Department of Pathogen Biology, School of Basic Medicine, Tongji Medical College, Huazhong University of Science and Technology, 13 Hangkong Road, Wuhan, Hubei 430030, China.
Shanghai Synchrotron Radiation Facility, Shanghai Advanced Research Institute, Chinese Academy of Sciences, Shanghai 201204, China.
Structure. 2023 Nov 2;31(11):1463-1472.e2. doi: 10.1016/j.str.2023.08.005. Epub 2023 Aug 30.
The type II restriction endonuclease Sau3AI cleaves the sequence 5'-GATC-3' in double-strand DNA producing two sticky ends. Sau3AI cuts both DNA strands regardless of methylation status. Here, we report the crystal structures of the active site mutant Sau3AI-E64A and the C-terminal domain Sau3AI-C with a bound GATC substrate. Interestingly, the catalytic site of the N-terminal domain (Sau3AI-N) is spatially blocked by the C-terminal domain, suggesting a potential self-inhibition of the enzyme. Interruption of Sau3AI-C binding to substrate DNA disrupts Sau3AI function, suggesting a functional linkage between the N- and C-terminal domains. We propose that Sau3AI-C behaves as an allosteric effector binding one GATC substrate, which triggers a conformational change to open the N-terminal catalytic site, resulting in the subsequent GATC recognition by Sau3AI-N and cleavage of the second GATC site. Our data indicate that Sau3AI and UbaLAI might represent a new subclass of type IIE restriction enzymes.
II 型限制内切酶 Sau3AI 可在双链 DNA 上切割 5'-GATC-3'序列,产生两个粘性末端。Sau3AI 会切割两条 DNA 链,而不受甲基化状态的影响。在这里,我们报告了活性位点突变体 Sau3AI-E64A 和带有结合 GATC 底物的 C 末端结构域 Sau3AI-C 的晶体结构。有趣的是,N 末端结构域(Sau3AI-N)的催化位点被 C 末端结构域空间阻断,这表明该酶可能存在自身抑制。Sau3AI-C 与底物 DNA 结合的中断破坏了 Sau3AI 的功能,这表明 N 末端和 C 末端结构域之间存在功能联系。我们提出 Sau3AI-C 作为结合一个 GATC 底物的别构效应物,它触发构象变化以打开 N 末端催化位点,从而导致 Sau3AI-N 随后识别 GATC 并切割第二个 GATC 位点。我们的数据表明,Sau3AI 和 UbaLAI 可能代表 II 型 E 类限制酶的一个新亚类。
