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大肠杆菌蛋白Fpg和Nth对簇状DNA损伤中碱基损伤的识别及切除动力学

Recognition and kinetics for excision of a base lesion within clustered DNA damage by the Escherichia coli proteins Fpg and Nth.

作者信息

David-Cordonnier M H, Laval J, O'Neill P

机构信息

Medical Research Council, Radiation and Genome Stability Unit, Harwell, Didcot, Oxon OX11 0RD, United Kingdom.

出版信息

Biochemistry. 2001 May 15;40(19):5738-46. doi: 10.1021/bi002605d.

Abstract

Ionizing radiation and radiomimetic anticancer agents induce clustered DNA damages that are thought to lead to deleterious biological consequences, due to the challenge that clustered damage may present to the repair machinery of the cell. Specific oligonucleotides, containing either dihydrothymine (DHT) or 7,8-dihydro-8-oxoguanine (8-oxoG) opposite to specific lesions at defined positions on the complementary strand, have been used to determine the kinetic constants, K(M), k(cat), and specificity constants, for excision of DHT and 8-oxoG by the Escherichia coli base excision repair proteins, endonuclease III (Nth) and formamidopyrimidine glycosylase (Fpg), respectively. For excision of DHT opposite to 8-oxoadenine by Nth or Fpg proteins, or 8-oxoG opposite to 8-oxoG by Fpg, the major change in the specificity constant occurs when the second lesion on the complementary strand is one base to the site opposite to DHT or 8-oxoG. The specificity constants for excision of DHT or 8-oxoG by both proteins are reduced by up to 2 orders of magnitude when an abasic site or a strand break is opposite on the complementary strand. Whereas the values of K(M) are only slightly affected by the presence of a second lesion, the major change is seen as a reduction in the values of k(cat). The binding of Fpg protein to oligonucleotides containing 8-oxoG is inhibited, particularly when a single strand break is near to 8-oxoG on the complementary strand. It is inferred that not only the binding affinity of Fpg protein to the base lesion but also the rate of excision of the damaged base is reduced by the presence of another lesion, particularly a single strand break or an AP site on the complementary strand.

摘要

电离辐射和类辐射抗癌剂会诱导产生簇状DNA损伤,由于这种簇状损伤可能给细胞的修复机制带来挑战,人们认为其会导致有害的生物学后果。含有二氢胸腺嘧啶(DHT)或7,8 - 二氢 - 8 - 氧代鸟嘌呤(8 - oxoG)且与互补链上特定位置的特定损伤相对的特定寡核苷酸,已被用于分别测定大肠杆菌碱基切除修复蛋白核酸内切酶III(Nth)和甲酰胺嘧啶糖基化酶(Fpg)切除DHT和8 - oxoG的动力学常数K(M)、催化常数k(cat)以及特异性常数。对于Nth或Fpg蛋白切除与8 - 氧代腺嘌呤相对的DHT,或Fpg切除与8 - oxoG相对的8 - oxoG而言,当互补链上的第二个损伤位于与DHT或8 - oxoG相对位点的一个碱基处时,特异性常数会发生主要变化。当互补链上存在一个无碱基位点或链断裂与DHT或8 - oxoG相对时,两种蛋白切除DHT或8 - oxoG的特异性常数会降低多达2个数量级。虽然K(M)的值仅受到第二个损伤存在的轻微影响,但主要变化表现为k(cat)值的降低。Fpg蛋白与含有8 - oxoG的寡核苷酸的结合受到抑制,尤其是当互补链上的单链断裂靠近8 - oxoG时。据推断,不仅Fpg蛋白与碱基损伤的结合亲和力会因另一个损伤的存在而降低,受损碱基的切除速率也会降低,特别是互补链上存在单链断裂或无嘌呤嘧啶位点时。

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