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异胞嘧啶和异鸟嘌呤之间碱基对的酶促识别。

Enzymatic recognition of the base pair between isocytidine and isoguanosine.

作者信息

Switzer C Y, Moroney S E, Benner S A

机构信息

Laboratory for Organic Chemistry, ETH Zurich, Switzerland.

出版信息

Biochemistry. 1993 Oct 5;32(39):10489-96. doi: 10.1021/bi00090a027.

Abstract

The ability of various polymerases to catalyze the template-directed formation of a base pair between isoguanine (iso-G) and isocytosine (iso-C) in duplex oligonucleotides has been investigated. A new procedure was developed for preparing derivatives of deoxyisoguanosine suitable for incorporation into DNA using an automated DNA synthesizer. T7 RNA polymerase, AMV reverse transcriptase, and the Klenow fragment of DNA polymerase all incorporated iso-G opposite iso-C in a template. T4 DNA polymerase did not. Several polymerases also incorporated iso-G opposite T, presumably through pairing with a minor tautomeric form of iso-G complementary to T. In a template, iso-G directs the incorporation of both iso-C and T when Klenow fragment is the catalyst and only U when T7 RNA polymerase is the catalyst. Further, derivatives of iso-C were found to undergo significant amounts of deamination under alkaline conditions used for base deprotection after automated oligonucleotide synthesis. Both the deamination reaction of iso-C and the ambivalent tautomeric forms of iso-G make it unlikely that the (iso-C).(iso-G) base pair was a part of information storage molecules also containing the A.T and G.C base pairs found in primitive forms of life that emerged on planet earth several billion years ago. Nevertheless, the extra letters in the genetic alphabet can serve useful roles in a contemporary laboratory setting.

摘要

研究了多种聚合酶催化双链寡核苷酸中异鸟嘌呤(iso-G)与异胞嘧啶(iso-C)之间模板导向碱基对形成的能力。开发了一种新方法,用于制备适合使用自动DNA合成仪掺入DNA的脱氧异鸟苷衍生物。T7 RNA聚合酶、禽成髓细胞瘤病毒逆转录酶和DNA聚合酶的Klenow片段都能在模板中将iso-G掺入到与iso-C相对的位置。T4 DNA聚合酶则不能。几种聚合酶还能将iso-G掺入到与胸腺嘧啶(T)相对的位置,推测是通过与iso-G的一种与T互补的次要互变异构体配对实现的。在模板中,当Klenow片段作为催化剂时,iso-G可指导iso-C和T的掺入;而当T7 RNA聚合酶作为催化剂时,iso-G仅指导尿嘧啶(U)的掺入。此外,发现异胞嘧啶衍生物在自动寡核苷酸合成后用于碱基脱保护的碱性条件下会发生大量脱氨反应。异胞嘧啶的脱氨反应和异鸟嘌呤的两性互变异构体使得(iso-C)·(iso-G)碱基对不太可能成为数十亿年前出现在地球上的原始生命形式中也包含A·T和G·C碱基对的信息存储分子的一部分。尽管如此,遗传字母表中的这些额外字母在当代实验室环境中仍可发挥有用作用。

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