键将补骨脂素基团连接到寡聚物的5'端,用4'-(氨基烷基)-4,5',8-三甲基补骨脂素进行衍生化。补骨脂素基团与寡聚物5'端之间的距离可以通过改变氨基烷基连接臂中亚甲基的数量来调节。补骨脂素衍生化的寡聚物特异性地与靶向mRNA上的互补序列交联。例如,与α-珠蛋白mRNA的56-67位核苷酸互补的寡聚物,在4℃照射该寡聚物和兔珠蛋白mRNA的溶液时,会特异性地与α-珠蛋白mRNA交联。用4'-[[N-(2-氨基乙基)氨基]甲基]-4,5',8-三甲基补骨脂素衍生化的寡聚物与mRNA的交联程度最高。交联程度还取决于寡聚物的链长和寡聚物结合位点的结构。与对单链特异性核酸酶水解敏感的mRNA区域互补的寡聚物,其交联程度比与对核酸酶水解不敏感区域互补的寡聚物高约10-30倍。(摘要截短于250字)

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