- Li, Na;
- Ma, Jianbing;
- Fu, Hang;
- Yang, Zhiwei;
- Xu, Chunhua;
- Li, Haihong;
- Zhao, Yimin;
- Zhao, Yizhen;
- Chen, Shuyu;
- Gou, Lu;
- Zhang, Xinghua;
- Zhang, Shengli;
- Li, Ming;
- Hou, Ximiao;
- Zhang, Lei;
- Lu, Ying
The structural diversity of biological macromolecules in different environments contributes complexity to enzymological processes vital for cellular functions. Fluorescence resonance energy transfer and electron microscopy are used to investigate the enzymatic reaction of T4 DNA ligase catalyzing the ligation of nicked DNA. The data show that both the ligase-AMP complex and the ligase-AMP-DNA complex can have four conformations. This finding suggests the parallel occurrence of four ligation reaction pathways, each characterized by specific conformations of the ligase-AMP complex that persist in the ligase-AMP-DNA complex. Notably, these complexes have DNA bending angles of ≈0°, 20°, 60°, or 100°. The mechanism of parallel reactions challenges the conventional notion of simple sequential reaction steps occurring among multiple conformations. The results provide insights into the dynamic conformational changes and the versatile attributes of T4 DNA ligase and suggest that the parallel multiple reaction pathways may correspond to diverse T4 DNA ligase functions. This mechanism may potentially have evolved as an adaptive strategy across evolutionary history to navigate complex environments.