In the evolutionary arms race between bacteria and viruses, retrons have emerged as distinctive antiphage defense systems. Here, we elucidate the structure and function of Retron-Eco2, which comprises a non-coding RNA (ncRNA) that encodes multicopy single-stranded DNA (msDNA, a DNAâRNA hybrid) and a fusion protein containing a reverse transcriptase (RT) domain and a topoisomerase-primase-like (Toprim) effector domain. The Eco2 msDNA and RT-Toprim fusion protein form a 1:1 stoichiometric nucleoprotein complex that further assembles into a trimer (msDNA:RT-Toprim ratio of 3:3) with a distinctive triangular configuration. The RNA portion of the msDNA in one protomer closely intertwines around the RT domain of an adjacent protomer, mediating the formation of this self-inhibitory assembly. Upon activation, the Toprim effector domain exhibits RNase activity, degrading RNA to arrest phage replication. We further reveal that phage mutants evading Eco2-mediated defense harbor mutations in the endonuclease IV-like protein DenB, underscoring DenB's critical role in triggering the activation of this system. Together, these findings provide key structural and functional insights into Retron-Eco2, laying the groundwork for harnessing its potential in biotechnology and synthetic biology applications.
Structural basis of the RNA-mediated Retron-Eco2 oligomerization.
RNA介导的Retron-Eco2寡聚化的结构基础
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作者:Wang Yanjing, Wang Chen, Yin Yongqi, Cui Yongqing, Dai Zhikang, Liu Chang, Chen Yanke, Guan Zeyuan, Zou Tingting
| 期刊: | Cell Discovery | 影响因子: | 12.500 |
| 时间: | 2025 | 起止号: | 2025 Sep 2; 11(1):73 |
| doi: | 10.1038/s41421-025-00823-y | 研究方向: | 其它 |
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