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ERH facilitates microRNA maturation through the interaction with the N-terminus of DGCR8.


ABSTRACT: The microprocessor complex cleaves the primary transcript of microRNA (pri-miRNA) to initiate miRNA maturation. Microprocessor is known to consist of RNase III DROSHA and dsRNA-binding DGCR8. Here, we identify Enhancer of Rudimentary Homolog (ERH) as a new component of Microprocessor. Through a crystal structure and biochemical experiments, we reveal that ERH uses its hydrophobic groove to bind to a conserved region in the N-terminus of DGCR8, in a 2:2 stoichiometry. Knock-down of ERH or deletion of the DGCR8 N-terminus results in a reduced processing of suboptimal pri-miRNAs in polycistronic miRNA clusters. ERH increases the processing of suboptimal pri-miR-451 in a manner dependent on its neighboring pri-miR-144. Thus, the ERH dimer may mediate 'cluster assistance' in which Microprocessor is loaded onto a poor substrate with help from a high-affinity substrate in the same cluster. Our study reveals a role of ERH in the miRNA biogenesis pathway.

SUBMITTER: Kwon SC 

PROVIDER: S-EPMC7641749 | biostudies-literature | 2020 Nov

REPOSITORIES: biostudies-literature

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ERH facilitates microRNA maturation through the interaction with the N-terminus of DGCR8.

Kwon S Chul SC   Jang Harim H   Shen Siyuan S   Baek S Chan SC   Kim Kijun K   Yang Jihye J   Kim Jeesoo J   Kim Jong-Seo JS   Wang Suman S   Shi Yunyu Y   Li Fudong F   Kim V Narry VN  

Nucleic acids research 20201101 19


The microprocessor complex cleaves the primary transcript of microRNA (pri-miRNA) to initiate miRNA maturation. Microprocessor is known to consist of RNase III DROSHA and dsRNA-binding DGCR8. Here, we identify Enhancer of Rudimentary Homolog (ERH) as a new component of Microprocessor. Through a crystal structure and biochemical experiments, we reveal that ERH uses its hydrophobic groove to bind to a conserved region in the N-terminus of DGCR8, in a 2:2 stoichiometry. Knock-down of ERH or deletio  ...[more]

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