LncRNA TubAR complexes with TUBB4A and TUBA1A to promote microtubule assembly and maintain myelination

Author:

Liang Xiaolin,Gong Meng,Wang Zhikai,Wang Jie,Guo Weiwei,Cai Aoling,Yang ZhenyeORCID,Liu XingORCID,Xu Fuqiang,Xiong Wei,Fu Chuanhai,Wang Xiangting

Abstract

AbstractA long-standing hypothesis proposes that certain RNA(s) must exhibit structural roles in microtubule assembly. Here, we identify a long noncoding RNA (TubAR) that is highly expressed in cerebellum and forms RNA–protein complex with TUBB4A and TUBA1A, two tubulins clinically linked to cerebellar and myelination defects. TubAR knockdown in mouse cerebellum causes loss of oligodendrocytes and Purkinje cells, demyelination, and decreased locomotor activity. Biochemically, we establish the roles of TubAR in promoting TUBB4A–TUBA1A heterodimer formation and microtubule assembly. Intriguingly, different from the hypomyelination-causing mutations, the non-hypomyelination-causing mutation TUBB4A-R2G confers gain-of-function for an RNA-independent interaction with TUBA1A. Experimental use of R2G/A mutations restores TUBB4A–TUBA1A heterodimer formation, and rescues the neuronal cell death phenotype caused by TubAR knockdown. Together, we uncover TubAR as the long-elusive structural RNA for microtubule assembly and demonstrate how TubAR mediates microtubule assembly specifically from αβ-tubulin heterodimers, which is crucial for maintenance of cerebellar myelination and activity.

Funder

National Natural Science Foundation of China

Anhui Science and Technology Department

Chinese Academy of Sciences

Publisher

Springer Science and Business Media LLC

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