ANT2 functions as a translocon for mitochondrial cross-membrane translocation of RNAs.

ANT2 作为转位子,负责 RNA 的线粒体跨膜转位

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作者:Wang Pengcheng, Zhang Lixiao, Chen Siyi, Li Renjian, Liu Peipei, Li Xiang, Luo Hongdi, Huo Yujia, Zhang Zhirong, Cai Yiqi, Liu Xu, Huang Jinliang, Zhou Guangkeng, Sun Zhe, Ding Shanwei, Shi Jiahao, Zhou Zizhuo, Yuan Ruoxi, Liu Liang, Wu Sipeng, Wang Geng
Bidirectional transcription of mammalian mitochondrial DNA generates overlapping transcripts that are capable of forming double-stranded RNA (dsRNA) structures. Release of mitochondrial dsRNA into the cytosol activates the dsRNA-sensing immune signaling, which is a defense mechanism against microbial and viral attack and possibly cancer, but could cause autoimmune diseases when unchecked. A better understanding of the process is vital in therapeutic application of this defense mechanism and treatment of cognate human diseases. In addition to exporting dsRNAs, mitochondria also export and import a variety of non-coding RNAs. However, little is known about how these RNAs are transported across mitochondrial membranes. Here we provide direct evidence showing that adenine nucleotide translocase-2 (ANT2) functions as a mammalian RNA translocon in the mitochondrial inner membrane, independent of its ADP/ATP translocase activity. We also show that mitochondrial dsRNA efflux through ANT2 triggers innate immunity. Inhibiting this process alleviates inflammation in vivo, providing a potential therapeutic approach for treating autoimmune diseases.

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