Division of Immunology, The Netherlands Cancer Institute, 1066 CX Amsterdam, The Netherlands.
DNA Repair (Amst). 2011 Oct 10;10(10):1051-9. doi: 10.1016/j.dnarep.2011.08.005. Epub 2011 Sep 1.
The generation of high affinity antibodies in B cells critically depends on translesion synthesis (TLS) polymerases that introduce mutations into immunoglobulin genes during somatic hypermutation (SHM). The majority of mutations at A/T base pairs during SHM require ubiquitination of PCNA at lysine 164 (PCNA-Ub), which activates TLS polymerases. By comparing the mutation spectra in B cells of WT, TLS polymerase η (Polη)-deficient, PCNA(K164R)-mutant, and PCNA(K164R);Polη double-mutant mice, we now find that most PCNA-Ub-independent A/T mutagenesis during SHM is mediated by Polη. In addition, upon exposure to various DNA damaging agents, PCNA(K164R) mutant cells display strongly impaired recruitment of TLS polymerases, reduced daughter strand maturation and hypersensitivity. Interestingly, compared to the single mutants, PCNA(K164R);Polη double-mutant cells are dramatically delayed in S phase progression and far more prone to cell death following UV exposure. Taken together, these data support the existence of PCNA ubiquitination-dependent and -independent activation pathways of Polη during SHM and DNA damage tolerance.
B 细胞中高亲和力抗体的产生严重依赖于跨损伤合成(TLS)聚合酶,这些聚合酶在体细胞高频突变(SHM)过程中向免疫球蛋白基因中引入突变。在 SHM 过程中 A/T 碱基对的大多数突变需要 PCNA 赖氨酸 164 的泛素化(PCNA-Ub),这会激活 TLS 聚合酶。通过比较 WT、TLS 聚合酶 η(Polη)缺陷、PCNA(K164R)突变和 PCNA(K164R);Polη 双突变小鼠的 B 细胞中的突变谱,我们现在发现,SHM 过程中大多数 PCNA-Ub 不依赖的 A/T 诱变是由 Polη 介导的。此外,在暴露于各种 DNA 损伤剂后,PCNA(K164R)突变细胞显示出 TLS 聚合酶的募集严重受损、子链成熟减少和超敏性。有趣的是,与单突变体相比,PCNA(K164R);Polη 双突变体细胞在 S 期进展中明显延迟,并且在暴露于 UV 后更易于细胞死亡。总之,这些数据支持在 SHM 和 DNA 损伤耐受过程中存在 PCNA 泛素化依赖性和非依赖性的 Polη 激活途径。
