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Synthesis of peptide-oilgonucleotide conjugates with single and multiple peptides attached to 2'-aldehydes through thiazolidine, oxime, and hydrazine linkages

机译:具有通过噻唑烷,肟和肼键与2'-醛连接的单个和多个肽的肽-油核苷酸缀合物的合成

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摘要

2'-Deoxyoligonucleotides and 2'-O-methyloligoribonucleotides carrying one or more 2'-aldehyde groups were synthesized and coupled to peptides containing an N-terminal cysteine, aminooxy, or hydrazide group to give peptide - oligonucleotide conjugates incorporating single or multiple peptides in good yield. The facile conjugation method allows specific coupling in aqueous solution of unprotected oligonucleotides containing aldehyde groups to unprotected N-terminally modified peptides and other small molecules. A 12-mer 2'-O-methyloligoribonucleotide complementary to the the HIV-1 TAR RNA stem-loop and containing two conjugated copies of an 8-mer model laminin peptide was hardly affected in TAR RNA binding and showed a similar level of inhibition of HIV-1 Tat-dependent in vitro transcription compared to the unconjugated 2'-O-methyloligoribonucleotide. Advantages of this conjugation method include (1) the ability to attach more than one peptide or other small molecule to oligonucleotide at defined nucleoside residue locations; (2) a conjugation route that does not affect significantly oligonucleotide binding to RNA structures; and (3) three alternative, facile, and mild conjugation reaction types that do not require use of a large excess of peptide reagent.
机译:合成带有一个或多个2'-醛基的2'-脱氧寡核苷酸和2'-O-甲基寡核糖核苷酸,并将其与含有N端半胱氨酸,氨氧基或酰肼基团的肽偶联,得到肽-寡核苷酸缀合物,其在单个或多个肽中掺入良品率高。简便的缀合方法允许未保护的含有醛基的寡核苷酸在水溶液中与未保护的N-末端修饰的肽和其他小分子特异性偶联。与HIV-1 TAR RNA茎环互补且包含两个8聚体模型层粘连蛋白肽的两个共轭拷贝的12聚体2'-O-甲基寡核糖核苷酸几乎不受TAR RNA结合的影响,并显示出相似的抑制作用与未缀合的2'-O-甲基寡核糖核苷酸相比,HIV-1 Tat依赖的体外转录。这种缀合方法的优点包括:(1)在确定的核苷残基位置将一个以上的肽或其他小分子连接至寡核苷酸的能力; (2)不显着影响寡核苷酸与RNA结构结合的结合途径; (3)不需要使用大量肽试剂的三种备选,简便和轻度的偶联反应类型。

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