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一个与丁型肝炎病毒核酶中金属离子反应偏好性转变相关的单核苷酸。

A single nucleotide linked to a switch in metal ion reactivity preference in the HDV ribozymes.

作者信息

Perrotta Anne T, Been Michael D

机构信息

Department of Biochemistry, Box 3711, Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

Biochemistry. 2007 May 1;46(17):5124-30. doi: 10.1021/bi602569x. Epub 2007 Apr 7.

Abstract

The two ribozymes of hepatitis delta virus (HDV) cleave faster in divalent metal ions than in monovalent cations, and a variety of divalent metal ions can act as catalysts in supporting these higher rates. Although the ribozymes are closely related in sequence and structure, they display a different metal ion preference; the genomic form cleaves moderately faster in Mg2+ than in Ca2+ while the reverse is true for the antigenomic ribozyme. This difference raises questions about understanding the catalytic role of the metal ion in the reaction. We found that the metal ion reactivity preference correlated with the identity of a single nucleotide 5' of the cleavage site (-1 position). It is a U in the genomic sequence and a C in the antigenomic sequence. With both ribozymes, the reactivity preference for Mg2+ and Ca2+ could be reversed with a change at this position (C to U or U to C). Moreover, with an A at position -1, there was a relative increase in cleavage rates in low concentrations of Mn2+ for both ribozymes. Metal ion reactivity preference was also linked to changes in pH, and the pH-rate profiles could be shifted with nucleotide changes at position -1. Together, the data provide biochemical evidence in support of an organized active site, as seen in the crystal structures, where at least one metal ion, an ionizable group, and the conformation of the phosphate backbone at the cleavage site interact in concert to promote cleavage.

摘要

丁型肝炎病毒(HDV)的两种核酶在二价金属离子中的切割速度比在单价阳离子中更快,并且多种二价金属离子可以作为催化剂来支持这些更高的反应速率。尽管这些核酶在序列和结构上密切相关,但它们表现出不同的金属离子偏好;基因组形式在Mg2+中的切割速度比在Ca2+中略快,而反基因组核酶则相反。这种差异引发了关于理解金属离子在反应中的催化作用的问题。我们发现金属离子反应性偏好与切割位点(-1位)5'端单个核苷酸的身份相关。在基因组序列中它是一个U,在反基因组序列中是一个C。对于这两种核酶,在这个位置发生变化(C变为U或U变为C)时,对Mg2+和Ca2+的反应性偏好可能会逆转。此外,在-1位为A时,两种核酶在低浓度Mn2+中的切割速率相对增加。金属离子反应性偏好也与pH值的变化有关,并且pH-速率曲线可以随着-1位核苷酸的变化而移动。总之,这些数据提供了生化证据,支持了晶体结构中所见的有组织的活性位点,其中至少一种金属离子、一个可电离基团以及切割位点处磷酸骨架的构象协同相互作用以促进切割。

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